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通过分析杂交传感器激酶探究HAMP连接子结构的保守性和信号转导机制。

Probing conservation of HAMP linker structure and signal transduction mechanism through analysis of hybrid sensor kinases.

作者信息

Appleman J Alex, Chen Li-Ling, Stewart Valley

机构信息

Section of Microbiology, University of California, Davis, California 95616-8665, USA.

出版信息

J Bacteriol. 2003 Aug;185(16):4872-82. doi: 10.1128/JB.185.16.4872-4882.2003.

DOI:10.1128/JB.185.16.4872-4882.2003
PMID:12897007
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC166472/
Abstract

The HAMP linker, a predicted structural element observed in many sensor kinases and methyl-accepting chemotaxis proteins, transmits signals between sensory input modules and output modules. HAMP linkers are located immediately inside the cytoplasmic membrane and are predicted to form two short amphipathic alpha-helices (AS-1 and AS-2) joined by an unstructured connector. HAMP linkers are found in the Escherichia coli nitrate- and nitrite-responsive sensor kinases NarX and NarQ (which respond to ligand by increasing kinase activity) and the sensor kinase CpxA (which responds to ligand by decreasing kinase activity). We constructed a series of hybrids with fusion points throughout the HAMP linker, in which the sensory modules of NarX or NarQ are fused to the transmitter modules of NarX, NarQ, or CpxA. A hybrid of the NarX sensor module and the CpxA HAMP linker and transmitter module (NarX-CpxA-1) responded to nitrate by decreasing kinase activity, whereas a hybrid in which the HAMP linker of NarX was replaced by that of CpxA (NarX-CpxA-NarX-1) responded to nitrate by increasing kinase activity. However, sequence variations between HAMP linkers do not allow free exchange of HAMP linkers or their components. Certain deletions in the NarX HAMP linker resulted in characteristic abnormal responses to ligand; similar deletions in the NarQ and NarX-CpxA-1 HAMP linkers resulted in responses to ligand generally similar to those seen in NarX. We conclude that the structure and action of the HAMP linker are conserved and that the HAMP linker transmits a signal to the output domain that ligand is bound.

摘要

HAMP连接子是在许多传感激酶和甲基接受趋化蛋白中观察到的一种预测结构元件,它在感觉输入模块和输出模块之间传递信号。HAMP连接子位于细胞质膜内侧,预计会形成两个由无结构连接体连接的短两性α螺旋(AS-1和AS-2)。HAMP连接子存在于大肠杆菌硝酸盐和亚硝酸盐响应传感激酶NarX和NarQ(通过增加激酶活性对配体作出反应)以及传感激酶CpxA(通过降低激酶活性对配体作出反应)中。我们构建了一系列在整个HAMP连接子上有融合点的杂种,其中NarX或NarQ的感觉模块与NarX、NarQ或CpxA的传递器模块融合。NarX传感模块与CpxA的HAMP连接子及传递器模块的杂种(NarX-CpxA-1)通过降低激酶活性对硝酸盐作出反应,而用CpxA的HAMP连接子取代NarX的HAMP连接子的杂种(NarX-CpxA-NarX-1)则通过增加激酶活性对硝酸盐作出反应。然而,HAMP连接子之间的序列差异不允许HAMP连接子或其组件自由交换。NarX的HAMP连接子中的某些缺失导致对配体产生特征性异常反应;NarQ和NarX-CpxA-1的HAMP连接子中的类似缺失导致对配体的反应通常与在NarX中看到的反应相似。我们得出结论,HAMP连接子的结构和作用是保守的,并且HAMP连接子向输出结构域传递配体已结合的信号。

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