| Literature DB >> 31162944 |
Chao Wang1, Bin Zhang2, Anna C Ratliff3, Justine Arrington3, Jingjuan Chen1, Yan Xiong2, Feng Yue1, Yaohui Nie1, Keping Hu2, Wen Jin2, W Andy Tao4,5, Christine A Hrycyna3,5, Xiaobo Sun2, Shihuan Kuang1,5.
Abstract
Skeletal muscles contain heterogeneous myofibers that are different in size and contractile speed, with type IIb myofiber being the largest and fastest. Here, we identify methyltransferase-like 21e (Mettl21e), a member of newly classified nonhistone methyltransferases, as a gene enriched in type IIb myofibers. The expression of Mettl21e was strikingly up-regulated in hypertrophic muscles and during myogenic differentiation in vitro and in vivo. Knockdown (KD) of Mettl21e led to atrophy of cultured myotubes, and targeted mutation of Mettl21e in mice reduced the size of IIb myofibers without affecting the composition of myofiber types. Mass spectrometry and methyltransferase assay revealed that Mettl21e methylated valosin-containing protein (Vcp/p97), a key component of the ubiquitin-proteasome system. KD or knockout of Mettl21e resulted in elevated 26S proteasome activity, and inhibition of proteasome activity prevented atrophy of Mettl21e KD myotubes. These results demonstrate that Mettl21e functions to maintain myofiber size through inhibiting proteasome-mediated protein degradation.-Wang, C., Zhang, B., Ratliff, A. C., Arrington, J., Chen, J., Xiong, Y., Yue, F., Nie, Y., Hu, K., Jin, W., Tao, W. A., Hrycyna, C. A., Sun, X., Kuang, S. Methyltransferase-like 21e inhibits 26S proteasome activity to facilitate hypertrophy of type IIb myofibers.Entities:
Keywords: Mettl21e; Myostatin; VCP/p97; muscle atrophy; non-histone methylation
Mesh:
Substances:
Year: 2019 PMID: 31162944 PMCID: PMC6993925 DOI: 10.1096/fj.201900582R
Source DB: PubMed Journal: FASEB J ISSN: 0892-6638 Impact factor: 5.834