Existence of multiple phosphorylated forms of human platelet actin binding protein.

M P Wu, D Jay, A Stracher
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Abstract

Platelet actin binding protein (ABP) as isolated from human platelets exists in at least four phosphorylated forms which we have designated ABP-0, ABP-1, ABP-2, and ABP-3 whose phosphate content ranges from 18 (ABP-0) to 40 (ABP-3) moles Pi/mole ABP. These forms differ in their resistance to calpain cleavage and ability to cross-link F-actin with ABP-3 being the best in each of these properties. Attempts to phosphorylate ABP-1, two or three with protein kinase C (PKC) were unsuccessful except if the proteins were pretreated with Escherichia coli alkaline phosphatase. All of the forms could be phosphorylated with cAMP-dependent kinase (PKA) and subsequent resistance to calpain cleavage conferred. Phosphorylation/dephosphorylation of ABP may be an important regulatory mechanism by which the cytoskeletal architecture is stabilized or transformed.

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人血小板肌动蛋白结合蛋白存在多种磷酸化形式。
从人血小板中分离出来的血小板肌动蛋白结合蛋白(ABP)至少存在四种磷酸化形式,我们将其命名为ABP-0、ABP-1、ABP-2和ABP-3,其磷酸盐含量从18 (ABP-0)到40 (ABP-3)摩尔π /摩尔ABP。这些形式对钙蛋白酶裂解的抗性和交联f -肌动蛋白的能力不同,其中ABP-3在这些性质中都是最好的。除非用大肠杆菌碱性磷酸酶预处理,否则用蛋白激酶C (PKC)磷酸化ABP-1、2或3都是不成功的。所有的形式都可以被camp依赖性激酶(PKA)磷酸化,从而获得对钙蛋白酶裂解的抗性。ABP的磷酸化/去磷酸化可能是细胞骨架结构稳定或转化的重要调控机制。
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