š¤ Authors: Miles D Witham, Claire McDonald, Nina Wilson, Katherine J Rennie, Michelle Bardgett, Penny Bradley, Andrew P Clegg, Stephen Connolly, Helen Hancock, Shaun Hiu, Karen Nicholson, Laura Robertson, Laura Simms, Alison J Steel, Claire J Steves, Bryony Storey, James Wason, Thomas von Zglinicki, Avan A Sayer
Metformin and physical performance in older people with probable sarcopenia and physical prefrailty or frailty in EnglandĀ (MET-PREVENT): a double-blind, randomised, placebo-controlled trial.
Metformin has effects on multiple biological systems relevant to ageing and has been posited as a candidate therapy for sarcopenia and physical frailty. We aimed to test the efficacy and safety of metformin, a candidate geroprotector, to improve physical performance in older people with probable sarcopenia and physical prefrailty or frailty.
In this double-blind, randomised, parallel-group, placebo-controlled trial (MET-PREVENT), participants aged 65Ā years and older with a 4-m walk speed of less than 0Ā·8Ā m/s and probable sarcopenia, characterised by low handgrip strength (<16Ā kg for women and <27Ā kg for men) or five times sit-to-stand time of longer than 15Ā s (or inability to complete five sit-to-stands) were recruited from primary care and hospital clinics in Gateshead and Newcastle, UK. Participants were randomly assigned (1:1), via a web-based system with minimisation to ensure balance by sex and baseline 4-m walk speed, to receive either 500Ā mg oral metformin or matching placebo three times a day for 4Ā months.
The primary outcome was the adjusted between-group difference in 4-m walk speed at 4Ā months. The primary outcome was analysed in the intention-to-treat population (ie, all participants randomly assigned to treatment) who had complete data, and safety was assessed in all participants who received at least one dose of study treatment.
This study is registered with the ISRCTN registry, ISRCTN29932357, and is now complete. Between Aug 1, 2021, and Sept 30, 2022, 268Ā individuals were screened for inclusion in the trial, and 72Ā participants were randomly assigned to either metformin (n=36) or placebo (n=36; intention-to-treat population).
Mean age was 80Ā·4Ā years (SD 5Ā·7), 42 (58%) of 72Ā participants were female, 30 (42%) were male, and 70 (97%) were White British. 70 (97%) of 72Ā participants had complete follow-up data (n=34Ā in the metformin group and n=36Ā in the placebo group). Mean 4-m walk speed at 4Ā months was 0Ā·57Ā m/s (SD 0Ā·19) in the metformin group and 0Ā·58Ā m/s (0Ā·24) in the placebo group (adjusted treatment effect 0Ā·001Ā m/s [95% CI -0Ā·06Ā to 0Ā·06]; p=0Ā·96). 108Ā adverse events occurred in 35 (100%) of 35Ā participants who received metformin and 77Ā adverse events occurred in 33Ā (92%) of 36Ā participants who received placebo, and 12 (34%) of 35Ā participants had hospital admissions in the metformin group versus three (8%) of 36Ā participants in the placebo group.
One death occurred, in the metformin group (oneĀ [3%] of 35), and was judged to be unrelated to study treatment. Metformin did not improve 4-m walk speed and was poorly tolerated in this population.
National Institute for Health and Care Research Newcastle Biomedical Research Centre.
