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NSP-CAS蛋白复合物:癌症中新兴的信号传导模块

NSP-CAS Protein Complexes: Emerging Signaling Modules in Cancer.

作者信息

Wallez Yann, Mace Peter D, Pasquale Elena B, Riedl Stefan J

机构信息

Sanford-Burnham Medical Research Institute, La Jolla, CA, USA.

出版信息

Genes Cancer. 2012 May;3(5-6):382-93. doi: 10.1177/1947601912460050.

Abstract

The CAS (CRK-associated substrate) family of adaptor proteins comprises 4 members, which share a conserved modular domain structure that enables multiple protein-protein interactions, leading to the assembly of intracellular signaling platforms. Besides their physiological role in signal transduction downstream of a variety of cell surface receptors, CAS proteins are also critical for oncogenic transformation and cancer cell malignancy through associations with a variety of regulatory proteins and downstream effectors. Among the regulatory partners, the 3 recently identified adaptor proteins constituting the NSP (novel SH2-containing protein) family avidly bind to the conserved carboxy-terminal focal adhesion-targeting (FAT) domain of CAS proteins. NSP proteins use an anomalous nucleotide exchange factor domain that lacks catalytic activity to form NSP-CAS signaling modules. Additionally, the NSP SH2 domain can link NSP-CAS signaling assemblies to tyrosine-phosphorylated cell surface receptors. NSP proteins can potentiate CAS function by affecting key CAS attributes such as expression levels, phosphorylation state, and subcellular localization, leading to effects on cell adhesion, migration, and invasion as well as cell growth. The consequences of these activities are well exemplified by the role that members of both families play in promoting breast cancer cell invasiveness and resistance to antiestrogens. In this review, we discuss the intriguing interplay between the NSP and CAS families, with a particular focus on cancer signaling networks.

摘要

衔接蛋白的CAS(CRK相关底物)家族由4个成员组成,它们共享一个保守的模块化结构域结构,该结构能够实现多种蛋白质-蛋白质相互作用,从而导致细胞内信号平台的组装。除了在多种细胞表面受体下游的信号转导中发挥生理作用外,CAS蛋白通过与多种调节蛋白和下游效应器结合,对致癌转化和癌细胞恶性程度也至关重要。在调节伙伴中,最近鉴定出的构成NSP(含新型SH2结构域蛋白)家族的3种衔接蛋白与CAS蛋白保守的羧基末端粘着斑靶向(FAT)结构域紧密结合。NSP蛋白利用一个缺乏催化活性的异常核苷酸交换因子结构域来形成NSP-CAS信号模块。此外,NSP SH2结构域可将NSP-CAS信号组装与酪氨酸磷酸化的细胞表面受体相连。NSP蛋白可通过影响关键的CAS属性(如表达水平、磷酸化状态和亚细胞定位)来增强CAS功能,从而对细胞粘附、迁移、侵袭以及细胞生长产生影响。这两个家族的成员在促进乳腺癌细胞侵袭和抗雌激素耐药性方面所起的作用很好地例证了这些活动的后果。在本综述中,我们讨论了NSP和CAS家族之间有趣的相互作用,特别关注癌症信号网络。

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