Insulin Federalism
In: Boston University Journal of Science and Technology Law, Band 27
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In: Boston University Journal of Science and Technology Law, Band 27
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In: Jordan Paradise, COVID-IP: Staring Down the Bayh-Dole Act with 2020 Vision, 7 Journal of Law & the Biosciences 1 (2020).
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Working paper
In: Jordan Paradise, Three Framings of "Faster" at the FDA and the Federal Right to Try, 11 Wake Forest Journal of Law & Policy 53 (2020).
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In May 2018, Congress passed the controversial Right to Try ("RTT") Act, creating a process for terminally ill patients to request access to investigational drugs. The federal RTT Act is not the first legal mechanism that fosters quicker access to investigational drugs. This new right to try is distinct from existing pathways created by law, regulation or federal administrative agency policy. Various mechanisms facilitated by the U.S. Food and Drug Administration ("FDA") are significantly more substantial and important in the context of "faster" access to therapeutic products. These mechanisms lie along a spectrum of product development spanning investigational new drug status to postmarket studies and surveillance. I categorize these mechanisms into three areas: expansion, acceleration, and extension. The federal right to try can be characterized as an expansion, expanding patient access to investigational new drugs as an alternative mechanism to the FDA's long-standing expanded access program. As the Senate notes, the RTT Act "does not establish a new entitlement or modify an existing entitlement, or otherwise establish a positive right" and "is consistent with and will act as an alternative pathway alongside existing expanded access policies of the Food and Drug Administration." This article positions the new RTT in proper context and explores additional FDA mechanisms that serve to speed up patient access. In Part I, this article will first discuss the content and scope of the RTT legislation, as well as the reasoning for the support and opposition for the legislation. The legislation is only four pages long, as enacted, and introduces a concise procedure for requests for access to investigational drugs. The article will next examine FDA mechanisms for expansion in Part II, comparing the RTT with the current expanded access program at the FDA. Part II will explore two mechanisms of expansion at the FDA: expanded access for patients to investigational drugs and devices (the "expanded access" program) and expanded input from patients about experiences with drugs and devices under review at the FDA ("patient experience" data). This expansion of patient input was initiated and implemented within the FDA but further directed by provisions within the 21st Century Cures Act. Part III will analyze several mechanisms of accelerated review and approval at the FDA, including FastTrack status, priority review, accelerated approval, Orphan Drug status, and Breakthrough designation of promising therapeutics. The collection of hastened mechanisms of review and approval are poorly understood and have led to confusion and misunderstanding by physicians and patients alike. They also alter the foundational new drug approval framework originally set forth by Congress in the Kefauver-Harris Drug Amendments enacted in 1962, which strengthened the drug approval process to include not only premarket safety review but also substantial evidence of efficacy demonstrated through "adequate and well-controlled" clinical trials. Recent empirical scholarship informs this Part, revealing that the growing array of statutory mechanisms to speed up clinical trials, review, and approval are cutting away at long-standing protections afforded by robust measures of safety and efficacy. Part IV will then discuss extension at the FDA, particularly the extension of evidence gathering in post-market clinical trials to support showings of safety and efficacy. The article concludes with several reflections on the relationship of the federal RTT to these FDA mechanisms of "faster" access, as well as potential implications of expansion, acceleration, and extension on patient safety, patent protections, and drug costs.
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In: 44 American Journal of Law and Medicine 309 (2018)
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In: Jordan Paradise, Regulatory Frameworks for Precision Medicine at the Food & Drug Administration, 15(1) SciTech Lawyer 12 (2018).
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In: Minnesota Law Review, Band 102
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Working paper
In: 41 American Journal of Law and Medicine 49 (2015).
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In: Northwestern Journal of Technology and Intellectual Property, Band 10, Heft 3, S. 169-207
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In: Seton Hall Law Review, Band 41, S. 501
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In: Jordan Paradise, Reassessing Safety for Nanotechnology Combination Products: What Do Biosimilars Add to Regulatory Challenges for the FDA?, 56 St. Louis U. L. J. 465 (2012).
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In: 117 Penn St. L. Rev. 53 (2012).
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In: John D. Blum & Jordan Paradise, Public Health Preparedness & Response: An Exercise in Administrative Law, 20 DEPAUL J. HEALTH CARE L. 1, 2019
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Responses to epidemics, pandemics, and other biological disasters require multiple coordinated initiatives that combine sophisticated planning, sound emergency management, effective stockpiles, solid geographic information systems, well-developed laboratory surveillance and response, and effective management capabilities. Critical to the noted elements of planning and response is the existence of a legal structure, which underpins the operations of necessary programs. While the law may not be the first public health tool considered in a disaster, it is fundamental to the effective functioning of multiple actors and must be harmonized across jurisdictional lines. This article explores the role of law in pandemics and other biological catastrophes, highlighting broad developments in public health law that have been sparked by recent events. The piece will consider general responses and trends in health disaster management in the context of administrative law with a particular focus on agency responses. Background discussion will also offer a broad overview of the evolution of federal and state laws, highlighting core areas where parallel legal frameworks have developed. The second half of this essay will paint a more detailed portrait of administrative law responses to public health disasters focusing on the Food and Drug Administration ("FDA"), exploring medical countermeasures pursued by this agency to enhance preparedness and response. Key FDA legislation and recent guidance, as well as emergency use authorization ("EUA") policies, will be analyzed, as a case study of how a pivotal agency has been shaped through law to deal with public health crises.
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In: Journal of Law, Medicine & Ethics, Vol. 37, pp. 543-545, 2009
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