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Analysis of Competitiveness & Cost-Effectiveness for Clinical Trial Host Country Selection

This analysis explores the current competitiveness and cost-effectiveness of different countries as potential host locations for clinical trials. Factors such as technological development, research infrastructure, human resources, and improved ethics in clinical research are considered. The study also examines advantages and disadvantages of leading countries in clinical trials.

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Analysis of Competitiveness & Cost-Effectiveness for Clinical Trial Host Country Selection

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  1. Analysis of Current Competitiveness and Cost-Effectiveness to Select the Host Country for a Clinical TrialNameInstitutional Affiliation

  2. Introduction • In modern society, drug companies face challenges in conducting new clinical trials (Biehl, 2006). • The amount of drugs entering global market has reduced. • Cost of clinical trials have escalated, R&D productivity slipping (Piachaud, 2002). • Therefore, there is increased need for cost-effective clinical trials • Countries are making efforts to provide the best environment for clinical trials leading to global competition.

  3. Offshoring Clinical Trials • Clinical trials are proven procedures of drug innovation (Piachaud, 2002). • Most clinical trial companies include biotechnology and pharmaceutical industries, hospitals, governments, ad research institutions (Boggs and Bayuk, 2009). • Clinical trial research promotes positive health outcomes significant for economic and social benefits. • Trials include screening, early treatment, improved medical procedures, and clinical management (Thakur & Rutgers University, 2010).

  4. Offshoring Clinical Trials Cont… • Most pharmaceutical companies have marginalized drug development procedures leading to seeking of new locations (Maiti & Raghavendra, 2007). • Most clinical research is based on ethical and regulatory frameworks. • Therefore, there is increased competitiveness and desire to conduct cost-effective trials (Petryna, 2009). • CROs development has promoted procedures of locating research site and other activities for cost-effectiveness. • CROs development has led to new trend in clinical research (Lamb & Setley, 2005).

  5. Major Countries Leading in Clinical trials • United States with $64 million investment • Asia • United Kingdom • Belgium • Rest of the World (RoW) countries with 6500 sites (Gross & Hirose, 2007) • India with 40-50 % lower than developed nations • China, Eastern and Central Europe, and South America are also emerging markets for clinical trials representing 36 % patient enrolment (European Commission, 2011).

  6. Advantages and disadvantage of Clinical Trials in Leading Nations • UK has barriers of unfavorable national regulations and legislation, lack of GCP. • Advantages include R&D investments, website development (Thiers, 2008). • Netherlands barriers include; unattractive legislation and long approval times • Netherlands key strengths include; robust patient information systems clinical trial agreements, insurance standardization, and good economy (Medicines Australia, 2011).

  7. Advantages and disadvantage of Clinical Trials in Leading Nations • Barriers of France includes, high number of clinical trial specialists, human resources to support investigators and short approval times • Challenges in France includes, high taxation on pharmaceutical products, neglect of small institutions • Australia strengths includes, strong R&D estimated at $29.5 billion, high quality infrastructure, ethically diverse population (PWC, 2012). • Weaknesses in Australia includes, geographically dispersed population and expensive Phase II and III trials

  8. Factors to Consider When Selecting a Host Country for Clinical Trials Technological Development • Pharmaceutical companies consider level of technology (Marks and Power, 2002) • Investment in website • Technological stakeholder initiatives (Patel and Vega, 1999) • Online networks • Digitalized clinical trials that offers patients with fast and easy to use information • Online participation and tools of decision support that facilitate process of informed consent (McKelvey & Orsenigo, 2002)

  9. Research Infrastructure and Human Resource • clinical trials are based on the high-quality input to research methodology (Archibugi and Pietrobelli, 2003). • Existence of clinical trial units that provide advice and support for design and analysis of clinical results. • A strong expertise capacity in disease outbreak areas (Patel & Vega, 2009). • Establishment of a public interest group to merge private and public clinical research stakeholders. • Specialist research centers • Training and education support (World Health Organization, 2013).

  10. Improved Ethics in Clinical Research Trials • main issues raised included the standard of care, reasonable availability, and the quality of informed consent (McAdam, 2004). • Absence of controversies on ethical issues • Existing ethical framework of a host nation • Reduced levels of exploitation of research subjects (Schüklenk, 2000). • Presence of developed partnerships with the markers of health policies, researchers, and the community (Kazdin, 2003). • Involvement in partnerships in sharing responsibilities

  11. Improved Ethics in Clinical Research Trials • Recognition of social value when selecting a host country for clinical trials (Levine, 2009). • Streamlined governance and ethics processes • Presence of developed individual centralized ethical review processes. • Jurisdictions on ethical reviews • Reviewing and monitoring clinical research trials • Established codes of conducting ethical clinical trials (Tal, 2011).

  12. Clinical Grant Development • Clinical grants bolster the credibility of CROs • Support given by host country to clinical trials (Lead Discovery, 2006). • Existence of medical research charities. • Offers on medical research grant charities to strengthen and support their research base. • Development of UK Clinical Research Network and building of internal expert research workforce (PWC, 2012). • Presence of constituted of dedicated and highly trained research staff in the healthcare

  13. Clinical Grant Development • Presence of research grant programs • Contribution by funding investigator-initiated and non-pharmaceutical trials (World Health Organization, 2013). • Clinical trial grants provide the additional support necessary for maintaining the quality of human capital • Provision of grants to hospitals • Funding of pilot studies (Reichert, 2003).

  14. Growing Pressure of R&D Spend • Increased Investment in R & D • Economic development of the host country • Return on revenue of pharmaceuticals (Roux, Pratt and Tengs, 2008). • Enhanced financial regulations • Drug prices • Existence of social security funds (PWC, 2012). • Better percentage of the budgetary financial allocations • Percentage share of total R & D budget used to support clinical trials (Petryna, 2009).

  15. Growing Pressure of R&D Spend cont.… • Budgetary allocation favorable for competitive clinical trials • Presence of a flexible framework based on ‘live licensing’ approach (Brown, Dunn & Butow, 2008). • Introduction of R & D Tax Credit in various phases of clinical trials, such an in Australia • Technological adjustment of R&D positions. • Level of internationalization and globalization of R&D-specific factors (Gattellari & MacLeod, 1999). • Degree of cooperation between R & D units • formulation of a clear strategic plan to promote clinical trials (Ellis, Dowsett & Tattersall, 1999).

  16. Promoting Clinical Trials • Offers competitiveness and cost effectiveness of clinical trial initiatives • There are current challenges stemming from clinical trial environments (Butow, Brindle and McConnell,1998). • Future environment presents better opportunities. • Emergence of evidence-based medicine promotes data gathering in clinical development and practice (Antonakis, 2001). • Development of ‘live licensing’ ensures continuous post-approval data gathered.

  17. Promoting Clinical Trials cont.… • Requires increased emphasis on traditional research • Current professionalism in research centers promotes clinical trials (Thakur & Rutgers University, 2010). • Existence of health economic data leads to transparent clinical trial activities. • Biobanking would increase competitiveness and cost-effectiveness. • Patient empowerment increases transparent clinical trials (Hrobjartsson & Gotzsche, 2001). • Increased patient access to clinical trials ensures competitiveness and cost-effectiveness.

  18. Promoting Clinical Trials cont.… • Revising and streamlining the clinical trial submission in process • development a procedure of co-operation between member states (Valdez-Martinez &Turnbull, 2006) • create a single submission portal regarding clinical trial applications • Upgrading of local clinical trials • Establishment of collaborative models of clinical trials. • Application of public to private partnerships, licensing arrangements, and co-development or outsourcing promotes clinical trials (TheLancet (2007).

  19. Promoting Clinical Trials cont.… • Standardization of clinical trials • Better patient recruitment approaches • Centralization of cost-effective trials (Commonwealth of Australia, 2011). • Improving clinical trial environment for further attraction • Integration of networks of specialized centers and high quality expertise. • Promotion of pooling and sharing of best practice and knowledge in clinical trials. • Better consultation among clinical trial stakeholders (Commonwealth of Australia, 2011).

  20. Promoting Clinical Trials cont.… • Requires standardization and setting up of ‘one-stop shop’ such as online portal for clinical trial submissions • standardization and harmonizing all the administrative tasks and procedures • Establishment of informed consent forms and procedures of negotiating contract agreements. • localization of favorable clinical trial participants • Support to clinical trials through facilitation to access to innovative drugs, capping the cost and fees that can be charged by clinical sites and investigators • Addressing barrier concerns • Enhancing biobanking regulations

  21. Conclusion • There is more to clinical trial than it is anticipated • Clinical trials creates employment, improves health of citizens, and provides revenue returns. • Ensuring selection of a better host country requires informed analysis of various factors including, R&D position, economy, health infrastructure, ethical concerns, and technological developments.

  22. References • Achilladelis, B & Antonakis, N. (2001). The dynamics of technological innovation: the case of the pharmaceutical industry. Research Policy (30), 535–588. • Archibugi, D. & Pietrobelli, D. (2003). The globalization of technology and its implications for developing countries: Windows of opportunity or further burden? Technology Forecasting and Social Change, (70), 861-883. • Biehl J. (2006). Pharmaceutical governance. In Petryna A. Lakoff A. & Kleinman A. (Eds), Global pharmaceuticals: Ethics, markets, practices. Durham, NC: Duke University Press. • Boggs, R, & Bayuk, L. (2009). Speeding developing cycles. Research Technology Management 42 (5), 33-38.

  23. References • Brown R, Dunn S. M, & Butow, P. (2008). Meeting patient expectations in the cancer consultation. Annals of Oncology, 8(9): 877-882. • Butow P. N, Brindle L. & McConnell D. (1998). Information booklets about cancer: Factors influencing patient satisfaction and utilization. Patient Education and Counseling, 33: 129-141. • Commonwealth of Australia. (2011). Clinically competitive: Boosting the business of clinical trials in Australia. Clinical trials action group report. Joint Submission to the Clinical Trials Action Group: • Ellis, M., Dowsett, M. & Tattersall N. (1999). Attitudes to randomised clinical trials among outpatients attending a medical oncology clinic. Health Expectations,1999, 2: 33-43.

  24. References • European Commission - European Medicines Agency: Report on the Conference on the Operation of the Clinical Trials Directive (Directive 2001/20/EC) and Perspectives for the Future. • Gattellari, M. & MacLeod, C. (1999). Misunderstanding in cancer patients: Why shoot the messenger. Annals of Oncology, 10: 39-46. • Gross, A. & Hirose, M. (2007). Conducting clinical trials in Asia. Pacific Bridge Medical • Hrobjartsson, A. &, Gotzsche P. C (2001). Is the Placebo Powerless? An Analysis of Clinical Trials Comparing Placebo with No Treatment. The New England Journal of Medicine, 344: 1594-1602. • Kazdin, A. E. (2003). Methodological issues & strategies in clinical research. Washington, DC: American Psychological Association. • Lamb, M. & Setley, D. (2005). Clinical Trial Logistics: The trial of Emerging Markets. Clinical Trial Services (November), 5.

  25. References • Lead Discovery. (2006). The Clinical Trials Market 2006. LeadDiscovery. 13 October. • Levine R. (2009). Ethics and Regulation of Clinical Research. New Haven and London: Yale University. Press. • Maiti, R. & Raghavendra, M. (2007). Clinical trials in India. Pharmacological Research, (56), 1-10. • Marks, L. and E. Power (2002). Using technology to address recruitment issues in the clinical trial process. Trends in Biotechnology 20 (3), 106-109. • McAdam, K. (2004). The Ethics of Research Related to Health Care in Developing Countries. ActaBioethica2004; 1: 49-55. • McKelvey, M. & Orsenigo, L. (2002). Pharmaceuticals as a sectorial innovation system’ paper presented at DRUID Academy Winter 2002 PhD Conference. • Medicines Australia. (2011). Keeping clinical trials in Australia why action is needed now. Occasional paper series 3. main.medaus.com.au/files/2011/02/Occasional-Paper-3...

  26. References • Patel, P. & Vega, M. (1999). Patterns of internationalization of corporate technology: location vs. home country advantages’, Research Policy (28), 145–155. • Patel, P. and M. Vega (2009). Patterns of internationalization of corporate technology: location vs. home country advantages’, Research Policy (28), 145–155. • Petryna, A. (2009). When experiments travel: Clinical trials and the global search for human subjects. Princeton: Princeton University Press. • Piachaud, B. (2002). Outsourcing in the pharmaceutical manufacturing process: an examination of the CRO experience. Technovation(22), 81-90. • PWC. (2012). Clinical research footprint and strategic plan to promote clinical trials in Belgium. Giving impetus to clinical trials in Belgium. • Reichert, J. (2003). Trends in development and approval times for new therapeutics in the United States’, Nature Reviews, (2), 695-702.

  27. References • Roux L, Pratt M, & Tengs T. (2008). Cost effectiveness of community-based physical activity interventions. Am J Prev Med; 35:578-88. • Schüklenk, H. (2000). Protecting the vulnerable: testing times for clinical research ethics. Social Science and Medicine,( 51), 969-977. • Tal, J. (2011). Strategy and statistics in clinical trials: A non-statisticians guide to thinking, designing, and executing. Amsterdam: Academic Press. • Thakur, P., & Rutgers University. (2010). Offshoring and outsourcing of core corporate activities: The global relocation of pharmaceutical industry clinical trials. • TheLancet (2007). Editorial: Strengthening clinical research in India. TheLancet, 369, 1233. • Thiers F. (2008). Trends in the globalization of clinical trials. Nat Rev Drug Discov 2008, 7:13-14. • Valdez-Martinez, E., & Turnbull, B. (2006). Descriptive Ethics: A quality study of local research ethics committees in Mexico’ Developing World Bioethics 6 (2), 95-105. • World Health Organization. (2013). Guidelines for good clinical practice (GCP) for trials on pharmaceutical products. The Use of Essential Drugs Sixth report of the WHO Expert Committee. Geneva. 97–137.

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