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蛋白磷酸酶1抑制剂CPI-17上新型的体外和体内磷酸化位点。

Novel in vitro and in vivo phosphorylation sites on protein phosphatase 1 inhibitor CPI-17.

作者信息

Dubois Thierry, Howell Steven, Zemlickova Eva, Learmonth Michele, Cronshaw Andy, Aitken Alastair

机构信息

Division of Biomedical and Clinical Laboratory Sciences, University of Edinburgh, UK.

出版信息

Biochem Biophys Res Commun. 2003 Mar 7;302(2):186-92. doi: 10.1016/s0006-291x(03)00130-x.

Abstract

CPI-17 is a protein phosphatase 1 (PP1) inhibitor that has been shown to act on the myosin light chain phosphatase. CPI-17 is phosphorylated on Thr-38 in vivo, thus enhancing its ability to inhibit PP1. Thr-38 has been shown to be the target of several protein kinases in vitro. Originally, the expression of CPI-17 was proposed to be smooth muscle specific. However, it has recently been found in platelets and we show in this report that it is endogenously phosphorylated in brain on Ser-128 in a domain unique to CPI-17. Ser-128 is within a consensus phosphorylation site for protein kinase A (PKA) and calcium calmodulin kinase II. However, these two kinases do not phosphorylate Ser-128 in vitro but phosphorylate Ser-130 and Thr-38, respectively. The kinase responsible for Ser-128 phosphorylation remains to be identified. CPI-17 has strong sequence similarity with PHI-1 (which is also a phosphatase inhibitor) and LimK-2 kinase. The novel in vivo and in vitro phosphorylation sites (serines 128 and 130) are in a region/domain unique to CPI-17, suggesting a specific interaction domain that is regulated by phosphorylation.

摘要

CPI-17是一种蛋白磷酸酶1(PP1)抑制剂,已被证明可作用于肌球蛋白轻链磷酸酶。CPI-17在体内的苏氨酸-38位点被磷酸化,从而增强其抑制PP1的能力。苏氨酸-38在体外已被证明是几种蛋白激酶的作用靶点。最初,CPI-17的表达被认为是平滑肌特异性的。然而,最近在血小板中发现了它,并且我们在本报告中表明它在脑中的丝氨酸-128位点在CPI-17特有的结构域内被内源性磷酸化。丝氨酸-128位于蛋白激酶A(PKA)和钙调蛋白激酶II的共有磷酸化位点内。然而,这两种激酶在体外不会使丝氨酸-128磷酸化,而是分别使丝氨酸-130和苏氨酸-38磷酸化。负责丝氨酸-128磷酸化的激酶仍有待确定。CPI-17与PHI-1(也是一种磷酸酶抑制剂)和LimK-2激酶具有很强的序列相似性。新发现的体内和体外磷酸化位点(丝氨酸128和130)位于CPI-17特有的区域/结构域内,表明存在一个受磷酸化调节的特定相互作用结构域。

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