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从人肾小球系膜细胞诱导生成多能干细胞。

Generation of induced pluripotent stem cells from human kidney mesangial cells.

机构信息

Monash Immunology and Stem Cell Laboratories (MISCL), Monash University, Building 75, West Ring Road, Clayton Victoria 3800, Australia.

出版信息

J Am Soc Nephrol. 2011 Jul;22(7):1213-20. doi: 10.1681/ASN.2010101022. Epub 2011 May 12.

Abstract

Glomerular injury and podocyte loss leads to secondary tubulointerstitial damage and the development of fibrosis. The possibility of genetically reprogramming adult cells, termed induced pluripotent stem cells (iPS), may pave the way for patient-specific stem-cell-based therapies. Here, we reprogrammed normal human mesangial cells to pluripotency by retroviral transduction using defined factors (OCT4, SOX2, KLF4 and c-Myc). The kidney iPS (kiPS) cells resembled human embryonic stem-cell-like colonies in morphology and gene expression: They were alkaline phosphatase-positive; expressed OCT3/4, TRA-1 to 60 and TRA-1 to 81 proteins; and showed downregulation of mesangial cell markers. Quantitative (qPCR) showed that kiPS cells expressed genes analogous to embryonic stem cells and exhibited silencing of the retroviral transgenes by the fourth passage of differentiation. Furthermore, kiPS cells formed embryoid bodies and expressed markers of all three germ layers. The injection of undifferentiated kiPS colonies into immunodeficient mice formed teratomas, thereby demonstrating pluripotency. These results suggest that reprogrammed kidney induced pluripotent stem cells may aid the study of genetic kidney diseases and lead to the development of novel therapies.

摘要

肾小球损伤和足细胞丢失导致继发性肾小管间质损伤和纤维化的发展。重编程成体细胞,即诱导多能干细胞(iPS)的可能性,为基于患者特异性干细胞的治疗方法铺平了道路。在这里,我们通过使用定义因子(OCT4、SOX2、KLF4 和 c-Myc)的逆转录病毒转导将正常的人类系膜细胞重编程为多能性。肾 iPS(kiPS)细胞在形态和基因表达上类似于人类胚胎干细胞样集落:它们呈碱性磷酸酶阳性;表达 OCT3/4、TRA-1 至 60 和 TRA-1 至 81 蛋白;并且表现出系膜细胞标志物的下调。定量(qPCR)显示 kiPS 细胞表达类似于胚胎干细胞的基因,并在分化的第四代通过沉默逆转录病毒转基因。此外,kiPS 细胞形成类胚体并表达所有三个胚层的标记物。未分化的 kiPS 集落的注射到免疫缺陷小鼠中形成畸胎瘤,从而证明了多能性。这些结果表明,重编程的肾脏诱导多能干细胞可能有助于研究遗传肾脏疾病并导致新疗法的发展。

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