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This article is for educational purposes only. It does not constitute individualized medical or dietary advice. Speak with your healthcare provider before changing your diet, starting supplements, or making any adjustments to your GLP-1 medication regimen.

The gut microbiome is the vast community of bacteria, fungi, and other microorganisms living in your digestive tract. It has emerged as one of the most intensively studied areas in metabolic health research. Now that GLP-1 receptor agonists like semaglutide and tirzepatide are among the most widely prescribed medications in the world, researchers are asking a natural question: what do these drugs actually do to the microbiome?

The answer, as of the most current evidence, is nuanced. GLP-1 medications appear to shift the composition of gut bacteria in ways that broadly parallel their metabolic effects. Whether those microbiome changes are a meaningful part of how these medications work, or largely a downstream consequence of the profound dietary and metabolic changes they produce, is an open and actively debated question. People on GLP-1 therapy typically eat less overall, yes, but they also eat differently, shifting toward foods that are easier to tolerate, higher in protein, and lower in ultraprocessed carbohydrates. That change in dietary pattern is itself a powerful driver of microbiome composition, independent of caloric intake. Here's what the research shows, and what it means practically.

What is the gut microbiome, and why does it matter for metabolic health?

Your gut hosts trillions of microorganisms, the majority of them bacteria, that collectively form an ecosystem as complex and individual as a fingerprint. This community is not passive. It produces short-chain fatty acids (SCFAs) that feed the gut lining and communicate with metabolic organs, synthesizes vitamins, modulates immune function, and directly influences how the body processes nutrients, stores fat, and regulates appetite.

In people with obesity, type 2 diabetes, and metabolic syndrome, the microbiome is consistently different from that of metabolically healthy individuals: lower in microbial diversity, lower in beneficial genera like Akkermansia muciniphila and Bifidobacterium, and higher in microbes associated with inflammation and impaired gut barrier integrity. This state of imbalance is called dysbiosis. Whether dysbiosis causes metabolic disease or results from it is still debated; most likely, both directions are true.

The gut–GLP-1 relationship is bidirectional

One of the most important things to understand about GLP-1 and the gut microbiome is that the relationship runs in both directions. That context matters considerably for how we interpret the research.

A two-way relationship, simplified
Gut Microbiome
SCFA-producing bacteria stimulate native GLP-1 secretion
STIMULATES ↑
endogenous GLP-1
↓ RESHAPES
microbial composition
GLP-1 Medications
semaglutide · tirzepatide · liraglutide
BOTH SUPPORT ↓
Metabolic Health

Short-chain fatty acids (SCFAs) produced by certain gut bacteria bind to FFAR2 receptors in the gut wall, stimulating native GLP-1 secretion (Tolhurst et al., Diabetes 2012). GLP-1 medications in turn alter gut motility, food intake, and microbial composition, making it genuinely difficult to disentangle direct pharmacological effects from the downstream consequences of eating differently and losing weight.

Certain gut bacteria, specifically the SCFA-producing species, stimulate your gut cells to release GLP-1 naturally. GLP-1 receptor agonists, in turn, slow gastric emptying, change food preferences, reduce overall intake, and produce weight loss, all of which alter the microbiome independently. This bidirectional relationship means that when researchers observe microbiome changes in people on GLP-1 medications, there is no straightforward way to conclude the drug itself was the cause.

What GLP-1 medications appear to change in the microbiome

A 2025 systematic review published in Nutrients (Gofron et al.) analyzed 38 studies examining the effects of GLP-1 analogues on gut microbiota composition, richness, and diversity. The headline findings were consistent across multiple drugs: GLP-1 analogues broadly increase the abundance of bacteria associated with improved metabolic function, particularly Akkermansia muciniphila, a species that has attracted significant attention in metabolic health research.

Akkermansia muciniphila: the standout finding

Akkermansia muciniphila is a mucus-dwelling bacterium that supports gut barrier integrity, reduces intestinal inflammation, and is consistently found at lower levels in people with obesity and type 2 diabetes compared to metabolically healthy controls. Its elevation has been linked to improved insulin sensitivity, lower cardiovascular risk markers, and better weight management outcomes. Across all GLP-1 analogues studied, Akkermansia levels increased, making it the most consistent microbiome finding in this body of research.

Other beneficial shifts

Beyond Akkermansia, GLP-1 medications have been associated with increases in other genera linked to favorable metabolic profiles: Bifidobacterium, Lactobacillus, Bacteroides, Faecalibacterium prausnitzii (an anti-inflammatory SCFA producer) and Ruminococcus. Many studies also report a reduction in the Firmicutes/Bacteroidetes ratio. This shift has been proposed, though not definitively established in humans, as a marker of improved metabolic health.

Evidence by medication

Semaglutide (Ozempic / Wegovy)
Most prescribed, most studied
  • Consistently increases Akkermansia muciniphila across both animal and human studies
  • Also elevates Alistipes and Alloprevotella, genera linked to reduced gut inflammation
  • Improves gut barrier integrity in murine models (reduced intestinal permeability markers)
  • Some studies report decreased overall microbial diversity, which is worth noting as a nuance
  • A 12-week human trial (Chen et al. 2025) showed measurable composition changes with metabolomic shifts
Human + animal evidence
Tirzepatide (Mounjaro / Zepbound)
Dual GLP-1/GIP agonist, emerging data
  • Reduces the Firmicutes/Bacteroidetes ratio in animal models, a favorable metabolic shift
  • Significantly reduces hepatic steatosis alongside microbiome changes in diabetic mice
  • Modulates bile acid metabolism, an important interface between gut bacteria and metabolic organs
  • Human-specific microbiome data is limited, and most evidence remains preclinical as of 2025
  • The SYNERGY-NASH trial showed 44–62% MASH resolution, likely involving gut-liver axis changes
Primarily animal models
Liraglutide (Saxenda / Victoza)
Longest-studied in microbiome research
  • Promotes growth of beneficial genera relevant to metabolic function
  • Normalizes Firmicutes/Bacteroidetes ratio in preclinical models
  • Increases Bifidobacterium and Lactobacillus spp. in animal studies
  • Enhances Akkermansia levels (consistent with class effect)
  • More robust animal data than human RCT data for microbiome endpoints
Human + animal evidence
Dulaglutide (Trulicity)
Favorable profile, limited microbiome data
  • Increases Bacteroides, Akkermansia, and Ruminococcus, all associated with improved metabolic homeostasis
  • Ruminococcus is an important butyrate producer; elevated levels support gut barrier function
  • Less extensively studied for microbiome endpoints than semaglutide or liraglutide
Human data available

Direct drug effects vs. what follows from eating less

This is the most important caveat in the entire field. A 2025 narrative review published in the Canadian Journal of Physiology and Pharmacology assessed the available evidence and reached a sobering conclusion. The primary drivers of microbiome changes observed after GLP-1 treatment are most likely dietary changes and weight loss rather than direct pharmacological action of the drug on gut bacteria.

When someone on semaglutide eats significantly less, changes their food choices, and loses 15% of their body weight, their microbiome will shift regardless of what the drug itself is doing. Separating these effects cleanly is one of the central methodological challenges in this field.

GLP-1 receptors are expressed on enteroendocrine cells throughout the gut, so direct drug–microbiome interaction is biologically plausible. Most studies don't include diet-matched or weight-matched control groups, making it impossible to isolate the drug's direct effect from the downstream consequences of the behavioral and metabolic changes it produces.

Mechanism Evidence strength Key finding
Akkermansia increase across all GLP-1 drugs Consistent Found in both animal and human studies across multiple GLP-1 analogues; the most robust finding in this literature
Shift toward beneficial genera broadly Consistent Bacteroides, Lactobacillus, Faecalibacterium increases seen across multiple studies and drugs
Reduced Firmicutes/Bacteroidetes ratio Likely but confounded Also occurs with weight loss alone; hard to attribute specifically to drug mechanism
Direct pharmacological effect on microbiome Unclear Biologically plausible; difficult to isolate from dietary changes and weight loss in existing studies
Diversity changes Mixed results Some studies show increased diversity; some (especially semaglutide) show decreased diversity, which appears to be population and context dependent
Tirzepatide human microbiome data Very limited Most tirzepatide microbiome data is preclinical as of 2025–2026; human studies are needed

GI symptoms and the microbiome connection

Nausea, constipation, and bloating are among the most common side effects of GLP-1 medications. The microbiome may play a role in both causing and mediating these symptoms, though the relationship is not straightforward. Slowed gastric emptying, the primary mechanism behind GLP-1-induced GI side effects, alters the transit time of food through the intestine, which changes the environment gut bacteria inhabit and the substrates they ferment.

Constipation, in particular, is associated with shifts in microbial composition. When stool transit slows, bacteria have more time to ferment residual carbohydrates, which can contribute to gas, bloating, and altered microbial balance. Strategies that address constipation on GLP-1 therapy, including adequate hydration, consistent fiber intake, and physical activity, also support the microbiome, making them doubly worthwhile.

Practical guidance: supporting your gut while on GLP-1 therapy

Regardless of whether the microbiome benefits of GLP-1 medications are direct or secondary, there are well-evidenced dietary strategies that support gut health, complement the metabolic benefits of these medications, and may help manage GI side effects. None of these require expensive supplements or complicated protocols.

🥦
Prioritize prebiotic fiber
Prebiotic fibers, found in vegetables, legumes, oats, and whole grains, feed SCFA-producing bacteria including the beneficial genera that GLP-1 medications appear to promote. Aim for 25–35g of dietary fiber per day from whole food sources. Reduced appetite on GLP-1 medications can make this harder, so build fiber-rich foods into smaller meals intentionally.
Best sources: garlic, onions, leeks, asparagus, oats, lentils, chickpeas, barley, slightly green bananas
🫙
Include fermented foods
Fermented foods such as yogurt, kefir, kimchi, sauerkraut, and miso introduce live cultures and have been shown in randomized trials (Wastyk et al., Cell 2021) to increase microbiome diversity and reduce inflammatory markers. They tend to be protein-rich and generally well-tolerated even with the appetite reduction and nausea that often accompany GLP-1 therapy.
Start with small amounts if GI symptoms are prominent; kefir and yogurt tend to be the best tolerated
💧
Stay well hydrated
Slowed gastric emptying on GLP-1 therapy increases constipation risk, which disrupts microbial balance. Adequate fluid intake is one of the most effective strategies for GI symptom management and supports healthy stool transit that the microbiome depends on. A general target of at least 8 cups per day, and more in hot weather or with exercise.
Sip consistently throughout the day rather than large volumes at once, especially if nausea is an issue
🥗
Emphasize dietary diversity
Microbial diversity, a marker of gut health, is strongly associated with dietary diversity. Aim for a wide variety of plant foods each week: different vegetables, fruits, whole grains, legumes, nuts, and seeds. Herbs and spices count as well. Turmeric, ginger, oregano, and cinnamon contain polyphenols that feed beneficial bacteria. The target of 30 different plant foods per week has been associated with significantly higher microbiome diversity in large observational studies.
Rotate your protein sources, add a new vegetable each shopping trip, vary your grains, and use herbs and spices generously
🫘
Don't neglect protein
GLP-1 medications reduce appetite substantially, which can lead to inadequate protein intake and accelerate muscle loss during weight loss. High-quality protein sources such as eggs, fish, poultry, Greek yogurt, and legumes are essential for preserving lean mass and also support a healthy gut environment. Use our protein calculator to find your target.
Prioritize protein at every meal before reaching for other foods. Build your plate around it.
🚶
Move consistently
Exercise independently improves microbiome diversity and composition, increases SCFA-producing bacteria, and supports bowel motility. Even 20 to 30 minutes of moderate daily walking improves gut transit and microbiome composition. The combination of GLP-1 therapy and consistent physical activity is among the most evidence-supported approaches to durable metabolic improvement.
Walking after meals supports both blood sugar regulation and GI motility

Do probiotics help?

This is one of the most common questions patients on GLP-1 therapy ask, and the honest answer is: robust evidence for probiotic supplementation specifically in the context of GLP-1 therapy does not yet exist. Probiotics are not regulated as medications, strains vary enormously in their studied effects, and most clinical trials of probiotics are small and strain-specific. A probiotic that worked in one trial cannot be assumed to have the same effects from a different product with different strains.

What we can reasonably say about probiotics on GLP-1 therapy: Multi-strain probiotic supplements are generally safe for most people and unlikely to cause harm. If GI symptoms such as bloating, constipation, or loose stools are prominent, a probiotic containing Lactobacillus and Bifidobacterium strains may help, though the evidence base is modest. Fermented foods containing live cultures are supported by better evidence than most supplement products, and they carry the added advantage of providing protein, micronutrients, and dietary diversity. Discuss with your provider before starting any supplement if you have a compromised immune system or are immunosuppressed.
A note on "Akkermansia" supplements: Akkermansia muciniphila supplements are now commercially available and heavily marketed in the context of GLP-1 therapy and metabolic health. While pasteurized Akkermansia has shown some promise in early trials (Plovier et al., Nature Medicine 2017; Depommier et al., Nature Medicine 2019), the evidence in humans is preliminary, trials are small, and no studies have tested Akkermansia supplementation alongside GLP-1 medications specifically. These products are not regulated as drugs, and quality control varies widely. This is a space worth watching, though it is not yet supported by robust clinical evidence.

A note for providers

Clinical context

GLP-1 medications and the gut microbiome

The 2025 PRISMA systematic review (Gofron et al., Nutrients), the most comprehensive synthesis to date, confirms that GLP-1 analogues consistently alter gut microbiota composition, with the most robust and reproducible finding being elevation of Akkermansia muciniphila across all agents studied. Whether this elevation reflects a class effect of GLP-1 receptor agonism, a consequence of altered gastric emptying, dietary changes, or weight-loss-mediated microbiome shifts cannot be definitively determined from existing literature, which lacks dietary controls and weight-matched comparisons.

Key clinical considerations:

  • Tirzepatide microbiome data is predominantly preclinical. The dual GLP-1/GIP mechanism may produce distinct microbiome effects from GLP-1 monotherapy, but human evidence is very limited as of 2025–2026. The SYNERGY-NASH trial's MASH resolution data (44–62%) suggests gut-liver axis involvement, but microbiome endpoints were not its primary focus.
  • Decreased microbial diversity in some semaglutide studies is worth monitoring. While overall composition shifts toward more favorable genera, reduced alpha diversity, if sustained, may have longer-term implications not yet characterized. Dietary fiber diversity is the most evidence-based countermeasure.
  • GI symptom management through dietary approaches, including fiber adequacy, hydration, and regular activity, supports both symptom burden and microbiome health simultaneously. This is a clinically efficient pairing. GI side effects are the most common reason for GLP-1 medication discontinuation; addressing them proactively improves retention.
  • Probiotic use is unlikely to cause harm in most patients and may support GI tolerability, but should not be recommended with the expectation of specific microbiome outcomes based on current evidence.
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Related article
Taking GLP-1 Medications: What to Expect
A practical guide to starting and maintaining GLP-1 therapy, including managing common GI side effects and the dietary strategies that support tolerability and gut health.
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Related article
Protein Needs on GLP-1 Medications
Why adequate protein intake is critical for preserving muscle mass during GLP-1-driven weight loss, and how to meet your targets when appetite is significantly reduced.

References and sources

  1. Gofron KK, Wasilewski A, Małgorzewicz S. Effects of GLP-1 analogues and agonists on the gut microbiota: a systematic review. Nutrients. 2025;17(8):1303. doi:10.3390/nu17081303
  2. Georgianos PI, Popovic DS. Dual incretin agonism and the gut microbiome: does the heart of metabolic regulation beat in the gut? Expert Review of Clinical Pharmacology. 2025. doi:10.1080/17512433.2025.2559907
  3. Narrative review: The potential for complex interplay between GLP-1 receptor agonists, gut microbiome, and obesity management. Canadian Journal of Physiology and Pharmacology. 2025. doi:10.1139/cjpp-2025-0219
  4. Interplay between GLP-1-based therapies, the gut microbiome, and MASLD/MASH in type 2 diabetes mellitus: a narrative review. Biomedicines. 2025;14(4):806. doi:10.3390/biomedicines14040806
  5. Tolhurst G, Heffron H, Lam YS, et al. Short-chain fatty acids stimulate glucagon-like peptide-1 secretion via the G-protein-coupled receptor FFAR2. Diabetes. 2012;61(2):364–371. doi:10.2337/db11-1019
  6. Wastyk HC, Fragiadakis GK, Perelman D, et al. Gut-microbiota-targeted diets modulate human immune status. Cell. 2021;184(16):4137–4153. doi:10.1016/j.cell.2021.06.019
  7. Depommier C, Everard A, Druart C, et al. Supplementation with Akkermansia muciniphila in overweight and obese human volunteers: a proof-of-concept exploratory study. Nature Medicine. 2019;25:1096–1103. doi:10.1038/s41591-019-0495-2
  8. FDA approval history: semaglutide (Wegovy) for chronic weight management, 2021; tirzepatide (Zepbound) 2023. fda.gov