Reticulocyte Binding Protein Homologue 5 is a target of balancing selection in the Plasmodium falciparum population of Papua New Guinea

Myo T Naung; Elijah Martin; Wilson Wong; Zahra Razook; Digjaya Utama; Andrew J Guy; Shannon Takala Harrison; Alan F Cowman; Enmoore Lin; Benson Kiniboro; Moses Laman; Ivo Mueller; Alyssa E Barry

doi:10.3389/fpara.2023.1288867

Reticulocyte Binding Protein Homologue 5 is a target of balancing selection in the Plasmodium falciparum population of Papua New Guinea

Front Parasitol. 2023 Dec 22:2:1288867. doi: 10.3389/fpara.2023.1288867. eCollection 2023.

Authors

Myo T Naung^{1

2

3

4}, Elijah Martin¹, Wilson Wong^{1

2}, Zahra Razook¹, Digjaya Utama^{1

2}, Andrew J Guy⁵, Shannon Takala Harrison⁶, Alan F Cowman^{1

2}, Enmoore Lin⁷, Benson Kiniboro⁷, Moses Laman⁷, Ivo Mueller^{1

2

8}, Alyssa E Barry^{1

2

3

4}

Affiliations

¹ Population Health and Immunity Division, Walter and Eliza Hall Institute of Medical Research, Parkville, VIC, Australia.
² Department of Medical Biology, University of Melbourne, Carlton, VIC, Australia.
³ Centre for Innovation in Infectious Diseases and Immunology Research (CIIDIR), Institute of Mental and Physical Health and Clinical Translation (IMPACT) and School of Medicine, Deakin University, Geelong, VIC, Australia.
⁴ Disease Elimination and Maternal and Child Health, Burnet Institute, Melbourne, VIC, Australia.
⁵ Bioscience and Food Technology, RMIT University, Melbourne, VIC, Australia.
⁶ Center for Vaccine Development and Global Health, University of Maryland School of Medicine, Baltimore, MD, United States.
⁷ Vector Borne Diseases Unit, Papua New Guinea Institute of Medical Research, Madang, Papua New Guinea.
⁸ Parasites and Insect Vectors, Pasteur Institute, Paris, France.

Abstract

Plasmodium falciparum Reticulocyte Binding Protein Homologue (RH5), a leading malaria vaccine candidate, is essential for erythrocyte invasion by the parasite, interacting with the human host receptor, basigin. RH5 has a small number of polymorphisms relative to other blood-stage antigens, and in vitro studies have shown that vaccine-induced antibodies raised against RH5 are strain-transcending, however most studies investigating RH5 diversity have been done in Africa. Understanding the genetic diversity and evolution of malaria antigens in other regions is important for their validation as vaccine candidates. In this study the rh5 gene was sequenced in 677 samples from a longitudinal cohort of Papua New Guinean (PNG) children aged 1-3 years. Of 677 samples successfully sequenced, 566 were identified as independent infections (i.e. one of each pair of identical sequences within hosts were removed). A total of 14 non-synonymous polymorphisms were identified, eight that are 'common' in the population (minor allele frequency > 1%), with 44 haplotypes ranging in frequency from 1% to 21%. Modeling of common SNPs to the cryo-EM structure of the RH5/CyRPA/RIPR complex mapped them to the Basigin binding site and near the contact point of CyRPA. Tajima's D analyses of the corresponding nucleotide sequences produced positive values indicating potential hotspots of balancing selection. We attempted to confirm whether these signals were due to immune selection by measuring the rate of polymorphism between independent infections within the same host, and the association with clinical symptoms, however, no such associations were identified. Together these results suggest that while there is evidence of balancing selection driving RH5 diversity in the PNG P. falciparum population, immune escape was not observed within the cohort of young children. Limited immunity and therefore low selective pressure may explain this result, alternatively other evolutionary forces may contribute to balancing selection at the RH5-BSG binding interface in PNG.

Keywords: Plasmodium falciparum; RH5; haplotypes; immune escape; malaria; polymorphisms; vaccine.

Grants and funding

The author(s) declare financial support was received for the research, authorship, and/or publication of this article. The genetic analysis of samples was funded by a Project Grant awarded to AB by the National Health and Medical Research Council (NHMRC) of Australia (GNT1161066). IM was supported by an Investigator Grant from the NHMRC, MN was supported by a University of Melbourne Postgraduate Award. The authors acknowledge the Victorian State Government Operational Infrastructure Support and Australian Government NHMRC Independent Research Institute Infrastructure Support Scheme (IRIISS).