Metagenomic sequencing of mpox virus clade Ib lesions identifies possible bacterial and viral co-infections in hospitalized patients in eastern DRC

Leonard Schuele; Leandre Murhula Masirika; Hayley Cassidy; Philip T. L. C. Clausen; Luca M. Zaeck; Marjan Boter; Pacifique Ndishimye; Jean Claude Udahemuka; Rory D. de Vries; Saria Otani; Richard Molenkamp; David F. Nieuwenhuijse; Justin Bengehya Mbiribindi; Freddy Belesi Siangoli; Marion Koopmans; Frank M. Aarestrup; Bas B. Oude Munnink

doi:10.1128/spectrum.00512-25

Metagenomic sequencing of mpox virus clade Ib lesions identifies possible bacterial and viral co-infections in hospitalized patients in eastern DRC

Leonard Schuele, Leandre Murhula Masirika^*, Hayley Cassidy, Philip T. L. C. Clausen, Luca M. Zaeck, Marjan Boter, Pacifique Ndishimye, Jean Claude Udahemuka, Rory D. de Vries, Saria Otani, Richard Molenkamp, David F. Nieuwenhuijse, Justin Bengehya Mbiribindi, Freddy Belesi Siangoli, Marion Koopmans, Frank M. Aarestrup, Bas B. Oude Munnink^*

^*Corresponding author for this work

Research output: Contribution to journal › Journal article › Research › peer-review

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Abstract

Mpox is an emerging zoonotic disease that caused two public health emergencies of international concern within two years. Less is known about the interplay of microbial organisms in mpox lesions which could result in superinfections that exacerbate outcomes or delay recovery. We utilized a unified metagenomic sequencing approach involving slow-speed centrifugation and differential lysis on 19 mpox lesion swabs of hospitalized patients in South Kivu province (eastern DRC) to characterize bacteria, antimicrobial resistance genes, mpox virus (MPXV), and viral co-infections. High-quality MPXV whole-genome sequences were obtained until a Ct value of 27. Furthermore, co-infections with other clinically relevant viruses, such as varicella zoster virus and herpes simplex virus-2, were detected and confirmed by real-time PCR. In addition, metagenomic sequence analysis of the bacterial content showed the presence of bacteria associated with skin and soft tissue infection in 10 of the 19 samples analyzed. These bacteria had a high abundance of resistance genes, with possible implications for antimicrobial treatment based on the predicted antimicrobial resistance. In conclusion, we report the presence of bacterial and viral pathogens in mpox lesions and detection of widespread resistance genes to the standard antibiotic treatment. The possibility of a co-infection, including antimicrobial resistance, should be considered when discussing treatment options, along with the determination of the case-fatality ratio.

IMPORTANCE
The mpox virus clade Ib lineage emerged in the eastern Democratic Republic of the Congo owing to continuous human-to-human transmission in a vulnerable patient population. A major challenge of this ongoing outbreak is its occurrence in regions with severely limited healthcare infrastructure. As a result, less is known about co-infections in affected patients. Identifying and characterizing pathogens, including their antimicrobial resistance, is crucial for reducing infection-related complications and improving antimicrobial stewardship. In this study, we applied a unified metagenomics approach to detect and characterize bacterial and viral co-infections in mpox lesions of hospitalized mpox patients in the eastern DRC.

Original language	English
Article number	e0051225
Journal	Microbiology Spectrum
ISSN	2165-0497
DOIs	https://doi.org/10.1128/spectrum.00512-25
Publication status	Accepted/In press - 2025

Keywords

Mpox
Mpox virus
Clade Ib
Metagenomics
Antimicrobial resistance
Co-infections
Monkeypox virus

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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Schuele, L., Masirika, L. M., Cassidy, H., Clausen, P. T. L. C., Zaeck, L. M., Boter, M., Ndishimye, P., Udahemuka, J. C., de Vries, R. D., Otani, S., Molenkamp, R., Nieuwenhuijse, D. F., Mbiribindi, J. B., Siangoli, F. B., Koopmans, M., Aarestrup, F. M., & Oude Munnink, B. B. (Accepted/In press). Metagenomic sequencing of mpox virus clade Ib lesions identifies possible bacterial and viral co-infections in hospitalized patients in eastern DRC. Microbiology Spectrum, Article e0051225. https://doi.org/10.1128/spectrum.00512-25

@article{6906ca09a5724f02a956fa5af6b83abf,

title = "Metagenomic sequencing of mpox virus clade Ib lesions identifies possible bacterial and viral co-infections in hospitalized patients in eastern DRC",

abstract = "Mpox is an emerging zoonotic disease that caused two public health emergencies of international concern within two years. Less is known about the interplay of microbial organisms in mpox lesions which could result in superinfections that exacerbate outcomes or delay recovery. We utilized a unified metagenomic sequencing approach involving slow-speed centrifugation and differential lysis on 19 mpox lesion swabs of hospitalized patients in South Kivu province (eastern DRC) to characterize bacteria, antimicrobial resistance genes, mpox virus (MPXV), and viral co-infections. High-quality MPXV whole-genome sequences were obtained until a Ct value of 27. Furthermore, co-infections with other clinically relevant viruses, such as varicella zoster virus and herpes simplex virus-2, were detected and confirmed by real-time PCR. In addition, metagenomic sequence analysis of the bacterial content showed the presence of bacteria associated with skin and soft tissue infection in 10 of the 19 samples analyzed. These bacteria had a high abundance of resistance genes, with possible implications for antimicrobial treatment based on the predicted antimicrobial resistance. In conclusion, we report the presence of bacterial and viral pathogens in mpox lesions and detection of widespread resistance genes to the standard antibiotic treatment. The possibility of a co-infection, including antimicrobial resistance, should be considered when discussing treatment options, along with the determination of the case-fatality ratio.IMPORTANCE The mpox virus clade Ib lineage emerged in the eastern Democratic Republic of the Congo owing to continuous human-to-human transmission in a vulnerable patient population. A major challenge of this ongoing outbreak is its occurrence in regions with severely limited healthcare infrastructure. As a result, less is known about co-infections in affected patients. Identifying and characterizing pathogens, including their antimicrobial resistance, is crucial for reducing infection-related complications and improving antimicrobial stewardship. In this study, we applied a unified metagenomics approach to detect and characterize bacterial and viral co-infections in mpox lesions of hospitalized mpox patients in the eastern DRC.",

keywords = "Mpox, Mpox virus, Clade Ib, Metagenomics, Antimicrobial resistance, Co-infections, Monkeypox virus",

author = "Leonard Schuele and Masirika, \{Leandre Murhula\} and Hayley Cassidy and Clausen, \{Philip T. L. C.\} and Zaeck, \{Luca M.\} and Marjan Boter and Pacifique Ndishimye and Udahemuka, \{Jean Claude\} and \{de Vries\}, \{Rory D.\} and Saria Otani and Richard Molenkamp and Nieuwenhuijse, \{David F.\} and Mbiribindi, \{Justin Bengehya\} and Siangoli, \{Freddy Belesi\} and Marion Koopmans and Aarestrup, \{Frank M.\} and \{Oude Munnink\}, \{Bas B.\}",

year = "2025",

doi = "10.1128/spectrum.00512-25",

language = "English",

journal = "Microbiology Spectrum",

issn = "2165-0497",

publisher = "American Society for Microbiology",

}

Schuele, L, Masirika, LM, Cassidy, H, Clausen, PTLC, Zaeck, LM, Boter, M, Ndishimye, P, Udahemuka, JC, de Vries, RD, Otani, S, Molenkamp, R, Nieuwenhuijse, DF, Mbiribindi, JB, Siangoli, FB, Koopmans, M, Aarestrup, FM & Oude Munnink, BB 2025, 'Metagenomic sequencing of mpox virus clade Ib lesions identifies possible bacterial and viral co-infections in hospitalized patients in eastern DRC', Microbiology Spectrum. https://doi.org/10.1128/spectrum.00512-25

TY - JOUR

T1 - Metagenomic sequencing of mpox virus clade Ib lesions identifies possible bacterial and viral co-infections in hospitalized patients in eastern DRC

AU - Schuele, Leonard

AU - Masirika, Leandre Murhula

AU - Cassidy, Hayley

AU - Clausen, Philip T. L. C.

AU - Zaeck, Luca M.

AU - Boter, Marjan

AU - Ndishimye, Pacifique

AU - Udahemuka, Jean Claude

AU - de Vries, Rory D.

AU - Otani, Saria

AU - Molenkamp, Richard

AU - Nieuwenhuijse, David F.

AU - Mbiribindi, Justin Bengehya

AU - Siangoli, Freddy Belesi

AU - Koopmans, Marion

AU - Aarestrup, Frank M.

AU - Oude Munnink, Bas B.

PY - 2025

Y1 - 2025

N2 - Mpox is an emerging zoonotic disease that caused two public health emergencies of international concern within two years. Less is known about the interplay of microbial organisms in mpox lesions which could result in superinfections that exacerbate outcomes or delay recovery. We utilized a unified metagenomic sequencing approach involving slow-speed centrifugation and differential lysis on 19 mpox lesion swabs of hospitalized patients in South Kivu province (eastern DRC) to characterize bacteria, antimicrobial resistance genes, mpox virus (MPXV), and viral co-infections. High-quality MPXV whole-genome sequences were obtained until a Ct value of 27. Furthermore, co-infections with other clinically relevant viruses, such as varicella zoster virus and herpes simplex virus-2, were detected and confirmed by real-time PCR. In addition, metagenomic sequence analysis of the bacterial content showed the presence of bacteria associated with skin and soft tissue infection in 10 of the 19 samples analyzed. These bacteria had a high abundance of resistance genes, with possible implications for antimicrobial treatment based on the predicted antimicrobial resistance. In conclusion, we report the presence of bacterial and viral pathogens in mpox lesions and detection of widespread resistance genes to the standard antibiotic treatment. The possibility of a co-infection, including antimicrobial resistance, should be considered when discussing treatment options, along with the determination of the case-fatality ratio.IMPORTANCE The mpox virus clade Ib lineage emerged in the eastern Democratic Republic of the Congo owing to continuous human-to-human transmission in a vulnerable patient population. A major challenge of this ongoing outbreak is its occurrence in regions with severely limited healthcare infrastructure. As a result, less is known about co-infections in affected patients. Identifying and characterizing pathogens, including their antimicrobial resistance, is crucial for reducing infection-related complications and improving antimicrobial stewardship. In this study, we applied a unified metagenomics approach to detect and characterize bacterial and viral co-infections in mpox lesions of hospitalized mpox patients in the eastern DRC.

AB - Mpox is an emerging zoonotic disease that caused two public health emergencies of international concern within two years. Less is known about the interplay of microbial organisms in mpox lesions which could result in superinfections that exacerbate outcomes or delay recovery. We utilized a unified metagenomic sequencing approach involving slow-speed centrifugation and differential lysis on 19 mpox lesion swabs of hospitalized patients in South Kivu province (eastern DRC) to characterize bacteria, antimicrobial resistance genes, mpox virus (MPXV), and viral co-infections. High-quality MPXV whole-genome sequences were obtained until a Ct value of 27. Furthermore, co-infections with other clinically relevant viruses, such as varicella zoster virus and herpes simplex virus-2, were detected and confirmed by real-time PCR. In addition, metagenomic sequence analysis of the bacterial content showed the presence of bacteria associated with skin and soft tissue infection in 10 of the 19 samples analyzed. These bacteria had a high abundance of resistance genes, with possible implications for antimicrobial treatment based on the predicted antimicrobial resistance. In conclusion, we report the presence of bacterial and viral pathogens in mpox lesions and detection of widespread resistance genes to the standard antibiotic treatment. The possibility of a co-infection, including antimicrobial resistance, should be considered when discussing treatment options, along with the determination of the case-fatality ratio.IMPORTANCE The mpox virus clade Ib lineage emerged in the eastern Democratic Republic of the Congo owing to continuous human-to-human transmission in a vulnerable patient population. A major challenge of this ongoing outbreak is its occurrence in regions with severely limited healthcare infrastructure. As a result, less is known about co-infections in affected patients. Identifying and characterizing pathogens, including their antimicrobial resistance, is crucial for reducing infection-related complications and improving antimicrobial stewardship. In this study, we applied a unified metagenomics approach to detect and characterize bacterial and viral co-infections in mpox lesions of hospitalized mpox patients in the eastern DRC.

KW - Mpox

KW - Mpox virus

KW - Clade Ib

KW - Metagenomics

KW - Antimicrobial resistance

KW - Co-infections

KW - Monkeypox virus

U2 - 10.1128/spectrum.00512-25

DO - 10.1128/spectrum.00512-25

M3 - Journal article

C2 - 40445195

SN - 2165-0497

JO - Microbiology Spectrum

JF - Microbiology Spectrum

M1 - e0051225

ER -

Metagenomic sequencing of mpox virus clade Ib lesions identifies possible bacterial and viral co-infections in hospitalized patients in eastern DRC

Abstract

Keywords

UN SDGs

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