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首页> 外文期刊>Journal of Molecular Biology >Kinetic analysis of the guanine nucleotide exchange activity of TRAPP, a multimeric Ypt1p exchange factor.
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Kinetic analysis of the guanine nucleotide exchange activity of TRAPP, a multimeric Ypt1p exchange factor.

机译:动力学分析的APP的鸟嘌呤核苷酸交换活性,一种多聚的Ypt1p交换因子。

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摘要

TRAPP complexes, which are large multimeric assemblies that function in membrane traffic, are guanine nucleotide exchange factors (GEFs) that activate the Rab GTPase Ypt1p. Here we measured rate and equilibrium constants that define the interaction of Ypt1p with guanine nucleotide (guanosine 5'-diphosphate and guanosine 5'-triphosphate/guanosine 5'-(beta,gamma-imido)triphosphate) and the core TRAPP subunits required for GEF activity. These parameters allowed us to identify the kinetic and thermodynamic bases by which TRAPP catalyzes nucleotide exchange from Ypt1p. Nucleotide dissociation from Ypt1p is slow (approximately 10(-4) s(-1)) and accelerated >1000-fold by TRAPP. Acceleration of nucleotide exchange by TRAPP occurs via a predominantly Mg(2+)-independent pathway. Thermodynamic linkage analysis indicates that TRAPP weakens nucleotide affinity by <80-fold and vice versa, in contrast to most other characterized GEF systems that weaken nucleotide binding affinities by 4-6 orders of magnitude. The overall net changes in nucleotide binding affinities are small because TRAPP accelerates both nucleotide binding and dissociation from Ypt1p. Weak thermodynamic coupling allows TRAPP, Ypt1p, and nucleotide to exist as a stable ternary complex, analogous to strain-sensing cytoskeleton motors. These results illustrate a novel strategy of guanine nucleotide exchange by TRAPP that is particularly suited for a multifunctional GEF involved in membrane traffic.
机译:TRAPP复合物是在膜运输中起作用的大型多聚体装配体,是激活Rab GTPase Ypt1p的鸟嘌呤核苷酸交换因子(GEF)。在这里,我们测量了速率和平衡常数,这些常数和平衡常数定义了Ypt1p与鸟嘌呤核苷酸(鸟苷5'-二磷酸和鸟苷5'-三磷酸/鸟苷5'-(β,γ-亚氨基)三磷酸)的相互作用以及GEF所需的核心TRAPP亚基活动。这些参数使我们能够确定TRAPP催化Ypt1p核苷酸交换的动力学和热力学基础。从Ypt1p解离核苷酸的速度很慢(大约10(-4)s(-1)),并通过TRAPP加速了> 1000倍。通过TRAPP的核苷酸交换加速主要通过Mg(2+)独立途径进行。热力学连锁分析表明,与大多数其他特征化的GEF系统将核苷酸结合亲和力降低4-6个数量级相比,TRAPP可以使核苷酸亲和力降低<80倍,反之亦然。核苷酸结合亲和力的总体净变化很小,因为TRAPP可以促进核苷酸结合和从Ypt1p解离。弱的热力学耦合使TRAPP,Ypt1p和核苷酸以稳定的三元复合物形式存在,类似于应变敏感的细胞骨架马达。这些结果说明了TRAPP鸟嘌呤核苷酸交换的新策略,特别适用于涉及膜运输的多功能GEF。

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