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Pax2基因剂量降低会增加细胞凋亡并减缓肾囊性疾病的进展。

Reduced Pax2 gene dosage increases apoptosis and slows the progression of renal cystic disease.

作者信息

Ostrom L, Tang M J, Gruss P, Dressler G R

机构信息

Department of Pathology, University of Michigan, Ann Arbor, Michigan, 48109, USA.

出版信息

Dev Biol. 2000 Mar 15;219(2):250-8. doi: 10.1006/dbio.2000.9618.

Abstract

The murine cpk mouse develops a rapid-onset polycystic kidney disease (PKD) with many similarities to human PKD. During kidney development, the transcription factor Pax2 is required for the specification and differentiation of the renal epithelium. In humans, Pax2 is also expressed in juvenile cystic kidneys where it correlates with cell proliferation. In this report, Pax2 expression is demonstrated in the cystic epithelium of the mouse cpk kidneys. To assess the role of Pax2 during the development of polycystic kidney disease, the progression of renal cysts was examined in cpk mutants carrying one or two alleles of Pax2. Reduced Pax2 gene dosage resulted in a significant inhibition of renal cyst growth while maintaining more normal renal structures. The inhibition of cyst growth was not due to reduced proliferation of the cystic epithelium, rather to increased cell death in the Pax2 heterozygotes. Increased apoptosis with reduced Pax2 gene dosage was also observed in normal developing kidneys. Thus, increased cell death is an integral part of the Pax2 heterozygous phenotype and may be the underlying cause of Pax gene haploinsufficiency. That the cystic epithelium requires Pax2 for continued expansion underscores the embryonic nature of the renal cystic cells and may provide new insights toward growth suppression strategies.

摘要

小鼠cpk模型会快速发展出一种多囊肾病(PKD),与人类PKD有许多相似之处。在肾脏发育过程中,转录因子Pax2对于肾上皮细胞的特化和分化是必需的。在人类中,Pax2也在青少年囊性肾中表达,且与细胞增殖相关。在本报告中,Pax2在小鼠cpk肾的囊性上皮中表达。为了评估Pax2在多囊肾病发展过程中的作用,研究了携带一个或两个Pax2等位基因的cpk突变体中肾囊肿的进展情况。Pax2基因剂量的减少导致肾囊肿生长显著受到抑制,同时维持了更正常的肾脏结构。囊肿生长的抑制并非由于囊性上皮细胞增殖减少,而是由于Pax2杂合子中细胞死亡增加。在正常发育的肾脏中也观察到随着Pax2基因剂量减少凋亡增加。因此,细胞死亡增加是Pax2杂合子表型的一个组成部分,可能是Pax基因单倍剂量不足的潜在原因。囊性上皮细胞需要Pax2来持续扩张,这突出了肾囊性细胞的胚胎性质,并可能为生长抑制策略提供新的见解。

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