Complement Factor H Gene Variant in a Patient with Thrombotic Microangiopathy on a Mixed Clinical Background.

Case Reports in Nephrology Pub Date : 2021-10-25 eCollection Date: 2021-01-01 DOI:10.1155/2021/2519918
Yoichi Iwafuchi, Tetsuo Morioka, Yuko Oyama, Shin Goto, Ichiei Narita
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Abstract

We report the case of a patient with complement factor H gene variant, who developed thrombotic microangiopathy on a mixed clinical background. A 79-year-old woman was transferred to Sanjo General Hospital for maintenance hemodialysis. She suffered from gastric non-Hodgkin lymphoma about two years ago and received chemotherapy and radiation therapy, leading to complete remission. About 13 weeks prior to her transfer to our hospital, she was referred to another hospital due to acute kidney injury, hemolytic anemia, and thrombocytopenia. Hemodialysis was immediately initiated, after which intravenous methylprednisolone and oral prednisolone were started; however, she became anuric within approximately week. The possibility of thrombotic microangiopathy was examined. However, she was in poor general condition and did not get the consent of her family, so no invasive searches such as a kidney biopsy were performed. Despite the cause of acute kidney insufficiency being unclear, she was transferred to us for maintenance hemodialysis. Her general condition was stable, and her renal function improved; hence, two months after transfer, a kidney biopsy was performed. Her clinical and typical renal histological findings indicated a diagnosis of thrombotic microangiopathy. There was a possible CFH gene of a very rare variant "c.526 T > C (p.Phe176Leu)" in exon 5. She was able to withdraw from hemodialysis therapy two weeks after the initiation of an angiotensin-converting enzyme inhibitor. Based on her clinical course and kidney biopsy findings, she was diagnosed with thrombotic microangiopathy with a very rare CFH variant. To ensure proper treatment choices such as eculizumab, the presence of complement dysregulation should be considered in cases of secondary thrombotic microangiopathy.

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补体因子H基因变异在一个混合临床背景下的血栓性微血管病患者。
我们报告的情况下,患者补体因子H基因变异,谁发展血栓性微血管病的混合临床背景。一名79岁妇女被转送到Sanjo总医院进行维持性血液透析。大约两年前,她患上了胃非霍奇金淋巴瘤,接受了化疗和放疗,病情完全缓解。在转到我院前约13周,她因急性肾损伤、溶血性贫血和血小板减少症转到另一家医院。立即开始血液透析,然后开始静脉注射甲基强的松龙和口服强的松龙;然而,她在大约一周内就无尿了。检查血栓性微血管病变的可能性。然而,由于患者总体状况不佳,且未征得其家人的同意,因此未进行肾活检等侵入性检查。尽管急性肾功能不全的原因尚不清楚,她还是被转到我们这里进行维持性血液透析。患者一般情况稳定,肾功能改善;因此,移植后两个月,进行了肾活检。她的临床和典型的肾脏组织学检查结果显示血栓性微血管病变的诊断。在第5外显子中存在一个非常罕见的变异“C .526 T > C (p.p e176leu)”可能的CFH基因。在开始使用血管紧张素转换酶抑制剂两周后,她能够停止血液透析治疗。根据她的临床过程和肾脏活检结果,她被诊断为血栓性微血管病变,伴有非常罕见的CFH变异。为了确保正确的治疗选择,如eculizumab,在继发性血栓性微血管病变的情况下,应考虑补体失调的存在。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Case Reports in Nephrology
Case Reports in Nephrology Medicine-Nephrology
CiteScore
1.70
自引率
0.00%
发文量
32
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