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Byr2激酶结构域的功能分析

Functional analysis of domains in the Byr2 kinase.

作者信息

Bauman P, Albright C F

机构信息

Department of Biochemistry, Vanderbilt University School of Medicine, Nashville, TN 37232-0146, USA.

出版信息

Biochimie. 1998 Jul;80(7):621-5. doi: 10.1016/s0300-9084(98)80015-1.

Abstract

The activation of mitogen-activated protein (MAP) kinase cascades by the Ras GTPase is an evolutionarily conserved signal transduction mechanism. To better understand the interaction between Ras and its target kinase, we study the yeast Schizosaccharomyces pombe where the Ras1 GTPase activates the Byr2 kinase. The Byr2 kinase contains an N-terminal regulatory region and a C-terminal kinase region. The regulatory region can be divided into a sterile-alpha motif (SAM) that binds Ste4, a Ras1-binding domain (RBD) that binds activated Ras1, and a catalytic binding domain (CBD) that interacts with the Byr2 kinase domain. To analyze the importance of functional domains of the Byr2 kinase, a biological assay was used that exploited the ability of Byr2 to partially bypass the need for Ras1 in sporulation. Analysis of mutants using this assay showed that SAM and RBD were very important for Ras1-stimulated sporulation. Three activating mutations were identified within the N-terminal lobe of the Byr2 kinase domain that partially bypassed the need for Ras1 for sporulation. These activating mutations may identify a region of the Byr2 kinase domain that interacts with the CBD since mutations in the CBD which disrupt binding to the kinase domain also increase Byr2 function.

摘要

Ras GTP酶激活丝裂原活化蛋白(MAP)激酶级联反应是一种进化上保守的信号转导机制。为了更好地理解Ras与其靶激酶之间的相互作用,我们研究了粟酒裂殖酵母,其中Ras1 GTP酶激活Byr2激酶。Byr2激酶包含一个N端调节区域和一个C端激酶区域。调节区域可分为与Ste4结合的无活性α基序(SAM)、与活化的Ras1结合的Ras1结合结构域(RBD)以及与Byr2激酶结构域相互作用的催化结合结构域(CBD)。为了分析Byr2激酶功能结构域的重要性,我们使用了一种生物学检测方法,该方法利用了Byr2在孢子形成过程中部分绕过对Ras1需求的能力。使用该检测方法对突变体进行分析表明,SAM和RBD对Ras1刺激的孢子形成非常重要。在Byr2激酶结构域的N端叶内鉴定出三个激活突变,这些突变在一定程度上绕过了孢子形成对Ras1的需求。这些激活突变可能确定了Byr2激酶结构域中与CBD相互作用的区域,因为CBD中破坏与激酶结构域结合的突变也会增加Byr2的功能。

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