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分泌型胶质母细胞瘤纳米囊泡含有以法尼基化依赖性方式整合的细胞内信号蛋白和活性Ras。

Secreted Glioblastoma Nanovesicles Contain Intracellular Signaling Proteins and Active Ras Incorporated in a Farnesylation-dependent Manner.

作者信息

Luhtala Natalie, Aslanian Aaron, Yates John R, Hunter Tony

机构信息

From the Molecular and Cell Biology Laboratory, Salk Institute for Biological Studies, La Jolla, California 92037 and.

the Department of Chemical Physiology, The Scripps Research Institute, La Jolla, California 92037.

出版信息

J Biol Chem. 2017 Jan 13;292(2):611-628. doi: 10.1074/jbc.M116.747618. Epub 2016 Dec 1.

Abstract

Glioblastomas (GBMs) are malignant brain tumors with a median survival of less than 18 months. Redundancy of signaling pathways represented within GBMs contributes to their therapeutic resistance. Exosomes are extracellular nanovesicles released from cells and present in human biofluids that represent a possible biomarker of tumor signaling state that could aid in personalized treatment. Herein, we demonstrate that mouse GBM cell-derived extracellular nanovesicles resembling exosomes from an H-RasV12 myr-Akt mouse model for GBM are enriched for intracellular signaling cascade proteins (GO: 0007242) and Ras protein signal transduction (GO: 0007265), and contain active Ras. Active Ras isolated from human and mouse GBM extracellular nanovesicles lysates using the Ras-binding domain of Raf also coprecipitates with ESCRT (endosomal sorting complex required for transport)-associated exosome proteins Vps4a and Alix. Although we initially hypothesized a role for active Ras protein signaling in exosome biogenesis, we found that GTP binding of K-Ras was dispensable for its packaging within extracellular nanovesicles and for the release of Alix. By contrast, farnesylation of K-Ras was required for its packaging within extracellular nanovesicles, yet expressing a K-Ras farnesylation mutant did not decrease the number of nanovesicles or the amount of Alix protein released per cell. Overall, these results emphasize the primary importance of membrane association in packaging of extracellular nanovesicle factors and indicate that screening nanovesicles within human fluids could provide insight into tissue origin and the wiring of signaling proteins at membranes to predict onset and behavior of cancer and other diseases linked to deregulated membrane signaling states.

摘要

胶质母细胞瘤(GBM)是恶性脑肿瘤,中位生存期不到18个月。GBM中存在的信号通路冗余导致其产生治疗抗性。外泌体是细胞释放的细胞外纳米囊泡,存在于人体生物流体中,代表肿瘤信号状态的一种可能生物标志物,有助于个性化治疗。在此,我们证明,来自H-RasV12 myr-Akt小鼠GBM模型的、类似外泌体的小鼠GBM细胞衍生的细胞外纳米囊泡富含细胞内信号级联蛋白(GO: 0007242)和Ras蛋白信号转导(GO: 0007265),并含有活性Ras。使用Raf的Ras结合结构域从人和小鼠GBM细胞外纳米囊泡裂解物中分离出的活性Ras也与ESCRT(转运所需的内体分选复合物)相关的外泌体蛋白Vps4a和Alix共沉淀。尽管我们最初假设活性Ras蛋白信号在外泌体生物发生中起作用,但我们发现K-Ras的GTP结合对于其在细胞外纳米囊泡中的包装以及Alix的释放是可有可无的。相比之下,K-Ras的法尼基化对于其在细胞外纳米囊泡中的包装是必需的,然而表达K-Ras法尼基化突变体并没有减少纳米囊泡的数量或每个细胞释放的Alix蛋白量。总体而言,这些结果强调了膜结合在细胞外纳米囊泡因子包装中的首要重要性,并表明在人体液体中筛选纳米囊泡可以深入了解组织起源以及膜上信号蛋白的连接方式,以预测癌症和其他与膜信号状态失调相关疾病的发生和行为。

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