Clinical Development of Therapeutic Agents for Hospitalized Patients With Influenza: Challenges and Innovations

James C King; John H Beigel; Michael G Ison; Richard E Rothman; Timothy M Uyeki; Robert E Walker; James D Neaton; John S Tegeris; James A Zhou; Kimberly L Armstrong; Wendy Carter; Peter S Miele; Melissa S Willis; Andrea F Dugas; LaRee A Tracy; David M Vock; Rick A Bright

doi:10.1093/ofid/ofz137

Clinical Development of Therapeutic Agents for Hospitalized Patients With Influenza: Challenges and Innovations

Open Forum Infect Dis. 2019 Mar 14;6(4):ofz137. doi: 10.1093/ofid/ofz137. eCollection 2019 Apr.

Authors

James C King¹, John H Beigel², Michael G Ison³, Richard E Rothman⁴, Timothy M Uyeki⁵, Robert E Walker¹, James D Neaton⁶, John S Tegeris¹, James A Zhou¹, Kimberly L Armstrong¹, Wendy Carter⁷, Peter S Miele⁷, Melissa S Willis¹, Andrea F Dugas⁸, LaRee A Tracy⁷, David M Vock⁶, Rick A Bright¹

Affiliations

¹ US Department of Health and Human Services, Biomedical Advanced Research and Development Authority, Washington, District of Columbia.
² National Institutes of Health, Division of Microbiology and Infectious Diseases, Bethesda, Maryland.
³ Divisions of Infectious Diseases, Northwestern University Feinberg School of Medicine, Chicago, Illinois.
⁴ Department of Emergency Medicine, Johns Hopkins Hospital, Johns Hopkins University School of Medicine, Baltimore, Maryland; for the ED Influenza Research Consortium.
⁵ Influenza Division, Centers for Disease Control and Prevention, Atlanta, Georgia.
⁶ Division of Biostatistics, School of Public Health, University of Minnesota, Minneapolis.
⁷ US Food and Drug Administration, Division of Antiviral Products, Silver Spring, Maryland.
⁸ Shady Grove Medical Center, Rockville, Maryland.

Abstract

Background: Since 1999, the US Food and Drug Administration approved neuraminidase and endonuclease inhibitors to treat uncomplicated outpatient influenza but not severe hospitalized influenza. After the 2009 pandemic, several influenza hospital-based clinical therapeutic trials were unsuccessful, possibly due to certain study factors. Therefore, in 2014, the US Health and Human Services agencies formed a Working Group (WG) to address related clinical challenges.

Methods: Starting in 2014, the WG obtained retrospective data from failed hospital-based influenza therapeutic trials and nontherapeutic hospital-based influenza studies. These data allowed the WG to identify factors that might improve hospital-based therapeutic trials. These included primary clinical endpoints, increased clinical site enrollment, and appropriate baseline enrollment criteria.

Results: During 2018, the WG received retrospective data from a National Institutes of Health hospital-based influenza therapeutic trial that demonstrated time to resolution of respiratory status, which was not a satisfactory primary endpoint. The WG statisticians examined these data and believed that ordinal outcomes might be a more powerful primary endpoint. Johns Hopkins' researchers provided WG data from an emergency-department (ED) triage study to identify patients with confirmed influenza using molecular testing. During the 2013-2014 influenza season, 4 EDs identified 1074 influenza-patients, which suggested that triage testing should increase enrollment by hospital-based clinical trial sites. In 2017, the WG received data from Northwestern Memorial Hospital researchers regarding 703 influenza inpatients over 5 seasons. The WG applied National Early Warning Score (NEWS) at patient baseline to identify appropriate criteria to enroll patients into hospital-based therapeutic trials.

Conclusions: Data received by the WG indicated that hospital-based influenza therapeutic trials could use ordinal outcome analyses, ED triage to identify influenza patients, and NEWS for enrollment criteria.

Keywords: antivirals; clinical site recruitment; enrollment criteria; influenza; therapeutic trial endpoints.