Mohd Shoeb Alam scite author profile

RTS,S is the most advanced malaria vaccine candidate, currently under phase-III clinical trials in Africa. This Plasmodium falciparum vaccine contains part of the central repeat region and the complete C-terminal T cell epitope region (Th2R and Th3R) of the circumsporozoite protein (CSP). Since naturally occurring polymorphisms at the vaccine candidate loci are critical determinants of the protective efficacy of the vaccines, it is imperative to investigate these polymorphisms in field isolates. In this study we have investigated the genetic diversity at the central repeat, C-terminal T cell epitope (Th2R and Th3R) and N-terminal T cell epitope regions of the CSP, in P. falciparum isolates from Madhya Pradesh state of India. These isolates were collected through a 5-year prospective study aimed to develop a well-characterized field-site for the future evaluation of malaria vaccine in India. Our results revealed that the central repeat (63 haplotypes, n = 161) and C-terminal Th2R/Th3R epitope (24 haplotypes, n = 179) regions were highly polymorphic, whereas N-terminal non-repeat region was less polymorphic (5 haplotypes, n = 161) in this population. We did not find any evidence of the role of positive natural selection in maintaining the genetic diversity at the Th2R/Th3R regions of CSP. Comparative analysis of the Th2R/Th3R sequences from this study to the global isolates (n = 1160) retrieved from the GenBank database revealed two important points. First, the majority of the sequences (∼61%, n = 179) from this study were identical to the Dd2/Indochina type, which is also the predominant Th2R/Th3R haplotype in Asia (∼59%, n = 974). Second, the Th2R/Th3R sequences in Asia, South America and Africa are geographically distinct with little allele sharing between continents. In conclusion, this study provides an insight on the existing polymorphisms in the CSP in a parasite population from India that could potentially influence the efficacy of RTS,S vaccine in this region.

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Host-Parasite Interaction: Selective Pv-fam-a Family Proteins ofPlasmodium vivaxBind to a Restricted Number of Human Erythrocyte Receptors

Zeeshan

Tyagi

et al. 2014

J Infect Dis.

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Interaction of Plasmodium vivax Tryptophan-rich Antigen PvTRAg38 with Band 3 on Human Erythrocyte Surface Facilitates Parasite Growth

Alam

Choudhary

Zeeshan

et al. 2015

Journal of Biological Chemistry

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Background: Plasmodium tryptophan-rich antigens are involved in host-parasite interaction. Results: Plasmodium vivax tryptophan-rich antigen PvTRAg38 interacts with three exofacial loops of Band 3 through its peptide domain KWVQWKNDKIRSWLSSEW to facilitate parasite growth. Conclusion: A novel receptor-ligand interaction between host and parasite has been defined. Significance:The study will help in understanding the host-parasite interaction and development of therapeutics for vivax malaria.

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Mohd Shoeb Alam

Genetic Variation in the Plasmodium falciparum Circumsporozoite Protein in India and Its Relevance to RTS,S Malaria Vaccine

Host-Parasite Interaction: Selective Pv-fam-a Family Proteins ofPlasmodium vivaxBind to a Restricted Number of Human Erythrocyte Receptors

Interaction of Plasmodium vivax Tryptophan-rich Antigen PvTRAg38 with Band 3 on Human Erythrocyte Surface Facilitates Parasite Growth

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