The increasing administrative burden associated with conducting clinical trials is a threat to patient safety, independent academic clinical research, and access to affordable innovation. While the Clinical Trials Regulation1—adopted by the European Parliament in 2014 to replace the Clinical Trials Directive2 (from 2001) and finally expected to become applicable in the course of 2020—will go some way in addressing bureaucracy overload, more action is needed. This article discusses the issues resulting from the exponential growth of regulatory and administrative requirements for the conduct of clinical studies and the impact this is having on researchers and patients. It also describes how the European Hematology Association (EHA) is coordinating a series of activities to advance potential solutions for these issues.
Issues of safety reporting
Nothing is more important than the safety of our patients in clinical trials and there is a need to communicate new and important safety data to investigators. However, researchers now receive a significant amount of information on (1) side effects that are already well known, (2) side effects alleged to be treatment-related that are not, or (3) suspected unexpected serious adverse reactions (SUSARs) that are revealed to be neither unexpected nor serious.3 This large and uncontrolled volume of information is now diluting and masking the truly important SUSAR reports, thereby compromising patient safety. It is evident that this issue is due, in part, to the overinterpretation of regulations by Contract Research Organizations (CROs),4,5 which require even minor events to be documented and reported to fulfill the frequent audits and inspections to which they are subjected.6 A simplified and less ambiguous formulation of the laws would help to prevent the overinterpretation of legislation. However, it is important to stress that physicians should not be encouraged to under-report serious adverse events (SAEs), as seemingly minor events could be significant if they occur in large numbers of patients.
Another issue with regard to safety reporting during clinical trials is that reported adverse events (AEs) tend to reflect investigators’ impressions of these events rather than actual patient experience.7,8 The methods currently used for detecting AEs in clinical trials are recognized as having limitations.9 It has been suggested that direct reporting of AEs by patients, as opposed to relying on data recorded by clinicians or trial practitioners, could be a better approach that would both improve the quality of safety information and allow the earlier detection of SAEs.10,11 We envision the introduction of simplified risk adapted reports, integrating data from electronic medical records.
We strongly recommend that regulators involve the key stakeholders—clinical researchers and patients—in the drafting of guidance documents for safety reporting. It is promising that the latest revision of the questions and answers document on Clinical Trials Regulation by the Directorate-General for Health and Food Safety of the European Commission now includes a separate chapter on safety reporting.12 Furthermore, the US Food and Drug Administration (FDA) is currently revising its guidelines for safety reporting13 and has recently issued a related questions and answers document.14
Informed consent forms
Several issues have been identified with the current informed consent process for participation in clinical trials. Informed consent forms (ICFs) are often too complicated for trial participants to understand, use complex scientific terminology, and demonstrate poor readability.15 In addition, they are often too long and cannot easily be translated into multiple languages.16 As a result, many participants, especially those from less developed countries, may not understand the clinical trial despite having signed the ICF.15
In the USA, it is required to include a key information section summarizing the ICF, but patients are still expected to read the complete form.17 We suggest that the key information page in an ICF be considered sufficient and only this page should be mandatory, with further details available for those who are interested. We also feel that ICFs should be critically reviewed by patient representatives and that their opinions should carry more weight than the opinions of lawyers, given that the document is aimed at patients.
Another issue is that re-consent is often required during the course of a clinical trial due to ICF amendments, but this can cause confusion and anxiety among some participants.18 It has been suggested that the re-signing of consent forms should only be necessary for ethical reasons, such as to protect participants from harm in the event of new findings about AEs, to maintain participant autonomy, or in the case of legally defective ICFs. Additionally, research review committees such as institutional review boards should oversee the re-consent process to ensure that participants are not contacted unnecessarily.18
As a starting point to simplify ICFs, EHA is developing a European ICF template through discussion with multiple stakeholders, including patient representatives. Another solution to the issue could be to make clinical trial documents publicly available to enable patients and other interested stakeholders to provide input into the ICFs. Alternatively, ICFs could be developed through procedures used for the drafting of other patient-focused documents, such as package leaflets. The latter must strictly adhere to the European Medicines Agency (EMA) Quality Review of Documents template and official glossaries,19 and their readability is validated and continuously reviewed.20
Regulatory challenges
The administrative demands associated with current regulatory processes for the conduct of clinical trials are time consuming, at times clinically irrelevant, and partly responsible for the rising costs of developing new drugs.3 CROs are necessary to manage this increasing amount of administration, but their personnel are not always experts in the area under investigation. Consequently, researchers often receive numerous queries from CROs that are unimportant yet involve an inordinate amount of paperwork.3 By law, clinical trial sponsors are ultimately responsible for the conduct of their clinical trials and, therefore, retain responsibility for the management of any contractor, including associated bureaucracy and any impact it may have. As a practical solution, regulators could set a framework for the conduct of CROs to prevent bureaucracy from spiraling out of control. If left uncontrolled, bureaucracy and the increasing costs of conducting clinical trials could lead to the disappearance of independent academic clinical researchers, particularly new researchers who may not have a supportive infrastructure to cope with these ever increasing administrative demands.3
Another channel for addressing these two interrelated issues—overinterpretation/over-reporting and an imbalanced relationship between CROs, sponsors and investigators—is the International Council for Harmonization of Technical Requirements for Pharmaceuticals for Human Use (ICH). ICH, which brings together regulatory authorities and the pharmaceutical industry, has released the E8 revised guideline on General Considerations for Clinical Trials for public consultation21 and is also revising guideline E6 on Good Clinical Practice.22 We are heartened to see that multiple stakeholders including healthcare providers, academia, and patient organizations, are being invited to participate in workshops organized as part of the revision process.
Role of EHA
EHA is identifying specific issues23 and is facilitating discussions between clinical researchers, regulators, and other relevant stakeholders to address the issues resulting from the increasing administrative burden associated with conducting clinical trials. As a first step, a workshop was held at the EHA Executive Office in The Hague on June 27, 2019, to discuss bureaucratic obstacles in clinical research.24 This workshop was attended by different stakeholders involved in the legislation and conduct of clinical trials, including clinical researchers, the European Commission, EMA, FDA, and patient organizations. As a follow-up to this meeting, EHA is actively participating in revisions of the ICH E8 and E6 guidelines and has provided input to the European Commission on the latest revision of the Clinical Trials Regulation questions and answers document.12 EHA is also aligning with key stakeholders, including the Biomedical Alliance in Europe, to develop specific actions. These include the creation of a ‘conduct of clinical research’ roadmap and a consensus opinion document on ICFs (for sharing with the European Commission). In addition, EHA is engaging with clinical researchers and patients outside of the hematology community to encourage cross-disciplinary debate of the current challenges associated with the conduct of clinical research.
Call for action
We call on regulators to ensure structural involvement of patients and clinical researchers in the formulation of informed consent forms and guidance documents for safety reporting and other aspects of clinical studies. Regulators should also set a framework for the conduct of CROs to prevent bureaucracy from spiraling out of control.
Clearly, bureaucracy in clinical research is a challenge faced not only by hematologists and their patients. EHA therefore calls on medical societies and patient organizations across disciplines to work together to develop a ‘roadmap towards patient-centric, bureaucracy-light clinical research’ in close dialogue with industry, policymakers, and regulators. Collectively, we must ensure that the interests of patients and clinicians are placed back at the center of the design and implementation of clinical trials.
Footnotes
Citation: Gribben J, Macintyre E, Sonneveld P, Doorduijn J, Gisselbrecht C, Jäger U, Le Gouill S, Rule S, Dreyling M. Reducing bureaucracy in clinical research: A call for action. HemaSphere, 2020;4:2(e352). http://dx.doi.org/10.1097/HS9.0000000000000352
Competing interests: Pieter Sonneveld is member of the EHA executive board, EHA past president, member of the EHA Education Committee, member of the European Affairs Committee, member of the Research committee, member of the Sponsor and Fundraising Committee, and chair of the SWG Committee. Martin Dreyling is member of the EHA executive board, member of the SWG Committee and vice-chair of the EHA Guidelines Committee. Elizabeth Macintyre is president elect of EHA and member of the European Affairs Committee. John Gribben is president of EHA and member of the European Affairs Committee. Ulrich Jäger is member of EHA European Affairs Committee.
References
- 1.European Commission. Regulation (EU) No 536/2014 of the European Parliament and of the Council on clinical trials on medicinal products for human use, and repealing Directive 2001/20/EC. 16 April 2014. https://ec.europa.eu/health/sites/health/files/files/eudralex/vol-1/reg_2014_536/reg_2014_536_en.pdf [Accessed December 3, 2019]. [Google Scholar]
- 2.European Commission. Directive 2001/20/EC of the European Parliament and of the Council on the approximation of the laws, regulations and administrative provisions of the Member States relating to the implementation of good clinical practice in the conduct of clinical trials on medicinal products for human use. 4 April 2001. https://ec.europa.eu/health/sites/health/files/files/eudralex/vol-1/dir_2001_20/dir_2001_20_en.pdf [Accessed November 11, 2019]. [PubMed] [Google Scholar]
- 3.Rule S, LeGouill S. Bureaucracy is strangling clinical research. Br Med J. 2019;364:l1097. [DOI] [PubMed] [Google Scholar]
- 4.Hearn J, Sullivan R. The impact of the ‘clinical trials’ directive on the cost and conduct of non-commercial cancer trials in the UK. Eur J Cancer. 2007;43:8–13. [DOI] [PubMed] [Google Scholar]
- 5.Sekeres M. Contract research agonizations. Editor's corner, perspectives. ASH Clinical News, 2017. https://www.ashclinicalnews.org/perspectives/editors-corner/contract-research-agonizations/ [Accessed November 6, 2019]. [Google Scholar]
- 6.Wright B. Shamley D, Wright B. Chapter 17 – Audits and inspections. A Comprehensive and Practical Guide to Clinical Trials. London: Academic Press; 2017;181–183. [Google Scholar]
- 7.Pakhomov SV, Jacobsen SJ, Chute CG, et al. Agreement between patient-reported symptoms and their documentation in the medical record. Am J Manag Care. 2008;14:1530–1539. [PMC free article] [PubMed] [Google Scholar]
- 8.Basch E. The missing voice of patients in drug-safety reporting. N Engl J Med. 2010;362:865–869. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 9.Allen EN, Chandler CI, Mandimika N, et al. Eliciting adverse effects data from participants in clinical trials. Cochrane Database Syst Rev. 2018;1:MR000039. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 10.Basch E, Bennett A, Pietanza MC. Use of patient-reported outcomes to improve the predictive accuracy of clinician-reported adverse events. J Natl Cancer Inst. 2001;103:1808–1810. [DOI] [PubMed] [Google Scholar]
- 11.Banerjee AK, Okun S, Edwards IR, et al. Patient-reported outcome measures in safety event reporting: PROSPER Consortium guidance. Drug Saf. 2013;36:1129–1149. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 12.European Commission Health and Food Safety Directorate-General. Clinical Trials Regulation (EU) No. 536/2014. Questions and answers, version 2.2, October 2019. https://ec.europa.eu/health/sites/health/files/files/eudralex/vol-10/regulation5362014_qa_en.pdf [Accessed November 11, 2019]. [Google Scholar]
- 13.US Food and Drug Administration. Safety assessment for IND safety reporting. Guidance for industry. December 2015. https://www.fda.gov/regulatory-information/search-fda-guidance-documents/safety-assessment-ind-safety-reporting-guidance-industryhttps://www.fda.gov/regulatory-information/search-fda-guidance-documents/safety-assessment-ind-safety-reporting-guidance-industry [Accessed October 21, 2019]. [Google Scholar]
- 14.US Food and Drug Administration. A risk-based approach to monitoring of clinical investigations questions and answers. Guidance for industry. March 2019. https://www.fda.gov/regulatory-information/search-fda-guidance-documents/risk-based-approach-monitoring-clinical-investigations-questions-and-answers [Accessed October 21, 2019]. [Google Scholar]
- 15.Kadam RA. Informed consent process: a step towards making it meaningful. Perspect Clin Res. 2017;8:107–112. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 16.Pandiya A. Readability and comprehensibility of informed consent forms for clinical trials. Perspect Clin Res. 2010;1:98–100. [PMC free article] [PubMed] [Google Scholar]
- 17.Department of Homeland Security; Department of Agriculture; Department of Energy; National Aeronautics; Space Administration; Department of Commerce; Social Security Administration; Agency for International Development; Department of Housing; Urban Development; Department of Labor; Department of Defense; Department of Education; Department of Veterans Affairs; Environmental Protection Agency; Department of Health; Human Services; National Science Foundation; Department of Transportation. Federal policy for the protection of human subjects. Fed Regist. 2017;82:7149–7274. https://www.govinfo.gov/content/pkg/FR-2017-01-19/pdf/2017-01058.pdf [Accessed November 10, 2019]28106360 [Google Scholar]
- 18.Resnik DB. Re-consenting human subjects: ethical, legal and practical issues. J Med Ethics. 2009;35:656–657. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 19.European Medicines Agency. Centralised procedures – Quality Review of Documents product-information version 10.1, September 2019. https://www.ema.europa.eu/en/human-regulatory/marketing-authorisation/product-information/product-information-templates#centralised-procedures---quality-review-of-documents-(qrd)-templates-section [Accessed November 6, 2019]. [Google Scholar]
- 20.European Medicines Agency. What is a package leaflet – how to review it? 21 January 2015. https://www.ema.europa.eu/en/documents/presentation/presentation-what-package-leaflet-how-review-it-claire-espinasse_en-0.pdf [Accessed November 10, 2019]. [Google Scholar]
- 21.European Medicines Agency. ICH guideline E8 (R1). General considerations for clinical studies. Draft version,;1; May 2019. https://www.ema.europa.eu/en/documents/scientific-guideline/draft-ich-guideline-e8-r1-general-considerations-clinical-studies-step-2b_en.pdf [Accessed October 21, 2019]. [Google Scholar]
- 22.European Medicines Agency. ICH E6 (R2) Good Clinical Practice. December 2016. https://www.ema.europa.eu/en/ich-e6-r2-good-clinical-practice#current-version---revision-2-section [Accessed November 6, 2019]. [Google Scholar]
- 23.Le Gouill S, Dreyling M, Caballero MD, et al. Is good clinical practice becoming poor clinical care? Hemasphere. 2017;1:e4. [DOI] [PMC free article] [PubMed] [Google Scholar]
- 24.European Hematology Association. Addressing the bureaucracy challenge. July 2019. https://ehaweb.org/organization/newsroom/news-and-updates/addressing-the-bureaucracy-challenge/ [Accessed November 6, 2019]. [Google Scholar]