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致癌信号传导和肿瘤进展中的CD44亚型-细胞骨架相互作用

CD44 isoform-cytoskeleton interaction in oncogenic signaling and tumor progression.

作者信息

Bourguignon L Y, Zhu D, Zhu H

机构信息

Department of Cell Biology and Anatomy, University of Miami Medical School, Miami, Fl. 33101, USA.

出版信息

Front Biosci. 1998 Jul 1;3:d637-49. doi: 10.2741/a308.

Abstract

CD44, a major hyaluronan receptor, exists as several isoforms and is widely distributed in different cells and tissues. The isoforms of CD44, such as CD44s (the standard form), CD44E (the epithelial form) and CD44v (variant isoforms) (arise from differential splicing of one to ten (or eleven) variable exons that encode portions of the membrane proximal extracellular domain. The molecular diversity of CD44 isoforms is further compounded by differential biosynthetic processes and post-translational modifications [e.g. N-/O-glycosylation or glycosaminoglycan (GAG) addition]. This structural arrangement, which occurs within either the invariant region or the extracellular domain of the variant region, is important for CD44-mediated communication between extracellular matrix materials [ECM-hyaluronic acid (HA), collagen and fibronectin] and intracellular protein components (e.g cytoskeletal proteins and various regulatory enzymes). The 15 amino acid sequence [e.g. NSGNGAVEDRKPSGL (in human) or NGGNGTVEDRKPSEL (in mouse)] residing in the cytoplasmic domain of CD44 isoforms is the ankyrin-binding domain of this family of transmembrane glycoproteins. Biochemical analyses plus in vitro mutagenesis indicate that the ankyrin-binding domain is required for CD44-mediated "outside-in" and "inside-out" cell activation events. Furthermore, CD44s-cytoskeleton interaction is tightly coupled with signal transducing molecules (e.g. p185HER2 or Src kinases) during oncogenic signaling. Moreover, the transmembrane linkage between CD44v isoforms (CD44v10 and CD44v3) and the cytoskeleton up-regulates invasive and metastatic-specific tumor phenotypes [e.g. matrix degradation (MMPs) activities, tumor cell invasion and migration]. These findings strongly suggest that the interaction between CD44 isoforms and the cytoskeleton plays a pivotal role in the onset of oncogenesis and tumor progression.

摘要

CD44是一种主要的透明质酸受体,以多种异构体形式存在,广泛分布于不同的细胞和组织中。CD44的异构体,如CD44s(标准形式)、CD44E(上皮形式)和CD44v(可变异构体),是由一至十个(或十一个)可变外显子的差异剪接产生的,这些可变外显子编码膜近端细胞外结构域的部分区域。CD44异构体的分子多样性还因不同的生物合成过程和翻译后修饰(如N- / O-糖基化或糖胺聚糖(GAG)添加)而进一步复杂化。这种结构排列发生在可变区域的恒定区域或细胞外结构域内,对于CD44介导的细胞外基质材料(细胞外基质 - 透明质酸(HA)、胶原蛋白和纤连蛋白)与细胞内蛋白质成分(如细胞骨架蛋白和各种调节酶)之间的通讯很重要。位于CD44异构体细胞质结构域的15个氨基酸序列[如NSGNGAVEDRKPSGL(人类)或NGGNGTVEDRKPSEL(小鼠)]是该跨膜糖蛋白家族的锚蛋白结合结构域。生化分析以及体外诱变表明,锚蛋白结合结构域是CD44介导的“由外向内”和“由内向外”细胞激活事件所必需的。此外,在致癌信号传导过程中,CD44s - 细胞骨架相互作用与信号转导分子(如p185HER2或Src激酶)紧密耦合。此外,CD44v异构体(CD44v10和CD44v3)与细胞骨架之间的跨膜连接上调侵袭性和转移性特异性肿瘤表型[如基质降解(MMPs)活性、肿瘤细胞侵袭和迁移]。这些发现强烈表明,CD44异构体与细胞骨架之间的相互作用在肿瘤发生和肿瘤进展的起始中起关键作用。

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