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ORIGINAL RESEARCH article

Front. Med., 31 May 2024
Sec. Regulatory Science

International regulatory and publicly-funded initiatives to advance drug repurposing

  • 1Dutch Medicines Evaluation Board, Utrecht, Netherlands
  • 2Division of Pharmacoepidemiology and Clinical Pharmacology, Utrecht Institute for Pharmaceutical Sciences (UIPS), Utrecht University, Utrecht, Netherlands

Introduction: Although drug repurposing holds great potential in addressing unmet needs, successful practical implementation is challenging and has been less widespread than anticipated. Regulators may play a critical role in addressing this, and recent years have seen the conception of regulator-initiated and publicly-funded repurposing initiatives, with significant regulator involvement.

Methods: International regulators and public funders (n = 8) were interviewed to obtain insight in how repurposing can be advanced from a regulatory perspective. Transcripts were thematically analyzed.

Results: Most initiatives employed a broad concept of repurposing. While patient access was the main focus, label extension remained the gold standard. Commonly perceived barriers were a lack of regulatory expertise, limited downstream drug development, insufficient financial incentives, inadequate awareness of challenges, and poor collaboration. Ways for regulators to facilitate repurposing include early and accessible involvement fostering education, collaboration, and awareness. Increased stakeholder engagement, including internationally, was recommended. Legislative changes may enable the current repurposing ecosystem to evolve.

Discussion: Regulators may play a central role in advancing repurposing by reconsidering their responsibilities within the current regulatory framework, both in mitigating repurposing pitfalls and actively encouraging repurposing initiatives by industry and non-traditional drug developers.

1 Introduction

Drug repurposing has increasingly been a focus of the drug developing ecosystem, ostensibly gaining traction since Ashburn & Thor’s landmark publication in 2004 (1). Drug repurposing can be defined as the identification, development, and/or use of an existing active pharmaceutical ingredient (API) or medicinal product for a new disease, patient population, dosage form, duration, route of administration, or combination of the aforementioned (2). From the most influential drugs in terms of revenue (sildenafil) and notoriety (thalidomide) (3), to unprecedented global urgency during the COVID-19 pandemic (dexamethasone, tocilizumab, and baricitinib in the UK RECOVERY trial) (4), prior examples illustrate the wealth of possibilities and untapped potential of repurposing.

Repurposing’s societal and scientific relevance stems from its potential to address unmet medical needs (e.g., rare or sporadic infections, emerging threats, rare cancers) in a safe and timely manner at a lower cost by leveraging existing knowledge of repurposing candidates. Examples include the use of propranolol in infantile hemangioma, and fenfluramine in treating the rare Dravet syndrome and Lennox–Gastaut syndrome (5).

While past decades have seen exceptional scientific and technological progress, pharmaceutical research and development (R&D) costs have increased exponentially without proportionate public health advancement (1, 6). Compounds that have already been established as safe during preclinical or human studies may present a de-risked approach to the notoriously failure-prone drug development process and “the valley of death,” in which only 0.1% of experimental entities proceed from preclinical to human testing (6). For drugs that have advanced to phase I clinical trials, an estimated 9 out of 10 candidates fail during clinical assessment and approval (7). For repurposed drugs, the success rate is thought to be higher (8), although a full overview of success rates in repurposing does not yet exist Repurposing may expedite the drug development process from initial concept to market access from an average 10–17 years to 3–12 years, through the use of previously established knowledge of repurposing candidates (1). Besides safety assessments, this may include known pharmacokinetic profiles, formulation development, and regulatory knowledge (3, 9). In some cases it may be possible to rely on prior data (e.g., target and compound discovery and screening, lead optimization, absorption, distribution, metabolism, excretion, toxicity (ADMET) assessment, phase I and II trials) for approval of a new indication, allowing for a more rapid progression to late-phase clinical trials, and ultimately patient access (1). For instance, the IRDiRC Drug Repurposing Guidebook provides ample starting points on how to optimize repurposing processes, highlighting which steps are of vital importance in doing so (e.g., patent status) (10). In short, repurposing may be safer and quicker than de novo drug development, at reduced costs. Given rapidly increasing health care costs, this presents a major advantage (11). The estimated total costs of bringing a repurposed drug to market are thought to be 50–60% of R&D costs of de novo drug development (12).

Repurposing’s advantages seem tantalizingly straightforward. However, its practical implementation has proven to be less widespread than initially hoped for (13). Major hurdles to repurposing were highlighted by Austin et al. in 2021, as discussed at the National Center for Advancing Translational Sciences (NCATS), Reagan-Udall Foundation (RUF) and FDA workshop on repurposing in 2019 (14). These include lack of centralization of information on repurposing resources, poor data access, barriers to clinical utilization of repurposed drugs (including on- versus off-label use), and lack of financial and regulatory incentives.

Of these barriers, regulatory challenges may present a distinct opportunity for improvement by addressing the cost in time and money of repurposing. Examples of regulatory hurdles include, but are not limited to, the following aspects. The current regulatory and legal framework offers little to no incentive for companies or other drug sponsors to pursue repurposing when it comes to off-patent drugs (9). Notwithstanding the aforementioned R&D savings, repurposing still requires substantial investments in terms of risk, costs, and workload. Without traditional exclusivity models and in the face of generic competition, it can be difficult for sponsors to secure a return on these investments (15). Reluctant industry engagement may present a challenge even if initial research efforts are led by other, non-commercial stakeholders, since, ultimately, only the marketing authorization holder (MAH) can apply for an original marketing authorization (MA) to be adjusted. For academia and not-for-profit developers, an important barrier may be lack of regulatory knowledge and experience. This is especially significant given that the majority of repurposing initiatives originate in academia, while the skills and resources to facilitate translational development traditionally lie with industry (16). This currently means that the majority of academia-initiated drug innovation never progresses beyond early development (17). To mitigate these and other issues, increased regulatory involvement and collaboration is often recommended in literature, by regulators and drug developers alike (18). By accommodating the aforementioned concerns, regulators can play a critical role in advancing drug repurposing as a whole (9). This call to action has not gone unnoticed, and recent years have seen the conception of several projects to address these challenges. Examples are the European Medicines Agency (EMA) pilot on repurposing of authorized medicines (19), the International Rare Diseases Research Consortium (IRDiRC) Drug Repurposing Guidebook (10), and the FDA and National Institutes of Health (NIH) joint initiative CURE ID, which focusses on data collection of real-world data on repurposed drugs (20).

An overview of existing regulator and publicly-funded initiatives, with significant regulator involvement, to stimulate and facilitate repurposing (referred to as ‘repurposing initiatives’ in this study) is lacking. Insight into the current regulatory landscape is critical in determining regulators’ current position on repurposing, and what can be learnt from existing initiatives. This study aimed to answer how drug repurposing can be advanced from a regulatory perspective, based on current regulator and publicly-funded repurposing initiatives.

2 Methods

A series of semi-structured interviews with international regulators and leaders of publicly-funded repurposing efforts was at the core of this study, and enabled a more in-depth investigation of identified initiatives and perceived regulatory considerations and challenges identified through a literature review-based landscape analysis of repurposing initiatives.

2.1 Literature review

Current literature and publicly accessible online resources were reviewed in order to create a landscape analysis of repurposing initiatives. PubMed, Google Scholar, and public websites for regulatory agencies and publicly-funded institutions were consulted between January 23th and March 3th 2023 for appropriate information using (a combination of) search terms, covering “drug repurposing, repositioning, reprofiling, redirecting, rediscovery,” “regulatory, regulator,” and the respective agencies’ names. Sources were selected based on relevancy (e.g., relating to the regulatory aspects of drug repurposing), reliability (e.g., peer reviewed) and recency, as relating to the main research question (articles published after 2003, as Ashburn and Thor published their landmark study in 2004). Search results were complemented by background literature on repurposing. These findings provided the basis for part II of this study.

2.2 Interviews

Eligible interview candidates were international regulators and leaders of publicly-funded repurposing initiatives, with significant regulator involvement, identified through purposive and snowball sampling resulting in a literature review-based landscape analysis of repurposing initiatives. Eligibility criteria for initiatives were: to be ongoing at the time of analysis (spring of 2023), to entail active involvement of one or more regulators in an official capacity, and to include multiple repurposing cases (e.g., not a project focused on the repurposing of a single drug).

Interview questions covered:

1. initiative characteristics—aims, definition of ‘repurposing’, applicants and drug candidates

2. initiative background and repurposing challenges

3. considerations on regulator involvement—role of the regulator, regulatory aims of repurposing initiatives

4. experiences & future perspectives—impact and results, practical solutions, recommendations

The complete interview guide is included in the Supplementary material.

2.3 Analysis

After obtaining interviewees’ written informed consent, the interviews were recorded and transcribed verbatim, or responses were obtained in writing. Thematic analysis according to Braun and Clarke (21) was conducted using NVIVO20 software, including mixed inductive and deductive coding based on the interview guide.

3 Results

Of the selected initiatives (n = 10), eight were included in the final analysis. Two organizations and initiatives were not included due to an inability to participate in the required timeframe (n = 1) or lack of response (n = 1). For one project, two representatives were interviewed on separate occasions, bringing the total number of interviews conducted to nine. An overview of participating agencies/institutions is shown in Table 1. A timeline of current initiatives, of which the majority (n = 7) have been running for two years or less, can be found in Figure 1. Respondents’ professional backgrounds ranged from regulatory affairs officer, director of national research centers, to executive directors of public private partnerships. Interviews were held individually, in-person (n = 1), remotely via video conferencing platform (n = 7), or by obtaining written responses to the interview questions (n = 1). A comprehensive overview of results is included in Table 2.

Table 1
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Table 1. Overview of invited interview candidates.

Figure 1
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Figure 1. Timeline of current repurposing initiatives. The majority (n = 7) have been running for two years or less. Source: literature review as part of the current study.

Table 2
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Table 2. Overview of interview results: key considerations and exemplary quotes.

3.1 Initiative characteristics

Respondents for all initiatives (n = 9) indicated that their projects aim to achieve one or more of the following: to provide education on drug repurposing, facilitate collaboration on repurposing projects, and/or optimize the overall repurposing process. The majority (n = 8) purposefully employ a broad conceptualization of repurposing, to attract as widespread a pool of (drug) candidates as possible, and to lower the threshold for involvement of drug developers. While most initiatives are open to a wide range of participants (n = 5), the majority target academia, not-for-profit organizations, or small companies (n = 5). Five initiatives also specifically target off-patent, marketed drugs. Two initiatives do not specifically target repurposing projects but include them as part of a broader program. The potential of shelved compounds (discontinued or put on hold during development) is also frequently considered (n = 4). All respondents (n = 9) agreed that the definition of repurposing remains hotly debated (e.g., the difference between repurposing and repositioning). These issues were perceived by four respondents to complicate repurposing efforts considerably, as certain examples may not even be acknowledged as ‘repurposing’ (quote 1).

“Even within regulatory agencies, there may be different definitions of repurposing in use. Sometimes we may be talking about repurposing in the same context but using a different term.” Quote 1.

3.2 Initiative background and repurposing challenges

The most commonly perceived barriers to repurposing were:

1. lack of familiarity with regulatory requirements (as illustrated by quote 2): repurposing projects conducted by non-traditional developers (entities not primarily associated with the pharmaceutical industry, such as academia) suffer from a knowledge gap by these developers of regulatory issues (e.g., they do not know what data is needed, or which questions to ask regulators) (n = 9). This also results in a limited downstream drug development perspective: non-traditional developers struggle to align and optimize their efforts along the drug development pathway (e.g., clinical trials are not set up in way that support MA) (n = 8). The knowledge gap may also lead to inadequate awareness of pitfalls and opportunities (as illustrated by quote 3): non-traditional drug developers tend to underestimate the complexities of repurposing and the added value of regulatory involvement can be unclear (n = 5)

2. insufficient financial incentives: industry is generally reluctant to engage in repurposing projects due to the lack of a business case and limited perceived return on investment (n = 9)

3. poor collaboration: multi-stakeholder engagement remains challenging, repurposing efforts are often fragmented and operate in siloes (n = 4)

“We still have a huge mismatch between an academic’s understanding of the regulatory process, and the fact that they are actually working in a regulatory environment.” Quote 2.

“There’s a lack of awareness, and perhaps a lack of appreciation for the regulatory system.” Quote 3.

3.3 Regulatory relevance

While patient access is the main focus for all initiatives (n = 8) (quote 4), label extension remains the gold standard (n = 6), to demonstrate safety and efficacy of the product, as well as for financial reasons. While label extension may be the preferred outcome, six lead respondents (n = 6) regarded widespread off-label use as ‘successful repurposing’, due to the challenges they perceived in obtaining regulatory approval for new indications in some cases. Regulatory approval offers advantages such as a pharmacovigilance framework, the ability of prescribers to prescribe with confidence, and equal access to evidence-based treatment. Reimbursement may also be dependent on whether an indication is included in the label. Ways for regulators to facilitate repurposing include early involvement (n = 8), education (n = 8), making regulators readily approachable for feedback on repurposing projects (n = 6), fostering collaboration (n = 8), and building awareness among drug developers (including atypical ones) about the regulatory support available and its added value (n = 4).

“The goal is to get drugs to patients, as widely as possible. On-label where possible, off-label only if really necessary.” Quote 4.

3.4 Experiences and future perspectives

The last several years have witnessed increasing interest in drug repurposing (n = 6). Seven initiatives have seen concrete success, from securing data packages from clinicians and industry to repurposed drugs making it into phase III trials, although six projects started relatively recently (Figure 1). How these successes are defined depends on the project specific aims, and do not necessarily have to include label extensions. Plans for impact analysis are in place for nearly all (n = 7). These include generation and publication of interim assessment reports based on stakeholder feedback, as well as analysis of drug prescription statistics. Several practical solutions were mentioned with regard to the initiation of a repurposing pilot. These include keeping proceedings as simple as possible to ensure efficiency (n = 2), maintaining a helicopter view of the entire process both up and downstream (n = 3) (e.g., design clinical trials based on a prospective change to the MA), and taking lessons from the COVID-19 pandemic, where sudden pressing unmet medical need enabled successes like the RECOVERY trial (n = 1). A rethinking of the role of the regulator was also suggested by four respondents: aiming to have a more informal approach towards non-traditional developers. Opportunities within the current regulatory and legal system can and should be utilized. Examples include incentivizing MAHs to change labels by creating financial incentives using publicly funded mechanisms to study repurposed drugs and have them labeled for their new indications (n = 3). More disruptive ideas were suggested by some (e.g., a pooled innovation fund focusing on payors (n = 1): if health insurers save money through repurposing, new repurposing projects could be funded by taking a percentage of those savings). Overall recommendations by respondents included increased (international) stakeholder engagement, which could be improved by actively engaging with and specifically addressing concerns raised by industry, (n = 4). Harmonization of repurposing endeavors was favored by seven respondents, for which they indicated that efforts are currently underway. Legislative changes may enable the current repurposing ecosystem to evolve, and the majority of interviewees (n = 7) were excited about the EU pharmaceutical legislation reform and repurposing’s prominence therein. Finally, a concern shared by most respondents (n = 5) is creating awareness that there is a problem in repurposing, underlining the need to start thinking in terms of practical solutions in order to move forward in a sustainable way (quote 5).

“How do you know you have a drinking problem? First of all, you have to admit that you have a problem, right? We have to admit there’s a problem in repurposing. Let us come together and talk about it from a global perspective.” Quote 5.

4 Discussion

In summary, this study found that the studied repurposing initiatives are in agreement regarding general aims and the preference for an inclusive approach. A lack of familiarity with regulatory requirements and financial incentives are widely recognized to be two of the main barriers to successful repurposing for non-traditional drug developers. As regulatory approval remains the gold standard, the relevance of regulator involvement is acknowledged across the board. Nevertheless, fundamental differences remain, most notably when it comes to the definition of repurposing.

Repurposing seems to have outgrown the initial phase of turmoil and underappreciation that characterized its beginnings as a topic of interest, as the community has developed a variety of concrete initiatives with a shared recognition of necessity, potential, and goals. Questions of definition and who will take ownership of repurposing ventures remain to be addressed. The lack of consensus on the exact definition of repurposing may hamper repurposing harmonization efforts (2). Some respondents were reluctant to even refer to their endeavors as repurposing. While this lack of consistency complicates matters, it does not seem to keep efforts from moving forward. Utilization of a broad definition of repurposing may be advantageous, as it opens programs to a wider variety of stakeholders. Moreover, it remains unclear who (government, not-for-profit, patient organizations, etc.) will lead repurposing ventures, particularly when drugs are off-patent. While the initiatives included in this study are all led by regulators or publicly-funded entities, multi-stakeholder involvement is considered essential.

Stakeholders share a recognition of repurposing’s necessity, potential, and goals, as well as general agreement on the primary barriers to its success. This could offer opportunities for collaboration and harmonization and confirms the progress the repurposing ecosystem has experienced since its inception. The knowledge gap in regulatory expertise for non-traditional repurposing programs is being addressed by initiatives like STARS and the IRDiRC Task Force but remains a challenge (17, 22, 23). In limited cases regulators are incentivizing industry to update labels using existing mechanisms within their regulatory framework. Though a shared vision for the general aims of an ideal repurposing ecosystem has developed, this agreement has not yet resulted in demonstration of large-scale successful repurposing projects. However, current, newly-initiated programs show the potential of repurposing when diverse stakeholders work together, and should be closely watched. REPO4EU is an example of another multi-stakeholder initiative, in which regulators are not (yet) directly involved, which aims to develop an online platform for drug repurposing. Time will tell if these and other initiatives result in concrete successes and scalable solutions. A very recent study of Liddicoat et al. (24) proposes five criteria that could be used to determine the success of these initiatives: the number of authorizations granted; their clinical impact; the number of patients treated in accordance with the new use; savings in public healthcare; and reductions in off-label use, especially if the earlier use was based on inadequate data. Exciting accomplishments such as the recent licensing of breast cancer drug anastrozole as preventive treatment by the Medicines and Healthcare products Regulatory Agency in the United Kingdom, supported by the NHS Medicines Repurposing Programme, are promising (25).

Regulators can help address these challenges by reassessing their role in the repurposing ecosystem. As respondents indicate, different regulators are already seeking to reshape their responsibilities in repurposing in different ways: from organizing accessible education sessions tailored to non-traditional drug developers to proactive involvement with academia. Regulators can help maintain consistently high research standards in drug trials by providing scientific advice, for example. To what extent this type of education should fall under the regulator’s scope or might be better suited to be taken up by academia themselves, is a topic of discussion. For regulators, while maintaining objectivity remains key, a shift to a more proactive, collaborative approach involving increased outreach to non-traditional drug developers seems apparent and necessary (especially within the rare disease realm). This reassessment could benefit from a two-tiered approach, one focusing on practical measures, the other on legislative changes. Practical actions may include the (international) upscaling of existing initiatives, early and accessible regulatory involvement in repurposing projects by providing clear and consistent guidance, and increased collaboration with, for instance, publicly funded entities. This is where legislative changes may also be helpful, as they would enable governments and non-traditional drug developers to take on responsibilities that have traditionally lain with industry. An example of a similar, successful approach is the Best Pharmaceuticals for Children Act (BPCA), that prioritizes pediatric therapeutic needs by bringing these on-label. In a similar vein, the newly proposed EU pharmaceutical legislation reforms mention repurposing as well (26). The draft text states that, in case of substantive evidence for a new therapeutic indication expected to fulfill an unmet medical need, “…marketing authorisation holders of the medicinal products concerned shall submit a variation to update the product information with the new therapeutic indication.” No matter the practical interpretation, it is encouraging to see that, on an advanced level, repurposing and its potential are firmly on the agenda.

Limitations of this study include the fact that despite stating various practical suggestions for advancing repurposing from a regulatory perspective, this study did not dive further into their feasibility. This study confirms that it remains challenging to get an easily attainable overview of available repurposing resources, including regulatory and publicly-funded initiatives, for researchers and developers alike. Despite these initial difficulties, active engagement with the international regulatory network (e.g., at C-Path’s CURE Drug Repurposing Collaboratory annual meeting in Washington DC in April 2023) enabled the establishment of the comprehensive overview of these projects presented here. Future research could focus on perspectives of other stakeholders (industry, academics, patients) in the current repurposing context, the use of innovative methods (such as artificial intelligence) in repurposing, assessment of the results of the repurposing initiatives currently underway (including international trend analysis), as well as the possible implications of the proposed EU pharmaceutical legislation reforms.

5 Conclusion

This study shows that, based on current regulator and publicly-funded initiatives to advance repurposing, the concept has entered a new phase, seeing a variety of concrete initiatives with a shared recognition of necessity, potential, and goals, as well as the identification of a lack of familiarity with regulatory requirements and financial incentives as two main barriers to its success. Within the confines of the current repurposing ecosystem, regulators may be able to provide educational support and guidance to organizations focused on drug repurposing for unmet medical needs, whilst maintaining their traditional and essential objectivity. Legislative initiatives may also help to further the use of drug repurposing for unmet medical needs.

Data availability statement

The original contributions presented in the study are included in the article/Supplementary material, further inquiries can be directed to the corresponding author.

Author contributions

ES: Formal analysis, Investigation, Methodology, Writing – original draft, Writing – review & editing. AM-T: Writing – review & editing. AP: Conceptualization, Formal analysis, Methodology, Writing – review & editing.

Funding

The author(s) declare that no financial support was received for the research, authorship, and/or publication of this article.

Acknowledgments

We greatly appreciate the invaluable input from Heather Stone and Maya Younoszai (FDA) throughout this study. We also thank Smith Heavner (Critical Path Institute, United States) for excellent advice on the interview guide and thematic analysis.

Conflict of interest

The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

The author(s) declared that they were an editorial board member of Frontiers, at the time of submission. This had no impact on the peer review process and the final decision.

Publisher’s note

All claims expressed in this article are solely those of the authors and do not necessarily represent those of their affiliated organizations, or those of the publisher, the editors and the reviewers. Any product that may be evaluated in this article, or claim that may be made by its manufacturer, is not guaranteed or endorsed by the publisher.

Supplementary material

The Supplementary material for this article can be found online at: https://www.frontiersin.org/articles/10.3389/fmed.2024.1387517/full#supplementary-material

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Glossary

Keywords: drug repurposing, drug repositioning, drug development, regulatory agencies, regulatory science

Citation: Spin EL, Mantel-Teeuwisse AK and Pasmooij AMG (2024) International regulatory and publicly-funded initiatives to advance drug repurposing. Front. Med. 11:1387517. doi: 10.3389/fmed.2024.1387517

Received: 17 February 2024; Accepted: 01 May 2024;
Published: 31 May 2024.

Edited by:

Cristiana Sessa, Oncology Institute of Southern Switzerland (IOSI), Switzerland

Reviewed by:

Annette Mollet, University of Basel, Switzerland
Annette Magnin, Cantonal Ethics Commission Zurich, Switzerland
Anastasios Stathis, Oncology Institute of Southern Switzerland (IOSI), Switzerland

Copyright © 2024 Spin, Mantel-Teeuwisse and Pasmooij. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.

*Correspondence: Anna Maria Gerdina Pasmooij, YW0ucGFzbW9vaWpAY2JnLW1lYi5ubA==

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