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通往 Ras 纳米团簇的药物靶向机会。

Drug targeting opportunities en route to Ras nanoclusters.

机构信息

Cancer Cell Biology and Drug Discovery Group, Department of Life Sciences and Medicine, University of Luxembourg, Esch-sur-Alzette, Luxembourg.

Cancer Cell Biology and Drug Discovery Group, Department of Life Sciences and Medicine, University of Luxembourg, Esch-sur-Alzette, Luxembourg.

出版信息

Adv Cancer Res. 2022;153:63-99. doi: 10.1016/bs.acr.2021.07.005. Epub 2021 Aug 20.

DOI:10.1016/bs.acr.2021.07.005
PMID:35101236
Abstract

Disruption of the native membrane organization of Ras by the farnesyltransferase inhibitor tipifarnib in the late 1990s constituted the first indirect approach to drug target Ras. Since then, our understanding of how dynamically Ras shuttles between subcellular locations has changed significantly. Ras proteins have to arrive at the plasma membrane for efficient MAPK-signal propagation. On the plasma membrane Ras proteins are organized into isoform specific proteo-lipid assemblies called nanocluster. Recent evidence suggests that Ras nanocluster have a specific lipid composition, which supports the recruitment of effectors such as Raf. Conversely, effectors possess lipid-recognition motifs, which appear to serve as co-incidence detectors for the lipid domain of a given Ras isoform. Evidence suggests that dimeric Raf proteins then co-assemble dimeric Ras in an immobile complex, thus forming the minimal unit of an active nanocluster. Here we review established and novel trafficking chaperones and trafficking factors of Ras, along with the set of lipid and protein modulators of Ras nanoclustering. We highlight drug targeting approaches and opportunities against these determinants of functional Ras membrane organization. Finally, we reflect on implications for Ras signaling in polarized cells, such as epithelia, which are a common origin of tumorigenesis.

摘要

上世纪 90 年代末,法尼基转移酶抑制剂替匹法尼阻断 Ras 固有膜组织的形成,这是靶向 Ras 的第一种间接方法。从那时起,我们对 Ras 如何在亚细胞位置之间动态穿梭的理解发生了重大变化。Ras 蛋白必须到达质膜才能有效地进行 MAPK 信号转导。在质膜上,Ras 蛋白被组织成称为纳米簇的同种型特异性蛋白脂组装体。最近的证据表明,Ras 纳米簇具有特定的脂质组成,这支持了效应器如 Raf 的募集。相反,效应器具有脂质识别模体,这些模体似乎充当给定 Ras 同种型的脂质域的巧合检测器。有证据表明,二聚体 Raf 蛋白然后在非活性复合物中共同组装二聚体 Ras,从而形成活性纳米簇的最小单位。在这里,我们回顾了 Ras 的已建立和新的运输伴侣和运输因子,以及 Ras 纳米簇形成的脂质和蛋白质调节剂。我们强调了针对这些功能性 Ras 膜组织决定因素的药物靶向方法和机会。最后,我们反思了 Ras 信号在极化细胞(如上皮细胞)中的意义,上皮细胞是肿瘤发生的常见起源。

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Drug targeting opportunities en route to Ras nanoclusters.通往 Ras 纳米团簇的药物靶向机会。
Adv Cancer Res. 2022;153:63-99. doi: 10.1016/bs.acr.2021.07.005. Epub 2021 Aug 20.
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Ras nanoclusters: a new drug target?Ras纳米簇:一个新的药物靶点?
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Ras nanoclusters: Versatile lipid-based signaling platforms.Ras纳米簇:多功能脂质信号平台。
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The efficacy of Raf kinase recruitment to the GTPase H-ras depends on H-ras membrane conformer-specific nanoclustering.Raf 激酶向 GTP 酶 H-ras 的募集效力取决于 H-ras 膜构象特异性纳米簇集。
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Targeting RAS Membrane Association: Back to the Future for Anti-RAS Drug Discovery?靶向RAS膜结合:抗RAS药物研发回归未来?
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