A Compound Heterozygous HPD Mutation in an Iranian Patient with Hypertyrosinemia Type III

International Journal of Medical Laboratory Pub Date : 2023-01-03 DOI:10.18502/ijml.v9i4.11619

F. Sarkargar, Seyed Ali Madani Manshadi, Ehsan Zare Mehrjardi, Hosein Khodaei, S. Kalantar, Seyed Ahmad Mohamamdi

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Abstract

Background and Aims: Hypertyrosinemia type 3 (HT3) is an inherited error in tyrosine metabolism caused by a mutation in the 4-hydroxyphenylpyruvate dioxygenase (HPD) gene. Here we report a one and half-year-old girl infant who was diagnosed based on increased serum tyrosine levels and increased urinary excretion of p-hydroxyphenyl derivatives. Materials and Methods: The proband was one and half-year-old Iranian girl who was diagnosed based on increased serum tyrosine levels and increased urinary excretion of p-hydroxyphenyl derivatives. In this study, we used Whole-Exome Sequencing to identify the genetic reason for the disease and the funded mutation confirmed by Sanger sequencing. Results and Conclusion: Through whole-exome sequencing screening of heterozygotes c.413C>T (p.T138M) and c.75G.A (p.W25Ter) in the HPD gene and genetically confirmed by Sanger sequencing. There were heterozygous conditions c.413C>T (p.T138M) and c.75G.A (p.W25Ter) in father and mother respectively. This mutation in her parents was also confirmed by Sanger sequencing.

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伊朗III型高酪氨酸血症患者的复合杂合HPD突变

背景和目的:高酪氨酸血症3型(HT3)是由4-羟基苯基丙酮酸双加氧酶(HPD)基因突变引起的酪氨酸代谢遗传错误。在这里，我们报告了一个一岁半的女婴，她被诊断为血清酪氨酸水平升高和尿中对羟基苯基衍生物排泄增加。材料与方法:先证者为1岁半的伊朗女孩，根据血清酪氨酸水平升高和尿中对羟基苯基衍生物排泄增加诊断。在这项研究中，我们使用全外显子组测序来确定疾病的遗传原因和Sanger测序证实的资助突变。结果与结论:通过全外显子组测序筛选杂合子c.413C>T (p.T138M)和c.75G。HPD基因中的A (p.W25Ter)，经Sanger测序证实。杂合条件为c.413C>T (p.T138M)和c.75G。A (p. w25)分别在父亲和母亲。她父母的这种突变也被桑格测序证实。

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International Journal of Medical Laboratory

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