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人类肾脏远端肾小管上皮的预处理先于肾钙质沉着症。

Preconditioning of the distal tubular epithelium of the human kidney precedes nephrocalcinosis.

作者信息

Verhulst Anja, Asselman Marino, De Naeyer Stephanie, Vervaet Benjamin A, Mengel Michael, Gwinner Wilfried, D'Haese Patrick C, Verkoelen Carl F, De Broe Marc E

机构信息

Department of Nephrology-Hypertension, University of Antwerp, Belgium.

出版信息

Kidney Int. 2005 Oct;68(4):1643-7. doi: 10.1111/j.1523-1755.2005.00584.x.

Abstract

BACKGROUND

Preterm neonates and renal transplant patients frequently develop nephrocalcinosis. Experimental studies revealed that crystal retention in the distal nephron, a process that may lead to nephrocalcinosis, is limited to proliferating/regenerating tubular cells expressing hyaluronan and osteopontin at their luminal surface. Fetal and transplant kidneys contain proliferating and/or regenerating cells since nephrogenesis is not completed until 36 weeks of gestation, while ischemia and nephrotoxic immunosuppressants may lead to injury and repair in renal transplants. This prompted us to investigate the expression of hyaluronan and osteopontin and to correlate this to the appearance of tubular calcifications both in fetal/preterm and transplanted kidneys.

METHODS

Sections of fetal/preterm kidneys and protocol biopsies of transplanted kidneys (12 and 24 weeks posttransplantation from the same patients) were stained for osteopontin, hyaluronan, and calcifications (von Kossa).

RESULTS

Hyaluronan and osteopontin were expressed at the luminal surface of the epithelial cells lining the distal tubules of all fetal kidneys at birth and in all kidney graft protocol biopsies 12 and 24 weeks posttransplantation. In 7 out of 18 surviving (at least 4 days) preterm neonates crystal retention developed. In renal allografts a striking increase (from 2/10 to 6/10) in tubular crystal retention between 12 and 24 weeks posttransplantation was observed. In addition, crystals were selectively retained in distal renal tubules containing cells with hyaluronan and osteopontin at their luminal surface.

CONCLUSION

The results of this study show that luminal expression of hyaluronan and osteopontin preceded renal distal tubular retention of crystals in preterm neonates and renal transplant patients. We propose that the presence of this crystal binding phenotype may play a general role in renal calcification processes.

摘要

背景

早产儿和肾移植患者经常发生肾钙质沉着症。实验研究表明,远端肾单位中的晶体潴留是一个可能导致肾钙质沉着症的过程,该过程仅限于在管腔表面表达透明质酸和骨桥蛋白的增殖/再生肾小管细胞。胎儿和移植肾中含有增殖和/或再生细胞,因为肾发生直到妊娠36周才完成,而缺血和肾毒性免疫抑制剂可能导致肾移植中的损伤和修复。这促使我们研究透明质酸和骨桥蛋白的表达,并将其与胎儿/早产儿和移植肾中肾小管钙化的出现相关联。

方法

对胎儿/早产儿肾脏切片以及移植肾的方案活检标本(来自同一患者移植后12周和24周)进行骨桥蛋白、透明质酸和钙化(冯·科萨染色)染色。

结果

出生时所有胎儿肾脏的远端肾小管内衬上皮细胞的管腔表面以及移植后12周和24周的所有肾移植方案活检标本中均表达透明质酸和骨桥蛋白。18例存活(至少4天)的早产儿中有7例发生了晶体潴留。在同种异体肾移植中,观察到移植后12周和24周之间肾小管晶体潴留显著增加(从2/10增至6/10)。此外,晶体选择性地潴留于管腔表面含有透明质酸和骨桥蛋白的远端肾小管中。

结论

本研究结果表明,透明质酸和骨桥蛋白的管腔表达先于早产儿和肾移植患者肾脏远端肾小管晶体潴留。我们认为这种晶体结合表型的存在可能在肾钙化过程中起普遍作用。

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