首页> 美国卫生研究院文献>Acta Crystallographica Section F: Structural Biology and Crystallization Communications >Structure of a truncated form of leucine zipper II of JIP3 reveals an unexpected antiparallel coiled-coil arrangement
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Structure of a truncated form of leucine zipper II of JIP3 reveals an unexpected antiparallel coiled-coil arrangement

机译:JIP3的亮氨酸拉链II的截短形式的结构揭示了意外的反平行卷曲线圈排列

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摘要

JIP3 and JIP4, two highly related scaffolding proteins for MAP kinases, are binding partners for two molecular motors as well as for the small G protein ARF6. The leucine zipper II (LZII) region of JIP3/4 is the binding site for these three partners. Previously, the crystal structure of ARF6 bound to JIP4 revealed LZII in a parallel coiled-coil arrangement. Here, the crystal structure of an N-terminally truncated form of LZII of JIP3 alone shows an unexpected antiparallel arrangement. Using molecular dynamics and modelling, the stability of this antiparallel LZII arrangement, as well as its specificity for ARF6, were investigated. This study highlights that N-terminal truncation of LZII can change its coiled-coil orientation without affecting its overall stability. Further, a conserved buried asparagine residue was pinpointed as a possible structural determinant for this dramatic structural rearrangement. Thus, LZII of JIP3/4 is a versatile structural motif, modifications of which can impact partner recognition and thus biological function.
机译:JIP3和JIP4是MAP激酶的两个高度相关的支架蛋白,是两个分子马达以及小G蛋白ARF6的结合伴侣。 JIP3 / 4的亮氨酸拉链II(LZII)区是这三个伴侣的结合位点。以前,与JIP4结合的ARF6的晶体结构以平行盘绕线圈排列形式显示LZII。在此,单独的JIP3的LZII的N末端截短形式的晶体结构显示出意想不到的反平行排列。使用分子动力学和建模,研究了这种反平行LZII排列的稳定性及其对ARF6的特异性。这项研究强调LZII的N端截短可以改变其卷曲螺旋方向,而不会影响其整体稳定性。此外,将保守的埋藏天冬酰胺残基精确定位为这种剧烈的结构重排的可能结构决定因素。因此,JIP3 / 4的LZII是一种通用的结构基序,对其修饰可能会影响伴侣识别,进而影响生物学功能。

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