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Expression and potential clinical significance of urothelial cytodifferentiation markers in the exstrophic bladder

机译:尿路上皮细胞分化标记物在膀胱外表皮细胞中的表达及其潜在临床意义

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Purpose: We characterize the urothelium from patients with classic bladder exstrophy-epispadias complex for the expression of proteins associated with urothelial differentiation, and discuss a potential impact of urothelial phenotype on the structural and functional properties of the bladder template following bladder closure. Materials and Methods: From 2005 to 2010 bladder biopsies from 32 infants with bladder exstrophy-epispadias complex obtained at primary bladder closure were collected. After histological assessment immunochemistry was used to investigate the expression of uroplakin IIIa, cytokeratin differentiation restricted antigens CK13 and CK20, and tight junction protein claudin 4. Results: Overall tissue morphology showed gross alterations with inflammatory, proliferative and metaplastic changes in most specimens. Sections of intact epithelium were present in 78% of biopsies. With respect to urothelial phenotype, CK13 was expressed in all specimens, whereas UPIIIa and CK20 were absent in 76% of the tissues examined. Of the biopsies 52% revealed an irregular expression pattern of tight junction protein Cl-4. Conclusions: This is the first study to our knowledge to characterize the urothelium from infants with bladder exstrophy-epispadias complex for the expression of urothelial differentiation associated antigens. Our findings suggest urothelial differentiation changes in a majority of exstrophic bladders, at least at primary bladder closure. Although the underlying etiology remains to be established, abnormal urothelial differentiation may result in a dysfunctional urothelial barrier with implications for the structural and functional properties of the bladder template. Despite the study limitations, our preliminary findings provide a platform for further investigation of the significance of the urothelium for the exstrophic bladder.
机译:目的:我们表征患有经典膀胱外翻-上睑下垂复合体的患者的尿路上皮,表达与尿路上皮分化相关的蛋白质,并讨论膀胱关闭后尿路上皮表型对膀胱模板的结构和功能特性的潜在影响。材料和方法:从2005年至2010年,收集了32例在初次膀胱闭合时获得的患有膀胱萎缩症-上睑外翻复合物的婴儿的膀胱活检。经过组织学评估后,采用免疫化学方法研究了尿激酶素IIIa,细胞角蛋白分化受限抗原CK13和CK20以及紧密连接蛋白claudin 4的表达。 78%的活检组织中存在完整的上皮切片。关于尿路上皮表型,CK13在所有标本中表达,而UPIIIa和CK20在76%的被检组织中不存在。在活组织检查中,有52%显示紧密连接蛋白Cl-4的不规则表达模式。结论:这是我们所知的第一项研究,该研究旨在表征患有膀胱萎缩症-上肢膜炎复合体的婴儿的尿路上皮,表达尿路上皮分化相关抗原。我们的研究结果表明,至少在原发性膀胱关闭时,大多数外来膀胱的尿路上皮分化变化。尽管尚有待确定的病因,但异常的尿路上皮分化可能会导致功能异常的尿路上皮屏障,影响膀胱模板的结构和功能特性。尽管有研究局限性,我们的初步发现为进一步研究尿路上皮对外来膀胱的重要性提供了平台。

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