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IgG4相关性肾病与腹膜后纤维化:最新进展

IgG4-related kidney disease and retroperitoneal fibrosis: An update.

作者信息

Kawano Mitsuhiro, Saeki Takako, Nakashima Hitoshi

机构信息

a Division of Rheumatology, Department of Internal Medicine , Kanazawa University Hospital , Kanazawa , Japan.

b Department of Internal Medicine , Nagaoka Red Cross Hospital , Nagaoka , Japan.

出版信息

Mod Rheumatol. 2019 Mar;29(2):231-239. doi: 10.1080/14397595.2018.1554321. Epub 2019 Jan 8.

DOI:10.1080/14397595.2018.1554321
PMID:30499730
Abstract

The most representative kidney lesion of IgG4-related disease (IgG4-RD) is plasma cell-rich tubulointerstitial nephritis (TIN) with distinctive imaging findings including multiple low-density lesions on contrast-enhanced computed tomography. In addition, membranous glomerulonephritis is a representative glomerular lesion of this disease. Recent advances have clarified that inflammation with IgG4-positive plasma cell infiltrates is not restricted to the renal parenchyma, but can be seen in outside the renal capsule, around medium-sized arteries such as lobar arteries, around nerves, and in the renal pelvis and periureter. Hypocomplementemia is a very important feature of IgG4-TIN, and serum complement level might serve as a convenient biomarker to predict relapse. Although good responsiveness to glucocorticoid has been considered characteristic of IgG4-RD, delayed start of treatment is associated with partial scarring in the kidneys on imaging study. Therefore, steroid therapy should be immediately initiated as soon as the diagnosis of IgG4-TIN is made. Future analyses of pathogenesis will be needed to more precisely define the optimal therapeutic strategies for the various subsets of Ig4-RD patients.

摘要

IgG4相关性疾病(IgG4-RD)最具代表性的肾脏病变是富含浆细胞的肾小管间质性肾炎(TIN),其具有独特的影像学表现,包括在对比增强计算机断层扫描上的多个低密度病变。此外,膜性肾小球肾炎是该疾病的一种代表性肾小球病变。最近的研究进展表明,IgG4阳性浆细胞浸润的炎症不仅局限于肾实质,还可见于肾包膜外、叶间动脉等中等大小动脉周围、神经周围以及肾盂和输尿管周围。低补体血症是IgG4-TIN的一个非常重要的特征,血清补体水平可能作为预测复发的便捷生物标志物。尽管对糖皮质激素的良好反应一直被认为是IgG4-RD的特征,但治疗开始延迟与影像学研究中肾脏的部分瘢痕形成有关。因此,一旦确诊IgG4-TIN,应立即开始使用类固醇治疗。未来需要对发病机制进行分析,以更精确地确定Ig4-RD患者不同亚组的最佳治疗策略。

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