Does market exclusivity hinder the development of Follow-on Orphan Medicinal Products in Europe?

Anne E M Brabers; Ellen H M Moors; Sonja van Weely; Remco L A de Vrueh

doi:10.1186/1750-1172-6-59

Does market exclusivity hinder the development of Follow-on Orphan Medicinal Products in Europe?

Orphanet J Rare Dis. 2011 Sep 5:6:59. doi: 10.1186/1750-1172-6-59.

Authors

Anne E M Brabers¹, Ellen H M Moors, Sonja van Weely, Remco L A de Vrueh

Affiliation

¹ NIVEL, Netherlands Institute for Health Services Research, PO Box 1568, 3500 BN Utrecht, The Netherlands. a.brabers@nivel.nl

Abstract

Background: We determined whether the market exclusivity incentive of the European Orphan Drug Regulation results in a market monopoly or that absence of another Orphan Medicinal Product (OMP) for the same rare disorder, a so-called follow-on OMP, is a matter of time or market size. In the interest of rare disorder patients better understanding of the effect of the market exclusivity incentive on follow-on OMP development is warranted.

Methods: First, the impact of various market-, product- and disease-related characteristics on follow-on OMP development in the EU was determined by comparing rare disorders with an approved OMP and at least one follow-on OMP (N = 26), with rare disorders with an approved OMP and no follow-on OMP (N = 18). Next, we determined whether manufacturers continued development of a follow-on OMP upon approval of the first OMP for the intended rare disorder. Since in the EU significant benefit of an OMP has to be established, we determined for each follow-on OMP for which development was continued on what grounds significant benefit was assumed by the sponsor. Data were collected from the public domain only.

Results: The likelihood of a rare disorder with an approved OMP to obtain at least one follow-on OMP development was strongly associated with disease prevalence, turnover of the first OMP, disease class, disease-specific scientific output and age of onset. Out of a total of 120 follow-on OMPs only one follow-on OMP could be identified for which development was discontinued upon approval of the first OMP for the same rare disorder. Only a substantial level of discontinuation of follow-on OMP development would have indicated the existence of a market monopoly. Moreover, sponsors that continued development of a follow-on OMP predominantly assumed that their product had an improved efficacy compared to the first approved OMP.

Conclusions: This study provides evidence that absence of follow-on OMP development is a matter of time or market size, rather than that the market exclusivity incentive of the European Orphan Drug Regulation creates a market monopoly.

MeSH terms

Drug Approval / legislation & jurisprudence
Drug Approval / statistics & numerical data*
Drug Design
Drug Industry / economics*
Drug Industry / legislation & jurisprudence
Drug Industry / trends
Europe
Humans
Orphan Drug Production / economics*
Orphan Drug Production / legislation & jurisprudence*
Orphan Drug Production / methods
Orphan Drug Production / statistics & numerical data
Prevalence
Rare Diseases / drug therapy*
Rare Diseases / epidemiology