Overview
At a Glance
SLU-PP-332 is a small molecule developed at Saint Louis University that activates estrogen-related receptors alpha and gamma (ERRα/ERRγ) — orphan nuclear receptors that serve as master regulators of mitochondrial biogenesis and oxidative metabolism. In mouse studies published in 2023, SLU-PP-332 increased fatigue-resistant muscle fibers, improved endurance, and boosted metabolic rate — effects that mimic exercise training — without the mice actually exercising. It has received widespread media attention as an "exercise in a pill." However, SLU-PP-332 is entirely preclinical: there are no human studies, no IND filing, no clinical trials, and no safety data in humans whatsoever. The gap between promising mouse data and a safe, effective human therapy is enormous.
SLU-PP-332 has been tested only in mice. There are no human pharmacokinetic, safety, tolerability, or efficacy studies. Nothing in this article should be interpreted as an endorsement of human use. The compound has no regulatory approval anywhere in the world.
SLU-PP-332 emerged from a drug discovery program led by Thomas Burris and colleagues at Saint Louis University, published in the Journal of Medicinal Chemistry in 2023. The compound belongs to a class of molecules known as "exercise mimetics" — agents designed to reproduce the molecular and physiological benefits of exercise without physical activity. The concept has been pursued since at least 2008, when landmark studies showed that the PPARδ agonist GW501516 (Cardarine) and the AMPK activator AICAR could enhance endurance in sedentary mice (Narkar et al., 2008).
What distinguishes SLU-PP-332 from earlier exercise mimetics is its molecular target. Rather than activating PPARδ (as GW501516 does) or AMPK (as AICAR does), SLU-PP-332 directly activates estrogen-related receptors — specifically ERRα and ERRγ. These are orphan nuclear receptors (meaning their natural ligand was unknown) that are constitutively active transcription factors. ERRα and ERRγ are among the most important regulators of mitochondrial function, fatty acid oxidation, and oxidative phosphorylation in tissues with high energy demands: skeletal muscle, heart, kidney, and brown adipose tissue (Giguère, 2008).
In the published mouse studies, SLU-PP-332 treatment produced measurable changes in muscle fiber composition — shifting toward slow-twitch, oxidative, fatigue-resistant fibers — and improved treadmill endurance without the animals undergoing any exercise training. The compound also increased whole-body metabolic rate and markers of mitochondrial biogenesis in treated muscle tissue (Bahri et al., 2023).
The media narrative of "exercise in a pill" has generated enormous public interest. But it is critical to understand what SLU-PP-332 is and is not at this stage: it is a promising early-stage research compound with interesting mouse data. It is not a drug. It has not been tested in humans. Its safety profile is entirely unknown in people. The history of exercise mimetics — particularly the cautionary tale of GW501516, which was abandoned after causing cancer in rodents — underscores that early preclinical promise frequently does not translate into safe, effective human therapeutics.
Quick Facts
| Property | Details |
|---|---|
| Chemical class | Small molecule (synthetic organic compound) |
| Target receptors | Estrogen-related receptor alpha (ERRα) and gamma (ERRγ) |
| Receptor family | Orphan nuclear receptors (NR3B subfamily) |
| Mechanism | Direct agonism — activates ERR transcriptional programs for mitochondrial biogenesis and oxidative metabolism |
| Species tested | Mice only |
| Human trials | None — no IND filed, no clinical development announced |
| FDA approval | None |
| Developer | Thomas Burris laboratory, Saint Louis University |
| Primary publication | Journal of Medicinal Chemistry, 2023 |
| WADA status | Not specifically listed, but exercise mimetics are a monitored category |
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
How It Works
The ERR Family: Master Regulators of Energy Metabolism
The estrogen-related receptors (ERRs) are a family of three orphan nuclear receptors — ERRα, ERRβ, and ERRγ — that were originally identified due to their structural similarity to estrogen receptors. Despite the name, ERRs do not bind estrogen and are not part of the estrogen signaling pathway. They are "orphan" receptors because no endogenous ligand has been definitively identified — they appear to be constitutively active, meaning they are always "on" to some degree (Giguère, 2008).
ERRα and ERRγ are highly expressed in tissues with enormous energy demands: cardiac muscle, skeletal muscle, kidney, and brown adipose tissue. They regulate the expression of hundreds of genes involved in:
- Mitochondrial biogenesis: The creation of new mitochondria — the cellular organelles responsible for aerobic energy production
- Fatty acid oxidation: The metabolic pathway by which fats are broken down for energy (beta-oxidation)
- Oxidative phosphorylation: The electron transport chain and ATP synthase — the final steps of aerobic energy generation
- Tricarboxylic acid (TCA) cycle: The central metabolic cycle that feeds electrons into the electron transport chain
- Glucose metabolism: Regulation of glucose uptake and glycolytic enzymes
The Exercise Connection: PGC-1α and ERR
When you exercise, your muscles activate a transcriptional coactivator called PGC-1α (peroxisome proliferator-activated receptor gamma coactivator 1-alpha). PGC-1α is often called the "master regulator of mitochondrial biogenesis" and is considered one of the key molecular mediators of exercise adaptation (Fan & Evans, 2017).
PGC-1α does not bind DNA directly. Instead, it works by docking onto and enhancing the activity of transcription factors — including ERRα and ERRγ. The PGC-1α/ERR axis is one of the most important transcriptional partnerships in exercise physiology:
- Exercise activates PGC-1α through AMPK and calcium signaling in contracting muscle
- PGC-1α coactivates ERRα and ERRγ on the promoters of metabolic target genes
- ERRα/γ drive transcription of mitochondrial, fatty acid oxidation, and oxidative metabolism genes
- Result: Increased mitochondrial density, improved endurance capacity, shift toward oxidative (slow-twitch) muscle fibers
SLU-PP-332 short-circuits this pathway by directly activating ERRα and ERRγ without requiring PGC-1α activation — and therefore without requiring exercise. The compound binds to the ERR ligand-binding domain and enhances its transcriptional activity, turning on the same gene programs that exercise activates through the PGC-1α intermediate (Bahri et al., 2023).
ERRα vs. ERRγ: Different but Overlapping Roles
| Feature | ERRα | ERRγ |
|---|---|---|
| Expression | Ubiquitous — highest in heart, muscle, kidney, brown fat | More restricted — heart, skeletal muscle, brain, kidney |
| Primary functions | Fatty acid oxidation, mitochondrial biogenesis, broad metabolic control | Oxidative phosphorylation, electron transport chain genes, muscle fiber type specification |
| Knockout phenotype (mice) | Reduced fat mass, impaired metabolic adaptation to cold stress | Neonatal lethality (heart defects) — demonstrating critical role in cardiac energy metabolism |
| Role in exercise | Broad metabolic adaptation | Oxidative muscle fiber specification, endurance capacity |
SLU-PP-332 activates both ERRα and ERRγ, which the researchers argue provides a more comprehensive activation of exercise-related metabolic programs than targeting either receptor alone (Bahri et al., 2023).
How SLU-PP-332 Differs from Other Exercise Mimetics
| Compound | Target | Mechanism | Status |
|---|---|---|---|
| SLU-PP-332 | ERRα/ERRγ | Nuclear receptor agonism — activates transcription of mitochondrial and metabolic genes | Preclinical (mice only) |
| GW501516 (Cardarine) | PPARδ | Nuclear receptor agonism — activates fatty acid oxidation and endurance gene programs | Abandoned — cancer in rodents |
| AICAR | AMPK | Kinase activation — mimics energy-depleted state, triggers metabolic adaptation | Research tool; poor oral bioavailability |
| Exercise itself | Multiple pathways | AMPK, calcium, PGC-1α, ERRs, PPARs, mTOR, and hundreds of other signals simultaneously | Gold standard; no substitute |
Important Limitations of the Mechanism
While the molecular mechanism is well-characterized, several caveats deserve emphasis:
- Exercise activates far more pathways than ERR alone. Physical activity triggers cardiovascular adaptation, neuroplasticity, immune modulation, bone remodeling, hormonal changes, and psychological benefits that a single receptor agonist cannot replicate.
- Nuclear receptor agonism has unpredictable tissue effects. ERRα and ERRγ are expressed in many tissues. Systemic activation may produce effects in tissues where enhanced metabolic activity is not desired or is potentially harmful.
- The PGC-1α/ERR axis has feedback mechanisms that may be disrupted by pharmacological activation. The long-term consequences of bypassing normal regulatory checkpoints are unknown.
- Mouse metabolism differs substantially from human metabolism. Mice have much higher basal metabolic rates, different muscle fiber composition, and different pharmacokinetics. Effects observed in mice frequently do not translate to humans.
Go Deeper
- Giguère (2008) — "Transcriptional control of energy homeostasis by the estrogen-related receptors" — Endocrine Reviews
- Fan & Evans (2017) — "Exercise Mimetics: Impact on Health and Performance" — Cell Metabolism
- Bahri et al. (2023) — "Pharmacological activation of ERRα/γ by SLU-PP-332" — Journal of Medicinal Chemistry
- Rangwala et al. (2010) — "Estrogen-related receptor gamma is a key regulator of muscle mitochondrial activity and oxidative capacity" — JBC
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Research
The Primary Study: Bahri et al. (2023)
The foundational and, as of this writing, only primary research paper on SLU-PP-332 was published in the Journal of Medicinal Chemistry by Bahri, Burris, and colleagues at Saint Louis University. The study described the design, synthesis, and in vivo testing of SLU-PP-332 as a dual ERRα/ERRγ agonist (Bahri et al., 2023).
Key findings from the mouse studies:
- Muscle fiber type shift: Treated mice showed a significant increase in type I (slow-twitch, oxidative) and type IIa (fast oxidative) muscle fibers relative to type IIb/IIx (fast glycolytic) fibers. This shift toward fatigue-resistant fibers is one of the hallmark adaptations of endurance exercise training.
- Improved endurance: SLU-PP-332-treated mice ran significantly longer on a treadmill exhaustion test compared to vehicle-treated controls — without having undergone any exercise training.
- Increased metabolic rate: Whole-body oxygen consumption (VO2) was elevated in treated animals, suggesting increased oxidative metabolism.
- Mitochondrial gene expression: Skeletal muscle from treated mice showed upregulation of genes involved in mitochondrial biogenesis, electron transport chain components, and fatty acid oxidation — consistent with ERRα/γ target gene activation.
- No obvious toxicity: The published data reported no overt toxicity in treated mice at the doses tested. However, formal toxicology studies were not described.
Context: The Exercise Mimetics Field
SLU-PP-332 did not emerge in a vacuum. The concept of pharmacologically mimicking exercise has a research history spanning nearly two decades:
| Year | Milestone | Significance |
|---|---|---|
| 2004 | GW501516 (PPARδ agonist) shown to enhance fatty acid oxidation in mice | Early proof-of-concept for exercise mimicry via nuclear receptor agonism |
| 2008 | Narkar et al. publish landmark Cell paper: GW501516 + AICAR enhance endurance in sedentary mice | Established "exercise in a pill" as a serious research concept (PMID: 18674809) |
| 2007–2009 | GW501516 development abandoned after rodent cancer findings | Cautionary tale: PPARδ agonism at therapeutic doses caused tumors in multiple organs in rats and mice |
| 2008 | Giguère reviews ERR biology and metabolic control | Established ERRs as potential therapeutic targets for metabolic disease (PMID: 18660465) |
| 2010 | Rangwala et al. characterize ERRγ role in muscle metabolism | Showed ERRγ drives oxidative capacity in skeletal muscle (PMID: 20089855) |
| 2017 | Fan & Evans review exercise mimetics landscape | Comprehensive review of molecular targets for exercise mimicry (PMID: 28768173) |
| 2023 | Bahri et al. publish SLU-PP-332 | First ERRα/γ dual agonist shown to mimic exercise effects in mice (PMID: 36719780) |
Comparison: SLU-PP-332 vs. GW501516 (Cardarine)
GW501516 is the most relevant comparison and the most important cautionary precedent for SLU-PP-332. Both are nuclear receptor agonists designed to mimic exercise, but they target different receptors and have different risk profiles:
| Feature | SLU-PP-332 | GW501516 (Cardarine) |
|---|---|---|
| Target | ERRα/ERRγ | PPARδ |
| Receptor family | Orphan nuclear receptors | Peroxisome proliferator-activated receptors |
| Primary effects (mice) | Muscle fiber type shift, endurance, metabolic rate | Fatty acid oxidation, endurance, fat loss |
| Cancer signal | None reported (limited data) | Tumors in multiple organs in rodents |
| Human studies | None | Phase 1/2 (abandoned before completion) |
| Development status | Early preclinical | Abandoned by GSK due to safety concerns |
| Black market availability | Limited but increasing | Widely available through research chemical suppliers |
GW501516 (Cardarine) was the previous leading "exercise mimetic" candidate. It produced impressive metabolic and endurance effects in mice and progressed to early human trials. It was then abandoned after preclinical safety studies revealed it caused tumors in the colon, liver, stomach, bladder, skin, tongue, and other organs in rats. Despite this, GW501516 is widely sold and used as a research chemical / performance enhancer. The fact that SLU-PP-332 acts through a different receptor (ERR vs. PPARδ) does not guarantee it will be safer — it simply means we do not yet know.
ERR Biology: Foundational Research
The scientific foundation for SLU-PP-332 rests on decades of ERR research:
- ERRα knockout mice (Dufour et al., 2007) have reduced fat mass and impaired adaptation to metabolic stress, confirming ERRα's role in energy homeostasis (PMID: 17612497).
- ERRγ is essential for cardiac function — ERRγ knockout mice die shortly after birth from heart failure due to inability to switch from glycolytic to oxidative metabolism (Alaynick, 2008).
- ERRγ specifies oxidative muscle fiber type. Rangwala et al. (2010) demonstrated that ERRγ overexpression in mouse skeletal muscle converts fast-twitch glycolytic fibers into slow-twitch oxidative fibers — the same phenotype produced by endurance training (PMID: 20089855).
- ERRs cooperate with PGC-1α to form the core transcriptional axis of exercise adaptation, controlling hundreds of metabolic target genes (Giguère, 2008).
Limitations of the Current Research
- Single primary publication: The SLU-PP-332 data comes from one research paper from one laboratory. Independent replication has not been published.
- Mouse studies only: No data exists in any other species, including humans.
- No formal toxicology: The absence of "obvious toxicity" in short-term mouse studies is not the same as establishing safety. Comprehensive toxicology studies (chronic dosing, carcinogenicity, reproductive toxicity, organ-specific toxicity panels) have not been published.
- Pharmacokinetics unknown in humans: Absorption, distribution, metabolism, excretion, half-life, and bioavailability in humans are entirely unknown.
- No dose-response in humans: The therapeutic index (ratio of effective dose to toxic dose) in humans is unknown.
- Long-term consequences unclear: Chronic activation of ERRα/γ across all tissues — not just skeletal muscle — may have unintended consequences that only manifest with prolonged exposure.
Further Reading
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Uses
SLU-PP-332 is not FDA-approved, not in clinical trials, and has not been tested in humans for any indication. All "uses" discussed below are theoretical extrapolations from mouse data and ERR biology. None should be interpreted as validated clinical applications.
Theoretical Applications
Based on the known biology of ERRα/ERRγ and the mouse data for SLU-PP-332, researchers have proposed several potential therapeutic applications — all of which remain speculative until human data is generated:
| Application | Rationale | Evidence Level |
|---|---|---|
| Obesity and metabolic syndrome | ERR activation increases fatty acid oxidation and metabolic rate. In mice, SLU-PP-332 increased whole-body oxygen consumption. Enhanced oxidative metabolism could theoretically improve metabolic syndrome markers. | Mouse data only |
| Muscle wasting / sarcopenia | Age-related muscle loss involves a shift from oxidative to glycolytic muscle fibers and a decline in mitochondrial function. ERRα/γ activation could counteract this by promoting oxidative fiber maintenance and mitochondrial biogenesis. | Theoretical — mechanism-based |
| Heart failure | The failing heart has impaired mitochondrial function and shifts from fatty acid oxidation to glycolysis. ERRα and ERRγ are critical regulators of cardiac energy metabolism. Restoring ERR activity could theoretically improve cardiac energetics. | Theoretical — mechanism-based |
| Exercise intolerance in mobility-impaired patients | Individuals who cannot exercise (post-surgical, wheelchair-bound, critically ill, frail elderly) miss the metabolic benefits of physical activity. An exercise mimetic could provide some of those benefits pharmacologically. | Conceptual rationale only |
| Post-surgical recovery | Prolonged bedrest after surgery leads to rapid muscle atrophy and metabolic deconditioning. Maintaining oxidative muscle capacity during immobility could speed recovery. | Conceptual rationale only |
| Type 2 diabetes | Exercise is one of the most effective interventions for type 2 diabetes. ERR-mediated improvements in fatty acid oxidation and mitochondrial function could improve insulin sensitivity and glucose control. | Mouse data only; no glucose data published for SLU-PP-332 |
What SLU-PP-332 Cannot Replace
Even in the most optimistic scenario, an ERR agonist cannot replicate the full spectrum of exercise benefits:
- Cardiovascular adaptation: Exercise improves cardiac output, blood vessel function, blood pressure regulation, and VO2max through hemodynamic stress. A pill that changes muscle metabolism does not condition the heart and vasculature.
- Neurological benefits: Exercise increases BDNF (brain-derived neurotrophic factor), improves mood, reduces depression and anxiety, enhances cognitive function, and may reduce dementia risk through multiple pathways that are independent of ERR signaling.
- Bone health: Weight-bearing exercise stimulates osteoblast activity and bone mineral density maintenance through mechanical loading signals. ERR activation does not provide mechanical stress to bone.
- Immune function: Moderate exercise enhances immune surveillance through mechanisms (improved lymphocyte circulation, reduced chronic inflammation) that are not mediated by ERR.
- Psychological benefits: The stress relief, social interaction, sense of accomplishment, and mental health benefits of exercise cannot be pharmacologically replicated.
The "Exercise in a Pill" Framing: Hype vs. Reality
The media narrative around SLU-PP-332 has focused on the "exercise in a pill" concept. This framing is misleading in several important ways:
- SLU-PP-332 activates one of many exercise pathways. Exercise simultaneously activates AMPK, mTOR, PGC-1α, PPARδ, ERRs, calcium signaling, hypoxia pathways, mechanical signaling, hormonal cascades, and dozens of other molecular systems. No single drug can replicate this complexity.
- The mouse data shows metabolic changes, not "exercise." Increased treadmill time and altered muscle fiber composition are specific, measurable endpoints — they are not equivalent to "doing exercise."
- Realistic framing: SLU-PP-332 is better described as a "metabolic enhancer that partially mimics one set of exercise adaptations" — which is less catchy but more accurate.
Further Reading
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Dosing
SLU-PP-332 has never been administered to humans in any clinical or research setting. There is no established human dose, no known therapeutic window, no pharmacokinetic profile, and no safety margin. The mouse dosing information below is provided solely for scientific context — it cannot and should not be extrapolated to human use. Self-administration of this compound carries unknown and potentially serious risks.
Mouse Study Dosing (Research Context Only)
In the published preclinical study, SLU-PP-332 was administered to mice as follows:
| Parameter | Details |
|---|---|
| Species | Mice (C57BL/6 strain) |
| Route of administration | Intraperitoneal (IP) injection |
| Dose range tested | Approximately 25–50 mg/kg |
| Dosing frequency | Once or twice daily |
| Treatment duration | Several weeks (varied by experiment) |
| Vehicle | Standard research vehicle (DMSO/carrier solution) |
Source: Bahri et al. (2023) — SLU-PP-332 mouse dosing parameters (Journal of Medicinal Chemistry).
Why Mouse Doses Cannot Be Translated to Humans
Converting mouse doses to human doses is not a simple matter of adjusting for body weight. Multiple factors make direct translation unreliable:
- Allometric scaling: Mice have much higher metabolic rates per kilogram of body weight than humans. A dose that is tolerable in a mouse may be vastly different (higher or lower) than what is appropriate in a human. The FDA uses body surface area (BSA) conversion, not simple weight conversion, and even BSA-based estimates are only rough approximations for novel compounds.
- Route of administration: SLU-PP-332 was given by intraperitoneal injection in mice — a route not used in human medicine. Oral bioavailability, which would be the practical route for a human "exercise pill," has not been published.
- Pharmacokinetics: Absorption, distribution, metabolism, and excretion in humans are completely unknown. The compound may be rapidly metabolized, poorly absorbed, or distributed differently in human tissues.
- Therapeutic index: The margin between an effective dose and a toxic dose in humans has not been established. Without this information, any human dosing is a guess with unknown risk.
- Species-specific metabolism: Mice and humans have different cytochrome P450 enzyme profiles, different plasma protein binding characteristics, and different organ-specific drug metabolism. A compound well-tolerated in mice may generate toxic metabolites in humans.
Online Dosing Claims
As SLU-PP-332 has appeared on the research chemical market, dosing recommendations have emerged in online forums and from supplement-adjacent marketing. These claims are:
- Not based on clinical data — no human dose-response studies exist
- Not based on pharmacokinetic data — human PK parameters are unknown
- Often derived from crude mouse-to-human weight conversions — which are pharmacologically unreliable
- Not validated for safety — there is no known safe dose in humans
Individuals who self-administer SLU-PP-332 obtained from research chemical suppliers are conducting uncontrolled self-experimentation with a compound that has no human safety data. The purity, identity, and potency of research chemical products are not guaranteed. This is not analogous to using a compound with Phase 1/2 safety data (such as some peptides) — SLU-PP-332 has literally zero human exposure data in any context.
Further Reading
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Results: What the Mouse Data Shows
Unlike compounds with Phase 1/2 clinical data and years of clinical use (e.g., ipamorelin, BPC-157), SLU-PP-332 has absolutely no human data. The results below are from published mouse studies only. Interpreting mouse metabolic data as predictive of human outcomes is a well-known source of error in drug development — approximately 90% of drugs that work in animal models fail in human clinical trials.
Published Mouse Study Results
| Endpoint | Finding | Significance |
|---|---|---|
| Treadmill endurance | SLU-PP-332-treated mice ran significantly longer before exhaustion compared to controls | Suggests improved aerobic/endurance capacity without exercise training. The hallmark finding of the study. |
| Muscle fiber type | Increased proportion of type I (slow oxidative) and type IIa (fast oxidative) fibers; decreased type IIb/IIx (fast glycolytic) fibers | This fiber type shift is characteristic of endurance exercise training. It indicates a genuine remodeling of muscle toward fatigue-resistant phenotype. |
| Metabolic rate | Increased whole-body oxygen consumption (VO2) | Suggests elevated oxidative metabolism at rest — consistent with increased mitochondrial activity in muscle and other tissues. |
| Mitochondrial markers | Upregulation of mitochondrial biogenesis genes (e.g., cytochrome c, COX subunits, ATP synthase components) in skeletal muscle | Molecular confirmation that ERR target genes are being activated in vivo, consistent with the proposed mechanism. |
| Body composition | Trends toward reduced fat mass in treated animals | Consistent with increased fatty acid oxidation, though not the primary endpoint of the published studies. |
| Overt toxicity | No obvious toxic effects reported at the doses and durations tested | Reassuring but very preliminary. "No obvious toxicity" in a short-term mouse study is a low bar — it is not the same as established safety. |
What These Results Mean — and Do Not Mean
- The endurance improvement is real in mice. The treadmill data is objective and reproducible within the study design. Mice treated with SLU-PP-332 genuinely ran longer. This is meaningful as proof-of-concept that pharmacological ERR activation can produce functional improvements.
- The fiber type shift is real in mice. Histological and molecular data confirmed the change in muscle fiber composition. This is the same adaptation seen with chronic endurance training.
- These results do not predict human outcomes. The majority of compounds that show efficacy in mice fail in human trials. Metabolism, pharmacokinetics, tissue distribution, and safety profiles differ enormously between species.
- "No toxicity observed" is not "safe." The study was not designed as a toxicology study. Short-term administration in young, healthy mice does not reveal chronic toxicity, organ-specific damage at higher doses, carcinogenicity, or reproductive toxicity.
Comparison: Preclinical Promise vs. Clinical Reality
To calibrate expectations, consider the track record of exercise mimetics that showed strong preclinical results:
| Compound | Mouse Results | Human Outcome |
|---|---|---|
| GW501516 | Dramatic endurance improvement, fat loss, metabolic enhancement | Abandoned — caused tumors in multiple organs in rodent safety studies before clinical program completed |
| AICAR | Improved endurance in sedentary mice | Poor oral bioavailability; not developed as a therapeutic. Remains a research tool only. |
| SRT1720 (sirtuin activator) | Extended lifespan and improved metabolism in obese mice | Development discontinued. Specificity of sirtuin activation questioned by independent researchers. |
| SLU-PP-332 | Endurance improvement, fiber type shift, metabolic enhancement | Unknown — no human studies conducted |
Anecdotal Reports from Self-Experimenters
Because SLU-PP-332 is available through research chemical suppliers, some individuals have self-administered it and posted reports online. These reports are:
- Unverified: The identity, purity, and dose of the compound consumed cannot be confirmed
- Uncontrolled: No baseline measurements, no placebo comparison, concurrent use of other compounds is common
- Subject to massive bias: Individuals who purchase a novel "exercise pill" and self-administer it are highly motivated to perceive positive effects
- Not medical evidence: Anecdotal self-experimentation reports have essentially zero evidentiary value for establishing safety or efficacy
Further Reading
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Side Effects
SLU-PP-332 has never been administered to humans in any controlled setting. There is no Phase 1 safety data, no tolerability data, no adverse event reporting, and no post-marketing surveillance. Anyone using this compound is accepting completely unknown risks. The information below discusses theoretical concerns — actual risks may be entirely different from what is predicted.
What the Mouse Data Shows About Safety
| Observation | Interpretation | Limitation |
|---|---|---|
| No overt toxicity at doses tested | The compound did not cause obvious illness, weight loss, or death in mice at the administered doses | Short treatment duration; not a formal toxicology study; "no obvious toxicity" is a very low bar |
| No reported organ damage | Histopathology of major organs was not described in detail in the primary publication | Absence of reported damage is not the same as confirmed organ safety |
| Normal behavior in treated mice | Animals appeared healthy and behaved normally during treatment | Mice do not report subjective symptoms; subtle toxicity may go undetected |
Theoretical Risks Based on ERR Biology
- Cardiac effects: ERRα and ERRγ are highly expressed in cardiac tissue and are critical regulators of heart energy metabolism. Pharmacological hyperactivation of these receptors in the heart could theoretically cause cardiac hypertrophy, arrhythmias, or altered cardiac energetics. ERRγ knockout is lethal due to heart failure — this underscores the sensitivity of the heart to ERR signaling disruption in either direction (Alaynick, 2008).
- Metabolic disruption: Chronic systemic ERR activation may alter glucose homeostasis, lipid metabolism, or insulin sensitivity in unpredictable ways. While the mouse data suggests beneficial metabolic effects, prolonged activation of oxidative metabolism in all tissues may have unintended consequences.
- Cancer risk: Some nuclear receptor agonists have been associated with increased cancer risk. GW501516 (PPARδ agonist) caused tumors in multiple organs. While ERRα/γ are different receptors, the possibility that chronic ERR activation could promote cell proliferation or interfere with tumor suppressor pathways cannot be excluded without long-term carcinogenicity data.
- Kidney effects: ERRα and ERRγ are highly expressed in the kidney, which has enormous energy demands for active transport. Altered ERR signaling could affect renal function, electrolyte balance, or acid-base homeostasis.
- Reproductive effects: Despite the "estrogen-related" name, ERRs do not directly mediate estrogen signaling. However, ERRα has been implicated in some estrogen-responsive pathways, and the effects of chronic pharmacological ERR activation on reproductive organs and fertility are completely unknown.
- Drug interactions: ERRα and ERRγ participate in metabolic gene regulation that overlaps with other nuclear receptor pathways (PPAR, LXR, etc.). Pharmacological ERR activation could interact with medications metabolized by the same enzymatic pathways.
- Off-target effects: The selectivity of SLU-PP-332 for ERRα/γ versus other nuclear receptors has been characterized in vitro, but off-target effects in a whole organism may differ from cell-based assays.
Lessons from GW501516 (Cardarine) Safety Profile
The most instructive precedent for SLU-PP-332 safety concerns is GW501516:
- GW501516 showed no obvious toxicity in short-term mouse studies — similar to what has been reported for SLU-PP-332
- GW501516 appeared safe in early human exposure (Phase 1 data)
- GW501516 was then found to cause tumors in multiple organs when tested at higher doses and for longer durations in rodent carcinogenicity studies required for regulatory approval
- This cancer signal was not apparent in the initial efficacy studies — it only emerged in formal toxicology studies
- Lesson: Early-stage "no toxicity" findings provide almost no assurance about long-term safety
Research Chemical Purity Risks
For individuals who obtain SLU-PP-332 through research chemical suppliers, additional risks include:
- Unknown purity: Research chemicals are not manufactured under pharmaceutical-grade GMP conditions. Impurities, degradation products, or synthesis byproducts may be present.
- Identity uncertainty: Without independent analytical testing, there is no guarantee that the product actually contains SLU-PP-332.
- Dose uncertainty: Potency may vary between batches and suppliers.
- No quality oversight: Research chemical suppliers are not regulated by the FDA for human-use products.
Further Reading
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Regulatory Status
FDA Status
| Category | Status |
|---|---|
| FDA approval | None — not approved for any indication |
| IND filing | None — no Investigational New Drug application has been filed |
| Clinical trials | None — not registered on ClinicalTrials.gov for any study |
| Compounding status | Not listed on the FDA bulk substances list (not a candidate for compounding pharmacy preparation) |
| Orphan drug designation | None |
| Fast track / breakthrough | None |
What This Means Practically
SLU-PP-332 exists in a regulatory gray zone common to novel research compounds:
- It is not a controlled substance: SLU-PP-332 is not listed under any DEA schedule, meaning possession is not a criminal offense.
- It is not approved for human consumption: Selling it for human use or marketing it with therapeutic claims would violate FDA regulations.
- It is sold as a "research chemical": Suppliers market it as "for research purposes only" or "not for human consumption" — a legal framework that permits sale while disclaiming responsibility for human use.
- No prescription pathway exists: Unlike some unapproved peptides available through compounding pharmacies, SLU-PP-332 has no physician-prescription pathway.
- No manufacturing standards apply: Products sold as SLU-PP-332 are not subject to any pharmaceutical manufacturing, quality, or purity standards.
Comparison: Regulatory Status of Exercise Mimetics
| Compound | Regulatory Status | Availability |
|---|---|---|
| SLU-PP-332 | No regulatory action; not scheduled; no IND | Research chemical market only |
| GW501516 (Cardarine) | Abandoned by GSK; not approved; not scheduled. WADA prohibited substance. | Widely available as research chemical. Prohibited in sport. |
| AICAR | Research reagent; not approved for human use. WADA prohibited substance. | Available as research chemical. |
| Exercise | Universally recommended by every medical authority | Free and widely available |
WADA and Anti-Doping Considerations
As of this writing, SLU-PP-332 is not specifically listed on the WADA Prohibited List by name. However:
- WADA's Prohibited List includes a catch-all provision for metabolic modulators and exercise mimetics under Section S4 (Hormone and Metabolic Modulators)
- WADA monitors emerging exercise mimetics and has the authority to add them to the prohibited list
- Athletes subject to anti-doping testing should assume that novel exercise mimetics carry significant anti-doping risk
- The detection of SLU-PP-332 in biological samples may be possible through high-resolution mass spectrometry methods used by WADA-accredited laboratories
The Path to Clinical Development (If It Happens)
For SLU-PP-332 to become an approved medication, it would need to complete the standard drug development pipeline:
- Formal preclinical studies: GLP-compliant toxicology, pharmacokinetics in multiple species, carcinogenicity testing, reproductive toxicity
- IND application: Submission to the FDA with preclinical safety data package
- Phase 1: First-in-human safety and pharmacokinetic study (typically 20–80 healthy volunteers)
- Phase 2: Dose-finding and preliminary efficacy in target patient population (typically 100–300 patients)
- Phase 3: Large-scale, randomized, placebo-controlled efficacy and safety trials (typically 1,000–3,000+ patients)
- NDA submission and FDA review
- Estimated timeline: 8–15 years from IND filing to potential approval, if everything goes well
None of these steps have been initiated for SLU-PP-332.
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Cost
SLU-PP-332 is not available through any legitimate pharmaceutical or compounding pharmacy channel. All products sold are marketed as research chemicals "not for human consumption." Quality, purity, and identity cannot be guaranteed. There is no regulatory oversight of these products.
Typical Pricing (Research Chemical Market)
| Source Type | Typical Price | What You Get | Quality Assurance |
|---|---|---|---|
| Research chemical supplier | $50–$150 per 250–500 mg | Powder or solution, labeled "for research only" | Variable. Some provide certificates of analysis (COA); quality ranges widely between suppliers. |
| Premium research supplier | $100–$200 per 250–500 mg | Higher-purity product with third-party testing documentation | Better documentation, but still no pharmaceutical-grade manufacturing standards |
| Compounding pharmacy | Not available | N/A | N/A — no compounding pharmacy produces SLU-PP-332 |
| Prescription pharmacy | Not available | N/A | N/A — no approved pharmaceutical product exists |
Insurance Coverage
No insurance plan covers SLU-PP-332. It is not an approved medication, not a compounded preparation, and has no billing code. All costs are entirely out-of-pocket.
Cost Comparison: Exercise Mimetics and Metabolic Compounds
| Compound | Typical Monthly Cost | Availability | Insurance |
|---|---|---|---|
| SLU-PP-332 | Unknown (no established dosing) | Research chemical only | Not covered |
| GW501516 (Cardarine) | $40–$80 | Research chemical | Not covered |
| Metformin | $4–$30 | Prescription (FDA-approved) | Covered for diabetes |
| Gym membership | $20–$80 | Universally available | Some HSA/FSA eligible |
| Exercise (walking, running) | Free | Universally available | N/A |
The True Cost: Risk vs. Benefit Calculation
Beyond the dollar cost, the relevant cost analysis for SLU-PP-332 includes:
- Unknown health risk: The compound has no human safety data. The cost of an adverse health event from an untested compound is potentially catastrophic.
- Uncertain product quality: Research chemical purity and identity issues add risk.
- Uncertain efficacy: Whether SLU-PP-332 produces any beneficial effects in humans is entirely unknown.
- Opportunity cost: Money and attention spent on an unproven compound could be invested in evidence-based approaches (exercise, nutrition, sleep optimization, proven medications).
Further Reading
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Questions & Answers
Q: Is SLU-PP-332 really "exercise in a pill"?
Answer: No. This is a media simplification that dramatically overstates what the compound does. SLU-PP-332 activates one transcriptional pathway (ERRα/γ) that is among the many pathways activated by exercise. In mice, this produced measurable improvements in endurance and muscle fiber composition. But exercise activates dozens of molecular systems simultaneously — cardiovascular, neurological, musculoskeletal, immune, hormonal, and psychological. A single-target small molecule cannot replicate the full spectrum of exercise benefits. A more accurate description would be: "a compound that activates one of the molecular pathways involved in exercise adaptation, producing partial exercise-like metabolic effects in mice" (Fan & Evans, 2017).
Q: Is SLU-PP-332 safer than GW501516 (Cardarine)?
Answer: Unknown. The only honest answer is that we do not have enough data to compare their safety profiles. GW501516 appeared safe in short-term studies before cancer was discovered in longer-term testing. SLU-PP-332 has only been through short-term mouse studies. The fact that it targets a different receptor (ERR vs. PPARδ) does not inherently make it safer — it simply means we have not yet tested it enough to know. Both are nuclear receptor agonists that broadly activate metabolic gene programs, and both carry theoretical risks that can only be assessed through comprehensive toxicology studies that have not been performed for SLU-PP-332 (Bahri et al., 2023).
Q: Can SLU-PP-332 replace exercise?
Answer: No — not even theoretically. Exercise provides cardiovascular conditioning, bone strengthening, neuroplasticity, immune modulation, hormonal balance, stress relief, social connection, and psychological well-being. ERR activation in skeletal muscle addresses only the metabolic component. Even in the most optimistic future scenario where an exercise mimetic reaches clinical use, it would likely be positioned as a supplement to exercise for people who cannot exercise fully — not as a replacement for physical activity (Hawley et al., 2014).
Q: Has SLU-PP-332 been tested in humans?
Answer: No. As of this writing, SLU-PP-332 has been tested only in mice. There are no published or registered human studies — no Phase 1, no pharmacokinetic studies, no tolerability data. No IND (Investigational New Drug) application has been filed with the FDA. The compound is years away from legitimate human testing, if it proceeds at all.
Q: I can buy SLU-PP-332 online. Is it safe to take?
Answer: There is no way to assess whether it is safe because no human safety data exists. Products sold online as SLU-PP-332 are research chemicals manufactured without pharmaceutical-grade quality controls. There is no guarantee of purity, identity, or potency. Individuals who self-administer these products are conducting uncontrolled self-experimentation with a compound that has literally zero human exposure data. This is qualitatively different from using a compound like ipamorelin, which has Phase 2 clinical trial data and years of clinical use — SLU-PP-332 has never been given to a human in any controlled setting.
Q: Does SLU-PP-332 affect estrogen or have estrogenic side effects?
Answer: No — despite the confusing name. "Estrogen-related receptors" (ERRs) were named because of their structural similarity to estrogen receptors at the DNA-binding domain level. However, ERRs do not bind estrogen, are not activated by estrogen, and do not participate in estrogen signaling. SLU-PP-332 activating ERRα/γ would not be expected to cause estrogenic effects such as gynecomastia, water retention from estrogen, or changes to the HPG axis. The name is a historical artifact of how the receptors were discovered, not a reflection of their function (Giguère, 2008).
Q: How does SLU-PP-332 compare to proven metabolic interventions?
Answer: There is no comparison. SLU-PP-332 has zero human clinical evidence. By contrast:
- Exercise: Thousands of randomized controlled trials, decades of epidemiological data, universally recommended by every medical authority
- Metformin: FDA-approved, decades of human safety data, proven metabolic benefits
- Caloric restriction: Extensive human data for weight management and metabolic improvement
- Sleep optimization: Well-established metabolic and health benefits
SLU-PP-332 is an interesting research compound. It is not in the same category as proven interventions.
Further Reading
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
Key Takeaways
Based on the available evidence:
- SLU-PP-332 is a small molecule ERRα/ERRγ agonist developed at Saint Louis University and published in 2023. It activates estrogen-related receptors — orphan nuclear receptors that are master regulators of mitochondrial biogenesis and oxidative metabolism — producing "exercise mimetic" effects in mice.
- In mouse studies, it produced measurable exercise-like adaptations: increased fatigue-resistant (slow-twitch, oxidative) muscle fibers, improved treadmill endurance, elevated metabolic rate, and upregulated mitochondrial gene expression — without the mice exercising.
- It has zero human data. No pharmacokinetics, no safety data, no tolerability data, no efficacy data in humans. No IND has been filed. No clinical trials are registered. This is purely preclinical research.
- "Exercise in a pill" is a media oversimplification. SLU-PP-332 activates one of the many molecular pathways involved in exercise adaptation. Exercise activates dozens of systems simultaneously (cardiovascular, neurological, musculoskeletal, immune, hormonal, psychological) that a single receptor agonist cannot replicate.
- The GW501516 cautionary tale is directly relevant. The previous leading exercise mimetic (GW501516/Cardarine) showed similarly impressive preclinical results before being abandoned due to cancer in rodent toxicology studies. SLU-PP-332 targeting a different receptor does not guarantee a different safety outcome.
- Safety in humans is completely unknown. The absence of "obvious toxicity" in short-term mouse studies provides minimal safety assurance. Formal toxicology, carcinogenicity, and chronic dosing studies have not been performed.
- It is available through research chemical suppliers despite having no human safety data — marketed as "for research purposes only." There is no pharmaceutical-grade product, no compounding pharmacy source, and no prescription pathway.
- The path to clinical use is long. If SLU-PP-332 proceeds through formal drug development, it would require years of preclinical toxicology, IND filing, and Phase 1/2/3 clinical trials — an 8–15 year timeline under the best circumstances, with a high probability of failure.
- Realistic framing: SLU-PP-332 is exciting basic science with important implications for understanding exercise biology and potential future therapeutics. It is not a drug, not a supplement, and not a substitute for exercise.
The Bottom Line
SLU-PP-332 represents a legitimate scientific advance in understanding how exercise-related molecular pathways can be pharmacologically activated. The ERRα/γ agonism approach is mechanistically sound and the mouse data is encouraging. But the distance between "promising mouse data" and "safe, effective human therapy" is enormous. Historically, the vast majority of compounds that work in mice never become human medications. Anyone considering self-administration of this compound should understand that they are taking on completely unknown risks with an untested substance — when a proven, free, and universally beneficial alternative exists: exercise itself.
Questions to Consider
- Is the potential benefit of an untested research compound worth the unknown risk, when exercise provides the same underlying benefits with a well-established safety profile?
- If you are interested in metabolic optimization, have you fully utilized evidence-based approaches (regular exercise, sleep optimization, nutrition, proven medications if indicated)?
- Are you aware that "works in mice" is the very first step in drug development, not evidence of human efficacy or safety?
- Do you understand that research chemical products have no quality guarantees and may contain impurities, incorrect amounts, or different compounds entirely?
- Would you be willing to wait for human clinical trial data before assuming this compound is safe and effective?
This content is for informational and educational purposes only. It is not intended as, and should not be interpreted as, medical advice. The information provided does not cover all possible uses, precautions, interactions, or adverse effects, and may not reflect the most recent medical research or guidelines. It should not be used as a substitute for the advice of a qualified healthcare professional. Never disregard professional medical advice or delay seeking treatment because of something you have read here. Always speak with your doctor or pharmacist before starting, stopping, or changing any prescribed medication or treatment. If you think you may have a medical emergency, call your doctor or emergency services immediately. GLPbase does not recommend or endorse any specific tests, physicians, products, procedures, or opinions. Use of this information is at your own risk.
Sources & Further Reading
SLU-PP-332 Primary Research
ERR Biology and Function
- Giguère (2008) — "Transcriptional Control of Energy Homeostasis by the Estrogen-Related Receptors" — Endocrine Reviews
- Rangwala et al. (2010) — "Estrogen-Related Receptor Gamma Is a Key Regulator of Muscle Mitochondrial Activity and Oxidative Capacity" — Journal of Biological Chemistry
- Alaynick (2008) — "Nuclear Receptors, Mitochondria and Lipid Metabolism" — Mitochondrion
- Dufour et al. (2007) — "Genome-wide Orchestration of Cardiac Functions by the Orphan Nuclear Receptors ERRα and ERRγ" — Cell Metabolism
Exercise Mimetics: Comparative Research
- Narkar et al. (2008) — "AMPK and PPARδ Agonists Are Exercise Mimetics" — Cell
- Fan & Evans (2017) — "Exercise Mimetics: Impact on Health and Performance" — Cell Metabolism
Exercise as Therapeutic Intervention
ERR Agonists as Therapeutic Targets
- Li et al. (2022) — "ERR Agonists as Potential Therapeutic Agents for Metabolic Disease" — Pharmacological Research
- Wall et al. (2023) — "Exercise Mimetics: Harnessing the Therapeutic Effects of Physical Activity" — Nature Reviews Drug Discovery
GW501516 (Cardarine) Safety Context
- Narkar et al. (2008) — GW501516 endurance data — Cell
- Fan & Evans (2017) — GW501516 development history and safety concerns — Cell Metabolism
Regulatory and Classification
This content is for informational purposes only and does not constitute medical advice. Always consult your healthcare provider.
