系统性自身炎症、IgA 肾小球肾炎和肾皮质坏死:巧合还是因果关系?

Pub Date : 2024-01-01
Carlos Chiurchiu, Pehuén Fernández, Walter Douthat, Javier De Arteaga, Marco Mazzotta, Maximiliano Alderete, Verónica Saurit, Francisco Caeiro, Jorge De La Fuente
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引用次数: 0

摘要

我们为您介绍一名患有罕见的系统性自身炎症疾病(甲羟戊酸激酶缺乏症-MKD-)的患者,该患者的甲羟戊酸激酶基因中存在两个杂合变异体(c.1129G>A 和 c.32C>T),并通过新一代测序技术检测到了这两个变异体以及高发的肾小球肾炎(IgA 肾病)。患者临床表现为从出生 12 天起每月反复周期性发热,伴有粘膜病变(四肢斑丘疹、口腔炎)、关节病变(踝关节、腕关节和膝关节关节痛)、淋巴病变(颈淋巴结炎)和肾小球肾炎(IgA 肾病)、淋巴(颈淋巴结病、脾肿大)、胃肠(腹泻、腹痛)和肾脏(血尿和蛋白尿),反复活检显示 IgA 肾病的活动性和慢性交替出现。在随访期间。患者对使用了 7 年的多种免疫抑制疗法(皮质类固醇、硫唑嘌呤、霉酚酸酯、环磷酰胺、利妥昔单抗和托珠单抗)疗效不佳,最后对卡那单抗反应良好。开始使用卡那珠单抗四年后,在一次肌肉脓肿引起的感染过程中,临床表现因严重的肾微血管事件(肾皮质坏死-RCN-)而变得复杂,并伴有急性肾损伤和透析需求。肌肉脓肿导致的炎症发作可能是肾小球肾炎再活化的诱因(这可以解释为什么患者对免疫抑制剂反应不佳,并迅速发展为组织学上的慢性肾炎),并产生一种微环境,在非严重感染的情况下诱发 RCN。IgA 分子在 MKD 中存在缺陷,这一现象在 IgA 肾病中也可观察到。这就提出了一个具有挑战性的假设,即患者的所有临床表现之间存在共同的致病联系。
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Systemic autoinflammatory disease, IgA glomerulonephritis and renal cortical necrosis: coincidence or causation?

We present a patient with a rare systemic autoinflammatory disease (mevalonate kinase deficiency -MKD-) with the identification of two heterozygous variants (c.1129G>A and c.32C>T) in the Mevalonate Kinase gene, detected by next generation sequencing and a highly prevalent glomerulonephritis (IgA nephropathy). The patient presents clinically with a monthly recurrent periodic fever from 12 days of age, accompanied by mucocutaneous lesions (maculopapular rash in extremities, aphthous stomatitis), joint (arthralgias in ankles, wrists and knees), lymphoid (cervical lymphadenopathy, splenomegaly), gastrointestinal (diarrhea, abdominal pain) and kidney (hematuria and proteinuria) with repeated biopsies showing IgA nephropathy alternating activity with chronicity. During follow-up. The patients presented a poor therapeutic response to multiple immunosuppressive regimens used for 7 years (corticosteroids, azathioprine, mycophenolate, cyclophosphamide, rituximab and tocilizumab), and finally a good response to canakinumab. Four years after starting canakinumab, during the course of an infection due to a muscle abscess, the clinical presentation is complicated by a severe renal microvascular event (renal cortical necrosis -RCN-) with acute kidney injury and dialysis requirement. Therecurrent episodes of inflammation due to MKD could act as triggers for the reactivation of glomerulonephritis (which would explain the poor response to immunosuppressants and the rapid progression to histological chronicity) and to generate a microenvironment that predisposes the development of RCN in the face of a non-serious infection. A defect in IgA molecules has been described in MKD, a phenomenon also observed in IgA nephropathy. This raises the challenging hypothesis of a common pathogenetic link between all the patient's clinical manifestations.

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