BAG3缺乏会导致暴发性肌病和早期死亡。
BAG3 deficiency results in fulminant myopathy and early lethality.
作者信息
Homma Sachiko, Iwasaki Masahiro, Shelton G Diane, Engvall Eva, Reed John C, Takayama Shinichi
机构信息
Burnham Institute for Medical Research, La Jolla, CA, USA.
出版信息
Am J Pathol. 2006 Sep;169(3):761-73. doi: 10.2353/ajpath.2006.060250.
Abstract
Bcl-2-associated athanogene 3 (BAG3) is a member of a conserved family of cyto-protective proteins that bind to and regulate Hsp70 family molecular chaperones. Here, we show that BAG3 is prominently expressed in striated muscle and colocalizes with Z-disks. Mice with homozygous disruption of the bag3 gene developed normally but deteriorated postnatally with stunted growth evident by 1 to 2 weeks of age and death by 4 weeks. BAG3-deficient animals developed a fulminant myopathy characterized by noninflammatory myofibrillar degeneration with apoptotic features. Knockdown of bag3 expression in cultured C2C12 myoblasts increased apoptosis on induction of differentiation, suggesting a need for bag3 for maintenance of myotube survival and confirming a cell autonomous role for bag3 in muscle. We conclude that although BAG3 is not required for muscle development, this co-chaperone appears to be critically important for maintenance of mature skeletal muscle.
摘要
Bcl-2相关抗凋亡基因3(BAG3)是一个保守的细胞保护蛋白家族的成员,该家族蛋白可与Hsp70家族分子伴侣结合并对其进行调节。在此,我们发现BAG3在横纹肌中显著表达,并与Z盘共定位。bag3基因纯合缺失的小鼠出生时发育正常,但出生后逐渐恶化,1至2周龄时生长明显迟缓,4周龄时死亡。BAG3缺陷动物发生暴发性肌病,其特征为具有凋亡特征的非炎性肌原纤维变性。在培养的C2C12成肌细胞中敲低bag3表达会增加诱导分化时的细胞凋亡,这表明维持肌管存活需要bag3,并证实了bag3在肌肉中具有细胞自主作用。我们得出结论,虽然BAG3不是肌肉发育所必需的,但这种共伴侣蛋白似乎对维持成熟骨骼肌至关重要。
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