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Clade I Mpox Virus Genomic Diversity in the Democratic Republic of the Congo, 2018-2024: Predominance of Zoonotic Transmission

Overview
Journal Cell
Publisher Cell Press
Specialty Cell Biology
Date 2024 Oct 25
PMID 39454573
Authors
Eddy Kinganda-Lusamaki
Adrienne Amuri-Aziza
Nicolas Fernandez-Nunez
Jean-Claude Makangara-Cigolo
Catherine Pratt
Emmanuel Hasivirwe Vakaniaki
Nicole A Hoff
Gradi Luakanda-Ndelemo
Prince Akil-Bandali
Sabin Sabiti Nundu
Noella Mulopo-Mukanya
Michel Ngimba
Brigitte Modadra-Madakpa
Ruth Diavita
Princesse Paku-Tshambu
Elisabeth Pukuta-Simbu
Sydney Merritt
Aine OToole
Nicola Low
Antoine Nkuba-Ndaye
Hugo Kavunga-Membo
Robert Shongo Lushima
Laurens Liesenborghs
Tony Wawina-Bokalanga
Koen Vercauteren
Daniel Mukadi-Bamuleka
Lorenzo Subissi
Jean-Jacques Muyembe-Tamfum
Jason Kindrachuk
Ahidjo Ayouba
Andrew Rambaut
Eric Delaporte
Sofonias Tessema
Eric DOrtenzio
Anne W Rimoin
Lisa E Hensley
Placide Mbala-Kingebeni
Martine Peeters
Steve Ahuka-Mundeke
Affiliations
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Abstract

Recent reports raise concerns on the changing epidemiology of mpox in the Democratic Republic of the Congo (DRC). High-quality genomes were generated for 337 patients from 14/26 provinces to document whether the increase in number of cases is due to zoonotic spillover events or viral evolution, with enrichment of APOBEC3 mutations linked to human adaptation. Our study highlights two patterns of transmission contributing to the source of human cases. All new sequences from the eastern South Kivu province (n = 17; 4.8%) corresponded to the recently described clade Ib, associated with sexual contact and sustained human-to-human transmission. By contrast, all other genomes are clade Ia, which exhibits high genetic diversity with low numbers of APOBEC3 mutations compared with clade Ib, suggesting multiple zoonotic introductions. The presence of multiple clade I variants in urban areas highlights the need for coordinated international response efforts and more studies on the transmission and the reservoir of mpox.

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