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Select agent

Select agents and toxins are biological agents and toxins designated by the federal government as having the potential to pose a severe threat to and safety, to animal or plant health, or to the safety of animal or plant products. These include certain , viruses, fungi, and toxins such as (anthrax), variola virus (), and botulinum neurotoxin, selected based on criteria like ease of dissemination, high mortality rates, and potential for mass casualties or economic disruption. The designation aims to mitigate risks from deliberate misuse, accidental release, or natural outbreaks through stringent regulatory controls. The Federal Select Agent Program (FSAP), a joint effort between the Centers for Disease Control and Prevention (CDC) under the Department of Health and Human Services and the Animal and Plant Health Inspection Service (APHIS) under the Department of Agriculture, oversees the possession, use, and transfer of these materials in the United States. Established under the Public Health Security and Bioterrorism Preparedness and Response Act of 2002 following post-9/11 concerns over bioterrorism, the program requires entities to register, implement biosafety and biosecurity measures, conduct personnel suitability checks, and undergo regular inspections. The select agent list, initially comprising 42 items in 1997, has evolved through periodic reviews—currently encompassing 63 agents and toxins—and includes a Tier 1 subcategory for those posing the highest deliberate misuse risk, such as Yersinia pestis (plague), mandating enhanced physical security and incident response protocols. While the program has facilitated secure into , diagnostics, and countermeasures against high-threat pathogens, it has faced over consistency, failures, and potential overreach in restricting legitimate scientific . Notable incidents, including unauthorized transfers and breaches at registered facilities, have prompted congressional reviews questioning the adequacy of oversight and from regulated entities. These challenges underscore ongoing debates about balancing imperatives with the demands of , particularly given the causal links between lapses in and historical outbreaks or near-misses.

Overview and Definition

Criteria for Designation

The designation of biological agents and toxins as select agents is governed by the Public Health Security and Preparedness and Response Act of 2002, which authorizes the Secretary of and Human Services (HHS) and the Secretary of (USDA) to identify those with the potential to pose a severe threat to and safety, animal health, plant health, or animal or plant products. This determination is codified in federal regulations, including 42 CFR Part 73 for HHS-regulated agents affecting human health, 9 CFR Part 121 for USDA-regulated agents affecting animal health, and 7 CFR Part 331 for plant health agents. The core criterion is the agent's capacity to cause significant harm through intentional misuse, weighed against factors such as severity and impact. Designation involves a multi-factor risk assessment incorporating biological characteristics like (e.g., or serious debilitation), transmissibility (e.g., person-to-person or spread), environmental stability, and ease of dissemination or production in quantities sufficient for harm. Non-biological elements are also evaluated, including the availability and efficacy of medical countermeasures (e.g., or antibiotics), susceptibility, diagnostic detectability, and historical association with or bioweapons programs. Pathogens exceeding thresholds across these criteria—such as high mortality rates without effective treatments—are prioritized, as seen in evaluations where agents like are designated due to their transmissibility and low-dose . The HHS and USDA conduct biennial reviews to assess the select list, incorporating emerging data on agent characteristics, threat intelligence, and advancements; this process has led to delistings (e.g., certain strains of Francisella tularensis in 2017) when risks diminish due to improved countermeasures. A subset designated as select agents (e.g., botulinum neurotoxins, ) undergoes heightened scrutiny based on amplified risks, including potential for mass casualties via small quantities and limited prophylaxis, triggering stricter security protocols. Designations remain dynamic, balancing empirical threat data against over-regulation that could hinder legitimate .

Risk Tiers and Categories

The Federal Select Agent Program, jointly administered by the Centers for Disease Control and Prevention (CDC) and the (USDA), designates biological select agents and toxins (BSAT) based on their potential to pose a severe threat to , animal health, plant health, or agricultural products. These agents are not formally divided into multiple numbered tiers beyond , but BSAT represent a critical subset identified for heightened risk due to their capacity for deliberate misuse resulting in mass casualties, widespread economic disruption, or significant environmental damage. Non- select agents, while still subject to registration, transfer restrictions, and protocols under 42 CFR Parts 73, 331, and 121, do not trigger the enhanced security mandates applicable to . Tier 1 designation, implemented via revisions to the select agent regulations in 2012, applies to agents with demonstrated attributes enabling high-consequence events, such as ease of dissemination, high lethality, or stability in aerosols. Examples include Ebolavirus (causing Ebola hemorrhagic fever), Francisella tularensis (tularemia), Yersinia pestis (plague), Variola major and Variola minor viruses (smallpox), Marburg virus, and botulinum neurotoxins, among others listed in the program's appendices. Entities possessing Tier 1 BSAT must implement additional measures, including pre-access suitability determinations for all personnel, enhanced physical security barriers, inventory controls with tamper-evident seals, and video monitoring of laboratories, beyond the baseline requirements for all select agents. These protocols aim to mitigate insider threats and unauthorized access, informed by risk assessments of historical bioterrorism vulnerabilities. The biennial review process, mandated by the Public Health Security and Bioterrorism Preparedness and Response Act of 2002, evaluates the select agent list for updates, considering factors like pathogenicity, transmissibility, availability of countermeasures, and emerging threats, but has maintained the framework without introducing further subdivisions as of the December 2024 review. Historical categorizations, such as pre-2012 CDC groupings of Category A (highest risk, e.g., , ) and Category B agents (moderate ease of ), informed the current system but were consolidated into the unified select agent list with overlay to prioritize resources on empirically highest-risk pathogens. This structure reflects causal assessments of agent attributes rather than uniform application, ensuring proportionality in regulatory burden while addressing dual-use research concerns.

Historical Development

Early Regulations and Precedents

The Antiterrorism and Effective Death Penalty Act of 1996 (AEDPA), signed into law on April 24, 1996, established the initial statutory framework for regulating biological agents and toxins in the United States by amending section 361 of the . This legislation directed the Secretary of Health and Human Services to promulgate regulations governing the transfer of agents that could pose a severe threat to and safety, aiming to prevent their diversion for illicit purposes such as . The Act identified criteria for such agents, including ease of dissemination, high mortality rates, and potential for public panic, marking the first federal mandate for a targeted registry of high-risk pathogens beyond general import controls. In June 1996, the Centers for Disease Control and Prevention (CDC) proposed interim final rules under 42 CFR Part 72 to implement AEDPA, defining "select agents" as specific infectious agents and toxins requiring oversight for interstate transfers. These rules, finalized in October 1996, mandated that facilities transferring or receiving select agents register with the CDC, undergo validation of security measures, and report suspicious activities, with an initial list encompassing approximately 24 agents such as Bacillus anthracis, Yersinia pestis, and botulinum toxin. Compliance was enforced through civil penalties up to $250,000 and criminal sanctions for willful violations, though the framework emphasized transfer controls over possession or in-house security, reflecting concerns from events like the 1995 Aum Shinrikyo sarin attacks that highlighted risks of non-state actors acquiring pathogens. Precedents for these regulations included longstanding CDC import permit requirements under 42 CFR Part 71 since the early 1970s, which restricted entry of etiologic agents to prevent accidental introductions, and the Biological Weapons Anti-Terrorism Act of 1989, which criminalized offensive use of biological agents in line with the 1972 but did not address legitimate research safeguards. The 1996 rules thus built on these by introducing domestic transfer restrictions and a nascent select agent list, informed by interagency assessments of dual-use risks from legitimate laboratories, though enforcement remained limited without background checks or Tiered security until post-2001 enhancements. This early system registered fewer than 300 entities by 2001, underscoring its preliminary scope amid growing awareness of insider threats.

Post-9/11 Establishment and Key Legislation

The terrorist attacks of September 11, 2001, and the subsequent letter attacks heightened national concerns over , prompting swift legislative action to strengthen controls on biological agents with high misuse potential. The Uniting and Strengthening America by Providing Appropriate Tools Required to Intercept and Obstruct Terrorism (USA PATRIOT) Act, signed into law on October 26, 2001, amended Section 175 of Title 18 of the U.S. Code to prohibit access to select agents and toxins by "restricted persons," including individuals convicted of certain crimes, those under for serious offenses, fugitives, illegal users, dishonorably discharged , undocumented immigrants, those deemed mentally defective or committed to mental institutions, and designated terrorists or members of terrorist organizations. This established the foundational criteria for security risk assessments, criminalizing unauthorized possession and requiring federal background checks for access. Building on the , the Public Health Security and Bioterrorism Preparedness and Response Act of 2002 (Bioterrorism Act), enacted on June 12, 2002, as 107-188, expanded regulatory authority over select agents and toxins to address possession, use, and transfer risks. The Act directed the Secretary of and (HHS) to regulate biological agents and toxins posing severe threats to , requiring registration of entities handling them, development of a select agent list via biennial review, implementation of and security standards, and safeguards against accidental or intentional release. Subtitle B, known as the Agricultural Bioterrorism Protection Act, extended parallel oversight to the U.S. Department of Agriculture (USDA) for agents affecting animal or plant , mandating similar registration, transfer controls, and reporting of theft or loss. These laws formalized the Federal Select Agent Program (FSAP) as a collaborative effort between the Centers for Disease Control and Prevention (CDC) under HHS and the Animal and Plant Health Inspection Service (APHIS) under USDA, issuing implementing regulations such as 42 CFR Part 73 (HHS/CDC) and 7 CFR Part 331/9 CFR Part 121 (USDA). By 2003, final rules required facilities to register, undergo inspections, and ensure physical security, marking a shift from prior voluntary or limited measures to mandatory, risk-based federal oversight aimed at preventing diversion to malicious actors while enabling legitimate research. Subsequent amendments, including the of 2015, refined prohibited person definitions but preserved the core framework.

Purpose and Security Rationale

Bioterrorism and Intentional Threats

Select agents and toxins are regulated under the Federal Select Agent Program due to their potential for intentional misuse in , defined as the deliberate deployment of biological agents to inflict mass casualties, generate public panic, or achieve coercive objectives against civilian populations. These materials are assessed for characteristics enabling effective weaponization, such as stability, environmental persistence, and low infectious doses, which amplify their threat in disseminated attacks. The program's security rationale prioritizes containment to deny access to non-state actors, including terrorists or rogue individuals, who could exploit these properties absent robust oversight. Designation as select agents hinges on statutory criteria from the Public Health Security and Bioterrorism Preparedness and Response Act of 2002, evaluating the agent's impact on human , degree of contagiousness and modes, efficacy of existing treatments or , and suitability for biological weaponry. agents, a subset like (causing ), (), and botulinum neurotoxin, warrant heightened scrutiny for their elevated risk, including potential for widespread dissemination via air or mail and mortality rates exceeding 50% in untreated cases. This tier reflects assessments of deliberate misuse likelihood, informed by intelligence on proliferation risks and historical precedents, rather than natural outbreak potentials alone. The 2001 Amerithrax attacks exemplified these vulnerabilities, where refined spores mailed to media outlets and offices infected 22 individuals, killing 5 and prompting national alerts, with dissemination achieved through postal systems without advanced infrastructure. Earlier attempts, such as the cult's 1990s efforts to aerosolize and in , failed due to technical limitations but highlighted non-state actors' intent and the agents' accessibility from environmental or lab sources. Regulations thus mandate risk-based plans, including personnel vetting via FBI checks and physical safeguards, to interdict pathways from legitimate to adversarial hands, as unauthorized possession could enable attacks rivaling chemical or radiological threats in scale. Biocrimes, involving targeted releases against individuals or small groups, represent a parallel intentional , though select agent controls emphasize terrorism's broader societal disruption potential. Empirical data from incident tracking shows rare but persistent risks, with 33 biological agent attacks logged globally from 1970 to 2019, yielding 9 fatalities and over 800 injuries, often leveraging culturable pathogens like those now classified as select. These controls do not preclude dual-use but impose accountability to balance innovation against the causal chain from theft or insider to engineered outbreaks.

Accidental Releases and Dual-Use Risks

Accidental releases of select agents pose significant risks due to the high infectivity, virulence, and potential for rapid spread of these pathogens and toxins outside controlled laboratory environments. Between 2003 and 2009, U.S. government laboratories reported 395 incidents involving potential releases of select agents, including equipment failures, spills, and procedural errors that could have led to exposure of personnel or the public. Regulations mandate immediate reporting of such events to the CDC or USDA, encompassing losses, thefts, or releases that threaten human, animal, or plant health, with protocols for containment and decontamination to mitigate outbreaks. Notable incidents include a 2014 CDC event where viable Bacillus anthracis spores were inadvertently shipped to external labs due to incomplete inactivation, exposing over 80 potentially at-risk individuals, though no infections resulted after prophylaxis. Another involved the 2014 discovery of viable variola virus (smallpox) vials forgotten in a National Institutes of Health storage facility since the 1950s, highlighting vulnerabilities in long-term inventory management. Despite these occurrences, federal records indicate no laboratory-acquired deaths or public illnesses attributable to select agent work through 2023. Dual-use risks arise from research on select agents that yields knowledge or technologies applicable to both beneficial medical advancements and malevolent purposes, such as enhanced pathogens for . Dual-use research of concern (DURC) encompasses life sciences studies reasonably anticipated to enable misuse, including alterations increasing transmissibility, , or resistance in agents like or SARS-CoV precursors, often overlapping with select agent lists. U.S. policy requires institutional review for DURC involving 15 specific agents/toxins, such as H5N1 and , to assess benefits against misuse potential, with mitigation plans for funding and dissemination. These risks extend to pathogens with enhanced potential (ePPP), where gain-of-function experiments could inadvertently or deliberately amplify threats, prompting federal oversight frameworks updated in 2024 to balance scientific progress with security. Empirical data from historical lab exposures, including 71 high-risk incidents from 1975 to 2016, underscore the causal pathway from procedural lapses to unintended dissemination, reinforcing the need for stringent levels (BSL-3/4) and dual-use ethical reviews.

Regulatory Framework

Federal Agencies and Oversight

The Federal Select Agent Program (FSAP) serves as the primary federal mechanism for regulating biological select agents and toxins, jointly administered by the Centers for Disease Control and Prevention (CDC), under the Department of Health and Human Services (HHS), and the Animal and Plant Health Inspection Service (APHIS), under the (USDA). This collaborative structure ensures coordinated oversight of agents posing severe threats to , animal health, or health, with FSAP developing, implementing, and enforcing regulations codified in 42 CFR Part 73, 7 CFR Part 331, and 9 CFR Part 121. Entities seeking to possess, use, or transfer select agents must register with FSAP, undergo FBI-conducted security risk assessments via the Criminal Justice Information Services Division, and comply with , security, and incident reporting standards. The CDC, through its Division of Regulatory Science and Compliance, regulates HHS select agents and toxins—primarily those with potential to cause severe human disease, such as and Ebola virus—focusing on threats to and safety. CDC oversight includes conducting site inspections (both announced and unannounced), reviewing entity security plans, and verifying compliance with possession limits, such as the 10 milligram threshold for certain toxins like . For overlapping agents affecting both humans and animals (e.g., viruses), CDC coordinates with USDA to apply dual regulatory requirements. USDA's APHIS divides its responsibilities between Veterinary Services (VS) for animal pathogens and Plant Protection and Quarantine (PPQ) for plant pathogens, regulating agents like Foot-and-mouth disease virus that threaten livestock or agriculture. APHIS enforces transfer controls, inventory audits, and emergency response protocols, with authority to suspend or revoke registrations for non-compliance. Joint FSAP activities include biennial reviews of the select agent list to assess risk based on factors like transmissibility and availability of countermeasures, as demonstrated in the December 2024 update maintaining 67 HHS agents/toxins and 25 USDA agents. Additional federal oversight is provided by the HHS Office of Inspector General (OIG), which audits FSAP operations to evaluate compliance risks and program efficacy, including reviews of laboratory security following incidents like the 2014 CDC exposure mishandling. FSAP publishes annual reports detailing inspections (over 1,200 conducted in 2024 across registered entities), violations, and corrective actions, promoting transparency while prioritizing risk-based enforcement. This multi-agency framework emphasizes prevention of misuse, with agents (e.g., ) subject to enhanced FBI screening and cybersecurity requirements.

Registration, Security, and Biosafety Requirements

Entities seeking to possess, use, or transfer biological select agents or toxins must register with the Federal Select Agent Program (FSAP), a collaborative effort between the Centers for Disease Control and Prevention (CDC) and the U.S. Department of Agriculture's Animal and Plant Health Inspection Service (APHIS). Registration applications are submitted via APHIS/CDC Form 1, which requires detailed information, identification of the specific select agents or toxins involved, and descriptions of proposed activities. Approval hinges on demonstrations of adequate , , and incident response capabilities, with the process typically involving on-site inspections and a suitability determination for the Responsible Official (RO), who oversees all compliance aspects. Registrations are valid for up to three years, subject to renewal and periodic audits to ensure ongoing adherence to 42 CFR Part 73 and 7 CFR Part 331 regulations. Security requirements mandate the development of a site-specific plan derived from a tailored to the agents' characteristics and facility vulnerabilities. This plan must include physical barriers, access controls such as keycard systems or , personnel reliability screening, and monitoring for unauthorized entry, with storage areas and laboratories prohibited from public access. For select agents—deemed highest risk due to low infectious doses or transmission potential—enhanced measures apply, including strict limitations on the number of approved personnel, additional physical barriers like reinforced doors, and continuous intrusion detection systems integrated with response protocols. All individuals requiring access undergo FBI-conducted risk assessments, with denials or revocations for those identified as restricted persons under . Inventory tracking, including viable agent counts and toxin quantities, must be conducted at least monthly, with discrepancies reported immediately to FSAP. Biosafety and biocontainment protocols require a comprehensive plan specifying , administrative safeguards, and work practices to prevent accidental , generation, or environmental release. Most select agents necessitate Level 3 (BSL-3) facilities with directional airflow, filtration, and hands-on in procedures like autoclaving and , while certain high-risk agents such as variola demand BSL-4 suits and III cabinets. For toxins, handling limits apply—e.g., no more than 100 mg of botulinum without exemption—and must occur in certified biological safety cabinets with spill response kits. is mandatory for all personnel, covering agent-specific hazards, use, and emergency procedures, with annual refreshers and documentation of proficiency. Valid medical surveillance, including vaccinations where available (e.g., for or ), and incident reporting within 24 hours ensure rapid of potential breaches.

Transfer, Possession, and Reporting Rules

Possession of select s and s is restricted to individuals or entities holding a valid of registration issued by the Centers for Disease Control and Prevention (CDC) for HHS-regulated agents or the Animal and Plant Health Inspection Service (APHIS) for USDA-regulated agents, unless an exemption applies. Exemptions include clinical or diagnostic laboratories that identify a select agent in a specimen for or , provided the agent or toxin is secured, transferred to a registered entity, or destroyed within 7 calendar days of identification, with immediate reporting of any theft, loss, or release. Additional exemptions cover proficiency testing programs, where specimens must be transferred or destroyed within 90 calendar days of receipt, and products regulated under federal statutes such as the Federal Food, Drug, and Cosmetic Act, provided they meet clearance criteria. Registration certificates specify the agents, quantities, and activities permitted, and possession without registration or exemption constitutes a violation subject to enforcement. Transfers of select agents and toxins may occur only between registered individuals or entities authorized to possess the specific agent or toxin, with prior approval required from CDC or APHIS via submission of APHIS/CDC Form 2 through the Federal Select Agent Program's eFSAP portal or other designated methods. The sender must verify the recipient's registration covers the agent, ensure packaging and shipping comply with applicable transportation regulations, and conduct transfers by individuals approved under the sender's security plan; approvals are valid for 30 calendar days or until any material facts change, such as registration revocation. Recipients must submit confirmation of receipt using Form 2 within 2 business days and immediately notify the Federal Select Agent Program if the shipment is not received within 48 hours or arrives damaged. For HHS-regulated toxins exceeding 100 nanograms in aggregate, transfers require documentation of the recipient's legitimate purpose and due diligence by the sender to prevent diversion. Parallel requirements apply under USDA regulations for plant and animal select agents, prohibiting transfers without equivalent authorization. Reporting rules mandate immediate notification to CDC or APHIS—and, for theft or loss, to federal, state, or local —upon discovery of any , loss, or release of a select or , followed by submission of APHIS/CDC Form 3 within 7 calendar days detailing the incident, including , , , and response actions. Releases triggering occupational or escape from primary barriers require the same immediate alert, specifying the number of exposed individuals, environmental impact, and measures. Entities must also the of a select or in diagnostic contexts using APHIS/CDC , with submissions due within 7 days for routine cases or immediately for high-risk agents like . These requirements ensure rapid response to potential risks, with records retained for at least 3 years, and apply uniformly across HHS and USDA jurisdictions to facilitate coordinated oversight.

Lists of Select Agents and Toxins

HHS/CDC Select Agents and Toxins

The HHS/CDC select agents and toxins are biological agents and toxins regulated by the Centers for Disease Control and Prevention (CDC) within the Department of Health and Human Services (HHS) due to their potential to cause severe harm to and , as codified in 42 CFR § 73.3. These exclude overlap agents jointly regulated with the USDA, focusing instead on pathogens and substances primarily affecting humans, such as certain hemorrhagic fever viruses, , and potent neurotoxins. The list undergoes biennial review, with updates effective January 16, 2025, reflecting assessments of risk based on factors like transmissibility, , and availability of countermeasures; notable prior adjustments included removals of agents like species from federal oversight following evaluations of diagnostic needs and low risk. Tier 1 designation applies to a of these agents—, , reconstructed 1918 , Variola major virus, Variola minor virus, biovar anthracis, , , and Botulinum neurotoxins—imposing enhanced security requirements, including full-time officers and personnel reliability programs, due to their capacity for widespread casualties or economic impact. Exclusions apply to non-viable forms, attenuated strains approved by the HHS , naturally occurring environmental samples, or toxin quantities below regulatory thresholds (e.g., less than 1 mg Botulinum neurotoxins or 100 mg ). Genetically modified variants or synthetic nucleic acids capable of producing viable agents remain regulated if they meet functional criteria. Viruses (HHS-only):
  • Crimean-Congo haemorrhagic fever virus
  • Eastern equine encephalitis virus
  • Ebolavirus* (Tier 1, encompassing all species)
  • Lassa fever virus
  • Lujo virus
  • Marburg virus* (Tier 1)
  • Monkeypox virus (excludes clade II if identified)
  • Reconstructed 1918 influenza A virus* (Tier 1)
  • SARS-CoV
  • SARS-CoV/SARS-CoV-2 chimeric viruses resulting in attenuation loss
  • South American haemorrhagic fever viruses (Chapare, Guanarito, Junín, Machupo, Sabia)
  • Tick-borne encephalitis complex (Far Eastern subtype, Siberian subtype)
  • Kyasanur Forest disease virus
  • Omsk haemorrhagic fever virus
  • Variola major virus* (Tier 1)
  • Variola minor virus* (Tier 1)
  • Madariaga virus (excluded if naturally identified)
Bacteria (HHS-only): Toxins (HHS-only, with possession limits):
  • (less than 1000 mg excluded)
  • Botulinum neurotoxins* (, less than 1 mg excluded; includes producing species)
  • Conotoxins (specific sequences with 30+ )
  • Diacetoxyscirpenol (less than 1000 mg excluded)
  • (less than 100 mg excluded)
  • (less than 100 mg excluded)
  • Staphylococcal enterotoxins (subtypes A through E, less than 100 mg each excluded)
  • T-2 toxin (less than 1000 mg excluded)
  • (less than 1000 mg excluded)

USDA Select Agents and Toxins

The (USDA) regulates select agents and toxins that pose a severe threat to animal health, plant health, or agricultural products and productivity, distinct from those primarily affecting health under HHS/CDC oversight. These are managed through the USDA Animal and Plant Health Inspection Service (APHIS), specifically the Division of Agricultural Select Agents and Toxins (DASAT), under 9 CFR Part 121 for animal agents and 7 CFR Part 331 for plant agents. The criteria for inclusion emphasize agents capable of causing widespread economic disruption via epizootics or crop devastation, with biennial reviews assessing risk based on transmissibility, , availability of countermeasures, and research impacts. USDA select agents are categorized into Veterinary Services (VS) agents affecting and , and Plant Protection and (PPQ) agents targeting crops. Tier 1 designation applies to agents like and virus, requiring enhanced security measures due to their potential for rapid international spread and severe agricultural consequences. No toxins are exclusively regulated by USDA; overlaps with HHS lists (e.g., ) fall under joint oversight. Exclusions exist for attenuated strains, low-pathogenicity variants (e.g., certain subtypes), and non-viable forms to facilitate research without compromising safety. VS Select Agents (Animal Pathogens):
  • Avian influenza virus
  • Classical swine fever virus
  • (Tier 1)
  • Goat pox virus
  • Lumpy skin disease virus
  • Mycoplasma capricolum/super_species (e.g., capripneumoniae)
  • Mycoplasma mycoides/super_species (e.g., mycoides)
  • Newcastle disease virus
  • Peste des petits ruminants virus
  • virus (Tier 1)
  • Sheep pox virus
  • Swine vesicular disease virus
PPQ Select Agents (Plant Pathogens):
  • Coniothyrium glycines
  • Ralstonia solanacearum (race 3, biovar 2)
  • Rathayibacter toxicus
  • Sclerophthora rayssiae var. zeae
  • Synchytrium endobioticum
  • Xanthomonas oryzae pv. oryzae
In the December 2024 biennial review, USDA and HHS removed Brucella species (abortus, melitensis, suis), African horse sickness virus, and Peronosclerospora philippinensis from the select agent lists to reduce research barriers while maintaining biosafety protocols, effective following Federal Register publication on December 16, 2024. These changes reflect assessments that diagnostic advancements and vaccine development have mitigated risks without necessitating continued select agent status.

Overlapping Agents and Toxins

Overlap select agents and toxins are biological agents and toxins regulated under both the HHS/CDC and USDA/APHIS lists due to their potential to pose severe threats to both and or products. These agents require coordinated oversight by the Federal Select Agent Program (FSAP), with entities possessing them needing to comply with dual-agency registration, security, and transfer protocols to mitigate risks from or accidental release. As of the 2024 biennial review finalized on December 17, 2024, the overlap list comprises five agents, reflecting assessments of their pathogenicity, transmissibility, and availability of countermeasures. The current overlap select agents are:
  • Bacillus anthracis: Causes , a zoonotic disease transmissible via spores from infected animals (e.g., , sheep) to humans through cutaneous, , or gastrointestinal routes; regulated for its weaponization history, including the 2001 U.S. anthrax attacks.
  • Burkholderia mallei: Etiologic agent of , primarily affecting equines like horses and donkeys, with rare but severe human infections via or contact; historically used in biological warfare attempts.
  • Burkholderia pseudomallei: Responsible for , an endemic soil-borne infection in and affecting humans and various animals (e.g., goats, sheep); high mortality in untreated cases, with environmental persistence enhancing dissemination risks.
  • Nipah virus: Emerged in 1998-1999 outbreaks in and , spilling over from bats to pigs and humans, causing with up to 75% fatality; no licensed or as of 2024.
  • Venezuelan equine encephalitis virus: An causing febrile illness and in humans, with primary reservoirs in and amplification in equines; epizootic strains pose dual human-animal threats, as seen in 1960s-1970s Latin American outbreaks affecting thousands.
Prior to the 2024 updates, the list included , , and , which were removed following biennial review criteria evaluating reduced bioterrorism risk due to attenuated in certain strains, effective for animal hosts, and diagnostic advancements. Overlap agents are subject to enhanced security measures if designated, including full-time security personnel, background checks, and inventory controls, with transfers requiring FSAP approval to prevent inter-agency regulatory gaps. Exclusions apply to attenuated strains or stocks under specific conditions, but possession of even small quantities demands registration to ensure traceability.

Compliance and Enforcement

Inspection and Audit Processes

The Federal Select Agent Program (FSAP), a collaborative effort between the Centers for Disease Control and Prevention (CDC) and the U.S. Department of Agriculture's Animal and Plant Health Inspection Service (APHIS), oversees inspection processes to verify compliance with select agent regulations. Registered entities are required to conduct annual internal inspections of each space where select agents or toxins are stored or used, assessing adherence to , , , incident response, and controls as outlined in 42 CFR Part 73. These internal audits, led by the entity's Responsible Official (RO), must document deviations from regulations and implement corrective actions, with records retained for federal review. FSAP performs federal on-site inspections using standardized checklists to evaluate laboratory safeguards, including physical security measures, access controls, viable organism inventories, and emergency procedures. These risk-based assessments occur periodically, with initial site visits required for registration approvals, often taking at least three months to complete. In 2024, FSAP conducted inspections resulting in 197 final reports issued on time, averaging 16 days for processing, and issued 10 immediate action directives for urgent risks. Inspection findings are categorized by severity, ranging from minor administrative lapses to critical security vulnerabilities, informing enforcement actions such as teaching letters, corrective action plans, or suspensions. Audit processes complement inspections through ongoing federal monitoring and entity self-audits of records, such as transfer logs and destruction certifications, to detect discrepancies in possession or reporting. The U.S. Department of Health and Human Services Office of Inspector General (OIG) provides additional oversight, reviewing FSAP's compliance verification for registered entities, which numbered 226 in 2023. Annual FSAP reports detail inspection outcomes, including common deviations like inadequate training documentation or inventory inaccuracies, to guide program improvements.

Notable Violations and Incidents

In 2014, the Centers for Disease Control and Prevention (CDC) experienced a significant biosafety lapse when laboratory personnel in a Biosafety Level 3 (BSL-3) facility failed to fully inactivate Bacillus anthracis spores during preparation of extracts for research, potentially exposing up to 84 staff members to live between June 6 and June 13. The incident stemmed from deviations from standard inactivation protocols and inadequate verification of spore viability, prompting an internal CDC that identified gaps in , communication, and procedural adherence, leading to temporary suspension of high-containment activities and enhanced safety reforms across CDC labs. No clinical illnesses resulted from the exposure, but prophylactic antibiotics were administered to affected personnel. In May 2015, the U.S. Army's Dugway Proving Ground in Utah shipped live Bacillus anthracis spores—intended to be inactivated via irradiation—to 194 laboratories and facilities across nine U.S. states and one overseas military base, due to insufficient post-treatment viability testing that failed to detect surviving spores. Subsequent investigations revealed systemic issues in inactivation validation, with 17 of 33 tested batches from Dugway's inventory confirming live growth, resulting in heightened decontamination efforts at recipient sites, no reported human or animal exposures, and a Department of Defense-wide overhaul of protocols including improved testing rigor and inventory audits. Enforcement actions have addressed various failures, such as a settlement where a Florida-based paid $100,000 to resolve allegations of violating select agent regulations, including failures in accuracy and measures for registered toxins. Similarly, a Wisconsin laboratory agreed to a $30,000 civil monetary penalty in an earlier case for permitting unauthorized access to areas storing select agents and toxins, breaching security requirements under 42 CFR Part 73. Broader data from Federal Select Agent Program reports indicate over 1,100 incidents involving select agents from 2003 to 2013, encompassing laboratory-acquired infections (e.g., cases in 2010), environmental releases (e.g., a 2008 outbreak in adjacent leading to a $425,000 fine and suspension), and security deficiencies, though specifics on many cases remain classified to mitigate risks. These events underscore persistent challenges in balancing needs with , prompting iterative regulatory tightening by the CDC and USDA.

Penalties and Corrective Actions

The Federal Select Agent Program (FSAP) employs a graduated approach to address regulatory departures identified during inspections, categorizing violations by severity to determine appropriate responses. Low-severity departures, such as minor recordkeeping inaccuracies, typically result in routine notifications without immediate penalties. Moderate-severity issues, like incomplete training, may prompt recommendations for voluntary remediation. Serious departures posing imminent risks, including unauthorized possession or breaches, trigger immediate action reports and potential cessation of activities. Corrective actions form the primary mechanism for resolving non-compliance, emphasizing risk mitigation over punishment for entities demonstrating . Entities receive an "opportunity to show cause" letter outlining deficiencies, after which they submit a Corrective Action Plan () addressing root causes, timelines, and verification methods. CAPs must typically be resolved within 30 days, with progress reports submitted to FSAP; failure to comply escalates to formal . For high-risk scenarios, such as failures in controls, FSAP may mandate interim measures like enhanced monitoring or work stoppages while allowing secure storage of agents to prevent release or theft. Civil money penalties (CMPs) are imposed by the Department of Health and Human Services Office of Inspector General (HHS OIG) for violations of select agent regulations under 42 CFR part 73 or the Public Health Security and Bioterrorism Preparedness and Response Act of 2002. The maximum penalty is $250,000 per violation for individuals or $500,000 for entities, adjusted annually for inflation pursuant to 42 CFR § 1003.210; amounts are determined based on factors including severity, intent, history of violations, and cooperation. In practice, settlements have ranged from $30,000 for isolated lapses, such as improper transfer documentation, reflecting negotiated resolutions rather than maximum fines. Criminal penalties apply to knowing violations, with FSAP referring cases to the (FBI) for prosecution under statutes like 18 U.S.C. § 175 (prohibiting possession for use as a ) or 42 U.S.C. § 262a. These can include fines and up to five years for unauthorized possession or transfer, escalating to life if linked to intent. In severe cases, FSAP issues entity-wide suspensions via cease-and-desist orders, halting all select agent activities until is restored, though secure is permitted. Revocations terminate registration entirely when an entity demonstrates inability to maintain or , as determined under 42 CFR § 73.8 or equivalent USDA provisions, barring future involvement without reapplication and approval.

Recent Developments

Biennial Reviews and List Updates

The Federal Select Agent Program, jointly administered by the U.S. Department of Health and Human Services (HHS) and the U.S. Department of Agriculture (USDA), mandates biennial reviews of the select agents and toxins lists under the Public Health Security and Bioterrorism Preparedness and Response Act of 2002 and the Agricultural Bioterrorism Protection Act of 2002. These reviews evaluate whether listed agents continue to pose a severe threat based on criteria including the potential for mass casualties or economic disruption through dissemination, ease of production and delivery as a weapon, and the availability and effectiveness of medical or agricultural countermeasures. Assessments incorporate input from subject matter experts, public comments, and advances in diagnostics, vaccines, and surveillance to determine if agents should be added, removed, or modified. The most recent biennial review cycle, culminating in proposals published on January 30, 2024, resulted in a final HHS on December 17, 2024, and a parallel USDA , both effective January 16, 2025. No agents were added to the lists; instead, five were removed to alleviate regulatory burdens on research while preserving , reflecting evaluations that risks had diminished due to improved controls and countermeasures. Key removals included:
  • Overlap agents (HHS/USDA): , Brucella melitensis, and Brucella suis, delisted due to low human case incidence (fewer than 100 annually in the U.S., mostly occupational), absence of human-to-human transmission, effective antibiotics and s, and robust veterinary surveillance reducing zoonotic spillover.
  • USDA veterinary agent: African horse sickness virus, removed to facilitate vaccine and diagnostic development amid effective international controls limiting U.S. introduction risks.
  • USDA plant agent: Peronosclerospora philippinensis (also known as Peronosclerospora sacchari), delisted following assessments of limited U.S. agricultural impact and available phytosanitary measures.
Additional modifications encompassed designating Nipah virus as a Tier 1 overlap agent owing to its high case fatality rate (40-100%), aerosol transmissibility, and lack of approved countermeasures; increasing the exclusion threshold for short, paralytic alpha conotoxins from 100 mg to 200 mg based on updated lethality modeling; and updating nomenclature for precision, such as renaming "Ebola virus" to "Ebolavirus" and "SARS coronavirus (SARS-CoV)" to "Severe acute respiratory syndrome coronavirus (SARS-CoV)." Proposals to add certain hantaviruses (e.g., Sin Nombre virus) were rejected due to insufficient evidence of severe threat potential under dissemination criteria. These updates processed over 37 public comments, prioritizing empirical risk data over unsubstantiated concerns. Earlier biennial reviews, such as the cycle documented in FSAP annual reports, focused on without major list alterations, as no agents met revised criteria for change amid stable threat assessments. The 2024-2025 updates represent the first significant delistings since , driven by multi-year expert deliberations emphasizing causal reductions in agent risks through technological and programmatic advancements.

2023-2025 Regulatory Changes

In March 2023, the Department of Health and Human Services (HHS) through the Centers for Disease Control and Prevention (CDC) published a final rule confirming the addition of SARS-CoV/SARS-CoV-2 chimeric viruses to the HHS select agents and toxins list. These viruses, defined as those resulting from any deliberate manipulation of SARS-CoV-2 to express the full or partial spike protein from SARS-CoV or another SARS-related coronavirus outside the receptor-binding domain, were included due to experimental evidence indicating potential for increased transmissibility or pathogenicity in mammalian models, posing a severe threat to public health. The rule adopted the prior interim final rule without modification, requiring registration and compliance for possession, use, or transfer by affected entities. On January 30, 2024, HHS/CDC and the U.S. Department of Agriculture's Animal and Plant Health Inspection Service (USDA/APHIS) proposed revisions to select agent regulations as part of the biennial review mandated under 42 U.S.C. § 262a, including potential enhancements to and requirements such as updated risk assessments for viable organisms and clarification of security planning for storage. These proposals aimed to balance risk mitigation with reduced burdens on low-risk activities, but a separate final rule addressing these non-list regulatory elements remained pending as of late 2024. In December 2024, HHS/CDC finalized a rule effective January 16, 2025, implementing select modifications beyond list alterations, including an increase in the exclusion limit for short, paralytic alpha conotoxins from 100 mg to 200 mg based on toxicity data showing negligible dissemination or risk at the higher threshold. The rule also standardized nomenclature across entries—such as renaming " coronavirus (-CoV)" to "Severe acute respiratory syndrome coronavirus (-CoV)" and " virus" to ""—to reflect current Committee on of Viruses (ICTV) classifications, facilitating consistent regulatory application without altering agent status. Coordinated USDA changes removed certain agents from the Veterinary Services list effective the same date, streamlining overlapping oversight. No further substantive regulatory amendments were enacted through October 2025.

Criticisms and Reforms

Burdens on Scientific

The Federal Select Agent Program (FSAP), administered jointly by the USDA and HHS, imposes stringent registration, , and transfer requirements on laboratories handling select agents and toxins, which stakeholders report create substantial administrative burdens that delay timelines. Approvals for personnel suitability assessments can take 3 to 24 months, deterring students and postdocs from entering the field and hindering project initiation. Inventory tracking and documentation demands often require dedicated full-time staff, with inconsistent interpretations across agencies like CDC and USDA exacerbating paperwork overload and inspection delays of six months or more. Financial costs associated with , particularly for agents, have escalated to levels that prompt institutions to forgo research altogether, as security enhancements such as armed guards can exceed $3 million annually and overall study expenses rise 2- to 5-fold due to facility upgrades and training. Manufacturers of veterinary and diagnostics have cited these rising compliance expenses, combined with low profit margins, as reasons for ceasing production, potentially undermining preparedness. Food processing labs handling agents like species have similarly reduced operations, with 2024 biennial review commenters arguing that such designations impose undue burdens impairing essential research without commensurate risk reduction. Operational constraints limit and , as transfer protocols and clearance mandates reduce inter-institutional partnerships and exchanges, affecting % of postdocs who are foreign nationals subject to heightened scrutiny. Regulations have led to the destruction of valuable microbial collections, including strains and Newcastle disease virus isolates, at unregistered facilities unable to navigate transfer ambiguities, resulting in irreplaceable losses for strain diversity studies. Scientific output suffers, evidenced by fewer publications on select agent strains compared to non-regulated counterparts, alongside smaller project scales and fewer registered entities—over 300 institutions and 13,000 individuals from 2004–2010, with trends indicating further decline due to avoidance. Stakeholders, including researchers and labs, describe a "love-hate" dynamic with the program: while acknowledging its intent, they criticize its bureaucratic rigidity for driving talent overseas and stifling domestic competitiveness, as U.S. rules exceed international norms. Recommendations from advisory panels include expedited approvals, portable assessments, and targeted exemptions for lower- activities to alleviate burdens without diluting oversight. These impacts, documented in government-commissioned reviews and analyses, highlight tensions between and viability, particularly for agents like where ongoing inclusion despite burden complaints perpetuates inefficiencies.

Effectiveness and Persistent Lapses

The Federal Select Agent Program has demonstrated effectiveness in preventing thefts of regulated biological select agents and toxins, with no reported instances of such thefts occurring since the program's , and the vast majority of documented losses attributed to recordkeeping discrepancies rather than breaches. This record suggests robust protocols in deterring unauthorized diversions, as losses have not indicated compromise or external threats. Additionally, the program facilitates critical research yielding advancements in detection, diagnostics, and countermeasures, balancing with scientific progress across approximately 250 entities handling 63 agents and toxins as of 2025. Despite these strengths, persistent lapses in safety and compliance undermine overall efficacy, with recurring incidents highlighting gaps in oversight and accountability. For instance, a 2015 incident at a Department of Defense laboratory involved the inadvertent shipment of live spores—intended to be inactivated—to over 190 facilities worldwide, exposing potential vulnerabilities in inactivation verification processes. Similarly, in 2016, a private laboratory shipped toxic to a U.S. training center on multiple occasions dating back to 2011, revealing failures in toxin handling and transfer protocols. A 2016 federal report documented 12 select agent losses in high-containment labs, including nine due to recordkeeping errors and three from mistaken destruction, underscoring ongoing issues with inventory accuracy. Government Accountability Office (GAO) evaluations have identified systemic weaknesses, such as the program's lack of a formal risk-based inspection strategy, leading to uneven targeting of high-risk activities and delays in 27 percent of Centers for Disease Control and Prevention (CDC) inspections exceeding 30-day targets in 2016. Enforcement inconsistencies persist, with only one suspension of a federal laboratory registration out of ten total actions from 2003 to 2016, despite evidence of self-inspections by the Animal and Plant Health Inspection Service (APHIS) on its own facilities in violation of interagency agreements. Workforce shortages, including seven vacancies at CDC out of 51 positions in 2017, and inadequate joint training plans further hamper consistent implementation. Between January and December 2018, regulators received eight reports of biological select agent and toxin incidents, including lapses in storage and shipping. Recent data indicate these issues endure into the 2020s, with a 2022 settlement by a laboratory paying $30,000 for select agent regulation violations, and a 2025 analysis noting continued incidents tied to storage protocols and a compliance-focused approach that prioritizes procedural adherence over enhanced and . The 2024 Federal Select Agent Program , released in September 2025, summarizes ongoing compliance monitoring but does not quantify reductions in violations, suggesting that while reactive measures address individual cases, structural reforms recommended by —such as assessments and improved planning—remain unimplemented, perpetuating vulnerabilities in high-containment operations.

Debates on Overregulation vs.

Critics of the Select Agent Program argue that its stringent requirements impose excessive administrative and financial burdens on legitimate scientific , potentially hindering advancements in and . For instance, compliance involves rigorous security protocols, personnel reliability screenings, and facility inspections that can delay experiments and increase operational costs, with some institutions reporting that the paperwork and approval processes for transfers alone consume hundreds of hours annually. A 2015 notice solicited public input on these impacts, highlighting concerns that overbroad categorization of agents as "select" captures pathogens with manageable risks under existing levels, diverting resources from high-priority threats. Proponents of , including some experts, contend that such measures foster a risk-averse culture that discourages innovative on dual-use technologies, as evidenced by slowed progress in and vaccine development where select agent status triggers unnecessary hurdles. Advocates for robust regulation emphasize that the program's controls are essential to mitigate catastrophic risks from or accidental releases, given the inherent dangers of agents capable of causing mass casualties. Established under the USA PATRIOT Act of 2001 and the Public Health Security and Preparedness and Response Act of 2002, the program has inspected over 300 registered entities and prevented unauthorized access through background checks on more than 20,000 individuals since inception, thereby enhancing national security without documented major breaches attributable to regulatory lapses. Empirical assessments, such as those from the National Academies, affirm that these safeguards provide tangible benefits by standardizing security in high-containment labs (BSL-3 and BSL-4), where lapses like the 2014 CDC exposures underscored the need for vigilance against threats or procedural errors. While acknowledging administrative inefficiencies, security-focused analyses argue that weakening rules could invite exploitation by non-state actors, as historical precedents like the demonstrate the feasibility of weaponizing regulated pathogens. Ongoing debates center on biennial reviews intended to refine the select agent list by removing low-risk entries, yet has been cautious, with only modest delistings since , fueling arguments for tiered risk assessments to alleviate burdens without compromising security. Reports from bodies like the Federal Experts Security Advisory Panel recommend mechanisms for expedited approvals during emergencies, such as pandemics, to balance agility with oversight, but critics note persistent gaps in evaluating the program's net effectiveness against evolving threats like . analyses identify opportunities for targeted mitigations, such as improved risk modeling, to address both overregulation complaints and unresolved vulnerabilities in personnel reliability. This tension reflects a causal : stringent rules demonstrably reduce misuse probabilities but at the cost of , with no on optimal calibration amid biased institutional incentives favoring caution over empirical cost-benefit scrutiny.

Former Select Agents

Agents Removed and Rationales

Several biological agents have been removed from the Select Agents and Toxins List through the Federal Select Agent Program's biennial reviews, which evaluate whether they continue to pose a severe threat to public health, animal health, plant health, or agricultural productivity based on factors including pathogenicity, transmissibility, availability of countermeasures, and incidence of misuse. Removals are infrequent, as the list prioritizes agents with high-risk profiles, but delistings occur when empirical assessments demonstrate reduced risk profiles, often supported by advances in diagnostics, vaccines, or therapeutics that mitigate potential impacts. In the most recent updates, effective January 16, 2025, the U.S. Department of Health and Human Services (HHS) removed three overlap select agents—Brucella abortus, Brucella melitensis, and Brucella suis—from its list following a biennial review informed by peer-reviewed scientific data and public input (37 comments in favor, none opposed). These bacterial species, which cause brucellosis primarily through zoonotic transmission from infected animals, were delisted due to their low human mortality rates (typically under 2% with treatment), absence of sustained human-to-human transmission, and the effectiveness of antibiotics such as doxycycline and streptomycin, which achieve cure rates exceeding 90% in uncomplicated cases. The review concluded that their biosecurity risks are minimal, as no deliberate misuse incidents have been documented, and retention on the list imposed undue regulatory burdens on research into vaccines and diagnostics without commensurate safety gains. Concurrently, the U.S. Department of Agriculture's Animal and Plant Health Inspection Service (APHIS) removed the same three Brucella species (as overlap agents), along with African horse sickness virus and Peronosclerospora philippinensis (a plant pathogen causing downy mildew in corn), totaling five delistings from its regulated list. For African horse sickness virus, an orbivirus affecting equids with mortality rates up to 90% in horses but no established U.S. reservoirs or vectors, removal was justified by the biennial assessment of limited domestic threat, effective veterinary countermeasures like vaccination, and the need to facilitate research on outbreak prevention without heightened security requirements. Similarly, Peronosclerospora philippinensis was delisted due to its absence from U.S. agriculture, low economic impact potential given resistant crop varieties, and the assessment that it no longer meets criteria for severe threat to plant health or products. These actions, stemming from proposed rules in January 2024 and finalized after public comment review, aim to streamline oversight while preserving biosafety recommendations (e.g., BSL-3 for Brucella work remains advised). Prior to 2024, full delistings were rare, with most adjustments involving exclusions of attenuated strains rather than wholesale removals; for instance, a 2017 review proposed but ultimately deferred changes to several agents pending further data, reflecting cautious application of risk-based criteria. This history underscores that removals require rigorous evidence of diminished threat, balancing national security with empirical advancements in pathogen control.
AgentAgencyKey Rationales for Removal
, B. melitensis, B. suisHHS & APHIS (overlap)Low mortality (<2%), no human-to-human transmission, effective antibiotics (>90% cure rate), no misuse history, enables /diagnostic research, reduces regulatory burden.
horse sickness virusAPHISHigh equid mortality but no U.S. presence, available , low deliberate misuse risk, supports development.
Peronosclerospora philippinensisAPHISNo U.S. occurrence, resistant crops mitigate impact, fails severe threat criteria for plant health/products.

Implications for Ongoing Oversight

The delisting of former select agents, such as the three species (B. abortus, B. suis, and B. melitensis) removed in December 2024, underscores the necessity for adaptive oversight frameworks beyond rigid select agent regulations. These removals, justified by assessments of attenuated misuse potential, effective treatments, and limited transmission risks, transition affected pathogens to standard (BSL) protocols rather than Tier 1 security measures. However, ongoing oversight must incorporate surveillance of emerging strains, antibiotic resistance patterns, and global incidence data to detect any shifts warranting re-listing, as biennial reviews by the Federal Select Agent Program (FSAP) explicitly evaluate such dynamic threats. Post-delisting, implications extend to enhanced capacity without FSAP's full registration and transfer restrictions, potentially accelerating and diagnostic for diseases like , which affect and pose zoonotic risks. Public comments during the 2024 review affirmed that these changes preserve nationally recognized practices in U.S. laboratories, mitigating concerns over reduced protections. Yet, causal analysis reveals that delisting could inadvertently lower scrutiny in non-federally regulated settings, necessitating robust integration with broader monitoring systems, such as those under the CDC's Emerging Program, to track inadvertent releases or natural outbreaks. Long-term oversight challenges include balancing delisting's research benefits against persistent biosecurity gaps, as evidenced by historical lapses in agent tracking even under stringent rules. FSAP's authority to reinstate agents based on new —such as advancements or epidemiological shifts—highlights the program's role in causal risk reassessment, ensuring that removals do not erode . This approach prioritizes data-driven adjustments over static regulation, though it demands verifiable inactivation validation and inter-agency coordination between HHS/CDC and USDA/APHIS to prevent regulatory silos.