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Case Studies of Expedited Review: AZT and L-Dopa

Published online by Cambridge University Press:  29 April 2021

Extract

The HIV epidemic has led to a reassessment of attitudes regarding public access to new therapeutic agents for the treatment of life-threatening and severely debilitating diseases. People with AIDS and their advocates have relentlessly attacked the process by which new drugs are developed and approved for marketing in this country, a process characterized as overly conservative, risk-averse, and paternalistic. In response to growing pressure to accelerate access to important new therapeutic agents, the Food and Drug Administration (FDA) has issued several bold initiatives designed to facilitate the development of experimental drugs used in the treatment of serious or immediately life-threatening diseases.

The clinical testing and regulatory review of new therapeutic agents in the United States are lengthy processes. A recent analysis of new chemical entities (NCE) approved by the FDA in 1987,1988, and 1989 has revealed that, on average, the clinical development phase for new drugs exceeds five years (63 months).

Type
Article
Copyright
Copyright © American Society of Law, Medicine and Ethics 1991

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References

Kaitin, K.I. DiCerbo, P.A. Lasagna, L., “The New Drug Approvals of 1987, 1988, and 1989: Trends in Drug Development”, Journal of Clinical Pharmacology, 31(1991): 116–22, at 117.Google Scholar
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Supra note 20.Google Scholar
This finding was corroborated in a recent PAR update covering the years 1985 and 1986. See Richard, B.W. Melville, A. Lasagna, L., “Postapproval Research as a Condition of Approval: An Update, 1985–1986”, Journal of Clinical Research and Drug Development, 3(1989): 247–57.Google Scholar
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