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膜联蛋白对Ca2+依赖性磷脂结合、囊泡聚集和膜融合的特性研究

Characterization of Ca2(+)-dependent phospholipid binding, vesicle aggregation and membrane fusion by annexins.

作者信息

Blackwood R A, Ernst J D

机构信息

Department of Pediatrics, San Francisco General Hospital, University of California 94143-0868.

出版信息

Biochem J. 1990 Feb 15;266(1):195-200. doi: 10.1042/bj2660195.

Abstract

The annexins are a family of structurally similar, Ca2(+)-dependent, phospholipid-binding proteins. We compared six members of this family (calpactin I heavy chain, lipocortins I and III, endonexin II, p68 and protein II) to determine their phospholipid-binding specificities, as well as their ability to promote aggregation and fusion of phospholipid vesicles. The Ca2+ requirement for all of the proteins was lowest for binding to vesicles composed of phosphatidic acid, followed by phosphatidylserine and then phosphatidylinositol. Only protein II, p68, lipocortin III and endonexin II bound to vesicles composed of phosphatidylethanolamine, and none bound to phosphatidylcholine. Both calpactin I heavy chain and lipocortin I promoted aggregation of phosphatidylserine- or phosphatidylinositol-containing vesicles in the presence of less than 10 microM-Ca2+. Lipocortin I promoted fusion of liposome membranes by lowering threshold Ca2+ concentrations. Although calpactin I heavy chain did not affect threshold Ca2+ concentrations, it did increase the rate and extent of spontaneous fusion. In contrast, p68 inhibited fusion at threshold Ca2+ concentrations. Whereas previous reports have emphasized properties that the annexins have in common, these findings reveal quantitative and qualitative differences among the annexins which may relate to distinct intracellular functions.

摘要

膜联蛋白是一类结构相似、依赖Ca2+的磷脂结合蛋白家族。我们比较了该家族的六个成员(钙结合蛋白I重链、脂皮质蛋白I和III、内毒素II、p68和蛋白II),以确定它们的磷脂结合特异性,以及促进磷脂囊泡聚集和融合的能力。所有蛋白质结合由磷脂酸组成的囊泡时对Ca2+的需求最低,其次是磷脂酰丝氨酸,然后是磷脂酰肌醇。只有蛋白II、p68、脂皮质蛋白III和内毒素II能结合由磷脂酰乙醇胺组成的囊泡,而没有一个能结合磷脂酰胆碱。在Ca2+浓度低于10μM时,钙结合蛋白I重链和脂皮质蛋白I都能促进含磷脂酰丝氨酸或磷脂酰肌醇的囊泡聚集。脂皮质蛋白I通过降低阈值Ca2+浓度促进脂质体膜的融合。虽然钙结合蛋白I重链不影响阈值Ca2+浓度,但它确实增加了自发融合速率和程度。相比之下,p68在阈值Ca2+浓度下抑制融合。尽管先前的报道强调了膜联蛋白的共同特性,但这些发现揭示了膜联蛋白之间的定量和定性差异,这可能与不同的细胞内功能有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f0fb/1131114/03add80f8d3a/biochemj00189-0196-a.jpg

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