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Ras and the Plasma Membrane: A Complicated Relationship

机译:Ras和血浆膜:复杂的关系

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摘要

The primary site of Ras signal transduction is the plasma membrane (PM). On the PM, the ubiquitously expressed Ras isoforms, H-, N-, and K-Ras, spatially segregate to nonoverlapping nanometer-sized domains, called nanoclusters, with further lateral segregation into nonoverlapping guanosine triphosphate (GTP)-bound and guanosine diphosphate (GDP)-bound nanoclusters. Effector binding and activation is restricted to GTP nanoclusters, rendering the underlying assembly mechanism essential to Ras signaling. Ras nanoclusters have distinct lipid compositions as a result of lipid-sorting specificity encoded in each Ras carboxy-terminal membrane anchor. The role of the G-domain in regulating anchor–membrane interactions is becoming clearer. Ras G-domains undergo significant conformational orientation changes on guanine nucleotide switch, leading to differential direct contacts between the G-domain and reorganization of the membrane anchor. Ras G-domains also contain weak dimer interfaces, resulting in homodimerization, which is an obligate step of nanoclustering. Modulating the formation of Ras dimers, the lipid composition of the PM or lateral dynamics of key PM phospholipids represent novel mechanisms whereby the extent of Ras nanoclustering can be regulated to tune the gain in Ras signaling circuits.
机译:RAS信号转导的主要部位是血浆膜(PM)。在PM上,普遍地表达Ras同种型,H-,N-和K-RA,在空间上分离为非传播的纳米尺寸的结构域,称为纳米能器,具有进一步的横向偏析,进入非传播的鸟氨酸三磷酸(GTP) - α-基磷酸(GTP)和鸟苷二磷酸( GDP)-Bound Nanoclusters。效应器结合和激活仅限于GTP纳米单元,使潜在的组装机制成为RAS信号。 Ras纳米能器具有不同的脂质组合物,其脂质分选特异性在每个Ras羧基末端膜锚定量中被编码。 G域在调节锚膜相互作用方面的作用变得更加清晰。 RAS G域对鸟嘌呤核苷酸开关进行显着的构象取向变化,导致G域和膜锚的重组之间的差异直接接触。 RAS G-域还含有弱二聚体界面,导致同型二聚体,这是纳米环节的缩小步骤。调节RAS二聚体的形成,PM PM磷脂的PM或横向动力学的脂质组合物代表了新的机制,由此可以调节RAS纳米弹性的程度以调节RA信号电路中的增益。

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