A High-Throughput Method for Quantifying Alleles and Haplotypes of the Malaria Vaccine Candidate Plasmodium falciparum Merozoite Surface Protein-1 19 kDa

May 27, 2010

by Shannon Takala David L. Smith O. Colin Stine Drissa Coulibaly Mahamadou Thera Ogobara Doumbo Christopher Plowe

Background

Malaria vaccine efficacy may be compromised if the frequency of non-target alleles increases following vaccination with a genetically polymorphic target. Methods are needed to monitor genetic diversity in polymorphic vaccine antigens, but determining which genetic variants of such antigens are present in infected individuals is complicated by the frequent occurrence of mixed infections.

The Findings

Pyrosequencing in conjunction with a haplotype-estimating algorithm provides accurate estimates of haplotypes present in infections with up to 3 haplotypes, and can be used to monitor genetic diversity in parasite populations prior to and following introduction of MSP-1- based malaria vaccines.

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A High-Throughput Method for Quantifying Alleles and Haplotypes of the Malaria Vaccine Candidate Plasmodium falciparum Merozoite Surface Protein-1 19 kDa

Background

The Findings

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