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αvβ8整合素配体结合特异性的分子基础

Molecular Basis of the Ligand Binding Specificity of αvβ8 Integrin.

作者信息

Ozawa Akio, Sato Yuya, Imabayashi Tsukasa, Uemura Toshihiko, Takagi Junichi, Sekiguchi Kiyotoshi

机构信息

From the Institute for Protein Research, Osaka University, 3-2 Yamadaoka, Suita, Osaka 565-0871, Japan.

From the Institute for Protein Research, Osaka University, 3-2 Yamadaoka, Suita, Osaka 565-0871, Japan

出版信息

J Biol Chem. 2016 May 27;291(22):11551-65. doi: 10.1074/jbc.M116.719138. Epub 2016 Mar 31.

Abstract

αvβ8 is an integrin that recognizes an Arg-Gly-Asp (RGD) motif and interacts with fibronectin, vitronectin, and latent TGF-β1. We comprehensively determined the binding activity of the αvβ8 integrin toward 25 secreted proteins having an RGD motif. The αvβ8 integrin strongly bound to latent TGF-β1 but showed marginal activity for other RGD-containing proteins, including fibronectin and vitronectin. Site-directed mutagenesis of latent TGF-β1 demonstrated that the high affinity binding of αvβ8 integrin to latent TGF-β1 was defined by Leu-218 immediately following the RGD motif within the latency-associated peptide of TGF-β1. Consistent with the critical role of Leu-218 in latent TGF-β1 recognition by αvβ8 integrin, a 9-mer synthetic peptide containing an RGDL sequence strongly inhibited interactions of latent TGF-β1 with αvβ8 integrin, whereas a 9-mer peptide with an RGDA sequence was ∼60-fold less inhibitory. Because αvβ3 integrin did not exhibit strong binding to latent TGF-β1 or distinguish between RGDL- and RGDA-containing peptides, we explored the mechanism by which the integrin β8 subunit defines the high affinity binding of latent TGF-β1 by αvβ8 integrin. Production of a series of swap mutants of integrin β8 and β3 subunits indicated that the high affinity binding of αvβ8 integrin with latent TGF-β1 was ensured by interactions between the Leu-218 residue and the β8 I-like domain, with the former serving as an auxiliary recognition residue defining the restricted ligand specificity of αvβ8 integrin toward latent TGF-β1. In support of this conclusion, high affinity binding toward the αvβ8 integrin was conferred on fibronectin by substitution of its RGDS motif with an RGDL sequence.

摘要

αvβ8是一种整合素,可识别精氨酸-甘氨酸-天冬氨酸(RGD)基序,并与纤连蛋白、玻连蛋白和潜伏转化生长因子-β1(TGF-β1)相互作用。我们全面测定了αvβ8整合素对25种具有RGD基序的分泌蛋白的结合活性。αvβ8整合素与潜伏TGF-β1紧密结合,但对其他含RGD的蛋白(包括纤连蛋白和玻连蛋白)表现出微弱的活性。对潜伏TGF-β1进行定点诱变表明,αvβ8整合素与潜伏TGF-β1的高亲和力结合是由TGF-β1潜伏期相关肽中RGD基序后的Leu-218所决定的。与Leu-218在αvβ8整合素识别潜伏TGF-β1中的关键作用一致,一种包含RGDL序列的9聚体合成肽强烈抑制潜伏TGF-β1与αvβ8整合素的相互作用,而具有RGDA序列的9聚体肽的抑制作用则小约60倍。由于αvβ3整合素对潜伏TGF-β1没有表现出强结合,也无法区分含RGDL和RGDA的肽,我们探究了整合素β8亚基决定αvβ8整合素对潜伏TGF-β1高亲和力结合的机制。一系列整合素β8和β3亚基交换突变体的产生表明,αvβ8整合素与潜伏TGF-β1的高亲和力结合是由Leu-218残基与β8 I样结构域之间的相互作用所确保的,前者作为一个辅助识别残基,决定了αvβ8整合素对潜伏TGF-β1有限的配体特异性。支持这一结论的是,通过将纤连蛋白的RGDS基序替换为RGDL序列,赋予了纤连蛋白对αvβ8整合素的高亲和力结合。

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