Zhou Jianhua, Huang Aixia, Liu Tonglin, Kuang Yujiu
Department of Pediatrics, Tongji Hospital, Tongji Medical College, Huazhong University of Science and Technology, Wuhan 430030, China.
J Huazhong Univ Sci Technolog Med Sci. 2005;25(5):538-42, 551. doi: 10.1007/BF02896011.
In order to characterize their relationship through clinicopathological comparison between IgA nephropathy and Henoch-Schönlein purpura nephritis (HSPN), 31 children with IgA nephropathy aged between 3 to 15 years and 120 children with HSPN aged between 4 to 15 years were compared with each other in clinical manifestation, blood biochemistry, serum immunology and follow-up study. Renal pathological findings under light microscope, immunofluorescence and electronic microscope were analyzed and also compared between 31 children with IgA nephropathy and 32 biopsied children with HSPN. The results showed that the onset age was over 12 years in 25.8% children with IgA nephropathy, but only 10% in HSPN (P < 0.05). The clinical patterns of IgA nephropathy and HSPN were similar, but extra-renal manifestations were more often in HSPN, all of them had skin purpura, 59% had gastrointestinal symptoms and 47% suffered from arthralgia, compared with only abdominal pain in 3.2% children with IgA nephropathy. The renal pathological investigation showed global sclerosis in 35.5% of IgA nephropathy and 3.1% of HSPN, mesangial sclerosis in 41.9% of IgA nephropathy and 6.3% of HSPN, but endothelial proliferation in 65.6% of HSPN and 29% of IgA nephropathy (all P < 0.01). Thin basement membrane nephropathy was only found in 6.5% children with IgA nephropathy, no in HSPN. The electronic dense deposits in HSPN were sparse, loose and wildly spread in glomerular mesangium, subendothelial area and even intra basement membrane, but it was dense, lumpy and mostly limited in mesangium and paramesangium in IgA nephropathy. Predominant IgA deposits were found in 81.2% of HSPN, and overwhelming IgG deposits in 12.5% of HSPN with relatively weak IgA deposits, moreover 6.3% of HSPN showed linear IgG deposits in glomerular capillary. Totally 71.9% of HSPN had IgG deposits in glomeruli and only 19.4% of IgA nephropathy showed glomerular IgG deposits (P < 0.01). No IgG deposit was observed in 81.6% of IgA nephropathy, among them most showed IgA and IgM and/or C3 deposits, moreover overwhelming IgG deposits and linear IgG deposits couldn't be found in IgA nephropathy. Mean 20 months follow-up showed complete remission in 72.5% of HSPN, but only 19.4% in IgA nephropathy after 34 months follow-up. Moreover, 64.5% of IgA nephropathy had consistent hematuria and proteinuria and 16.1% had active nephritides (P < 0.05). It was concluded that significant clinico-pathological difference was found between HSPN and IgA nephropathy, which didn't support the one disease entity hypothesis. HSPN and IgA nephropathy are probably two diseases with similar immune abnormalities.
为了通过IgA肾病与过敏性紫癜性肾炎(HSPN)的临床病理比较来描述它们之间的关系,对31例3至15岁的IgA肾病患儿和120例4至15岁的HSPN患儿进行了临床表现、血液生化、血清免疫学及随访研究方面的相互比较。分析了31例IgA肾病患儿和32例经活检的HSPN患儿的光镜、免疫荧光及电镜下的肾脏病理表现,并进行了比较。结果显示,25.8%的IgA肾病患儿发病年龄超过12岁,而HSPN中仅为10%(P<0.05)。IgA肾病和HSPN的临床类型相似,但HSPN的肾外表现更常见,所有患儿均有皮肤紫癜,59%有胃肠道症状,47%有关节痛,而IgA肾病患儿中仅有3.2%有腹痛。肾脏病理检查显示,35.5%的IgA肾病和3.1%的HSPN有全球硬化,41.9%的IgA肾病和6.3%的HSPN有系膜硬化,但65.6%的HSPN和29%的IgA肾病有内皮细胞增生(均P<0.01)。薄基底膜肾病仅在6.5%的IgA肾病患儿中发现,HSPN中未发现。HSPN中的电子致密沉积物稀疏、松散且广泛分布于肾小球系膜、内皮下区域甚至基底膜内,而IgA肾病中的沉积物致密、块状且大多局限于系膜和系膜旁区。81.2%的HSPN有主要的IgA沉积,12.5%的HSPN有压倒性的IgG沉积且IgA沉积相对较弱,此外6.3%的HSPN在肾小球毛细血管中有线性IgG沉积。总计71.9%的HSPN在肾小球中有IgG沉积,而仅19.4%的IgA肾病有肾小球IgG沉积(P<0.01)。81.6%的IgA肾病未观察到IgG沉积,其中大多数表现为IgA和IgM及/或C3沉积,此外IgA肾病中未发现压倒性的IgG沉积和线性IgG沉积。平均20个月的随访显示,72.5%的HSPN完全缓解,而IgA肾病在34个月随访后仅有19.4%完全缓解。此外,64.5%的IgA肾病有持续性血尿和蛋白尿,16.1%有活动性肾炎(P<0.05)。结论是,HSPN和IgA肾病之间存在显著的临床病理差异,这不支持单一疾病实体假说。HSPN和IgA肾病可能是两种具有相似免疫异常的疾病。
Zotero 插件