Neoplastic Reprogramming of Patient-Derived Adipose Stem Cells by Prostate Cancer Cell-Associated Exosomes

生物 癌症研究 微泡 肿瘤转化 重编程 间充质干细胞 癌症干细胞 干细胞 前列腺癌 癌变 细胞瘤 肿瘤微环境 癌症 细胞 病理 细胞生物学 小RNA 医学 遗传学 基因 肿瘤细胞
作者
Zakaria Y. Abd Elmageed,Yijun Yang,Raju Thomas,Manish Ranjan,Debasis Mondal,Krzysztof Moroz,Zhide Fang,Bashir M. Rezk,Krishnarao Moparty,Suresh C. Sikka,Oliver Sartor,Asim B. Abdel‐Mageed
出处
期刊:Stem Cells [Oxford University Press]
卷期号:32 (4): 983-997 被引量:295
标识
DOI:10.1002/stem.1619
摘要

Abstract Emerging evidence suggests that mesenchymal stem cells (MSCs) are often recruited to tumor sites but their functional significance in tumor growth and disease progression remains elusive. Herein we report that prostate cancer (PC) cell microenvironment subverts PC patient adipose-derived stem cells (pASCs) to undergo neoplastic transformation. Unlike normal ASCs, the pASCs primed with PC cell conditioned media (CM) formed prostate-like neoplastic lesions in vivo and reproduced aggressive tumors in secondary recipients. The pASC tumors acquired cytogenetic aberrations and mesenchymal-to-epithelial transition and expressed epithelial, neoplastic, and vasculogenic markers reminiscent of molecular features of PC tumor xenografts. Our mechanistic studies revealed that PC cell-derived exosomes are sufficient to recapitulate formation of prostate tumorigenic mimicry generated by CM-primed pASCs in vivo. In addition to downregulation of the large tumor suppressor homolog2 and the programmed cell death protein 4, a neoplastic transformation inhibitor, the tumorigenic reprogramming of pASCs was associated with trafficking by PC cell-derived exosomes of oncogenic factors, including H-ras and K-ras transcripts, oncomiRNAs miR-125b, miR-130b, and miR-155 as well as the Ras superfamily of GTPases Rab1a, Rab1b, and Rab11a. Our findings implicate a new role for PC cell-derived exosomes in clonal expansion of tumors through neoplastic reprogramming of tumor tropic ASCs in cancer patients. Stem Cells 2014;32:983–997
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