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人肾祖细胞对肾小球足细胞的再生作用。

Regeneration of glomerular podocytes by human renal progenitors.

作者信息

Ronconi Elisa, Sagrinati Costanza, Angelotti Maria Lucia, Lazzeri Elena, Mazzinghi Benedetta, Ballerini Lara, Parente Eliana, Becherucci Francesca, Gacci Mauro, Carini Marco, Maggi Enrico, Serio Mario, Vannelli Gabriella Barbara, Lasagni Laura, Romagnani Sergio, Romagnani Paola

机构信息

Excellence Center for Research, Transfer and High Education Denothe, University of Florence, 50139, Firenze, Italy.

出版信息

J Am Soc Nephrol. 2009 Feb;20(2):322-32. doi: 10.1681/ASN.2008070709. Epub 2008 Dec 17.

Abstract

Depletion of podocytes, common to glomerular diseases in general, plays a role in the pathogenesis of glomerulosclerosis. Whether podocyte injury in adulthood can be repaired has not been established. Here, we demonstrate that in the adult human kidney, CD133+CD24+ cells consist of a hierarchical population of progenitors that are arranged in a precise sequence within Bowman's capsule and exhibit heterogeneous potential for differentiation and regeneration. Cells localized to the urinary pole that expressed CD133 and CD24, but not podocyte markers (CD133+CD24+PDX- cells), could regenerate both tubular cells and podocytes. In contrast, cells localized between the urinary pole and vascular pole that expressed both progenitor and podocytes markers (CD133+CD24+PDX+) could regenerate only podocytes. Finally, cells localized to the vascular pole did not exhibit progenitor markers, but displayed phenotypic features of differentiated podocytes (CD133-CD24-PDX+ cells). Injection of CD133+CD24+PDX- cells, but not CD133+CD24+PDX+ or CD133-CD24- cells, into mice with adriamycin-induced nephropathy reduced proteinuria and improved chronic glomerular damage, suggesting that CD133+CD24+PDX- cells could potentially treat glomerular disorders characterized by podocyte injury, proteinuria, and progressive glomerulosclerosis.

摘要

足细胞耗竭是一般肾小球疾病的共同特征,在肾小球硬化的发病机制中起作用。成年期足细胞损伤是否能够修复尚未明确。在此,我们证明,在成人肾脏中,CD133+CD24+细胞由一群分级排列的祖细胞组成,这些祖细胞在肾小囊内按精确顺序排列,并表现出分化和再生的异质性潜能。定位于尿极且表达CD133和CD24但不表达足细胞标志物(CD133+CD24+PDX-细胞)的细胞能够再生肾小管细胞和足细胞。相比之下,定位于尿极与血管极之间且同时表达祖细胞和足细胞标志物(CD133+CD24+PDX+)的细胞仅能再生足细胞。最后,定位于血管极的细胞不表现祖细胞标志物,但显示出分化足细胞的表型特征(CD133-CD24-PDX+细胞)。将CD133+CD24+PDX-细胞而非CD133+CD24+PDX+或CD133-CD24-细胞注射到阿霉素诱导的肾病小鼠体内,可降低蛋白尿并改善慢性肾小球损伤,这表明CD133+CD24+PDX-细胞可能潜在地治疗以足细胞损伤、蛋白尿和进行性肾小球硬化为特征地肾小球疾病。

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本文引用的文献

1
Stem-cell approaches for kidney repair: choosing the right cells.用于肾脏修复的干细胞方法:选择合适的细胞。
Trends Mol Med. 2008 Jul;14(7):277-85. doi: 10.1016/j.molmed.2008.05.005. Epub 2008 Jun 12.
5
CD133+ neural stem cells in the ependyma of mammalian postnatal forebrain.哺乳动物出生后前脑室管膜中的CD133 +神经干细胞。
Proc Natl Acad Sci U S A. 2008 Jan 22;105(3):1026-31. doi: 10.1073/pnas.0710000105. Epub 2008 Jan 14.
9
Mesenchymal stem cells in acute kidney injury.急性肾损伤中的间充质干细胞
Annu Rev Med. 2008;59:311-25. doi: 10.1146/annurev.med.59.061506.154239.
10
Immigrating progenitor cells contribute to human podocyte turnover.迁移的祖细胞有助于人类足细胞更新。
Kidney Int. 2007 Dec;72(12):1468-73. doi: 10.1038/sj.ki.5002524. Epub 2007 Sep 26.

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