C reactive protein utilisation, a biomarker for early COVID-19 treatment, improves lenzilumab efficacy: results from the randomised phase 3 'LIVE-AIR' trial

Zelalem Temesgen; Colleen F Kelley; Frank Cerasoli; Adrian Kilcoyne; Dale Chappell; Cameron Durrant; Omar Ahmed; Gabrielle Chappell; Victoria Catterson; Christopher Polk; Andrew Badley; Vincent C Marconi; LIVE-AIR Study Group

doi:10.1136/thoraxjnl-2022-218744

C reactive protein utilisation, a biomarker for early COVID-19 treatment, improves lenzilumab efficacy: results from the randomised phase 3 'LIVE-AIR' trial

Thorax. 2023 Jun;78(6):606-616. doi: 10.1136/thoraxjnl-2022-218744. Epub 2022 Jul 6.

Authors

Collaborators

LIVE-AIR Study Group:
Meghan Lewis, Linda Sher, Michael Bowdish, Noah Wald-Dickler, Subarna Biswas, Lydia Lam, Khang Vo, Roy Poblete, May M Lee, Douglass Hutcheon, Zelalem Temesgen, Andrew D Badley, Charles D Burger, Claudia R Libertin, F L Jacksonville, Jason Baker, William S Aronstein, Cameron Durrant, Dale Chappell, Omar Ahmed, Gabrielle Chappel, Robert Orenstein, Roberto Patron, Vincent C Marconi, Colleen F Kelley, John Gharbin, Caitlin Moran, Sheetal Kandiah, Valeria Cantos, Paulina Rebolledo, Carlos Del Rio, Jeffrey Lennox, Carmen Polito, Paulina Rebolledo, Anandi Sheth, Anup Patel, Homero Paniagua, Seife Yohannes, Alpesh Amin, Richard Lee, Miki Watanabe, Lanny Hsieh, Martin Cearras, Amay Parikh, Jason Sniffen, Wilfred Onyia, Christopher Polk, Michael Boger, Lisa Davidson, Kiran Gajurel, Michael Leonard, Lewis McCurdy, Nestor Quezada, Mindy Sampson, Zainab Shahid, Stephanie Strollo, David Weinrib, Sara Zulfigar, Cheryl McDonald, John Hollingsworth, John Burk, Joshua Berg, Daniel Barbaro, Andrew Miller, Lakshmi Sambathkumar, Stuart McDonald, Obinna Okoye, Juan Pulido, Jennifer Fulton, William Gill, Richard Zuckerman, Lionel Lewis, Chaitanya Mandapakala, Matthew Robinson, Brian Metzger, Maqsood Alam, Chrisoula Politis, Anne Frosch, Linh Ngo, Fernando Carvalho Neuenschwander, Estevão Figueiredo, Gualter Cançado, Gustavo Araujo, Lucas Guimarães, Ricardo Diaz, Natalia Bacellar, Celso Silva, Paulo Ferreira, Marina Andrade Lima, Caroline UberGhisi, Camila Anton, Ricardo Albaneze, Daniel Wagner de Castro Lima Santos, Ana Caroline Iglessias, Marianna Lago, Paula Pietrobom, Maysa Alves, Juvencio José Duailibe Furtado, Leopoldo Trevelin, Valeria Telles, Francini Correa, Fabiano Ramos, Marina de A R Da Silva, Rebeca C Lacerda Garcia, Ana Elizabeth G Maldonado, Ana Carolina M Beheregaray, Ana Maria T Ortiz, Kleber Luz, Eveline Pipolo Milan, Janine Soaresde Castro, Matheus José Barbosa Moreira, Renata Bezerra Onofre, Tácito do Nascimento Jácome, Victor Barreto Garcia, Victor Matheus Rolimde Souza, Felipe Dal Pizzol, Cristiane Ritter, Marcelo B Vinhas, Adilson Joaquim Westheimer Cavalcante, Julia Minghini, Loni Dorigo, Marina Salgado Miranda, Martti Anton Antila, Rebeca Brugnolli, Henrikki Antila

Affiliations

¹ Division of Infectious Diseases, Mayo Clinic, Rochester, Minnesota, USA temesgen.zelalem@mayo.edu.
² Division of Infectious Diseases, Emory University School of Medicine, Grady Memorial Hospital, Atlanta, Georgia, USA.
³ Medical Affairs, Rx Medical Dynamics, LLC, New York, New York, USA.
⁴ Humanigen Inc, Burlingame, California, USA.
⁵ BioSymetrics, Inc, New York, New York, USA.
⁶ Infectious Disease, Atrium Health, Charlotte, North Carolina, USA.
⁷ Division of Infectious Diseases, Mayo Clinic, Rochester, Minnesota, USA.
⁸ Division of Infectious Disease, Emory University School of Medicine, Rollins School of Public Health, and Emory Vaccine Center, Atlanta, Georgia, USA.

Abstract

Objective: COVID-19 severity is correlated with granulocyte macrophage colony-stimulating factor (GM-CSF) and C reactive protein (CRP) levels. In the phase three LIVE-AIR trial, lenzilumab an anti-GM-CSF monoclonal antibody, improved the likelihood of survival without ventilation (SWOV) in COVID-19, with the greatest effect in participants having baseline CRP below a median of 79 mg/L. Herein, the utility of baseline CRP to guide lenzilumab treatment was assessed.

Design: A subanalysis of the randomised, blinded, controlled, LIVE-AIR trial in which lenzilumab or placebo was administered on day 0 and participants were followed through Day 28.

Participants: Hospitalised COVID-19 participants (N=520) with SpO2 ≤94% on room air or requiring supplemental oxygen but not invasive mechanical ventilation.

Interventions: Lenzilumab (1800 mg; three divided doses, q8h, within 24 hours) or placebo infusion alongside corticosteroid and remdesivir treatments.

Main outcome measures: The primary endpoint was the time-to-event analysis difference in SWOV through day 28 between lenzilumab and placebo treatments, stratified by baseline CRP.

Results: SWOV was achieved in 152 (90%; 95% CI 85 to 94) lenzilumab and 144 (79%; 72 to 84) placebo-treated participants with baseline CRP <150 mg/L (HR: 2.54; 95% CI 1.46 to 4.41; p=0.0009) but not with CRP ≥150 mg/L (HR: 1.04; 95% CI 0.51 to 2.14; p=0.9058). A statistically significant interaction between CRP and lenzilumab treatment was observed (p=0.044). Grade ≥3 adverse events with lenzilumab were comparable to placebo in both CRP strata. No treatment-emergent serious adverse events were attributed to lenzilumab.

Conclusion: Hospitalised hypoxemic patients with COVID-19 with baseline CRP <150 mg/L derived the greatest clinical benefit from treatment with lenzilumab.

Trial registration number: NCT04351152; ClinicalTrials.gov.

Keywords: ARDS; COVID-19; Critical Care; Cytokine Biology; GM-CSF; Pneumonia; Respiratory Infection.

Publication types

Randomized Controlled Trial
Clinical Trial, Phase III
Research Support, Non-U.S. Gov't
Research Support, N.I.H., Extramural

MeSH terms

Antibodies, Monoclonal, Humanized / therapeutic use
Biomarkers
C-Reactive Protein
COVID-19 Drug Treatment
COVID-19*
Humans
SARS-CoV-2
Treatment Outcome

Substances

C-Reactive Protein
lenzilumab
Antibodies, Monoclonal, Humanized
Biomarkers

Associated data

ClinicalTrials.gov/NCT04351152

Grants and funding

K08 AI141761/AI/NIAID NIH HHS/United States