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新型血小板反应蛋白1 I型重复序列融合蛋白的表达与特性分析

Expression and characterization of novel thrombospondin 1 type I repeat fusion proteins.

作者信息

Qabar A N, Bullock J, Matej L, Polverini P

机构信息

Department of Clinical Investigation, Madigan Army Medical Center, Tacoma, WA 98431, USA.

出版信息

Biochem J. 2000 Feb 15;346 Pt 1(Pt 1):147-53.

Abstract

Thrombospondin (TSP)1 is a trimeric extracellular matrix protein that is held together by two cysteine residues. It is one of five TSP proteins that have been described to date with almost a universal heparin binding capability (TSP5 being the exception). The existence of two conformationally distinct structures in the TSP family (trimers and pentamers) prompted us to investigate the contribution of TSP1 trimeric structure to its inhibitory role in angiogenesis. We expressed full-length recombinant human TSP1, its type I repeats, and murine TSP3 in a human embryonic kidney cell line and evaluated their effect on human dermal microvascular endothelial cell (HMVEC) proliferation and sprouting into tube-like structures in vitro. Additionally, two chimaeric molecules were constructed so that the type I repeats of TSP1 were expressed as either dimers (TSP1-Ig chimaera) or pentamers (TSP1-TSP3 chimaera). Dimeric and pentameric type I constructs are novel structures. We found that, similarly to full-length TSP1, intact trimeric type I repeats were inhibitory to HMVEC angiogenesis in vitro. However, dimeric and pentameric type I repeats of TSP1 only partially inhibited HMVEC proliferation and sprouting in vitro. TSP3, which is lacking type I repeats, had no inhibitory activity, confirming that type I repeats elicit the anti-angiogenic activity of TSP1.

摘要

血小板反应蛋白(TSP)1是一种三聚体细胞外基质蛋白,由两个半胱氨酸残基维系在一起。它是迄今已描述的五种TSP蛋白之一,几乎具有普遍的肝素结合能力(TSP5除外)。TSP家族中存在两种构象不同的结构(三聚体和五聚体),这促使我们研究TSP1三聚体结构对其在血管生成中抑制作用的贡献。我们在人胚肾细胞系中表达了全长重组人TSP1、其I型重复序列和小鼠TSP3,并评估了它们对人真皮微血管内皮细胞(HMVEC)增殖以及在体外形成管状结构的发芽的影响。此外,构建了两种嵌合分子,使TSP1的I型重复序列分别以二聚体(TSP1-Ig嵌合体)或五聚体(TSP1-TSP3嵌合体)形式表达。二聚体和五聚体I型构建体是新型结构。我们发现,与全长TSP1类似,完整的三聚体I型重复序列在体外对HMVEC血管生成具有抑制作用。然而,TSP1的二聚体和五聚体I型重复序列仅部分抑制HMVEC在体外的增殖和发芽。缺乏I型重复序列的TSP3没有抑制活性,这证实I型重复序列引发了TSP1的抗血管生成活性。

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