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内体上 KRas 的动力学:酸性磷脂参与其结合。

Dynamics of KRas on endosomes: involvement of acidic phospholipids in its association.

机构信息

Departament de Biologia Cel·lular, Immunologia i Neurociències, Facultat de Medicina, Institut d'Investigacions Biomèdiques August Pi i Sunyer (IDIBAPS), and.

Unitat de Microscopia Òptica Avançada, Facultat de Medicina, Centres Científics i Tecnològics, Universitat de Barcelona, Barcelona, Spain;

出版信息

FASEB J. 2014 Jul;28(7):3023-37. doi: 10.1096/fj.13-241158. Epub 2014 Apr 9.

DOI:10.1096/fj.13-241158
PMID:24719356
Abstract

The endocytic compartment is emerging as a functional platform for controlling important cellular processes. We have found that ∼10 to 15% of total KRas, a protein that is frequently mutated in cancer, is present on endosomes, independent of its activation state. The dynamics of GFP-KRas wild-type (WT) and constitutively active or inactive mutants on endosomes were analyzed by fluorescence recovery after photobleaching (FRAP) microscopy. The measurements revealed an extraordinarily fast recovery of KRas WT [half-time (HT), ∼1.3 s] compared to HRas, Rab5, and EGFR, with the active KRasG12V mutant being significantly faster and more mobile (HT, ∼1 s, and ∼82% of exchangeable fraction) than the inactive KRasS17N (HT, ∼1.6 s, and ∼60% of exchangeable fraction). KRas rapidly switches from the cytoplasm to the endosomal membranes by an electrostatic interaction between its polybasic region and the endosomal acidic phospholipids, mainly phosphatidylserine.-Gelabert-Baldrich, M., Soriano-Castell, D., Calvo, M., Lu, A., Viña-Vilaseca, A., Rentero, C., Pol, A., Grinstein, S. Enrich, C., Tebar, F. Dynamics of KRas on endosomes: involvement of acidic phospholipids in its association.

摘要

内吞小体正在成为控制重要细胞过程的功能平台。我们发现,在癌症中经常发生突变的蛋白质 KRas 的约 10%到 15%存在于内体上,而与 KRas 的激活状态无关。通过荧光恢复后荧光漂白(FRAP)显微镜分析 GFP-KRas 野生型(WT)和组成型激活或失活突变体在内体上的动力学。测量结果显示,KRas WT 的恢复速度非常快[半衰期(HT),约 1.3 秒],与 HRas、Rab5 和 EGFR 相比,而活性 KRasG12V 突变体的恢复速度更快,流动性更高(HT,约 1 秒,可交换分数的 82%),而失活的 KRasS17N(HT,约 1.6 秒,可交换分数的 60%)。KRas 通过其多碱性区域与内体酸性磷脂(主要是磷脂酰丝氨酸)之间的静电相互作用,快速从细胞质转移到内体膜。-Gelabert-Baldrich,M.,Soriano-Castell,D.,Calvo,M.,Lu,A.,Viña-Vilaseca,A.,Rentero,C.,Pol,A.,Grinstein,S.,Enrich,C.,Tebar,F.内体上 KRas 的动力学:酸性磷脂在其结合中的作用。

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