62例儿童Alport综合征临床和病理特点  被引量：4

作　　者：尹晓玲[1] 周艳梅[1] 邹敏书[1] 王嘉[1] 刘桐林[1] 唐锦辉[1] 仇丽茹[1] 陈瑜[1] 袁惠卿[1] 周建华[1] 

机构地区：[1]华中科技大学同济医学院附属同济医院儿科,湖北武汉430032

出　　处：《临床儿科杂志》2013年第12期1125-1128,共4页Journal of Clinical Pediatrics

基　　金：国家自然科学基金资助项目(No.81070557)

摘　　要：目的：了解儿童Alport综合征临床和病理特点。方法回顾性分析1989年3月到2012年6月住院并明确诊断为Alport综合征62例患儿的临床及病理资料。结果 X连锁Alport综合征（XL-AS）58例，常染色体隐性遗传Alport综合征（AR-AS）4例。在XL-AS患儿中，男47例，女11例。多数患儿以上呼吸道感染为诱因，以血尿和（或）蛋白尿起病。不同性别XL-AS患儿的阳性家族史、肾小管功能异常、高血压、肾功能受损、眼或耳病变比例及肾组织光镜下病理改变的差异均无统计学意义。电镜下广泛性肾小球基底膜致密层撕裂分层男83.0%（39/47），女18.2%（2/11）），性别差异有统计学意义（P=0.000），其余患儿表现为部分基底膜致密层撕裂、分层。男性XL-AS蛋白尿进展与年龄显著相关（r=0.501，P=0.000）。5例XL-AS男性患儿在11~16岁发生肾衰竭。结论 Alport综合征以X连锁显性遗传为主，男性电镜下基底膜广泛致密层撕裂比例高，且蛋白尿随年龄进展显著；肾脏或皮肤Ⅳ型胶原检测有助于诊断和判断遗传类型。Objective To analyze the clinical and pathological characteristics of Alport syndrome in children. Methods Clinical and pathological information gathered from 62 patients during March 1989 to August 2012 was retrospectively analyzed. Results Four autosomal recessive Alport syndromes （AR-AS） and 58 X-linked Alport syndromes （XL-AS） were analyzed. Of the XL-AS, 47 were boys and 11 were girls. Most of patients induced by upper respiratory tract infections, and onset with hematuria and proteinuria. There was no signiifcant gender difference in family history, impaired renal tubular proteins, hypertension, im-paired renal function, hearing loss, ocular abnormalities or renal pathological changes under light microscopy. However, extensive lamination and split of glomerular basement membrane （GBM） dense layers were found in 83.0%male and 18.2%female patients （P=0.000） and the rest patients were presented with limited distribution of typical GBM changes. Proteinuria progressed signiif-cantly with age in XL-AS males （r=0.501, P=0.000）. Five XL-AS patients developed to end stage renal disease （ESRD） between 11 to 16 years old. Conclusions XL-AS is the main inherited type and severe changes of GBM are common in XL-AS males. Proteinuria increases remarkably with age. The detection of type IV collagen in renal tissue or skin is helpful to diagnose Alport syndrome and conifrm inheritance modes.

关 键 词：Alport综合征  临床特点 病理改变 儿童 

分 类 号：R725.9[医药卫生—儿科]