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短肽序列活性位点定义的胸腺肽β4 的生物学活性。

Biological activities of thymosin beta4 defined by active sites in short peptide sequences.

机构信息

Department of Opthalmology and Anatomy/Cell Biology, Wayne State University School of Medicine, Detroit, MI 48201, USA.

出版信息

FASEB J. 2010 Jul;24(7):2144-51. doi: 10.1096/fj.09-142307. Epub 2010 Feb 23.

DOI:10.1096/fj.09-142307
PMID:20179146
Abstract

Thymosin beta(4), a small ubiquitous protein containing 43 aa, has structure/function activity via its actin-binding domain and numerous biological affects on cells. Since it is the major actin-sequestering molecule in eukaryotic cells and is found essentially in all cells and body fluids, thymosin beta(4) has the potential for significant roles in tissue development, maintenance, repair, and pathology. Several active sites with unique functions have been identified, including the amino-terminal site containing 4 aa (Ac-SDKP) that generally blocks inflammation and reduces fibrosis. Another active site at the amino terminus contains 15 aa, including Ac-SDKP, and promotes cell survival and blocks apoptosis, while a short sequence containing LKKTETQ, the central actin-binding domain (aa 17-23) plus 1 additional amino acid (Q), promotes angiogenesis, wound healing, and cell migration. Several additional biological activities have been identified but not yet localized in the molecule, including its antimicrobial activity, the induction of various genes (including laminin-5, MMPs, TGF beta, zyxin, terminal deoxynucleotidyl transferase, and angiogenesis-related proteins), and the ability to activate ILK/PINCH/Akt, and other signaling molecules important in both apoptosis and inflammatory pathways. This review details these important physiologically and pathologically active sites and their potential therapeutic uses.

摘要

胸腺素β 4(Thymosin beta(4))是一种含有 43 个氨基酸的小而普遍存在的蛋白质,通过其肌动蛋白结合结构域具有结构/功能活性,并对细胞具有许多生物学影响。由于它是真核细胞中主要的肌动蛋白隔离分子,并且基本上存在于所有细胞和体液中,因此胸腺素β 4(Thymosin beta(4))在组织发育、维持、修复和病理学方面具有重要作用。已经确定了几个具有独特功能的活性部位,包括含有 4 个氨基酸的氨基末端位点(Ac-SDKP),通常可阻止炎症并减少纤维化。氨基末端的另一个活性位点包含 15 个氨基酸,包括 Ac-SDKP,可促进细胞存活并阻止细胞凋亡,而包含 LKKTETQ 的短序列,即中心肌动蛋白结合结构域(氨基酸 17-23)加 1 个额外氨基酸(Q),可促进血管生成、伤口愈合和细胞迁移。已经确定了其他一些生物学活性,但尚未在该分子中定位,包括其抗菌活性、诱导各种基因(包括层粘连蛋白-5、MMPs、TGF-β、zyxin、末端脱氧核苷酸转移酶和与血管生成相关的蛋白质)的能力,以及激活 ILK/PINCH/Akt 和其他在细胞凋亡和炎症途径中都很重要的信号分子的能力。本文综述了这些重要的生理和病理活性部位及其潜在的治疗用途。

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