If you are taking Garcinia cambogia / HCA right now, stop. Stop today if you have any liver-risk factor (active liver disease, hepatitis, regular alcohol, statins) or you are on an SSRI / SNRI / MAOI antidepressant. The single highest-quality trial showed no weight loss, and the case-report literature includes transplant-requiring liver failure.
That's the general answer. Your stack is different.
Check your whole stackThe biggest weight-loss supplement of the 2010s flunked its own JAMA trial, and the case-report literature on liver failure goes all the way to transplant.
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If you are taking Garcinia cambogia / HCA right now, stop. Stop today if you have any liver-risk factor (active liver disease, hepatitis, regular alcohol use, statins) or you are on an SSRI / SNRI / MAOI antidepressant.
The Verdict
Don't take it. The single best independent trial showed no weight loss, and case reports of liver failure on Garcinia keep being published in 2025.
Nobody, on the current evidence. No identified population subgroup beats the hepatotoxicity tail risk.
Everyone — but especially anyone with liver-risk factors, on serotonergic medications, on hepatotoxic drugs, pregnant, or under 18.
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There is no recommended protocol because the evidence does not support routine use. The dosing reference below documents what the trial literature has used, so you can recognise a bottle dose, not so anyone should be following it.
| Population | Trial-literature dose | Form | Status |
|---|---|---|---|
| Trial-replication reference (Heymsfield 1998 dose) | 1500 mg/day HCA | Calcium-potassium HCA salt (HCA-SX), 30–60 min pre-meal × 3 | Null in the canonical RCT |
| SR-included trial range | 1000–2800 mg/day HCA | Calcium / calcium-potassium HCA salt | Pooled SR/MA effect crosses zero in good-quality subset |
| Liver-risk factors (active liver disease, hepatitis B/C carrier, NAFLD, regular alcohol ≥2 drinks/d, on hepatotoxic medications) | — | — | CONTRAINDICATED |
| On SSRIs, SNRIs, MAOIs, triptans, tramadol, fentanyl, MDMA | — | — | CONTRAINDICATED — serotonin syndrome risk |
| Pregnancy / lactation / children / adolescents | — | — | CONTRAINDICATED by precaution |
| Form | Bioavailability | Cost | Notes |
|---|---|---|---|
| Free hydroxycitric acid | Low | £ | Superseded by salt forms (poor absorption) |
| Calcium-HCA salt | Better than free HCA | ££ | Older trial replication form |
| Calcium-potassium HCA (HCA-SX / Super CitriMax) | Highest in branded comparisons | £££ | Sabinsa-developed branded ingredient. Industry-collaborative trial pattern. |
| Garcinia rind powder (kokum / kudampuli) | Variable (HCA 10–30% dry weight) | £ | Traditional culinary use at gram-level intake; not equivalent to standardised extract dosing |
| Botanical blends (IQP-GC-101, Hydroxycut family historically) | Not attributable to Garcinia | £££+ | Garcinia + green tea blends carry additive hepatotoxicity (LiverTox/DILIN 2022) |
| Liposomal / nano-encapsulated / "rapid-release" Garcinia | No human outcome data | £££+ | Premium-form trap — pharmacokinetic chart, not clinical benefit |
The hepatotoxicity case literature spans 2005 to 2025 and includes more than a dozen published papers. It does not depend on whether Garcinia "works" for weight loss. Even if the efficacy story were positive, the safety signal would still make routine consumer use indefensible.
2014 Medical Toxicology case report [cite-unverified] documents serotonin syndrome with HCA + SSRI co-administration. Mechanism-plausible, severity high when it occurs. Avoid the combination at any dose.
2022 LiverTox/DILIN case series (PMID 34400337) confirms Garcinia alone or in combination with green tea causes moderate-to-severe liver injury. The "fat burner" stack is the worst-of-both-worlds combination.
Theoretical compounding hepatotoxicity risk against background of drug-induced liver enzyme elevation. Avoid in patients with elevated baseline transaminases.
Right-upper-abdominal pain, jaundice, dark urine, light-coloured stools, persistent nausea, fatigue out of context, pruritus, peripheral oedema (signs of hepatic injury); or agitation, hyperthermia, hyperreflexia, autonomic instability (signs of serotonin syndrome). Go directly to urgent care or A&E. Bring the bottle.
The body-weight effect is null in the highest-quality monotherapy trial (Heymsfield 1998 JAMA, N=135). The pooled SR/MA effect (−0.88 kg) disappears in the high-quality subset. The hepatotoxicity case literature is large, growing, and includes transplant-requiring acute liver failure across 12+ retrieved PMIDs spanning 2005 to 2025.
To upgrade efficacy: an independent (non-industry, non-Sabinsa-collaborative), double-blind RCT of ≥250 healthy overweight adults at ≥1500 mg/day standardised HCA for ≥24 weeks, primary endpoints body weight and DXA-measured fat mass with active dietary monitoring, reporting >2 kg absolute body-weight difference vs placebo with 95% CI not crossing zero, AND zero serious hepatic adverse events at the prespecified safety cutoff. To downgrade hepatotoxicity: a rigorous case-control or large prospective cohort study showing the signal is confounded by adulterants rather than HCA itself.
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SubscribeThe Garcinia cambogia / hydroxycitric acid (HCA) marketing pitch is unusually consistent. The rind of the Malabar tamarind contains HCA, HCA inhibits ATP-citrate lyase, ACLY is the rate-limiting step of de novo lipogenesis, so HCA "blocks fat storage" and helps the body "burn fat instead of store it". The blockbuster Dr Oz segment from the early 2010s gave it a household name. A second strand of the marketing claims HCA increases serotonin signalling and therefore suppresses appetite as a bonus.
The forms multiplied to match the demand: free HCA, calcium-HCA salts, calcium-potassium HCA (HCA-SX / Super CitriMax), magnesium-HCA, "rapid-release" liposomal versions, and proprietary blends with green tea, white kidney bean, raspberry ketones, and caffeine. The mechanism is biochemically real. The translation to "loses meaningful weight in adult humans on a 12-week trial" is where the story falls apart.
| Claimed benefit | Evidence | Verdict |
|---|---|---|
| Body weight loss (overweight adults, 12 wk monotherapy) | Heymsfield 1998 JAMA RCT (PMID 9820262, N=135, 1500 mg/d HCA): null on body weight and fat mass | DEBUNKED |
| Pooled SR/MA body weight | Onakpoya 2011 SR/MA (PMC3010674) [cite-unverified]: −0.88 kg pooled, NS in good-quality subset | LOW |
| Body composition / fat mass | Null in canonical RCT (PMID 9820262) | LOW |
| Acute appetite suppression / satiety | Mattes & Bormann 2000 (PMID 11134690) crossover: null on appetitive variables | LOW |
| Obesity indices (BMI, waist) pooled MA | Maia-Landim 2020 (PMID 32951714): modest pooled reduction, high heterogeneity, direction-only | LOW–MODERATE |
| Lipid profile | Inconsistent (PMID 14965155, PMID 15051593) | LOW |
| Glycaemic control in pre-diabetes (rind powder) | NCT07419074 trial registry only [cite-unverified], not peer-reviewed | LOW (PENDING) |
| Long-term + Glucomannan combination, genotype-stratified | Maia-Landim 2018 (PMID 29361938): combination intervention, can't isolate Garcinia | LOW–MODERATE direction-only |
| Branded blends (IQP-GC-101, Hydroxycut historically) | PMID 24797657: multi-ingredient, can't attribute to Garcinia | NOT EVALUABLE |
| Hepatotoxicity safety signal | 12+ PMID case-series 2005–2025 including transplant-requiring ALF (PMID 28018115); LiverTox/DILIN 2022 (PMID 34400337) | HIGH · HARM |
| Serotonin syndrome with SSRI/SNRI/MAOI | 2014 Med Toxicology case [cite-unverified], mechanism-plausible | MODERATE · HARM |
| Premium liposomal / rapid-release outcome superiority | No human outcome RCT | NONE |
HCA is a competitive inhibitor of ATP-citrate lyase (ACLY), the cytosolic enzyme that converts citrate into acetyl-CoA. Acetyl-CoA is the substrate for fatty-acid synthesis, so blocking ACLY blocks de novo lipogenesis (DNL). The bottle's pitch is: less DNL, less stored fat, less weight gain.
The clinical translation falls apart at one specific point. In normally-fed humans, DNL is a minor pathway. Most adipose-tissue triglyceride is dietary-fat-derived rather than synthesised from carbohydrate via DNL. Inhibiting a small fraction of fat storage in normally-fed people produces a small physiological consequence. The Heymsfield 1998 trial confirmed the prediction.
The secondary "HCA increases serotonin and suppresses appetite" claim has the awkward feature that human acute crossover trials (Mattes & Bormann 2000, PMID 11134690) found no effect on hunger, satiety, or energy intake, while the case literature has documented serotonin syndrome when HCA is combined with SSRIs. Whatever serotonergic activity is present is too weak to drive intake reduction but real enough to compound a serotonergic drug into clinical territory.
−0.88 kg vs placebo, statistically significant when all 9 poolable trials are combined.
Restricted to the 2 trials judged of "good methodological quality": MD −0.88 kg, 95% CI −0.33 to 2.10. Not significant.
Quality of constituent trials drives the pooled signal. The high-quality subset extinguishes the effect. Classic "positive pooled, null in good trials" pattern.
Independent academic, double-blind, N=135, 1500 mg/day × 12 weeks. Null on body weight and fat mass.
Industry-collaborative, branded HCA-SX (Sabinsa-developed). Positive on multiple endpoints.
Funding-source-of-effect pattern. The blinded independent trial is the benchmark. The branded-form trials cluster on the positive side; the independent academic monotherapy clusters on null.
Multi-ingredient blend with Camellia sinensis (green tea) and other compounds. Reductions in body weight and body fat.
Garcinia alone. Null.
Active-ingredient attribution to Garcinia is impossible in a multi-ingredient blend. The blend may work; the Garcinia component is not the demonstrated active.
Lab: industry-collaborative trials with Sabinsa-developed HCA-SX / Super CitriMax forms return positive.
Reality: independent academic monotherapy is null. Real-world consumers are buying a benefit attached to the wrong half of the literature.
Lab: trials use third-party-assayed standardised extracts.
Reality: commercial Garcinia products often lack the labelled active ingredient. The hepatotoxicity case literature can't fully separate "HCA hepatotoxicity" from "contamination / adulteration", and the practical implication is the same either way.
Lab: even if HCA produced a small metabolic effect, NEAT compensation (Careau 2021 DLW) and intake compensation across 12-week windows would predict the effect to be small at best.
Reality: real-world adherence and dose accuracy collapse the ceiling further. Less effective in real-world chronic use than already-modest pooled-MA estimates suggest.
Dietary chili pepper / capsaicinoid 6 mg/day is a more defensible option in this aisle. It carries a small but population-replicated SR/MA body-composition signal (BMI −0.25 kg/m² in overweight/obese adults) and no comparable liver case literature. Capsaicin is not a weight-loss agent either, but its risk-adjusted profile is materially different.
Caloric deficit, protein at ≥1.6 g per kg body weight, resistance training 2–3 sessions per week, sleep ≥7 hours, alcohol reduction. Each of those has more weight-management evidence than every Garcinia bottle on the shelf combined.
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