Repurposed antiviral drugs for COVID-19 –interim WHO SOLIDARITY trial results

Hongchao Pan; Richard Peto; Quarraisha Abdool Karim; Marissa Alejandria; Ana María Henao-Restrepo; César Hernández García; Marie-Paule Kiény; Reza Malekzadeh; Srinivas Murthy; Marie‐Pierre Préziosi; Srinath Reddy; Mirta Roses Periago; Vasee Moorthy; John-Arne Røttingen; Soumya Swaminathan

doi:10.1101/2020.10.15.20209817

Repurposed antiviral drugs for COVID-19 –interim WHO SOLIDARITY trial results

Hongchao Pan(University of Oxford), Richard Peto(University of Oxford), Quarraisha Abdool Karim(Centre for the AIDS Programme of Research in South Africa), Marissa Alejandria(University of the Philippines Manila), Ana María Henao-Restrepo(World Health Organization), César Hernández García, Marie-Paule Kiény(Inserm), Reza Malekzadeh(Ministry of Health and Medical Education), Srinivas Murthy(University of British Columbia), Marie‐Pierre Préziosi(World Health Organization), Srinath Reddy(Public Health Foundation of India), Mirta Roses Periago, Vasee Moorthy(World Health Organization), John-Arne Røttingen(The Research Council of Norway), Soumya Swaminathan(World Health Organization)

medRxiv

October 15, 2020

10.1101/2020.10.15.20209817

Cited by 635Open Access

Full Text

Abstract

ABSTRACT BACKGROUND WHO expert groups recommended mortality trials in hospitalized COVID-19 of four re-purposed antiviral drugs. METHODS Study drugs were Remdesivir, Hydroxychloroquine, Lopinavir (fixed-dose combination with Ritonavir) and Interferon-β1a (mainly subcutaneous; initially with Lopinavir, later not). COVID-19 inpatients were randomized equally between whichever study drugs were locally available and open control (up to 5 options: 4 active and local standard-of-care). The intent-to-treat primary analyses are of in-hospital mortality in the 4 pairwise comparisons of each study drug vs its controls (concurrently allocated the same management without that drug, despite availability). Kaplan-Meier 28-day risks are unstratified; log-rank death rate ratios (RRs) are stratified for age and ventilation at entry. RESULTS In 405 hospitals in 30 countries 11,266 adults were randomized, with 2750 allocated Remdesivir, 954 Hydroxychloroquine, 1411 Lopinavir, 651 Interferon plus Lopinavir, 1412 only Interferon, and 4088 no study drug. Compliance was 94-96% midway through treatment, with 2-6% crossover. 1253 deaths were reported (at median day 8, IQR 4-14). Kaplan-Meier 28-day mortality was 12% (39% if already ventilated at randomization, 10% otherwise). Death rate ratios (with 95% CIs and numbers dead/randomized, each drug vs its control) were: Remdesivir RR=0.95 (0.81-1.11, p=0.50; 301/2743 active vs 303/2708 control), Hydroxychloroquine RR=1.19 (0.89-1.59, p=0.23; 104/947 vs 84/906), Lopinavir RR=1.00 (0.79-1.25, p=0.97; 148/1399 vs 146/1372) and Interferon RR=1.16 (0.96-1.39, p=0.11; 243/2050 vs 216/2050). No study drug definitely reduced mortality (in unventilated patients or any other subgroup of entry characteristics), initiation of ventilation or hospitalisation duration. CONCLUSIONS These Remdesivir, Hydroxychloroquine, Lopinavir and Interferon regimens appeared to have little or no effect on hospitalized COVID-19, as indicated by overall mortality, initiation of ventilation and duration of hospital stay. The mortality findings contain most of the randomized evidence on Remdesivir and Interferon, and are consistent with meta-analyses of mortality in all major trials. (Funding: WHO. Registration: ISRCTN83971151 , NCT04315948 )

Related Papers

No related papers found

Powered by citation graph analysis