Emerging Infectious Diseases (Dec 2023)

Tecovirimat Resistance in Mpox Patients, United States, 2022–2023

  • Todd G. Smith,
  • Crystal M. Gigante,
  • Nhien T. Wynn,
  • Audrey Matheny,
  • Whitni Davidson,
  • Yong Yang,
  • Rene Edgar Condori,
  • Kyle O’Connell,
  • Lynsey Kovar,
  • Tracie L. Williams,
  • Yon C. Yu,
  • Brett W. Petersen,
  • Nicolle Baird,
  • David Lowe,
  • Yu Li,
  • Panayampalli S. Satheshkumar,
  • Christina L. Hutson

DOI
https://doi.org/10.3201/eid2912.231146
Journal volume & issue
Vol. 29, no. 12
pp. 2426 – 2432

Abstract

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During the 2022 multinational outbreak of monkeypox virus (MPXV) infection, the antiviral drug tecovirimat (TPOXX; SIGA Technologies, Inc., https://www.siga.com) was deployed in the United States on a large scale for the first time. The MPXV F13L gene homologue encodes the target of tecovirimat, and single amino acid changes in F13 are known to cause resistance to tecovirimat. Genomic sequencing identified 11 mutations previously reported to cause resistance, along with 13 novel mutations. Resistant phenotype was determined using a viral cytopathic effect assay. We tested 124 isolates from 68 patients; 96 isolates from 46 patients were found to have a resistant phenotype. Most resistant isolates were associated with severely immunocompromised mpox patients on multiple courses of tecovirimat treatment, whereas most isolates identified by routine surveillance of patients not treated with tecovirimat remained sensitive. The frequency of resistant viruses remains relatively low (<1%) compared with the total number of patients treated with tecovirimat.

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