Clade I Mpox virus genomic diversity in the Democratic Republic of the Congo, 2018 - 2024: Predominance of Zoonotic Transmission

Author:

Kinganda-Lusamaki EddyORCID,Amuri-Aziza AdrienneORCID,Fernandez NicolasORCID,Makangara-Cigolo Jean-ClaudeORCID,Pratt CatherineORCID,Hasivirwe Vakaniaki EmmanuelORCID,Hoff Nicole A.ORCID,Luakanda Gradi,Akil-Bandali Prince,Sabiti Nundu SabinORCID,Mulopo-Mukanya Noella,Ngimba Michel,Modadra-Madakpa Brigitte,Diavita Ruth,Paku Princesse,Pukuta-Simbu Elisabeth,Merritt SydneyORCID,O’Toole Áine,Low NicolaORCID,Nkuba-Ndaye Antoine,Kavunga-Membo HugoORCID,Shongo Robert,Liesenborghs LaurensORCID,Wawina-Bokalanga TonyORCID,Vercauteren KoenORCID,Mukadi-Bamuleka DanielORCID,Subissi LorenzoORCID,Muyembe Jean-JacquesORCID,Kindrachuk JasonORCID,Ayouba Ahidjo,Rambaut Andrew,Delaporte EricORCID,Tessema SofoniasORCID,D’Ortenzio EricORCID,Rimoin Anne W.ORCID,Hensley Lisa E.ORCID,Mbala-Kingebeni PlacideORCID,Peeters MartineORCID,Ahuka-Mundeke Steve

Abstract

ABSTRACTBackgroundRecent reports raise concerns on the changing epidemiology of mpox in the Democratic Republic of the Congo (DRC), with increasing case counts, sexual contact-mediated clusters, and sustained human-to-human transmission driven by a novel monkeypox virus (MPXV) subclade, clade Ib. However, only a limited number of clade I MPXV genomes have been characterized so far, from a limited number of regions.MethodsWe conducted whole genome sequencing of 603 mpox-positive samples that were collected from 581 patients between 2018-2024 in 17 of the 26 provinces of the DRC.ResultsGenome coverage was at least 70% for 429/603 (71.1%) samples and near full-length MPXV genomes (>90% coverage) were obtained for 348/603 (57.7%) samples from 337 patients. All newly generated MPXV sequences belonged to clade I, among which 17 were clade Ib strains, all from patients infected in 2024 in the South-Kivu province. The large majority (>95%) of the new strains fall within previously described clade Ia groups and potential new groups have also been observed. The low number of APOBEC3 mutations found among clade Ia suggests that most human mpox cases are probably linked to zoonotic transmissions. Genetically diverse MPXV lineages co-circulate in small geographic areas during the same outbreak suggesting multiple zoonotic introductions over a short period from one or multiple reservoir species. Recent identification of mpox cases in Kinshasa shows that multiple lineages circulate in a large urban center, indicating separate introduction events.ConclusionThe mpox epidemic in the DRC exhibits two distinct patterns. In traditional endemic regions, the epidemic is predominated by zoonotic spill-over events involving clade Ia. Conversely, in the eastern part of the country, the clade Ib outbreak is driven by human-to-human transmission highlighting the need for a coordinated response effort at the national, regional and international levels.

Publisher

Cold Spring Harbor Laboratory

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