Abstract
AbstractEarly access programs (EAPs) generally refer to patient access to medicines/indications before marketing authorization, possibly extended to price and reimbursement approval. These programs include compassionate use, which is usually covered by pharmaceutical companies, and EAPs reimbursed by third-party payers. This paper aims at comparing EAPs in four European countries (France, Italy, Spain, UK) and providing empirical evidence on EAPs in Italy. The comparative analysis was conducted through a literature review (including scientific and grey literature), complemented by 30-min semi-structured interviews with local experts. The Italian empirical analysis employed data available on the National Medicines Agency website. Although EAPs are very different across countries, they exhibit some common features: (i) eligibility criteria refer to the absence of valid therapeutic alternatives and a presumed favourable risk–benefit profile; (ii) payers do not allocate a pre-determined budget to these programs; (iii) total spending on EAPs is unknown. The French EAPs seem to be the most structured, financed through social insurance, covering pre-marketing, post-marketing and pre-reimbursement phases and providing for data collection. Italy’s approach to EAPs has been varied, with several programs covered by different payers, including the cohort-based 648 List (for both early access and off-label use), the nominal-based 5% Fund, and Compassionate Use. Most applications to EAPs are from the Antineoplastic and immunomodulating drug class (ATC L). Some 62% of indications in the 648 List are either not under clinical development or have never been approved (pure off-label use). For those subsequently approved, most approved indications coincide with those covered through EAPs. Only the 5% Fund provides data on economic impact (€ 81.2 million in 2021; average cost per patient € 61.5K). Diverse EAPs are a possible source of inequalities in access to medicines across Europe. A harmonization of these programs, though difficult to achieve, could be modelled on the French EAPs and provide key advantages, not least of which a common effort to collect real-world data in parallel with clinical trials and clear separation between EAPs and off-label use programs.
Reference17 articles.
1. https://www.ema.europa.eu/en/human-regulatory/research-development/compassionate-use. European Medicines Agency (EMA). https://www.EmaEuropaEu/En/Human-Regulatory/Research-Development/Compassionate-Use n.d.
2. Pignatti F, Gravanis I, Herold R, Vamvakas S, Jonsson B, Marty M. The European Medicines Agency: an overview of its mission, responsibilities, and recent initiatives in cancer drug regulation. Clin Cancer Res. 2011;17:5220–5. https://doi.org/10.1158/1078-0432.CCR-11-0623.
3. Martinalbo J, Bowen D, Camarero J, Chapelin M, Démolis P, Foggi P, et al. Early market access of cancer drugs in the EU. Ann Oncol. 2016;27:96–105. https://doi.org/10.1093/annonc/mdv506.
4. Kempf E, Zalcman G, Lebbe C. National early access programs and clinical trials: what opportunities for early access to therapeutic innovations for patients with malignant melanoma? Cancer. 2021;127:2181–3. https://doi.org/10.1002/cncr.33495.
5. IQVIA. EFPIA Patients W.A.I.T. Indicator 2021 Survey - Updated July 2022. https://www.EfpiaEu/Media/676539/Efpia-Patient-Wait-Indicator_update-July-2022_finalPdf n.d.
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