Scientists have identified some red blood cell traits in children that can increase or decrease their risk for malaria disease.
The findings by the researchers at the National Institute of Allergy and Infectious Diseases, could help identify future targets for new malaria drugs and vaccines.
From 2008 to 2011, NIAID scientists and their collaborators followed 1,543 children ranging from 6 months to 17 years old in Mali, a West African country with a high incidence of childhood malaria. Throughout the study period, the children experienced a total of 4,091 episodes of malaria. Investigators observed that several red blood cell variants--inherited disorders associated with abnormal forms or decreased production of the oxygen-carrying blood protein hemoglobin--were associated with malaria risk.
Specifically, the sickle-cell trait HbAS, which means an individual carries only one defective gene that causes the production of abnormal hemoglobin, appeared to correlate with protection from malaria in early childhood and reduced the density of malaria parasites in children who did become ill. HbAS.
Researchers also found that a genetic condition known as homozygous X-linked G6PD deficiency correlated with a reduced risk of malaria in girls only. Meanwhile, HbC-trait, in which the body makes an abnormal hemoglobin called hemoglobin C, appeared to increase malaria risk in children. Scientists hope this study will lead to further research into the molecular mechanisms of the malaria-protective effects of red blood cell variants.
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