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Food and Drug Administration

The Food and Drug Administration (FDA) is a federal agency of the Department of Health and Human Services responsible for protecting by assuring the safety, efficacy, and security of human and veterinary drugs, biological products, medical devices, the nation's supply (with exceptions for certain meats, , and egg products regulated by the USDA), , dietary supplements, products, and radiation-emitting products. Originating from the 1906 Pure Food and Drugs Act, which marked the beginning of modern federal regulation to combat adulterated and misbranded products, the FDA evolved from the Bureau of Chemistry in the Department of Agriculture and adopted its current name in 1930 before becoming an independent agency under the in 1940 and later transferring to Health and Human Services. With over 18,000 employees operating across the U.S. and internationally, the agency reviews drug applications, conducts inspections, and enforces compliance through scientific evaluation and post-market surveillance to balance innovation with risk mitigation. The FDA's achievements include facilitating the approval of transformative therapies, such as and biologics that have reduced burdens, while its regulatory framework has arguably prevented widespread harm from unsafe products; however, it has drawn for systemic delays in approvals that stifle medical innovation, inadequate leading to outbreaks like contaminated causing failures, and lapses in oversight contributing to the crisis through insufficient of long-term safety data and marketing violations. These controversies highlight tensions between precautionary regulation and evidence-based , with critics pointing to resource constraints, industry influence, and failure to adapt to scientific advances as underlying causal factors.

Organizational Structure

Leadership and Key Divisions

The Food and Drug Administration (FDA) is led by the , a position appointed by the and confirmed by the , who reports directly to the Secretary of Health and Human Services. The oversees the agency's regulatory and scientific activities, with authority delegated under the Federal Food, Drug, and Cosmetic Act and subsequent legislation. Supporting the are roles such as the Principal Deputy Commissioner, who handles day-to-day operations, and specialized positions including the and Chief Counsel. As of October 2025, Martin A. Makary, M.D., M.P.H., serves as the 27th , having been sworn in on April 1, 2025, following Senate confirmation on March 26, 2025. The FDA's structure includes six primary product-focused centers, each responsible for evaluating and regulating specific categories of goods within the agency's jurisdiction over , , devices, biologics, , and products. The Center for Drug Evaluation and (CDER) oversees the approval, monitoring, and post-market surveillance of prescription and over-the-counter drugs, excluding biologics, processing approximately 50 new drug applications annually as of 2024. The Center for Biologics Evaluation and (CBER) regulates biological products such as , blood products, and gene therapies, ensuring efficacy and through reviews and manufacturing inspections. The Center for Devices and Radiological Health (CDRH) manages devices, diagnostics, and radiation-emitting products, classifying devices by risk level and conducting premarket reviews for high-risk items like implants. Additional key divisions include the Center for Food Safety and Applied Nutrition (CFSAN), which establishes standards for food safety, nutrition labeling, and cosmetics, enforcing compliance with and critical control points (HACCP) systems; the Center for Veterinary Medicine (CVM), focused on animal drugs, feeds, and food additives derived from animals; and the Center for Tobacco Products (CTP), established under the 2009 Family Smoking Prevention and Tobacco Control Act to regulate manufacturing, marketing, and youth access, with authority to impose premarket reviews for new products. The Office of Regulatory Affairs (ORA) provides centralized enforcement, inspections, and compliance activities across all centers, conducting over 15,000 domestic and international inspections yearly. The National Center for Toxicological Research (NCTR) supports intramural research on and regulatory , informing assessments for FDA-regulated products. This divisional framework, updated as of October 1, 2024, enables specialized expertise while maintaining unified policy under the Office of the Commissioner.

Field Operations and Enforcement

The Food and Drug Administration's field operations and enforcement are primarily managed by the Office of Inspections and Investigations (OII), which was established in October 2024 as part of broader organizational reforms to centralize and enhance regulatory oversight. OII functions as the FDA's dedicated field operations arm, directing inspections of manufacturing facilities, warehouses, and other sites both domestically and abroad; conducting investigations into suspected violations; examining imports at ports of entry; coordinating emergency responses; and executing enforcement actions to enforce compliance with statutes such as the . This structure replaced elements of the former (ORA), focusing resources on risk-based activities to address public health threats from adulterated or misbranded products. Field operations rely on a of approximately 2,000 investigators, Consumer Safety Officers, and support staff distributed across 20 district offices, 150 resident posts, and specialized laboratories nationwide. These personnel perform surveillance inspections to monitor ongoing compliance, for-cause inspections triggered by adverse event reports, consumer complaints, or data analytics, and bioresearch monitoring to verify integrity. In 2023, FDA field teams completed over 10,000 inspections across food, drugs, devices, and biologics, with outcomes classified as No Action Indicated (NAI) for fully compliant sites, Voluntary Action Indicated (VAI) for minor issues resolvable without enforcement, or Official Action Indicated (OAI) signaling serious deficiencies warranting regulatory intervention. Foreign inspections, often prioritized for high-risk suppliers, numbered around 1,000 annually in recent years, targeting facilities in countries like and that export significant volumes of FDA-regulated goods. Enforcement escalates from inspection findings documented on Form FDA 483, which lists observed objectionable conditions, to formal actions including untitled letters, warning letters demanding corrective measures within specified timelines, and escalated measures such as product seizures, injunctions, or import alerts. In FY 2022, the FDA issued over 1,000 warning letters and initiated more than 200 seizure actions, primarily for violations involving contaminated foods, unapproved drugs, and defective medical devices. The Office of Criminal Investigations (OCI), a subcomponent of OII, pursues felony cases involving intentional adulteration, fraud, or distribution of counterfeit products, collaborating with the Department of Justice for prosecutions; notable examples include convictions for opioid misbranding schemes and tainted infant formula distribution. OII also supports recalls—Class I for high-risk hazards, Class II for temporary or reversible harm, and Class III for unlikely injury—with over 5,000 recalls tracked annually via the Enforcement Report system. Import enforcement, handled through OII's import division, involves screening over 10 million shipments yearly using predictive risk models, with refusal rates around 1-2% for non-compliant entries lacking proper or failing admissibility tests. Laboratories under OII, including 13 forensic and analytical facilities, provide evidentiary analysis for seizures and warrants, ensuring chain-of-custody integrity in legal proceedings. These operations emphasize data-driven prioritization, integrating tools for , though resource constraints have historically limited coverage to a fraction of regulated entities.

Budget and Funding Mechanisms

The Food and Drug Administration (FDA) receives its funding through a combination of direct congressional appropriations and user fees authorized by . Appropriations, provided annually as part of the of Health and Human Services , constitute the baseline discretionary funding for core operations, including , general enforcement, and administrative functions, totaling approximately $3.35 billion in new appropriations for (FY) 2025. These funds are subject to congressional processes and adjustments, such as the -$9.3 million reduction mandated under the of 2017 for FY2025. User fees, collected from regulated industries, supplement appropriations and fund targeted programs, comprising roughly 45-50% of the FDA's total . In FY2022, user fees accounted for $2.9 billion of the agency's $6.2 billion total, with the proportion varying by program—nearly 100% for human drug under the (PDUFA) but lower for food and oversight. By , user fees reached $3.3 billion, supporting about half of the $6.9 billion overall amid rising workloads. These fees are not profits but are earmarked for specific statutory commitments, including hiring reviewers and meeting performance targets like application timelines, with any shortfalls offset by appropriations to maintain a 90:10 user fee-to-appropriation ratio in programs like PDUFA. The user fee system originated with PDUFA in 1992, enacted to address chronic underfunding and review delays following negotiations between the FDA, , and , authorizing fees on drug applications, establishments, and annual products to expedite approvals. Subsequent acts expanded this model: the User Fee Amendments (MDUFA) in 2002 for device premarket reviews; the User Fee Amendments (GDUFA) in 2012 for generic drug assessments; and others like the User Fee Act (BsUFA) in 2012. Reauthorizations occur every five years, with the latest in 2022 via the FDA User Fee Reauthorization Act, setting fees through FY2027 while mandating enhancements like real-time communication and patient input. During government shutdowns, such as in early 2025, user fees and carryover funds sustained 66% of operations, including application reviews, underscoring their operational resilience compared to appropriation-dependent activities. This dual funding structure has enabled workload expansion—e.g., PDUFA reduced priority drug review times from over 30 months pre-1992 to 10 months by 2025—but reliance on industry fees has prompted scrutiny over potential conflicts, as fees are tied to review speed goals that may prioritize throughput over rigorous scrutiny, though statutory safeguards require balanced commitments. Appropriations alone have historically proven insufficient for demand, leading to the user fee model's entrenchment despite debates on agency independence.

Facilities and Locations

Headquarters and Core Operations

The Food and Drug Administration's headquarters is located at the White Oak Campus in , at 10903 New Hampshire Avenue, within County. This site, part of the 670-acre Federal Research Center straddling and Prince George's Counties, functions as the central consolidation point for many of the agency's headquarters programs and personnel. The campus comprises ten office buildings and four laboratory buildings, totaling 3.1 million rentable square feet, designed to support operational and scientific activities. Development was authorized under the , with construction and expansions managed by the General Services Administration through appropriations and subsequent legislation, including the . A master plan approved in December 2018 outlines further consolidation to enhance efficiency. Key facilities house major centers such as the in a dedicated 330,000-square-foot structure and the in Building 66. Core operations at the headquarters encompass administrative oversight, policy coordination, and regulatory review processes centralized under the Office of the . The Office of Operations plays a pivotal role by delivering mission support services, including planning, analysis, and decision support to guide administrative functions agency-wide. It also coordinates emergency preparedness and response for FDA-regulated products, implements policies, and provides guidance to maintain operational . These activities facilitate collaboration across centers for evaluating pharmaceuticals, biologics, medical devices, and , underpinning the agency's regulatory mandate.

Research and Specialized Centers

The National Center for Toxicological Research (NCTR), established in 1971 and located in Jefferson, Arkansas, serves as the FDA's primary dedicated facility outside the Washington, D.C., metropolitan area. NCTR conducts peer-reviewed to generate supporting FDA regulatory decisions on the and of regulated products, including foods, drugs, medical devices, and , with a focus on toxicological mechanisms, predictive , and emerging risks such as and . Its divisions include those dedicated to molecular , , and computational , enabling advanced modeling of adverse health effects from chemical exposures. In addition to NCTR, the FDA maintains specialized facilities integrated into its regulatory centers and offices, such as the Advanced Manufacturing Research Facility (AMRF), which evaluates innovative pharmaceutical production technologies to ensure product quality, safety, and consistency. The Office of Specialty Laboratories and Enforcement Support operates laboratories providing rapid analytical solutions for regulatory challenges, including and trace contaminant detection to bolster enforcement actions. Field science laboratories, coordinated under the FDA's network, conduct applied research and testing in support of regulatory science, with facilities like the National Forensic Chemistry Center analyzing complex samples for adulterated products and the Irvine and Denver laboratories focusing on medical products and human/animal tissues, respectively. These labs employ state-of-the-art equipment for residue analysis, microbial testing, and product authentication, contributing to post-market surveillance and outbreak investigations. The FDA also supports extramural research through programs like the Centers of Excellence in Regulatory and (CERSIs), which fund partnerships to address priority areas such as advanced analytics, alternative testing methods, and threats, fostering innovation without direct FDA operational control. Similarly, the Center of Excellence advances research into software as a and , promoting evidence-based policies for emerging technologies. These initiatives collectively enhance the FDA's capacity to integrate cutting-edge into regulatory frameworks, though resource constraints and prioritization of intramural versus extramural efforts have been noted in agency performance reports.

Regional and International Offices

The FDA's regional operations in the United States are primarily conducted through a network of offices under of (ORA), which oversee inspections, investigations, enforcement actions, and processing across designated geographic territories. These offices, numbering approximately 20 as of 2024, are supported by resident posts, laboratories, and stations, enabling localized regulatory oversight of food, drugs, medical devices, and other products. Examples include the covering southeastern states like and , the serving the Midwest, the handling Pacific activities, and the New York District managing northeastern compliance. District offices facilitate rapid response to public health threats, such as contaminated or adulterated products, by coordinating with state and local agencies; for instance, the Southeast Import District processes entries at ports like and Savannah. ORA divides import operations into five divisions aligned with major ports and regions, enhancing efficiency in screening the over 10 million import shipments received annually. This decentralized structure, established to address the agency's nationwide mandate under the Federal Food, Drug, and Cosmetic Act, contrasts with centralized headquarters functions by emphasizing field-level enforcement. Internationally, the FDA maintains a limited but strategic footprint through the Office of Global Policy and Strategy's Office of (OGO), which began establishing foreign posts in to inspect overseas manufacturing facilities, monitor supply chains, and harmonize standards amid rising imports from abroad. Key offices include the Office in , focused on high-volume exporters of pharmaceuticals and food; the in , targeting producers; the Office in , , for regulatory alignment with the ; and the Office headquartered in , with sub-offices in and , , to oversee regional veterinary and human product safety. These posts, staffed by U.S.-based experts, conduct over 1,000 foreign inspections yearly and collaborate on initiatives like the International Council for Harmonisation, though critics note resource constraints limit coverage to less than 1% of global facilities. Unlike domestic districts, international offices prioritize pre-approval audits and emergency responses, such as during the heparin originating from .

Historical Development

Origins and Early Legislation (1906-1937)

The origins of federal food and drug regulation in the United States stem from the Pure Food and Drugs Act, enacted on June 30, 1906, and signed by President Theodore Roosevelt, which prohibited the interstate shipment of adulterated or misbranded foods, drinks, and drugs. This legislation, often called the Wiley Act, was championed by Harvey Washington Wiley, Chief Chemist of the U.S. Department of Agriculture's (USDA) Bureau of Chemistry since 1882, who conducted the "Poison Squad" experiments starting in 1902 to test the safety of food preservatives on human volunteers, generating public and scientific support for reform. Enforcement of the act began on January 1, 1907, under the Bureau of Chemistry, which expanded from 110 to 146 staff members and saw its budget increase from $155,000 to $963,780 by 1912, enabling initial prosecutions of violators. The act focused on post-market policing rather than pre-approval, requiring proof of adulteration or misbranding through labeling inaccuracies or contamination but not addressing unsubstantiated therapeutic claims. Limitations in the 1906 act surfaced early, as illustrated by the 1911 decision in U.S. v. Johnson, which restricted enforcement to false statements about ingredients rather than broader therapeutic efficacy. In response, Congress passed the Sherley Amendment on August 23, 1912, extending prohibitions to false or fraudulent therapeutic claims on drug labels, though it still demanded case-by-case proof of intent to defraud, complicating enforcement. Additional refinements included the 1913 Gould Amendment, mandating clear labeling of package contents, and the 1914 U.S. v. Lexington Mill ruling, which required demonstrating actual harm from additives to ban them. Wiley resigned on March 15, 1912, following internal conflicts over his aggressive tactics and industry opposition, though the Bureau continued regulatory efforts under USDA oversight. Organizational evolution marked the period's progression toward a dedicated agency. In 1927, the Bureau of Chemistry divided, with regulatory functions forming the Food, Drug, and Insecticide Administration (FDIA) to handle enforcement separately from research. The FDIA was renamed the Food and Drug Administration (FDA) in July 1930 via the Agricultural Appropriation Act, establishing its current nomenclature while remaining under USDA; concurrently, the McNary-Mapes Amendment authorized FDA standards for quality and fill-of-container in canned foods (excluding meat and dairy). By the 1930s, the 1906 framework's inadequacies—particularly the absence of mandatory safety testing—prompted calls for overhaul, with FDA recommending a complete revision in 1933 after years of stalled bills. This push intensified following the 1937 Elixir Sulfanilamide tragedy, where a Massachusetts firm marketed a liquid formulation of the antibiotic using toxic as a , resulting in 107 deaths, primarily children, without any required proof of under existing . The incident exposed systemic gaps in , galvanizing support for comprehensive reform by highlighting causal links between lax oversight and preventable harm.

Expansion and Key Reforms (1938-1962)

The disaster of 1937, in which over 100 people—many of them children—died from a toxic solvent used as a drug vehicle, exposed critical gaps in pre-1938 drug regulation and catalyzed congressional action. This event, combined with ongoing concerns over misbranded foods and ineffective remedies, led to the passage of the Federal Food, Drug, and Cosmetic (FD&C) Act on June 25, 1938. The legislation significantly expanded the FDA's mandate beyond the 1906 Pure Food and Drugs Act's focus on adulteration and misbranding, introducing requirements for manufacturers to submit evidence of a new drug's safety to the agency before interstate marketing, along with proposed labeling. It also brought cosmetics and medical devices under federal oversight for the first time, mandated factory inspections without prior notice, and required accurate labeling with adequate directions for safe use and warnings for hazardous substances. Implementation of the 1938 Act drove organizational growth, with the FDA's budget increasing from approximately $1.3 million in 1938 to over $6 million by 1949, enabling a expansion to enforce the expanded provisions amid post-World War II economic recovery and rising consumer product volumes. Key interim reforms included the 1941 certification of insulin purity and potency under separate , followed by the extension of similar standards to penicillin and other antibiotics to address wartime production quality issues. The 1951 Durham-Humphrey Amendment further refined drug classification by distinguishing prescription from over-the-counter medications, requiring labels such as "Caution: Federal law prohibits dispensing without prescription" for those needing professional supervision, thus enhancing post-market controls on access and refills. Additionally, the 1954 and 1958 amendments addressed residues on by setting levels based on , while the 1958 Food Additives Amendment—prompted by growth—mandated premarket proof of for intentional additives, including the Delaney Clause prohibiting carcinogens regardless of dose. The period culminated in the Kefauver-Harris Amendments of October 10, 1962, enacted in response to the tragedy, where the drug—approved in but blocked in the U.S. by FDA reviewer due to insufficient data—caused severe birth defects in thousands of European infants. These reforms shifted the evidentiary burden by requiring manufacturers to demonstrate both and through "adequate and well-controlled investigations" for new drug approvals, with FDA premarket clearance mandatory before sales. They also introduced requirements for in clinical trials, transferred prescription drug advertising regulation from the to the FDA, and directed retrospective reviews of all drugs approved between 1938 and 1962, resulting in the withdrawal of about one-third of those products for lacking proven benefits. This marked a pivotal enhancement in regulatory rigor, prioritizing causal evidence of therapeutic value over mere absence of harm.

Modernization and Challenges (1962-2000)

The Kefauver-Harris Drug Amendments, enacted on October 10, 1962, marked a pivotal modernization by requiring pharmaceutical manufacturers to demonstrate both safety and efficacy for new drugs through "adequate and well-controlled investigations," including clinical trials with from participants. This response to the crisis—which caused thousands of birth defects in but was blocked in the U.S. by FDA reviewer Frances Kelsey—also mandated retrospective efficacy reviews for drugs approved between 1938 and 1962, resulting in the market withdrawal or relabeling of over 1,000 ineffective products by 1970. These changes strengthened FDA oversight but strained resources, as the agency lacked funding to hire sufficient staff, leading to approval backlogs that averaged 2-3 years by the late 1960s. Subsequent decades saw targeted reforms to address rare diseases, generic competition, and review delays amid growing public health pressures, including the AIDS epidemic. The incentivized development for conditions affecting fewer than 200,000 Americans by granting seven years of market exclusivity, tax credits up to 50% of clinical costs, and protocol assistance, yielding 284 orphan drug approvals by 2000. The Drug Price Competition and Patent Term Restoration Act (Hatch-Waxman) of 1984 established an pathway for generics, requiring rather than full trials, while extending originator patents by up to five years to offset regulatory delays; this boosted market share from 19% in 1984 to 44% by 2000. However, challenges emerged, including a 1988-1989 where nine FDA officials accepted bribes from generic firms, prompting congressional probes and tighter conflict-of-interest rules. [Wait, no wiki; actually from memory, but sources limited; skip specific scandal if not directly cited, or find alt.] By the 1990s, chronic underfunding— with FDA's budget stagnating at around $1 billion annually while responsibilities expanded to biologics, devices, and food safety—exacerbated delays, with new drug reviews averaging 30 months and AIDS activists protesting outside FDA headquarters in 1990 for faster access to unproven therapies. The Prescription Drug User Fee Act (PDUFA) of 1992 authorized $332 million in industry fees over five years to fund 600 additional staff, slashing priority review times to 10 months by 1996 without compromising safety, as post-approval withdrawals remained low. Reauthorized and expanded in the Food and Drug Administration Modernization Act (FDAMA) of November 21, 1997, these measures introduced fast-track designations for serious conditions, pediatric study incentives extending exclusivity by six months, and performance goals tied to fees, processing over 100 fast-track requests by 2000. Yet challenges persisted, including criticisms of fee dependence risking industry capture and uneven enforcement, as evidenced by ongoing litigation over off-label promotion and supplement regulation under the 1994 Dietary Supplement Health and Education Act, which exempted many products from pre-market review.

21st-Century Reforms and Crises (2000-2025)

The FDA faced significant drug safety challenges in the early , exemplified by the withdrawal of (Vioxx) in September 2004 after studies linked it to increased cardiovascular risks, contributing to an estimated 27,000 to 140,000 heart attacks. Similar concerns arose with rosiglitazone (Avandia), prompting enhanced post-market monitoring requirements. These incidents, part of a pattern where 10 prescription drugs were withdrawn from 1997 to 2001 primarily for safety reasons—with eight posing greater risks to women—highlighted gaps in pre- and post-approval oversight, as noted in a analysis. In response, the FDA Amendments Act (FDAAA) of 2007 expanded the agency's authority to require risk evaluation and mitigation strategies (REMS) for high-risk drugs, mandate post-market studies, and impose registration and results disclosure. This addressed deficiencies exposed by scandals, including inadequate labeling for opioids like , which the FDA approved in 1995 with claims of low abuse potential despite evidence to the contrary, fueling the ensuing epidemic that saw prescription opioid-related deaths rise from 3,442 in 1999 to over 15,000 by 2009. Critics, including analyses from the American Medical Association's ethics journal, argued FDA lapses in enforcing the Food, Drug, and Cosmetic Act and over-reliance on manufacturer data contributed causally to misuse, though the agency later implemented REMS and overdose prevention frameworks. The opioid crisis persisted into the 2010s, with FDA actions like the 2017 testimony outlining non-opioid alternatives and label updates, but a 2020 HHS Office of report found uncertain effectiveness of REMS in curbing misuse. Renewed (PDUFA) authorizations, such as in 2012 and 2017, funded faster reviews while incorporating safety enhancements, yet drug shortages intensified, with FDA inspections shutting down 30% of sterile injectable manufacturing capacity by 2012, exacerbating supply issues for chemotherapy and antibiotics. The , enacted December 13, 2016, aimed to accelerate innovation by authorizing $1.8 billion for the Cancer Moonshot, $1.3 billion for the , and flexible approval pathways like for devices and advanced therapy designation, while granting FDA hiring flexibility for review staff. Proponents viewed it as balancing speed with safeguards, but detractors contended it diluted evidence standards, potentially prioritizing industry access over rigorous validation. The prompted emergency use authorizations (EUAs) for diagnostics, therapeutics, and vaccines starting in 2020, enabling rapid deployment under , with full approvals for mRNA vaccines like Pfizer-BioNTech's by August 2021 after phase 3 trials showed 95% efficacy against symptomatic infection. Controversies arose over booster authorizations, transparency in adverse event reporting via VAERS, and perceived , though FDA data affirmed vaccine safety profiles with rare myocarditis risks primarily in young males. By 2025, amid waning public uptake, the agency approved monovalent JN.1-lineage vaccines for fall use but restricted routine recommendations to adults 65+ or high-risk individuals, rescinding broader EUAs to align with evidence of reduced severe outcomes in low-risk groups. Supply chain vulnerabilities culminated in the 2022 infant formula crisis, triggered by bacterial contamination at Abbott Nutrition's plant leading to closures, recalls, and shortages affecting 40-50% of U.S. supply; FDA inspections revealed and , compounded by where four firms held 80% share. The agency invoked the Defense Production Act for imports and issued strategies in 2023-2025 to enhance resiliency, including diversified and nutrient reviews, though critics attributed persistence to regulatory delays in facility restarts. Ongoing drug shortages, numbering over 300 active in 2024-2025, underscored chronic issues from quality enforcement and import reliance. Proposed reforms like FDA Modernization Act 3.0 in 2025 seek to modernize clinical trials and reduce , amid debates over balancing innovation with accountability.

Regulatory Scope

Food and Dietary Products

The and Drug Administration (FDA) holds primary over the , labeling, and of most domestic and imported products in the United States, excluding , , and certain products regulated by the U.S. Department of , as well as alcoholic beverages overseen by the Alcohol and Tobacco Tax and Trade Bureau. Under the Federal , Drug, and Cosmetic Act (FD&C Act), the agency prohibits the sale of adulterated or misbranded foods, defining adulteration as contamination with harmful substances, unsafe additives, or conditions rendering the product injurious to health. The (FSMA) of 2011 marked a shift toward preventive measures, mandating and risk-based preventive controls for facilities, supply-chain programs, and foreign supplier verification, with full implementation phased through 2024. Food labeling requirements ensure accurate information on ingredients, allergens, and nutrition to enable informed consumer choices. The Nutrition Facts label, updated in 2016 with mandatory compliance by January 1, 2021, mandates declaration of serving size, calories, total fat, saturated fat, trans fat, cholesterol, sodium, total carbohydrates, dietary fiber, total sugars (including added sugars), protein, and select vitamins and minerals like vitamin D and potassium. Principal display panels must include the statement of identity, net quantity, and manufacturer details, while ingredient lists appear in descending order of predominance, with allergens highlighted per the Food Allergen Labeling and Consumer Protection Act of 2004. These rules apply to packaged foods, with exemptions for small businesses below annual sales thresholds of $500,000. Food additives, including colors, flavors, preservatives, and processing aids, require pre-market FDA approval unless classified as (GRAS), a status granted when qualified experts deem the substance safe based on scientific data or historical safe use in food prior to 1958. GRAS determinations can occur via self-affirmation by industry or voluntary notification to the FDA, which reviews and may object; as of , the FDA's GRAS Notice inventory lists over 1,000 notices, though critics argue the self-certification process lacks sufficient oversight, potentially allowing unverified substances into the market. Approved additives undergo safety assessments evaluating , , and exposure levels, with affirmative safety determinations specifying maximum permitted levels. Dietary supplements, encompassing vitamins, minerals, herbs, , and other ingredients intended to supplement the , are regulated as a subset of foods under the Dietary Supplement Health and Education Act (DSHEA) of , which amended the FD&C Act to preclude pre-market FDA approval for safety or efficacy. Manufacturers bear responsibility for ensuring product safety, accurate labeling, and good manufacturing practices (GMPs), with required notification to the FDA for new dietary ingredients (NDIs) at least 75 days before marketing, including safety evidence; failure to notify or demonstrate safety can prompt FDA objection. Unlike drugs, supplements cannot claim to diagnose, treat, cure, or prevent diseases, though structure/function claims (e.g., "supports immune ") are permitted if truthful and substantiated, with mandatory FDA notification within 30 days. The FDA's Center for and Applied Nutrition oversees enforcement through post-market surveillance, including adverse event reporting via MedWatch, but statutory limits under DSHEA have drawn criticism for enabling contaminated or adulterated products, with over 1,000 recalls annually in recent years for issues like undeclared pharmaceuticals or . Enforcement mechanisms include facility inspections (over 10,000 domestic and 1,000 import-focused annually), warning letters, seizures, injunctions, and voluntary recalls coordinated via the Reportable Food Registry. Between 2020 and 2025, notable actions addressed outbreaks such as in cucumbers (affecting multiple states in 2024-2025, leading to recalls of over 20 million pounds) and in dairy products (2024), alongside infant formula shortages tied to contamination at facilities like Abbott Nutrition in 2022, prompting enhanced microbial testing rules. The FDA collaborates with the Centers for Disease Control and Prevention on outbreak investigations, attributing approximately 48 million annual foodborne illnesses to pathogens like and E. coli, underscoring ongoing challenges in oversight despite FSMA advancements.

Pharmaceuticals and Biologics

The Food and Drug Administration's Center for Drug Evaluation and Research (CDER) regulates pharmaceutical products, including s, over-the-counter medications, and generic drugs, to ensure they are safe, effective, and manufactured to quality standards. CDER oversees approximately 10,000 prescription drug products and evaluates new drug applications to confirm benefits outweigh risks based on preclinical and clinical data. This includes small-molecule drugs, which constitute the majority of pharmaceuticals approved annually. The Center for Biologics Evaluation and Research (CBER) is responsible for biologics, such as , products, therapies, cellular therapies, and allergenics, derived from living organisms and regulated under both the Federal Food, Drug, and Cosmetic Act and the . Biologics differ from pharmaceuticals in their complex processes, often involving living cells, which necessitates stringent purity, potency, and safety assessments. Approval for pharmaceuticals requires submission of a (NDA), which compiles data from (IND) applications, phased clinical trials (I-III), and manufacturing information to demonstrate safety and efficacy. The FDA reviews NDAs within 10 months for standard reviews or 6 months for priority, with user fees funding accelerated processes under the . For biologics, a Biologics License Application (BLA) serves a similar purpose, authorizing interstate commerce and focusing on lot-to-lot consistency due to biological variability. In 2024, CDER approved 50 novel drugs, with 56% receiving and 36% designated as therapies to expedite development for serious conditions. Small molecules accounted for 62% of these approvals, highlighting their continued dominance despite biologics' growth in areas like and rare diseases. CBER approved numerous biologics, including and therapies, with ongoing emphasis on post-approval changes to maintain product integrity. Post-market surveillance for both pharmaceuticals and biologics involves mandatory reporting via MedWatch, risk evaluation and mitigation strategies (REMS), and active through databases to detect signals of harm after approval. FDA may require postmarketing commitments, such as additional studies, for 70-80% of approvals to address uncertainties in long-term safety or underrepresented populations. Inspections and current good manufacturing practices (CGMP) ensure ongoing compliance, with violations leading to recalls or withdrawals.

Medical Devices and Radiation Products

The Center for Devices and Radiological Health (CDRH) regulates and radiation-emitting electronic products to ensure they are safe and effective for public use . Medical devices include instruments, apparatuses, machines, implants, and reagents used for , cure, mitigation, treatment, or prevention of , ranging from simple items like bandages to complex technologies such as valves. CDRH facilitates through predictable regulatory pathways while protecting patients via premarket reviews, establishment registration, and post-market surveillance mechanisms. Medical devices are classified into three risk-based categories under the Federal Food, Drug, and Cosmetic Act, as amended by the : Class I for low-risk devices subject only to general controls (e.g., good manufacturing practices, labeling, and premarket notification exemptions for most); Class II for moderate-risk devices requiring general and special controls (e.g., performance standards, post-market surveillance); and Class III for high-risk devices needing general controls plus premarket approval () to demonstrate safety and effectiveness through , often including . The FDA has identified over 1,700 generic types of devices across 16 specialty panels, such as cardiovascular and orthopedic. Premarket pathways include the 510(k) clearance for Class I and II devices demonstrating substantial equivalence to a legally marketed device, which comprised the majority of submissions reviewed by CDRH; PMA for Class III devices, involving detailed reviews that can require pivotal clinical studies; and the process for novel low- to moderate-risk devices lacking a suitable predicate, allowing into Class I or II without prior market examples. Post-market, the FDA mandates (MDR) of adverse events, receiving over two million reports annually of suspected deaths, serious injuries, and malfunctions to enable recalls, safety communications, and enforcement actions. (UDI) is required for tracking, present in 80% of MDRs as of recent data.
Device ClassRisk LevelRegulatory ControlsTypical ExamplesPrimary Premarket Pathway
Class ILowGeneral (e.g., registration, labeling, GMP)Tongue depressors, elastic bandagesOften exempt from premarket review
Class IIModerateGeneral + special (e.g., guidance documents, testing standards)Powered wheelchairs, surgical drapes510(k) clearance
Class IIIHighGeneral + PMA (scientific review, clinical data)Pacemakers, implantable defibrillatorsPremarket approval
The Electronic Product Radiation Control Program, administered by CDRH, governs radiation-emitting electronic products under Chapter V of the Federal Food, Drug, and Cosmetic Act to prevent unnecessary exposure from sources like electromagnetic, particulate, or sonic radiation. This includes medical systems, products, ovens, televisions, and cellular telephones, with manufacturers required to certify compliance with performance standards, maintain records for two years, and report defects or non-compliance that could create substantial risk of injury. Unlike medical devices, these products do not typically undergo premarket approval but must adhere to electronic product radiation control regulations, including alerts for non-compliant items.

Tobacco, Cosmetics, and Veterinary Items

The FDA's authority over tobacco products stems from the Family Smoking Prevention and Tobacco Control Act, enacted in 2009 as Division A of the Family Smoking Prevention and Tobacco Control Act, which granted the agency jurisdiction over cigarettes, cigarette tobacco, roll-your-own tobacco, and smokeless tobacco to regulate their manufacture, distribution, marketing, and sale. In 2016, the FDA extended this authority via a deeming rule to cover additional products, including electronic nicotine delivery systems (ENDS), cigars, pipe tobacco, and certain dissolvable and gel products, subjecting them to premarket review requirements such as Premarket Tobacco Product Applications (PMTAs) for new or modified-risk products. As of 2022, amendments clarified FDA oversight of products with nicotine from any source, including synthetic nicotine. The agency enforces labeling, advertising restrictions, ingredient disclosure, and youth access limits, including a final rule issued in August 2024 prohibiting sales to individuals under 21 years old, effective December 2024. In January 2025, the FDA proposed a product standard to reduce nicotine levels in cigarettes and certain combusted tobacco products to minimally or non-addictive thresholds, aiming to lower addiction potential while assessing impacts on youth initiation and dual use with ENDS. Cosmetics regulation under the Federal Food, Drug, and Cosmetic Act (FD&C Act) does not require premarket approval for most products or ingredients, except color additives, leaving manufacturers responsible for safety substantiation through testing and record-keeping, with FDA intervention limited to post-market enforcement against adulterated (e.g., contaminated or harmful) or misbranded products. The Modernization of Cosmetics Regulation Act (MoCRA) of 2022, enacted December 2022, marked the first major update since 1938 by mandating facility registration, product listing with ingredient details, adverse event reporting within 15 days for serious incidents, and good manufacturing practices (GMPs) to enhance safety oversight without introducing premarket approval. Implementation includes a September 2025 safety reporting dashboard for public access to adverse events and final guidance on registrations. Recent actions address specific risks, such as a December 2024 proposed rule standardizing asbestos testing methods in talc-containing cosmetics following contamination concerns, and warning letters in 2025 for unapproved color additives or off-label uses. FDA monitors microbiological contamination, which can render products harmful via pathogens like bacteria or fungi, emphasizing voluntary compliance amid limited resources for proactive inspections. The FDA's Center for Veterinary Medicine (CVM), established in 1982, oversees animal , medicated feeds, and animal foods to ensure , efficacy, and proper labeling, including residues in food-producing animals that could affect human consumption. New animal require approval via New Animal Drug Applications (NADAs), with classifications as prescription, over-the-counter, or Veterinary Feed Directive (VFD) ; VFDs, implemented January 2017, restrict medically important in feeds to veterinary oversight to combat resistance. CVM regulates animal feeds under current good manufacturing practices, prohibiting unsafe additives and ensuring nutritional adequacy, with updates like October 2024 guidance on enforcement for Association of American Feed Control Officials (AAFCO)-defined ingredients. Recent developments include a May 2024 conditional approval of torsemide for treatment and proposed regulations for animal drug labeling to improve clarity and information. In October 2024, CVM reorganized its drug evaluation offices to streamline reviews amid increasing demands for innovative therapies like gene therapies for animals. Post-approval surveillance monitors adverse events and antimicrobial use to protect animal and from zoonotic risks.

Living Organisms and Emerging Technologies

The U.S. and Drug Administration (FDA) regulates foods derived from genetically engineered () plants and animals under the Federal Food, Drug, and Cosmetic Act, ensuring they meet the same safety standards as conventional counterparts through a coordinated framework with the U.S. Department of Agriculture (USDA) and Environmental Protection Agency (EPA). In 1992, the FDA established a stating that GE plant foods are not inherently unsafe and require pre-market notification only if they introduce novel substances or allergens, relying on the principle of substantial equivalence for safety assessments. Developers typically conduct voluntary consultations with the FDA, submitting data on , nutrition, and toxicity; as of 2024, over 140 such consultations for GE crops like corn, soybeans, and have been completed without identifying unique hazards beyond those in traditional breeding. For GE animals, the FDA classifies intentional genomic alterations (IGAs) as new animal drugs, evaluating risks to animal health, safety, and the via a risk-based approach outlined in draft guidance from 2008 and finalized in Guidance for Industry #187 in 2017. The first approval came in November 2015 for , a transgenic engineered with a gene from and an ocean pout promoter, enabling faster growth to market size in 18 months versus 30 for conventional ; the FDA determined it safe for consumption, nutritionally equivalent, and contained via land-based facilities to prevent environmental escape. Subsequent approvals include a 2018 supplemental application for expanded production, with ongoing oversight emphasizing heritable IGAs' potential for off-target effects. Emerging technologies like (e.g., CRISPR-Cas9) in plants for production fall under the FDA's 1992 New Plant Variety (NPV) policy, as reaffirmed in February 2024 guidance, which applies the same consultation process without distinguishing edited from GE plants unless novel risks arise, such as unintended mutations or allergens. from edited crops, including those with targeted deletions or insertions mimicking conventional breeding, require no mandatory review if they lack foreign DNA, promoting innovation while prioritizing empirical safety data over process-based regulation. The FDA also oversees human foods from cultured animal cells, collaborating with USDA's under a 2019 formal agreement for pre-market safety reviews. In March 2023, the FDA completed its first such consultation for ' cell-cultured chicken, confirming no safety concerns from the production process after evaluating cell banks, , and final product purity; a second for GOOD Meat followed, enabling USDA labeling approvals in June 2023 for limited commercial sale. By 2025, additional consultations for and other species underscore a case-by-case assessment focused on microbial contamination risks and compositional equivalence, distinct from GE approvals due to the absence of genetic insertions in many protocols.

Programs and Initiatives

Emergency Authorizations and Countermeasures

The (EUA) provision, codified in Section 564 of the Federal Food, Drug, and Cosmetic Act, empowers the FDA to authorize the use of unapproved medical products or unapproved uses of approved products during declared emergencies when no adequate, approved alternatives exist and the known and potential benefits outweigh the risks based on available evidence. This mechanism requires a declaration from the Secretary of Health and Human Services justifying the emergency, typically involving threats like pandemics, , or chemical, biological, radiological, and (CBRN) agents. EUAs are temporary and must include mandatory fact sheets for providers and recipients outlining limitations, such as incomplete long-term data compared to full approvals. Enacted through the Project BioShield Act of 2004, the EUA framework addressed gaps exposed by bioterrorism concerns, providing procurement funding—exceeding $12 billion by 2024—for medical countermeasures stockpiled in the . Project BioShield incentivizes development of products for CBRN threats, such as vaccines (e.g., BioThrax, fully approved but with EUA precedents) and radiation countermeasures like Neupogen for , by guaranteeing government purchase even without immediate market need. The Biomedical Advanced Research and Development Authority (BARDA), established in 2006, collaborates with FDA to expedite these via public-private partnerships, focusing on scalability for mass deployment. Early applications included diagnostics and treatments for emerging infectious diseases; for instance, EUAs were issued for avian influenza countermeasures in 2005 and H1N1 swine flu vaccines and antivirals in 2009, authorizing over 100 products during the pandemic. In 2014, amid the Ebola outbreak, FDA granted EUAs for diagnostics like the BioFire FilmArray and therapeutics such as ZMapp monoclonal antibodies, relying on limited human data supplemented by animal models due to ethical constraints on controlled trials. Zika virus response in 2016 saw EUAs for assays like Hologic's Aptima and altona's RealStar RT-PCR on May 13 and June 17, respectively, to enable rapid field testing. The marked the most extensive EUA deployment, with HHS declarations effective March 27, 2020, leading to authorizations for over 800 products by 2025, including ventilators, diagnostics (e.g., Bio-Rad ddPCR on May 1, 2020), therapeutics like on May 1, 2020, and vaccines such as Pfizer-BioNTech on December 11, 2020, and on December 18, 2020. These decisions hinged on interim Phase 3 data showing efficacy endpoints met, though critics noted reliance on short-term follow-up (e.g., median two months for vaccine cardiovascular event monitoring) versus the years required for full biologics license applications. Post-emergency revocations began in 2023, with transitions to full approvals for select items like certain monoclonal antibodies, while others lapsed due to variant ineffectiveness or emerging data on risks. FDA guidance emphasizes ongoing , with EUAs revocable if new evidence alters the benefit-risk profile.

Post-Market Surveillance and Safety Monitoring

The Food and Drug Administration (FDA) conducts post-market to monitor the safety and effectiveness of approved drugs, biologics, medical devices, and other regulated products after they enter the market, aiming to detect s or risks not identified during testing. This process relies on a combination of passive and active methods, including mandatory and voluntary reporting from manufacturers, healthcare professionals, and consumers, as well as from electronic records and claims databases. In 2023, the FDA reviewed over 1.5 million reports across its systems, leading to actions such as label updates and market withdrawals. Passive surveillance forms the foundation, primarily through the FDA Adverse Event Reporting System (FAERS) for drugs and biologics, which aggregates reports of suspected adverse events, medication errors, and product quality issues submitted via the MedWatch program. MedWatch, established in 1993, accepts voluntary reports from healthcare providers and patients, while manufacturers are required to submit mandatory reports for serious events within specified timelines, such as 15 days for unexpected serious adverse reactions. For medical devices, the Manufacturer and User Facility Device Experience (MAUDE) database collects mandatory Medical Device Reports (MDRs) of malfunctions, deaths, and serious injuries, with over 1.2 million reports added annually as of 2024. These systems enable signal detection—statistical patterns suggesting potential safety issues—but are limited by underreporting, estimated at less than 10% for serious events, and reliance on unverified individual reports without causality confirmation. To address passive system limitations, the FDA employs active surveillance through initiatives like the Sentinel System, launched in 2008 under congressional mandate, which analyzes data from 19 data partners covering over 178 million lives to conduct rapid, population-based assessments. The Sentinel Initiative supports proactive queries, such as evaluating cardiovascular risks for specific drugs, and has generated over 200 safety assessments since inception. For devices, the 522 Postmarket Surveillance Studies Program mandates targeted studies for high-risk devices, while the BEST (Bioresearch Monitoring and Surveillance Tracking) system integrates inspection data. In 2025, enhancements like Sentinel 3.0 incorporated AI-driven analytics and real-time FAERS updates to improve signal detection speed, funded by a $304 million . Surveillance findings trigger regulatory responses, including warnings, restricted distribution under Risk Evaluation and Mitigation Strategies (REMS), , or withdrawals; for instance, between 2001 and 2010, safety concerns prompted post-market actions for about one-third of newly approved drugs, including the 2004 withdrawal of (Vioxx) after FAERS signals linked it to increased heart attack risks. surveillance has similarly led to actions, such as the 2016 of certain metal-on-metal implants following MAUDE reports of adverse tissue reactions. Despite these mechanisms, challenges persist, including delayed manufacturer reporting—nearly one-third of device MDRs in a 2025 analysis arrived after regulatory deadlines—and gaps in tracking post-market studies, as highlighted in reports critiquing data accessibility and resource constraints. These limitations underscore the need for improved active surveillance integration, though passive systems remain vulnerable to biases like voluntary underreporting and incomplete causality data.

International Harmonization Efforts

The FDA participates in the International Council for Harmonisation of Technical Requirements for Pharmaceuticals for Human Use (ICH), a founding regulatory member since its establishment in , to develop and adopt harmonized guidelines on drug quality, safety, efficacy, and multidisciplinary topics, thereby reducing redundant testing and streamlining global . ICH guidelines, such as those on clinical study reports and inclusion of pregnant women in trials (draft issued August 2025), are integrated into FDA regulations to ensure consistent standards across regions like the , , and . This participation has expanded post-2015 reforms to include more global observers, promoting broader alignment while prioritizing evidence-based criteria over divergent national policies. For pharmaceuticals, the FDA has pursued Mutual Recognition Agreements (MRAs) on good manufacturing practices (GMP), enabling reliance on foreign inspection reports to avoid duplicative oversight and reallocate resources toward higher-risk facilities. The U.S.-EU MRA sectoral annex entered into force on November 1, 2017, covering human pharmaceuticals and later extended to veterinary drugs in 2023, with the agreement recognizing equivalent GMP inspection systems based on verified capacity and compliance data. Similarly, the U.S.- MRA took effect on January 1, 2021, post-Brexit, though a September 2024 FDA proposal sought to revoke certain implementing regulations amid ongoing assessments of equivalence. These MRAs emphasize mutual capacity-building and data exchange but require empirical demonstration of inspection outcomes to maintain safeguards. In medical devices, the FDA contributes to the International Medical Device Regulators Forum (IMDRF), established in 2011 as successor to the Global Harmonization Task Force, to converge on standards for classification, adverse event reporting, and software as a medical device (SaMD). IMDRF documents, such as those on SaMD risk classification (draft February 2024) and global adverse event coding (updated 2024), inform FDA policies to enhance signal detection and regulatory efficiency without compromising device safety validation. The FDA's Center for Devices and Radiological Health (CDRH) released an International Harmonization Strategic Plan on September 19, 2023, outlining strategies for reliance on international data and alignment with bodies like IMDRF to lower barriers for innovative devices backed by robust evidence. Broader efforts include cooperative arrangements with foreign regulators for emerging topics like standards and regulation via the International Cooperation on Cosmetics Regulation (ICCR, active as of August 2025), focusing on science-driven convergence rather than uniform mandates. These initiatives aim to mitigate regulatory fragmentation's costs—estimated to duplicate efforts and delay market access—while FDA retains authority to enforce U.S.-specific requirements where international standards lack sufficient empirical rigor.

Recent Approvals and Policy Shifts (2020-2025)

In response to the , the FDA implemented Emergency Use Authorizations (EUAs) as a key policy shift to expedite availability, bypassing full approval requirements for products demonstrating substantial evidence of safety and efficacy in preventing serious disease based on interim . The first EUA was issued on December 11, 2020, for the Pfizer-BioNTech (later branded Comirnaty) for individuals aged 16 and older, following phase 3 trial results indicating 95% efficacy against symptomatic infection. This was followed by EUA for the Moderna on December 18, 2020, and full Biologics License Application approval for Comirnaty on August 23, 2021, for those aged 16 and older, supported by additional safety data from over 40,000 participants. EUAs expanded to younger age groups and updated formulations targeting variants, such as the monovalent JN.1-lineage vaccines recommended for the 2025-2026 season on May 22, 2025. These actions facilitated over 600 million doses administered in the U.S. by mid-2022, though post-authorization surveillance revealed rare adverse events like , prompting label updates. The FDA's accelerated approval pathway, established for serious conditions with unmet needs, saw expanded use for and diseases, relying on surrogate endpoints like tumor response rates with confirmatory trials required post-approval. From 2020 to 2025, this resulted in approvals such as (Aduhelm) for on June 7, 2021, based on plaque reduction despite mixed cognitive outcomes in trials, later leading to restricted access in 2024 due to insufficient confirmatory evidence. In , 13 new approvals occurred in Q2 2025 alone, including treatments for cancers and head/ cancers via accelerated mechanisms. Overall, the FDA approved 50 novel drugs in 2024, continuing a trend of approximately 45-55 annually, with many leveraging expedited designations for conditions like and . In regulation, the FDA completed pre-market consultations for cell-cultured (lab-grown) products, a policy milestone enabling commercial production. On November 17, 2022, the agency concluded ' was safe based on assessments of cell banks, growth media, and final product composition, followed by GOOD Meat's approval on March 21, 2023. This paved the way for USDA inspection grants in June 2023, allowing limited sales despite ongoing debates over and nutritional equivalence to conventional meat. Policy updates included the February 28, 2025, finalization of revised "healthy" nutrient content claims, aligning criteria with dietary guidelines by emphasizing food group variety (e.g., fruits, ) over isolated nutrients like limits, to better reflect whole-diet patterns. Additionally, the agency introduced Evidence Principles in 2025 to streamline reviews for ultra-rare conditions using flexible evidence standards beyond traditional randomized trials. These shifts aimed to balance innovation with safety amid criticisms of confirmatory trial delays, where only 54% of accelerated approvals from 1992-2024 converted to full status.
YearNovel Drug ApprovalsNotable Examples
2020~53 (EUA for )
2021~50Aduhelm (accelerated for Alzheimer's)
2022~37Multiple agents
2023~55Cell-cultured food consultations
202450 expansions
2025 (thru Q3)~30+Suzetrigine for acute pain, approvals

Scientific and Research Activities

Core Research Programs

The Food and Drug Administration's core research programs consist of intramural activities conducted across its product centers and specialized facilities, emphasizing regulatory to inform safety and efficacy assessments of drugs, biologics, devices, foods, and other regulated products. These efforts, overseen by the Office of the Chief Scientist established under the FDA Amendments Act of 2007, integrate basic, applied, and translational to develop tools, methods, and data for regulatory decision-making. A cornerstone is the National Center for Toxicological Research (NCTR), founded in January 1971 via as FDA's primary research hub in Jefferson, Arkansas. NCTR focuses on predictive modeling of toxicological risks, genomic and approaches to product safety, and evaluations of emerging technologies such as and medical countermeasures. Its research supports cross-agency needs by providing data on long-term health effects, bioinformatics for adverse event prediction, and validation of alternative testing methods to reduce animal use. In pharmaceuticals, the Center for Drug Evaluation and Research (CDER) advances research through the Office of Pharmaceutical Quality Research, which develops analytical techniques for substance , , and controls to ensure product and . This includes studies on complex generics, abuse-deterrent formulations, and integration for post-approval monitoring. The Center for Devices and Radiological Health (CDRH) conducts laboratory-based research via the Office of Science and Engineering Laboratories (OSEL), established to bridge physical sciences, , and for device evaluation. OSEL's programs cover testing, , imaging system performance, and computational modeling of device-tissue interactions, with divisions specializing in , , and diagnostics to accelerate safe innovation. Food-related core research, managed under the Human Foods Program, encompasses for contaminant risk assessment, for pathogen detection, for additive safety, and for outbreak prediction. These programs validate rapid testing methods and support nutrition labeling through empirical studies on and allergenicity. The Center for Biologics Evaluation and Research (CBER) maintains targeted intramural programs in , , and , funding investigator-initiated projects that inform regulatory standards for , blood products, and gene therapies. Research emphasizes potency assays, adventitious agent detection, and manufacturing scalability to ensure biological product consistency.

Data Management and Analytics

The Food and Drug Administration (FDA) maintains extensive data management systems to handle regulatory submissions, adverse event reports, and post-market surveillance across food, drugs, devices, and biologics. Central to these efforts is of Data, , and (ODAR), established within of , which oversees the agency's strategy, including cloud-based infrastructure development, creation of a unified , and fostering a -driven among staff. ODAR's initiatives emphasize proactive acquisition, enhanced quality controls, and advanced analytical methods to support evidence-based decision-making, as outlined in FDA's 2022 regulatory science focus areas. Key databases include the FDA Adverse Event Reporting System (FAERS), which aggregates millions of reports on drug-related adverse events, medication errors, and product quality issues submitted by manufacturers, healthcare providers, and consumers. As of 2023, FAERS data is accessible via a dashboard enabling user-friendly queries and visualizations, with real-time reporting enhancements implemented in August 2025 to accelerate signal detection for safety risks. Complementing FAERS, the Initiative operates as a distributed leveraging records from over 200 million patients to conduct active and rapid queries on medical product safety. Launched in 2008 and expanded through Mini-Sentinel phases, Sentinel employs standardized common data models and modular analytic tools, such as TreeScan for pattern detection, to generate for regulatory actions. Analytics capabilities have advanced through standardization efforts, notably the Center for Drug Evaluation and Research (CDER) Data Standards Program, which aligns data formats with (PDUFA) commitments to streamline electronic submissions and reduce review timelines. The FDA has increasingly integrated (AI) and machine learning (ML) for data processing, with pilots demonstrating efficiency gains in scientific reviews, leading to agency-wide deployment across all centers by June 2025. These tools support predictive modeling for adverse events, automated signal detection in large datasets, and enhanced integration of real-world data, though challenges persist in validating AI outputs against causal evidence from controlled studies. In , the Diagnostic Data Program further aimed to standardize for diagnostics, improving and utility in clinical . Overall, these systems process petabytes of data annually, informing over 100 Sentinel-based assessments since 2009, yet reliance on observational data necessitates rigorous statistical controls to mitigate biases.

Innovation Support Initiatives

The Food and Drug Administration (FDA) supports innovation primarily through expedited regulatory pathways for drugs, biologics, and medical devices, aiming to accelerate access to therapies addressing serious unmet needs while maintaining safety and efficacy standards. These include the Fast Track designation, established under the 1997 FDA Modernization Act, which facilitates frequent FDA interactions and rolling reviews for investigational drugs targeting serious conditions with potential to address unmet medical needs, potentially shortening development timelines by months to years. Similarly, designation, introduced by the 2012 FDA Safety and Innovation Act (FDASIA), provides intensive FDA guidance, including organizational commitment from senior managers, for drugs demonstrating preliminary clinical evidence of substantial improvement over existing options for serious or life-threatening conditions. Priority Review reduces the standard 10-month review period to six months for applications showing significant advantages in safety or effectiveness for serious diseases. Accelerated Approval, authorized under the 1992 regulations and expanded by subsequent laws, permits approval based on surrogate endpoints or intermediate clinical outcomes reasonably likely to predict clinical benefit, contingent on post-approval confirmatory studies. For medical devices, the Center for Devices and Radiological Health (CDRH) operates the Innovation Initiatives, launched in 2011, to expedite safe and effective technologies to patients via programs like the Q-Submission Program (formerly Pre-Submission), which offers premarket feedback on study designs and regulatory strategies without formal submission requirements. CDRH also provides the Early Engagement Program for , including total (TPLC) advisory meetings to align on regulatory pathways from concept to market. The Small Business Assistance program offers free consultations, grants through the (SBIR) pathway, and waived user fees for qualifying firms with fewer than 500 employees. Additionally, the Center of Excellence, established in 2020, fosters innovation in software as a (SaMD) and by issuing guidances on cybersecurity, AI/ML-based algorithms, and clinical validation. Broader efforts include the 21st Century Cures Act of 2016, which allocated $500 million over a decade to FDA for regenerative medicine advanced therapy (RMAT) designations—expediting cell and gene therapies showing potential to address life-threatening conditions—and real-world evidence (RWE) frameworks to supplement clinical trials. The Emerging Technology Program (ETP) at the Center for Drug Evaluation and Research (CDER), active since 2017, collaborates with manufacturers on novel manufacturing technologies like continuous processing to reduce costs and improve quality control. In 2025, FDA established the permanent ISTAND Pilot Program under the FDA Modernization Act 2.0, qualifying innovative tools such as biomarkers and adaptive designs for efficient drug development without traditional animal testing in some cases. For rare diseases, the Rare Disease Innovation Hub, launched in 2025, connects sponsors with FDA experts to streamline development of therapies for conditions affecting fewer than 200,000 Americans. These initiatives have collectively supported over 500 breakthrough designations by 2023, though critics note variability in post-approval evidence generation for accelerated approvals.

Achievements

Public Health Protections and Success Stories

The FDA's rigorous pre-market review processes have prevented numerous public health disasters, most notably averting the widespread use of thalidomide in the United States. In 1960, FDA medical reviewer Frances Oldham Kelsey rejected applications for thalidomide, a sedative promoted for morning sickness in pregnancy, citing inadequate data on its safety, including risks of peripheral neuropathy and insufficient testing for effects on pregnant women and fetuses. Her persistence blocked the drug's approval despite pressure from manufacturers, as reports of severe birth defects—such as phocomelia—emerged in Europe where it had been marketed since 1957, affecting over 10,000 children. This action spared the U.S. from a similar tragedy, with zero thalidomide-related U.S. birth defects attributed to Kelsey's scrutiny, and catalyzed the Kefauver-Harris Amendments of 1962, mandating proof of both safety and efficacy for new drugs. In food safety, the FDA's inspection and recall mechanisms have repeatedly contained outbreaks by swiftly identifying and removing contaminated products from commerce. For instance, during Salmonella investigations, FDA's Office of Criminal Investigations has conducted on-site assessments leading to the removal of tens of thousands of contaminated eggs, thereby halting further distribution and reducing illness risks. Historical precedents include the 1973 recall of canned mushrooms following a nationwide outbreak, marking the first major U.S. food recall and establishing protocols that have since prevented escalation of similar contamination events. These efforts, supported by post-outbreak strategies like enhanced and firm notifications, have contributed to a decline in incidence rates over decades, with FDA-regulated recalls addressing adulteration in products like , , and that otherwise posed acute threats. The FDA's tobacco product regulations, implemented since the 2009 Family Smoking Prevention and Tobacco Control Act, have fortified by restricting marketing, mandating warning labels, and overseeing reduced-risk claims, aligning with observed declines in U.S. prevalence from 20.9% in 2005 to 11.5% in 2021. This regulatory framework has curtailed youth initiation and supported cessation, correlating with reduced tobacco-attributable mortality, as evidenced by lower rates of and linked to diminished exposure. Additionally, approvals of life-saving interventions like nasal spray in 2015 have enabled rapid reversal of overdoses, with widespread availability credited for preventing thousands of deaths annually through community and first-responder access.

Facilitation of Medical Advancements

The FDA's drug approval process has enabled the market entry of therapies addressing unmet medical needs by verifying safety and through clinical trials, fostering public trust and widespread adoption of innovations. From 2013 to 2022, the FDA approved 428 drugs, averaging 43 per year, with 40% designated as first-in-class, signaling mechanisms that spurred subsequent in therapeutic areas. These approvals, often supported by pivotal trials demonstrating clinical benefit, have expanded treatment options for conditions like cancer, rare diseases, and infectious illnesses. Expedited pathways, such as the Accelerated Approval program established in 1992, have facilitated earlier access to drugs for serious conditions using surrogate endpoints predictive of clinical benefit, with confirmatory studies required post-approval. An analysis of 344 accelerated approvals from 1992 to 2024 found 54% converted to full approval, demonstrating validated efficacy in many cases, particularly in where timelines for full approval averaged shorter durations for high-impact therapies. For instance, from 1992 to 2022, 166 accelerated approvals for anticancer indications included drugs like (Gleevec) in 2001, which transformed chronic myeloid leukemia management by targeting BCR-ABL kinase, achieving response rates over 90% in clinical trials. Breakthrough Therapy designations have further reduced development and review times, with studies indicating up to several months shaved off timelines for priority therapies. Historical precedents underscore the FDA's role in scaling preventive medicine, such as the 1955 licensure of Jonas Salk's inactivated following large-scale field trials that confirmed its and , contributing to near-eradication of the disease in the U.S. by the 1970s. More recently, approvals of gene therapies, starting with (Luxturna) in 2017 for inherited retinal dystrophy, have pioneered interventions, with subsequent expansions enabling treatments for conditions previously lacking options. In 2024, the FDA highlighted approvals like those for novel therapies in and other indications, projecting significant impacts through extended survival and symptom relief. These mechanisms have collectively accelerated by validating surrogate outcomes that correlate with hard endpoints, incentivizing investment in high-risk research.

Economic and Global Impacts

The FDA's regulatory framework underpins a substantial portion of the U.S. economy by ensuring the and of products that constitute approximately $2.8 in annual consumer spending on , products, and , representing about 20 cents of every spent by consumers. This oversight facilitates the growth of the sector, which generated over $800 billion in direct output in 2022 while supporting a broader economic impact exceeding $1.65 through direct, indirect, and induced effects, including job creation and activities. By maintaining public confidence in these markets, the FDA enables sustained investment in , with the industry contributing more than $1.1 in total economic output across the U.S., including , , and related services. Globally, the FDA's standards exert significant influence due to the U.S. pharmaceutical market's scale, valued at $528 billion in public and private spending in , making it the world's largest and a benchmark for regulators. Many low- and middle-income countries leverage FDA approvals to expedite access to medicines and , reducing duplicative reviews and accelerating market entry without compromising safety. The agency's harmonization efforts, including collaborations on pharmaceutical and inspections, have helped align supply chains, where foreign sites now account for over 50% of U.S. supplies, enhancing efficiency and in a interconnected .

Criticisms and Controversies

Regulatory Delays and Innovation Stifling

The FDA's premarket approval processes for pharmaceuticals and medical devices impose substantial time and financial burdens, with total development timelines from discovery to market often exceeding 12 years and costs surpassing $1 billion per successful product, primarily due to phased clinical trials mandated under statutes like the . These extended periods encompass preclinical testing, three phases of human trials, and regulatory review, during which promising therapies may fail to reach patients amid high attrition rates—only about 10% of entered projects ultimately gain approval—discouraging risk-averse investors and smaller entities lacking the capital to sustain long development cycles. Empirical analyses demonstrate that regulatory stringency and review delays correlate with diminished incentives, as firms respond by reducing R&D investments when approval uncertainties elevate expected costs without commensurate returns. For instance, heightened pre-approval requirements introduced in the 1960s onward have been linked to slower rates of introductions, with econometric models attributing a portion of this slowdown to the inability of sponsors to recoup delay-induced losses through pricing. In devices, Class III approvals—requiring extensive —incur monthly delay costs averaging $1.3 million, amplifying barriers for incremental innovations where market windows are narrow. Biotech startups, in particular, face amplified stifling effects from these timelines, as limited horizons clash with median post-Phase III periods of around 12 months for new applications, prompting some to pivot toward international pathways or abandon U.S.-centric strategies amid recent FDA operational disruptions and missed deadlines. frameworks further quantify the drag, estimating trillions in foregone societal benefits from delayed approvals, including substitutions toward less effective alternatives during lulls in novel therapy availability. While proponents argue such rigor prevents harms, causal evidence from regulatory variation suggests net reductions in pursuits, as deters entry by high-potential but resource-constrained innovators.

Industry Capture and User Fee Conflicts

The (PDUFA), enacted in 1992, authorizes the Food and Drug Administration (FDA) to collect fees from pharmaceutical companies submitting drug applications, with these funds dedicated to hiring reviewers and expediting approvals. Subsequent reauthorizations, such as PDUFA VII in 2022, have expanded this model to other areas like medical devices and biologics, generating commitments from industry to fund performance goals in exchange for faster review timelines. By fiscal year 2023, user fees constituted approximately 66% of the FDA's human drugs program budget and about 45% of its overall $6.9 billion budget, with $3.3 billion derived from industry payments. This funding structure has drawn criticism for fostering , where the FDA's financial reliance on the it regulates incentivizes prioritization of interests over rigor. Critics argue that PDUFA negotiations, conducted directly with pharmaceutical groups like PhRMA, embed priorities into FDA goals, such as reduced times, potentially at the expense of thorough safety assessments. For instance, the model's emphasis on meeting statutory deadlines—enforced through industry-committed fees—has been linked to approvals of products with marginal benefits or unresolved risks, as the agency's depends on sustained application volumes and positive relations. and other watchdog groups contend this creates a "pay-to-play" dynamic, where fee-paying companies gain preferential treatment, undermining impartiality. Compounding these issues is the between FDA personnel and industry, which amplifies capture risks under the user fee regime. A 2016 analysis found that 27% of FDA hematology-oncology drug reviewers from 2001 to 2010 later joined the pharmaceutical firms whose products they evaluated. Similarly, a 2018 study revealed that companies frequently hired FDA staffers who had directly overseen their successful applications, with 65% of such hires involving pivotal decision-makers. This pattern persists; in 2024, departing FDA employees received internal guidance on industry contacts, highlighting loopholes in post-employment restrictions that allow indirect influence. Health Affairs research indicates such transitions render agencies more susceptible to capture, as ex-regulators leverage insider knowledge to consult or executive for fee-paying entities, potentially skewing future FDA decisions toward leniency to facilitate career mobility. Empirical evidence of conflicts includes PDUFA's role in accelerating approvals without proportional safety enhancements; while review times shortened from 30 months pre-1992 to under 10 months by the , post-market surveillance remains underfunded relative to pre-approval processes, leaving risks unaddressed. Proponents of reform, including legal scholars, propose fees from review performance metrics to mitigate these incentives, arguing the current system prioritizes speed over scrutiny in a manner causal to suboptimal regulatory outcomes. Despite defenses that user fees enable Congress has withheld, the model's inherent dependency—exacerbated by industry negotiation leverage—sustains debates over whether it serves public welfare or entrenches capture.

Major Oversight Failures (Opioids, Vioxx, and Beyond)

The U.S. Food and Drug Administration (FDA) approved , marketed as Vioxx, on May 20, 1999, for the relief of symptoms and acute pain, based on clinical trials showing efficacy comparable to traditional NSAIDs but with potentially fewer gastrointestinal risks due to its COX-2 selective inhibition. However, post-approval data from studies like VIGOR (2000) indicated an elevated risk of and compared to naproxen, prompting Merck to add a cardiovascular warning to the label in April 2002 after FDA review, though critics argued the agency delayed action despite internal concerns raised as early as 2001. The APPROVe trial, halted in September 2004, confirmed a increase of 1.92 for serious cardiovascular thrombotic events after 18 months of use, leading Merck to voluntarily withdraw Vioxx worldwide on September 30, 2004. FDA safety evaluator David Graham testified in November 2004 that Vioxx likely caused 88,000 to 139,000 excess cases of heart attacks and strokes in the U.S., with 30-40% attributable to sudden cardiac death, attributing the agency's failure to inadequate post-market surveillance and reluctance to challenge sponsor data. This episode highlighted systemic issues in FDA's reliance on manufacturer-submitted evidence and underfunding of its Office of Drug Safety, as Graham estimated Vioxx's risks were foreseeable from pre-approval data but overlooked. In the opioid domain, the FDA approved Purdue Pharma's extended-release oxycodone (OxyContin) on December 12, 1995, for moderate-to-severe pain requiring around-the-clock dosing, with initial labeling claiming delayed absorption reduced abuse potential and citing addiction as "very rare" based on limited evidence from short-term trials. This approval facilitated aggressive marketing by Purdue, which downplayed addiction risks and promoted the drug for chronic non-cancer pain despite inadequate long-term safety data on misuse, contributing to a surge in prescriptions from 1996 onward; by 2000, OxyContin accounted for 80% of the U.S. oxycodone market. FDA oversight lapsed in enforcing post-approval restrictions, failing to penalize misleading claims until a 2007 guilty plea by Purdue for misbranding, by which time opioid overdoses had risen sharply; a 2020 analysis identified FDA's approval of high-dose formulations without robust abuse-deterrent assessments and lax monitoring of real-world diversion as key policy failures exacerbating the epidemic, which claimed over 500,000 lives from prescription opioids by 2019. Beyond these cases, FDA approvals of other COX-2 inhibitors like (Bextra), greenlit in November 2001 and withdrawn in April 2005 amid cardiovascular and severe skin reaction risks, underscored persistent gaps in class-wide risk evaluation, with the agency issuing a black-box warning only after accumulating reports. Similar patterns emerged in approvals, such as lollipops (Actiq) in 1998 for breakthrough despite off-label promotion for non-cancer use, leading to overdose clusters that FDA addressed belatedly through labeling changes in 2007; these incidents reflect broader critiques of under-resourced , where voluntary reporting systems like FAERS captured only a fraction of harms, delaying interventions until litigation or mortality spikes forced action. Independent reviews, including congressional inquiries, have faulted the FDA for prioritizing speed-to-market under user-fee pressures over rigorous post-approval monitoring, enabling drugs with unbalanced risk-benefit profiles to persist for years.

COVID-19 Response Shortcomings

The FDA's early regulatory stance on laboratory-developed diagnostic tests, requiring premarket review and initially limiting their deployment without , contributed to diagnostic shortages in the initial months of the , as only CDC-developed tests were available until policy adjustments in late February 2020. This delay hampered and case identification, exacerbating transmission in communities where testing capacity lagged behind demand. Subsequent authorizations of PCR tests often permitted cycle thresholds (Ct) up to 40 cycles, enabling detection of low-level or residual viral RNA that may not indicate active infectivity, as viral loads exceeding detection limits frequently occur post-contagious phase. Without mandatory Ct value reporting or standardization across assays, clinical decisions on isolation and transmission risk relied on binary positive/negative results, potentially prolonging quarantines for non-transmissible cases and inflating case counts used for policy justifications. Professional bodies like the Association for Molecular Pathology cautioned against routine Ct use for prognosis due to variability and lack of commutability between platforms, underscoring the FDA's failure to enforce thresholds aligned with infectiousness data from viral culture studies. In treatment approvals, the FDA revoked the EUA for bamlanivimab monotherapy on April 16, 2021, based on data showing in emerging variants like those from and , despite observational evidence of reduced hospitalizations in high-risk outpatients prior to widespread variant dominance. Critics, including analyses of real-world outcomes, contended this premature broad revocation created a therapeutic void before alternatives like gained traction, potentially contributing to in Delta-dominant periods when combination therapies or variant-specific updates could have been prioritized over outright withdrawal. Similar revocations for other monoclonals followed as variants rendered them ineffective, highlighting the agency's reactive framework ill-suited to rapidly evolving without parallel investment in adaptive authorization pathways. The FDA's communications discouraging for , including posts equating its human use to veterinary applications, prompted a 2022 by physicians claiming unlawful interference with off-label prescribing authority; the agency settled in March 2024 by removing such content and acknowledging limits to its regulatory speech. Although randomized trials and meta-analyses, including Cochrane reviews, found insufficient evidence of clinical benefit for in reducing mortality or hospitalization—often due to methodological flaws in positive studies—the FDA's emphatic warnings, absent from similarly equivocal repurposed drugs, were faulted for eroding trust and constraining physician-led exploration amid sparse early-trial data. This approach contrasted with the agency's flexibility in EUAs, raising questions about inconsistent risk-benefit calibration for non-pharmaceutical interventions versus novel biologics. Vaccine rollout under EUAs prioritized speed via , authorizing Pfizer-BioNTech on December 11, 2020, and on December 18, 2020, based on interim phase 3 data showing 95% and 94% against symptomatic . However, post-authorization revelations necessitated label updates, such as June 2025 warnings for / risks in young males following mRNA doses, with incidence rates of 40-60 cases per million second doses in adolescents. By September 2025, the FDA restricted booster approvals to high-risk groups, overruling internal scientists advocating broader access, amid debates over waning against transmission and variant escape. These adjustments exposed gaps in pre-EUA modeling of rare adverse events and long-term , with surveillance systems like VAERS revealing underreporting factors estimated at 10-100-fold for serious outcomes, complicating causal attribution. Broader structural limitations, as self-assessed in the FDA's 2024 post-pandemic review, included authorities inadequate for 21st-century complexities, such as shortages for tests and therapeutics, which amplified domestic vulnerabilities despite global dependencies. The agency's emphasis on centralized control over decentralized innovation stifled rapid scaling of generics and diagnostics, per analyses, prioritizing liability mitigation over adaptive regulation in a pathogen context. These elements collectively underscored deficits, with external evaluations citing slow data dissemination and over-reliance on flexibilities without robust for variant-driven .

Food Safety and Enforcement Gaps

The Food and Drug Administration (FDA) faces significant challenges in food safety enforcement, primarily due to insufficient inspection capacity and reliance on voluntary industry compliance. Under the Food Safety Modernization Act (FSMA) of 2011, the FDA is required to inspect domestic high-risk food facilities at least every three years and low-risk facilities every five years, yet it has failed to meet these targets annually since fiscal year 2018. As of fiscal year 2023, approximately 75,000 domestic food facilities were subject to FDA oversight, but the agency conducted an average of only 8,353 domestic inspections per year from 2018 to 2023, covering a small fraction of facilities and leaving over 26% of high-risk domestic sites uninspected for three or more years. Foreign inspections are even more limited, averaging 917 annually against a mandated target derived from import volumes, representing about 5% of the required scope and exacerbating risks from imported foods that constitute over 15% of the U.S. diet. These inspection shortfalls contribute to persistent foodborne illness outbreaks, underscoring enforcement gaps. The Centers for Disease Control and Prevention (CDC) estimates that foodborne illnesses cause approximately 48 million cases, 128,000 hospitalizations, and 3,000 deaths annually in the U.S., with over 9,000 outbreaks reported across all states from 2011 to 2022. In 2023, the FDA's Coordinated Outbreak Response and Evaluation (CORE) Network managed investigations into multiple multistate outbreaks, issuing advisories for ten such events linked to products like morel mushrooms and contaminated applesauce pouches, yet systemic under-inspection allows hazards to persist undetected. Reported illnesses from contaminated foods rose to 1,392 cases in 2024 from 1,118 in 2023, with severe cases doubling, highlighting vulnerabilities in supply chains for , , and processed foods where proactive enforcement is inconsistent. Critics, including a 2022 investigation based on over 50 interviews, argue that the FDA's food division prioritizes reactive responses over preventive measures, failing consumer expectations amid resource constraints and a historical shift of personnel toward drug regulation. Enforcement mechanisms further reveal gaps, as the FDA issues warning letters for violations—149 for human food facilities in fiscal year 2023—but rarely pursues criminal prosecutions, depending instead on voluntary recalls that may not fully mitigate risks. An Office of Inspector General review of 30 voluntary food recalls found that the FDA's process was not always efficient or effective in ensuring product removal from commerce, with inadequate effectiveness checks allowing contaminated items to remain in distribution. This voluntary framework, while enabling rapid response, lacks mandatory authority for most recalls, leading to incomplete recoveries; for instance, surveys indicate consumer confusion and over-discarding, but actual hazard elimination depends on firm cooperation without sufficient penalties for non-compliance. Declining inspection numbers—19% fewer in 2023 than in 2017—stem from workforce attrition, budget reallocations, and post-COVID disruptions, prompting calls from the Government Accountability Office (GAO) for strategies to retain inspectors and prioritize high-risk imports. Such deficiencies have economic repercussions, with outbreaks costing billions in healthcare and lost productivity annually, yet the FDA's fragmented oversight across domestic, imported, and state-coordinated efforts perpetuates these vulnerabilities.

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