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DOI: 10.1055/a-1524-2794
Classic Psychedelic Coadministration with Lithium, but Not Lamotrigine, is Associated with Seizures: An Analysis of Online Psychedelic Experience Reports
Abstract
Introduction Psychedelics show promise in treating unipolar depression, though patients with bipolar disorder have been excluded from recent psychedelic trials. There is limited information on the use of classic psychedelics (e. g., LSD or psilocybin) in individuals using mood stabilizers to treat bipolar disorder. This is important to know, as individuals with bipolar depression may attempt to treat themselves with psychedelics while on a mood stabilizer, particularly given enthusiastic media reports of the efficacy of psilocybin for depression.
Methods This study analyzed reports of classic psychedelics administered with mood stabilizers from 3 websites (Erowid.org, Shroomery.org, and Reddit.com).
Results Strikingly, 47% of 62 lithium plus psychedelic reports involved seizures, and an additional 18% resulted in bad trips while none of 34 lamotrigine reports did. Further, 39% of lithium reports involved medical attention. Most of the lamotrigine reports (65%) but few (8%) of the lithium reports were judged to not affect the psychedelic experience.
Discussion Although further research is needed, we provisionally conclude that psychedelic use may pose a significant seizure risk for patients on lithium.
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Introduction
After more than 6 decades of research into and popular use of classic psychedelics (defined here as a class of drugs that produce a unique profile of subjective effects and have a principal site of action at the 5HT2A receptor, such as LSD or psilocybin), recent promising trials investigating the effects of psilocybin therapy for the treatment of depression [1] [2], anxiety and depression in cancer patients [3] [4], tobacco smoking [5], and alcohol use disorder [6] have inspired additional medical, commercial, and public interest in using psychedelics as treatments for psychiatric disorders. Interest has also grown in understanding whether psilocybin therapy may be effective for a wider range of indications [7] [8] [9].
Depressive episodes in individuals with bipolar disorder (“bipolar depression”) in particular have been discussed as targets of interest, with at least one study planned in patients with bipolar II disorder (Clinicaltrials.gov identifier NCT04433845). However, the risk of adverse events in this patient population merits special consideration in light of the possibility of precipitating mania and concerns about possible interactions with other drugs commonly used to treat bipolar disorder.
Bipolar disorder is a chronic condition characterized by episodes of mania or hypomania and predominantly depressive episodes [10]. Pharmacologic treatment of bipolar disorder can be challenging due to the need to address alternating extremes of mood [11]. Treatment usually includes “mood stabilizers” such as lithium, certain anti-epileptic drugs, and anti-psychotics. Lithium remains the gold-standard treatment with particular efficacy for relapse prevention and treatment of acute mania [12] [13]. However, treatment options specifically targeting depressive episodes in bipolar disorder are limited.
Modern psychedelic trials typically exclude people with bipolar disorder [14]. This was considered to be a prudent safety measure, given the potential for precipitating psychosis or mania in patients with a personal or family history of schizophrenia or bipolar spectrum disorders [15], but it also leaves open the question of whether psychedelic drugs may be effective in treating patients with bipolar depression. The combination of promising evidence for psilocybin in treating unipolar depression, the fact that bipolar depression is difficult to treat, the lack of clear information on problematic drug interactions, the increasing availability of psilocybin mushrooms, and the extensive positive media coverage of anecdotal reports suggesting therapeutic benefits of psilocybin in depression may lead individuals with bipolar disorder to take psychedelic drugs in addition to continuing their existing medications.
There is very little information concerning the effects of concurrent psychedelics and mood stabilizers. An online survey noted 2 subjects who reported taking LSD while on lithium (600 mg and 1000 mg) and described intensified subjective effects from LSD [16].
Here we report on anecdotal descriptions of reactions to the use of psychedelic drugs when taken with a concurrent mood stabilizer. Data were drawn from a systematic search of self-reported experiences posted or published in public online forums focused on psychedelic drugs. While this method cannot conclusively determine safety, it could establish some signal for risk in the potential for harmful interactions between psychedelic and typical therapeutic drugs.
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Methods
Data collection
Three websites were used as data sources—Erowid.org, Shroomery.org, and Reddit.com. These are publicly accessible sites and online communities that include user-created and user-driven content in which people can anonymously share information related to psychedelic drug use. These online communities frequently receive “trip reports” (henceforth experience reports), or descriptions, often quite detailed, of psychedelic drug experiences. Though mostly anonymous, individuals typically post under a pseudonym. Experience reports on these websites are organized in a fashion that is amenable to automated collection and analysis of these reports (see individual descriptions below). For this paper, reports from each internet site were filtered for duplicate usernames to eliminate double-reporting on the same individual to the extent possible.
Most experience reports did not include demographic information such as age, prior psychedelic use, psychiatric and medical history, etc. in any systematic way, so these were not collected.
Experience reports were searched for a series of terms related to the use of mood stabilizers in combination with psychedelics. Antipsychotics and antidepressants were not separately queried, but the presence of an antipsychotic or antidepressant (among other psychoactive drugs) was coded in all selected experience reports at a later stage (see Coding of Reports below). Mood stabilizer search terms included: lithium, lamotrigine, valproic acid, carbamazepine, and oxcarbazepine, including generic and trade names and different chemical names (e. g., valproate, Depakote, etc.) Because good quality empirical laboratory studies have been published involving coadministration of haloperidol and risperidone with psilocybin, antipsychotics were not included in the search of the current, lower-quality data [17]. Psychedelic search terms included LSD, psilocybin mushrooms, DMT, mescaline, peyote, San Pedro, and ayahuasca, all of which are 5-HT2A receptor agonists commonly used in recreational settings.
Erowid
Erowid is a curated online resource founded in 1995 for information related to psychoactive drugs, which also contains sections for user-generated and submitted content including experience reports for each drug and drug class that is covered on the website. Erowid’s reports are tagged before publication with the drugs described in each report. Erowid has an application programming interface (API)—a purpose-built programming interface typically used to allow programmers to gain custom access to a data source or computing infrastructure. An API provided by Erowid was accessed via a custom python script on August 7, 2020, and used to identify and collect experience reports for the current analysis.
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Shroomery
The Shroomery is an online community related to psychedelic drug use, nominally focused on psilocybin mushroom use but containing information posted by users for a wide range of psychedelic substances. The Shroomery has a specific section of its website dedicated to experience reports. Experience report entries on Shroomery.org were accessed on August 21, 2020, with a custom programming script written using R statistical software [18] using the packages rvest [19] and RSelenium [20]. These packages allow for “web scraping,” which is a systematic search and accessing of all of the contents of a given website without the need for an API.
In addition to specific experience reports, Shroomery.com also has a wide array of additional forums with posts that could have relevance. These were not searched as those posts would require excessive manual coding to extract the relevant data and are far less likely to include codable and relevant data than the specific “trip reports” section of the community.
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Reddit is one of the largest collections of online communities in the world, with innumerable “subreddits” or sections dedicated to particular topics. Reddit was chosen as a third source due to ease of access to data through an API. Posts on the subreddits r/Drugs, r/Shrooms, r/Psychonaut, r/TripReports, r/Psychedelics, r/LSD, r/Acid, and r/Epilepsy were accessed on August 22, 2020, with a script written in the python coding language [21] and using the Python Reddit API Wrapper (PRAW), a python package designed to interface with Reddit’s API [22]. Search terms were similar to the above.
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Coding of reports
All experience reports (including comments, in the case of Reddit posts) that contained both a mood stabilizer search term and a psychedelic search term were collected and then manually coded by a research assistant and an author (SMN) for the presence of direct first-person or witnessed second-person reports of the experience encountered when a psychedelic was consumed by an individual who was also taking a mood stabilizer. This step was mainly relevant for Reddit as experience reports from Erowid and the Shroomery were already coded by drug pre-selected to involve accounts of consumption. In contrast, Reddit posts frequently included questions and comments without specific accounts of drug use.
Those experience reports that contained such a first- or second-hand report were then coded for the presence or absence of the mention of other psychiatric medications and psychoactive drugs (including caffeine, cannabinoids, benzodiazepines, and antipsychotics, stimulants, etc.), the reported effect, and whether or not a microdose of a psychedelic had been consumed. If the dose was not mentioned, it was assumed that the reported experience occurred in the context of a typical psychoactive dose (i. e., not a microdose). Experience reports that included both lithium and lamotrigine were removed (2 from Erowid, 0 from Shroomery, and 2 from Reddit), to separately compare reports of these 2 mood stabilizers taken with psychedelics. Three Reddit posts with duplicate content were identified and removed.
Experience reports involving “microdoses” of psychedelics—very low doses with minimal subjective effects—were not included. Likewise, very small doses of lithium (such as less than 30 mg, as is sometimes taken in the form of lithium orotate over the counter) were also not included due to less likelihood of physiological effects with low doses and the different clinical population that might take these.
Effects were coded in 6 mutually exclusive categories based on the author’s description and interpretation of the effect of the concomitant mood-stabilizing medication on the psychedelic drug effect. 1) “seizure” was coded if the report indicated a seizure; 2) “bad trip” was coded if there was an explicit description of an overall negatively valenced or noxious experience excluding seizure; 3) “intensified psychedelic effects” was coded if the medication intensified the psychedelic effects excluding reports coded as seizures or bad trips; 4) “decreased psychedelic effect” was coded if the medication reduced the subjective psychedelic effect excluding reports coded as no psychedelic effect; 5) “no psychedelic effect” was coded if the medication completely prevented a subjective psychedelic effect, and 6) “neutral” was coded if there was either no particular mention of an effect or an explicit mention of no effect on the psychedelic experience. SMN manually coded these reports, which were then reviewed by NG, with discrepancies resolved by discussion.
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Results
Experience Reports
All reports from Erowid and the Shroomery that met search criteria also met criteria for analysis as they were already selected to include an account of a drug experience and organized by drugs consumed. In contrast, Reddit required a great degree of manual coding following the search to identify reports that met the criteria for analysis.
Only reports involving lithium and lamotrigine were analyzed as there were few search results involving valproic acid (1 on Erowid, 15 on Reddit), carbamazepine (8 on Reddit), and oxcarbazepine (9 on Reddit). Ultimately, 96 total reports involving lithium or lamotrigine were identified and met the criteria to be analyzed. An additional 4 reports involved both lithium and lamotrigine and a concurrent psychedelic—these are reported separately.
Verbatim text from all experience reports is included in the online Supplementary Materials.
Lithium reports
There were a total of 62 analyzed lithium reports across all 3 sites ([Fig. 1]). Erowid had 16 qualifying lithium experience reports (15 [93.8%] with LSD and 1 [6.2%] with psilocybin mushrooms). The Shroomery contained 2 lithium trip reports (1 with LSD and the other with psilocybin mushrooms). Reddit had 44 qualifying lithium reports (39 with LSD [88.6%], 4 [9.1%] with psilocybin mushrooms, and 1 [2.3%] with DMT).
Of available experience reports from Erowid, the Shroomery, and Reddit involving lithium plus a psychedelic, 29 of 62 (46.8%) reports were seizures, and an additional 11 of 62 (17.7%) were bad trips. An additional 12 of 62 (19.4%) reports were described as intensified. Only 5 of 62 (8.1%) reports were described as neutral, with lithium not described to affect the psychedelic experience.
Of the 55 reports of lithium plus LSD, 27 (49.1%) were seizures. Of the 6 reports of lithium plus psilocybin, 2 (33.3%) were seizures. The sole report of lithium plus DMT did not involve seizures. Removing the 18 lithium reports that contained another psychoactive drug (most commonly serotonin reuptake inhibitors [n=5]), 54.5% of reports still involved seizures.
Notably, 39% of reports involving lithium and a psychedelic included mention of emergency medical treatment either in the form of an ambulance being called or ending up in a hospital.
Experience reports involving an additional class of more rarely used psychedelics, the 5-HT2A agonist drugs 2C-B, 2C-E, and 2C-I, were not included in the main analysis due to the low number of reports (2 Erowid reports for 2C-I with concurrent lithium, 1 Erowid report for 2C-C with concurrent lithium). However, it is noteworthy that both reports involving 2C-I use and concurrent lithium involved seizures, and the report of the 2C-C plus lithium report was described as intensified.
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Lamotrigine reports
There were a total of 34 analyzed reports of lamotrigine combined with a psychedelic across the 3 sites ([Fig. 2]). Erowid had 6 reports (3 with LSD, 2 with psilocybin mushrooms, and 1 with smoked DMT). The Shroomery had a single report (psilocybin mushrooms). Reddit had 27 qualifying lamotrigine (or Lamictal) reports (19 [55.9%] with LSD, 7 [20.6%] with psilocybin mushrooms, and 1 [2.9%] with DMT).
In the majority of lamotrigine reports, authors did not clearly express a view that lamotrigine impacted the experience of the psychedelic one way or another. In 22 of 34 (64.7%) lamotrigine reports, the drug was not reported to have impacted the psychedelic experience. In 6 of 34 (17.6%) lamotrigine reports, the psychedelic effect was decreased, and in 3 of 34 (8.8%) reports, there was no psychedelic effect at all. No reports were described as bad trips. The remaining 3 of 34 (8.8%) reports were described as intensified without an overall negative valence.
Removing the 12 lamotrigine reports that included another psychoactive drug apart from a psychedelic did not substantially change results—in 73.1% of reports, lamotrigine was not described as affecting the psychedelic experience.
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Lithium plus lamotrigine reports
Excluded from the above analysis were 4 reports that included both lithium and lamotrigine with a psychedelic. One of 4 (25%) of these reports involved a seizure (though this person also took the MAOI Syrian Rue), and the remaining 3 were described as intensified.
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Discussion
There is a paucity of data about the concurrent use of psychedelic substances with commonly prescribed psychiatric medications, which is concerning given increasing public attention to psilocybin-containing mushrooms and the proliferation of enthusiastic and uncritical media reports extolling the benefits of psychedelics such as psilocybin for the treatment of depression and other psychiatric conditions. It is increasingly likely that patients taking conventional psychiatric medications may attempt to treat themselves with psychedelics.
In this study, we collected psychedelic experience reports from 3 large online sources where individuals share such reports (Erowid.org, Shroomery.org, and relevant subreddits from Reddit.com). This study focused on first- or second-person accounts of a psychedelic used in combinations with the commonly prescribed mood stabilizers, lithium or lamotrigine.
Seizures were frequently associated with lithium
The most notable finding of this study is that 47% of reports of the use of a classic psychedelic by individuals using lithium involved seizures. This was more frequently reported with LSD but also occurred with psilocybin. As mentioned above, it is also notable that 2 of 3 reports involving a 2C drug and lithium involved seizures (though these were not included in the main analysis).
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Affectively negative experiences (“bad trips”) were more common with lithium than lamotrigine
In addition to reports involving seizures, lithium reports were more likely than lamotrigine reports to be categorized as bad trips (18% versus 0%, respectively).
If seizure reports are excluded (because the categories were mutually exclusive), then 11 of 33 (33%) non-seizure lithium reports were classified as bad trips.
Below are illustrative examples of verbatim experience reports of lithium and LSD that were classified as non-seizure bad trips:
“Pro Tip: DON’T FUCK WITH THIS. Speaking from experience, Lithium can cause HIGHLY UNPREDICTABLE reactions to dosing. Sometimes 3 150 ug hits do nothing or, in my case, 2 hits had me wandering around [ ... ] all night with no shoes on in full ego death, mumbling to myself like a homeless guy, wandering into traffic, etc. I was fine, but it was SUPER STUPID in hindsight. As such, I no longer take lithium.”[ 1 ]
“I took lsd while on 900 mg of lithium and experienced the worst, most horrific trip of my life and haven’t touched lsd since. I had only taken 1 tab but the effects were akin to having doses 5+tabs. I completely lost all touch with reality, everything I saw was drenched in blood, and I felt my throat closing up and felt like I was on fire-like my skin was burning. I somehow still managed to take a Seroquel despite having lost all touch with reality which brought me out of it after an hour or so I’m guessing (completely lost touch with time) and once I stopped hallucinating I was unable to speak for several hours.”[ 2 ]
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Caveats and clinical implications
The online reports used here are “low quality evidence” [23] [24] due to lack of standardization, selection bias, and lack of clinical verification. Furthermore, it is possible that the same individual posted multiple times on different websites or the same websites with different usernames. In addition, the lithium reports largely did not include information about lithium dose, so we are unable to speculate on dose effects. Despite these caveats, the risk of potentially lethal reactions and the absence of compelling non-causal explanations suggests that the most conservative approach would be to assume a causal relationship—that taking a classic psychedelic (e. g., a non-microdose of LSD or psilocybin) in combination with the therapeutic use of lithium can cause seizures as well as increase the likelihood of otherwise affectively negative experiences.
Thus, we advise individuals taking lithium to avoid taking classic psychedelic drugs. Reports of psychedelic microdoses were not included, thus we are unable to comment on this. It is possible that seizure risk could be mitigated by first tapering and discontinuing lithium, but there is not enough information to make a recommendation.
The benignity of experience reports with lamotrigine does not mean that it is necessarily safe to administer psychedelics to those prescribed it, but the relative lack of signal for increased risk in the analyzed reports could aid future decision-making for clinical trials. For example, a trial of psychedelic treatment for bipolar disorder involving the continuation of mood stabilizers might avoid lithium in favor of lamotrigine due to a lower probability of risk.
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Mechanistic conjectures
There are several possible explanations for seizures in individuals who take psychedelics while using lithium. One possibility is that those who are prescribed lithium may have unique propensities for seizures independent of any risks associated with lithium itself. The current data are limited in that we do not have any medical history information, including seizure risk. People with unipolar depression do have a higher risk of seizure disorder than the general population [25] [26] [27], though it is less clear if this is true for bipolar disorder.
A second possible mechanism is that co-administration of lithium and psychedelics could increase systemic concentrations of 1 or both drugs leading to seizures. Though lithium has been found safe to administer to patients with epileptic disorders, elevated lithium levels confer an increased risk for seizures [28]. Classic psychedelics are known to increase cortical excitability [29] and can also, in rare cases, precipitate seizures [30]. However, a metabolic interaction affecting systemic concentrations of either drug is unlikely due to a relative lack of overlap in their metabolic pathways. LSD and psilocybin undergo hepatic metabolism to more water-soluble forms before excretion through urine and other body fluids [31] [32]. Lithium, in contrast, is principally renally excreted without undergoing any hepatic alteration.
A third explanation involves changes in local concentrations of lithium and/or psychedelics in the brain. Sartorius et al. also report a case of serotonin syndrome that developed within hours of ECT in a patient who had been treated with lithium, though this did not result in seizures [33]. This raises the question of whether some of the seizures described in these reports occurred in the context of serotonin syndrome. A review of the reports that included seizures found that a substantial portion of cases presented with other signs that may be consistent with serotonin syndrome, including diaphoresis, tachycardia, vomiting, mydriasis, agitation, confusion, and loss of coordination. However, these additional symptoms are more difficult to interpret as they may overlap with the expected effects of psychedelics.
A final and more likely category of explanation would be that concomitant use of lithium and psychedelics results in a synergistic effect on neurotransmission or second messenger effects that increase the likelihood of seizures. The psychoactive effects of psychedelics are mediated primarily by 5-HT2A agonism, and 5-HT2A agonism by psychedelics is generally understood to increase cortical excitability [29] [34]. Psychedelics also have an indirect effect of reducing the tonic activity of the locus coeruleus [35] [36] [37] [38]. Locus coeruleus activation can be protective against seizures [39] [40] [41] [42] [43] [44], suggesting that psychedelic reduction of tonic locus coeruleus activity may represent a potential indirect mechanism by which psychedelic drug administration could reduce the seizure threshold.
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Conclusion
Almost half of online psychedelic experience reports involving lithium and a classic psychedelic (a non-microdose of LSD or psilocybin) involved seizures (47%) and 18% involved otherwise negative experiences. Furthermore, 39% of these reports involved emergency medical treatment. In contrast, lamotrigine was not judged to have impacted the experience of the psychedelic drug in the majority of lamotrigine plus psychedelic experiences (64.7%). Removing all reports that mentioned concurrent use of other psychoactive drugs (most commonly serotonin reuptake inhibitors) did not alter these general findings. Although we acknowledge the substantial limitations of data based on anonymous online psychedelic experience reports, we believe that at present, lithium should be considered a contraindication to psychedelic use.
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Conflict of Interest
RRG is on the board of directors of the Heffter Research Institute. SMN serves on a Data Safety and Monitoring Board for Maryland Oncology Hematology. EE and FE are employed by Erowid Center, the non-profit that operates Erowid.org, one of the data sources.
Acknowledgments
We thank Alex Cook for providing experience report data that were accessed through the Erowid API.
1 Source: Why does LSD and lithium cause serotonin syndrome if LSD is a serotonin receptor agonist, which does not release serotonin? 2020; Im Internet: https://www.reddit.com/r/Acid/comments/dwn00y/why_does_lsd_and_lithium_cause_serotonin_syndrome/
2 Source: Lithium and lsd? 2019; Im Internet: https://www.reddit.com/r/Psychonaut/comments/95itb8/lithium_and_lsd/
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Correspondence
Publication History
Received: 28 February 2021
Received: 11 May 2021
Accepted: 25 May 2021
Article published online:
04 August 2021
© 2021. Thieme. All rights reserved.
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References
- 1 Davis AK, Barrett FS, May DG. et al. Effects of psilocybin-assisted therapy on major depressive disorder: A randomized clinical trial. JAMA Psychiatry 2021; 78: 481-489
- 2 Carhart-Harris RL, Bolstridge M, Rucker J. et al. Psilocybin with psychological support for treatment-resistant depression: An open-label feasibility study. Lancet Psychiatry 2016; 3: 619-627
- 3 Griffiths RR, Johnson MW, Carducci MA. et al. Psilocybin produces substantial and sustained decreases in depression and anxiety in patients with life-threatening cancer: A randomized double-blind trial. J Psychopharmacol 2016; 30: 1181-1197
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