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Pathological Role of Tonsillar B Cells in IgA Nephropathy

机译:扁桃体B细胞在IgA肾病中的病理作用

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Although impaired immune regulation along the mucosa-bone marrow axis has been postulated to play an important role, the pathogenesis of IgA nephropathy (IgAN) is unknown; thus, no disease-specific therapy for this disease exists. The therapeutic efficacy of tonsillectomy or tonsillectomy in combination with steroid pulse therapy for IgAN has been discussed. Although randomized control trials for these therapies are ongoing in Japan, the scientific rationale for these therapies remains obscure. It is now widely accepted that abnormally glycosylated IgA1 and its related immune complex (IC) are probably key molecules for the pathogenesis, and are thus considered possible noninvasive biomarkers for this disease. Emerging evidence indicates that B cells in mucosal infections, particularly in tonsillitis, may produce the nephritogenic IgA. In this paper, we briefly summarize characteristics of the nephritogenic IgA/IgA IC, responsible B cells, and underlying mechanisms. This clinical and experimental information may provide important clues for a therapeutic rationale.
机译:尽管已经假定沿粘膜-骨髓轴的免疫调节受损可能起重要作用,但尚不清楚IgA肾病(IgAN)的发病机制;因此,不存在针对该疾病的疾病特异性疗法。讨论了扁桃体切除术或扁桃体切除术联合类固醇脉冲疗法治疗IgAN的疗效。尽管在日本正在进行针对这些疗法的随机对照试验,但是对于这些疗法的科学依据仍然不清楚。现已被广泛接受,异常糖基化的IgA1及其相关的免疫复合物(IC)可能是发病机理的关键分子,因此被认为是该疾病的可能的非侵入性生物标志物。新兴证据表明,粘膜感染(尤其是扁桃体炎)中的B细胞可能会产生肾炎性IgA。在本文中,我们简要总结了生肾的IgA / IgA IC,负责的B细胞及其潜在机制的特征。该临床和实验信息可能为治疗原理提供重要线索。

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