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KRas 通过可溶、捕获和囊泡运输的空间循环定位于质膜。

KRas localizes to the plasma membrane by spatial cycles of solubilization, trapping and vesicular transport.

机构信息

Department of Systemic Cell Biology, Max Planck Institute for Molecular Physiology, Otto-Hahn-Straße 11, 44227 Dortmund, Germany.

Department of Systemic Cell Biology, Max Planck Institute for Molecular Physiology, Otto-Hahn-Straße 11, 44227 Dortmund, Germany; Fakultät Chemie, Technische Universität Dortmund, Otto-Hahn-Straße 6, 44221 Dortmund, Germany.

出版信息

Cell. 2014 Apr 10;157(2):459-471. doi: 10.1016/j.cell.2014.02.051.

Abstract

KRas is a major proto-oncogene product whose signaling activity depends on its level of enrichment on the plasma membrane (PM). This PM localization relies on posttranslational prenylation for membrane affinity, while PM specificity has been attributed to electrostatic interactions between negatively charged phospholipids in the PM and basic amino-acids in the C terminus of KRas. By measuring kinetic parameters of KRas dynamics in living cells with a cellular-automata-based data-fitting approach in realistic cell-geometries, we show that charge-based specificity is not sufficient to generate PM enrichment in light of the total surface area of endomembranes. Instead, mislocalized KRas is continuously sequestered from endomembranes by cytosolic PDEδ to be unloaded in an Arl2-dependent manner to perinuclear membranes. Electrostatic interactions then trap KRas at the recycling endosome (RE), from where vesicular transport restores enrichment on the PM. This energy driven reaction-diffusion cycle explains how small molecule targeting of PDEδ affects the spatial organization of KRas.

摘要

KRas 是一种主要的原癌基因产物,其信号活性取决于其在质膜(PM)上的富集水平。这种 PM 定位依赖于翻译后对膜亲和力的 prenylation,而 PM 的特异性则归因于 PM 中带负电荷的磷脂和 KRas C 末端的碱性氨基酸之间的静电相互作用。通过在真实的细胞几何形状中使用基于细胞自动机的数据拟合方法来测量活细胞中 KRas 动力学的动力学参数,我们表明,鉴于内质网膜的总表面积,基于电荷的特异性不足以产生 PM 富集。相反,错误定位的 KRas 被胞质 PDEδ 连续隔离在内质网上,以 Arl2 依赖的方式卸载到核周膜。然后,静电相互作用将 KRas 捕获在再循环内体(RE)中,从那里囊泡运输将 KRas 重新富集到 PM 上。这种能量驱动的反应扩散循环解释了小分子靶向 PDEδ 如何影响 KRas 的空间组织。

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