International Journal of Infectious Diseases (Feb 2021)

CCR5 inhibition in critical COVID-19 patients decreases inflammatory cytokines, increases CD8 T-cells, and decreases SARS-CoV2 RNA in plasma by day 14

  • Bruce K. Patterson,
  • Harish Seethamraju,
  • Kush Dhody,
  • Michael J. Corley,
  • Kazem Kazempour,
  • Jay Lalezari,
  • Alina P.S. Pang,
  • Christopher Sugai,
  • Eisa Mahyari,
  • Edgar B. Francisco,
  • Amruta Pise,
  • Hallison Rodrigues,
  • Helen L. Wu,
  • Gabriela M. Webb,
  • Byung S. Park,
  • Scott Kelly,
  • Nader Pourhassan,
  • Alina Lelic,
  • Lama Kdouh,
  • Monica Herrera,
  • Eric Hall,
  • Benjamin N. Bimber,
  • Matthew Plassmeyer,
  • Raavi Gupta,
  • Oral Alpan,
  • Jane A. O’Halloran,
  • Philip A. Mudd,
  • Enver Akalin,
  • Lishomwa C. Ndhlovu,
  • Jonah B. Sacha

Journal volume & issue
Vol. 103
pp. 25 – 32

Abstract

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Objective: Infection with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is now a global pandemic. Emerging results indicate a dysregulated immune response. Given the role of CCR5 in immune cell migration and inflammation, we investigated the impact of CCR5 blockade via the CCR5-specific antibody leronlimab on clinical, immunological, and virological parameters in severe COVID-19 patients. Methods: In March 2020, 10 terminally ill, critical COVID-19 patients received two doses of leronlimab via individual emergency use indication. We analyzed changes in clinical presentation, immune cell populations, inflammation, as well as SARS-CoV-2 plasma viremia before and 14 days after treatment. Results: Over the 14-day study period, six patients survived, two were extubated, and one discharged. We observed complete CCR5 receptor occupancy in all donors by day 7. Compared with the baseline, we observed a concomitant statistically significant reduction in plasma IL-6, restoration of the CD4/CD8 ratio, and resolution of SARS-CoV2 plasma viremia (pVL). Furthermore, the increase in the CD8 percentage was inversely correlated with the reduction in pVL (r = −0.77, p = 0.0013). Conclusions: Our study design precludes clinical efficacy inferences but the results implicate CCR5 as a therapeutic target for COVID-19 and they form the basis for ongoing randomized clinical trials.

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