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鉴定一种在骨骼肌中高表达的新型AMP活化蛋白激酶β亚基异构体。

Identification of a novel AMP-activated protein kinase beta subunit isoform that is highly expressed in skeletal muscle.

作者信息

Thornton C, Snowden M A, Carling D

机构信息

Medical Research Council Clinical Sciences Centre, Cellular Stress Group, Imperial College School of Medicine, Hammersmith Hospital, DuCane Road, London W12 0NN, United Kingdom.

出版信息

J Biol Chem. 1998 May 15;273(20):12443-50. doi: 10.1074/jbc.273.20.12443.

DOI:10.1074/jbc.273.20.12443
PMID:9575201
Abstract

The AMP-activated protein kinase (AMPK) is a member of a growing family of related kinases, including the SNF1 complex in yeast, which respond to nutritional stress. AMPK is a heterotrimeric complex of a catalytic subunit (alpha) and two regulatory subunits (beta and gamma), and proteins related to all three subunits have been identified in the SNF1 complex. We have used the two-hybrid system in order to identify proteins interacting with the catalytic subunit (alpha2). Using this approach, we have isolated a novel AMPKbeta isoform, which we designate AMPKbeta2. The N-terminal region of beta2 differs significantly from that of the previously characterized isoform (beta1), suggesting that this region could play a role in isoform-specific AMPK activity. Comparison of the C-terminal sequences of beta1 and beta2 with their related proteins in yeast identifies two highly conserved regions predicted to be involved in binding of the alpha and gamma subunits. The expression of beta1 and beta2 was examined in a number of tissues, revealing that the beta1 isoform is highly expressed in liver with low expression in skeletal muscle, whereas the opposite pattern is observed for the beta2 isoform. These results suggest that the beta isoforms have tissue-specific roles, which may involve altered responses to upstream signaling and/or downstream targeting of the AMPK complex.

摘要

AMP激活的蛋白激酶(AMPK)是一个不断壮大的相关激酶家族的成员,其中包括酵母中的SNF1复合物,它们对营养应激作出反应。AMPK是由一个催化亚基(α)和两个调节亚基(β和γ)组成的异源三聚体复合物,并且在SNF1复合物中已鉴定出与所有三个亚基相关的蛋白质。我们利用双杂交系统来鉴定与催化亚基(α2)相互作用的蛋白质。通过这种方法,我们分离出了一种新的AMPKβ亚型,我们将其命名为AMPKβ2。β2的N端区域与先前鉴定的亚型(β1)有显著差异,这表明该区域可能在亚型特异性的AMPK活性中发挥作用。将β1和β2的C端序列与其在酵母中的相关蛋白质进行比较,鉴定出两个高度保守的区域,预计它们参与α和γ亚基的结合。我们检测了β1和β2在多种组织中的表达情况,发现β1亚型在肝脏中高表达,而在骨骼肌中低表达,而β2亚型的表达模式则相反。这些结果表明,β亚型具有组织特异性作用,这可能涉及对上游信号的反应改变和/或AMPK复合物的下游靶向作用。

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J Biol Chem. 1998 May 15;273(20):12443-50. doi: 10.1074/jbc.273.20.12443.
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