Fibrosis in the kidney: is a problem shared a problem halved?

Fibrogenesis & Tissue Repair Pub Date : 2012-06-06 eCollection Date: 2012-01-01 DOI:10.1186/1755-1536-5-S1-S14
Tim D Hewitson
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引用次数: 71

Abstract

Fibrotic disorders are commonplace, take many forms and can be life-threatening. No better example of this exists than the progressive fibrosis that accompanies all chronic renal disease. Renal fibrosis is a direct consequence of the kidney's limited capacity to regenerate after injury. Renal scarring results in a progressive loss of renal function, ultimately leading to end-stage renal failure and a requirement for dialysis or kidney transplantation. Although it manifests itself histologically as an increase in extracellular matrix, we know that the histological appearance can be caused by a de novo synthesis of matrix (primarily collagen), or a disproportionate loss of renal parenchyma. In both cases the process depends on a resident mesenchymal cell, the so-called myofibroblast, and is independent of disease etiology. Potentially we can ameliorate fibrosis, either indirectly by modifying the environment the kidney functions in, or more directly by interfering with activation and function of myofibroblasts. However, while renal fibrosis shares many features in common with the wound healing response in other organs, we also recognise that the consequences can be highly kidney specific. This review highlights the similarities and differences between this process in the kidney and other organs, and considers the therapeutic implications.

Abstract Image

肾脏纤维化:一个共同的问题是一个减半的问题吗?
纤维化疾病很常见,有多种形式,可能危及生命。没有比所有慢性肾脏疾病所伴随的进行性纤维化更好的例子了。肾纤维化是损伤后肾脏再生能力有限的直接后果。肾瘢痕形成导致肾功能逐渐丧失,最终导致终末期肾功能衰竭,需要透析或肾移植。虽然它在组织学上表现为细胞外基质的增加,但我们知道组织学上的表现可能是由基质(主要是胶原蛋白)的重新合成或肾实质不成比例的损失引起的。在这两种情况下,这一过程都依赖于一种常驻间充质细胞,即所谓的肌成纤维细胞,与疾病病因无关。我们有可能通过间接地改变肾脏功能的环境,或者更直接地通过干扰肌成纤维细胞的激活和功能来改善纤维化。然而,尽管肾纤维化与其他器官的伤口愈合反应有许多共同的特征,但我们也认识到其后果可能是高度肾脏特异性的。这篇综述强调了肾脏和其他器官中这一过程的异同,并考虑了其治疗意义。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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