肾小管再生:肾脏何时能从损伤中再生,是什么使失败变为成功?

Nephron Experimental Nephrology Pub Date : 2014-01-01 Epub Date: 2014-05-19 DOI:10.1159/000360671
Martin E Johansson
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This is at odds with other epithelia such as those of the skin and intestine, where stem cells maintain a continuous flow of new cells from designated niches.</p><p><strong>Summary: </strong>This review discusses the classical concept of renal regeneration, i.e. stochastically surviving cells undergoing dedifferentiation (or epithelial-mesenchymal transition) followed by replenishment of the tubular epithelium. Furthermore however, this view has recently been challenged by the concept of organ-confined stem/progenitor cells, bone marrow-derived stem cells, or mesenchymal stem cells taking part in the regenerative events. Whereas results from animal models support the classical view, morphologically distinct cells have been demonstrated in human kidneys, requiring interpretation. 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引用次数: 6

摘要

背景:急性肾损伤/肾功能衰竭最常见的肾内原因是肾小管损伤。肾小管被排列成细胞嵌合体的隔间来执行它们的功能,在休息时,人体几乎五分之一的ATP消耗被分配给从滤液中重新吸收物质,特别是近端小管对氧气和/或营养剥夺高度敏感。正常情况下,小管上皮在有丝分裂时处于静止状态,如果给予支持性护理,则损伤后小管上皮表现出活跃的再生反应,从而允许功能恢复。尽管如此,再生能力背后的细胞机制仍然没有明确的定义。这与皮肤和肠等其他上皮细胞不同,在这些细胞中,干细胞保持来自指定壁龛的新细胞的连续流动。摘要:本文讨论了肾再生的经典概念,即随机存活的细胞经历去分化(或上皮-间质转化),然后再补充小管上皮。然而,这一观点最近受到器官限制的干细胞/祖细胞、骨髓来源的干细胞或间充质干细胞参与再生事件的概念的挑战。尽管动物模型的结果支持经典观点,但在人类肾脏中已证实存在形态不同的细胞,这需要进一步解释。这篇综述介绍了一些以前的工作和技术,并强调了需要协调的问题。关键信息:在成年人中,肾小管含有分散的细胞,这些细胞具有独特的标记物和特性,例如在肾小管损伤期间增强的稳健性。这些细胞可能是由损伤引起的,也可能是常驻的祖细胞池。迄今为止,使用谱系追踪方法的动物研究支持归纳情景。在人类中,情况就不太清楚了,人们可能会推测细胞的异质性可能反映了细胞重编程到类似祖细胞状态的要素,可能是通过诱导。然而,由于密集的调查工作,可能很快就会达成科学共识,这将有利于进一步的研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Tubular regeneration: when can the kidney regenerate from injury and what turns failure into success?

Background: The most common intrarenal cause for acute kidney injury/renal failure is tubular damage. The kidney tubules are arranged as compartments of cellular mosaics to perform their functions, and at rest almost a fifth of the human ATP consumption is allotted to the reabsorption of substances from the filtrate, rendering especially the proximal tubules highly sensitive to oxygen and/or nutrient deprivation. Normally mitotically quiescent, the tubular epithelium shows a brisk regenerative response following injury if supportive care is offered, allowing functional restoration. Despite this, the cellular machinery behind the regenerative capacity is still not unequivocally defined. This is at odds with other epithelia such as those of the skin and intestine, where stem cells maintain a continuous flow of new cells from designated niches.

Summary: This review discusses the classical concept of renal regeneration, i.e. stochastically surviving cells undergoing dedifferentiation (or epithelial-mesenchymal transition) followed by replenishment of the tubular epithelium. Furthermore however, this view has recently been challenged by the concept of organ-confined stem/progenitor cells, bone marrow-derived stem cells, or mesenchymal stem cells taking part in the regenerative events. Whereas results from animal models support the classical view, morphologically distinct cells have been demonstrated in human kidneys, requiring interpretation. This review presents some of the previous work and techniques and highlights issues that need to be reconciled.

Key messages: In adult humans, the kidney tubules contain scattered cells with a distinct set of markers and properties, such as increased robustness during tubular damage. These cells may be induced by injury or represent a resident progenitor cell pool. To date, animal studies using lineage-tracing methods argue for an inductive scenario. In humans, the situation is less clear and one might speculate that the cellular heterogeneity might reflect elements of cellular reprogramming to a progenitor-like state, perhaps by induction. Due to intense investigational efforts, however, a scientific consensus may soon be reached, which will benefit further research.

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Nephron Experimental Nephrology
Nephron Experimental Nephrology 医学-泌尿学与肾脏学
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