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Congenital lactic acidosis, cerebral cysts and pulmonary hypertension in an infant with FOXRED1 related complex I deficiency

机译:患有FOXRED1相关复合物I缺乏症的婴儿的先天性乳酸性酸中毒,脑囊肿和肺动脉高压

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Mitochondrial complex I is encoded by 38 nuclear-encoded and 7 mitochondrial-encoded genes. FOXRED1 is one of the 13 additional nuclear genes known as assembly factors. So far, four patients have been described with complex I deficiency caused by autosomal recessive mutations in FOXRED1. Here, we report the fifth patient with FOXRED1 related complex 1 deficiency presenting with prenatal onset of bilateral periventricular cysts, congenital lactic acidosis, and persistent life-limiting pulmonary hypertension. Whole exome sequencing identified a compound heterozygosity for a known pathogenic variant (c.612_615dupAGTG; p.A206SfsX15) (paternal) and a likely pathogenic variant (c.874G??A; p.Gly292Arg) (maternal). Deficiency of complex I was demonstrated by the absence of complex I on Blue Native Gel Electrophoresis and by a significantly reduced complex I enzyme activity in the patient's fibroblasts. Compared with the previous known FOXRED1 cases, unique clinical features observed in our patient include bilateral periventricular cysts and severe pulmonary hypertension. Whole exome sequencing was instrumental in recognizing the underlying gene defect in this patient.
机译:线粒体复合体I由38个核编码基因和7个线粒体编码基因编码。 FOXRED1是另外13个被称为装配因子的核基因之一。到目前为止,已经有4名患者因FOXRED1的常染色体隐性突变引起复杂I型缺乏。在这里,我们报告了第五例患有FOXRED1相关复合物1缺乏症的患者,其产前发作有双侧脑室囊肿,先天性乳酸性酸中毒和持续性限制生命的肺动脉高压。整个外显子组测序鉴定了已知病原体变异体(c.612_615dupAGTG; p.A206SfsX15)(父系)和可能的病原体变异体(c.874G?>ΔA; p.Gly292Arg)(母体)的化合物杂合性。蓝色天然凝胶电泳上不存在复合物I,并且患者成纤维细胞中复合物I酶的活性明显降低,从而证明了复合物I的缺乏。与先前已知的FOXRED1病例相比,在我们的患者中观察到的独特临床特征包括双侧脑室囊肿和严重的肺动脉高压。整个外显子组测序有助于识别该患者的潜在基因缺陷。

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