Autophagy induction in atrophic muscle cells requires ULK1 activation by TRIM32 through unanchored K63-linked polyubiquitin chains.

Optimal autophagic activity is crucial to maintain muscle integrity, with either reduced or excessive levels leading to specific myopathies. LGMD2H is a muscle dystrophy caused by mutations in the ubiquitin ligase TRIM32, whose function in muscles remains not fully understood. Here, we show that TRIM32 is required for the induction of muscle autophagy in atrophic conditions using both in vitro and in vivo mouse models. Trim32 inhibition results in a defective autophagy response to muscle atrophy, associated with increased ROS and MuRF1 levels. The proautophagic function of TRIM32 relies on its ability to bind the autophagy proteins AMBRA1 and ULK1 and stimulate ULK1 activity via unanchored K63-linked polyubiquitin. LGMD2H-causative mutations impair TRIM32's ability to bind ULK1 and induce autophagy. Collectively, our study revealed a role for TRIM32 in the regulation of muscle autophagy in response to atrophic stimuli, uncovering a previously unidentified mechanism by which ubiquitin ligases activate autophagy regulators.

[Frequency of locus E1 variants of plasma butyrylcholinesterase in a French population]. / Fréquence des variants du locus E1 de la butyrylcholinestérase plasmatique dans une population française.

Human plasma cholinesterase (E.C.3.1.1.8) from 1,594 blood donors was phenotyped on the basis of dibucaïne, fluoride, chloride and succinylcholine differential inhibitions according to the criteria of Brown et coll. The observed gene frequencies are: E1u = 0.970,8, E1a = 0.188,0, E1f = 0.103,0.