Clinical Characteristics and Outcomes of Patients With Mpox Who Received Tecovirimat in a New York City Health System

Author:

Vo Christopher1ORCID,Zomorodi Rustin1,Silvera Richard1,Bartram Logan1,Lugo Luz Amarilis1,Kojic Erna2,Urbina Antonio1,Aberg Judith1,Sigel Keith1ORCID,Chasan Rachel1,Patel Gopi1

Affiliation:

1. Division of Infectious Diseases, Department of Medicine, Icahn School of Medicine at Mount Sinai , NewYork, New York , USA

2. Division of Infectious Diseases, Department of Medicine, Landspítali University Hospital , Reykjavík , Iceland

Abstract

Abstract Background The 2022 global mpox outbreak was notable for transmission between persons outside of travel and zoonotic exposures and primarily through intimate contact. An understanding of the presentation of mpox in people with human immunodeficiency virus (HIV) and other immunocompromising conditions and knowledge of the efficacy of tecovirimat continue to evolve. Methods This retrospective study describes clinical features and outcomes of persons with mpox who received tecovirimat. Data were obtained via medical record review of patients prescribed tecovirimat in a health system in New York City during the height of the outbreak in 2022. Results One hundred thirty people received tecovirimat between 1 July and 1 October 2022. People with HIV (n = 80) experienced similar rates of recovery, bacterial superinfections, and hospitalization compared to patients without immunocompromising conditions. Individuals determined to be severely immunocompromised (n = 14) had a higher risk of hospitalization than those without severe immunocompromise (cohort inclusive of those with well-controlled HIV, excluding those without virologic suppression, n = 101): 50% versus 9% (P < .001). Hospitalized patients (n = 18 [13% of total]) were primarily admitted for bacterial superinfections (44.4%), with a median hospital stay of 4 days. Of those who completed follow-up (n = 85 [66%]), 97% had recovery of lesions at time of posttreatment assessment. Tecovirimat was well tolerated; there were no reported severe adverse events attributed to therapy. Conclusions There were no significant differences in outcomes between people with HIV when evaluated as a whole and patients without immunocompromising conditions. However, mpox infection was associated with higher rates of hospitalization in those with severe immunocompromise, including patients with HIV/AIDS. Treatment with tecovirimat was well tolerated. Key Points: In our mpox cohort, people with HIV had similar rates of recovery and complications as those without HIV or other immunocompromising conditions. Severe immunocompromise was associated with a higher hospitalization rate. Tecovirimat was well tolerated, with minimal side effects.

Publisher

Oxford University Press (OUP)

Subject

Infectious Diseases,Oncology

Reference39 articles.

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3. Human monkeypox—Kasai Oriental, Democratic Republic of Congo, February 1996 October 1997;Aplogan;J Am Med Assoc,1998

4. Emergence of monkeypox—West and Central Africa, 1970–2017;Durski;MMWR Morb Mortal Wkly Rep,2018

5. Epidemiology of human mpox—worldwide, 2018–2021;McCollum;MMWR Morb Mortal Wkly Rep,2023

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