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膜辅因子蛋白(CD46)是一种不被内吞的基底外侧蛋白。羧基末端四肽FTSL的重要性。

Membrane cofactor protein (CD46) is a basolateral protein that is not endocytosed. Importance of the tetrapeptide FTSL at the carboxyl terminus.

作者信息

Maisner A, Zimmer G, Liszewski M K, Lublin D M, Atkinson J P, Herrler G

机构信息

Institut für Virologie, Philipps-Universität Marburg, D-35037 Marburg, Germany.

出版信息

J Biol Chem. 1997 Aug 15;272(33):20793-9. doi: 10.1074/jbc.272.33.20793.

Abstract

Membrane cofactor protein (MCP) is a widely distributed complement regulatory protein that is expressed on the basolateral surface of polarized epithelial cells. The basolateral targeting of the BC1 isoform of MCP was analyzed by generating deletion mutants and point mutants within the cytoplasmic tail of 16 amino acids. A sequence of four amino acids, FTSL, was found to be indispensable for the basolateral transport of MCP. This tetrapeptide has two unique features compared with the targeting motifs of other basolateral proteins: (i) it contains a phenylalanine rather than a tyrosine at position 1; (ii) it is located at the very COOH-terminal end. Replacement of the phenylalanine or the leucine by an alanine resulted in a nonpolarized delivery to the cell surface. On the other hand, substitution of a tyrosine for the phenylalanine did not affect the basolateral transport of MCP. The latter mutant, however, was efficiently internalized, whereas the wild type protein was not subject to endocytosis. Our results indicate that the targeting signal YXX-large aliphatic that is involved in various sorting events has been modulated in MCP in such a way that it allows basolateral transport but not endocytosis.

摘要

膜辅因子蛋白(MCP)是一种广泛分布的补体调节蛋白,在极化上皮细胞的基底外侧表面表达。通过在16个氨基酸的细胞质尾部产生缺失突变体和点突变体,分析了MCP的BC1亚型的基底外侧靶向。发现一段由四个氨基酸组成的序列FTSL对于MCP的基底外侧转运是必不可少的。与其他基底外侧蛋白的靶向基序相比,这个四肽有两个独特的特征:(i)在第1位含有苯丙氨酸而不是酪氨酸;(ii)它位于COOH末端。用丙氨酸取代苯丙氨酸或亮氨酸会导致细胞表面的非极化递送。另一方面,用酪氨酸取代苯丙氨酸并不影响MCP的基底外侧转运。然而,后一种突变体被有效地内化,而野生型蛋白不发生内吞作用。我们的结果表明,参与各种分选事件的靶向信号YXX-大脂肪族在MCP中以允许基底外侧转运但不允许内吞作用的方式进行了调节。

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