Rapamycin is the most reproducible life-extension drug in mammals, extending lifespan in mice by 9–25% even when started in late life — but human longevity evidence is absent and significant immunosuppressive risks limit its use.
Rapamycin (sirolimus) inhibits mTORC1, a central regulator of cell growth and aging. It is the most reproducible life-extension drug in mammals, extending lifespan in mice by 9–25% even when started at 20 months of age (equivalent to approximately 60 human years). However, no human longevity RCT data exist, and rapamycin's immunosuppressive effects — it is used to prevent organ transplant rejection — limit its use in healthy individuals.
Harrison et al. (2009) in Nature demonstrated that rapamycin extended lifespan in genetically heterogeneous mice by 9% in males and 14% in females when started at 20 months of age — a landmark finding because it showed that mTOR inhibition could extend lifespan even when started in late life. Miller et al. (2011) replicated this finding across three independent research sites, with lifespan extensions of 10–25%. Mannick et al. (2014) in Science Translational Medicine conducted the first human trial of an mTOR inhibitor (RAD001, an everolimus analogue) in older adults and found that 6 weeks of treatment improved influenza vaccine responses by 20% — suggesting that mTOR inhibition may reverse some aspects of immune aging in humans.
"Rapamycin extended lifespan in mice by 9–25% even when started at 20 months of age — equivalent to starting treatment at approximately age 60 in humans."
— Harrison et al., Nature 2009; Miller et al., Aging Cell 2011
The NIA's Interventions Testing Program (ITP) has tested rapamycin in mice across multiple sites, consistently finding lifespan extension. The NIA notes that rapamycin is one of the most promising longevity drug candidates but that its immunosuppressive effects and side effect profile (impaired wound healing, metabolic effects, potential increased infection risk) make it unsuitable for use in healthy humans outside of carefully designed clinical trials. No regulatory authority has approved rapamycin for longevity use.
Rapamycin should not be self-prescribed for longevity. Its immunosuppressive effects increase infection risk and impair wound healing. Some longevity physicians are experimenting with intermittent low-dose rapamycin protocols (once weekly) to minimise immunosuppression while engaging mTOR inhibition, but this is experimental and lacks safety data. The mTOR pathway can be partially engaged through safer means: regular aerobic exercise, protein cycling (periods of lower protein intake), and avoiding chronic caloric excess all reduce mTOR signalling.
Vitaei verdict
Rapamycin has the strongest animal longevity evidence of any drug, but human longevity data are absent and its immunosuppressive effects are a significant concern. It should not be used for longevity outside of clinical trials.
What Is the Evidence for Metformin as a Longevity Drug?
Metformin activates AMPK and inhibits mTOR — the same pathways engaged by caloric restriction — and observational data suggest diabetic patients on metformin outlive matched non-diabetic controls, but RCT longevity evidence in non-diabetics is pending.
How Does Caloric Restriction Extend Lifespan and What Is the Human Evidence?
Caloric restriction extends lifespan in virtually every organism studied, from yeast to primates, through activation of AMPK, inhibition of mTOR, and sirtuins — but human evidence remains limited to biomarker improvements rather than direct longevity data.