๐ค Authors: Roger A Fielding, Michael M Dao, Kevin Cannon, Moise Desvarieux, Sam S Miller, Michael Paul Gimness, Donald M Brandon, Dennis T Villareal, Olivier Bruyere, Ivan Bautmans, Kyle Rickner, Robert Perry, Stephen B Kritchevsky, Nicolas Musi, Joe M Chehade, Judith L Kirstein, Evelien Gielen, Paul Pickrell, Pierre Dilda, Rene Lafont, Carole Margalef, Yves Rolland, Susanna Del Signore, Jean Mariani, Samuel Agus, Cendrine Tourette, Waly Dioh, Rob van Maanen, Stanislas Veillet
BIO101 in Sarcopenic Seniors at Risk of Mobility Disability: Results of a Double-Blind Randomised Interventional Phase 2b Trial.
Sarcopenia is a progressive muscle disorder that may lead to mobility disability. No pharmaceutical interventions are currently available, and treatment relies on physical exercise and nutrition.
The aim of SARA-INT was to investigate whether BIO101 (20-hydroxyecdysone), an activator of the MAS receptor, is safe and improves muscle function and physical performance of community dwelling older sarcopenic patients. SARA-INT was a randomised three-arm interventional study (BIO101 175โmg bid /350โmg bid/placebo) with a planned 6-month treatment (up to 9โmonths in 50 subjects).
Eligibility criteria for sarcopenia were meeting FNIH criteria for sarcopenia and Short Physical Performance Battery (SPPB) score โคโ8/12 in men and women aged โฅโ65โyears. Primary endpoint was the change from baseline (CFB) in gait speed (GS) measured by 400-m walking test (400MWT), secondary endpoints being CFB in other physical performance tests.
A total of 233 participants were randomised (mean age 75.5โยฑโ7.12; 54.3% female), of whom 232 and 156 were included in the full analysis set (FAS) and per-protocol (PP) populations, respectively. Due to COVID-19 pandemic, 55% of on-site end-of-treatment efficacy assessments were lost, reducing the studies' power.
In the primary analysis (mix of 6/9โmonths), BIO101 350โmg bid treatment after 6/9โmonths was associated with an improvement in the 400MWT of 0.07โm/s versus placebo in the FAS population (not significant) and of 0.09โm/s in the PP population (pโ=โ0.008). BIO101 350โmg bid treatment effect on the 400MWT GS was also observed in pre-defined subpopulations at higher risk of mobility disability (0.0474โm/s for slow walkers, 0.0521โm/s for obese and 0.0662โm/s for chair stand sub-score โคโ2 from SPPB in the FAS population), with a trend for a dose response.
BIO101 showed a good safety profile at both doses (number of subjects with related treatment emergent adverse events (TEAEs) of 13 (16.0%), 10 (13.3%) and 10 (13.5%) in the placebo, 175โmg and 350โmg BIO101 groups, respectively). After 6 to 9โmonths of treatment, BIO101 350โmg bid showed strong trends consistent with a clinically relevant effect on the 400MWT GS, close to the minimal clinically important difference (MCID) in sarcopenia (0.1โm/s).
This was also shown in predefined subpopulations at higher risk of mobility disability. BIO101 showed a good safety profile.
Taken together, efficacy and safety data of this Phase 2 trial encourage us to pursue further development of BIO101 for the treatment of sarcopenia.
