Sideroblastic anemia: functional study of two novel missense mutations in ALAS2.

Autor: Méndez M; Instituto de Investigación Hospital 12 de Octubre Madrid Spain., Moreno-Carralero MI; Instituto de Investigación Hospital 12 de Octubre Madrid Spain., Morado-Arias M; Departamento de Hematología Hospital La Paz Madrid Spain., Fernández-Jiménez MC; Departamento de Hematología Complejo Hospitalario de Toledo Toledo Spain., de la Iglesia Iñigo S; Departamento de Hematología Hospital Doctor Negrín Las Palmas de Gran Canaria Madrid Spain., Morán-Jiménez MJ; Instituto de Investigación Hospital 12 de Octubre Madrid Spain.
Jazyk: angličtina
Zdroj: Molecular genetics & genomic medicine [Mol Genet Genomic Med] 2016 Jan 13; Vol. 4 (3), pp. 273-82. Date of Electronic Publication: 2016 Jan 13 (Print Publication: 2016).
DOI: 10.1002/mgg3.202
Abstrakt: Background: X-linked sideroblastic anemia (XLSA) is a disorder characterized by decreased heme synthesis and mitochondrial iron overload with ringed sideroblasts in bone marrow. XLSA is caused by mutations in the erythroid-specific gene coding 5-aminolevulinate synthase (ALAS2). Anemia in XLSA is extremely variable, characteristically microcytic and hypochromic with poikilocytosis, and the red blood cell distribution width is increased and prominent dimorphism of the red cell population. Anemia in XLSA patients responds variably to supplementation with pyridoxine.
Methods and Results: We report four patients with XLSA and three mutations in ALAS2: c.611G>A (p.Arg204Gln), c.1218G>T (p.Leu406Phe) and c.1499A>G (p.Tyr500Cys). The in silico predictions of three ALAS2 mutations and the functional consequences of two ALAS2 mutations were assessed. We performed in silico analysis of these mutations using ten different softwares, and all of them predicted that the p.Tyr500Cys mutation was deleterious. The in vitro prokaryotic expression showed that the p.Leu406Phe and p.Tyr500Cys mutations reduced the ALAS2 specific activity (SA) to 14% and 7% of the control value, respectively.
Conclusion: In view of the results obtained in this study, a clear relationship between genotype and phenotype cannot be established; clinical variability or severity of anemia may be influenced by allelic variants in other genes or transcription factors and environmental conditions.
Databáze: MEDLINE
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