M'Dimegh Saoussen, Aquaviva-Bourdain Cécile, Omezzine Asma, M'Barek Ibtihel, Souche Geneviéve, Zellama Dorsaf, Abidi Kamel, Achour Abdelattif, Gargah Tahar, Abroug Saoussen, Bouslama Ali
Biochemistry Department, LR12SP11, Sahloul University Hospital, 4054 Sousse,
J Genet. 2016 Sep;95(3):659-66. doi: 10.1007/s12041-016-0676-4.
Primary hyperoxaluria type I (PH1) is an autosomal recessive metabolic disorder caused by inherited mutations in the AGXT gene encoding liver peroxisomal alanine : glyoxylate aminotransferase (AGT) which is deficient or mistargeted to mitochondria. PH1 shows considerable phenotypic and genotypic heterogeneity. The incidence and severity of PH1 varies in different geographic regions. DNA samples of the affected members from two unrelated Tunisian families were tested by amplifying and sequencing each of the AGXT exons and intron-exon junctions. We identified a novel frameshift mutation in the AGXT gene, the c.406_410dupACTGC resulting in a truncated protein (p.Gln137Hisfs19). It is found in homozygous state in two nonconsanguineous unrelated families from Tunisia. These molecular findings provide genotype/phenotype correlations in the intrafamilial phenotypic and permit accurate carrier detection, and prenatal diagnosis. The novel p.Gln137Hisfs19 mutation detected in our study extend the spectrum of known AGXT gene mutations in Tunisia.
I型原发性高草酸尿症(PH1)是一种常染色体隐性代谢紊乱疾病,由编码肝脏过氧化物酶体丙氨酸:乙醛酸转氨酶(AGT)的AGXT基因突变所致,该酶缺乏或错误定位于线粒体。PH1表现出显著的表型和基因型异质性。PH1的发病率和严重程度在不同地理区域有所不同。通过对两个突尼斯无关家庭中受影响成员的DNA样本进行AGXT外显子和内含子 - 外显子连接区的扩增和测序来进行检测。我们在AGXT基因中鉴定出一种新的移码突变,即c.406_410dupACTGC,导致截短蛋白(p.Gln137Hisfs19)。在来自突尼斯的两个非近亲无关家庭中发现其处于纯合状态。这些分子学发现提供了家族内表型的基因型/表型相关性,并允许进行准确的携带者检测和产前诊断。我们研究中检测到的新的p.Gln137Hisfs19突变扩展了突尼斯已知AGXT基因突变的范围。
