Published on 29/12/2025
Ensuring Patient Diversity in UK Clinical Trials
Diversity in clinical research is increasingly recognised as a regulatory, ethical, and scientific priority. In the United Kingdom (UK), ensuring that trial populations reflect the demographics of the patients who will ultimately use new therapies is central to public trust and scientific credibility. Regulatory bodies such as the Medicines and Healthcare products Regulatory Agency (MHRA) and the Health Research Authority (HRA) have introduced requirements and guidance to strengthen inclusion and transparency in participant recruitment. NHS Trusts, academic institutions, and Contract Research Organisations (CROs) are equally challenged to improve outreach to underrepresented populations, including ethnic minorities, older adults, women, and socioeconomically disadvantaged groups.
This article explores the regulatory framework, challenges, and best practices related to patient diversity in UK clinical trials, highlighting the role of NHS infrastructure, NIHR initiatives, and evolving MHRA expectations.
Background and Regulatory Framework
MHRA Expectations on Diversity
MHRA emphasises that patient populations in clinical trials should be representative of the real-world population. Inspections increasingly assess whether recruitment strategies are inclusive and whether data stratification supports diversity analyses.
HRA Guidance
The HRA requires sponsors to explain recruitment strategies in ethics applications, ensuring that barriers to participation—such as language, travel, and cultural
Global Context
While the FDA in the US has explicit diversity action plans, UK regulators rely on guidance, transparency, and best practices, encouraging sponsors to adopt strategies that meet global harmonisation requirements.
Core Insights on Diversity in UK Trials
1. Ethnic and Cultural Representation
Despite the UK’s multicultural population, minority ethnic participation in trials remains low. Barriers include mistrust, lack of outreach, and limited accessibility of trial sites.
2. Gender Balance
Women, particularly pregnant and lactating women, are often underrepresented in trials. MHRA encourages inclusive eligibility criteria where scientifically justified.
3. Age Inclusion
Older adults, despite being primary consumers of many therapies, are frequently excluded due to comorbidities. Trials must adapt protocols to include realistic patient populations.
4. Socioeconomic Barriers
Travel costs, time commitments, and lack of awareness often limit participation among disadvantaged groups. Sponsors should consider reimbursement and flexible participation models.
5. Rare Diseases and Small Populations
Diversity in rare disease trials focuses on equitable access across geographic regions, often requiring collaboration between NHS Trusts and international networks.
Best Practices for Improving Diversity
- Develop community engagement programmes to build trust with underrepresented groups.
- Provide translated patient materials and interpreters where needed.
- Offer travel reimbursements and flexible scheduling to reduce socioeconomic barriers.
- Leverage decentralised trial models to reach patients in remote or underserved regions.
- Include diversity metrics in recruitment plans and monitor progress continuously.
Scientific and Regulatory Evidence
- Medicines for Human Use (Clinical Trials) Regulations 2004
- ICH E6(R2) – Good Clinical Practice
- HRA Equality, Diversity, and Inclusion in Research Guidance
- MHRA GCP Inspection Reports
- NIHR Diversity and Inclusion Framework
Special Considerations
- Oncology Trials: Require proactive outreach to ensure inclusion of diverse populations often disproportionately affected by cancer.
- Pediatrics: Age-appropriate consent and assent processes are critical for including children in trials.
- Rare Diseases: Collaborative biobank and registry use can help capture diverse patient data.
- Decentralised Trials: Offer opportunities to improve representation by reducing travel burdens.
When Sponsors Should Seek Regulatory Advice
- If designing diversity action plans for high-impact global submissions.
- When trials involve vulnerable populations with ethical complexities.
- If inspection findings reveal poor recruitment diversity.
- For rare disease and paediatric trials with small and diverse cohorts.
- When developing strategies for decentralized models that impact recruitment patterns.
FAQs
1. Why is patient diversity important in UK clinical trials?
Diverse populations ensure trial results are generalisable and reflect real-world patient use, strengthening safety and efficacy data.
2. Does MHRA mandate diversity quotas?
No. MHRA does not mandate quotas but expects sponsors to adopt inclusive recruitment strategies and justify eligibility criteria.
3. How can NHS Trusts support diversity?
Through outreach programmes, partnerships with community organisations, and integration of recruitment into routine healthcare.
4. What are common barriers to diversity in UK trials?
Language barriers, mistrust of research, socioeconomic constraints, and lack of accessible trial sites.
5. Are there UK-specific diversity initiatives?
Yes. NIHR has developed frameworks to strengthen equality, diversity, and inclusion in research.
6. Do sponsors need to report diversity metrics?
While not mandatory, reporting diversity metrics is encouraged and often required for global submissions.
7. How does decentralised research affect diversity?
Decentralised models improve access for patients in remote or underserved communities, supporting diversity goals.
Conclusion
Patient diversity in UK clinical research is both a regulatory expectation and an ethical responsibility. With MHRA and HRA oversight, NHS infrastructure, and NIHR diversity initiatives, the UK has the foundation to improve representation across trials. Sponsors, CROs, and investigators must adopt proactive recruitment strategies, community engagement programmes, and decentralised models to achieve equitable inclusion. By addressing barriers systematically, UK trials can produce results that are scientifically robust, ethically sound, and globally credible.