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The '''Antibiotic Development to Advance Patient Treatment (ADAPT) Act''' ({{USBill|113|HR|3742}}) was introduced in the [[United States Congress|U.S. Congress]] on December 12, 2013 by Representative [[Phil Gingrey]] of Georgia and fifty-two cosponsors. Responding to the lack of financial incentives for drug manufacturers to innovate new antibiotics and antifungals and the regulatory barriers to their doing so, it proposed an expedited pathway for testing drugs intended for diseases for which no cure yet existed. After it died in committee, a similar version of the Act was re-introduced by Representative [[John Shimkus]] of Illinois and his cosponsor Representative [[Gene Green]] of Texas. Though this Act likewise failed to make it out of committee, several of its provisions were codified in the [[21st Century Cures Act]], which was signed into law on December 13, 2016. These include the expedited testing pathway for new antibiotics and a similar provision for [[Antibiotic sensitivity|antimicrobial susceptibility tests]].


== Background ==
The '''Antibiotic Development to Advance Patient Treatment (ADAPT)''' Act of 2013 was introduced in the [[U.S. Congress]] on 12 December 2013.


=== Antibiotic resistance and the barriers to new treatments===
The ADAPT Act aims to fast track the drug development in order to combat the growing [[public health]] threat of 'superbugs'. Under this Act, FDA can approve antibiotics and antifungals needed for life-threatening infections based on data from smaller [[clinical trial]]s.
The cost of [[Antimicrobial resistance|antibiotic resistance]], in dollars and in lives, motivated the Act’s sponsors and the community stakeholders that supported its passage. In September 2014, the [[United States House Energy Subcommittee on Health|Subcommittee on Health]] of the [[United States House Committee on Energy and Commerce|House Committee on Energy and Commerce]] held a hearing at which officials from the [[Food and Drug Administration]] (FDA), [[The Pew Charitable Trusts|Pew Charitable Trusts]], and other organizations testified in favor of the ADAPT and 21st Century Cures Acts.<ref>''21st Century Cures: Examining Ways to Combat Antibiotic Resistance and Foster New Drug Development; Hearing Before the Subcommittee. on Health of the Comm. on Energy and Commerce'', 113th Cong. (2014) [hereinafter ''Hearing Before Health'' ''Comm.''].[https://archive.org/stream/gov.gpo.fdsys.CHRG-113hhrg93933/CHRG-113hhrg93933_djvu.txt]</ref> Opening the hearing, Subcommittee Chairman [[Joe Pitts (Pennsylvania politician)|Joseph R. Pitts]] (R-PA) quoted then-Prime Minister [[David Cameron|David Cameron’s]] recent admonition that failure to “confront the threat of antibiotic resistance” could “cast [humanity] back into the dark ages.”<ref>''Hearing Before Health Comm.'', ''supra'', at 1 (statement of Joseph R. Pitts, Pennsylvania Rep. and Chairman of the Subcomm. on Health).[https://archive.org/stream/gov.gpo.fdsys.CHRG-113hhrg93933/CHRG-113hhrg93933_djvu.txt]</ref> Speaking at this same hearing, Representative Phil Gingrey (R-GA) (the 2013 Act’s principal sponsor) referenced [[Centers for Disease Control and Prevention|Centers for Disease Control]] (CDC) statistics, which placed the number of Americans who die from drug-resistant infections each year at around 23,000.<ref name="Hearing at 5">''Hearing Before Health Comm.'', ''supra'', at 5 (statement of Phil Gingrey, Georgia Rep.).[https://archive.org/stream/gov.gpo.fdsys.CHRG-113hhrg93933/CHRG-113hhrg93933_djvu.txt]</ref> Representative Gingrey asserted that the financial losses from such infections amount to $55 billion annually.<ref name="Hearing at 5"/> Representative John Shimkus (R-IL) would later note these same figures in a House debate over the Acts in July 2015.<ref>Press Release, Congressman John Shimkus, With Over 10,000 Diseases and Only 500 Treatments--Shimkus Votes for Cures (July 10, 2015) ("Each year in the United States, at least 2 million people are infected with an antibiotic-resistant bacteria and at least 23,000 of them die as a direct result of those infections, according to the CDC.").[https://shimkus.house.gov/media-center/press-releases/with-over-10000-diseases-only-500-treatments-shimkus-votes-for-cures]</ref>


Equally worrisome to the ADAPT Act’s proponents were the economic and regulatory impediments to developing new treatments for drug-resistant illnesses. Citing the FDA, Representative Gingrey lamented during the 2014 hearing that “new antibiotic approval ha[d] decreased by 70 percent since the mid 1980s.”<ref name="Hearing at 5"/> Representative [[Michael C. Burgess]] (R-TX) likewise took issue with the “lack of a pipeline of new drugs” to respond to the threat of super bugs.<ref>''Hearing Before Health Comm.'', ''supra'', at 3 (statement of Michael C. Burgess, Texas Rep.).[https://archive.org/stream/gov.gpo.fdsys.CHRG-113hhrg93933/CHRG-113hhrg93933_djvu.txt]</ref> Several blamed inadequate market incentives for this paucity of remedies. As Dr. Barbara E. Murray, then-President of the [[Infectious Diseases Society of America]], observed, “Antibiotics are typically priced low [and] used for a short duration.”<ref>''Hearing Before Health Comm.'', ''supra'', at 60 (statement of Barbara E. Murray, MD, President of the Infectious Disease Society of America.).[https://archive.org/stream/gov.gpo.fdsys.CHRG-113hhrg93933/CHRG-113hhrg93933_djvu.txt]</ref> Pharmaceutical companies can reap greater returns in other areas of research; hence, the development of new antibiotics flounders.<ref>''See Hearing Before Health Comm.'', ''supra'', at 4 (statement of Frank Pallone, New Jersey Rep.).[https://archive.org/stream/gov.gpo.fdsys.CHRG-113hhrg93933/CHRG-113hhrg93933_djvu.txt]</ref>
The [[Centers for Disease Control and Prevention|CDC]] will reinforce the monitoring of the use of [[antibiotic]]s that treat serious and life-threatening infections and the emerging resistance, and make the data publicly available. The [[FDA]] antibiotics labeling process, 'Susceptibility Test Interpretive Criteria for Microbial Organisms'' or 'breakpoints' is also streamlined to allow the most up-to-date and cutting-edge data available to healthcare professionals under the new Act.<ref>{{cite web|url=http://green.house.gov/press-release/green-gingrey-introduce-adapt-act-safeguard-public-health|title=Green, Gingrey Introduce ADAPT Act to Safeguard Public Health|author=Press Release|publisher=U.S .Congress|date=12 December 2013}}</ref><ref>{{cite web|url=http://assets.fiercemarkets.net/public/lifesciences/HR3742.pdf|title=Antibiotic Development to Advance Patient Treatment Act of 2013|publisher=U.S. Congress|date=12 December 2013}}</ref> 


Compounding the scant financial motives for drug development, creators of new treatments were made to contend with "serious regulatory barriers".<ref name="Hearing at 61">''Hearing Before Health Comm.'', ''supra'', at 61 (statement of Barbara E. Murray, MD, President of the Infectious Disease Society of America.).[https://archive.org/stream/gov.gpo.fdsys.CHRG-113hhrg93933/CHRG-113hhrg93933_djvu.txt]</ref> Dr. Murray observed that the small number of patients infected by novel diseases made it difficult for manufacturers to find enough test subjects in order to comply with federal agencies’ n-count requirements.<ref name="Hearing at 61"/> The unavailability of diagnostic tests for these new infectious agents also demanded a large investment to find eligible study participants, while generating little information about drug effectiveness.<ref name="Hearing at 61"/> Stagnant innovation becomes self-perpetuating. The more antibiotics to which a pathogen becomes resistant, the fewer controls there are against which to measure an experimental treatment.<ref name="Hearing at 61"/>
Congress has been urged in 2014 from several parties to aid the development of new drugs via bills such as ADAPT. Allan Coukell, director of drugs and medical devices at The [[Pew Charitable Trusts]], testified in front of the House Committee, in a statement published by [[Reuters]], that "By allowing drug developers to rely on smaller datasets, and clarifying FDA's authority to tolerate a higher level of uncertainty for these drugs when making a risk/benefit calculation, ADAPT would make the clinical trials more feasible."<ref>{{cite web|last1=Clarke|first1=Toni|title=U.S. Congress urged to pass bill to speed development of antibiotics|url=http://www.reuters.com/article/2014/09/19/us-usa-congress-antibiotics-idUSKBN0HE25W20140919|publisher=Reuters|accessdate=19 September 2014}}</ref>


==References==
===The GAIN Act===
In 2012, one of Congress’s earliest attempts at rectifying these barriers to new drug-resistant antibiotics came in the form of the [[GAIN Act|Generating Antibiotics Now (GAIN) Act]].<ref name="Khachatryan">''See'' Kevin Khachatryan, Note, ''[https://journals.library.columbia.edu/index.php/stlr/article/view/4014 Incentivizing Drug Development: Novel Reforms of Pharmaceutical Innovation]'', 18 COLUM. SCI. & TECH. L. REV. 139, 156-57 (2016).</ref> GAIN was passed as an amendment to the [[Federal Food, Drug, and Cosmetic Act|Federal Food, Drug, and Cosmetic (FD&C) Act]].<ref name="Khachatryan"/> Its strategy for generating new antibiotics is to offer manufacturers an artificial monopoly on any qualifying drugs that they produce.<ref name="Khachatryan"/> Such drugs must treat illnesses with “the potential to pose a serious threat to the public health.”<ref name="Khachatryan"/> However, beyond this blanket criterion, GAIN gave significant deference to the Secretary of the [[United States Department of Health and Human Services|Department of Health and Human Services]] (the Secretary).<ref name="Khachatryan"/> This latitude was subject only to the requirements that she consider a given pathogen’s “impact on public health” and “morbidity and mortality rates” and consult with the CDC, FDA, and the medical community.<ref name="Khachatryan"/> Manufacturers who satisfied GAIN’s conditions were guaranteed five years of market exclusivity over the pertinent drug.<ref name="Khachatryan"/> These years could stack with the drug’s “five year exclusivity as a [[new chemical entity]] (NCE), three year clinical investigation exclusivity, and seven-year [[orphan drug]] exclusivity.” Moreover, any qualifying drugs were eligible for fast-track review.<ref>''See'' Kevin Khachatryan, Note, ''[https://journals.library.columbia.edu/index.php/stlr/article/view/4014 Incentivizing Drug Development: Novel Reforms of Pharmaceutical Innovation]'', 18 COLUM. SCI. & TECH. L. REV. 139, 157-58 (2016).</ref>
{{reflist}}


GAIN’s value proposition proved to be an effective one. As Representative [[Frank Pallone]] (D-NJ) commented during the 2014 ADAPT Act hearing, within two years, GAIN had led to FDA approval of numerous new antibiotics.<ref name="Hearing at 4">''Hearing Before Health Comm.'', ''supra'', at 4 (statement of Frank Pallone, New Jersey Rep.).[https://archive.org/stream/gov.gpo.fdsys.CHRG-113hhrg93933/CHRG-113hhrg93933_djvu.txt]</ref> The expedited review procedure further ensured that these drugs would be “able to combat an imminent infectious disease threat and reach patients at an accelerated pace".<ref name="Hearing at 4"/> At the same time, Representative Pallone and others were concerned about the consumer harms that these decades of exclusivity might yield. Representative [[Henry Waxman|Henry A. Waxman]] (D-CA) warned that exclusivity “allow[s drug companies] to charge higher prices,” which “imposes a significant burden on patients and on the healthcare system overall.”<ref>''Hearing Before Health Comm.'', ''supra'', at 8 (statement of Henry A. Waxman, California Rep.).[https://archive.org/stream/gov.gpo.fdsys.CHRG-113hhrg93933/CHRG-113hhrg93933_djvu.txt]</ref> To justify “the carrot of marketing and regulatory exclusivities,” Representative Pallone exhorted his fellow members of Congress to ensure that their efforts “achieve[] the necessary impact on the pipeline of new drugs.”<ref name="Hearing at 4"/>
[[Category:United States proposed federal health legislation]]


== Provisions ==

===Purpose and Scope===
The ADAPT Act complemented GAIN. Representative Gingrey introduced it to the House as the “logical next step to the GAIN Act.”<ref name="archive.org">''Hearing Before Health Comm.'', ''supra'', at 6 (statement of Phil Gingrey, Georgia Rep.).[https://archive.org/stream/gov.gpo.fdsys.CHRG-113hhrg93933/CHRG-113hhrg93933_djvu.txt]</ref> To that end, it did not merely render the development of new treatments more lucrative but more feasible as well. The centerpiece of this proposal was ADAPT’s creation of a Limited Population Antibacterial Drug (LPAD) approval pathway for certain antibiotics.<ref>Donna Hanrahan, ''Federal Efforts to Reduce Overuse, Curb Misuse, and Incentivize the Development of Antibiotic Drugs'', 26 ANNALS HEALTH L. 67, 85-86 (2017)[http://www.annalsofhealthlaw.com/annalsofhealthlaw/vol__26_issue_1?pg=74#pg74]</ref> Faced with a disease of sufficient severity for which alternatives do not yet exist, ADAPT would empower the Secretary to dispense with the usual testing requirements and allow manufacturers to go to market based on more limited efficacy tests.<ref>''See id.''</ref> As Allan Coukell, Director of Drug, Medical Device, and Food Programs at the Pew Charitable Trusts, observed, a patient with multi-drug-resistant [[pneumonia]] will likely die without access to a new antibiotic.<ref name="ReferenceA">''Hearing Before Health Comm.'', ''supra'', at 113 (statement of Allan Coukell, Director of Drug, Medical Device, and Food Programs, Pew Charitable Trusts).[https://archive.org/stream/gov.gpo.fdsys.CHRG-113hhrg93933/CHRG-113hhrg93933_djvu.txt]</ref> In that case, the uncertainty of an unproven remedy was preferable to the near certainty of death. In conducting such a risk-benefit assessment, ADAPT allowed the FDA to “accept less data” in approving a lifesaving drug.<ref>''Id.''</ref> As Representative Shimkus later commended, this “new, streamlined pathway” saved “thousands of lives” by making [[experimental drug]]s available to those who would otherwise have no cure.<ref>[https://shimkus.house.gov/media-center/press-releases/with-over-10000-diseases-only-500-treatments-shimkus-votes-for-cures Press Release, ''supra'']</ref>

Given the uncertainty inherent in drugs approved via LPAD, ADAPT’s advocates were careful to constrain its reach to “high-need populations” suffering from the gravest threats.<ref name="archive.org"/> Dr. Janet Woodcock, Director of the FDA Center for Drug Evaluation and Research, claimed that ADAPT would be restricted to “rare resistant organisms where there are really very few treatment options available.”<ref>''Hearing Before Health Comm.'', ''supra'', at 37 (statement of Janet Woodcock, Director of the Food & Drug Administration Center for Drug Evaluation and Research).[https://archive.org/stream/gov.gpo.fdsys.CHRG-113hhrg93933/CHRG-113hhrg93933_djvu.txt]</ref> Within the population of patients affected by these diseases, the Act’s application would be further constrained to “the limited population in most need of the therapy, as opposed to all patients.”<ref>''Hearing Before Health Comm.'', ''supra'', at 62 (statement of Barbara E. Murray, MD, President of the Infectious Disease Society of America.).[https://archive.org/stream/gov.gpo.fdsys.CHRG-113hhrg93933/CHRG-113hhrg93933_djvu.txt]</ref> As such, ADAPT would not lower the federal review standard for new drugs, but merely contour it to the needs of “a specific population that is different from the general population.”<ref name="ReferenceA"/>

===Relationship Between the 2013 and 2015 Acts===
The two versions of the ADAPT Act—H.R. 3742 (2013)<ref>Antibiotic Development to Advance Patient Treatment (ADAPT) Act of 2013, H.R. 3742, 113th Cong. (2013).[https://www.congress.gov/bill/113th-congress/house-bill/3742/text]</ref> and H.R. 2629 (2015)<ref>Antibiotic Development to Advance Patient Treatment (ADAPT) Act of 2015, H.R. 2629, 114th Cong. (2015).[https://www.congress.gov/bill/114th-congress/house-bill/2629/text?q=%7B%22search%22%3A%5B%22%5C%22Antibiotic+Development+to+Advance+Patient+Treatment+%5C%22%22%5D%7D&r=1&s=3]</ref>—contain the same three overriding provisions discussed above. Both would amend Section 505 of FD&C (21 U.S.C. § 355) to formally include the expedited testing pathway.<ref>H.R. 3742, § 2(a); H.R. 2629, § 2(b).</ref> Each prescribes certain labeling requirements for manufacturers<ref>H.R. 3742, § 2 (x)(C)[https://www.congress.gov/bill/113th-congress/house-bill/3742/text]; H.R. 2629, § 2(b)(x)(3)[https://www.congress.gov/bill/114th-congress/house-bill/2629/text?q=%7B%22search%22%3A%5B%22%5C%22Antibiotic+Development+to+Advance+Patient+Treatment+%5C%22%22%5D%7D&r=1&s=3].</ref> and charges the Secretary of Health and Human Services with conducting the aforementioned breakpoint review.<ref>H.R. 3742 § 3(a)[https://www.congress.gov/bill/113th-congress/house-bill/3742/text]; H.R. 2629 § 3(a)[https://www.congress.gov/bill/114th-congress/house-bill/2629/text?q=%7B%22search%22%3A%5B%22%5C%22Antibiotic+Development+to+Advance+Patient+Treatment+%5C%22%22%5D%7D&r=1&s=3].</ref> Under a modification to Title III of the [[Public Health Service Act]] (42 U.S.C. § 247b-22), the Secretary is also to monitor “the use of antibacterial and antifungal drugs” as well as “[c]hanges in bacterial and fungal resistance to drugs.”<ref name="congress.gov">H.R. 3742 § 2(c)[https://www.congress.gov/bill/113th-congress/house-bill/3742/text]; H.R. 2629 § 2(g)[https://www.congress.gov/bill/114th-congress/house-bill/2629/text?q=%7B%22search%22%3A%5B%22%5C%22Antibiotic+Development+to+Advance+Patient+Treatment+%5C%22%22%5D%7D&r=1&s=3].</ref> This new responsibility of the Secretary encompasses drugs approved both through LPAD as well as the standard procedure.<ref name="congress.gov"/> The results of the Secretary’s resistance analysis, like the breakpoint research, are to be made public.<ref name="congress.gov"/>

The 2013 and 2015 Acts differed slightly in scope and the precise process they envisioned. Under the 2013 Act, the Secretary could approve drugs to treat “a limited population of patients for which there is an unmet need,” based on her assessment of either traditional comprehensive studies, “datasets of limited size,” “such other confirmatory evidence as [she] deems necessary,” or some combination of the above.<ref>H.R. 3742 § 2(c)[https://www.congress.gov/bill/113th-congress/house-bill/3742/text].</ref> The 2015 version expands this list of sources of proof, holding that the Secretary may consult nonclinical tests—assessments not conducted on humans—in deciding on whether to approve a drug.<ref>H.R. 2629 § 2(g)[https://www.congress.gov/bill/114th-congress/house-bill/2629/text?q=%7B%22search%22%3A%5B%22%5C%22Antibiotic+Development+to+Advance+Patient+Treatment+%5C%22%22%5D%7D&r=1&s=3].</ref>

At the same time, this later version limited the Act’s applicability via a purpose statement with language evocative of a sliding scale. The Act serves to “help expedite the development and availability of treatments for serious or life-threatening bacterial or fungal infections,” but this goal depends on “the severity of the infection and the availability or lack of alternative treatments.”<ref>H.R. 2629 § 2(a)[https://www.congress.gov/bill/114th-congress/house-bill/2629/text?q=%7B%22search%22%3A%5B%22%5C%22Antibiotic+Development+to+Advance+Patient+Treatment+%5C%22%22%5D%7D&r=1&s=3].</ref> Furthermore, the 2015 Act contained a new precondition. In this version of the legislation, the Secretary did not simply decide what level of proof would be necessary for a drug’s approval but actively collaborated with the manufacturer to create a “written agreement” that stipulated the necessary evidence.<ref>H.R. 2629 § 2(b)(x)(1)(A)[https://www.congress.gov/bill/114th-congress/house-bill/2629/text?q=%7B%22search%22%3A%5B%22%5C%22Antibiotic+Development+to+Advance+Patient+Treatment+%5C%22%22%5D%7D&r=1&s=3].</ref> Only if such an agreement is reached may the Secretary approve the drug via the LPAD pathway.<ref>H.R. 2629 § 2(b)(x)(1)(B)[https://www.congress.gov/bill/114th-congress/house-bill/2629/text?q=%7B%22search%22%3A%5B%22%5C%22Antibiotic+Development+to+Advance+Patient+Treatment+%5C%22%22%5D%7D&r=1&s=3].</ref> To the end of reaching this agreement, the 2015 Act provides for consultative meetings between manufacturers and the Secretary.<ref>H.R. 2629 § 2(b)(x)(2)[https://www.congress.gov/bill/114th-congress/house-bill/2629/text?q=%7B%22search%22%3A%5B%22%5C%22Antibiotic+Development+to+Advance+Patient+Treatment+%5C%22%22%5D%7D&r=1&s=3].</ref>

In regard to labeling, the 2013 Act would have mandated that LPAD drugs bear the warning label noted above: “This drug is indicated for use in a limited and specific population of patients.”<ref>H.R. 3742, § 2 (x)(C)[https://www.congress.gov/bill/113th-congress/house-bill/3742/text].</ref> However, on its terms, this requirement applied only to the drug’s [[Medication package insert|“prescribing information”]]—not necessarily to its packaging or bottle.<ref>''Id.''</ref> The 2015 Act broadened the labeling provision. In addition to the warning on prescriptions, this version entailed placing a label on the product itself that states “Limited Population” and features “in a prominent manner . . . adjacent to . . . the brand name of the product.”<ref>H.R. 2629, § 2(b)(x)(3)[https://www.congress.gov/bill/114th-congress/house-bill/2629/text?q=%7B%22search%22%3A%5B%22%5C%22Antibiotic+Development+to+Advance+Patient+Treatment+%5C%22%22%5D%7D&r=1&s=3].</ref>

Finally, the 2015 version of the Act expanded its applicability relative to the prior version. For one, it allowed the Secretary to expand LPAD to new arenas outside its original superbug context. Should she determine “that the public health would benefit from expansion of the limited-use pathway,” other medical areas may be subsumed within the Act’s expedited provisions.<ref>H.R. 2629, § 2(f)[https://www.congress.gov/bill/114th-congress/house-bill/2629/text?q=%7B%22search%22%3A%5B%22%5C%22Antibiotic+Development+to+Advance+Patient+Treatment+%5C%22%22%5D%7D&r=1&s=3].</ref> Secondly, it pulls antimicrobial susceptibility tests into the LPAD pathway. So long as a given test satisfies the exigency conditions for antimicrobial drug treatments, “the Secretary may authorize the marketing of such device” under LPAD—subject to cautionary labeling requirements.<ref>H.R. 2629, § 2(e)[https://www.congress.gov/bill/114th-congress/house-bill/2629/text?q=%7B%22search%22%3A%5B%22%5C%22Antibiotic+Development+to+Advance+Patient+Treatment+%5C%22%22%5D%7D&r=1&s=3].</ref>

===Limitations===

Kevin Khachatryan noted, that the ADAPT Act did not impose responsibilities for [[Antimicrobial stewardship]] for antibiotics developed under this pathway.”<ref>Khachatryan, ''supra'', at 161.</ref> Coupled with the incentive for manufacturers to produce all that they can during their monopoly window, “[t]his can lead to overuse of these antibiotics and contribute to resistant microbes.”<ref>''Id.'' at 162.</ref> Additionally, the Act placed a premium of speed while sidelining other objectives of testing, namely diverse representation among test subjects.<ref>''Id.''</ref> This could impede the gathering of data about certain populations respond to experimental drugs, namely “women, children, and [the] elderly.”<ref>''Id.''</ref>

== Incorporation into the 21st Century Cures Act ==
The day Representative Gingrey and fifty-two cosponsors introduced the ADAPT Act, it was referred to the Subcommittee on Health.<ref>H.R. 3742, 113th Cong. (2013) (on the bar in the middle of the page, click the "Actions" tab).[https://www.congress.gov/bill/113th-congress/house-bill/3742/text]</ref> It never left.<ref>''Id.''</ref> A little over a year later, Representative Shimkus, joined by cosponsor Gene Green (D-TX), resuscitated the Act.<ref>[https://www.congress.gov/bill/114th-congress/house-bill/2629/text?q=%7B%22search%22%3A%5B%22%5C%22Antibiotic+Development+to+Advance+Patient+Treatment+%5C%22%22%5D%7D&r=1&s=3 H.R. 2629]</ref> Again, it died in committee.<ref>''Id.''</ref> Nevertheless, “[m]any of [its] provisions were ultimately incorporated into the 21st Century Cures Act [Cures Act]."<ref>Khachatryan, ''supra'', at 162.</ref> A [[Bipartisanship|bipartisan effort]] ranging from such varied policy areas as [[Medicare (United States)|Medicare savings]] to [[tick-borne disease]]s, the Cures Act was signed into law three years and a day after the ADAPT Act’s initial proposal.<ref>[https://www.congress.gov/bill/114th-congress/house-bill/34/text?q=%7B%22search%22%3A%5B%22h.r.+34%22%5D%7D&r=1&s=8 21st Century Cures Act, H.R. 34, §§ 2062, 5001 (2015)]</ref>

Section 3042 (concerning the “expedited testing of new antibacterial and antifungal drugs”) of the Cures Act derives nearly verbatim from the 2015 ADAPT Act.<ref>[https://www.congress.gov/bill/114th-congress/house-bill/34/text?q=%7B%22search%22%3A%5B%22h.r.+34%22%5D%7D&r=1&s=8 H.R. 34, § 3042]</ref> At the request of a drug manufacturer, the Secretary may approve a given medication based on substandard data—provided that it “is intended to treat a serious or life-threatening infection in a limited population of patients with unmet needs.”<ref>''Id.''</ref> However, in the vein of the 2015 ADAPT Act’s purpose statement, Section 3042 requires the Secretary to balance the benefits of expedited remedies against their costs.<ref>''Id.''</ref> Drugs approved under the Cures Act’s LPAD pathway are subject to much the same labeling requirements as under the ADAPT Act. All labeling and advertising associated with such medications “shall contain the statement ‘Limited Population’ in a prominent manner and adjacent to . . . the proprietary name of such drug.”<ref>[https://www.congress.gov/bill/114th-congress/house-bill/34/text?q=%7B%22search%22%3A%5B%22h.r.+34%22%5D%7D&r=1&s=8 H.R. 34, § 3041]</ref> Section 3044 underscores the Secretary’s ability to update and issue new susceptibility criteria for antimicrobial drugs and her requirement make this information public.<ref>[https://www.congress.gov/bill/114th-congress/house-bill/34/text?q=%7B%22search%22%3A%5B%22h.r.+34%22%5D%7D&r=1&s=8 H.R. 34, § 3044]</ref> Finally, Section 3043 includes similar language (relative to the 2015 ADAPT Act) in regard to the expedited production of new ASTs and their labeling requirements.<ref>[https://www.congress.gov/bill/114th-congress/house-bill/34/text?q=%7B%22search%22%3A%5B%22h.r.+34%22%5D%7D&r=1&s=8 H.R. 34, § 3043]</ref>

==References==
{{reflist}}


[[Category:United States federal health legislation]]
{{US-law-stub}}
[[Category:Proposed legislation of the 113th United States Congress]]
[[Category:Acts of the 114th United States Congress]]

Latest revision as of 08:21, 29 May 2024

The Antibiotic Development to Advance Patient Treatment (ADAPT) Act (H.R. 3742) was introduced in the U.S. Congress on December 12, 2013 by Representative Phil Gingrey of Georgia and fifty-two cosponsors. Responding to the lack of financial incentives for drug manufacturers to innovate new antibiotics and antifungals and the regulatory barriers to their doing so, it proposed an expedited pathway for testing drugs intended for diseases for which no cure yet existed. After it died in committee, a similar version of the Act was re-introduced by Representative John Shimkus of Illinois and his cosponsor Representative Gene Green of Texas. Though this Act likewise failed to make it out of committee, several of its provisions were codified in the 21st Century Cures Act, which was signed into law on December 13, 2016. These include the expedited testing pathway for new antibiotics and a similar provision for antimicrobial susceptibility tests.

Background

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Antibiotic resistance and the barriers to new treatments

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The cost of antibiotic resistance, in dollars and in lives, motivated the Act’s sponsors and the community stakeholders that supported its passage. In September 2014, the Subcommittee on Health of the House Committee on Energy and Commerce held a hearing at which officials from the Food and Drug Administration (FDA), Pew Charitable Trusts, and other organizations testified in favor of the ADAPT and 21st Century Cures Acts.[1] Opening the hearing, Subcommittee Chairman Joseph R. Pitts (R-PA) quoted then-Prime Minister David Cameron’s recent admonition that failure to “confront the threat of antibiotic resistance” could “cast [humanity] back into the dark ages.”[2] Speaking at this same hearing, Representative Phil Gingrey (R-GA) (the 2013 Act’s principal sponsor) referenced Centers for Disease Control (CDC) statistics, which placed the number of Americans who die from drug-resistant infections each year at around 23,000.[3] Representative Gingrey asserted that the financial losses from such infections amount to $55 billion annually.[3] Representative John Shimkus (R-IL) would later note these same figures in a House debate over the Acts in July 2015.[4]

Equally worrisome to the ADAPT Act’s proponents were the economic and regulatory impediments to developing new treatments for drug-resistant illnesses. Citing the FDA, Representative Gingrey lamented during the 2014 hearing that “new antibiotic approval ha[d] decreased by 70 percent since the mid 1980s.”[3] Representative Michael C. Burgess (R-TX) likewise took issue with the “lack of a pipeline of new drugs” to respond to the threat of super bugs.[5] Several blamed inadequate market incentives for this paucity of remedies. As Dr. Barbara E. Murray, then-President of the Infectious Diseases Society of America, observed, “Antibiotics are typically priced low [and] used for a short duration.”[6] Pharmaceutical companies can reap greater returns in other areas of research; hence, the development of new antibiotics flounders.[7]

Compounding the scant financial motives for drug development, creators of new treatments were made to contend with "serious regulatory barriers".[8] Dr. Murray observed that the small number of patients infected by novel diseases made it difficult for manufacturers to find enough test subjects in order to comply with federal agencies’ n-count requirements.[8] The unavailability of diagnostic tests for these new infectious agents also demanded a large investment to find eligible study participants, while generating little information about drug effectiveness.[8] Stagnant innovation becomes self-perpetuating. The more antibiotics to which a pathogen becomes resistant, the fewer controls there are against which to measure an experimental treatment.[8]

The GAIN Act

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In 2012, one of Congress’s earliest attempts at rectifying these barriers to new drug-resistant antibiotics came in the form of the Generating Antibiotics Now (GAIN) Act.[9] GAIN was passed as an amendment to the Federal Food, Drug, and Cosmetic (FD&C) Act.[9] Its strategy for generating new antibiotics is to offer manufacturers an artificial monopoly on any qualifying drugs that they produce.[9] Such drugs must treat illnesses with “the potential to pose a serious threat to the public health.”[9] However, beyond this blanket criterion, GAIN gave significant deference to the Secretary of the Department of Health and Human Services (the Secretary).[9] This latitude was subject only to the requirements that she consider a given pathogen’s “impact on public health” and “morbidity and mortality rates” and consult with the CDC, FDA, and the medical community.[9] Manufacturers who satisfied GAIN’s conditions were guaranteed five years of market exclusivity over the pertinent drug.[9] These years could stack with the drug’s “five year exclusivity as a new chemical entity (NCE), three year clinical investigation exclusivity, and seven-year orphan drug exclusivity.” Moreover, any qualifying drugs were eligible for fast-track review.[10]

GAIN’s value proposition proved to be an effective one. As Representative Frank Pallone (D-NJ) commented during the 2014 ADAPT Act hearing, within two years, GAIN had led to FDA approval of numerous new antibiotics.[11] The expedited review procedure further ensured that these drugs would be “able to combat an imminent infectious disease threat and reach patients at an accelerated pace".[11] At the same time, Representative Pallone and others were concerned about the consumer harms that these decades of exclusivity might yield. Representative Henry A. Waxman (D-CA) warned that exclusivity “allow[s drug companies] to charge higher prices,” which “imposes a significant burden on patients and on the healthcare system overall.”[12] To justify “the carrot of marketing and regulatory exclusivities,” Representative Pallone exhorted his fellow members of Congress to ensure that their efforts “achieve[] the necessary impact on the pipeline of new drugs.”[11]

Provisions

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Purpose and Scope

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The ADAPT Act complemented GAIN. Representative Gingrey introduced it to the House as the “logical next step to the GAIN Act.”[13] To that end, it did not merely render the development of new treatments more lucrative but more feasible as well. The centerpiece of this proposal was ADAPT’s creation of a Limited Population Antibacterial Drug (LPAD) approval pathway for certain antibiotics.[14] Faced with a disease of sufficient severity for which alternatives do not yet exist, ADAPT would empower the Secretary to dispense with the usual testing requirements and allow manufacturers to go to market based on more limited efficacy tests.[15] As Allan Coukell, Director of Drug, Medical Device, and Food Programs at the Pew Charitable Trusts, observed, a patient with multi-drug-resistant pneumonia will likely die without access to a new antibiotic.[16] In that case, the uncertainty of an unproven remedy was preferable to the near certainty of death. In conducting such a risk-benefit assessment, ADAPT allowed the FDA to “accept less data” in approving a lifesaving drug.[17] As Representative Shimkus later commended, this “new, streamlined pathway” saved “thousands of lives” by making experimental drugs available to those who would otherwise have no cure.[18]

Given the uncertainty inherent in drugs approved via LPAD, ADAPT’s advocates were careful to constrain its reach to “high-need populations” suffering from the gravest threats.[13] Dr. Janet Woodcock, Director of the FDA Center for Drug Evaluation and Research, claimed that ADAPT would be restricted to “rare resistant organisms where there are really very few treatment options available.”[19] Within the population of patients affected by these diseases, the Act’s application would be further constrained to “the limited population in most need of the therapy, as opposed to all patients.”[20] As such, ADAPT would not lower the federal review standard for new drugs, but merely contour it to the needs of “a specific population that is different from the general population.”[16]

Relationship Between the 2013 and 2015 Acts

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The two versions of the ADAPT Act—H.R. 3742 (2013)[21] and H.R. 2629 (2015)[22]—contain the same three overriding provisions discussed above. Both would amend Section 505 of FD&C (21 U.S.C. § 355) to formally include the expedited testing pathway.[23] Each prescribes certain labeling requirements for manufacturers[24] and charges the Secretary of Health and Human Services with conducting the aforementioned breakpoint review.[25] Under a modification to Title III of the Public Health Service Act (42 U.S.C. § 247b-22), the Secretary is also to monitor “the use of antibacterial and antifungal drugs” as well as “[c]hanges in bacterial and fungal resistance to drugs.”[26] This new responsibility of the Secretary encompasses drugs approved both through LPAD as well as the standard procedure.[26] The results of the Secretary’s resistance analysis, like the breakpoint research, are to be made public.[26]

The 2013 and 2015 Acts differed slightly in scope and the precise process they envisioned. Under the 2013 Act, the Secretary could approve drugs to treat “a limited population of patients for which there is an unmet need,” based on her assessment of either traditional comprehensive studies, “datasets of limited size,” “such other confirmatory evidence as [she] deems necessary,” or some combination of the above.[27] The 2015 version expands this list of sources of proof, holding that the Secretary may consult nonclinical tests—assessments not conducted on humans—in deciding on whether to approve a drug.[28]

At the same time, this later version limited the Act’s applicability via a purpose statement with language evocative of a sliding scale. The Act serves to “help expedite the development and availability of treatments for serious or life-threatening bacterial or fungal infections,” but this goal depends on “the severity of the infection and the availability or lack of alternative treatments.”[29] Furthermore, the 2015 Act contained a new precondition. In this version of the legislation, the Secretary did not simply decide what level of proof would be necessary for a drug’s approval but actively collaborated with the manufacturer to create a “written agreement” that stipulated the necessary evidence.[30] Only if such an agreement is reached may the Secretary approve the drug via the LPAD pathway.[31] To the end of reaching this agreement, the 2015 Act provides for consultative meetings between manufacturers and the Secretary.[32]

In regard to labeling, the 2013 Act would have mandated that LPAD drugs bear the warning label noted above: “This drug is indicated for use in a limited and specific population of patients.”[33] However, on its terms, this requirement applied only to the drug’s “prescribing information”—not necessarily to its packaging or bottle.[34] The 2015 Act broadened the labeling provision. In addition to the warning on prescriptions, this version entailed placing a label on the product itself that states “Limited Population” and features “in a prominent manner . . . adjacent to . . . the brand name of the product.”[35]

Finally, the 2015 version of the Act expanded its applicability relative to the prior version. For one, it allowed the Secretary to expand LPAD to new arenas outside its original superbug context. Should she determine “that the public health would benefit from expansion of the limited-use pathway,” other medical areas may be subsumed within the Act’s expedited provisions.[36] Secondly, it pulls antimicrobial susceptibility tests into the LPAD pathway. So long as a given test satisfies the exigency conditions for antimicrobial drug treatments, “the Secretary may authorize the marketing of such device” under LPAD—subject to cautionary labeling requirements.[37]

Limitations

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Kevin Khachatryan noted, that the ADAPT Act did not impose responsibilities for Antimicrobial stewardship for antibiotics developed under this pathway.”[38] Coupled with the incentive for manufacturers to produce all that they can during their monopoly window, “[t]his can lead to overuse of these antibiotics and contribute to resistant microbes.”[39] Additionally, the Act placed a premium of speed while sidelining other objectives of testing, namely diverse representation among test subjects.[40] This could impede the gathering of data about certain populations respond to experimental drugs, namely “women, children, and [the] elderly.”[41]

Incorporation into the 21st Century Cures Act

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The day Representative Gingrey and fifty-two cosponsors introduced the ADAPT Act, it was referred to the Subcommittee on Health.[42] It never left.[43] A little over a year later, Representative Shimkus, joined by cosponsor Gene Green (D-TX), resuscitated the Act.[44] Again, it died in committee.[45] Nevertheless, “[m]any of [its] provisions were ultimately incorporated into the 21st Century Cures Act [Cures Act]."[46] A bipartisan effort ranging from such varied policy areas as Medicare savings to tick-borne diseases, the Cures Act was signed into law three years and a day after the ADAPT Act’s initial proposal.[47]

Section 3042 (concerning the “expedited testing of new antibacterial and antifungal drugs”) of the Cures Act derives nearly verbatim from the 2015 ADAPT Act.[48] At the request of a drug manufacturer, the Secretary may approve a given medication based on substandard data—provided that it “is intended to treat a serious or life-threatening infection in a limited population of patients with unmet needs.”[49] However, in the vein of the 2015 ADAPT Act’s purpose statement, Section 3042 requires the Secretary to balance the benefits of expedited remedies against their costs.[50] Drugs approved under the Cures Act’s LPAD pathway are subject to much the same labeling requirements as under the ADAPT Act. All labeling and advertising associated with such medications “shall contain the statement ‘Limited Population’ in a prominent manner and adjacent to . . . the proprietary name of such drug.”[51] Section 3044 underscores the Secretary’s ability to update and issue new susceptibility criteria for antimicrobial drugs and her requirement make this information public.[52] Finally, Section 3043 includes similar language (relative to the 2015 ADAPT Act) in regard to the expedited production of new ASTs and their labeling requirements.[53]

References

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  1. ^ 21st Century Cures: Examining Ways to Combat Antibiotic Resistance and Foster New Drug Development; Hearing Before the Subcommittee. on Health of the Comm. on Energy and Commerce, 113th Cong. (2014) [hereinafter Hearing Before Health Comm.].[1]
  2. ^ Hearing Before Health Comm., supra, at 1 (statement of Joseph R. Pitts, Pennsylvania Rep. and Chairman of the Subcomm. on Health).[2]
  3. ^ a b c Hearing Before Health Comm., supra, at 5 (statement of Phil Gingrey, Georgia Rep.).[3]
  4. ^ Press Release, Congressman John Shimkus, With Over 10,000 Diseases and Only 500 Treatments--Shimkus Votes for Cures (July 10, 2015) ("Each year in the United States, at least 2 million people are infected with an antibiotic-resistant bacteria and at least 23,000 of them die as a direct result of those infections, according to the CDC.").[4]
  5. ^ Hearing Before Health Comm., supra, at 3 (statement of Michael C. Burgess, Texas Rep.).[5]
  6. ^ Hearing Before Health Comm., supra, at 60 (statement of Barbara E. Murray, MD, President of the Infectious Disease Society of America.).[6]
  7. ^ See Hearing Before Health Comm., supra, at 4 (statement of Frank Pallone, New Jersey Rep.).[7]
  8. ^ a b c d Hearing Before Health Comm., supra, at 61 (statement of Barbara E. Murray, MD, President of the Infectious Disease Society of America.).[8]
  9. ^ a b c d e f g See Kevin Khachatryan, Note, Incentivizing Drug Development: Novel Reforms of Pharmaceutical Innovation, 18 COLUM. SCI. & TECH. L. REV. 139, 156-57 (2016).
  10. ^ See Kevin Khachatryan, Note, Incentivizing Drug Development: Novel Reforms of Pharmaceutical Innovation, 18 COLUM. SCI. & TECH. L. REV. 139, 157-58 (2016).
  11. ^ a b c Hearing Before Health Comm., supra, at 4 (statement of Frank Pallone, New Jersey Rep.).[9]
  12. ^ Hearing Before Health Comm., supra, at 8 (statement of Henry A. Waxman, California Rep.).[10]
  13. ^ a b Hearing Before Health Comm., supra, at 6 (statement of Phil Gingrey, Georgia Rep.).[11]
  14. ^ Donna Hanrahan, Federal Efforts to Reduce Overuse, Curb Misuse, and Incentivize the Development of Antibiotic Drugs, 26 ANNALS HEALTH L. 67, 85-86 (2017)[12]
  15. ^ See id.
  16. ^ a b Hearing Before Health Comm., supra, at 113 (statement of Allan Coukell, Director of Drug, Medical Device, and Food Programs, Pew Charitable Trusts).[13]
  17. ^ Id.
  18. ^ Press Release, supra
  19. ^ Hearing Before Health Comm., supra, at 37 (statement of Janet Woodcock, Director of the Food & Drug Administration Center for Drug Evaluation and Research).[14]
  20. ^ Hearing Before Health Comm., supra, at 62 (statement of Barbara E. Murray, MD, President of the Infectious Disease Society of America.).[15]
  21. ^ Antibiotic Development to Advance Patient Treatment (ADAPT) Act of 2013, H.R. 3742, 113th Cong. (2013).[16]
  22. ^ Antibiotic Development to Advance Patient Treatment (ADAPT) Act of 2015, H.R. 2629, 114th Cong. (2015).[17]
  23. ^ H.R. 3742, § 2(a); H.R. 2629, § 2(b).
  24. ^ H.R. 3742, § 2 (x)(C)[18]; H.R. 2629, § 2(b)(x)(3)[19].
  25. ^ H.R. 3742 § 3(a)[20]; H.R. 2629 § 3(a)[21].
  26. ^ a b c H.R. 3742 § 2(c)[22]; H.R. 2629 § 2(g)[23].
  27. ^ H.R. 3742 § 2(c)[24].
  28. ^ H.R. 2629 § 2(g)[25].
  29. ^ H.R. 2629 § 2(a)[26].
  30. ^ H.R. 2629 § 2(b)(x)(1)(A)[27].
  31. ^ H.R. 2629 § 2(b)(x)(1)(B)[28].
  32. ^ H.R. 2629 § 2(b)(x)(2)[29].
  33. ^ H.R. 3742, § 2 (x)(C)[30].
  34. ^ Id.
  35. ^ H.R. 2629, § 2(b)(x)(3)[31].
  36. ^ H.R. 2629, § 2(f)[32].
  37. ^ H.R. 2629, § 2(e)[33].
  38. ^ Khachatryan, supra, at 161.
  39. ^ Id. at 162.
  40. ^ Id.
  41. ^ Id.
  42. ^ H.R. 3742, 113th Cong. (2013) (on the bar in the middle of the page, click the "Actions" tab).[34]
  43. ^ Id.
  44. ^ H.R. 2629
  45. ^ Id.
  46. ^ Khachatryan, supra, at 162.
  47. ^ 21st Century Cures Act, H.R. 34, §§ 2062, 5001 (2015)
  48. ^ H.R. 34, § 3042
  49. ^ Id.
  50. ^ Id.
  51. ^ H.R. 34, § 3041
  52. ^ H.R. 34, § 3044
  53. ^ H.R. 34, § 3043
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