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Control of biochemical reactions through supramolecular RING domain self-assembly

机译:通过超分子RING域自组装控制生化反应

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摘要

RING domains act in a variety of unrelated biochemical reactions, with many of these domains forming key parts of supramolecular assemblies in cells. Here, we observe that purified RINGs from a variety of functionally unrelated proteins, including promyelocytic leukemia protein, KAP-1/TIF1β, Z, Mel18, breast cancer susceptibility gene product 1 (BRCA1), and BRCA1-associated RING domain (BARD1), self-assemble into supramolecular structures in vitro that resemble those they form in cells. RING bodies form polyvalent binding surfaces and scaffold multiple partner proteins. Separation of RING bodies from monomers reveals that self-assembly controls and amplifies their specific activities in two unrelated biochemistries: reduction of 5′ mRNA cap affinity of eIF4E by promyelocytic leukemia protein and Z, and E3 ubiquitin conjugation activity of BARD1:BRCA1. Functional significance of self-assembly is underscored by partial restoration of assembly and E3 activity of cancer predisposing BRCA1 mutant by forced oligomerization. RING self-assembly creates bodies that act structurally as polyvalent scaffolds, thermodynamically by amplifying activities of partner proteins, and catalytically by spatiotemporal coupling of enzymatic reactions. These studies reveal a general paradigm of how supramolecular structures may function in cells.
机译:RING域在多种不相关的生化反应中起作用,其中许多域构成细胞中超分子组装的关键部分。在这里,我们观察到从多种功能无关的蛋白(包括早幼粒细胞白血病蛋白,KAP-1 /TIF1β,Z,Mel18,乳腺癌易感性基因产物1(BRCA1)和与BRCA1相关的RING域(BARD1),在体外自组装成超分子结构,类似于它们在细胞中形成的结构。 RING体形成多价结合表面并支撑多个伴侣蛋白。 RING体与单体的分离揭示了在两个不相关的生物化学中自组装控制并放大了它们的特定活性:早幼粒细胞白血病蛋白和Z降低eIF4E的5'mRNA帽亲和力,以及BARD1:BRCA1的E3泛素结合活性。通过强制寡聚化,部分易恢复的癌症和易患BRCA1突变的癌症的E3活性突出了自组装的功能重要性。 RING自组装产生的物体在结构上起多价支架的作用,通过增加伴侣蛋白的活性在热力学上发挥作用,并通过酶反应的时空偶合来催化作用。这些研究揭示了超分子结构如何在细胞中起作用的一般范例。

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