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肾侧群细胞显示出多谱系分化潜能和肾功能能力,但也存在细胞异质性。

Kidney side population reveals multilineage potential and renal functional capacity but also cellular heterogeneity.

作者信息

Challen Grant A, Bertoncello Ivan, Deane James A, Ricardo Sharon D, Little Melissa H

机构信息

Institute for Molecular Bioscience, The University of Queensland, Brisbane, Queensland, QLD, 4072, Australia.

出版信息

J Am Soc Nephrol. 2006 Jul;17(7):1896-912. doi: 10.1681/ASN.2005111228. Epub 2006 May 17.

DOI:10.1681/ASN.2005111228
PMID:16707564
Abstract

Side population (SP) cells in the adult kidney are proposed to represent a progenitor population. However, the size, origin, phenotype, and potential of the kidney SP has been controversial. In this study, the SP fraction of embryonic and adult kidneys represented 0.1 to 0.2% of the total viable cell population. The immunophenotype and the expression profile of kidney SP cells was distinct from that of bone marrow SP cells, suggesting that they are a resident nonhematopoietic cell population. Affymetrix expression profiling implicated a role for Notch signaling in kidney SP cells and was used to identify markers of kidney SP. Localization by in situ hybridization confirmed a primarily proximal tubule location, supporting the existence of a tubular "niche," but also revealed considerable heterogeneity, including the presence of renal macrophages. Adult kidney SP cells demonstrated multilineage differentiation in vitro, whereas microinjection into mouse metanephroi showed that SP cells had a 3.5- to 13-fold greater potential to contribute to developing kidney than non-SP main population cells. However, although reintroduction of SP cells into an Adriamycin-nephropathy model reduced albuminuria:creatinine ratios, this was without significant tubular integration, suggesting a humoral role for SP cells in renal repair. The heterogeneity of the renal SP highlights the need for further fractionation to distinguish the cellular subpopulations that are responsible for the observed multilineage capacity and transdifferentiative and humoral activities.

摘要

成年肾脏中的侧群(SP)细胞被认为代表祖细胞群体。然而,肾脏SP细胞的大小、起源、表型和潜能一直存在争议。在本研究中,胚胎和成年肾脏的SP细胞比例占总活细胞群体的0.1%至0.2%。肾脏SP细胞的免疫表型和表达谱与骨髓SP细胞不同,表明它们是驻留的非造血细胞群体。Affymetrix表达谱分析表明Notch信号通路在肾脏SP细胞中发挥作用,并用于鉴定肾脏SP细胞的标志物。原位杂交定位证实主要位于近端小管,支持管状“生态位”的存在,但也显示出相当大的异质性,包括肾巨噬细胞的存在。成年肾脏SP细胞在体外表现出多谱系分化,而显微注射到小鼠后肾中显示SP细胞比非SP主要群体细胞对发育中肾脏的贡献潜力大3.5至13倍。然而,尽管将SP细胞重新引入阿霉素肾病模型可降低蛋白尿:肌酐比值,但这并未伴有明显的管状整合,提示SP细胞在肾脏修复中起体液作用。肾脏SP细胞的异质性突出了进一步分级分离的必要性,以区分负责观察到的多谱系能力、转分化和体液活性的细胞亚群。

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