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Alpha-thalassemia in Papua New Guinea
Authors:P Yenchitsomanus  K M Summers  P G Board  K K Bhatia  G L Jones  K Johnston  G T Nurse
Institution:(1) Department of Human Genetics, John Curtin School of Medical Research, Australian National University, P.O. Box 334, 2601 Canberra, A.C.T., Australia;(2) Papua New Guinea Institute of Medical Research, Goroka, Eastern Highlands Province, Papua New Guinea;(3) Department of Biochemistry, Nutrition and Microbiology, University of New England, 2351 Armidale, N.S.W., Australia;(4) Blood Transfusion Service, Papua New Guinea Red Cross, Boroko, Papua New Guinea
Abstract:Summary A study of the distribution of agr-thalassemia in Papua New Guinea (PNG) was carried out by DNA analysis. A total of 664 DNA samples were screened for agr-thalassemia 2 and agr-thalassemia 1 caused respectively by either deletion of one or both of the duplicated agr-globin genes. agr-Thalassemia 2 was detected in high frequencies in coastal and lowland regions where malaria has been holo- to hyperendemic but in low frequencies in non-malarious highland regions. The highest frequency was observed in the north coast of PNG. The distribution of agr-thalassemia 2 seems to be in accordance with other conditions such as ovalocytosis and G6PD deficiency which are also prevalent in this population, suggesting that they may interact in protection against malaria. However, it appears to be negatively correlated with beta-thalassemia and agr-thalassemia 1, the latter being extremely rare in this population. Analysis of the types and subtypes of the single agr-globin gene deletion revealed a predominance of the –agr4.2 type in general, except in some regions in the south where the –agr3.7 type is prevalent. The –agr3.7 I subtype is the common form of the –agr3.7 deletion in the PNG mainland. The –agr3.7 III subtype, previously reported to be unique in Melanesians and Polynesians, was detected in an offshore island of PNG. However, this subtype is very rare in Melanesians from the PNG mainland.
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