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肿瘤干细胞在肿瘤细胞的自我更新、肿瘤的发生、耐药性和转移中扮演着重要角色。膀胱癌干细胞(Bladder Cancer Stem Cells,BCSCs)的起源和基因基础目前仍不甚明确。本研究对来源于3份膀胱癌标本的59个细胞进行了单细胞测序,其中包括膀胱癌干细胞(Bladder Cancer Stem Cells,BCSCs)、膀胱癌非干细胞(Bladder Cancer Non-Stem Cells,BCNSCs)、膀胱上皮干细胞(Bladder Epithelial Stem Cells,BESCs)和膀胱上皮非干细胞(Bladder Epithelial Non-Stem Cells,BENSCs)。通过进化分析发现BCSCs起始于BESCs或BCNSCs。对BCSCs中发生突变的21个关键基因进行了鉴定,发现了6个未在膀胱癌中报道过的基因(ETS1,GPRC5A,MKL1,PAWR, PITX2, RGS9BP)。ARID1A,GPRC5A和MLL2联合突变可显著增强BCNSCs的自我更新能力。这是首次通过单细胞测序描述了BCSCs的基因概况,并阐明了人类BCSCs的起源。
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Single-cell sequencing reveals variants in ARID1A, GPRC5A and MLL2 driving self-renewal of human bladder cancer stem cells.
Cancer stem cells are considered responsible for many important aspects of tumors such as their self-renewal, tumor-initiating, drug-resistance and metastasis. However, the genetic basis and origination of human bladder cancer stem cells (BCSCs) remains unknown. Here, we conducted single-cell sequencing on 59 cells including BCSCs, bladder cancer non-stem cells (BCNSCs), bladder epithelial stem cells (BESCs) and bladder epithelial non-stem cells (BENSCs) from three bladder cancer (BC) specimens. Specifically, BCSCs demonstrate clonal homogeneity and suggest their origin from BESCs or BCNSCs through phylogenetic analysis. Moreover, 21 key altered genes were identified in BCSCs including six genes not previously described in BC (ETS1, GPRC5A, MKL1, PAWR, PITX2 and RGS9BP). Co-mutations of ARID1A, GPRC5A and MLL2 introduced by CRISPR/Cas9 significantly enhance the capabilities of self-renewal and tumor-initiating of BCNSCs. To our knowledge, our study first provides an overview of the genetic basis of human BCSCs with single-cell sequencing and demonstrates the biclonal origin of human BCSCs via evolution analysis.
PATIENT SUMMARY:Human bladder cancer stem cells show the high level of consistency and may derived from bladder epithelial stem cells or bladder cancer non-stem cells. Mutations of ARID1A, GPRC5A and MLL2 grant bladder cancer non-stem cells the capability of self-renewal.
Copyright © 2016 European Association of Urology. Published by Elsevier B.V. All rights reserved.
bladder cancer; bladder cancer stem cells; genetic alteration; self-renewal; single-cell sequencing; tumor evolution
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