The Gut-Immune System and Hormones Role in Overall Wellness

Dive into the world of the gut-immune system and hormones and their crucial role in supporting immune health and overall wellness.

Abstract

I wrote this educational post to share how I moved from medication stacks to a systems-biology model that begins in the gut and extends through the immune, endocrine, and nervous systems. Drawing on modern methods such as metagenomic sequencing, metabolomics, intestinal permeability assays, and autonomic measures (e.g., HRV), I explain how dysbiosis, leaky gut, and LPS-driven inflammation disrupt estrogen metabolism, thyroid hormone conversion, insulin sensitivity, and mood. You will learn why supporting the estrobolome, optimizing vitamin D3–K2–A cofactors, and balancing iodine–selenium for thyroid are pivotal. I discuss practical protocols using diet, prebiotics, probiotics, butyrate support, DIM/I3C, calcium D-glucarate, glutamine, methylation cofactors, and, when appropriate, shilajit to sustain free testosterone. I also show where integrative chiropractic care fits: improving vagal tone, diaphragmatic mechanics, and autonomic balance to normalize motility, lower inflammation, and help good plans work. Throughout, I reference my clinical observations from ChiroMed and the latest findings from leading researchers, so you can see the rationale behind each step and apply this roadmap safely and effectively.

Why I Now Start With The Gut, Then Layer Hormones, Thyroid, And Structure

I trained in conventional models and spent years optimizing hormones and metabolism. I prescribed intensively, studied incretins and GLP-1, and did everything I could to improve diabetes and endocrine care. Many patients improved—but too many plateaued. The turning point came when I consistently addressed gut integrity and the neuroimmune axis first: patients’ medication burdens decreased, weight and energy normalized, and mood and cycles stabilized. When I dug deeper into the 25–30% who still struggled, I found a common thread: dysbiosis, intestinal permeability, and autonomic dysregulation blocked progress.
My clinical lesson: persistent symptoms usually reflect a convergence of microbiome imbalance, barrier dysfunction, immune activation, autonomic imbalance, and environmental mismatch. These systems converge in the gut. That’s why my care integrates functional nutrition, targeted supplementation, hormone and thyroid optimization, and integrative chiropractic to restore nervous system balance and biomechanics. Across my clinical work at ChiroMed and case reflections I share on LinkedIn, a gut-first framework reliably transforms outcomes (Jimenez, n.d.-a; Jimenez, n.d.-b).

The Gut Microbiome As A Neuroendocrine And Immune Control Center

The microbiome is a living organ system. In a healthy state, it:

Produces short-chain fatty acids (SCFAs)—especially butyrate, propionate, and acetate—that fuel colonocytes, tighten epithelial tight junctions, and tame inflammation (Canfora et al., 2019).
Trains GALT and regulatory T cells (Tregs), fostering immune tolerance (Turnbaugh & Gordon, 2019).
Maintains barrier integrity, preventing lipopolysaccharide (LPS) translocation and downstream TLR4–NF-κB signaling (Camilleri, 2019).
Modulates neurotransmitters and the HPA axis, influencing serotonin via enterochromaffin cells and stress resilience (Cryan & Dinan, 2015).
Shapes hormone metabolism, including the estrobolome, insulin sensitivity, and thyroid conversion.

When dysbiosis develops, we see reduced butyrate-producing bacteria, an excess of pathobionts, and elevated beta-glucuronidase—an enzyme that can deconjugate estrogens and promote estrogen recirculation. Clinically, this presents as bloating, irregular stools, acne, brain fog, fatigue, weight plateaus, and hormone therapy that “doesn’t stick.” Mechanistically, increased LPS fuels systemic inflammation and insulin resistance; reduced SCFAs loosen junctions and weaken mucosal defense; and neuroendocrine signaling drifts toward anxiety, low mood, and poor sleep.

Intestinal Permeability, Zonulin, and the Inflammation–Endocrine Loop

“Leaky gut” is a measurable phenomenon. Tight junctions—regulated by proteins like claudin, occludin, and zonulin—hold epithelial cells together. When zonulin rises in response to gluten, infections, dysbiosis, or stress, the junctions loosen, allowing dietary antigens and microbial fragments to enter the circulation (Fasano, 2012). The consequences:

Immune activation: Elevated TNF-α and IL-6 amplify systemic inflammation.
Endocrine disruption: Cytokines increase cortisol and insulin, blunt T4→T3 conversion, and alter sex hormone balance.
Metabolic effects: Raised insulin and cortisol promote fat storage and alter appetite circuits.

Repeated postprandial endotoxemia (LPS spikes after meals) is well documented with high-fat, ultra-processed diets, fueling insulin resistance and barrier erosion (Cani et al., 2007). In my practice, I routinely see elevated zonulin, LPS-binding protein, low SCFAs, and high beta-glucuronidase in stressed, symptomatic patients. When we seal the barrier and calm LPS, endocrine therapies begin to work the way we expect.

The Estrobolome, Beta-Glucuronidase, And Estrogen Recirculation

The estrobolome—the gut microbial genes that metabolize estrogens—determines whether estrogens are excreted or recirculated. In the liver, estrogens are conjugated (often glucuronidated) and excreted via bile. If the microbiome produces excess beta-glucuronidase, it deconjugates estrogens in the intestine, thereby enabling reabsorption through the intestinal wall (Plottel & Blaser, 2011; Flores et al., 2012). Add constipation, and you compound recirculation. Clinically, I see:

Worsened PMS, mastalgia, fibrocystic changes, and heavier cycles.
Frustration with hormone therapy due to increased metabolites returning to circulation.
Mood variability and breast density changes when the 2-OH:16-OH balance is unfavorable.

Supporting fiber, calcium D-glucarate, DIM/I3C, methylation cofactors, bile flow, and daily bowel movements can reverse this loop.

PCOS, Endometriosis, And The Gut–Hormone Axis

PCOS: Dysbiosis raises LPS and zonulin, driving inflammation and insulin resistance, which increases ovarian theca cell androgen production. Result: hyperandrogenism, anovulation, acne, and metabolic risk (Qi et al., 2022). When I rebuild the barrier, raise SCFAs, and add resistance training with targeted nutrition, fasting insulin drops, cycles stabilize, and skin clears.
Endometriosis: Elevated beta-glucuronidase and permeability raise circulating estrogen and pelvic inflammation. Estrogen metabolism favors 2-hydroxylation over proliferative or genotoxic pathways when supported with DIM, I3C, methylation, and glucuronidation aids (Yager & Davidson, 2006; Taylor et al., 2020). My patients often report lighter cycles and reduced pain when transit improves, and recirculation decreases.

Thyroid Conversion, Iodine–Selenium Synergy, and Hashimoto’s

Thyroid function hinges on substrate availability and redox safety:

Iodine is essential for T4/T3 synthesis, but it must be managed carefully—especially in autoimmune thyroiditis.
Selenium-dependent enzymes (glutathione peroxidases, deiodinases) detoxify H2O2 used by TPO and convert T4 to T3. Low selenium levels increase oxidative stress and can heighten antibody activity; supplementation can lower TPO antibody levels in some patients (Gärtner et al., 2002).

In Hashimoto’s, dysbiosis and intestinal permeability elevate cytokine levels, impairing T4→T3 conversion and nutrient absorption (Caturegli et al., 2014). Correcting the microbiome, supporting the barrier, and using vitamin D3–K2–A with magnesium (for vitamin D metabolism) improves immune tolerance and thyroid status. In my clinic, combining selenium (100–200 mcg/day) with gut repair and stress modulation often stabilizes symptoms and antibody trends.

Vitamin D3, K2, Magnesium, And Vitamin A: Directing Calcium And Calming Immunity

Many patients take vitamin D3 without cofactors. For safety and efficacy:

Magnesium supports the enzymes that convert D into its active forms.
Vitamin K2 (MK-7) activates osteocalcin and matrix Gla protein (MGP), directing calcium to bones and away from arteries (Beulens et al., 2013).
Vitamin A (retinol) works synergistically with D and K to balance bone remodeling and epithelial integrity.

I generally target 25(OH)D at 50–70 ng/mL, titrating based on labs, with D3 taken with fat and magnesium, plus K2 (and judicious vitamin A when indicated) (Pilz et al., 2019; Mitchell et al., 2022). Clinically, this reduces musculoskeletal aches, improves mood and immune balance, and safeguards vascular health during endocrine optimization.

Akkermansia, SCFAs, And Metabolic Flexibility

I pay close attention to Akkermansia muciniphila, a mucin-degrading bacterium associated with stronger mucus layers and better metabolic profiles. Low levels of Akkermansia correlate with barrier fragility and weight-loss resistance (Everard & Cani, 2013). When I support mucosal nutrition (polyphenols from berries and pomegranates; prebiotic fibers; omega-3s), Akkermansia often rebounds. When combined with fiber-induced SCFAs, patients regain insulin sensitivity, see improved fasting glucose, and break stubborn weight plateaus.

Evidence-Based Tools That Inform Personalization

Modern research methods help move from guesswork to precision:

Metagenomics identifies microbial composition and functional genes (e.g., SCFA producers, Enterobacteriaceae) to target interventions (Turnbaugh & Gordon, 2019).
Metabolomics measures functional outputs—such as SCFAs, bile acids, and indoles—to gauge progress.
Permeability assays (e.g., serum zonulin, lactulose/mannitol) and markers like LPS-binding protein quantify barrier function (Camilleri, 2019).
Neurogastroenterology and HRV assessments tailor autonomic and motility interventions (Tracey, 2002).

This data-driven approach, combined with clinical observation, improves accuracy, safety, and recovery speed.

Integrative Chiropractic Care: Why Structure And Autonomics Matter

As a chiropractor and nurse practitioner, I witness how biomechanics and the autonomic nervous system shape gut and endocrine function:

Vagal tone: Gentle cervical work, rib mechanics, diaphragmatic release, and paced breathing increase parasympathetic output, improving gastric accommodation and GI motility, while reducing visceral hypersensitivity.
Spinal and pelvic mechanics: Thoracolumbar and sacral segments modulate sympathetic and parasympathetic outflow to the GI tract; restoring mobility reduces nociceptive drive and systemic cytokine levels.
Movement prescriptions: Rhythmic aerobic work and resistance training improve insulin sensitivity and myokine profiles, enhancing metabolic resilience.

In my practice, adding HRV-guided breathing, diaphragmatic training, and targeted adjustments accelerates gut recovery and stabilizes mood and sleep. Structural integration is not optional; it is central to steady autonomic balance and endocrine stability (Tracey, 2002; Cryan & Dinan, 2015; Jimenez, n.d.-a; Jimenez, n.d.-b).

DIM, I3C, And Safer Estrogen Metabolism

Diindolylmethane (DIM) and indole-3-carbinol (I3C) help steer estrogen toward the 2-hydroxy (2-OH) pathway, away from 4-OH quinone-prone and 16-OH proliferative metabolites. Mechanisms include modulation of CYP enzymes and support of COMT-mediated methylation (Bradlow, 2019; Kabat et al., 2006). In practice:

Women: DIM 100–150 mg/day, titrating up to 300 mg/day when PMS, mastalgia, or estrogen dominance persists.
Men: DIM 300 mg/day, up to 600 mg/day in select prostate risk scenarios while monitoring.

I pair DIM with methylated B vitamins and sulforaphane (Nrf2 activation) to ensure conjugation and detox pathways keep pace (Singh et al., 2011). Clinically, patients report improved breast density profiles and better tolerance to HRT when DIM is maintained.

Calcium D-Glucarate, Methylation, Bile Flow, And Daily Excretion

To reduce beta-glucuronidase reactivation and enterohepatic recirculation, I use:

Calcium D-glucarate to support glucuronidation.
Methylation support (methylfolate, methylcobalamin, B6/P5P, TMG) to detoxify catechol estrogens and maintain COMT function—especially when 4-OH is elevated.
Bile flow support with bitters (e.g., gentian, dandelion) and hydration to carry conjugated estrogens into the intestine.
Transit optimization with fiber and gentle movement. Constipation is a nonstarter—daily bowel movements are mandatory for estrogen safety.

This Phase I–II–III strategy ensures metabolites are formed safely (Phase I), conjugated (Phase II), and eliminated (Phase III).

Glutamine, Zinc Carnosine, And Mucosal Repair

When permeability is high or mucosal stress is severe, I deploy:

L-glutamine to fuel enterocytes and bolster tight junction protein expression.
Zinc carnosine to stabilize mucosal surfaces and reduce oxidative stress (Ueda et al., 2007).
Omega-3s and demulcents as needed.

Patients often experience reduced bloating, better stool quality, and calmer skin when mucosal repair is prioritized.

Shilajit And Free Testosterone: Sustaining Benefits Across Pellet Cycles

Late in testosterone pellet cycles, many patients report symptom drift despite acceptable total testosterone. The culprit is often a decline in free testosterone, the bioavailable fraction that drives receptor signaling. Purified shilajit has shown significant increases in both total and free testosterone (e.g., ~31% and ~51% respectively at 250 mg twice daily in a randomized, placebo-controlled trial), likely via fulvic acid–mediated mitochondrial and transport effects (Pandit et al., 2016). In my clinic:
Adding purified shilajit during the latter half of a pellet cycle stabilizes free testosterone without pushing total levels into side-effect territory.
Patients report steadier energy, drive, and recovery.
I integrate shilajit into a comprehensive HRT support stack (DIM, methylated B’s, sulforaphane, CoQ10) to support balanced metabolism and oxidative protection.
For women with PCOS or androgen sensitivity, I avoid raising androgens and instead emphasize estrogen detoxification and an insulin-sensitizing lifestyle.

Practical, Stepwise Clinical Plan

Here is how I typically structure care:

Phase 1: Calm the fire
- Remove ultra-processed foods, dyes, and excess alcohol.
- Establish hydration, protein adequacy, and high-fiber, polyphenol-rich meals.
- Start multi-strain probiotics, prebiotics (inulin, FOS, GOS, resistant starch), and L-glutamine; add zinc carnosine if mucosal stress is evident.
- Begin paced breathing (≈6 breaths/min), humming or gargling, and chiropractic sessions to downshift sympathetic tone.
- Target sleep: a consistent schedule, a cool, dark room, and morning light.
Phase 2: Restore and rebalance
- Add DIM/I3C based on symptoms or metabolite data; support methylation (methylfolate, B12, B6, TMG).
- Introduce calcium D-glucarate for glucuronidation; enhance transit with diverse fibers.
- Train with progressive resistance (3x/week) and zone 2 cardio (2x/week).
- Ensure daily bowel movements and support bile flow with bitters.
Phase 3: Optimize and personalize
- Reassess stool metrics (zonulin, SCFAs, beta-glucuronidase, Akkermansia) and hormone metabolites.
- Correct nutrient deficits (vitamin D, magnesium, omega-3s, iron, zinc).
- Support Akkermansia with polyphenols and mucin-feeding fibers; maintain D3–K2–A for calcium handling and immune balance.
- For pellet-based HRT, consider shilajit to sustain free testosterone; for PCOS or estrogen dominance, lean on detox supports without increasing androgens.
- Maintain integrative chiropractic care to reinforce autonomic balance and movement quality.

Modulating Women’s Hormones- Video

Clinical Observations From My Practice

From my work at ChiroMed and professional updates I share on LinkedIn:

Patients with “great labs” but persistent symptoms often harbor dysbiosis, increased permeability, or elevated beta-glucuronidase—addressing these unlocks progress (Jimenez, n.d.-a; Jimenez, n.d.-b).
Pairing resistance training with gut repair stabilizes cycles and insulin in PCOS; skin and mood follow.
Akkermansia repletion tracks with breaking weight-loss plateaus, even after GLP-1 use.
Integrative chiropractic care improves adherence and resilience—when pain and sleep improve, nutrition and movement protocols stick, accelerating gut and hormone balance.

Why These Techniques Work: Physiology-First Reasoning

Prebiotics and fiber → raise SCFAs, especially butyrate, tightening junctions and lowering inflammatory signaling (Canfora et al., 2019). This reduces LPS leakage and stabilizes endocrine pathways.
Synbiotics (probiotics + prebiotics) → re-seed commensals and feed them, improving stool form, immune markers, and motility in IBS and dysbiosis.
Glutamine and zinc carnosine → restore epithelial energy and mucosal structure, lowering antigen translocation (Ueda et al., 2007).
DIM/I3C → steer estrogen toward 2-OH and away from 4-OH/16-OH, lowering quinone burden and proliferative signaling (Bradlow, 2019; Kabat et al., 2006).
Methylation support → completes detox of catechol estrogens and protects DNA via COMT and related pathways.
Calcium D-glucarate → promotes glucuronidation and reduces beta-glucuronidase-driven recirculation.
D3–K2–A with magnesium → improves immune modulation and calcium trafficking, protecting bone and vasculature (Beulens et al., 2013; Pilz et al., 2019; Mitchell et al., 2022).
Iodine with selenium → restores thyroid hormone synthesis while protecting against H2O2-driven oxidative damage; supports deiodinases (Gärtner et al., 2002; Zimmermann, 2003).
Shilajit → raises free testosterone and supports mitochondrial function, smoothing symptom curves across pellet cycles (Pandit et al., 2016).
Chiropractic-informed autonomic care → increases vagal tone and reduces nociception, lowering cytokines and improving motility, digestion, and sleep (Tracey, 2002; Cryan & Dinan, 2015).

Putting It All Together: A Gut-First, Whole-Person Strategy

When we respect the body’s systems biology, we see why a gut-first strategy with autonomic balance makes hormones and thyroid therapies work predictably. By:

Sealing the barrier and raising SCFAs,
Lowering LPS and cytokines,
Steering estrogen metabolism toward safer pathways with DIM/I3C and ensuring excretion with calcium D-glucarate, fiber, and bile flow,
Optimizing vitamin D3–K2–A with magnesium and carefully integrating iodine–selenium for thyroid,
Supporting bioavailable androgens with shilajit when appropriate,
And integrating chiropractic care to normalize autonomic tone and movement.

We consistently move patients from symptom management to durable health. This approach is practical, measurable, and aligned with modern, evidence-based methods. In my experience, it is also the fastest, safest way to feel well and stay well.

References

Microbiome and human health: from basic science to clinical applications (Turnbaugh, P. J., & Gordon, J. I., 2019). Nature Medicine.
Short-chain fatty acids and human health (Canfora, E. E., Wopereis, S., & Blaak, E. E., 2019). Trends in Endocrinology & Metabolism.
Gut barrier function and the microbiome (Camilleri, M., 2019). Nature Reviews Gastroenterology & Hepatology.
Microbiota and the brain: mechanisms of the gut–brain axis (Cryan, J. F., & Dinan, T. G., 2015). Nature Reviews Neuroscience.
Intestinal permeability and the pathophysiology of leaky gut (Fasano, A., 2012). Annals of the New York Academy of Sciences.
Metabolic endotoxemia initiates obesity and insulin resistance (Cani, P. D., et al., 2007). Diabetes.
The estrobolome and estrogen metabolism in health and disease (Plottel, C. S., & Blaser, M. J., 2011). Gut Microbes.
Gut microbiota, beta-glucuronidase, and estrogen metabolism (Flores, R. et al., 2012). Journal of Translational Medicine.
Endometriosis, inflammation, and the microbiome (Taylor, H. S., et al., 2020). Frontiers in Endocrinology.
Estrogen metabolism pathways and clinical implications (Yager, J. D., & Davidson, N. E., 2006). Nature Reviews Cancer.
Selenium supplementation and thyroid autoimmunity (Gärtner, R. et al., 2002). The Journal of Clinical Endocrinology & Metabolism.
Hashimoto’s thyroiditis: pathophysiology and management (Caturegli, P., De Remigis, A., & Rose, N. R., 2014). Endocrine Reviews.
Vitamin D and risk of disease: meta-analyses and randomized trials (Pilz, S., Trummer, C., Pandis, M., et al., 2019). Nature Reviews Endocrinology.
Global prevalence of vitamin D deficiency and health implications (Mitchell, E. et al., 2022). Nutrients.
Vitamin K2 in bone and cardiovascular health (Beulens, J. W. J., et al., 2013). Advances in Nutrition.
Iodine nutrition and thyroid disorders (Zimmermann, M. B., 2003). The Journal of Clinical Endocrinology & Metabolism.
Vagus nerve regulation of inflammation (Tracey, K. J., 2002). Nature Immunology.
Diindolylmethane: mechanisms of estrogen metabolism modulation and clinical applications (Bradlow, H. L., 2019). Phytotherapy Research.
The estrogen metabolite ratio and breast tissue risk (Kabat, G. C., et al., 2006). Cancer Epidemiology, Biomarkers & Prevention.
Sulforaphane, Nrf2 activation, and phase II detoxification (Singh, A. et al., 2011). Oncogene.
Shilajit and testosterone in healthy males: RCT (Pandit, R. et al., 2016). Andrologia.
Akkermansia muciniphila and metabolic health: evidence and mechanisms (Everard, A., & Cani, P. D., 2013). Nature Reviews Microbiology.
Zinc carnosine and mucosal healing (Ueda, Y. et al., 2007). Alimentary Pharmacology & Therapeutics.
The estrobolome and estrogen metabolism (Kwa, M. et al., 2018). Frontiers in Endocrinology.
Clinical observations and resources:
ChiroMed El Paso (Jimenez, A., n.d.-a).
Professional profile and practice updates (Jimenez, A., n.d.-b).

SEO tags: gut health, dysbiosis, intestinal permeability, LPS, SCFAs, estrobolome, beta-glucuronidase, estrogen metabolism, DIM, I3C, calcium D-glucarate, vitamin D3, vitamin K2, vitamin A, iodine, selenium, Hashimoto’s, thyroid conversion, Akkermansia muciniphila, shilajit, free testosterone, HRT pellets, integrative chiropractic care, vagal tone, HRV, functional medicine, microbiome sequencing, metabolomics, NF-κB, TLR4, COMT, Nrf2

April 16, 2026

Gut Health and Hormone Balance Treatment

Abstract

I am Dr. Alexander Jimenez, DC, APRN, FNP-BC, CFMP, IFMCP, ATN, CCST. In this educational post, I guide you through the science and practice of optimizing hormones by treating the gut–liver–hormone axis and reinforcing micronutrient and mitochondrial foundations. I explain how dysbiosis, intestinal permeability, and microbial enzymes like beta-glucuronidase reshape estrogen metabolism and influence conditions such as PCOS, endometriosis, and autoimmunity, and how lipopolysaccharide (LPS) and short-chain fatty acids (SCFAs) affect insulin sensitivity, mood, and inflammation. I translate current research on vitamin D, K2, iodine, selenium, methylated B vitamins, DIM, and shilajit into clinic-ready protocols, and I show where integrative chiropractic care fits by supporting vagal tone, motility, neuromusculoskeletal dynamics, and autonomic balance. You will find practical frameworks, dosing concepts, lab-monitoring advice, and rationale for each intervention, with citations to leading researchers.

Why Hormones Are Microbiome-Dependent: The Gut–Liver–Hormone Axis

When I first connected hormone symptoms to gut physiology, I saw a pattern: many “hormone” problems began as microbiome and barrier problems. The gut microbiome—a complex community of bacteria, viruses, fungi, and archaea—regulates digestion, immune tolerance, barrier integrity, and the enterohepatic circulation that clears estrogens. From the earliest studies linking metabolic endotoxemia to insulin resistance, it has become clear that LPS-driven inflammation can disrupt cardiometabolic and reproductive health (Cani et al., 2007).

When the microbiome is balanced, commensals generate SCFAs (notably butyrate) that nourish colonocytes, tighten junctions, and reduce inflammatory signaling.
When dysbiosis develops, beta-glucuronidase-producing taxa expand, and LPS permeates, amplifying NF-κB cytokine cascades that alter hormone receptors, hepatic detoxification, and insulin signaling (Fasano, 2012; Slyepchenko et al., 2017).

Clinically, if you manage estrogen symptoms, insulin resistance, or autoimmune patterns, you are managing the microbiome—whether you realize it or not.

Dysbiosis and Leaky Gut Explained: Distinct Problems that Reinforce Each Other

Two related but distinct issues commonly coexist:

Dysbiosis: A shift away from beneficial microbes, with loss of diversity and expansion of pathobionts. Consequences include increased LPS, altered bile acid signaling, and elevated beta-glucuronidase.
Leaky gut (increased intestinal permeability): Disruption of tight junction proteins (occludin, claudins, ZO-1) allows antigens and endotoxins to enter circulation, thereby increasing systemic inflammation and immune activation (Fasano, 2012).

Why that matters for hormones:

LPS activates TLR4–NF-κB, increasing TNF-α, IL-1β, and IL-6—cytokines that reduce insulin signaling and alter steroid hormone receptor function (Cani et al., 2007).
Permeability increases immune load and oxidative stress, thereby consuming methyl donors and glutathione needed for safe phase II detox (methylation, glucuronidation, sulfation) of estrogens.

I screen for these drivers whenever patients report PMS, heavy cycles, PCOS features, endometriosis pain, acne or hair loss, mood changes, fatigue, or autoimmune flares. Correcting the gut often increases the safety and efficacy of hormone therapy.

Estrogen Metabolism 101: Enterohepatic Circulation and the Estrobolome

The liver metabolizes estrogens via phase I hydroxylation (CYP1A1, CYP1B1) and phase II conjugation (COMT methylation, glucuronidation, sulfation). Conjugated metabolites pass into bile and should be excreted. In dysbiosis, microbial beta-glucuronidase deconjugates these estrogens, promoting reabsorption and recirculation—the biochemical basis of “estrogen dominance,” even with careful dosing (Plottel & Blaser, 2011).

2-hydroxylation generally produces less proliferative metabolites.
4- and 16α-hydroxylation yield more proliferative or potentially genotoxic metabolites if methylation and conjugation are suboptimal.

In complex cases or when there is a family history of estrogen-dependent cancers, I consider urinary metabolite testing to map pathways and guide targeted support.

PCOS, Endometriosis, and Autoimmunity: What the Microbiome Adds

Recent studies sharpen the microbiome’s role:

PCOS: Dysbiosis with fewer SCFA producers and higher LPS correlates with insulin resistance, hyperandrogenism, and impaired GLP-1 signaling (Lindheim et al., 2017; Qi et al., 2019). Restoring butyrate producers improves metabolic tone.
Endometriosis: Altered microbiota, increased permeability, and immune activation correlate with symptom severity. Increased beta-glucuronidase raises estrogen recirculation that can exacerbate lesions and pain (Chen et al., 2017; Jiang et al., 2017).
Autoimmunity: Barrier dysfunction and loss of tolerogenic species permit pathobiont translocation and molecular mimicry, priming autoimmune activity (Manfredo Vieira et al., 2018).

Clinical translation: Addressing the gut can reduce hormone dosing requirements, expand the therapeutic window, and stabilize mood, sleep, and metabolism.

The Simple Question with Big Impact: Are You Pooping Daily?

I ask every patient: “Do you have a daily bowel movement?”

Estrogen metabolites exit via bile and stool. Constipation increases residence time, giving beta-glucuronidase more opportunity to deconjugate and recirculate estrogens.
Correcting bowel habits is a core risk-reduction strategy for estrogen-driven conditions.

Practical steps I use:

Increase hydration and electrolytes.
Ramp fiber to 25–35 g/day; add PHGG (partially hydrolyzed guar gum) 4–6 g/day for low-bloat prebiotic support.
Add magnesium glycinate or citrate at night for stool regularity and sleep.
Encourage postprandial walks and vagal toning (slow exhale breathing, humming).

A 3-by-3 Framework for Gut Repair: Remove, Replace, Repair

To keep things doable, I use a 3-by-3 approach:

Remove/Reduce Irritants

Clean up the diet: favor whole foods; limit alcohol, ultra-processed items, added sugars; consider a gluten-light or gluten-free trial for sensitive individuals.
Medication review: minimize NSAIDs and PPI overuse when clinically safe.
Stress load: hard-wire breath work, walks, and sleep hygiene.

Replace and Restore

Fiber and prebiotics: 25–35 g/day total fiber; add PHGG for gentle SCFA support.
Probiotics: multi-strain Lactobacillus and Bifidobacterium blends (e.g., L. rhamnosus GG, B. lactis) for barrier and immune balance.
Digestive support: bitters and meal hygiene for hypochlorhydria/slow motility; phosphatidylcholine and balanced fats for bile flow.

Repair and Rebalance

Barrier repair: L-glutamine 5 g/day, zinc carnosine, N-acetyl-D-glucosamine, omega-3s as indicated.
Inflammation control: Berberine for dysbiosis-associated endotoxemia; curcumin and quercetin for NF-κB calming.
Lifestyle anchors: 150 minutes/week activity; 10-minute post-meal walks; consistent 7–9 hours of sleep.

Why this approach works:

Prebiotics increase SCFAs, reinforce tight junctions, and support T-regs via HDAC inhibition.
Probiotics competitively inhibit pathobionts, reduce beta-glucuronidase activity, and enhance mucosal IgA.
L-glutamine fuels enterocytes and accelerates barrier recovery.
Berberine improves the microbial balance and activates AMPK to improve insulin sensitivity.

Nutrient Foundations for Receptor-Level Hormone Action: D, K2, A, Magnesium, Iodine, Selenium, and Methylation

I frequently see patients with robust serum hormones but poor tissue effects. The missing link is often receptor signaling, cofactors, and membranes.

Vitamin D3 behaves like a secosteroid hormone that modulates transcription through the VDR. Low vitamin D is associated with all-cause and cardiovascular mortality and can blunt androgen signaling even when total testosterone appears normal (Pilz et al., 2011; Holick, 2017).
Magnesium is a cofactor for D activation (25- and 1α-hydroxylases); deficiency dampens VDR signaling (Rosanoff et al., 2016).
Vitamin K2 directs calcium into bone and away from soft tissues by activating matrix Gla protein and osteocalcin; it complements D to protect vessels and build bone (Schurgers & Vermeer, 2000; Beulens et al., 2013).
Vitamin A supports epithelial integrity, immune balance, and nuclear receptor synergy with vitamin D.

I often use an ADK formula (D3 with K2 and A) alongside magnesium to safely improve receptor-mediated effects, while monitoring 25(OH)D, calcium, and PTH (Rosen et al., 2012).

Thyroid resilience: iodine and selenium synergy

Iodine is essential for T4/T3 synthesis, but safe utilization depends on selenium-dependent enzymes (glutathione peroxidases, thioredoxin reductases) to quench the H2O2 generated during iodide organification (Ventura et al., 2017).
Inadequate selenium increases oxidative stress at the thyroid, raising the risk of autoimmunity when iodine intake rises (Gartner & Gasnier, 2003).
I pair iodine (200–400 mcg) with selenium (100–200 mcg selenomethionine) and often zinc (10–30 mg), titrated to labs and symptoms (Zimmermann & Boelaert, 2015).

Methylation for estrogen safety

Methylated B vitamins—methylfolate and methylcobalamin—support COMT-mediated methylation of catechol estrogens, reducing genotoxic stress and stabilizing phase II clearance.

These micronutrients are the bedrock that allows hormones to “dock” and trigger healthy cellular responses.

DIM and Estrogen Metabolites: Steering Toward Safer Pathways

Diindolylmethane (DIM) shifts estrogen metabolism toward 2-hydroxylation and away from 16α- and 4-hydroxylation pathways associated with proliferative and genotoxic risk (Zeligs et al., 2006; Reed et al., 2006). Preclinical studies suggest that DIM may also upregulate BRCA1 signaling and promote apoptosis in cancer cell lines (Fan et al., 2009; Li et al., 2010).

How I apply it:

Women with estrogen-dominant symptoms or unfavorable metabolite profiles: 150–300 mg/day, adjusted to labs and tolerance.
Men with prostate risk or aromatization-driven symptoms: 300–600 mg/day, personalized.
I pair DIM with omega-3s, iodine/selenium, and fiber/probiotics to support the entire estrobolome–liver–stool axis.

Rationale: By changing metabolite balance and supporting conjugation, DIM decreases receptor overstimulation and DNA-adduct risk while improving symptom stability.

Shilajit for Free Testosterone and Mitochondrial Support

Some patients—particularly young males—present with high total testosterone but low free testosterone and low vitality. Shilajit, a purified, fulvic-acid–rich resin, has randomized data showing increases in total (~31%), free (~51%), and DHT (~37%) over ~90 days at 250 mg twice daily (Pandit et al., 2016). Mechanisms likely include improved mitochondrial function, nutrient transport, and hypothalamic–pituitary–gonadal signaling.

How I use it:

In those seeking endogenous support without exogenous hormones, I combine shilajit with vitamin D, magnesium, zinc, B12, and iodine/selenium when indicated, then track changes in free T, SHBG, energy, and body composition.

Why this works: Enhancing mitochondrial ATP and cofactor availability raises tissue responsiveness; changes in binding dynamics can increase the bioactive fraction without pushing total testosterone to excessive levels.

Vitamin D as a Systemic Modulator: Barrier, Immunity, and Receptors

I routinely optimize vitamin D because it acts at the intersection of immunity, barrier integrity, and endocrine signaling. Observational data tie suboptimal 25(OH)D to higher risks across diseases (Bouillon et al., 2019). Mechanistically, D supports tight junction proteins, cathelicidin, and endocrine receptor sensitivity. Clinically, many patients feel “stuck” until D is restored to an optimal range; I often target 60–80 ng/mL with appropriate monitoring to avoid hypercalcemia (Holick, 2017; Rosen et al., 2012).

Integrative Chiropractic Care: The Neuroimmune–Endocrine Interface

As a chiropractor and nurse practitioner, I see daily how autonomic balance, fascial mobility, and pain modulation determine whether patients can absorb nutrients, move consistently, and sleep well—foundations for endocrine success.

Vagal tone and motility: Gentle spinal and cervical adjustments can influence autonomic balance, improving gut motility, secretory IgA, and anti-inflammatory vagal pathways. Patients with low vagal tone present with constipation, bloating, and poor stress resilience.
Fascia and diaphragm: Thoracolumbar fascial restrictions and diaphragmatic stiffness impair breathing mechanics and lymphatic flow, promoting sympathetic overdrive. Mobility restores circulation and reduces pain.
Pain reduction without NSAIDs: Lowering nociception decreases cortisol and protects the mucosa from NSAID-induced permeability.
Behavioral activation: When pain decreases, patients walk, train, and sleep—activities that increase SCFAs, improve insulin sensitivity, and stabilize mood.

These neurophysiologic effects align with published observations on autonomic modulation and musculoskeletal care (Pickar, 2002; Lehman et al., 2012) and help nutrition and endocrine strategies “stick” in daily life.

For examples of how we operationalize this, see my resources at Chiromed and my professional updates on LinkedIn.

A Phased, Clinic-Ready Protocol for Gut and Hormone Optimization

I layer care to build momentum and safety.

Phase 1: Stabilize and Build Trust (Weeks 0–4)

Ensure daily bowel movements; add PHGG, hydration, and magnesium as needed.
Start a multi-strain probiotic (Lactobacillus + Bifidobacterium).
Begin vitamin D3 with K2 and magnesium; consider ADK formulations.
Introduce walks after meals and fixed sleep schedules.
Provide chiropractic adjustments and diaphragmatic work to normalize autonomics and reduce pain.
Baseline labs: CBC, CMP, 25(OH)D, calcium, PTH, thyroid panel (TSH, free T4/T3), thyroid antibodies as needed, ferritin, B12, folate, magnesium, zinc, selenium, CRP, fasting insulin/glucose, lipid profile, estradiol, total and free testosterone, SHBG.

Phase 2: Targeted Gut Repair and Hormone Pathways (Weeks 4–12)

Add L-glutamine 5 g/day for barrier support when indicated.
Short berberine course for endotoxemia/dysbiosis; replete with probiotics.
Add DIM if clinical or metabolite data show proliferative pathways.
Start a methylated B complex to support COMT and phase II detox.
Maintain chiropractic care cadence for autonomic and biomechanical resilience.

Phase 3: Personalize, Monitor, and Maintain (Months 3+)

Reassess symptoms, bowel habits, and targeted labs; titrate to the lowest effective doses.
Reinforce lifestyle anchors: fiber intake, movement, sleep, and stress practices.
Schedule periodic tune-ups for the spine, fascia, and breath mechanics to sustain vagal tone and support recovery.

This sequencing respects physiology and behavior: patients feel better first, then commit to more significant changes—resulting in better adherence and durable outcomes.

Special Focus: PCOS and Endometriosis

PCOS

Emphasize insulin sensitization through fiber, postprandial walks, resistance training, and, where appropriate, berberine.
Reduce LPS: probiotics, polyphenols, and barrier repair to lower endotoxemia.
Consider inositols for ovulatory support alongside gut therapy.
Monitor androgenic symptoms as gut protocols progress; improvements often track with better bile acid and SCFA signaling.

Endometriosis

Reduce beta-glucuronidase pressure via probiotics and fiber to limit estrogen recirculation.
Calm neuroimmune inflammation with omega-3s, curcumin, and sleep optimization.
Use gentle movement and manual therapy to address pelvic floor tension and diaphragm mobility; sympathetic downshift reduces pain tone.
Coordinate with gynecology; gut protocols augment, not replace, indicated care.

Case Reflection: High Total Testosterone, Low Vitality

I saw an 18–19-year-old male with low mood, low energy, weight gain, and “low-T” symptoms. His total testosterone was ~900 ng/dL—clearly not low. What we found: very low vitamin D, low B12, and signs of micronutrient insufficiency. I started a robust B-complex, ADK (D3 + K2 + A), iodine paired with selenium, and magnesium. At follow-up, his mother said, “He’s a totally different person.” Energy, mood, and cognition improved, and multiple medications were discontinued. The physiology: hormones were present, but receptor signaling and cellular machinery were underpowered. Restoring micronutrients enabled the hormones to “work.”

In other young men with high total but low free testosterone, I have added shilajit and structured resistance training. Free fractions improved, and vitality followed—without pushing total testosterone into excess.

Safety, Lab Monitoring, and Personalization

Monitor: 25(OH)D, calcium, PTH for vitamin D repletion; thyroid panel and antibodies for iodine–selenium strategies; ferritin, B12, folate, magnesium, zinc, selenium, CRP for micronutrient and inflammatory status; sex hormones including free testosterone and SHBG.
Adjust doses to labs and symptoms. If vitamin D stays low despite oral dosing, assess bile flow, fat absorption, and adherence; consider supervised loading.
Cautions:
- Vitamin A: avoid hypervitaminosis; use caution in pregnancy.
- Iodine: go slowly with autonomous nodules or hyperthyroidism; collaborate with endocrinology.
- Zinc: long-term high dosing can lower copper; keep the balance.
- DIM and shilajit: use third-party-tested products; personalize the dose.
- Berberine: short targeted courses; watch for GI sensitivity and drug interactions.

How Integrative Chiropractic Care Complements Endocrine and Gut Strategies

Mechanistically, chiropractic-informed care bridges biochemistry and behavior:

Reduces nociception and sympathetic overdrive, lowering cortisol drag on thyroid conversion and gonadal axes (Lehman et al., 2012).
Improves respiratory mechanics and fascial glide, supporting lymphatic flow, nutrient delivery, and waste clearance.
Enhances vagal tone, supporting motility, secretory IgA, and peristalsis—foundations for microbiome stability.
Facilitates movement prescriptions (resistance training, mobility, aerobic intervals) that reduce aromatase activity, improve insulin sensitivity, and raise androgen receptor density.

In my practice, patients combining endocrine protocols with spinal–fascial optimization report better sleep, steadier energy, more predictable lab trajectories, and lower required doses—an elegant synergy of systems biology and hands-on care. Explore our integrative approach at Chiromed and my professional notes on LinkedIn.

Why Each Technique Matters: Systems Biology Rationale

Fiber/PHGG: Feeds SCFA producers, tightens junctions, and supports GLP-1 signaling.
Probiotics: Reduce beta-glucuronidase, improve barrier integrity, and temper endotoxemia.
L-glutamine: Primary fuel for enterocytes; accelerates epithelial repair.
Berberine: Reshapes the gut microbiota, lowers LPS levels, and activates AMPK to improve insulin sensitivity.
DIM: Steers estrogen toward 2-hydroxylation, lowering proliferative load.
Methylated B vitamins: Enable COMT activity and conjugation; reduce genotoxicity of catechol estrogens.
Vitamin D + K2 + A + Mg: Align receptor signaling and calcium kinetics; protect vessels and bone.
Iodine + selenium: Support thyroid synthesis while detoxifying H2O2 to prevent autoimmune escalation.
Shilajit: Enhances endogenous androgens via mitochondrial and HPG-axis support.
Chiropractic care: Normalizes autonomic function, reduces pain, and supports movement habits that sustain microbiome and endocrine gains.

Each intervention nudges a different lever; together, they realign the system.

Clinical Observations from Practice

Across patient cohorts at my clinic, we see reproducible patterns:

Resolving constipation reduces PMS and “estrogen rollercoaster” symptoms within weeks.
Regular adjustments correlate with improved sleep and stress tolerance, enabling consistent training and meal timing that benefit the microbiome.
Vitamin D optimization often coincides with improved mood, less joint pain, and better responses to both gut and hormone protocols.

These observations are consistent with the mechanistic and clinical literature, reinforcing the rationale for why foundational steps deliver outsized results. For more, visit Chiromed and my LinkedIn updates.

References

Bouillon, R., Marcocci, C., Carmeliet, G., Bikle, D., White, J. H., Dawson-Hughes, B., Lips, P., Munns, C. F., Lazaretti-Castro, M., Giustina, A., & Bilezikian, J. (2019). Skeletal and extraskeletal actions of vitamin D: Current evidence and outstanding questions. Endocrine Reviews, 40(4), 1109–1151.
Cani, P. D., Amar, J., Iglesias, M. A., Poggi, M., Knauf, C., Bastelica, D., Neyrinck, A. M., Fava, F., Tuohy, K. M., Chabo, C., et al. (2007). Metabolic endotoxemia initiates obesity and insulin resistance. Diabetes, 56(7), 1761–1772.
Chen, C., Song, X., Wei, W., & Zhong, H. (2017). The role of the gut microbiota in the pathogenesis of endometriosis. Digestive Diseases and Sciences, 62(9), 2345–2355.
Fasano, A. (2012). Leaky gut and autoimmune diseases. Clinical Reviews in Allergy & Immunology, 42(1), 71–78.
Holick, M. F. (2017). The vitamin D deficiency pandemic: Approaches for diagnosis, treatment and prevention. Reviews in Endocrine and Metabolic Disorders, 18, 153–165.
Jiang, I., Desailloud, R., & Rousset, B. (2017). Gut microbiota and endometriosis: A bidirectional relationship. Best Practice & Research Clinical Endocrinology & Metabolism, 31(4), 613–621.
Lindheim, L., Bashir, M., Münzker, J., Trummer, C., Zachhuber, V., Pieber, T. R., Gorkiewicz, G., Höfner, G., Jesner, R., & Obermayer-Pietsch, B. (2017). The gut microbiome: A key player in the pathophysiology of PCOS. Endocrine, 58(3), 467–479.
Manfredo Vieira, S., Hiltensperger, M., Kumar, V., Zegarra-Ruiz, D., Dehner, C., Khan, N., Costa, F. R. C., Tiniakou, E., Greiling, T. M. S., Ruff, W. E., & Kriegel, M. A. (2018). Translocation of a gut pathobiont drives autoimmunity in the presence of other triggers. Science, 359(6380), 1156–1161.
Pandit, S., et al. (2016). Clinical evaluation of purified shilajit in healthy volunteers: Effects on testosterone and gonadotropic hormones. Andrologia, 48(5), 570–575.
Pilz, S., et al. (2011). Vitamin D and mortality in older men and women. Clinical Endocrinology, 75(3), 341–347.
Plottel, C. S., & Blaser, M. J. (2011). Microbiome and malignancy. Nature Reviews Cancer, 11(11), 782–792.
Reed, G. A., et al. (2006). Single-dose pharmacokinetics and tolerability of absorption-enhanced 3,3′-diindolylmethane. Cancer Epidemiology, Biomarkers & Prevention, 15(12), 2477–2481.
Rosen, C. J., et al. (2012). Calcium and vitamin D supplementation revisited. Journal of Bone and Mineral Research, 27(2), 223–230.
Rosanoff, A., Weaver, C. M., & Rude, R. K. (2016). Suboptimal magnesium status in the United States: Are the health consequences underestimated? Nutrition Reviews, 74(3), 169–182.
Schurgers, L. J., & Vermeer, C. (2000). Determination of gamma-carboxyglutamic acid residues in proteins by HPLC. Thrombosis and Haemostasis, 84(6), 958–962.
Beulens, J. W., et al. (2013). Vitamin K intake and all-cause mortality in The Netherlands. Journal of Nutrition, 143(6), 1029–1035.
Fan, S., et al. (2009). BRCA1 and BRCA2 as primary targets for chemoprevention of breast cancer. Journal of Cellular Biochemistry, 106(1), 24–32.
Li, Y., et al. (2010). Indole-3-carbinol and DIM in cancer prevention and therapy. Anti-Cancer Agents in Medicinal Chemistry, 10(9), 727–731.
Qi, X., Yun, C., Pang, Y., & Qiao, J. (2019). The impact of the gut microbiota on the cardiovascular system and obesity. Frontiers in Microbiology, 10, 2155.
Slyepchenko, A., et al. (2017). Tryptophan catabolites, inflammation, and the gut–brain axis in depression. Progress in Neuro-Psychopharmacology & Biological Psychiatry, 80, 1–19.
Calder, P. C. (2015). Marine omega-3 fatty acids and inflammatory processes: Effects, mechanisms and clinical relevance. Biochimica et Biophysica Acta, 1851(4), 469–484.
Gartner, R., & Gasnier, B. C. (2003). Selenium in the treatment of autoimmune thyroiditis. BioFactors, 19(3–4), 145–152.
Ventura, M., et al. (2017). Selenium and thyroid disease: From pathophysiology to clinical evidence. Acta Clinica Belgica, 72(5), 326–333.
Zimmermann, M. B., & Boelaert, K. (2015). Iodine deficiency and thyroid disorders. The Lancet Diabetes & Endocrinology, 3(4), 286–295.
Pickar, J. G. (2002). Neurophysiological effects of spinal manipulation. The Spine Journal, 2(5), 357–371.
Lehman, G. J., et al. (2012). The role of spinal manipulation in modulating pain and autonomic function. Journal of Manipulative and Physiological Therapeutics, 35(8), 611–623.

April 2, 2026

The Clinical Approach to Endocrine Health & Hormonal Balance

Learn about hormone optimization and its impact on health in this comprehensive look at the clinical approach to hormonal balance.

Introduction & Abstraction

As a Doctor of Chiropractic (DC) and a board-certified Family Nurse Practitioner (FNP-BC, APRN), I have pursued a clinical journey of continuous learning and integration. At our clinic, Injury Medical & Chiropractic Clinic, we observe the complex interplay of the human body daily. This educational post distills that experience and combines it with the groundbreaking work of leading researchers in functional and integrative medicine. We will move beyond the traditional, symptom-based model to explore the deep physiological underpinnings of health and disease. This is not a lecture, but a narrative exploration of modern, evidence-based research, designed to empower both practitioners and the health-conscious public.
Our journey begins at the cellular level, examining the critical role of the cell membrane. We will explore how its health, particularly the balance of essential fatty acids such as Omega-6 and Omega-3, dictates the body’s inflammatory state. You will learn why the standard Western diet, with its skewed fatty acid ratio, is a primary driver of chronic, low-grade inflammation, and how this “silent” inflammation is the bedrock for a host of chronic diseases, from cardiovascular conditions to autoimmune disorders. We will dissect the biochemical pathways of eicosanoids, understanding how arachidonic acid (an Omega-6 fatty acid) fuels pro-inflammatory cascades, while EPA and DHA (Omega-3 Fatty Acids) generate powerful anti-inflammatory and pro-resolving molecules called resolvins and protectins.
From there, we will transition to the gut, the “second brain” and the epicenter of our immune system. We will delve into the concept of intestinal permeability, or “leaky gut,” and explain how a compromised gut barrier allows undigested food particles, toxins, and bacterial components such as lipopolysaccharides (LPS) to enter the bloodstream. This breach triggers a systemic inflammatory response that can manifest in myriad ways, including joint pain, brain fog, skin issues, and autoimmune flare-ups. We will discuss the crucial role of the gut microbiome and how imbalances, or dysbiosis, contribute to this breakdown. Furthermore, we will illuminate the critical connection between gut health and hormonal balance, with a specific focus on the estrobolome—the collection of gut bacteria capable of metabolizing estrogens—and its profound impact on conditions such as estrogen dominance.
Finally, we will integrate these concepts into a holistic clinical framework. We will discuss the vital importance of detoxification, not as a fad but as a fundamental biological process essential for clearing hormonal metabolites, environmental toxins, and inflammatory byproducts. We’ll examine the phases of liver detoxification and the key nutrients required for their optimal function. This comprehensive understanding leads us to the 4R Program for gut restoration—Remove, Replace, Reinoculate, and Repair—a systematic, evidence-based protocol to heal the gut lining, rebalance the microbiome, and quench systemic inflammation. Through this detailed exploration, we aim to provide a clear, actionable roadmap for understanding and addressing the root causes of chronic illness, moving from cellular inflammation to systemic wellness. This is the future of proactive, personalized healthcare.

Navigating the Modern Health Landscape: A Clinician’s Perspective

Welcome. As both a chiropractor and a family nurse practitioner, I stand at a unique crossroads in healthcare. My days are filled with the narratives of patients whose stories, while unique, often share common threads of chronic pain, fatigue, and a frustrating search for answers. At our clinic, we’ve learned that looking at the site of pain is only the beginning. The real story is often written at a much deeper, cellular level. The purpose of this discussion is to share with you what we, as clinicians and researchers, are learning about the fundamental drivers of health and disease in the 21st century. We’re moving past the “a pill for every ill” mindset and into a new era of evidence-based, systems-based medicine. We are not just managing symptoms; we are investigating and addressing the root causes.
The insights I’m presenting today are not just my own but are built upon the pioneering work of leading researchers in functional medicine. These are the individuals meticulously mapping the biochemical pathways that connect our diet, environment, and genes to our overall health. Through modern, evidence-based research methods—from randomized controlled trials to advanced metabolomic profiling—they are providing the “why” behind what we observe clinically. My goal is to translate this complex science into a clear, understandable narrative, weaving in my own clinical observations to illustrate how these concepts play out in real people. We will journey from the microscopic world of the cell membrane to the complex ecosystem of the gut, and finally, to the systemic influence of our hormones, creating a holistic map of human health.

The Cell Membrane: Ground Zero for Inflammation

When a patient comes into my office with chronic joint pain, brain fog, or persistent fatigue, my investigation begins at the most fundamental unit of their body: the cell. More specifically, I focus on the cell membrane. This isn’t just a passive bag holding the cell’s contents; it’s a dynamic, intelligent gatekeeper that controls everything that enters and exits. It’s the communication hub, receiving signals from hormones, neurotransmitters, and immune messengers. The health and fluidity of this membrane dictate the health of the cell, and by extension, the health of the entire organism.

The Omega-6 and Omega-3 Imbalance: Fueling the Fire

The cell membrane is primarily composed of a phospholipid bilayer. Embedded within this layer is our diet, which directly influences various types of fats and their composition. This is where the story of modern chronic disease truly begins, with two key players: Omega-6 fatty acids and Omega-3 fatty acids.
Both are polyunsaturated fatty acids (PUFAs) and are considered essential, meaning our bodies cannot produce them; we must obtain them from our food.

Omega-6 Fatty Acids: The primary Omega-6 is linoleic acid (LA), which is abundant in industrial seed oils like soybean, corn, safflower, and sunflower oil. When consumed, LA can be converted into arachidonic acid (AA).
Omega-3 Fatty acids: The primary plant-based Omega-3 is alpha-linolenic acid (ALA), found in flaxseeds, chia seeds, and walnuts. However, the most biologically active forms are eicosapentaenoic acid (EPA) and docosahexaenoic acid (DHA), which are found predominantly in fatty, cold-water fish and algae.

From an evolutionary perspective, our ancestors consumed a diet in which the ratio of Omega-6 to Omega-3 was approximately 1:1 or 2:1, providing a balanced inflammatory potential. The modern Western diet, however, has completely upended this balance. With the proliferation of processed foods and industrial seed oils, the average ratio today is estimated to range from 15:1 to 25:1.
This dramatic shift is not trivial. It has profound and devastating consequences for our cellular health. When the cell membrane is overloaded with arachidonic acid due to excess Omega-6s, the cell is primed for an aggressive inflammatory response. Think of it as having a pile of dry, flammable kindling surrounding every cell in your body.

Eicosanoids: The Messengers of Inflammation and Resolution

When a cell experiences stress or injury—whether from a physical trauma, a pathogen, or a toxin—enzymes like phospholipase A2 (PLA2) are activated. PLA2 cleaves fatty acids from the cell membrane, making them available for conversion into powerful signaling molecules called eicosanoids.
The type of eicosanoid produced depends entirely on the fatty acid that was cleaved:

From Arachidonic Acid (Omega-6): The enzymes cyclooxygenase (COX) and lipoxygenase (LOX) convert AA into highly pro-inflammatory eicosanoids. These include:
- Prostaglandin E2 (PGE2): Promotes pain, fever, and inflammation. This is the target of NSAID drugs like ibuprofen.
- Thromboxane A2 (TXA2): Promotes blood clotting and vasoconstriction.
- Leukotriene B4 (LTB4): A powerful chemoattractant that recruits immune cells to the site of injury, amplifying the inflammatory response.
From EPA and DHA (Omega-3): These fatty acids are converted into a different class of signaling molecules that are either less inflammatory or, more importantly, are actively anti-inflammatory and pro-resolving.
- EPA competes with AA for the same COX and LOX enzymes, producing less inflammatory prostaglandins (like PGE3) and leukotrienes (like LTB5).
- Crucially, EPA and DHA are precursors to a specialized class of molecules known as Specialized Pro-resolving Mediators (SPMs). These include resolvins, protectins, and maresins.

Resolvins and Protectins: The “Off-Switch” for Inflammation

For decades, we believed that inflammation “faded away.” Groundbreaking research has shown this is incorrect. The resolution of inflammation is an active, highly orchestrated biological process, and SPMs are the conductors.
While the initial inflammatory response is essential for dealing with acute threats—clearing pathogens and debris—it is designed to be a short-term event. The problem in chronic disease is that this “on-switch” is stuck. The flood of Omega-6s keeps producing pro-inflammatory signals, while a deficiency of Omega-3s means we lack the raw materials to produce the “off-switch” signals.
Resolvins and protectins do not block inflammation in the way a drug like an NSAID does. Instead, they actively resolve it. Their functions include:

Stopping the recruitment of neutrophils (a type of inflammatory white blood cell).
Promoting the clearance of dead cells and debris by macrophages (a process called efferocytosis).
Enhancing microbial killing.
Reducing pain signals.

In my clinical practice, I see the effects of this imbalance daily. A patient with rheumatoid arthritis, for example, is experiencing a classic inflammatory cascade driven by an overabundance of pro-inflammatory eicosanoids. While conventional treatment might focus on suppressing the immune system or blocking the COX enzymes, a functional approach seeks to rebalance the underlying fatty acid composition of their cell membranes. By significantly increasing their intake of EPA and DHA and reducing their intake of industrial Omega-6s, we provide the body with the necessary building blocks to manufacture its own powerful, endogenous anti-inflammatory and resolvin agents. This is not just masking the symptoms; it is addressing the fire at its source.

The Gut: Your Body’s Grand Central Station

If the cell membrane is ground zero for inflammation, the gastrointestinal tract is the command center that often determines whether that inflammation becomes a local skirmish or a full-blown systemic war. The gut is far more than a simple tube for digestion. It houses over 70% of our immune system, contains a vast neural network often called the “second brain,” and is home to a complex ecosystem of trillions of microorganisms known as the gut microbiome. The health of this intricate system is paramount to overall health, and its dysfunction is a root cause of countless chronic conditions I see in my clinic.

Intestinal Permeability: When the Wall Is Breached

The lining of our small intestine is a remarkable structure. It has the surface area of a tennis court, yet it is only one cell thick. This single layer of epithelial cells is held together by protein structures called tight junctions. These junctions act as a highly selective barrier, meticulously controlling what passes from the gut lumen into the bloodstream. In a healthy state, only fully digested nutrients, water, and electrolytes are allowed through.
Intestinal permeability, colloquially known as “leaky gut,” occurs when these tight junctions become loose or damaged. This allows larger, undigested food particles, toxins, and bacterial components to “leak” into the bloodstream, where they do not belong.
When these foreign invaders enter the circulation, the immune system, which is heavily concentrated just on the other side of this gut wall (in an area called the Gut-Associated Lymphoid Tissue, or GALT), identifies them as hostile. It mounts a powerful immune response, releasing a flood of inflammatory cytokines like Tumor Necrosis Factor-alpha (TNF-α), Interleukin-6 (IL-6), and Interleukin-1 (IL-1).
This is a critical point: the inflammation is no longer contained within the gut. These cytokines travel throughout the body, creating a state of chronic, low-grade systemic inflammation.

This inflammation can manifest in the joints as arthritis.
It can cross the blood-brain barrier, contributing to brain fog, anxiety, depression, and even neurodegenerative diseases.
It can appear on the skin as eczema, psoriasis, or acne.
It can trigger or exacerbate autoimmune diseases like Hashimoto’s thyroiditis, lupus, or multiple sclerosis.

In our clinic, when a patient presents with widespread, seemingly unrelated symptoms, one of my first lines of inquiry is the patient’s gut health. A 45-year-old woman with joint pain, migraines, and fatigue might have been told she has fibromyalgia. But when we dig deeper, we often find a history of antibiotic use, a diet high in processed foods, and chronic stress—all major contributors to leaky gut.

The Role of Zonulin and Lipopolysaccharide (LPS)

Two key molecules are central to the science of leaky gut: zonulin and lipopolysaccharide (LPS).
Zonulin is a protein that acts as the primary modulator of tight junction function. It’s the “gatekeeper of the gut.” When zonulin levels rise, it signals the tight junctions to open. This is a normal physiological process to a degree, but certain triggers can cause a chronic overproduction of zonulin, leading to a persistently leaky gut. The two most well-documented triggers for zonulin release are:

Gliadin: A protein component of gluten. For a significant portion of the population, not just those with celiac disease, gliadin can trigger a zonulin response.
Gut Bacteria: Certain imbalances in gut flora can also stimulate zonulin release.

Lipopolysaccharide (LPS) is a component of the outer membrane of gram-negative bacteria, which are a normal part of the gut microbiome. LPS itself is not inherently “bad” when it stays within the gut lumen. However, when the gut barrier is compromised, LPS leaks into the bloodstream. This event is known as metabolic endotoxemia.
LPS is one of the most potent triggers of inflammation known to the human immune system. Even minuscule amounts in the bloodstream can set off a powerful inflammatory cascade. The immune system recognizes LPS via a receptor called Toll-like Receptor 4 (TLR4), which is found on immune cells such as macrophages. Activation of TLR4 triggers the massive release of pro-inflammatory cytokines, driving the systemic inflammation associated with insulin resistance, obesity, cardiovascular disease, and non-alcoholic fatty liver disease (NAFLD).
Therefore, a leaky gut creates a vicious cycle: gut barrier dysfunction allows LPS to enter the bloodstream, which causes systemic inflammation. This systemic inflammation, in turn, can further damage the gut lining, increasing its permeability and allowing even more LPS to leak through.

The Microbiome and the Estrobolome: Gut-Hormone Crosstalk

The gut is not just an immune and digestive organ; it is also a major endocrine (hormone-regulating) organ. The connection between gut health and hormonal balance is one of the most exciting and clinically relevant areas of modern research. This is particularly evident when we examine estrogen metabolism.

The Estrobolome: Your Gut’s Estrogen-Regulating Machinery

The estrobolome is a specific collection of bacteria within the gut microbiome that possesses a unique set of genes capable of metabolizing estrogens. These bacteria produce an enzyme called beta-glucuronidase. To understand its significance, we must first look at how the body eliminates estrogen.

Phase I & II Detoxification in the Liver: After estrogen has done its job in the body, it is sent to the liver for further processing before elimination. The liver modifies the estrogen and then attaches a glucuronic acid molecule to it in a process called glucuronidation. This “tags” the estrogen, making it water-soluble and ready for excretion via the bile, which is then released into the gut.
The Role of Beta-Glucuronidase: In a healthy gut with a balanced microbiome, this conjugated (tagged) estrogen passes through the intestines and is excreted in the stool. However, in a state of dysbiosis (an imbalanced microbiome), an overgrowth of certain bacteria can lead to high levels of the enzyme beta-glucuronidase.
Reactivation and Recirculation: Beta-glucuronidase acts like a pair of scissors. It cleaves the glucuronic acid tag off the estrogen. This “un-conjugates” the estrogen, converting it back into its active form. This free, active estrogen is now small enough to be reabsorbed from the gut back into the bloodstream.

This process undermines the body’s primary mechanism for clearing excess estrogen. The estrogen that was supposed to be eliminated is now recirculated, leading to an overall increase in the body’s estrogen load. This condition is known as estrogen dominance.

Clinical Implications of Estrogen Dominance

In my practice, estrogen dominance is a frequent finding in women presenting with a wide array of symptoms:

Premenstrual Syndrome (PMS): Severe mood swings, bloating, breast tenderness, and cramping.
Heavy or Irregular Menstrual Bleeding.
Uterine Fibroids and Endometriosis.
Fibrocystic Breasts.
Weight Gain: Particularly around the hips, thighs, and abdomen.
Increased Risk of Hormone-Sensitive Cancers: Such as breast, uterine, and ovarian cancer.

A patient may come to me seeking help for her debilitating PMS. The conventional approach might be to prescribe birth control pills to regulate her cycle or an SSRI for her mood symptoms. A functional medicine approach, however, asks why her hormones are imbalanced. By running a comprehensive stool analysis, we might discover elevated beta-glucuronidase levels, indicating an unhealthy estrobolome.
The treatment, therefore, is not to manipulate her hormones directly with synthetic drugs, but to heal her gut. By addressing dysbiosis, we can reduce beta-glucuronidase activity, allowing her body to excrete estrogen properly. This restores the natural balance between estrogen and progesterone, often resolving her symptoms at the source. This is a perfect example of how addressing a root cause in one system (the gut) can resolve symptoms in another (the endocrine system).

The Critical Role of Detoxification

The concepts of a leaky gut and a dysfunctional estrobolome highlight the immense burden placed on the body’s detoxification systems. Detoxification is not a trendy “cleanse” involving lemon water and cayenne pepper; it is a fundamental, continuous series of metabolic processes that the body uses to neutralize and eliminate harmful substances. These substances include not only external toxins from our environment (xenobiotics), such as pesticides, plastics, and heavy metals, but also internal byproducts of our own metabolism (endotoxins), such as hormones and inflammatory mediators.
The liver is the master organ of detoxification. This process is broadly divided into two phases, with a crucial third phase involving excretion.

Phase I Detoxification: The Activation Pathway

Phase I is the body’s first line of defense. It involves a family of enzymes known as the Cytochrome P450 (CYP450) superfamily. These enzymes use processes such as oxidation, reduction, and hydrolysis to transform fat-soluble toxins into more water-soluble forms.
Think of Phase I as taking a large, non-biodegradable piece of plastic and breaking it into smaller, more reactive pieces. This process is essential, but it can also be dangerous. The intermediate molecules created during Phase I are often more volatile and potentially more damaging (carcinogenic) than the original toxin. These are highly reactive molecules with unpaired electrons, known as free radicals.
This is why it’s critical that Phase II function optimally and immediately follow Phase I. An imbalance where Phase I is overactive and Phase II is sluggish can lead to a significant buildup of these toxic intermediates, causing cellular damage and increasing cancer risk.
Nutrients that support Phase I include:

B Vitamins: B2, B3, B6, B12, and folate.
Antioxidants: Vitamins A, C, and E, which help neutralize the free radicals produced.
Minerals: Such as iron and magnesium.

Phase II Detoxification: The Conjugation Pathway

Phase II is the conjugation (attachment) pathway. Its job is to take the highly reactive intermediates from Phase I and attach another molecule to them, making them water-soluble, non-toxic, and ready for excretion. There are several key Phase II pathways:

Glucuronidation: This is the primary pathway for detoxifying hormones (like estrogen), bilirubin, and many drugs. It involves attaching glucuronic acid. As we discussed, high beta-glucuronidase activity in the gut can reverse this process.
Sulfation: This pathway is crucial for detoxifying neurotransmitters, steroid hormones, and some xenobiotics. It requires sulfur-containing compounds. Patients with poor sulfation capacity may experience adverse reactions to sulfur-rich foods (such as garlic and onions) or supplements (such as MSM).
Glutathione Conjugation: Glutathione is the body’s master antioxidant and detoxifier. The enzyme glutathione S-transferase (GST) attaches glutathione to toxins, neutralizing them. This is a primary defense against heavy metals, pesticides, and the carcinogenic byproducts of Phase I.
Acetylation, Amino Acid Conjugation, and Methylation: These are additional important pathways that target specific toxins. Methylation, in particular, is a vast and critical biochemical process involved in everything from DNA expression to neurotransmitter synthesis and hormone clearance.

Key nutrients for supporting Phase II pathways are specific to each pathway:

Sulfation: Sulfur-rich amino acids like methionine and cysteine (found in eggs, cruciferous vegetables, garlic, onions), and molybdenum.
Glutathione Conjugation: N-acetylcysteine (NAC), glycine, glutamine, and selenium.
Methylation: Methionine, B12 (methylcobalamin), B6 (P-5-P), and folate (5-MTHF).

Phase III Detoxification: The Elimination Pathway

This Phase is often overlooked but is just as critical. Once toxins are conjugated in the liver, they must be transported out of the body. The primary routes are:

Bile: Fat-soluble toxins conjugated in the liver are released into bile, which flows into the small intestine and is then carried out of the body in the stool.
Urine: Water-soluble toxins are filtered by the kidneys and excreted in urine.

This is where gut health becomes paramount once again. If a person is chronically constipated, toxins released into the gut via bile are not eliminated efficiently. They can sit in the colon, where they may be reabsorbed back into circulation or be acted upon by gut bacteria (like the beta-glucuronidase we discussed), reversing the detoxification process. A healthy gut with regular bowel movements and adequate fiber to bind to toxins is essential for completing the detoxification cycle.
Clinically, I assess a patient’s detoxification capacity by reviewing their history and symptoms, and sometimes using advanced functional testing to measure the activity of these pathways. A person with chronic fatigue, chemical sensitivities, and hormonal imbalances is almost certainly dealing with a compromised detoxification system. Our therapeutic approach involves not just “detoxing” them, but systematically supporting each Phase with targeted nutrition, lifestyle changes, and botanicals to restore the body’s innate ability to clean house.

The 4R Program: A Systematic Approach to Gut Healing

Understanding the interconnectedness of inflammation, gut permeability, and detoxification provides us with a powerful “why.” The “how” is a systematic clinical protocol that has become a cornerstone of functional medicine: the 4R Program for gut restoration. This isn’t a quick fix; it’s a comprehensive, multi-phased approach designed to address the root causes of gut dysfunction and, by extension, a wide range of systemic health issues.
I guide my patients through this program step by step, customizing it to their unique physiology, history, and test results. It is a partnership that requires commitment from the patient and careful guidance from the clinician.

1. Remove

The first and most critical step is to remove the triggers that are driving inflammation and damaging the gut lining. We cannot hope to heal the gut while it is still under constant assault. This Phase involves two main components: dietary changes and pathogen eradication.
Dietary Removal:

The Elimination Diet: the gold standard for identifying food sensitivities. We typically remove the most common inflammatory triggers for 4-6 weeks. These include:
- Gluten: Due to its potential to trigger zonulin release and its cross-reactivity with other proteins.
- Dairy: Specifically, the casein and whey proteins, which are common allergens.
- Soy: Often genetically modified and can be a gut irritant for many.
- Corn: Another common allergen and source of pro-inflammatory Omega-6s.
- Eggs, Nuts, and Nightshades (tomatoes, peppers, eggplant, potatoes): Removed in more sensitive individuals.
- Processed Foods, Sugar, and Industrial Seed Oils (Omega-6s): These are non-negotiable removals as they are primary drivers of inflammation and gut dysbiosis.
The goal is to calm the immune system. After the elimination period, foods are reintroduced one by one, carefully monitoring for any return of symptoms. This process helps the patient create a personalized, long-term anti-inflammatory diet.

Pathogen Removal:

If stool testing reveals an overgrowth of pathogenic bacteria, yeast (such as Candida), or parasites, we must address it. This is often done using targeted antimicrobial therapy.
Herbal Antimicrobials: I often prefer to start with broad-spectrum herbal agents that are effective yet gentle on the host. These include berberine, oregano oil, garlic (allicin), and grapefruit seed extract. These botanicals often have the added benefit of disrupting biofilms, protective shields that colonies of bacteria and yeast form to hide from the immune system and antibiotics.
Pharmaceuticals: In some cases, targeted prescription antifungals (like Nystatin or Fluconazole) or antibiotics (like Rifaximin for Small Intestinal Bacterial Overgrowth, or SIBO) may be necessary.

2. Replace

Once we’ve removed the irritants, we need to ensure the body has what it needs for proper digestion and absorption. Chronic gut inflammation and poor diet can lead to deficiencies in essential digestive factors.

Stomach Acid (Hydrochloric Acid – HCl): Many people, especially as they age or under chronic stress, have low stomach acid (hypochlorhydria). This is a major problem, as adequate acid is needed to sterilize food, kill pathogens, and begin protein digestion. Without it, proteins putrefy in the gut, feeding the wrong bacteria, and minerals like iron, calcium, and B12 are poorly absorbed. We may use Betaine HCl with meals to support this.
Digestive Enzymes: A compromised pancreas or gut lining may not produce enough enzymes to break down fats, proteins, and carbohydrates. Supplementing with a broad-spectrum digestive enzyme formula can reduce bloating and gas and ensure that nutrients are properly broken down for absorption, preventing them from serving as food for pathogenic microbes.
Bile Support: Bile is essential for fat digestion and absorption of fat-soluble vitamins (A, D, E, K). It also acts as an antimicrobial agent in the small intestine. For patients who have had their gallbladder removed or who show signs of poor fat digestion (e.g., floating stools), supporting bile flow with compounds such as taurine, glycine, ox bile, or dandelion root can be very beneficial.

3. Reinoculate

With the gut environment cleared of major offenders and digestive function supported, it’s time to rebuild the beneficial microbial community. This is about restoring a diverse, balanced, and resilient microbiome.

Probiotics: These are live, beneficial bacteria. We use high-quality, multi-strain probiotics to help repopulate the gut. The key strains we look for include various species of Lactobacillus and Bifidobacterium. Under specific conditions, we might use targeted strains such as Saccharomyces boulardii, a beneficial yeast that is effective against Candida and C. difficile.
Prebiotics: These are the food for your good bacteria. Probiotics will not survive and thrive without adequate fuel. Prebiotics are specific types of fermentable fiber. Excellent food sources include Jerusalem artichokes, chicory root, garlic, onions, leeks, and asparagus. We can also supplement with prebiotic fibers such as inulin, Fructooligosaccharides (FOS), or Galactooligosaccharides (GOS), although we must introduce them slowly to avoid gas and bloating.

A diet rich in a wide variety of plant fibers is the best long-term strategy for maintaining a healthy microbiome. Each type of fiber feeds different species of bacteria, so diversity in your diet leads to diversity in your gut.

4. Repair

The final step is to provide the nutrients needed to heal and regenerate the gut lining, closing the “leaks” and restoring the barrier’s integrity. This Phase runs concurrently with the others, but its focus intensifies as the inflammation subsides.

L-Glutamine: This amino acid is the primary fuel source for the cells that line the small intestine (enterocytes). It is essential for repairing a leaky gut. Supplementing with L-glutamine provides the building blocks for these cells to regenerate and tighten the junctions between them.
Zinc Carnosine: This chelated compound has been extensively studied in Japan for the treatment of stomach ulcers and gut inflammation. It has a unique ability to adhere to the inflamed lining of the GI tract, where it provides sustained healing, reducing inflammation and promoting tissue repair.
Deglycyrrhizinated Licorice (DGL): This form of licorice has had the glycyrrhizin component removed (which can raise blood pressure). DGL is a powerful demulcent, meaning it soothes and coats the mucous membranes of the GI tract, reducing irritation and promoting the secretion of protective mucus.
Aloe Vera: Similar to DGL, aloe has potent anti-inflammatory and soothing properties that help heal the inflamed epithelial lining.
Omega-3 Fatty Acids (EPA/DHA): As discussed earlier, these fats are the precursors to the powerful anti-inflammatory and pro-resolving resolvins and protectins. High-dose fish oil is often a key part of the repair phase, actively turning off inflammatory signaling in the gut wall.
Bone Broth: Rich in collagen, gelatin, and amino acids like glycine and proline, bone broth provides a readily absorbable source of the raw materials needed to rebuild connective tissue, including the gut lining.

By systematically following the 4R Program, we can guide the body back to balance. We remove the insults, support natural digestive processes, rebuild the beneficial microbial army, and provide the raw materials for healing. This is the essence of functional medicine: understanding the body’s intricate systems and providing targeted support to help it heal itself.

Summary

This educational post, published on January 16, 2026, has journeyed through the core principles of modern functional medicine, presenting a systems-based view of health and chronic disease. We began by establishing the cell membrane as the fundamental battleground for inflammation. We learned that the dietary imbalance between pro-inflammatory Omega-6 fatty acids (from industrial seed oils) and anti-inflammatory Omega-3 fatty acids (from fish oil) primes our cells for chronic, low-grade inflammation. This imbalance disrupts the production of signaling molecules, favoring inflammatory eicosanoids over the crucial, inflammation-resolving resolvins and protectins. From there, we identified the gut as the epicenter of systemic health and dissected the mechanism of intestinal permeability, or “leaky gut.” We explored how damage to the gut’s single-cell-thick barrier allows inflammatory triggers, such as lipopolysaccharides (LPS), to enter the bloodstream, driving systemic inflammation that manifests as joint pain, brain fog, and autoimmune conditions. We further elucidated the gut’s role as an endocrine organ, focusing on the estrobolome—gut bacteria that regulate estrogen levels—and how dysfunction of the estrobolome can lead to estrogen dominance and related health issues. This led us to recognize the critical importance of the body’s liver detoxification pathways, which clear these inflammatory molecules and hormonal byproducts. Finally, we tied these concepts together with a practical, evidence-based clinical strategy: the 4R Program (Remove, Replace, Reinoculate, Repair), a systematic protocol for healing the gut, rebalancing the microbiome, and quenching the fires of chronic inflammation.

Conclusion

The paradigm of healthcare is shifting. The prevailing model of the 20th century, which often focused on managing symptoms with pharmaceuticals, is giving way to a more nuanced, root-cause-oriented approach. As both a chiropractor and a family nurse practitioner, I have seen firsthand the power of this integrated perspective. The conditions that plague modern society—autoimmune diseases, hormonal imbalances, chronic pain, metabolic syndrome, and neurocognitive issues—are not isolated pathologies. They are the downstream consequences of upstream dysfunctions, primarily rooted in chronic inflammation originating from our cells and our gut. By understanding the intricate biochemistry of fatty acids, the profound impact of gut barrier integrity, the complex interplay between the microbiome and our hormones, and the essential role of detoxification, we can intervene meaningfully. The 4R Program is not merely a protocol; it is a logical framework for restoring the body’s innate capacity for self-regulation and healing. The future of medicine lies in this personalized, systems-based approach, empowering patients and practitioners to build a foundation of true, resilient health from the cells up.

Key Insights

Cellular inflammation is the Foundation: The ratio of Omega-6 to Omega-3 fatty acids in your cell membranes dictates your body’s inflammatory tone. A diet high in processed foods and industrial seed oils directly induces a pro-inflammatory state at the cellular level, serving as the bedrock of most chronic diseases.
Leaky Gut Drives Systemic Disease: A compromised gut barrier is not a localized digestive issue; it is a primary driver of systemic inflammation. The leakage of bacterial components, such as LPS, into the bloodstream triggers body-wide immune activation that can manifest as arthritis, skin disorders, brain fog, and autoimmunity.
The Gut Regulates Your Hormones: The health of your gut microbiome, particularly the estrobolome, directly and profoundly affects your hormone balance. An imbalanced gut can lead to the recirculation of estrogen, contributing to estrogen dominance and a host of related symptoms and health risks.
Healing is a Systematic Process: Restoring health from chronic illness requires a structured approach. The 4R Program (Remove, Replace, Reinoculate, Repair) provides a comprehensive and effective framework for addressing the root causes of gut dysfunction, thereby resolving many systemic issues. It emphasizes removing inflammatory triggers, supporting digestion, rebuilding the microbiome, and providing key nutrients for tissue repair.

References

Serhan, C. N. (2014). Pro-resolving lipid mediators are leads for resolution physiology. Nature, 510(7503), 92–101.
Fasano, A. (2011). Zonulin and its regulation of intestinal barrier function: the biological door to inflammation, autoimmunity, and cancer. Physiological Reviews, 91(1), 151–175.
Cani, P. D., Amar, J., Iglesias, M. A., Poggi, M., Knauf, C., Bastelica, D., … & Burcelin, R. (2007). Metabolic endotoxemia initiates obesity and insulin resistance. Diabetes, 56(7), 1761–1772.
Baker, J. M., Al-Nakkash, L., & Herbst-Kralovetz, M. M. (2017). Estrogen–gut microbiome axis: Physiological and clinical implications. Maturitas, 103, 45–53.
Liska, D. J. (1998). The detoxification enzyme systems. Alternative Medicine Review, 3(3), 187-198.
Bland, J. S., & Barrager, E. (2016). Clinical Approaches to Leaky Gut Syndrome (Intestinal Permeability). Institute for Functional Medicine.

Keywords

Inflammation, Omega-3 Fatty Acids, Cell Membrane, Leaky Gut, Intestinal Permeability, Gut Microbiome, Estrobolome, Estrogen, Dominance, Detoxification, 4R Program, Functional Medicine, Dr. Alexander Jimenez, Resolvins, Lipopolysaccharide (LPS), Zonulin

Disclaimer: This content is for informational and educational purposes only. It is not intended to provide medical advice or to replace medical advice or treatment from a personal physician. All readers/viewers of this content are advised to consult their doctors or qualified health professionals regarding specific health questions. Neither Dr. Alexander Jimenez nor the publisher of this content takes responsibility for possible health consequences of any person or persons reading or following the information in this educational content.
Personal Medical Advice Disclaimer: All individuals must obtain recommendations for their personal health situations from their own medical providers. The information presented here is for educational purposes and should not be considered a substitute for consultation with a licensed healthcare professional.

March 19, 2026

Why Gut Pain Can Continue Even When You Eat “Healthy”

An Integrative Medicine Perspective

Many people feel frustrated when they clean up their diet but still deal with bloating, cramping, gas, reflux, constipation, loose stools, or stomach pain. They may cut out fast food, drink more water, eat more vegetables, and choose “healthy” meals, yet their gut still does not feel right. That happens because healthy eating is important, but it does not always solve the deeper problem. Sometimes the real issue is not just what you eat. It is how your digestive system is working, how your nervous system is responding to stress, and whether hidden gut problems are still active (Fasano, 2012; Sorathia, 2023).

At ChiroMed, the goal is not just to quiet symptoms for a few days. The goal is to understand why your body keeps reacting in the first place. ChiroMed describes its mission as patient-centered, root-cause care that brings together chiropractic, nurse practitioner services, nutrition, rehabilitation, acupuncture, and other supportive therapies under one roof. That whole-person model fits well with chronic gut complaints because persistent digestive symptoms often have multiple causes simultaneously (ChiroMed, n.d.).

Healthy food can still cause symptoms when the gut is not functioning well

A person can eat grilled chicken, vegetables, smoothies, soups, fruit, and clean snacks and still feel miserable. That does not always mean the food is unhealthy. It may mean the digestive system is irritated or not functioning properly. For example, some people have trouble breaking down food due to low stomach acid, low digestive enzyme levels, poor bile flow, altered gut motility, or an imbalanced microbiome. In that situation, even nutritious foods can lead to pressure, bloating, or discomfort (Segersten, 2025; Dukowicz et al., 2007).

This is why ChiroMed’s integrated care approach matters. The clinic emphasizes personalized treatment plans instead of one-size-fits-all advice. That is important in digestive health because two people can have the same symptom but entirely different causes. One person may have hidden food sensitivities. Another may have dysbiosis. Another may be stuck in chronic stress mode, which changes digestion from the top down (ChiroMed, n.d.; The Well House, n.d.).

Leaky gut may be one reason symptoms continue

A healthy intestinal lining works like a protective filter. It is supposed to allow nutrients to pass through while helping block toxins, bacteria, and large food particles from moving across too easily. Fasano explains that intestinal permeability is controlled by structures called tight junctions, and when this regulation breaks down, it can contribute to inflammation and immune dysfunction (Fasano, 2012).

This is the idea behind what many people call “leaky gut.” Whole Health Chicago explains that when the gut barrier becomes overly permeable, unwanted substances can pass through more easily, triggering irritation or immune reactions. The article also notes that possible contributors include irritating foods, alcohol, certain medications such as NSAIDs, parasites, Candida, and poor dietary patterns (Whole Health Chicago, 2023).

Leaky gut is not the answer for every digestive complaint, but it is one important piece of the puzzle. In a root-cause setting like ChiroMed, increased intestinal permeability would not be treated as a trendy buzzword. It would be considered one possible reason why symptoms persist even after a person starts eating better.

Hidden food sensitivities can be easy to miss

Some people assume that if they are not eating fried food, sugar, or processed snacks, then food cannot be causing their symptoms. But the issue may not be “bad food.” It may be a food that is not working well for that individual’s body. Common triggers include dairy, wheat, eggs, soy, corn, and other foods that seem healthy in many situations but may still cause inflammation or irritation in certain people (Whole Health Chicago, 2023).

A study in Frontiers in Nutrition found associations between food-specific IgG antibodies and biomarkers of intestinal permeability. The authors noted links involving common foods such as wheat, dairy, and eggs, though they also stressed that the topic remains debated and that these findings do not, by themselves, establish causation (Vita et al., 2022). This is important because it shows why guessing is not enough.

A careful, guided process is better than randomly cutting out foods. At ChiroMed, a personalized care model makes more sense than handing every patient the same food list. The best plan is to look at symptom timing, food patterns, overall inflammation, stress, and other digestive factors before deciding what needs to change.

Low stomach acid and low digestive enzymes may be part of the problem

Digestive discomfort is not always about food sensitivity. Sometimes it is about poor digestion. The body needs sufficient stomach acid, digestive enzymes, bile, chewing, and proper gut motility to break food down properly. When these functions are weak, food may sit too long, ferment, and create gas, fullness, and pain (Segersten, 2025).

StatPearls notes that the small intestine normally has relatively low bacterial levels, partly because stomach acid and intestinal movement help control bacterial growth. When those defenses weaken, bacterial overgrowth becomes more likely (Sorathia, 2023). A broader review on SIBO states that low stomach acid and reduced motility are important risk factors for bacterial overgrowth in the small intestine (Dukowicz et al., 2007).

That means a patient may believe they are reacting to healthy food, when the deeper problem is incomplete digestion. In an integrative setting, it makes sense to ask:

Is the stomach producing enough acid?
Are digestive enzymes doing their job?
Is the person eating too fast or under stress?
Is there bacterial overgrowth or poor motility?
Is the gut ready to handle high-fiber foods yet?

These questions are more useful than simply saying, “Stop eating this food forever.”

Dysbiosis and SIBO may make healthy foods feel worse

Dysbiosis means the gut microbiome is out of balance. SIBO, or small intestinal bacterial overgrowth, is one form of that imbalance. It can cause bloating, abdominal pain, diarrhea, gas, and poor nutrient absorption (Sorathia, 2023). For some people, symptoms worsen after eating foods that are normally healthy, especially fermentable carbohydrates found in onions, garlic, beans, some fruits, and certain vegetables.

That does not mean those foods are “bad.” It means the gut environment may not be handling them correctly right now. A person with SIBO may react strongly to foods that would normally support good health in someone else. This is why personal evaluation matters. ChiroMed’s integrated model is especially helpful here because persistent symptoms may need a combination of nutrition guidance, medical evaluation, nervous system support, and follow-up care rather than a simple list of foods to avoid (ChiroMed, n.d.).

Chronic stress can keep the gut inflamed

Stress is one of the biggest reasons digestive problems do not fully calm down. When the body stays in fight-or-flight mode, digestion becomes less efficient. Blood flow, stomach acid, and enzyme production can decline; gut motility can become abnormal; and the intestinal barrier may become more vulnerable (Segersten, 2025).

Carolina Total Wellness also explains that chronic stress can weaken protective immune defenses in the gut, including secretory IgA, which helps support intestinal health (Carolina Total Wellness, n.d.). In simple terms, stress can make the gut more reactive and less protected.

This is one reason chiropractic and integrative care may be valuable for people with ongoing digestive symptoms. Chiropractic care alone is not a cure for every gut condition, but an integrative chiropractor often considers how pain, posture, stress, sleep, nervous system overload, and muscle tension may affect digestive function. ChiroMed’s site emphasizes that its services are designed to work in harmony. That kind of team-based care is useful when gut symptoms are connected to both physical stress and metabolic stress (ChiroMed, n.d.).

Why professional guidance is better than guessing

Many people keep trying new diets, supplements, and online advice, but never get lasting relief. That is often because they are treating symptoms in a general way rather than identifying the real trigger. One functional medicine source explains that the more important goal is to find the cause of the irritated state in the intestines rather than merely reacting to symptoms after they show up (Ask Dr. Olsen, n.d.).

A professional evaluation may help uncover issues such as:

Hidden food sensitivities
Poor digestion from low stomach acid or low enzymes
Dysbiosis or SIBO
Chronic stress and nervous system overload
Medication-related irritation
Poor meal timing or eating habits
Inflammation tied to sleep, pain, or lifestyle patterns

At ChiroMed, this type of evaluation fits the clinic’s personalized, multidisciplinary care style. The clinic already highlights chiropractic care, nurse practitioner services, nutrition, rehabilitation, acupuncture, and patient-specific plans as core components of its model. That makes it a strong setting for people who need more than generic diet advice (ChiroMed, n.d.).

What a root-cause gut healing plan may include

A gut-healing program should be built around the individual, not copied from an online trend. Depending on the cause, an integrative plan may include:

Temporary removal of known trigger foods
Careful reintroduction of foods instead of permanent restriction
Support for stomach acid, enzymes, or bile when appropriate
Stress reduction and nervous system regulation
Better meal habits, such as slower eating and improved chewing
Support for dysbiosis or SIBO when indicated
Nutrition changes that match the person’s actual tolerance level
Referral for additional testing when symptoms suggest a more serious condition

This kind of plan lines up well with ChiroMed’s philosophy of addressing root causes and creating individualized treatment strategies. It also reflects the kind of integrative clinical reasoning that Dr. Alexander Jimenez, DC, APRN, FNP-BC, often discusses in his broader functional and multidisciplinary work, in which digestive symptoms are viewed in relation to inflammation, stress, nutrition, and overall body function (Jimenez, n.d.).

Final thoughts

If your gut still hurts even though you are eating “healthy,” that does not mean you are doing everything wrong. It may simply mean that food quality is only one part of the picture. Problems like leaky gut, hidden food sensitivities, low stomach acid, poor enzyme output, dysbiosis, SIBO, and chronic stress can all continue to drive symptoms. Real progress usually comes from finding the specific cause, not from trying harder to follow a general healthy diet (Fasano, 2012; Sorathia, 2023).

ChiroMed’s integrated medicine model is built for this kind of bigger-picture thinking. Instead of only asking what you are eating, the better question is why your body is still reacting. When care is personalized and root-cause focused, people often have a better chance of understanding their triggers, calming inflammation, and supporting lasting digestive health.

Tag: intestinal permeability

The Gut-Immune System and Hormones Role in Overall Wellness

Abstract

Why I Now Start With The Gut, Then Layer Hormones, Thyroid, And Structure

The Gut Microbiome As A Neuroendocrine And Immune Control Center

Intestinal Permeability, Zonulin, and the Inflammation–Endocrine Loop

The Estrobolome, Beta-Glucuronidase, And Estrogen Recirculation

PCOS, Endometriosis, And The Gut–Hormone Axis

Thyroid Conversion, Iodine–Selenium Synergy, and Hashimoto’s

Vitamin D3, K2, Magnesium, And Vitamin A: Directing Calcium And Calming Immunity

Akkermansia, SCFAs, And Metabolic Flexibility

Evidence-Based Tools That Inform Personalization

Integrative Chiropractic Care: Why Structure And Autonomics Matter

DIM, I3C, And Safer Estrogen Metabolism

Calcium D-Glucarate, Methylation, Bile Flow, And Daily Excretion

Glutamine, Zinc Carnosine, And Mucosal Repair

Shilajit And Free Testosterone: Sustaining Benefits Across Pellet Cycles

Practical, Stepwise Clinical Plan

Modulating Women’s Hormones- Video

Clinical Observations From My Practice

Why These Techniques Work: Physiology-First Reasoning

Putting It All Together: A Gut-First, Whole-Person Strategy

References

Gut Health and Hormone Balance Treatment

Abstract

Why Hormones Are Microbiome-Dependent: The Gut–Liver–Hormone Axis

Dysbiosis and Leaky Gut Explained: Distinct Problems that Reinforce Each Other

Estrogen Metabolism 101: Enterohepatic Circulation and the Estrobolome

PCOS, Endometriosis, and Autoimmunity: What the Microbiome Adds

The Simple Question with Big Impact: Are You Pooping Daily?

A 3-by-3 Framework for Gut Repair: Remove, Replace, Repair

Nutrient Foundations for Receptor-Level Hormone Action: D, K2, A, Magnesium, Iodine, Selenium, and Methylation

Thyroid resilience: iodine and selenium synergy

Methylation for estrogen safety

DIM and Estrogen Metabolites: Steering Toward Safer Pathways

Shilajit for Free Testosterone and Mitochondrial Support

Vitamin D as a Systemic Modulator: Barrier, Immunity, and Receptors

Integrative Chiropractic Care: The Neuroimmune–Endocrine Interface

A Phased, Clinic-Ready Protocol for Gut and Hormone Optimization

Special Focus: PCOS and Endometriosis

Case Reflection: High Total Testosterone, Low Vitality

Safety, Lab Monitoring, and Personalization

How Integrative Chiropractic Care Complements Endocrine and Gut Strategies

Why Each Technique Matters: Systems Biology Rationale

Clinical Observations from Practice

References

The Clinical Approach to Endocrine Health & Hormonal Balance

Introduction & Abstraction

Navigating the Modern Health Landscape: A Clinician’s Perspective

The Cell Membrane: Ground Zero for Inflammation

The Omega-6 and Omega-3 Imbalance: Fueling the Fire

Eicosanoids: The Messengers of Inflammation and Resolution

Resolvins and Protectins: The “Off-Switch” for Inflammation

The Gut: Your Body’s Grand Central Station

Intestinal Permeability: When the Wall Is Breached

The Role of Zonulin and Lipopolysaccharide (LPS)

The Microbiome and the Estrobolome: Gut-Hormone Crosstalk

The Estrobolome: Your Gut’s Estrogen-Regulating Machinery

Clinical Implications of Estrogen Dominance

The Critical Role of Detoxification

Phase I Detoxification: The Activation Pathway

Phase II Detoxification: The Conjugation Pathway

Phase III Detoxification: The Elimination Pathway

The 4R Program: A Systematic Approach to Gut Healing

1. Remove

2. Replace

3. Reinoculate

4. Repair

Summary

Conclusion

Key Insights

References

Keywords

Why Gut Pain Can Continue Even When You Eat “Healthy”

An Integrative Medicine Perspective

Healthy food can still cause symptoms when the gut is not functioning well

Leaky gut may be one reason symptoms continue

Hidden food sensitivities can be easy to miss

Low stomach acid and low digestive enzymes may be part of the problem

Dysbiosis and SIBO may make healthy foods feel worse