Severe Clade I (subclade Ib) mpox in advanced HIV complicated by multidrug-resistant bacterial superinfection and ocular involvement: A case report from Uganda
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Background: Mpox in people living with HIV (PLHIV) with advanced immunosuppression is poorly understood in sub-Saharan Africa, where high HIV prevalence intersects with limited access to mpox-specific antivirals. Urgent evidence is needed to guide clinical management and improve outcomes for this vulnerable population in resource-limited outbreak settings. Case presentation: We report a 30-year-old Ugandan man with advanced HIV (CD4 55 cells/µL, HIV-1 RNA 645,000 copies/mL) who presented with two weeks of disseminated mucocutaneous disease, circumferential necrotic penile ulceration with severe dysuria, and periocular involvement. Mpox was confirmed by real-time PCR from multiple anatomical sites, with sequencing identifying Clade I (subclade Ib) infection. Longitudinal sampling showed persistently low Ct values in skin and genital lesions despite rising salivary Ct values, indicating differential compartmental viral clearance. Serial pus cultures from ulcerated lesions yielded multi-resistant gram-negative bacilli and coagulase-negative staphylococci, initially resistant to first-line agents. Later isolates showed susceptibility to meropenem and intermittently ciprofloxacin, possibly reflecting organism turnover. Management & Outcome: Empirical ceftriaxone and metronidazole proved ineffective. Culture-guided escalation to intravenous meropenem, along with intensive wound care, pain management, ocular prophylaxis, and resumption of antiretroviral therapy (ART), resulted in gradual clinical improvement. The patient was discharged after four weeks with healed skin lesions and mild residual ocular discomfort. At three months, immune reconstitution was observed (CD4 173 cells/µL; HIV-1 RNA 72 copies/mL) with complete functional recovery. Conclusions: Severe Clade Ib (subclade Ib) mpox in advanced HIV can present with genital necrosis, ocular involvement, persistent lesion-site viral burden, and multidrug-resistant bacterial superinfection. Even in the absence of specific antivirals, favourable outcomes can be achieved through integrated HIV care, early culture-guided antimicrobial stewardship, and proactive ocular management.