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RAF 抑制剂诱导的 KSR1/B-RAF 结合及其对 ERK 级联信号转导的影响。

RAF inhibitor-induced KSR1/B-RAF binding and its effects on ERK cascade signaling.

机构信息

Laboratory of Cell and Developmental Signaling, Center for Cancer Research, National Cancer Institute-Frederick, Frederick, MD 21702, USA.

出版信息

Curr Biol. 2011 Apr 12;21(7):563-8. doi: 10.1016/j.cub.2011.02.033. Epub 2011 Mar 31.

DOI:10.1016/j.cub.2011.02.033
PMID:21458265
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3075323/
Abstract

RAF kinase inhibitors can induce ERK cascade signaling by promoting dimerization of RAF family members in the presence of oncogenic or normally activated RAS. This interaction is mediated by a dimer interface region in the RAF kinase domain that is conserved in members of the ERK cascade scaffold family, kinase suppressor of RAS (KSR). In this study, we find that most RAF inhibitors also induce the binding of KSR1 to wild-type and oncogenic B-RAF proteins, including V600E B-RAF, but promote little complex formation between KSR1 and C-RAF. The inhibitor-induced KSR1/B-RAF interaction requires direct binding of the drug to B-RAF and is dependent on conserved dimer interface residues in each protein, but, unexpectedly, is not dependent on binding of B-RAF to activated RAS. Inhibitor-induced KSR/B-RAF complex formation can occur in the cytosol and is observed in normal mouse fibroblasts, as well as a variety of human cancer cell lines. Strikingly, we find that KSR1 competes with C-RAF for inhibitor-induced binding to B-RAF and, as a result, alters the effect of the inhibitors on ERK cascade signaling.

摘要

RAF 激酶抑制剂可在致癌或正常激活的 RAS 存在的情况下通过促进 RAF 家族成员的二聚化来诱导 ERK 级联信号传导。这种相互作用由 RAF 激酶结构域中的二聚体界面区域介导,该区域在 ERK 级联支架家族成员、RAS 激酶抑制剂(KSR)中保守。在这项研究中,我们发现大多数 RAF 抑制剂还诱导 KSR1 与野生型和致癌性 B-RAF 蛋白(包括 V600E B-RAF)结合,但很少促进 KSR1 与 C-RAF 之间形成复合物。抑制剂诱导的 KSR1/B-RAF 相互作用需要药物与 B-RAF 的直接结合,并且依赖于每种蛋白质中保守的二聚体界面残基,但出乎意料的是,它不依赖于 B-RAF 与激活的 RAS 的结合。抑制剂诱导的 KSR/B-RAF 复合物形成可发生在细胞质中,并在正常的小鼠成纤维细胞以及各种人类癌细胞系中观察到。引人注目的是,我们发现 KSR1 与 C-RAF 竞争抑制剂诱导的与 B-RAF 的结合,从而改变了抑制剂对 ERK 级联信号传导的影响。

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