Author:
Lev Shaul,Gottesman Tamar,Sahaf Levin Gal,Lederfein Doron,Berkov Evgeny,Diker Dror,Zaidman Aliza,Nutman Amir,Ilan Ber Tahel,Angel Alon,Kellerman Lior,Barash Eran,Navon Roy,Boico Olga,Israeli Yael,Rosenberg Michal,Gelman Amir,Kalfon Roy,Simon Einav,Avni Noa,Hainrichson Mary,Zarchin Oren,Gottlieb Tanya M.,Oved Kfir,Eden Eran,Tadmor Boaz
Abstract
Background
Treatment of severely ill COVID-19 patients requires simultaneous management of oxygenation and inflammation without compromising viral clearance. While multiple tools are available to aid oxygenation, data supporting immune biomarkers for monitoring the host-pathogen interaction across disease stages and for titrating immunomodulatory therapy is lacking.
Methods
In this single-center cohort study, we used an immunoassay platform that enables rapid and quantitative measurement of interferon γ-induced protein 10 (IP-10), a host protein involved in lung injury from virus-induced hyperinflammation. A dynamic clinical decision support protocol was followed to manage patients infected with severe acute respiratory syndrome coronavirus 2 and examine the potential utility of timely and serial measurements of IP-10 as tool in regulating inflammation.
Results
Overall, 502 IP-10 measurements were performed on 52 patients between 7 April and 10 May 2020, with 12 patients admitted to the intensive care unit. IP-10 levels correlated with COVID-19 severity scores and admission to the intensive care unit. Among patients in the intensive care unit, the number of days with IP-10 levels exceeding 1,000 pg/mL was associated with mortality. Administration of corticosteroid immunomodulatory therapy decreased IP-10 levels significantly. Only two patients presented with subsequent IP-10 flare-ups exceeding 1,000 pg/mL and died of COVID-19-related complications.
Conclusions
Serial and readily available IP-10 measurements potentially represent an actionable aid in managing inflammation in COVID-19 patients and therapeutic decision-making.
Trial registration
Clinicaltrials.gov, NCT04389645, retrospectively registered on May 15, 2020.
Publisher
Public Library of Science (PLoS)
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