Increased epithelial cell proliferation and abnormal extracellular matrix in rat polycystic kidney disease.

IF 9.4 1区医学 Q1 UROLOGY & NEPHROLOGY Journal of The American Society of Nephrology Pub Date : 1998-06-01 DOI:10.1681/ASN.V96937

K Ramasubbu, N Gretz, S Bachmann

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Abstract

Proliferation of renal tubular epithelial cells is considered a major factor leading to cyst formation in human polycystic kidney disease (PKD). The Han:SPRD rat model for inherited PKD permits a close scrutiny, especially for early stages of the disease, and shows numerous similarities to human autosomal dominant PKD (ADPKD). In this study, the exact in vivo proliferation rate in Han:SPRD rat kidneys was evaluated in a cell type-specific manner, using immunohistochemistry with antibody to proliferating cell nuclear antigen (PCNA). The proliferation index (PI; percentage of PCNA-positive cell nuclei) was determined in normal and cystically altered tissue, and a relationship between proliferative activity and alterations in extracellular matrix expression was established using in situ hybridization for collagen I and IV mRNA. Heterozygously affected rats (cy/+) showed strong increases of PI values in cystically altered nephron portions that were mostly derived from proximal tubule. Cell proliferation obviously preceded cyst formation, because early in the progression of the disease, the normal-appearing tubules from PKD kidneys had markedly increased PI values compared with healthy controls (14.1-fold in 3-mo-old rats and 11.9-fold in 12-mo-old rats; P < 0.05), whereas later stages revealed a more generalized cystic degeneration of the nephron, with increases in PI between 14- and 82-fold, depending on the respective category of cystic epithelia. In cysts with a distal phenotype, changes were less pronounced. No significant differences were encountered between the two age groups. Proliferation was also present in interstitial cells, whereas glomeruli were unchanged. Increases in epithelial and interstitial proliferation coincided with an overexpression of matrix compounds. For comparison, changes in homozygously affected rats (cy/cy) showed up to several hundred-fold elevated PI values. These results indicate that in the Han:SPRD model for ADPKD, cystic malformation of the nephron is preceded by and coincides with enhanced epithelial and interstitial cell proliferation. Altered cell-matrix interactions seem to be directly involved in the disruption of epithelial differentiation.

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大鼠多囊肾病中上皮细胞增殖增加和细胞外基质异常。

肾小管上皮细胞的增殖被认为是导致人类多囊肾病(PKD)囊肿形成的主要因素。遗传性PKD的Han:SPRD大鼠模型允许仔细检查，特别是在疾病的早期阶段，并显示出与人类常染色体显性PKD (ADPKD)的许多相似之处。本研究采用针对增殖细胞核抗原(PCNA)抗体的免疫组织化学方法，以细胞类型特异性的方式评估Han:SPRD大鼠肾脏的确切体内增殖率。增殖指数(PI;在正常组织和囊变组织中测定了pcna阳性细胞核的百分比，并利用胶原I和IV mRNA的原位杂交技术建立了增殖活性与细胞外基质表达改变之间的关系。杂合影响大鼠(cy/+)显示，主要来自近端肾小管的囊性改变部分的PI值明显升高。细胞增殖明显先于囊肿形成，因为在疾病进展的早期，来自PKD肾脏的正常小管的PI值与健康对照相比显着增加(3岁大鼠14.1倍，12岁大鼠11.9倍);P < 0.05)，而晚期显示更广泛的肾细胞囊性变性，PI增加14- 82倍，这取决于囊性上皮的不同类别。在远端表型的囊肿中，变化不太明显。两个年龄组之间没有明显差异。间质细胞也有增殖，而肾小球没有变化。上皮和间质增生的增加与基质化合物的过度表达一致。相比之下，纯合影响大鼠的变化(cy/cy)显示PI值升高了数百倍。这些结果表明，在Han:SPRD ADPKD模型中，肾单位囊性畸形发生之前，并与上皮细胞和间质细胞增殖增强相吻合。细胞-基质相互作用的改变似乎直接参与了上皮分化的破坏。

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来源期刊

Journal of The American Society of Nephrology 医学-泌尿学与肾脏学

CiteScore

22.40

自引率

2.90%

发文量

492

审稿时长

3-8 weeks

期刊介绍： The Journal of the American Society of Nephrology (JASN) stands as the preeminent kidney journal globally, offering an exceptional synthesis of cutting-edge basic research, clinical epidemiology, meta-analysis, and relevant editorial content. Representing a comprehensive resource, JASN encompasses clinical research, editorials distilling key findings, perspectives, and timely reviews. Editorials are skillfully crafted to elucidate the essential insights of the parent article, while JASN actively encourages the submission of Letters to the Editor discussing recently published articles. The reviews featured in JASN are consistently erudite and comprehensive, providing thorough coverage of respective fields. Since its inception in July 1990, JASN has been a monthly publication. JASN publishes original research reports and editorial content across a spectrum of basic and clinical science relevant to the broad discipline of nephrology. Topics covered include renal cell biology, developmental biology of the kidney, genetics of kidney disease, cell and transport physiology, hemodynamics and vascular regulation, mechanisms of blood pressure regulation, renal immunology, kidney pathology, pathophysiology of kidney diseases, nephrolithiasis, clinical nephrology (including dialysis and transplantation), and hypertension. Furthermore, articles addressing healthcare policy and care delivery issues relevant to nephrology are warmly welcomed.