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Clinical Manifestation of Patients With Atypical Hemolytic Uremic Syndrome With the C3 p.I1157T Variation in the Kinki Region of Japan

机译:日本近畿地区C3 p.I1157T变异的非典型溶血性尿毒症患者的临床表现

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摘要

The gain-of-function variation p.I1157T in C3 was previously identified in 8 patients with atypical hemolytic uremic syndrome (aHUS) at Mie University Hospital. In the present study, we identified another 11 patients with aHUS with this variation, including 10 pediatric patients (onset age: 1-16 years). The variation seems to be geographically concentrated around Mie Prefecture in Japan. Fifteen of the 19 patients with aHUS experienced infection as probable triggering events. All 19 patients had renal dysfunction. Seven patients, including 2 from the previous study and 5 from the present study, were treated with eculizumab, with all showing a good response with hematological normalization. Among the 5 eculizumab-treated patients in the present study, 3 had an ambiguous diagnosis of aHUS due to low-grade hemolysis even with elevated levels of lactate dehydrogenase and bilirubin. In those cases, in-house targeted DNA sequencing identified the C3 p.I1157T variation carriers, which enabled the early initiation of treatment with eculizumab. The present study supports the early introduction of eculizumab in patients with aHUS, especially pediatric patients.
机译:在三重大学医院的8例非典型溶血性尿毒症综合征(aHUS)患者中,先前确定了C3的功能增强p.I1157T。在本研究中,我们确定了另外11例具有这种变异的aHUS患者,包括10例儿科患者(发病年龄:1-16岁)。这种变化似乎集中在日本三重县附近。 19例aHUS患者中有15例可能是触发事件而感染。全部19例患者均患有肾功能不全。用依库丽单抗治疗了7例患者,包括先前研究的2例和本研究的5例,所有患者血液学正常化均显示出良好的反应。在本研究中5例接受依库丽单抗治疗的患者中,有3例因低度溶血而诊断为aHUS,即使乳酸脱氢酶和胆红素水平升高也是如此。在这些情况下,通过内部靶向DNA测序鉴定出C3 p.I1157T变异载体,从而能够尽早开始使用依库丽单抗治疗。本研究支持依库丽单抗早期用于aHUS患者,尤其是儿科患者。

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