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跨膜表面糖蛋白内化的酪氨酸识别信号的特征

Characteristics of the tyrosine recognition signal for internalization of transmembrane surface glycoproteins.

作者信息

Ktistakis N T, Thomas D, Roth M G

机构信息

Department of Biochemistry, University of Texas Southwestern Medical Center, Dallas 72935-9038.

出版信息

J Cell Biol. 1990 Oct;111(4):1393-407. doi: 10.1083/jcb.111.4.1393.

Abstract

A tyrosine residue in the cytoplasmic domain of a class of cell surface receptors is necessary, but not sufficient, for internalization through coated pits. To identify the amino acid context enabling a tyrosine to serve as a signal for endocytosis, we mutated the short cytoplasmic domain of a mutant influenza virus hemagglutinin that is competent for internalization, HA-Y543, and determined the effect of each change on internalization. From these results and a comparison of sequences of other proteins recognized by coated pits, a "tyrosine internalization signal" was proposed. Site-directed mutagenesis was employed to insert complete, or incomplete "tyrosine internalization signals" into the cytoplasmic domain of a protein normally not endocytosed, human glycophorin A. Only the complete signal caused internalization of mutant glycophorins by coated pits. The signal is formed by a short amino acid sequence, with polar or basic residues preferred at certain positions on either side of the tyrosine. Amino acids, which in proteins of known structure are frequently found in turns, are clustered near the tyrosine on the side of the signal nearest the transmembrane domain.

摘要

一类细胞表面受体胞质结构域中的酪氨酸残基对于通过被膜小窝进行内化是必要的,但并非充分条件。为了确定能使酪氨酸作为内吞信号的氨基酸环境,我们对一种有内化能力的突变型流感病毒血凝素HA-Y543的短胞质结构域进行了突变,并确定了每种变化对内化的影响。根据这些结果以及对其他被膜小窝识别的蛋白质序列的比较,提出了一个“酪氨酸内化信号”。采用定点诱变将完整或不完整的“酪氨酸内化信号”插入到一种通常不被内吞的蛋白质——人血型糖蛋白A的胞质结构域中。只有完整的信号才能使突变型血型糖蛋白通过被膜小窝进行内化。该信号由一段短的氨基酸序列构成,在酪氨酸两侧的特定位置上,极性或碱性残基更为可取。在已知结构的蛋白质中经常呈转角形式的氨基酸,聚集在信号中靠近跨膜结构域一侧的酪氨酸附近。

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