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Mutational and kinetic analyses of the GTPase-activating protein (GAP)-p21 interaction: the C-terminal domain of GAP is not sufficient for full activity.

机译：GTPase激活蛋白（GAP）-p21相互作用的突变和动力学分析：GAP的C末端结构域不足以发挥全部活性。

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摘要

The GTPase-activating protein (GAP) stimulates the GTPase reaction of p21 by 5 orders of magnitude such that the kcat of the reaction is increased to 19 s-1. Mutations of residues in loop L1 (Gly-12 and Gly-13), in loop L2 (Thr-35 and Asp-38), and in loop L4 (Gln-61 and Glu-63) influence the reaction in different ways, but all of these mutant p21 proteins still form complexes with GAP. The C-terminal domain of the human GAP gene product, GAP334, which comprises residues 714 to 1047, is 20 times less active than full-length GAP on a molar basis and has a fourfold lower affinity. This finding indicates that the N terminus of GAP containing the SH2 domains modifies the interaction between the catalytic domain and p21.

机译：GTPase激活蛋白（GAP）将p21的GTPase反应刺激了5个数量级，从而使反应的kcat增加到19 s-1。 L1回路（Gly-12和Gly-13），L2回路（Thr-35和Asp-38）和L4回路（Gln-61和Glu-63）中残基的突变以不同的方式影响反应，但是所有这些突变的p21蛋白仍与GAP形成复合物。人GAP基因产物GAP334的C末端结构域（包含残基714至1047），其活性比全长GAP低20摩尔（摩尔），亲和力低四倍。该发现表明，含有SH2结构域的GAP的N末端修饰了催化结构域与p21之间的相互作用。

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作者
Gideon, P; John, J; Frech, M; Lautwein, A; Clark, R; Scheffler, J E; Wittinghofer, A;
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年度 1992
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正文语种 en
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1. Mutational and kinetic analyses of the GTPase-activating protein (GAP)-p21 interaction: the C-terminal domain of GAP is not sufficient for full activity. [J] . P Gideon, J John, M Frech, Molecular and Cellular Biology . 1992 ,第5期

机译：GTPase激活蛋白（GAP）-p21相互作用的突变和动力学分析：GAP的C末端结构域不足以发挥全部活性。
2. KINETICS OF INORGANIC PHOSPHATE RELEASE DURING THE INTERACTION OF P21RAS WITH THE GTPASE-ACTIVATING PROTEINS, P120-GAP AND NEUROFIBROMIN [J] . Nixon AE, Brune M, Lowe PN, Biochemistry . 1995 ,第47期

机译：P21RAS与GTPase活化蛋白，P120-GAP和神经纤维蛋白相互作用时无机磷酸盐释放的动力学
3. MUTATION-DELETION ANALYSIS OF A CA2+-DEPENDENT PHOSPHOLIPID BINDING (CALB) DOMAIN WITHIN P120 GAP, A GTPASE-ACTIVATING PROTEIN FOR P21 RAS [J] . Gawler DJ, Zhang LJW, Moran MF The Biochemical Journal . 1995 ,第Pta2期

机译：在P120间隙内的CA2 +依赖性磷脂结合（CALB）域（用于P21 RAS的GTPase活化蛋白）的突变缺失分析
4. FUNCTIONAL ANALYSIS OF THE NIFA GAP DOMAIN OF AZOSPIRILLUM BRASILENSE: EFFECT OF TYR-PHE MUTATIONS IN NIFA AND INTERACTION OF THE MUTATED PROTEINS WITH GLNB USING THE YEAST TWO-HYBRID SYSTEM [C] . Sanfeng Chen, Li Liu, Xiaoyu Zhou, International Nitrogen Fixation Congress . 2005

机译：Azospirillum Brasilensense NiFa间隙结构域的功能分析：使用酵母双杂交系统对NiFa中Tyr-Phe突变在NiFa中突变蛋白与GLNB的相互作用
5. Novel mechanisms of regulation of the Cdc42 GTPase-activating protein CdGAP/ARHGAP31, a protein involved in cell migration and adhesion. [D] . Primeau, Martin. 2011

机译：调节Cdc42 GTPase活化蛋白CdGAP / ARHGAP31的新机制，该蛋白参与细胞迁移和粘附。
6. Mutational and kinetic analyses of the GTPase-activating protein (GAP)-p21 interaction: the C-terminal domain of GAP is not sufficient for full activity. [O] . P Gideon, J John, M Frech, 1992

机译：GTPase激活蛋白（GAP）-p21相互作用的突变和动力学分析：GAP的C末端结构域不足以发挥全部活性。
7. Mutational and kinetic analyses of the GTPase-activating protein (GAP)-p21 interaction: the C-terminal domain of GAP is not sufficient for full activity [O] . Gideon, P., John, J., Frech, M., 1992

机译：GTp酶活化蛋白（Gap）-p21相互作用的突变和动力学分析：Gap的C末端结构域不足以完全活动

Mutational and kinetic analyses of the GTPase-activating protein (GAP)-p21 interaction: the C-terminal domain of GAP is not sufficient for full activity.

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