Population genetic and biophysical evidences reveal that purifying selection shapes the genetic landscape of Plasmodium falciparum RH ligands in Chhattisgarh and West Bengal, India

Ghoshal, Sharmistha; Chowdhury, Pramita; Ray, Subhankar; Mitra, Mitashree; Kanjilal, Sumana Datta; Sen, Siddhartha; Dasgupta, Anjan Kr.; Sengupta, Sanghamitra

doi:10.1186/s12936-020-03433-z

Cited by 3 publications

(1 citation statement)

References 49 publications

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“…We found three polymorphic residues in the epitope of 42D6, two of which (Pf3D7 E1671K, L1692F) have been confirmed not to significantly impact binding, while the effect on binding and potency of the third residue (Pf3D7 G1623R) remains uncharacterized and thus unknown. In contrast, Rh5 is uniquely well-conserved among blood-stage antigens, as previously reported 93 . Most potent antibodies to Rh5 were found around the binding interface of Rh5 and human protein Basigin 81 .…”

Section: Discussionsupporting

confidence: 72%

Diversity and selection analyses identify transmission-blocking antigens as the optimal vaccine candidates inPlasmodium falciparum

Ciubotariu,

Broyles,

Xie

et al. 2024

Preprint

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Background A highly effective vaccine for malaria remains an elusive target, at least in part due to the under-appreciated natural parasite variation. This study aimed to investigate genetic and structural variation, and immune selection of leading malaria vaccine candidates across the Plasmodium falciparum life cycle. Methods We analyzed 325 P. falciparum whole genome sequences from Zambia, in addition to 791 genomes from five other African countries available in the MalariaGEN Pf3k Rdatabase. Ten vaccine antigens spanning three life-history stages were examined for genetic and structural variations, using population genetics measures, haplotype network analysis, and 3D structure selection analysis. Findings Among the ten antigens analyzed, only three in the transmission-blocking vaccine category display P. falciparum 3D7 as the dominant haplotype. The antigens AMA1, CSP, MSP119 and CelTOS, are much more diverse than the other antigens, and their epitope regions are under moderate to strong balancing selection. In contrast, Rh5, a blood stage antigen, displays low diversity yet slightly stronger immune selection in the merozoite-blocking epitope region. Except for CelTOS, the transmission-blocking antigens Pfs25, Pfs48/45, Pfs230, Pfs47, and Pfs28 exhibit minimal diversity and no immune selection in epitopes that induce strain-transcending antibodies, suggesting potential effectiveness of 3D7-based vaccines in blocking transmission. Interpretations These findings offer valuable insights into the selection of optimal vaccine candidates against P. falciparum. Based on our results, we recommend prioritizing conserved merozoite antigens and transmission-blocking antigens. Combining these antigens in multi-stage approaches may be particularly promising for malaria vaccine development initiatives.

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Section: Discussionsupporting

confidence: 72%

Diversity and selection analyses identify transmission-blocking antigens as the optimal vaccine candidates inPlasmodium falciparum

Ciubotariu,

Broyles,

Xie

et al. 2024

Preprint

View full text Add to dashboard Cite

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Diversity and selection analyses identify transmission-blocking antigens as the optimal vaccine candidates in Plasmodium falciparum

Ciubotariu,

Broyles,

Xie

et al. 2024

eBioMedicine

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Genetic Diversity of thePlasmodium falciparumReticulocyte Binding protein Homologue-5 which is a potential Malaria Vaccine Candidate: Baseline data from areas of varying malaria endemicity in Mainland Tanzania

Kisambale,

Lyimo,

Pereus

et al. 2024

Preprint

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Background: The limited efficacy of the two malaria vaccines, RTS,S/AS01 and R21/Matrix M, which were recently approved vaccines by the World Health Organization, highlights the need for alternative vaccine candidate genes beyond these pre-erythrocytic-based vaccines. Plasmodium falciparum Reticulocyte Binding Protein Homologue 5 (Pfrh5) is a potential malaria vaccine candidate, given its limited polymorphism compared to other parasites blood stage antigens. This study evaluated the genetic diversity of thePfrh5gene among parasites from regions with varying malaria transmission intensities in Mainland Tanzania, to generate baseline data for this potential malaria vaccine candidate.Methods: This study utilized secondary data of 697 whole-genome sequences from Mainland Tanzania, which were generated by the MalariaGEN Community Network. The samples which were sequenced to generate the data were collected between 2010 and 2015 from five districts within five regions of Mainland Tanzania, with varying endemicities (Morogoro urban district in Morogoro region, Muheza district in Tanga region, Kigoma-Ujiji district in Kigoma region, Muleba district in Kagera region, and Nachingwea district in Lindi region). The genetic diversity of thePfrh5gene was assessed using different genetic metrics, including Wright′s fixation index (FST), Wright′s inbreeding coefficient (Fws), Principal Component analysis (PCA), nucleotide diversity (π), haplotype network, haplotype diversity (Hd), Tajma′s D, and Linkage disequilibrium (LD).Results. Of the sequences used in this study (n=697), 84.5% (n = 589/697) passed quality control and 313 (53.1%) were monoclonal, and these monoclonal sequences were used for haplotype diversity and haplotype network analysis. High within-host diversity (Fws <0.95) was reported in Kigoma-Ujiji (60.7%), Morogoro urban (53.1%), and Nachingwea (50.8%), while Muleba (53.9%) and Muheza (61.6%) had low within host diversity (Fws≥ 0.95). PCA did not show any population structure across the five districts and the mean FSTvalue among the study populations was 0.015. Low nucleotide diversity values were observed across the study sites with the mean nucleotide diversity of 0.00056. A total of 27 haplotypes were observed among the 313 monoclonal samples. The Pf3D7 was detected as Hap_1, and it was detected in 16/313 (5.1%) sequences, and these sample sequences were from Muheza (62.5%, n=10/16), Kigoma-Ujiji (18.8%, n=3/16), and Muleba (18.8%, n=3/16). Negative Tajima′s D values were observed among the parasite populations in all the study sites.Conclusion. In this study, we observed low levels of polymorphism in thePfrh5gene, as it exhibited low nucleotide and haplotype diversity, a lack of population structure and negative Tajima′s D values as signatures of purifying selection. This study provides an essential framework of the diversity of thePfrh5gene to be considered in development of the next generation malaria vaccines. Robust and intensive studies of this and other candidate genes are required for characterization of the parasites from areas with varying endemicity, and are crucial to support the prioritization of thePfrh5gene for potential inclusion in a broadly cross-protective malaria vaccine.

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Population genetic and biophysical evidences reveal that purifying selection shapes the genetic landscape of Plasmodium falciparum RH ligands in Chhattisgarh and West Bengal, India

Cited by 3 publications

References 49 publications

Diversity and selection analyses identify transmission-blocking antigens as the optimal vaccine candidates inPlasmodium falciparum

Diversity and selection analyses identify transmission-blocking antigens as the optimal vaccine candidates inPlasmodium falciparum

Diversity and selection analyses identify transmission-blocking antigens as the optimal vaccine candidates in Plasmodium falciparum

Genetic Diversity of thePlasmodium falciparumReticulocyte Binding protein Homologue-5 which is a potential Malaria Vaccine Candidate: Baseline data from areas of varying malaria endemicity in Mainland Tanzania

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