Trump Signs Executive Order Fast-Tracking Psychedelic Drug Reviews, With Joe Rogan at His Side

On April 18, 2026, President Donald Trump signed an executive order directing the FDA to accelerate its review of psychedelic drugs designated as breakthrough therapies, committing $50 million in federal matching funds for state-level research programs, and opening a right-to-try pathway for ibogaine — a psychoactive compound derived from an African shrub that remains a Schedule I controlled substance [1][2]. The signing ceremony featured an unusual guest list: Health Secretary Robert F. Kennedy Jr., FDA Commissioner Marty Makary, former Navy SEAL Marcus Luttrell, and podcaster Joe Rogan, who told reporters he had texted Trump about ibogaine and received the reply, "Sounds great. Do you want FDA approval? Let's do it" [3].

"If these turn out to be as good as people are saying, it's going to have a tremendous impact," Trump said at the signing [1].

The order represents the most significant federal action on psychedelic medicine to date. It also raises difficult questions: whether the White House is directing scientific review that should remain independent, whether the clinical evidence is strong enough to justify accelerated approval, and who will actually be able to afford these treatments.

What the Executive Order Does

The order contains several distinct provisions [4][2]:

Commissioner's National Priority Vouchers (CNPV): The FDA will issue priority vouchers for three psychedelic drug candidates, reducing new drug application review timelines from the standard 10–12 months to as little as 1–2 months. Additional vouchers will be available for drugs holding Breakthrough Therapy Designation. This is the first time the FDA has offered this fast-tracking mechanism to psychedelics [2][4].

Federal Research Funding: The Advanced Research Projects Agency for Health (ARPA-H) is directed to provide $50 million in match-funding for state investments in psychedelic research, drawn from the existing EVIDENT initiative, a $100 million mental health program. Texas, which passed its own $50 million ibogaine research bill, is the initial beneficiary [2][4].

Expedited DEA Rescheduling Reviews: The Attorney General is directed to begin DEA scheduling reviews after Phase 3 trial completion but before the FDA renders its approval decision — a change from the current sequential process that aims to eliminate up to three months of regulatory lag [2].

Right-to-Try Expansion: The order clarifies that Schedule I substances are accessible under the Right to Try Act, enabling eligible patients with treatment-resistant conditions to access experimental psychedelic therapies under medical supervision [2].

IND Clearance for Ibogaine: FDA Commissioner Makary announced investigational new drug clearance for ibogaine, permitting U.S. clinical trials to formally begin [2][4].

Which Compounds Hold Breakthrough Therapy Designation

The FDA's Breakthrough Therapy Designation (BTD) — a status created in 2012 to speed development of drugs for serious conditions where preliminary evidence shows substantial improvement over existing treatments — has been granted to five psychedelic-related compounds [5][6][7]:

• MDMA (Lykos Therapeutics) for PTSD, designated in 2017
• Psilocybin (Compass Pathways) for treatment-resistant depression, designated in 2018
• Psilocybin (Usona Institute) for major depressive disorder, designated in 2019
• CYB003, a deuterated psilocybin analogue (Cybin Inc.) for major depressive disorder, designated in 2024
• MM120/LSD D-Tartrate (MindMed) for generalized anxiety disorder, designated in 2024

Source: FDA / Psychedelic Alpha

Data as of Apr 18, 2026CSV

Ibogaine does not currently hold BTD status. Its inclusion in the executive order — with IND clearance and right-to-try access — represents a distinct pathway from the breakthrough therapy process applied to the other compounds.

The MDMA Precedent: Can an Executive Order Override an FDA Rejection?

The executive order arrives less than two years after the FDA issued a Complete Response Letter to Lykos Therapeutics in August 2024, declining to approve MDMA-assisted therapy for PTSD [8]. An independent FDA advisory panel had voted 9–2 against supporting MDMA's effectiveness and 10–1 that its benefits did not outweigh risks, citing concerns about clinical trial methodology and data reliability [8][9].

The advisory committee flagged several problems: potential ethical violations in clinical trials, questions about functional unblinding (participants knowing whether they received MDMA or placebo), and the difficulty of separating drug effects from the intensive psychotherapy that accompanied each session [9][10]. Lykos subsequently reduced its workforce by 75% and entered discussions with the FDA about a potential additional Phase 3 study [11].

The executive order does not explicitly direct the FDA to reverse its MDMA decision. However, the CNPV mechanism and expedited review timelines apply to any compound with BTD status — which MDMA still holds. Legal scholars have debated whether White House direction of FDA scientific review compromises the agency's independence. The FDA has historically operated with substantial autonomy in drug approval decisions, and direct presidential involvement in specific drug reviews is rare [12].

Supporters of the order argue it removes bureaucratic delays without overriding scientific standards. Critics counter that compressing review timelines from 10–12 months to 1–2 months fundamentally changes the rigor of the evaluation process.

The Blinding Problem: A Structural Challenge for Psychedelic Trials

The strongest scientific objection to accelerating psychedelic approvals centers on a methodological challenge that has no easy solution: participants in psychedelic trials almost always know whether they received the drug [13][14].

The subjective effects of a full-dose psychedelic — altered perception, emotional intensity, visual distortion — are so pronounced that conventional placebo-controlled trial designs break down. When participants know they received the active drug, their expectations can inflate reported benefits. When participants know they received the placebo, disappointment can deflate their outcomes. This "functional unblinding" makes it structurally difficult to establish efficacy through the standard randomized controlled trial framework that the FDA applies to other drugs [13][14].

Researchers have proposed several partial solutions: using active placebos (low-dose psychedelics or other psychoactive substances), recruiting participants with no prior psychedelic experience, employing independent raters blind to treatment assignment, and developing statistical models that account for expectancy effects [13]. But none of these fully resolve the problem, and the FDA's advisory committee cited blinding concerns as a factor in its MDMA rejection [9].

The executive order does not specify what methodological standards the FDA review will apply, nor does it address the blinding critique directly. Whether the CNPV review process will apply the same evidentiary bar as a standard review — or a reduced one — remains unclear.

Who Is Behind the Order: Rogan, Perry, and the Ibogaine Lobby

Joe Rogan's presence at the signing was not incidental. The podcaster had become increasingly vocal about his frustrations with Trump's domestic and foreign policy decisions, and the executive order was widely reported as an effort by the administration to repair that relationship [3][15].

Rogan has featured ibogaine advocacy prominently on his podcast. Former Texas Governor Rick Perry, who co-founded a group called Americans for Ibogaine, appeared on Rogan's show twice in two years to advocate for reducing federal restrictions on the drug [3]. Bryan Hubbard, CEO of Americans for Ibogaine, was present at the signing ceremony alongside Rogan and Mehmet Oz, the administrator for the Centers for Medicare and Medicaid Services [3][15].

The commercial psychedelic therapy market is projected to reach $7.8 billion by 2030 and $12.9 billion by the mid-2030s, growing at a compound annual rate of roughly 13–16% [16][17]. In 2025, AbbVie entered a deal worth up to $1.2 billion for a psychedelic asset targeting depression, the largest transaction in the sector to date [18].

Source: Precedence Research / Mordor Intelligence

Data as of Apr 18, 2026CSV

Venture capital has been the primary funding source for psychedelic startups, with the high-risk, high-reward profile of the sector making it a better fit for VC than private equity, according to industry analysts [18]. The executive order's provisions — particularly accelerated FDA review and right-to-try access — directly benefit the companies developing these compounds.

Veterans: The Most Visible Beneficiaries

Military veterans with treatment-resistant PTSD have been the most politically compelling advocates for psychedelic therapy. Marcus Luttrell told Trump at the signing, "It absolutely changed my life for the better" [1].

The Department of Veterans Affairs has approximately 30 ongoing psychedelic studies across VA sites and has expanded psychedelic-assisted therapy trials to nine VA facilities for PTSD, treatment-resistant depression, and anxiety disorders [19][20]. The VA also funds MDMA and psilocybin research directly — a first for the agency [19].

Existing compassionate-use and expanded-access pathways have allowed some veterans to receive MDMA-assisted therapy, but these mechanisms are limited by scale. They require individual patient applications, physician sponsorship, and FDA authorization for each case — a process that can take months and is inaccessible to most veterans who lack connections to participating research institutions [21]. Nonprofits like the Heroic Hearts Project and VETS have filled part of this gap by funding veterans to travel to countries where psychedelic therapy is legal, but this approach is inherently limited to those who can travel and who learn about these programs [22][23].

The executive order's right-to-try provision for ibogaine could expand access for veterans with treatment-resistant conditions, but the right-to-try framework requires that a drug has completed Phase 1 trials and be in an active investigational process — a threshold ibogaine had not cleared in the U.S. until the IND clearance announced alongside the order [2].

Safety Concerns: Ibogaine's Track Record

Ibogaine occupies a different risk category than psilocybin or MDMA. The compound has been linked to more than 30 deaths, primarily from fatal cardiac arrhythmias [4][24]. Frederick Barrett, a Johns Hopkins researcher, noted the historical difficulty of studying ibogaine precisely because of its cardiovascular toxicity [4].

A recent Stanford study of 30 veterans who received ibogaine treatment in Mexico reported improvements in PTSD and traumatic brain injury symptoms, but the study lacked a placebo comparison group, limiting the strength of its conclusions [4]. The IND clearance announced by Commissioner Makary will permit controlled U.S. trials — but the right-to-try pathway opens access before those trials produce safety data from a U.S. regulatory context.

International Comparison: Australia and Canada

Australia became the first country to permit prescribed psilocybin and MDMA therapy in July 2023, through a decision by the Therapeutic Goods Administration (TGA) [25]. More than 180 patients have received treatment under the program, supported by over 50 trained psychiatrists. Australian regulators have recorded zero serious adverse events across the program [26].

However, uptake has been slow. Barriers include a shortage of qualified clinical staff, the absence of standardized training programs, and high costs — roughly $30,000 AUD ($19,000 USD) for a three-dose MDMA therapy program [25][26]. More than half of MDMA-treated patients reported significant relief from PTSD symptoms, but critics have noted that the two-year-old program has not produced the kind of large-scale, controlled data that would satisfy FDA-level scrutiny [27].

Canada has taken a narrower approach through Section 56 exemptions under the Controlled Drugs and Substances Act, which allow the Health Minister to grant individual patient access for medical or scientific purposes [28]. Over 100 Canadians have received compassionate access to psilocybin since 2020, initially limited to palliative patients with end-of-life distress [28][29]. A longitudinal study of these patients found that the lack of standardization — in therapist training, safety assessments, and inclusion criteria — introduced risks exceeding those observed in controlled clinical settings, with one in eight participants reporting worsening symptoms across several psychological domains [30].

These international experiences suggest both the promise and the limits of accelerated access: clinical improvements are real for many patients, but the absence of rigorous controls creates uncertainty about the size of the treatment effect and the frequency of adverse outcomes.

Rescheduling: The Legal Bottleneck

Even if the FDA approves a psychedelic compound, it remains a Schedule I controlled substance until the DEA acts. The Controlled Substances Act provides three rescheduling pathways: legislative action by Congress, an administrative process initiated by the DEA or HHS, or a judicial challenge after a denied scheduling petition [31][32].

The administrative pathway — the most likely route — requires HHS to provide a scientific and medical evaluation, followed by a DEA notice of proposed rulemaking, a public comment period, and a final rule. For cannabis, this process took more than two years from the initial HHS recommendation [33]. The executive order attempts to compress this timeline by directing the Attorney General to begin DEA reviews concurrently with late-stage FDA review rather than sequentially — but it cannot eliminate the notice-and-comment requirements mandated by the Administrative Procedure Act [2][31].

Legal experts have noted that an executive order cannot compel DEA rescheduling without the statutory process. What it can do is signal administration priorities and direct agencies to act with urgency within existing legal frameworks [31][32]. The precedent of cannabis rescheduling — which remains incomplete as of early 2026 — suggests the process will take months at minimum, regardless of executive direction.

Who Pays: The Access Question the Order Does Not Answer

Psychedelic-assisted therapy is expensive. A treatment course involving multiple supervised sessions with a licensed therapist typically costs $5,000–$15,000 out of pocket [34]. In Australia, comparable programs run as high as $19,000 USD [26].

The executive order contains no directive on insurance coverage, VA reimbursement rates, or equity of access [2]. As long as psychedelics remain Schedule I — which they will until the rescheduling process concludes — federal and private insurers cannot reimburse for their use. The American Medical Association has introduced preliminary Category III CPT billing codes for psychedelic-assisted therapy, but these are not yet reimbursable under Medicare, Medicaid, or private insurance [34][35].

The VA has covered ketamine therapy for some veterans at participating facilities, but this coverage is not universal and does not extend to other psychedelics [36]. Enthea, a private company, offers employers ketamine-assisted psychotherapy health plans, representing an early experiment in employer-sponsored coverage [34].

If accelerated approval proceeds without a corresponding insurance or reimbursement framework, the immediate beneficiaries will be patients who can pay out of pocket — a population that does not overlap significantly with the veteran and treatment-resistant PTSD communities most often cited in support of the policy.

What Comes Next

The executive order sets several near-term milestones: FDA issuance of priority vouchers within a week, the beginning of U.S. ibogaine clinical trials under the new IND clearance, and the start of concurrent DEA scheduling reviews [2]. The $50 million in ARPA-H matching funds will flow first to Texas's ibogaine program [2][4].

The broader questions — whether compressed FDA review timelines will produce approvals that meet established evidentiary standards, whether the rescheduling process will move faster than the cannabis precedent suggests, and whether approved psychedelic therapies will be accessible to patients beyond those who can pay thousands of dollars out of pocket — will take months or years to answer.

What is clear is that the federal government's posture toward psychedelic medicine has shifted decisively. The policy consequences of that shift depend on details the executive order leaves unresolved.