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细胞内分拣的小肽识别序列。

Small peptide recognition sequence for intracellular sorting.

机构信息

Department of Physiology, Tulane University Health Sciences Center, School of Medicine, New Orleans, LA 70112, USA.

出版信息

Curr Opin Biotechnol. 2010 Oct;21(5):611-20. doi: 10.1016/j.copbio.2010.08.007.

Abstract

Increasing evidence indicate that complex arrays of short signals and recognition peptide sequence ensure accurate trafficking and distribution of transmembrane receptors and/or proteins and their ligands into intracellular compartments. Internalization and subsequent trafficking of cell-surface receptors into the cell interior is mediated by specific short-sequence peptide signals within the cytoplasmic domains of these receptor proteins. The short signals usually consist of small linear amino acid sequences, which are recognized by adaptor coat proteins along the endocytic and sorting pathways. In recent years, much has been learned about the function and mechanisms of endocytic pathways responsible for the trafficking and molecular sorting of membrane receptors and their ligands into intracellular compartments, however, the significance and scope of the short-sequence motifs in these cellular events is not well understood. Here a particular emphasis has been given to the functions of short-sequence signal motifs responsible for the itinerary and destination of membrane receptors and proteins moving into subcellular compartments.

摘要

越来越多的证据表明,复杂的短信号和识别肽序列阵列可确保跨膜受体和/或蛋白质及其配体准确地运输和分布到细胞内隔室中。细胞表面受体通过这些受体蛋白细胞质结构域内的特定短序列肽信号被内化并随后运输到细胞内部。这些短信号通常由小的线性氨基酸序列组成,这些序列被沿着内吞和分拣途径的衔接蛋白外壳蛋白识别。近年来,人们对负责膜受体及其配体运输和分子分拣到细胞内隔室的内吞途径的功能和机制有了更多的了解,然而,这些细胞事件中短序列基序的意义和范围尚不清楚。这里特别强调了负责进入亚细胞隔室的膜受体和蛋白质移动的行程和目的地的短序列信号基序的功能。

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