Inefficient tissue immune response against MPXV in an immunocompromised mpox patient

Author:

Matschke Jakob1,Hartmann Kristin12,Pfefferle Susanne3,Wang Yue1,Valdes Pablo A.45,Thies Edda1,Schweizer Michaela6,Lütgehetmann Marc3,Schmiedel Stefan7,Bernreuther Christian8,Boyden Edward S.910,Glatzel Markus1,Krasemann Susanne12ORCID

Affiliation:

1. Institute of Neuropathology University Medical Center Hamburg‐Eppendorf Hamburg Germany

2. Core Facility for (Mouse) Pathology University Medical Center Hamburg‐Eppendorf Hamburg Germany

3. Institute for Medical Microbiology, Virology and Hygiene University Medical Center Hamburg‐Eppendorf Hamburg Germany

4. Departments of Neurosurgery and Neurobiology University of Texas Medical Branch Galveston Texas USA

5. Department of Electrical and Computer Engineering Rice University Houston Texas USA

6. Morphology and Electron Microscopy Core Facility, Center for Molecular Neurobiology (ZMNH) University Medical Center Hamburg‐Eppendorf Hamburg Germany

7. Division of Infectious Diseases, I. Department of Internal Medicine University Medical Center Hamburg‐Eppendorf Hamburg Germany

8. Institute of Pathology University Medical Center Hamburg‐Eppendorf Hamburg Germany

9. MIT Cambridge Massachusetts USA

10. Howard Hughes Medical Center Cambridge Massachusetts USA

Abstract

AbstractThe recent outbreak of monkeypox virus (MPXV) was unprecedented in its size and distribution. Those living with uncontrolled HIV and low CD4 T cell counts might develop a fulminant clinical mpox course with increased mortality, secondary infections, and necrotizing lesions. Fatal cases display a high and widespread MPXV tissue burden. The underlying pathomechanisms are not fully understood. We report here the pathological findings of an MPXV‐driven abscess in gastrocnemius muscle requiring surgery in an immunocompromised patient with severe mpox. Presence of virus particles and infectivity were confirmed by electron microscopy, expansion microscopy, and virus culture, respectively. MPXV tissue distribution by immunohistochemistry (IHC) showed a necrotic core with infection of different cell types. In contrast, at the lesion rim fibroblasts were mainly infected. Immune cells were almost absent in the necrotic core, but were abundant at the infection rim and predominantly macrophages. Further, we detected high amounts of alternatively activated GPNMB+‐macrophages at the lesion border. Of note, macrophages only rarely colocalized with virus‐infected cells. Insufficient clearance of infected cells and infection of lesion‐associated fibroblasts sustained by the abundance of profibrotic macrophages might lead to the coalescing of lesions and the severe and persistent clinical mpox course observed in immunocompromised patients.

Publisher

Wiley

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