PIEZO1基因突变(c.2005G>T)引起铁超载心肌病1例报告

Sumei Cui, Huixia Lu, Shujian Wei, Chuanbao Li, F. Xu, Yuguo Chen
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摘要

摘要背景:心肌病有多种病因。在这里,我们报告了一例铁过载心肌病(IOC)合并遗传性口细胞增多症(HST),由于PIEZO1基因的罕见突变。病例总结:一名31岁男性以新发疲劳和腹胀就诊。患者有9年胆石症病史,4年溶血性贫血病史,7个月糖尿病病史,6个月性欲低下病史。古铜色皮肤、肝掌、黄眼、糖尿病和心肌病的具体特征使我们怀疑血色素沉着症,血清铁蛋白浓度升高和高转铁蛋白饱和度证实了这一点。超声心动图和心血管磁共振(CMR)成像显示所有心腔扩张,左心室射血分数为30%。CMR T2 *测图显示心肌、肝脏和胰腺黄素沉着。下一代测序鉴定出PIEZO1基因的一个错义变异(c.2005G>T),该变异导致HST和高铁蛋白血症。我们对他的近亲进行了筛查,发现他的儿子是这种变异的杂合携带者,患有间歇性黄疸。结论:在本病例中,piezo1c . 2005g >T突变导致HST和IOC,并伴有胆石症、糖尿病和性欲低下。青铜色皮肤、肝硬化、心肌病和糖尿病是危险信号,而磁共振成像T2 *作图、血铁代谢标记物和基因检测在诊断中是有价值的。
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The PIEZO1 gene mutation (c.2005G>T) causes iron overload cardiomyopathy: a case report
Supplemental Digital Content is available in the text Abstract Background: Cardiomyopathy has a variety of etiologies. Here, we report a case of iron overload cardiomyopathy (IOC) in combination with hereditary stomatocytosis (HST) due to a rare mutation in the PIEZO1 gene. Case summary: A 31-year-old man presented to the clinic with a new onset of fatigue and abdominal distension. He had a history of 9-year cholelithiasis, 4-year hemolytic anemia, 7-month diabetes mellitus (DM), and 6-month low sex drive. The specific features of bronze skin, liver palms, yellow eyes, DM, and cardiomyopathy raised our suspicion of hemochromatosis, which was confirmed by an elevated serum ferritin concentration and high transferrin saturation. Echocardiography and cardiovascular magnetic resonance (CMR) imaging demonstrated dilation of all cardiac cavities with a left ventricular ejection fraction of 30%. CMR T2∗ mapping showed myocardial, hepatic, and pancreatic siderosis. Next-generation sequencing identified one missense variant in the PIEZO1 gene (c.2005G>T), which conferred HST and hyperferritinemia. We screened his close family members and identified his son as a heterozygous carrier of this variant, who had intermittent jaundice. Conclusion: In this case, the PIEZO1 c.2005G>T mutation conferred HST and IOC, complicated with cholelithiasis, DM, and low sex drive. Bronze skin, liver cirrhosis, cardiomyopathy, and DM are red flags, while magnetic resonance imaging T2∗ mapping, blood iron metabolism markers, and gene testing are valuable in the diagnosis.
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