Genetic diversity and neutral selection in Plasmodium vivax erythrocyte binding protein correlates with patient antigenicity

Genetic diversity and neutral selection in Plasmodium vivax erythrocyte binding protein correlates with patient antigenicity

© 2020 Han et al. Plasmodium vivax is the most widespread and difficult to treat cause of human malaria. The development of vaccines against the blood stages of P. vivax remains a key objective for the control and elimination of vivax malaria. Erythrocyte binding-like (EBL) protein family mem-bers s...

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Main Authors: Jin Hee Han, Jee Sun Cho, Jessica J.Y. Ong, Ji Hoon Park, Myat Htut Nyunt, Edwin Sutanto, Hidayat Trimarsanto, Beyene Petros, Abraham Aseffa, Sisay Getachew, Kanlaya Sriprawat, Nicholas M. Anstey, Matthew J. Grigg, Bridget E. Barber, Timothy William, Gao Qi, Yaobao Liu, Richard D. Pearson, Sarah Auburn, Ric N. Price, Francois Nosten, Laurent Rénia, Bruce Russell, Eun Taek Han
Other Authors: The Jenner Institute
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Published: 2020
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Medicine
Online Access:https://repository.li.mahidol.ac.th/handle/123456789/58114
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spelling th-mahidol.581142020-08-25T17:34:21Z Genetic diversity and neutral selection in Plasmodium vivax erythrocyte binding protein correlates with patient antigenicity Jin Hee Han Jee Sun Cho Jessica J.Y. Ong Ji Hoon Park Myat Htut Nyunt Edwin Sutanto Hidayat Trimarsanto Beyene Petros Abraham Aseffa Sisay Getachew Kanlaya Sriprawat Nicholas M. Anstey Matthew J. Grigg Bridget E. Barber Timothy William Gao Qi Yaobao Liu Richard D. Pearson Sarah Auburn Ric N. Price Francois Nosten Laurent Rénia Bruce Russell Eun Taek Han The Jenner Institute A-Star, Singapore Immunology Network Medical College of Soochow University Jiangsu Institute of Parasitic Diseases Armauer Hansen Research Institute Addis Ababa University Eijkman Institute for Molecular Biology Shoklo Malaria Research Unit Menzies School of Health Research University of Otago Mahidol University Nuffield Department of Medicine Wellcome Sanger Institute University of Oxford Medical Sciences Division Kangwon National University Gleneagles Hospital Infectious Diseases Society Sabah-Menzies School of Health Research Clinical Research Unit Queen Elizabeth Hospital Medicine © 2020 Han et al. Plasmodium vivax is the most widespread and difficult to treat cause of human malaria. The development of vaccines against the blood stages of P. vivax remains a key objective for the control and elimination of vivax malaria. Erythrocyte binding-like (EBL) protein family mem-bers such as Duffy binding protein (PvDBP) are of critical importance to erythrocyte invasion and have been the major target for vivax malaria vaccine development. In this study, we focus on another member of EBL protein family, P. vivax erythrocyte binding protein (PvEBP). PvEBP was first identified in Cambodian (C127) field isolates and has subse-quently been showed its preferences for binding reticulocytes which is directly inhibited by antibodies. We analysed PvEBP sequence from 316 vivax clinical isolates from eight coun-tries including China (n = 4), Ethiopia (n = 24), Malaysia (n = 53), Myanmar (n = 10), Papua New Guinea (n = 16), Republic of Korea (n = 10), Thailand (n = 174), and Vietnam (n = 25). PvEBP gene exhibited four different phenotypic clusters based on the insertion/deletion (indels) variation. PvEBP-RII (179–479 aa.) showed highest polymorphism similar to other EBL family proteins in various Plasmodium species. Whereas even though PvEBP-RIII-V (480–690 aa.) was the most conserved domain, that showed strong neutral selection pressure for gene purifying with significant population expansion. Antigenicity of both of PvEBP-RII (16.1%) and PvEBP-RIII-V (21.5%) domains were comparatively lower than other P. vivax antigen which expected antigens associated with merozoite invasion. Total IgG recognition level of PvEBP-RII was stronger than PvEBP-RIII-V domain, whereas total IgG inducing level was stronger in PvEBP-RIII-V domain. These results suggest that PvEBP-RII is mainly recognized by natural IgG for innate protection, whereas PvEBP-RIII-V stimulates IgG production activity by B-cell for acquired immunity. Overall, the low antigenic-ity of both regions in patients with vivax malaria likely reflects genetic polymorphism for strong positive selection in PvEBP-RII and purifying selection in PvEBP-RIII-V domain. These observations pose challenging questions to the selection of EBP and point out the importance of immune pressure and polymorphism required for inclusion of PvEBP as a vaccine candidate. 2020-08-25T10:34:21Z 2020-08-25T10:34:21Z 2020-07-01 Article PLoS Neglected Tropical Diseases. Vol.14, No.7 (2020), 1-16 10.1371/journal.pntd.0008202 19352735 19352727 2-s2.0-85087818951 https://repository.li.mahidol.ac.th/handle/123456789/58114 Mahidol University SCOPUS https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85087818951&origin=inward
institution Mahidol University
building Mahidol University Library
continent Asia
country Thailand
Thailand
content_provider Mahidol University Library
collection Mahidol University Institutional Repository
topic Medicine
spellingShingle Medicine
Jin Hee Han
Jee Sun Cho
Jessica J.Y. Ong
Ji Hoon Park
Myat Htut Nyunt
Edwin Sutanto
Hidayat Trimarsanto
Beyene Petros
Abraham Aseffa
Sisay Getachew
Kanlaya Sriprawat
Nicholas M. Anstey
Matthew J. Grigg
Bridget E. Barber
Timothy William
Gao Qi
Yaobao Liu
Richard D. Pearson
Sarah Auburn
Ric N. Price
Francois Nosten
Laurent Rénia
Bruce Russell
Eun Taek Han
Genetic diversity and neutral selection in Plasmodium vivax erythrocyte binding protein correlates with patient antigenicity
description © 2020 Han et al. Plasmodium vivax is the most widespread and difficult to treat cause of human malaria. The development of vaccines against the blood stages of P. vivax remains a key objective for the control and elimination of vivax malaria. Erythrocyte binding-like (EBL) protein family mem-bers such as Duffy binding protein (PvDBP) are of critical importance to erythrocyte invasion and have been the major target for vivax malaria vaccine development. In this study, we focus on another member of EBL protein family, P. vivax erythrocyte binding protein (PvEBP). PvEBP was first identified in Cambodian (C127) field isolates and has subse-quently been showed its preferences for binding reticulocytes which is directly inhibited by antibodies. We analysed PvEBP sequence from 316 vivax clinical isolates from eight coun-tries including China (n = 4), Ethiopia (n = 24), Malaysia (n = 53), Myanmar (n = 10), Papua New Guinea (n = 16), Republic of Korea (n = 10), Thailand (n = 174), and Vietnam (n = 25). PvEBP gene exhibited four different phenotypic clusters based on the insertion/deletion (indels) variation. PvEBP-RII (179–479 aa.) showed highest polymorphism similar to other EBL family proteins in various Plasmodium species. Whereas even though PvEBP-RIII-V (480–690 aa.) was the most conserved domain, that showed strong neutral selection pressure for gene purifying with significant population expansion. Antigenicity of both of PvEBP-RII (16.1%) and PvEBP-RIII-V (21.5%) domains were comparatively lower than other P. vivax antigen which expected antigens associated with merozoite invasion. Total IgG recognition level of PvEBP-RII was stronger than PvEBP-RIII-V domain, whereas total IgG inducing level was stronger in PvEBP-RIII-V domain. These results suggest that PvEBP-RII is mainly recognized by natural IgG for innate protection, whereas PvEBP-RIII-V stimulates IgG production activity by B-cell for acquired immunity. Overall, the low antigenic-ity of both regions in patients with vivax malaria likely reflects genetic polymorphism for strong positive selection in PvEBP-RII and purifying selection in PvEBP-RIII-V domain. These observations pose challenging questions to the selection of EBP and point out the importance of immune pressure and polymorphism required for inclusion of PvEBP as a vaccine candidate.
author2 The Jenner Institute
author_facet The Jenner Institute
Jin Hee Han
Jee Sun Cho
Jessica J.Y. Ong
Ji Hoon Park
Myat Htut Nyunt
Edwin Sutanto
Hidayat Trimarsanto
Beyene Petros
Abraham Aseffa
Sisay Getachew
Kanlaya Sriprawat
Nicholas M. Anstey
Matthew J. Grigg
Bridget E. Barber
Timothy William
Gao Qi
Yaobao Liu
Richard D. Pearson
Sarah Auburn
Ric N. Price
Francois Nosten
Laurent Rénia
Bruce Russell
Eun Taek Han
format Article
author Jin Hee Han
Jee Sun Cho
Jessica J.Y. Ong
Ji Hoon Park
Myat Htut Nyunt
Edwin Sutanto
Hidayat Trimarsanto
Beyene Petros
Abraham Aseffa
Sisay Getachew
Kanlaya Sriprawat
Nicholas M. Anstey
Matthew J. Grigg
Bridget E. Barber
Timothy William
Gao Qi
Yaobao Liu
Richard D. Pearson
Sarah Auburn
Ric N. Price
Francois Nosten
Laurent Rénia
Bruce Russell
Eun Taek Han
author_sort Jin Hee Han
title Genetic diversity and neutral selection in Plasmodium vivax erythrocyte binding protein correlates with patient antigenicity
title_short Genetic diversity and neutral selection in Plasmodium vivax erythrocyte binding protein correlates with patient antigenicity
title_full Genetic diversity and neutral selection in Plasmodium vivax erythrocyte binding protein correlates with patient antigenicity
title_fullStr Genetic diversity and neutral selection in Plasmodium vivax erythrocyte binding protein correlates with patient antigenicity
title_full_unstemmed Genetic diversity and neutral selection in Plasmodium vivax erythrocyte binding protein correlates with patient antigenicity
title_sort genetic diversity and neutral selection in plasmodium vivax erythrocyte binding protein correlates with patient antigenicity
publishDate 2020
url https://repository.li.mahidol.ac.th/handle/123456789/58114
_version_ 1763495073571405824

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