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AN ODD CASE OF HETEROALLELIC ACUTE INTERMITTENT PORPHYRIA IN THE ARGENTINEAN POPULATION

机译:阿根廷人群中的异种急性间歇性卟啉症

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摘要

AIP is an acute liver disorder caused by a deficiency of porphobilinogen deaminase (PBGD) characterized by neuroabdominal symptoms. It is an autosomal dominant disease. However, homozygous dominant AIP (HD-AIP) have been described. In some cases erythrodontia was observed. CEP is an autosomal recessive disease produced by mutations in the uroporphyrinogen III synthase gene (UROS), characterized by severe cutaneous lesions and erythrodontia. The aim of the work was to establish the differential diagnosis of porphyria in a patient with abdominal pain, neurological attacks, skin symptoms and erythrodontia. The PBGD activity was reduced 50% and the genetic analysis indicated the presence of two genetic variants in the PBGD gene, p.G111R and p.E258G, a new genetic variant, revealing a case of heteroallelic HD-AIP. The patient, first diagnosed as a carrier of a dual porphyria: AIP / CEP based on the excretion profile of porphyrins, precursors and her clinical symptoms, would be an atypical case of human HD-AIP. These results would also suggest the presence of a phenocopy of the CEP, induced by an endogenous or exogenous factor. Our findings highlight the importance of genetic studies for a proper diagnosis of porphyria, prevention of its manifestation and its treatment.
机译:AIP是一种由以神经腹症状为特征的胆色素原脱氨酶(PBGD)缺乏引起的急性肝脏疾病。它是常染色体显性遗传疾病。然而,已经描述了纯合显性AIP(HD-AIP)。在某些情况下,观察到红斑。 CEP是由尿卟啉原III合酶基因(UROS)突变产生的常染色体隐性遗传疾病,其特征是严重的皮肤损伤和红斑。该工作的目的是为患有腹痛,神经系统疾病,皮肤症状和红斑症的患者建立卟啉症的鉴别诊断。 PBGD活性降低了50%,遗传分析表明PBGD基因中存在两个遗传变异,即新的遗传变异p.G111R和p.E258G,揭示了一个等位基因HD-AIP病例。该患者首先根据卟啉,前体的排泄情况和她的临床症状被诊断为双卟啉症的携带者:AIP / CEP,将是人类HD-AIP的非典型病例。这些结果还将暗示由内源性或外源性因子诱导的CEP表型的存在。我们的发现突出了基因研究对正确诊断卟啉症,预防其表现和治疗的重要性。

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