Abstract

BackgroundAdenylate kinase (AK) deficiency is a rare red cell enzymopathy associated with moderate to severe congenital nonspherocytic hemolytic anemia, along with mental and psychomotor retardation (in exceptional cases). Only ten mutations have been detected in the AK1 gene to date. In this study, we aimed to diagnose the unexplained issue of haemolytic anaemia and offer antenatal screening to the family.MethodsGenomic DNA was isolated from whole blood by a standard protocol. Targeted next-generation sequencing (t-NGS) was performed to identify pathogenic variants in the patient and control samples. A chronic villus sample was collected at 11 weeks of gestation from the mother, and molecular testing was performed. Genetic confirmation was concluded by Sanger DNA sequencing. Bioinformatics tools predicted the pathogenicity of the variant.Resultst-NGS revealed a homozygous variant (c.301C > A, p. Gln101Lys) in the AK1 gene in the patient and heterozygosity in the fetus and parental samples. The prediction tools SIFT, Polyphen2, Provean, PMUT, Mutation taster, and Mutation Assessor, confirmed the damaging effect of the variant on the AK1 protein structureConclusionWe have presented a novel mutation in the AK1 gene (p. Gln101Lys) associated with adenylate kinase deficiency. It is the first prenatal diagnosis of AK deficiency in India, where heterogeneity is exceptionally high.

Highlights

  • Adenylate kinase (AK) deficiency is a rare red cell enzymopathy associated with moderate to severe congenital nonspherocytic hemolytic anemia, along with mental and psychomotor retardation

  • Adenylate kinase (AK) deficiency (OMIM 103000) is an autosomal recessive disorder associated with moderate to severe congenital hemolytic anemia, with psychomotor impairment observed in few cases [1]

  • This study investigated the molecular basis of erythrocyte AK deficiency in an Indian family and provided prenatal diagnosis to them for subsequent pregnancy

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Summary

Introduction

Adenylate kinase (AK) deficiency is a rare red cell enzymopathy associated with moderate to severe congenital nonspherocytic hemolytic anemia, along with mental and psychomotor retardation (in exceptional cases). Ten mutations have been detected in the AK1 gene to date. Adenylate kinase (AK) deficiency (OMIM 103000) is an autosomal recessive disorder associated with moderate to severe congenital hemolytic anemia, with psychomotor impairment observed in few cases [1]. The enzyme involved in this disorder is adenylate kinase type I (AK1), which catalyzes the conversion of adenine. AK1 belongs to the cytosolic enzyme family (EC 2.7.4.3). The AK1 gene is located on chromosome 9 on location 9q34. 11 (NCBI Gene ID: 203) and is highly expressed mainly in tissues with a high turnover rate, such as blood, brain, and muscles[2].

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