Please use this identifier to cite or link to this item: http://repository.kln.ac.lk/handle/123456789/10841
Title: Genetic modifier of Hereditary Hemochromatosis gene (HFE) in transfusion dependent thalassemia: phenotype genotype relationship in a Sri Lankan population
Authors: Padeniya, A.G.P.M.
Keywords: Hereditary Haemochromatosis (HH)
Hereditary Haemochromatosis gene (HFE)
thalassaemia patients
Issue Date: 2015
Publisher: Staff Development Center, University of Kelaniya
Citation: Padeniya, A.G.P.M. (2015). Genetic modifier of Hereditary Hemochromatosis gene (HFE) in transfusion dependent thalassemia: phenotype genotype relationship in a Sri Lankan population. In: Research Forum E Proceeding, Staff Development Centre Research Forum, Cycle 14-2015, University of Kelaniya, Kelaniya, pp 21-22.
Abstract: Background and Purpose: Iron overload is a major complication in patients with transfusion dependant thalassaemia and co- existence of Hereditary Haemochromatosis (HH) aggravates this complication. Two common missence mutations in the HFE gene 845G>A (p.C282Y) and c.187C>G (p.H63D) are associated with HH. The aim of this study was to genotype c.845G>A and c.187C>G mutations in regularly transfused β thalassaemia patients and to correlate the association between these mutations with their serum ferritin levels. Method: 125 patients with β thalassaemia who were on regular blood transfusions referred to ward 2, 3, 4 and 9, Lady Ridgway Hospital, Colombo and who were at Thalassaemia center, Teaching Hospital, Anuradhapura were recruited to the study. HFE gene was tested for c.845G>A and c.187C>G mutations by Amplification Refractory Mutation System Polymerase Chain Reaction. Serum ferritin level was measured using electrochemiluminescense method. The C-reactive protein (CRP), erythrocyte sedimentation level (ESR), and Serum Glutamine Aspartate Transaminase (SGPT) levels were done to exclude coexisting inflammatory states and liver disease. The results were analyzed using Student’s t-test. Results: None had the p.C282Y variant. 23 were heterozygous for the p.H63D variant. Allele frequencies of the two variants; p.C282Y and p.H63D, were 0% and 9.2% respectively. There was no statistically significant difference (p = 0.865) between the mean ferritin level of carriers and wild type of the p.H63D variant; the levels were 4987ng/ml and 4571ng/ml respectively. CRP, ESR and SGPT were elevated in 9 (7.2%; c.187CC 4, c.187CG 5), 65(52%; c.187CC 50, c.187CG 15), 82(65.6%; c.187CC 64, c.187CG 18) respectively. The confounding effect of inflammation and liver disease on the serum ferritin level could not be analyzed due to small sample size. Conclusions: In Sri Lankan patients with transfusion dependant thalassaemia the p.C282Y mutation is rare and cannot be considered as a risk factor for iron over load. The p.H63D mutation may be a potential risk factor for iron overload; this needs to be verified using larger cohort studies.
URI: http://repository.kln.ac.lk/handle/123456789/10841
ISSN: 2448-9743
Appears in Collections:Cycle 14 - 2015

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