Ask yourself one question. Are you pregnant, planning pregnancy, on a blood-pressure medication, or buying raw resin from a marketplace? If yes to any of those, skip shilajit entirely. If no, you still do not need it — the energy and longevity claims have zero RCT support, and the testosterone claim is one study from 2016 the manufacturer never repeated.
Shilajit is a Himalayan rock-tar people grind into a powder, push into a capsule, and sell as a testosterone or energy supplement. Almost every positive trial uses one specific manufacturer's purified extract called PrimaVie, and the raw resin most people buy on Amazon is a different product with documented lead, arsenic, and mercury in lab analyses. Reading the trial evidence and buying the cheaper resin is like reading a clinical trial of a prescription drug and assuming the unregulated street version of the same chemical works the same way.
That's the general answer. Your stack is different.
Check your whole stackHerbal · Adaptogen · Mineral-pitch resin
The Himalayan resin sold as a natural testosterone booster. One trial, eight years of silence, and lab-documented heavy metals in the raw resin most people actually buy.
Skip · Conditional Yes in three narrow contextsAsk yourself one question. Are you pregnant, planning pregnancy, on a blood-pressure medication, or buying raw resin from a marketplace? If yes to any of those, skip shilajit entirely. If no, you still do not need it.
The energy and longevity claims have zero RCT support. The testosterone claim is one study from 2016 the manufacturer never repeated. The raw resin on Amazon has documented lead, arsenic, and mercury contamination in lab testing.
Takes less than 30 seconds. No equipment needed.
The Verdict
Almost every positive shilajit trial uses one specific manufacturer's purified extract called PrimaVie, made by Natreon Inc. The raw resin most people buy on Amazon or in health-food shops is a different product with documented lead, arsenic, and mercury in lab analyses. Reading the trial evidence and buying the cheaper resin is like reading a clinical trial of a prescription drug and assuming the unregulated street version of the same chemical works the same way.
Postmenopausal women with osteopenia as a clinician-supervised adjunct after first-line treatment is in place. Men with low sperm counts under urology supervision. Healthy men 45-55 self-experimenting with the 2016 testosterone claim using PrimaVie and a stopping rule.
You are pregnant or planning pregnancy. You are on blood-pressure medication, a potassium-sparing diuretic, or have high blood pressure or low potassium. You are buying raw resin online. You are under 45, healthy, and buying for energy, cognition, mitochondria, fat loss, endurance, or longevity.
The protocol, safety, and full evidence below
Every positive human RCT uses PrimaVie standardised extract from Natreon Inc. at 250-1000 mg per day. The dosing table below covers every population studied. If you are taking shilajit outside one of these contexts, you are taking it without evidence.
| Population | Dose | Duration | Form | Evidence |
|---|---|---|---|---|
| General healthy adult (retail) | NOT INDICATED | — | — | No consumer claim clears MODERATE-recommend |
| Postmenopausal w/ osteopenia (clinician adjunct, after first-line SoC) | 250-500 mg/day | 48 weeks | PrimaVie standardised extract | Pohrt 2022 PMID 35933897 (single trial) |
| Oligospermic infertile men (urology-supervised adjunct) | 100 mg twice daily (200 mg/day) | 90 days | Processed shilajit capsule | Biswas 2010 PMID 20078516 (open-label N=35) |
| Eugonadal men 45-55y (self-experiment, stopping rule) | 250 mg twice daily (500 mg/day) with meals | 90 days + baseline & day-90 LC-MS/MS T panel | PrimaVie standardised extract | Pandit 2016 PMID 26395129 (Natreon-funded N=75) |
| Recreationally-active men (fatigue-induced strength decline) | 500 mg/day | 8 weeks | PrimaVie standardised extract | Keller 2019 PMID 30728074 (Natreon-funded N=63) |
| Healthy adults seeking energy / cognition / mitochondrial / adaptogen / fat loss / hypertrophy / endurance / longevity / cortisol | NOT INDICATED | — | — | Zero RCT support in any population |
| Pregnancy and lactation | HARD CONTRAINDICATION | — | — | Velmurugan 2018 pseudohyperaldosteronism case + heavy-metal teratogenic concern |
| Adults on antihypertensives / K-sparing diuretics / MR antagonists / with HTN or hypokalemia | HARD CONTRAINDICATION | — | — | 11β-HSD2 / mineralocorticoid pathway interaction |
| Anyone buying raw resin or non-PrimaVie products | HARD NEGATIVE RECOMMENDATION | — | — | Heavy-metal contamination floor + form-substitution-not-validated |
| Children and adolescents | NOT INDICATED | — | — | No pediatric data; class-level heavy-metal concern |
Two distinct safety signals matter: a documented case of pseudohyperaldosteronism in pregnancy via the same mechanism that makes licorice dangerous, and a documented heavy-metal contamination floor in retail raw resin. Neither is hypothetical.
Documented mumijo-induced pseudohyperaldosteronism (licorice-like syndrome) — hypertension, hypokalemia, suppressed renin/aldosterone via 11β-HSD2 inhibition (Velmurugan 2018 case report). HARD CONTRAINDICATION in pregnancy.
Theoretical additive blood-pressure effect via mineralocorticoid pathway. AVOID; if used, monitor BP every 2-4 weeks.
Direct 11β-HSD2 / mineralocorticoid pathway interaction. AVOID.
Divalent-cation chelation by the mineral fraction reduces drug absorption. Separate dosing by 2-4 hours, or avoid during course.
Theoretical herbal-anticoagulant interaction. No clinical-event data published. Conservative avoid; if used, document and monitor.
Variable iron content in shilajit (Khalid 2022 analytical study). Avoid in hemochromatosis, polycythemia, iron-replete adults.
Theoretical herbal-immunosuppressant or mineral-handling interaction. Specialist-supervised; avoid without consult.
Single-trial-per-claim across the entire PrimaVie program with no independent replication in eight years. BMD postmenopausal-osteopenia is the strongest single positive (MODERATE single-trial). Collagen-synthesis biomarkers MODERATE but biomarker-only. Everything else LOW, NONE, or DEBUNKED-by-absence.
Three trials would shift the conviction tiers: (1) Independent, non-Natreon, double-blind, placebo-controlled RCT of N≥150 healthy eugonadal men aged 25-65 using PrimaVie 500 mg/d × 12 weeks with LC-MS/MS total + free T endpoints, showing greater than 12% absolute total T increase, would upgrade eugonadal testosterone from LOW to MODERATE. (2) Independent N≥200 postmenopausal-osteopenia trial replicating Pohrt 2022 over 24 months with a head-to-head arm against a bisphosphonate or denosumab would upgrade BMD from MODERATE to HIGH. (3) A functional connective-tissue outcome trial (tendon stiffness by shear-wave elastography or skin elasticity by cutometry) replicating the Tinsley 2024 biomarker signal would upgrade the collagen pathway from MODERATE-biomarker-only to MODERATE-clinical. Until at least the first one lands, the rational position is the current one.
Go Deeper
Want to stop wasting money on supplements built on one industry-funded trial? The Verdict reviews one supplement every week — free, with the evidence stack laid out the way it actually is.
Subscribe to The VerdictEvidence-scored dosing, timing, forms, and who should skip it. One page, no fluff.
Get the protocolConviction-scored verdicts on supplements, nutrition, training, physio, and recovery.