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Molecular characterization of six new cases of red blood cell hexokinase deficiency yields four novel mutations in HK1. | LitMetric

AI Article Synopsis

  • * This study analyzes six new cases of HK deficiency, identifying six distinct mutations in the HK1 gene, four of which are newly discovered.
  • * The research also confirmed the harmful nature of these mutations through biochemical tests and structural analysis, further enhancing understanding of the disease's underlying mechanisms and the relationship between genotype and phenotype in HK deficiency.

Article Abstract

Hexokinase (HK) is a key enzyme of glycolysis, the only metabolic pathway able to provide the red blood cell with ATP. HK deficiency is a very rare hereditary disorder with severe chronic nonspherocytic hemolytic anemia (HNSHA) as a major clinical feature. To date, only 24 patients with HK deficiency have been identified. Here, we report the molecular analysis of six new cases of HK deficiency. A total of six different mutations were detected in HK1, four of them described here for the first time: c.2599C>T p.(His867Tyr), c.1799C>T p.(Thr600Met), c.873-2A>G and c.493-1G>A. The pathogenic nature of the identified missense mutations was confirmed by biochemical and 3-dimensional structural analysis. The effects of the novel splice site mutation c.873-2A>G were studied at the level of pre-mRNA processing, and confirmed at the protein level. All together, these results provide a better insight into the pathogenesis of this rare red cell disorder, and contribute to a better understanding of the genotype-phenotype correlation in HK deficiency.

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Source
http://dx.doi.org/10.1016/j.bcmd.2016.04.002DOI Listing

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