Primary hyperoxaluria: Comprehensive mutation screening of the disease causing genes and spectrum of disease‐associated pathogenic variants

原发性高草酸尿 移码突变 遗传学 生物 错义突变 人口 无义突变 等位基因 基因 次等位基因频率 肾钙质沉着症 突变 等位基因频率 医学 环境卫生
作者
Aiysha Abid,Ali Raza,Abdul Rafay Khan,Sadaf Firasat,Saba Shahid,Seema Hashmi,Mirza Naqi Zafar,Sajid Sultan,Shagufta Khaliq,Syed Adib‐ul‐Hasan Rizvi
出处
期刊:Clinical Genetics [Wiley]
卷期号:103 (1): 53-66 被引量:9
标识
DOI:10.1111/cge.14240
摘要

The primary hyperoxalurias are rare disorders of glyoxylate metabolism. Accurate diagnosis is essential for therapeutic and management strategies. We conducted a molecular study on patients suffering from recurrent calcium-oxalate stones and nephrocalcinosis and screened primary hyperoxaluria causing genes in a large cohort of early-onset cases. Disease-associated pathogenic-variants were defined as missense, nonsense, frameshift-indels, and splice-site variants with a reported minor allele frequency <1% in controls. We found pathogenic-variants in 34% of the cases. Variants in the AGXT gene causing PH-I were identified in 81% of the mutation positive cases. PH-II-associated variants in the GRHPR gene are found in 15% of the pediatric PH-positive population. Only 3% of the PH-positive cases have pathogenic-variants in the HOGA1 gene, responsible to cause PH-III. A population-specific AGXT gene variant c.1049G>A; p.Gly350Asp accounts for 22% of the PH-I-positive patients. Pathogenicity of the identified variants was evaluated by in-silico tools and ACMG guidelines. We have devised a rapid and low-cost approach for the screening of PH by using targeted-NGS highlighting the importance of an accurate and cost-effective screening platform. This is the largest study in Pakistani pediatric patients from South-Asian region that also expands the mutation spectrum of the three known genes.
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