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人膜辅因子蛋白(MCP)的分子克隆与染色体定位。纳入补体调节蛋白多基因家族的证据。

Molecular cloning and chromosomal localization of human membrane cofactor protein (MCP). Evidence for inclusion in the multigene family of complement-regulatory proteins.

作者信息

Lublin D M, Liszewski M K, Post T W, Arce M A, Le Beau M M, Rebentisch M B, Lemons L S, Seya T, Atkinson J P

机构信息

Department of Pathology, Washington University, St. Louis, Missouri 63110.

出版信息

J Exp Med. 1988 Jul 1;168(1):181-94. doi: 10.1084/jem.168.1.181.

Abstract

Membrane cofactor protein (MCP), a regulatory molecular of the complement system with cofactor activity for the factor I-mediated inactivation of C3b and C4b, is widely distributed, being present on leukocytes, platelets, endothelial cells, epithelial cells, and fibroblasts. MCP was purified from a human T cell line (HSB2) and the NH2-terminal 24-amino acid sequence obtained by Edman degradation. An oligonucleotide probe based on this sequence was used to identify a clone from a human monocytic (U937) cDNA library. Nucleotide sequencing showed a 43-bp 5'-untranslated region, an open reading frame of 1,152 bp, and a 335-bp 3'-untranslated region followed by a 16-bp poly(A) track. The deduced full-length MCP protein consists of a 34-amino acid signal peptide and a 350-amino acid mature protein. The protein has, beginning at the NH2 terminus, four approximately 60-amino acid repeat units that match the consensus sequence found in a multigene family of complement regulatory proteins (C3b-receptor or CR1, C3d-receptor or CR2, decay-accelerating factor, C4-binding protein, and factor H), as well as several other complement and non-complement proteins. The remainder of the MCP protein consists of 25 amino acids that are rich in serine and threonine (probable site of heavy O-linked glycosylation of MCP), 17 amino acids of unknown significance, and a 23-amino acid transmembrane hydrophobic region followed by a 33-amino acid cytoplasmic tail. The MCP gene was localized to human chromosome 1, bands 1q31-41, by analysis of human x rodent somatic cell hybrid clones and by in situ hybridization. This same genetic region contains the multigene family of complement-regulatory proteins, which is thereby enlarged to include the functionally and structurally related MCP.

摘要

膜辅因子蛋白(MCP)是补体系统的一种调节分子,对I因子介导的C3b和C4b失活具有辅因子活性,广泛分布于白细胞、血小板、内皮细胞、上皮细胞和成纤维细胞中。从人T细胞系(HSB2)中纯化出MCP,并通过埃德曼降解法获得其氨基末端24个氨基酸的序列。基于该序列的寡核苷酸探针用于从人单核细胞(U937)cDNA文库中鉴定一个克隆。核苷酸测序显示有一个43bp的5'非翻译区、一个1152bp的开放阅读框、一个335bp的3'非翻译区,其后是一个16bp的聚腺苷酸尾。推导的全长MCP蛋白由一个34个氨基酸的信号肽和一个350个氨基酸的成熟蛋白组成。该蛋白从氨基末端开始有四个约60个氨基酸的重复单元,与补体调节蛋白多基因家族(C3b受体或CR1、C3d受体或CR2、衰变加速因子、C4结合蛋白和I因子H)以及其他一些补体和非补体蛋白中的共有序列相匹配。MCP蛋白的其余部分由25个富含丝氨酸和苏氨酸的氨基酸(可能是MCP的O-连接重糖基化位点)、17个意义不明的氨基酸以及一个23个氨基酸的跨膜疏水区域和一个33个氨基酸的胞质尾组成。通过对人-啮齿动物体细胞杂种克隆的分析和原位杂交,MCP基因定位于人染色体1的1q31-41带。同一基因区域包含补体调节蛋白多基因家族,因此该家族扩大到包括功能和结构相关的MCP。

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