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骨骼肌在发育和疾病过程中的凋亡。

Apoptosis of skeletal muscles during development and disease.

作者信息

Sandri M, Carraro U

机构信息

CNR Unit for Muscle Biology and Physiopathology, Department of Biomedical Sciences, University of Padova, Italy.

出版信息

Int J Biochem Cell Biol. 1999 Dec;31(12):1373-90. doi: 10.1016/s1357-2725(99)00063-1.

Abstract

Cells from multicellular organisms self-destroy when no longer needed or when damaged. They do this by activating genetically controlled machineries that lead to apoptosis. Skeletal muscles in adult animals are fully differentiated syncytial cells. Apoptosis has been described in developing and, recently, in adult skeletal muscle. The cellular and molecular aspects of myoblast and myofibre apoptosis and their role in disease are analysed in this review. Alterations in the pathways that regulate myoblasts proliferation/differentiation lead to induction of apoptosis during myogenesis both in vivo and in vitro. In adult muscle myofibres apoptosis seems to start from segmental areas of myofibres often producing loss of a single myonucleus. The bcl2/bax system is active in muscle when apoptosis occurs. On the other hand conflicting results are reported on the role played by FasL/Fas system. These findings are confirmed by in vitro results on myotubes and on their susceptibility to apoptosis. Though apoptosis has been shown to occur in the skeletal muscle, the role played in diseases and the pattern followed in myogenic cells are far from being clear.

摘要

多细胞生物的细胞在不再需要或受损时会自我毁灭。它们通过激活导致细胞凋亡的基因控制机制来做到这一点。成年动物的骨骼肌是完全分化的多核细胞。细胞凋亡在发育中的骨骼肌中已有描述,最近在成年骨骼肌中也有报道。本文综述了成肌细胞和肌纤维细胞凋亡的细胞和分子层面及其在疾病中的作用。调节成肌细胞增殖/分化的途径发生改变会导致在体内和体外的肌生成过程中诱导细胞凋亡。在成年肌肉中,肌纤维凋亡似乎始于肌纤维的节段区域,常常导致单个肌细胞核的丢失。当细胞凋亡发生时,bcl2/bax系统在肌肉中发挥作用。另一方面,关于FasL/Fas系统所起的作用,报道的结果相互矛盾。这些发现通过对肌管及其对细胞凋亡敏感性的体外实验结果得到了证实。尽管已经证明细胞凋亡会在骨骼肌中发生,但它在疾病中所起的作用以及在成肌细胞中遵循的模式仍远未明确。

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