Genomic epidemiology of the rotavirus G2P[4] strains in coastal Kenya pre- and post-rotavirus vaccine introduction, 2012–8

Author:

Makori Timothy O12ORCID,Bargul Joel L23ORCID,Lambisia Arnold W1ORCID,Mwanga Mike J1,Murunga Nickson1,de Laurent Zaydah R1,Lewa Clement S1,Mutunga Martin1,Kellam Paul45,Cotten Matthew67ORCID,Nokes D James18ORCID,Phan My67ORCID,Agoti Charles N19ORCID

Affiliation:

1. Epidemiology and Demography Department Kenya Medical Research Institute (KEMRI)-Wellcome Trust Research Programme, Off Hospital Road, P.O BOX 230-80108, Kilifi, Kenya

2. Department of Biochemistry, Jomo Kenyatta University of Agriculture and Technology , Kalimoni, PO Box 62000-00200, Juja, Kenya

3. International Centre of Insect Physiology and Ecology, Animal Health Theme , ICIPE Road Kasarani, P.O BOX 30772-00100, Nairobi, Kenya

4. Department of Infectious Diseases, Faculty of Medicine, Imperial College London , Exhibition Road, London SW7 2AZ, UK

5. Kymab Ltd , The Bennet Building (B930), Babraham Research Campus, Cambridge CB22 3AT, UK

6. Medical Research Centre (MRC)/Uganda Virus Research Institute , Plot No: 51-59 Nakiwogo Road, P.O.Box 49, Entebbe, Uganda

7. MRC-University of Glasgow, Centre for Virus Research Glasgow , 464 Bearsden Road, Glasgow G61 1QH UK

8. School of Life Sciences and Zeeman Institute (SBIDER), The University of Warwick , Gibbet Hill Campus, Coventry CV4 7AL, UK

9. School of Health and Human Sciences, Pwani University , Kilifi-Malindi Road, P.O BOX 195-80108, Kilifi, Kenya

Abstract

Abstract The introduction of rotavirus vaccines into the national immunization programme in many countries has led to a decline in childhood diarrhoea disease burden. Coincidentally, the incidence of some rotavirus group A (RVA) genotypes has increased, which may result from non-vaccine-type replacement. Here, we investigate the evolutionary genomics of rotavirus G2P[4] which has shown an increase in countries that introduced the monovalent Rotarix® vaccine. We examined sixty-three RVA G2P[4] strains sampled from children (aged below 13 years) admitted to Kilifi County Hospital, coastal Kenya, pre- (2012 to June 2014) and post-(July 2014 to 2018) rotavirus vaccine introduction. All the sixty-three genome sequences showed a typical DS-1-like genome constellation (G2-P[4]-I2-R2-C2-M2-A2-N2-T2-E2-H2). Pre-vaccine G2 sequences predominantly classified as sub-lineage IVa-3 and co-circulated with low numbers of sub-lineage IVa-1 strains, whereas post-vaccine G2 sequences mainly classified into sub-lineage IVa-3. In addition, in the pre-vaccine period, P[4] sub-lineage IVa strains co-circulated with low numbers of P[4] lineage II strains, but P[4] sub-lineage IVa strains predominated in the post-vaccine period. On the global phylogeny, the Kenyan pre- and post-vaccine G2P[4] strains clustered separately, suggesting that different virus populations circulated in the two periods. However, the strains from both periods exhibited conserved amino acid changes in the known antigenic epitopes, suggesting that replacement of the predominant G2P[4] cluster was unlikely a result of immune escape. Our findings demonstrate that the pre- and post-vaccine G2P[4] strains circulating in Kilifi, coastal Kenya, differed genetically but likely were antigenically similar. This information informs the discussion on the consequences of rotavirus vaccination on rotavirus diversity.

Funder

Wellcome Trust

Initiative to Develop African Research Leaders (IDeAL) through the DELTAS Africa Initiative

Publisher

Oxford University Press (OUP)

Subject

Virology,Microbiology

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