Bipolar Disorder
Bipolar disorder is the area where the honest message about psychedelics is caution, not promise. Classic psychedelics such as psilocybin and LSD can trigger mania or hypomania, so people with bipolar disorder are excluded from almost every psychedelic trial, and combining them with lithium can cause seizures. The compound with real bipolar evidence is ketamine, used as a closely monitored, short-acting add-on to a mood stabiliser. One small, intensively supervised psilocybin trial in bipolar II is an early, fragile exception, not a green light.
How does psychedelic research approach bipolar disorder? Bipolar disorder involves episodes of depression alongside periods of elevated or irritable mood, and it needs careful management because some treatments can trigger mania. For this reason most psychedelic trials have excluded people with bipolar disorder, and the evidence is limited and cautious. Interest exists in the bipolar depression phase, where options are few, and small studies and case reports are beginning to explore ketamine and, more tentatively, psilocybin under close supervision. The central concern is safety: the risk that a psychedelic or rapid-acting antidepressant could destabilise mood. Open questions include who might be screened in safely and how to monitor for a switch into mania. Blossom tracks the trials, papers and safety signals behind bipolar disorder research so you can weigh the evidence carefully.
Data updated
Key Insights
- 1
This is a safety-first topic. The dominant finding is risk, not benefit: classic psychedelics (psilocybin, LSD, ayahuasca) can trigger manic, hypomanic or mixed episodes, and people with bipolar disorder are excluded from almost all modern psychedelic trials as a precaution.
- 2
A survey of 541 people with bipolar disorder who took psilocybin found about a third reported new or worsening symptoms afterwards, prominently manic symptoms, sleep problems and anxiety. Real-world use is not the same as a monitored trial.
- 3
Combining classic psychedelics with lithium, a first-line mood stabiliser, is specifically dangerous: an analysis of online reports found seizures in 47% of lithium-plus-psychedelic experiences, versus none with lamotrigine.
- 4
Ketamine is the only compound with a genuine bipolar evidence base. As a rapid-acting add-on to a mood stabiliser it reduces depressive symptoms and suicidal thoughts within hours (response around 60% vs about 5% on placebo), but the effect fades within one to two weeks and it is not a cure.
- 5
The one cautious classic-psychedelic exception is a single open-label trial of psilocybin in bipolar II depression (n=15) that saw large improvement with no mania under intensive supervision, but it is tiny, uncontrolled, bipolar II only, and a separate pilot did see hypomania, so it proves nothing yet.
By the numbers
- 51
- Trials tracked
- 125
- Papers tracked
- 6,662
- Trial participants
as of June 2026
as of June 2026
as of June 2026
Questions & Answers
The questions readers most often ask about Bipolar Disorder, answered with the data Blossom tracks.
Are psychedelics safe in bipolar disorder?
Most trials exclude people with bipolar disorder because of the risk that a psychedelic or rapid-acting antidepressant could trigger mania. Evidence is limited and cautious. Blossom tracks the safety signals.
Is any psychedelic studied for bipolar depression?
Small studies and case reports explore ketamine and, more tentatively, psilocybin under close supervision for the depressive phase. Blossom lists the relevant research.
What is Bipolar Disorder?
Bipolar disorder is a serious mood disorder defined by episodes of depression alternating with periods of mania or hypomania (abnormally elevated, energised or irritable mood). It affects around 40 million people worldwide[1] and is associated with a high risk of suicide. Bipolar I involves full manic episodes; bipolar II involves hypomania (a milder, shorter form) together with depression. That distinction matters a great deal on this page, because almost all of the limited psychedelic research is in bipolar II, the lower-risk form.
Most people with bipolar disorder spend far more time depressed than manic, and bipolar depression is notoriously hard to treat, which is why rapid-acting and novel treatments are of interest. But bipolar disorder is also the single population where psychedelics raise the most serious safety concerns, because the same serotonergic mechanism that may lift depression can also tip a vulnerable brain into mania. This page therefore leads with the risks, then describes the narrow, carefully bounded evidence, rather than the other way round.
A note on scope and tone: this is a research summary written to inform, not to encourage. Where the evidence supports caution or contraindication rather than treatment, that is what we say. Nothing here should be read as a suggestion that someone with bipolar disorder try a psychedelic, least of all outside a supervised clinical trial.
Current Treatments
The foundation of bipolar treatment is long-term mood stabilisation, usually with lithium, anticonvulsants such as valproate or lamotrigine, or atypical antipsychotics, combined with psychological support, sleep and routine management, and careful monitoring. Lithium in particular has strong evidence for preventing relapse and reducing suicide risk. Antidepressants are used cautiously and rarely alone, because they can themselves trigger a switch into mania.
Bipolar depression remains the harder half to treat, and the options that work for ordinary depression do not all transfer safely. That gap is the reason ketamine and, very tentatively, psilocybin are being studied here. But the bar for any new treatment in bipolar disorder is higher than usual: it must not destabilise mood. None of the compounds on this page is approved for bipolar disorder, and the classic psychedelics are investigational and, for most people with bipolar disorder, currently considered too risky to use outside a trial.
This report summarises what Blossom’s database shows about psychedelic and dissociative compounds in bipolar disorder, and it leads with the part that matters most: the risks. Bipolar disorder is the one population where the dominant, best-supported finding about classic psychedelics is not benefit but danger, the danger of triggering mania. The evidence for any benefit is narrow, early and confined to the lower-risk form of the illness, and the compound with the most support, ketamine, is a short-acting, closely monitored add-on rather than a cure. Read this as a map of where caution is warranted, not as encouragement.
A note before the evidence
This page is a research summary, not medical advice, and nothing here is a treatment recommendation. Bipolar disorder is a serious illness that needs specialist care; its treatment, including any decision about novel or rapid-acting medicines, belongs with a psychiatrist. Classic psychedelics can destabilise mood and trigger mania in people with bipolar disorder, and they can be dangerous in combination with common medicines such as lithium. Nobody with bipolar disorder should take a psychedelic to self-treat, and the supervised trials described here are not a model for doing so at home. If you are struggling, please contact your care team or a crisis service.
A word on the numbers. Blossom tracks 125 papers and 50 trials tagged to this topic, and those counts appear on this page. The tag is leaky: most of those papers are ketamine or esketamine studies in general or treatment-resistant depression that merely include or mention bipolar patients, plus mechanism and neuroimaging work. The genuinely bipolar-specific clinical core is small, on the order of twenty studies, and the controlled trials among them are smaller still. Read the counts as breadth of coverage, not as a deep bipolar evidence base.
The central issue: manic switch
The reason this page is framed around caution is mechanistic and well documented. The serotonergic action that may lift depression can also push a bipolar brain toward mania, and sleep loss during a long psychedelic experience compounds the risk. A survey of 541 people with bipolar disorder who had taken psilocybin found about a third reported new or worsening symptoms afterwards, prominently manic symptoms, difficulty sleeping and anxiety[1]. Published case reports document manic episodes triggered by ayahuasca in bipolar disorder[2], and mania following ibogaine use even in people with no prior bipolar diagnosis[3].
This is why bipolar patients are excluded from nearly every modern psychedelic-depression trial, and why a broad analysis of psychedelic adverse events found serious events concentrated in participants with pre-existing psychiatric conditions, including worsening mood, suicidal behaviour, psychosis and convulsions[4]. The favourable safety record often quoted for psychedelics comes from carefully screened, mostly healthy or unipolar volunteers, and does not transfer to bipolar disorder.
The lithium danger
One specific interaction deserves its own warning. Lithium is a first-line, life-saving mood stabiliser, and combining it with a classic psychedelic appears to be hazardous. An analysis of online experience reports found that of 62 cases combining lithium with a psychedelic, 47% involved seizures and a further 18% involved severe adverse experiences, while none of 34 reports combining lamotrigine with a psychedelic involved seizures[5]. The data come from unsupervised real-world use rather than a trial, but the signal is strong and biologically plausible, and it means the very medicine many people with bipolar disorder rely on makes psychedelic use markedly more dangerous.
Ketamine: the one real evidence base
Ketamine is the exception that genuinely helps, within limits. It is not a classic psychedelic but a dissociative anaesthetic, and in bipolar depression it is given as a single, monitored, rapid-acting add-on to a mood stabiliser. Two foundational randomised crossover trials at the US National Institute of Mental Health established the effect: the first (n=18) found 71% responded to ketamine versus 6% to placebo, with the difference peaking around day two[6], and the second (n=15) found rapid improvement in depression and suicidal ideation within 40 minutes[7].
A systematic review of six studies (135 patients, all maintained on a mood stabiliser) found about 61% responded to ketamine versus 5% to placebo, and manic symptoms in only one ketamine and one placebo participant[8], which is reassuring on switch risk in a monitored, mood-stabilised setting. The honest limit is durability: a pooled meta-analysis showed the antidepressant effect peaks at day one and loses its advantage by roughly day ten[9]. Ketamine buys rapid, short-term relief, including from suicidal crisis, but it is an adjunct that must be repeated, not a stand-alone or lasting treatment, and esketamine’s bipolar evidence is thinner still[10].
Psilocybin in bipolar II: the cautious exception
The single piece of controlled-ish classic-psychedelic evidence is an open-label trial of a single 25 mg dose of psilocybin in bipolar II depression (n=15), which reported a large improvement, a 24-point fall in MADRS depression scores at three weeks, with 12 of 15 responding and 11 in remission, and, importantly, no manic symptoms and no rise in suicidality[11]. It was conducted with intensive psychological support, careful screening, and medications withdrawn beforehand, and it is the reason the field is willing to test this carefully at all.
It must be read with its limits in full view. It enrolled 15 people, had no control group, was conducted at a single site, and, like every psilocybin bipolar study, was restricted to bipolar II, the lower-risk form. The safety picture is also not uniform: a separate open-label bipolar II pilot saw three participants develop suicidal ideation or hypomania, which resolved with support[12]. So the most that can honestly be said is that, in the lower-risk subgroup and under intensive supervision, a single psilocybin dose showed a large antidepressant signal without clear destabilisation in one small study, and that this is a reason to run proper controlled trials, not a reason to treat.
Bipolar II is not bipolar I
A point easily lost: every scrap of classic-psychedelic clinical data in bipolar disorder is in bipolar II, and that is deliberate. Bipolar II involves hypomania, which is milder and shorter than the full mania of bipolar I, so the consequences of a switch are less catastrophic and the researchers judged the risk just acceptable enough to study. Bipolar I, the higher-risk form, has essentially no controlled psychedelic data at all, and the manic-switch concern is correspondingly greater. Any cautious optimism from the bipolar II trials should not be generalised to bipolar I, where the honest stance remains that classic psychedelics are too risky to use outside the most carefully designed research.
Monitored trial versus real life
The single most important distinction on this page is between the supervised trial and the world outside it. The encouraging psilocybin result came from a setting with weeks of screening, withdrawn medications, two therapists, an eight-hour monitored session and structured follow-up. The discouraging survey result, a third of people reporting new or worsening, often manic, symptoms, came from people taking psilocybin in ordinary life. The lithium-seizure data is entirely from unsupervised use. The same drug, the same diagnosis, very different outcomes depending on the container. For bipolar disorder more than almost any other condition, the supervision is not optional packaging around the treatment; it is most of what makes the difference between a possible benefit and a serious harm.
Reading this honestly
So where does bipolar disorder sit? It is the clearest example in this whole field of why honest framing matters. There is a real, useful, short-term role for ketamine as a monitored add-on, and there is one small, fragile, genuinely interesting signal for psilocybin in bipolar II under intensive supervision. But the loudest and best-supported message in the literature is a warning: classic psychedelics can trigger mania, they are dangerous with lithium, they are untested in bipolar I, and the favourable safety story told elsewhere does not apply here. The right posture is neither dismissal of the early ketamine and psilocybin signals nor enthusiasm that ignores the hazard, but careful, supervised, lower-risk research and, for everyone else, caution. For people living with bipolar disorder, that caution is not the field being timid. It is the field taking their safety seriously.
Psychedelic Effect Matrix
Compound efficacy and evidence levels for Bipolar Disorder.
| Compound | Magnitude | Evidence | Consistency |
|---|---|---|---|
| Ketamine The best-evidenced compound here. As a rapid add-on to a mood stabiliser, single-dose IV ketamine reduces bipolar depression and suicidal ideation within hours (response around 60% vs about 5% on placebo across small RCTs), with manic switch rare. But the benefit fades within one to two weeks and it is adjunctive, not curative. | Medium | Moderate | Moderate |
| Esketamine Approved for unipolar treatment-resistant depression, not bipolar. Bipolar-specific data is naturalistic and small: real-world esketamine reduced suicidality with no clear difference from unipolar patients. Used adjunctively with mania monitoring; durability and bipolar-specific evidence are limited. | Medium | Low | Moderate |
| Psilocybin A single open-label bipolar II trial (n=15) reported large depression improvement with no mania under intensive supervision, but it is tiny, uncontrolled and bipolar II only; a separate pilot did see hypomania. There is essentially no controlled data in bipolar I, and manic-switch risk keeps it experimental. | Medium | Very Low | Low |
| LSD No clinical trials in bipolar disorder. The relevant evidence is the risk side: LSD’s long, intense action and serotonergic mechanism carry a recognised risk of triggering mania, so it is effectively contraindicated outside research. No demonstrated benefit. | None | Very Low | Low |
Ketamine and Bipolar Disorder
Ketamine is the only compound here with a real bipolar evidence base, and it is used in a very specific way: as a single, monitored, rapid-acting add-on to an existing mood stabiliser, not as a stand-alone treatment. Two small randomised crossover trials established the signal: a 2010 trial (n=18) found 71% responded to ketamine versus 6% to placebo[1], and a 2012 replication (n=15) found rapid improvement in both depression and suicidal ideation within 40 minutes[2].
A systematic review of six studies (135 patients, all on a mood stabiliser) found about 61% responded to ketamine versus 5% to placebo, with manic symptoms in only one ketamine and one placebo participant[3]. The crucial caveat is durability: a pooled meta-analysis showed the antidepressant effect peaks at day one and loses its advantage by about day ten[4]. Ketamine is a tool for rapid, short-term relief under supervision, not a lasting fix, and the mood-stabiliser backbone is part of why mania has stayed rare.
Esketamine and Bipolar Disorder
Esketamine (Spravato), the nasal-spray version of ketamine, is approved for treatment-resistant unipolar depression, not for bipolar disorder. The bipolar-specific evidence is thin and naturalistic rather than from dedicated trials: a real-world study of subcutaneous esketamine reduced suicidality within 24 hours, with no clear difference between bipolar and unipolar patients[1].
As with racemic ketamine, any use in bipolar disorder would be adjunctive, alongside a mood stabiliser and with close monitoring for switching. The honest position is that esketamine inherits ketamine’s rapid-but-short-lived profile, but has much less bipolar-specific evidence behind it, and is not approved or established for this condition.
Psilocybin and Bipolar Disorder
Psilocybin is the one classic psychedelic with any controlled bipolar data, and it comes with heavy qualifications. The key study is an open-label trial of a single 25 mg dose in bipolar II depression (n=15), which reported a large fall in depression (MADRS down 24 points at three weeks) with no manic symptoms and no increase in suicidality[1] under intensive psychological support and screening. It is genuinely encouraging, and genuinely fragile: tiny, uncontrolled, single-site, bipolar II only, with medications withdrawn beforehand.
The safety picture is not uniformly clean. A separate open-label bipolar II pilot saw three of its participants develop suicidal ideation or hypomania, which resolved with support[2], and every one of these studies deliberately enrolled bipolar II rather than the higher-risk bipolar I. Several larger trials are now under way, but until they report, psilocybin for bipolar disorder is an experimental signal in the lower-risk subgroup, not an established or safe treatment.
LSD and Bipolar Disorder
LSD has no clinical trials in bipolar disorder, so there is no efficacy story to tell. What the literature does contain is the risk side. Its long duration (up to about ten hours) and strong serotonergic action are exactly the features that make a manic switch plausible, and case reports document mania triggered by serotonergic psychedelics such as ayahuasca in people with bipolar disorder[1].
For practical purposes LSD is treated as contraindicated in bipolar disorder outside tightly controlled research, and no such research has produced bipolar efficacy data. Including it here is about being honest that the absence of benefit data sits alongside a real and specific hazard, not about suggesting a use.
Clinical Outlook
The near-term picture splits cleanly. Ketamine and esketamine will continue to be used and studied as rapid, adjunctive options for bipolar depression and acute suicidality, with the open questions being durability, maintenance dosing and how to deliver them safely. On the classic-psychedelic side, the field is taking the unusual step of cautiously testing psilocybin in bipolar II specifically, after a promising but small open-label trial[1], with several controlled trials now recruiting. Those results, not the current pilots, will determine whether there is a real and safe role here.
What is very unlikely to change soon is the caution around bipolar I and around unsupervised use. The safest reading of the trajectory is that any legitimate role for psychedelics in bipolar disorder will be narrow (lower-risk patients, intensive monitoring, mood-stabiliser cover) and slow to arrive, and that the gap between careful trial conditions and real-world use will remain the central safety problem. For most people with bipolar disorder, the evidence-based stance for the foreseeable future is caution.
Industrial Landscape
Bipolar disorder has a smaller and more cautious commercial landscape than depression, precisely because of the safety concerns. On the ketamine side, the work is largely academic and clinical, building on the foundational NIMH bipolar trials, with esketamine owned by Johnson & Johnson but approved only for unipolar depression. On the classic-psychedelic side, the notable mover is COMPASS Pathways, whose synthetic psilocybin funded the first controlled bipolar II trial[1], alongside academic groups running the cautious bipolar II studies.
Several developers that tested rapid-acting agents in bipolar II have pulled back, and bipolar I remains largely off-limits for classic-psychedelic development. The result is a field defined more by careful, mostly academic exploration in a narrow lower-risk subgroup than by a commercial race. For an honest broker, that restraint is appropriate: bipolar disorder is the population where moving slowly and screening carefully is not timidity but good medicine.
Quick Indicators
Related Topics
Organisations
Search →Janssen Research & Development
Janssen Research & Development is the pharmaceutical research and development arm of Johnson & Johnson (J&J). Operating under J&J's Innovative Medicine division, Janssen has sponsored clinical trials into ketamine-derived compounds, including esketamine (Spravato), the first FDA-approved psychedelic-adjacent treatment for treatment-resistant depression.
COMPASS Pathways
COMPASS Pathways is a UK-listed biopharmaceutical company developing COMP360 synthetic psilocybin therapy for treatment-resistant depression, with two successful Phase 3 trials making it the leading candidate for the first regulatory approval of a classic psychedelic medicine.
University of British Columbia
The University of British Columbia is a Canadian public research university with major campuses in Vancouver and the Okanagan. Its clinical and behavioural research activity includes investigator-led studies relevant to psychedelic-assisted therapy and mental health.
National Institute on Drug Abuse (NIDA)
U.S. federal institute setting addiction-research priorities and portfolios, including psychedelic-related investigations.
Radboud University
Radboud University Medical Center (Radboudumc) is one of the Netherlands' leading academic medical centers, located in Nijmegen. It combines patient care, education, and scientific research under one roof, with a particular strength in neuroscience through its Donders Centre for Medical Neuroscience. Radboudumc is known for its translational research approach. The medical centre bridges fundamental science and clinical practice across areas including oncology, rare diseases, and psychiatry. In the field of psychedelic medicine, Radboudumc has been involved in ibogaine research, conducting studies through its Department of Pharmacology–Toxicology and Department of Psychiatry, examining ibogaine as a potential treatment for opioid use disorder. This work included a clinical study evaluating the cardiac, cerebellar, and psychomimetic safety of ibogaine in opioid-dependent patients, contributing important safety data to the broader scientific understanding of this compound.
National Institute of Mental Health (NIMH)
U.S. federal institute defining mental-health research agendas and evidence-generation priorities including psychedelic-relevant studies.
University of Amsterdam
The University of Amsterdam (UvA) is one of the Netherlands' leading research universities, with its Amsterdam UMC Department of Psychiatry conducting clinical trials on psilocybin and psychedelic-assisted therapies for treatment-resistant mental health conditions.
University of California, San Francisco
University of California, San Francisco (UCSF) hosts major psychedelic research activity through the Translational Psychedelic Research Program (TrPR), Neuroscape Psychedelics Division, and psychiatry-led clinical research on psychedelic-assisted therapies.
Integrative Mental Health University
The Integrative Mental Health University (IMHU) is a nonprofit continuing education platform founded by Emma Bragdon PhD in 2013, offering accredited courses for mental health professionals on psychedelic-assisted therapy, spiritual emergence, and integrative healing modalities. IMHU serves clinicians seeking to incorporate psychedelic therapy and spiritual emergency response into their professional practice.
Centre for Addiction and Mental Health
The Centre for Addiction and Mental Health (CAMH) is Canada's largest mental health teaching hospital, located in Toronto, Ontario. CAMH is a major hub for psychedelic research in Canada, running trials on psilocybin, MDMA, and ketamine across a range of psychiatric indications.
Usona Institute
Usona Institute is a US-based 501(c)(3) non-profit medical research organisation headquartered in Madison, Wisconsin. Usona develops and supports clinical research on psilocybin and other consciousness-expanding medicines with a mission-driven access model. Its psilocybin programme received FDA Breakthrough Therapy Designation for major depressive disorder in 2019. After completing the Phase 2 PSIL201 study, Usona launched the Phase 3 uAspire trial in 2024, a 240-participant randomised, double-blind multicentre study of 25 mg psilocybin with psychosocial support for adults with MDD. In April 2026, industry reporting said Usona confirmed it had received an FDA Commissioner National Priority Voucher for psilocybin in MDD, potentially shortening review if an NDA is filed and accepted. Usona is also exploring 5-MeO-DMT in early-stage research.
Icahn School of Medicine at Mount Sinai
Icahn School of Medicine at Mount Sinai is a leading US academic medical institution home to the Parsons Research Center for Psychedelic Healing, which runs rigorous clinical trials of MDMA- and psilocybin-assisted therapies for PTSD and trauma in veteran and civilian populations.
People
Search →Hartej Gill
Researcher in mood disorders psychopharmacology at the University of Toronto / University Health Network
Notable for coauthoring multiple reviews and meta-analyses on ketamine, esketamine, suicidality, cognition, and psychedelic drug trials in psychiatric research.
Attila Szabo
Researcher in psychoneuroimmunology and psychedelic science; affiliated with the University of Oslo
He is a notable contributor to psychedelic immunology research, including widely cited work on DMT, 5-MeO-DMT, psilocybin, and immune modulation.
Jeanine Kamphuis
Psychiatrist and researcher at the Department for Mood Disorders, University Hospital Groningen (UMCG)
She studies ketamine, esketamine, and classic psychedelics for treatment-resistant psychiatric disorders, including depression, and is a coauthor on multiple psychedelic/ketamine reviews and clinical studies.
Kayla Teopiz
Researcher in psychiatry and ketamine/psychedelic medicine research; likely affiliated with the University of Toronto/Trillium Health Partners research network
Teopiz coauthors multiple systematic reviews and clinical studies on ketamine, esketamine, and psilocybin in depression and suicidality, helping synthesize the evidence base for psychedelic and glutamatergic treatments in psychiatry.
Jolien Veraart
Psychiatrist and PhD researcher at the University Medical Center Groningen / University of Groningen
She is a leading clinical researcher on ketamine and oral esketamine for treatment-resistant depression, including safety, efficacy, and real-world implementation.
Joshua Di Vincenzo
MSc researcher / clinical research staff member at the University Health Network and University of Toronto
He coauthors multiple systematic reviews and real-world studies on ketamine for treatment-resistant depression, making him a visible contributor to the evidence base on psychedelic-adjacent psychiatric therapeutics.
John Kelly
Associate Professor / Consultant General Psychiatrist at Trinity College Dublin
John R. Kelly is a leading academic psychiatrist in Ireland whose work has helped shape modern psychedelic psychiatry, including psilocybin research across depression, service-user attitudes, and transdiagnostic treatment frameworks.
Kenji Hashimoto
Professor, Division of Clinical Neuroscience, Chiba University Center for Forensic Mental Health
He is a leading Japanese psychiatric researcher whose work on ketamine, arketamine, and related biomarkers has helped shape modern rapid-acting antidepressant research.
David Mathai
Psychiatrist and Assistant Professor at The Johns Hopkins University School of Medicine
He is a psychiatric researcher at Johns Hopkins whose work spans psilocybin, ketamine/esketamine, and psychedelic-assisted psychotherapy, with multiple publications on experiential and therapeutic outcomes.
Bing Cao
PhD researcher at the Key Laboratory of Cognition and Personality, Faculty of Psychology, Southwest University
He is a recurring coauthor on multiple ketamine and psychedelic-adjacent systematic reviews and mechanistic studies, making him a visible contributor to contemporary rapid-acting antidepressant research.
Scott Tyler Aaronson
Chief Science Officer, Institute for Advanced Diagnostics and Therapeutics at Sheppard Pratt; Adjunct Professor of Psychiatry, University of Maryland School of Medicine
He is a leading psychiatrist in treatment-resistant depression and a key investigator on psilocybin studies, including work on preparation, dosing, outcomes, and mechanisms of psychedelic-assisted therapy.
Andrea Fagiolini
Professor of Psychiatry at the University of Siena; Director of Psychiatry at Siena University Hospital
He is a major clinical psychiatry researcher with work spanning depression, bipolar disorder, ketamine/esketamine, and broader neuropsychiatric treatment innovation.
Connected Evidence
The latest clinical data and verified academic findings associated with Bipolar Disorder.