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环化酶相关蛋白 1(CAP1)是 Rap1 GTPase 的异戊烯基结合伙伴。

Cyclase-associated protein 1 (CAP1) is a prenyl-binding partner of Rap1 GTPase.

机构信息

From the Department of Pharmacology and Chemical Biology, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania 15261 and.

Department of Physiology and Biophysics, School of Medicine, Case Western Reserve University, Cleveland, Ohio 44116.

出版信息

J Biol Chem. 2018 May 18;293(20):7659-7673. doi: 10.1074/jbc.RA118.001779. Epub 2018 Apr 4.

DOI:10.1074/jbc.RA118.001779
PMID:29618512
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5961064/
Abstract

Rap1 proteins are members of the Ras subfamily of small GTPases involved in many biological responses, including adhesion, cell proliferation, and differentiation. Like all small GTPases, they work as molecular allosteric units that are active in signaling only when associated with the proper membrane compartment. Prenylation, occurring in the cytosol, is an enzymatic posttranslational event that anchors small GTPases at the membrane, and prenyl-binding proteins are needed to mask the cytoplasm-exposed lipid during transit to the target membrane. However, several of these proteins still await discovery. In this study, we report that cyclase-associated protein 1 (CAP1) binds Rap1. We found that this binding is GTP-independent, does not involve Rap1's effector domain, and is fully contained in its C-terminal hypervariable region (HVR). Furthermore, Rap1 prenylation was required for high-affinity interactions with CAP1 in a geranylgeranyl-specific manner. The prenyl binding specifically involved CAP1's C-terminal hydrophobic β-sheet domain. We present a combination of experimental and computational approaches, yielding a model whereby the high-affinity binding between Rap1 and CAP1 involves electrostatic and nonpolar side-chain interactions between Rap1's HVR residues, lipid, and CAP1 β-sheet domain. The binding was stabilized by the lipid insertion into the β-solenoid whose interior was occupied by nonpolar side chains. This model was reminiscent of the recently solved structure of the PDEδ-K-Ras complex; accordingly, disruptors of this complex, deltarasin, blocked the Rap1-CAP1 interaction. These findings indicate that CAP1 is a geranylgeranyl-binding partner of Rap1.

摘要

Rap1 蛋白是 Ras 亚家族小分子 GTP 酶的成员,参与许多生物反应,包括黏附、细胞增殖和分化。与所有小分子 GTP 酶一样,它们作为分子变构单元发挥作用,只有与适当的膜隔室结合时才具有信号活性。发生在细胞质中的 prenylation 是一种酶促翻译后事件,将小分子 GTP 酶锚定在膜上,并且需要 prenyl 结合蛋白在转运到靶膜时掩盖暴露在细胞质中的脂质。然而,其中一些蛋白质仍有待发现。在这项研究中,我们报告 cyclase-associated protein 1 (CAP1) 与 Rap1 结合。我们发现这种结合是 GTP 非依赖性的,不涉及 Rap1 的效应结构域,并且完全包含在其 C 末端高变区 (HVR) 中。此外,Rap1 的 prenylation 以 geranylgeranyl 特异性方式与 CAP1 高亲和力相互作用是必需的。prenyl 结合特异性涉及 CAP1 的 C 末端疏水性 β-折叠结构域。我们提出了实验和计算方法的组合,得出了一个模型,即 Rap1 和 CAP1 之间的高亲和力结合涉及 Rap1 的 HVR 残基、脂质和 CAP1 β-折叠结构域之间的静电和非极性侧链相互作用。脂质插入β-螺线管稳定了结合,其内部被非极性侧链占据。这种模型类似于最近解决的 PDEδ-K-Ras 复合物结构;因此,该复合物的破坏剂 deltarasin 阻断了 Rap1-CAP1 相互作用。这些发现表明 CAP1 是 Rap1 的 geranylgeranyl 结合伴侣。

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