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Lessons learned from COVID-19 to overcome challenges in conducting outpatient clinical trials to find safe and effective therapeutics for the next infectious pandemic

Published online by Cambridge University Press:  15 October 2024

Minn A. Oh Open the ORCID record for Minn A. Oh [Opens in a new window] ,
Judith Currier ,
Akram Khan Open the ORCID record for Akram Khan [Opens in a new window] ,
Eleftherios Mylonakis ,
Matthew Newell ,
Rachel Bender Ignacio ,
Nick Jilg ,
Basmah Safdar ,
Lisa H. Merck  and
Davey M. Smith Open the ORCID record for Davey M. Smith [Opens in a new window]
Minn A. Oh*
Affiliation:
Department of Medicine, Oregon Health & Science University, Portland, OR, USA
Judith Currier
Affiliation:
Department of Medicine, University of California, Los Angeles, CA, USA
Akram Khan
Affiliation:
Department of Medicine, Oregon Health & Science University, Portland, OR, USA
Eleftherios Mylonakis
Affiliation:
Department of Medicine, Houston Methodist Hospital, Houston, TX, USA
Matthew Newell
Affiliation:
Global Health and Infectious Diseases, University of North Carolina School of Medicine, Chapel Hill, NC, USA
Rachel Bender Ignacio
Affiliation:
Department of Medicine, University of Washington, Seattle, WA, USA
Nick Jilg
Affiliation:
Department of Medicine, Harvard Medical School, Massachusetts General Hospital, Brigham and Women’s Hospital, Boston, MA, USA
Basmah Safdar
Affiliation:
Department of Emergency Medicine, Yale University, New Haven, CT, USA
Lisa H. Merck
Affiliation:
Department of Energy Medicine, Virginia Commonwealth, Richmond, VA, USA
Davey M. Smith
Affiliation:
Altman Clinical and Translational Research Institute, University of California, San Diego, CA, USA
*
Corresponding author: M. A. Oh; Email: [email protected]
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Abstract

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Type
Perspective
Information
Journal of Clinical and Translational Science , Volume 8 , Issue 1 , 2024 , e153
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (https://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution and reproduction, provided the original article is properly cited.
Copyright
© The Author(s), 2024. Published by Cambridge University Press on behalf of Association for Clinical and Translational Science

The National Institutes of Health (NIH) initiated the Accelerating COVID-19 Therapeutic Interventions and Vaccines (ACTIV) public-private partnership on April 17, 2020, to develop treatments and vaccines combatting coronavirus disease 2019 (COVID-19) [1]. Investigators from seven outpatient ACTIV trial sites in US assembled to document challenges associated with deployment of outpatient clinical trials, as well as to identify solutions for future pandemic responses.

Infrastructure

Conducting outpatient clinical trials during the COVID-19 pandemic was significantly challenging, due to global limitations of infrastructure and resources, such as the closure of non-emergency services and well-equipped research sites [2]. Essential supplies, including personal protective equipment (PPE) and testing materials, were in short supply, and transportation limitations further decreased access to treatment trials [3Reference Kim5]. Despite these obstacles, temporary regulatory allowances, mobile pod units, and provisional treatment facilities allowed for surge capacity and outpatient clinical trial activities [Reference Petrova, Farinholt and Joshi6Reference Aung, Hill, Bennet, Song and Oriol8]. Creative strategies to improve access to study materials were developed, such as video modules for asynchronous training, virtual lab manuals, centralized study updates, and transfer of experienced personnel to COVID research from non-COVID clinical assignments (such as pharmacists, phlebotomists, and frontline clinicians). Further, collaboration with the federal government enabled patient triage and care in disaster tents. Remote consent, virtual examinations, and drive-through testing mechanisms were also rapidly implemented, with some facilities mailing capillary phlebotomy kits for remote sample collection. These lessons from these mobilization efforts and decentralized clinical trial designs will inform future pandemic responses, like the importance of establishing infrastructure for surge capacity, diversifying supply chains, and integrating pandemic response training with standard staff onboarding.

Regulatory

Clinical trials could not be conducted under standard regulatory processes during the COVID-19 pandemic due to several limitations, including staffing shortages, lack of material resources (lab kits, PPE), and the constant nature of pandemic response operations. Institutional review board (IRB) submissions were fast-tracked, while many sites struggled to identify staff trained to manage federal regulatory compliance. Similarly, FDA expedited reviews to help launch trials quickly, which could mean changes in endpoints later in the trial. Further, social distancing, investigator workload, staff turnover, and remote work coordination further hindered workflow, often causing delays or obstructions to trial initiations [Reference Shiely, Foley and Stone9,Reference Mitchell, Ahmed and Breeman10]. Deployment of staff necessitated extensive, rapid training. Protocols evolved rapidly due to frequent modifications in standard of care and turbulent public health guidance, adding to the regulatory burden. Successful strategies for trial conduct included instituting emergency IRB coverage for expedited trial review, creating separate COVID IRBs able to meet regularly to prioritize rapid study deployment, and the utilization of Health Insurance Portability and Accountability Act waivers to facilitate communication/data sharing [11]. Remote informed consent and electronic data collection methods were rapidly adopted, streamlining study flow and reducing the need for in-person contact [12]. Future pandemic response should include these processes for streamlining regulatory requirements, maintaining pandemic-specific IRB procedures, developing composite endpoints for future trials, and deploying centralized IRB teams to address regulatory reviews in concert. Improving access to training verifications, centralizing site regulatory approvals, and using electronic tools for study start-up/maintenance enhance efficiency and reduce the burden on individual research sites. Such efforts enhance trial recruitment/management and improve efficiency in response to public health emergencies.

Staffing

Personnel shortages and the redirection of trained research professionals to frontline clinical care significantly hindered clinical trial operations [13]. Additionally, inadequate training in Good Clinical Practice and investigational new drug-enabling research posed substantial obstacles. Institutional barriers related to onsite versus remote work, hiring freezes, and uncertainty around staff availability further complicated study deployment. Many institutions faced challenges due to unclear infection control policies and the reluctance of staff to work with persons with COVID-19, particularly before vaccines were available [14]. To combat such challenges in the future, centralized command centers and frequent updates can keep research teams informed, and integration of pandemic preparedness into staff training and institutional protocols is vital. Training should cover isolation precautions, mobile unit operations, resource allocation, and emergency central command response. Access to a national repository of essential supplies, such as PPE and lab testing kits, will facilitate study deployment and efficacy, while also enhancing staff confidence.

Recruitment

Recruiting and retaining participants for outpatient clinical trials was significantly challenging due to patient limitations (transportation, illness, access to information about trial opportunities, and study sites) as well as restrictions posed by the health care system (limited access to swift COVID testing, procedures for remote consent, provider training, and PPE access). Further, cross-study eligibility, verification of positive tests, and the impact of misinformation on medication/vaccine acceptability also hindered recruitment efforts. In addition, many smaller sites struggled to obtain expedited approvals for public health or third-party testing results, creating research access disparities. Protocols required stratification for enrollment opportunities. To mitigate these obstacles, study activities were conducted remotely, utilizing virtual recruitment methods, and establishing a national database of active studies and site qualifications. These strategies helped to mitigate disparity in access to trials due to geography and local resources. To improve future research, expanding remote data collection methods, coordinating public-facing recruitment campaigns, and establishing pre-existing agreements for data sharing and trial execution are essential. Enhancing community outreach through partnerships with local groups and integrating research opportunities into clinical guidelines and public health information could also improve recruitment and retention efforts.

Conclusion

The challenges we faced during trial recruitment amid the COVID-19 pandemic have provided valuable lessons that shape the future of medical research (Figure 1). The COVID-19 pandemic clearly illuminated flaws in our biomedical research system which highlight the indispensable role of critical infrastructure resources to pandemic responses. Regulatory readiness across sites is a cornerstone of clinical trial execution and proper forward planning to strengthen our clinical trial resources and infrastructure will improve survival outcomes when the next pandemic arrives. These lessons pave the way to accelerate medical care in the post-pandemic era for individuals and communities worldwide.

Figure 1. Lessons learned from COVID-19 in conducting outpatient clinical trials.

Author contributions

MAO, JC, AK, EM, MN, RBI, NJ, BS, LHM, DMS: conception and design of work, MAO, JC, AK, EM, MN, RBI, NJ, BS, LHM, DMS: collection or contribution of data, MAO, JC, DMS: contributions of analysis tools or expertise, MAO, JC, AK, EM, MN, RBI, NJ, BS, LHM, DMS: conduct and interpretation of analysis, MAO, JC, AK, EM, MN, RBI, NJ, BS, LHM, DMS: drafting of the manuscript, DMS: responsibility for the manuscript as a whole.

Funding statement

The ACTIV clinical trials referenced in this manuscript received funding from various US Government funding agencies. The views and conclusions contained in this document are those of the authors and should not be interpreted as representing the official policies, either expressed or implied, of the NIH. Open Access publication funding courtesy of the Foundation for the National Institutes of Health.

Competing interests

None.

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Figure 0

Figure 1. Lessons learned from COVID-19 in conducting outpatient clinical trials.