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Cited 12 time in webofscience Cited 18 time in scopus
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Prevalence of glucose-6-phosphate dehydrogenase (G6PD) deficiency among malaria patients in Upper Myanmaropen access

Authors
Lee, JinyoungKim, Tae ImKang, Jung-MiJun, HojongLe, Huong GiangThi Lam ThaiSohn, Woon-MokMyint, Moe KyawLin, KhinKim, Tong-SooNa, Byoung-Kuk
Issue Date
16-Mar-2018
Publisher
BMC
Keywords
Glucose-6-phosphate dehydrogenase (G6PD); G6PD deficiency; Malaria; Primaquine; Myanmar
Citation
BMC INFECTIOUS DISEASES, v.18
Indexed
SCIE
SCOPUS
Journal Title
BMC INFECTIOUS DISEASES
Volume
18
URI
https://scholarworks.bwise.kr/gnu/handle/sw.gnu/11803
DOI
10.1186/s12879-018-3031-y
ISSN
1471-2334
Abstract
Background: Glucose-6-phosphate dehydrogenase (G6PD; EC 1.1.1.49) deficiency is one of the most common X-linked recessive hereditary disorders in the world. Primaquine (PQ) has been used for radical cure of P. vivax to prevent relapse. Recently, it is also used to reduce P. falciparum gametocyte carriage to block transmission. However, PQ metabolites oxidize hemoglobin and generate excessive reactive oxygen species which can trigger acute hemolytic anemia in malaria patients with inherited G6PD deficiency. Methods: A total of 252 blood samples collected from malaria patients in Myanmar were used in this study. G6PD variant was analysed by a multiplex allele specific PCR kit, DiaPlexC (TM) G6PD Genotyping Kit [Asian type]. The accuracy of the multiplex allele specific PCR was confirmed by sequencing analysis. Results: Prevalence and distribution of G6PD variants in 252 malaria patients in Myanmar were analysed. Six different types of G6PD allelic variants were identified in 50 (7 females and 43 males) malaria patients. The predominant variant was Mahidol (68%, 34/50), of which 91.2% (31/34) and 8.8% (3/34) were males and females, respectively. Other G6PD variants including Kaiping (18%, 9/50), Viangchan (6%, 3/50), Mediterranean (4%, 2/50), Union (2%, 1/50) and Canton (2%, 1/50) were also observed. Conclusions: Results of this study suggest that more concern for proper and safe use of PQ as a radical cure of malaria in Myanmar is needed by combining G6PD deficiency test before PQ prescription. Establishment of a follow-up system to monitor potential PQ toxicity in malaria patients who are given PQ is also required.
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