Hostname: page-component-586b7cd67f-rdxmf Total loading time: 0 Render date: 2024-11-26T19:30:25.425Z Has data issue: false hasContentIssue false

Adverse psychiatric effects of psychedelic drugs: a systematic review of case reports

Published online by Cambridge University Press:  20 November 2024

B. Yildirim
Affiliation:
FIDMAG Hermanas Hospitalarias Research Foundation and CIBERSAM, ISCIII, Barcelona, Spain
S. S. Sahin
Affiliation:
Department of Psychiatry, Bakırkoy Mazhar Osman Mental Health and Neurological Diseases Education and Research Hospital, Istanbul, Türkiye
A. Gee
Affiliation:
Department of Psychological Medicine, Institute of Psychiatry, Psychology and Neuroscience, King's College London, London, UK
S. Jauhar
Affiliation:
Department of Psychological Medicine, Institute of Psychiatry, Psychology and Neuroscience, King's College London, London, UK
J. Rucker
Affiliation:
Department of Psychological Medicine, Institute of Psychiatry, Psychology and Neuroscience, King's College London, London, UK South London & Maudsley NHS Foundation Trust, Bethlem Royal Hospital, Kent, UK
P. Salgado-Pineda
Affiliation:
FIDMAG Hermanas Hospitalarias Research Foundation and CIBERSAM, ISCIII, Barcelona, Spain
E. Pomarol-Clotet
Affiliation:
FIDMAG Hermanas Hospitalarias Research Foundation and CIBERSAM, ISCIII, Barcelona, Spain
P. McKenna*
Affiliation:
FIDMAG Hermanas Hospitalarias Research Foundation and CIBERSAM, ISCIII, Barcelona, Spain
*
Corresponding author: P. McKenna; Email: [email protected]
Rights & Permissions [Opens in a new window]

Abstract

Background

Psychedelic drugs are a focus of interest in the treatment of depression and other disorders but there are longstanding concerns about possible adverse psychiatric consequences. Because the relevant literature is largely informal, the seriousness of these risks is difficult to evaluate.

Methods

Searches were made for case reports of schizophrenia-spectrum, affective or other psychiatric disorders after use of psychedelic drugs. Case reports of flashbacks were also searched for. Individuals with recent use of other drugs (apart from cannabis and alcohol) and/or a previous history of major psychiatric disorder were excluded. Symptoms were tabulated using the Syndrome Check List of the Present State Examination (PSE-9).

Results

We found 17 case reports of schizophrenia spectrum disorder, 17 of affective disorder (depression, mania, or both), 3 cases of anxiety, 1 of depersonalization, and 1 of unclassifiable illness. The states could develop after a single use of the drug (5/17 schizophrenia; 6/17 affective disorder), and duration was highly variable. Recovery was the rule in cases of affective disorder but not in schizophrenia spectrum disorder. Twelve of 29 cases of flashbacks showed psychiatric symptomatology definitely outlasting the attacks, mainly anxiety (5 cases) and depression (8 cases). Flashback symptoms resolved within twelve months in approximately half of the cases but in a few persisted for years.

Conclusions

Reliable descriptions of schizophrenia spectrum disorder and major affective disorder after psychedelic drug use disorder exist but are relatively uncommon. Flashbacks are sometimes but not always associated with psychiatric symptomatology, mainly anxiety or depression.

Type
Review Article
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution and reproduction, provided the original article is properly cited.
Copyright
Copyright © The Author(s), 2024. Published by Cambridge University Press

Introduction

After early interest, followed by criminalization and the halting of almost all human research (Lieberman, Reference Lieberman2021; Rucker, Iliff, & Nutt, Reference Rucker, Iliff and Nutt2018), the potential therapeutic effects of psychedelic drugs are once again a focus of worldwide attention. Four recent trials (Carhart-Harris et al., Reference Carhart-Harris, Giribaldi, Watts, Baker-Jones, Murphy-Beiner, Murphy and Nutt2021; Goodwin et al., Reference Goodwin, Aaronson, Alvarez, Arden, Baker, Bennett and Malievskaia2022; Raison et al., Reference Raison, Sanacora, Woolley, Heinzerling, Dunlop, Brown and Griffiths2023; von Rotz et al., Reference von Rotz, Schindowski, Jungwirth, Schuldt, Rieser, Zahoranszky and Vollenweider2023) (one of them large, N = 233; Goodwin et al., Reference Goodwin, Aaronson, Alvarez, Arden, Baker, Bennett and Malievskaia2022) have found evidence for psilocybin's effectiveness in major depressive disorder, leading to the FDA designating it a ‘breakthrough therapy’ for treatment-resistant patients with the disorder. A 2020 review (Reiff et al., Reference Reiff, Richman, Nemeroff, Carpenter, Widge, Rodriguez and McDonald2020) also identified four contemporary trials of psychedelics (three of psilocybin and one of LSD) for anxiety and/or depression associated with life-threatening disease, with another published since then (Holze, Gasser, Muller, Dolder, & Liechti, Reference Holze, Gasser, Muller, Dolder and Liechti2023). The same review found two trials of ayahuasca, a hallucinogenic preparation used in South American shamanic ceremonies whose active ingredient is dimethyltryptamine (DMT), for major depression. Two double-blind placebo-controlled trials of psilocybin for obsessive-compulsive disorder are currently underway (Ching et al., Reference Ching, Amoroso, Bohner, D'Amico, Eilbott, Entezar and Kelmendi2023a, Reference Ching, Grazioplene, Bohner, Kichuk, DePalmer, D'Amico and Kelmendi2023b).

The therapeutic benefits of psychedelics may come at a price, however. After initially being considered infrequent (Cohen, Reference Cohen1960), reports of adverse psychiatric effects increased dramatically after recreational use of LSD became widespread (Schwarz, Reference Schwarz1968; Smart & Bateman, Reference Smart and Bateman1967). Prominent among these were schizophrenia: reviewing the literature in 1979, Klawans, Tanner, and Goetz (Reference Klawans, Tanner, Goetz, Fuxe and Calne1979) concluded that there was evidence for a chronic psychosis associated with use of LSD, which usually occurred in individuals who had taken it 50 or more times and whose symptoms included ‘paranoid ideation, prominent use of denial and projection, poorly organized and bizarre thoughts, intermittent visual hallucinations, shallow affect, withdrawn behavior, and loss of long-term memory.’ The presentation was considered comparable to chronic undifferentiated schizophrenia, with the exception that interpersonal functioning was preserved in some cases.

In contrast, affective disorder as a complication of psychedelic drug use has historically attracted little attention. After analyzing case reports up to 1967, Smart and Bateman (Reference Smart and Bateman1967) concluded that purely depressive states appeared to be rare, and they found only one case of a ‘motor excitatory state’. Depression was not mentioned at all in a later review (Strassman, Reference Strassman1984). In the view of Cohen (Reference Cohen1985), an author who wrote extensively on LSD, manic and depressive episodes could be seen, although less frequently than schizophrenia-like states. This author also noted the occurrence of other disorders characterized by anxiety, panic, or confusion, as well as dissociative states and states characterized by depersonalization.

The explosion of use of LSD and other psychedelic drugs also led to recognition of a further adverse psychiatric effect: flashbacks, spontaneous recurrences of aspects of the psychedelic experience, particularly the perceptual changes. This phenomenon had occasionally been noted by early authors after use of LSD and mescaline therapeutically or experimentally (Cooper, Reference Cooper1955; Harley-Mason, Laird, & Smythies, Reference Harley-Mason, Laird and Smythies1958; Sandison & Whitelaw, Reference Sandison and Whitelaw1957). However, credit for its formal description is probably due to Cohen and Ditman (Reference Cohen and Ditman1963): they described two regular LSD users who saw faces or skulls moving on walls, and a child who accidentally took LSD and a week later experienced movements on the TV screen and ‘light halos’ with his eyes closed; in all three cases the experience was accompanied by anxiety. Further descriptions followed (e.g. Cohen, Reference Cohen1966; Horowitz, Reference Horowitz1970; Rosenthal, Reference Rosenthal1964; Smart & Bateman, Reference Smart and Bateman1967), and in 1987 the term hallucinogen persisting perception disorder (HPPD) was introduced in DSM-III-R. This included a requirement for flashback symptoms to be associated with clinically significant distress or impairment in social, occupational, or other areas of functioning. The criteria for the disorder remain essentially unchanged in DSM-5.

Notwithstanding an extensive literature, determining whether and to what extent psychedelic drugs can cause psychosis or other psychiatric disorders faces difficulties. Firstly, many of the relevant studies date from the 1960s and 1970s, when the concept of schizophrenia was looser than it is today, especially in the United States, where the use of psychodynamic terminology like ego-fragmentation and projection also complicates interpretation. Secondly, psychedelic users who develop psychiatric disorders will likely have used other drugs as well, and some of them may have had pre-existing psychiatric disorders. Similar problems apply to the literature on flashbacks/HPPD, which remains a generally under-researched topic.

One strategy for establishing how far psychedelics are associated with development of psychiatric disorders is by means of systematic review of case reports. Such an approach can help define the range of disorders seen and, in the case of flashbacks/HPPD, answer questions about the nature of perceptual changes that characterize them, as well as potentially shedding light on how far they are distressing and/or associated with impaired functioning. In this study we searched the worldwide case report literature on psychiatric complications of use of psychedelic drugs, excluding individuals who showed concurrent use of other drugs (apart from cannabis and alcohol) and those who had a previous history of major psychiatric disorder, and formally tabulating the symptoms described.

Method

We searched PubMed (which includes MEDLINE), Embase and psycINFO for articles reporting individual cases of any kind of adverse psychiatric event in the context of use of psychedelic drugs. Drugs considered as psychedelics included LSD, lysergic acid amide (morning glory seeds and Hawaiian baby woodrose seeds), mescaline/peyote, psilocybin, dimethyltryptamine (DMT)/ayahuasca and the amphetamine-related drugs, 2,5-dimethoxy-amphetamine (STP or DOM), and 2,5-dimethoxy-bromoamphetamine (brolamfetamine, bromo-DMA). These drugs all have 5HT2A receptor partial agonism as their principal mode of action, the property now recognized as responsible for conferring psychedelic effects (Nichols, Reference Nichols2016). Bufotenine was also included in the search although there is some doubt about whether its effects are truly psychedelic and to what extent it exhibits 5HT2A agonism (Lyttle, Goldstein, & Gartz, Reference Lyttle, Goldstein and Gartz1996) (in the event no relevant articles were found for this drug). Ibogaine and MDMA were not included. Ibogaine's experiential effects do not closely resemble those of classical psychedelic drugs and its mechanism of action appears to be only minimally related to activity at 5HT2A receptors (Alper, Reference Alper2001; Mash, Reference Mash2023). The experiential effects of MDMA are also different from those of psychedelic drugs and its major pharmacological effect is stimulation of serotonin release (Iversen, Reference Iversen2008).

Search terms included hallucinogens, individual drug names, and terms relating to adverse psychiatric effects. The databases were searched up to 21/06/23 and 26/06/23 (for two searches in PubMed, with and without a ‘case report’ filter) and 30/6/23 (for PsycINFO and Embase). No start dates were specified, but we did not formally consider articles published before 1950, as it became clear these only described the psychedelic experience, not complications of it. Four of the authors (BY, SS, AG, PJM), working in groups of two or three, examined the titles and abstracts of publications identified by the electronic search and obtained full versions of all that were considered potentially relevant. We hand-searched reference lists of case reports, studies and review articles, and also checked a number of books that were found. There were no restrictions on language. We considered reports in adolescents and adults with no upper age limit; cases in children were also considered (one such case was included). Details of the searches are given in the Supplementary Information and also in Open Science Framework, where the protocol is registered (https://osf.io/k47g6).

To be included, we required publications to (a) report one or more cases, and (b) give sufficient description of symptoms to allow tabulation using a structured instrument (see below); articles providing only summarized information (e.g. conference abstracts) were not included. Cases were excluded if there was a history of major mental illness (schizophrenia, major depression, bipolar disorder) prior to the index episode, or if there was presence of neurological or other disease affecting brain function, or if the symptoms did not outlast the period of intoxication (defined as 24 hours after taking the drug or 3 days in the case of STP/DOM). We excluded case reports of patients who had used other drugs within a year of the episode, with two exceptions, cannabis and non-dependent use of alcohol.

Symptoms were tabulated using the Syndrome Check-List (SCL) of the Present State Examination (PSE), 9th edition (Wing, Cooper, & Sartorius, Reference Wing, Cooper and Sartorius1974), which was developed to be applied to non-interview information such as casenotes. Typically, one or more symptoms contributing to a syndrome need to be rated for the syndrome to be considered present. Following the checklist guidelines, we did not rate simple statements that the patient had delusions or hallucinations, but required description of the content. Similarly, the SCL syndromes incoherent speech and depersonalization (which covers both depersonalization and derealization) were only rated if there was some additional description to make it clear that the relevant symptoms were being described.

The SCL rates depression under three syndromes, simple depression (inefficient thinking, depressed mood, hopelessness, suicidal plans or acts, depression on examination), special features of depression (self-depreciation, guilty ideas of reference, guilt, dulled perception, lost affect) and other symptoms of depression (morning depression, loss of appetite, early waking, loss of libido, premenstrual exacerbation). An additional syndrome, loss of interest and concentration is also relevant to depression, and there is a psychotic syndrome, depressive delusions and hallucinations. Manic symptoms are rated under hypomania, comprising subjective euphoria, ideomotor pressure, grandiose ideas and actions, hypomanic affect and hypomanic content of speech. Perceptual changes of the kind seen in flashbacks/HPPD were rated under the SCL item non-specific psychosis, which contains items for heightened perception, changed perception and minor visual, auditory and other hallucinations, among other symptoms; each case's individual clinical features were also recorded.

Extraction and tabulation of symptom data was carried out by PJM, who is trained in the use of the PSE. Where there were doubts about inclusion, the PSE glossary of symptoms was consulted.

Results

A flow chart is shown in Fig. 1. Thirty-nine case reports of psychiatric disorders (other than flashbacks/HPPD) from 33 publications were finally included and 29 case reports of flashbacks/HPPD from 23 publications.

Figure 1. Flow chart of the results of the search process.

Schizophrenia spectrum disorder

There were 17 case reports of schizophrenia spectrum psychosis; the findings are summarized in Table 1. The psychedelic drugs taken were LSD (9 cases), lysergic acid amide (3 cases, including one who took both LSD and lysergic acid amide), ayahuasca (2 cases), mescaline (1 case) psilocybin (1 case) and bromo-DMA (1 case). In 5 cases the state developed after a single dose was taken, in 2 after two doses were taken and in 4 after less than ten doses (including one reported as ‘several times’). The remaining cases were regular users over months or years. Cannabis use was commented on in seven cases and alcohol use in one. As can be seen from Table 1, psychotic symptoms included delusions (referential, persecutory, religious, sexual and fantastic grandiose and guilty), hallucinations (auditory and visual), formal thought disorder, and affective flattening and incongruity; three cases had catatonic symptoms. There was evidence of a mood component to the illness in several cases: in 4 the state was associated with depressed mood and in 1 more there was prominent guilt and rumination; 3 more cases showed overactivity.

Table 1. PSE syndromes in 17 case reports of psychosis

The duration of the state was reported in 15 cases and ranged from a few days to 2 weeks in six cases (5, 10, 14, 15, 16, 17); from 3 to 6 weeks in two (12, 13); and from 2 to 6 months (or longer, given the reported lack of improvement) in seven (1, 3, 4, 6, 8, 9, 11). With respect to outcome, 11 cases recovered or were left with only minor symptoms (3, 4, 5, 9, 10, 11, 13, 14, 15, 16, 17). Three cases were described as improved (1, 6, 12) and two as unimproved (7, 8). A further patient committed suicide while acutely ill (case 2).

Affective disorder

There were 17 cases of affective disorder: 11 of depression, 3 of mania, and 3 of depression and mania in the same or different episodes (see Table 2). A majority of cases (12) occurred in the context of use of LSD, but there were also cases associated with use of ayahuasca (2), lysergic acid amide (1), mescaline (1, with some doubt about whether this was the drug taken) and psilocybin (1). Six cases developed after only a single dose was taken, 1 after two doses, 1 after three doses, 1 after four doses, 2 after five doses, and the remainder after multiple or unknown numbers of doses. Psychotic symptoms were present in seven cases. Concurrent cannabis use was noted in eight cases. Alcohol use was commented on in three cases with one more patient having drunk heavily up to a year previously.

Table 2. PSE syndromes in 17 cases of affective disorder

There were no cases with brief durations (≤2 weeks). Duration ranged from between 2–3 weeks and 2 months in nine cases (18, 21, 23, 25, 28, 31, 32, 33, 34), and from 3 to 12 months in seven cases (19, 22, 24, 26, 27, 29, 30). One patient committed suicide after making an apparent full recovery following approximately 4 months of illness (case 20). Not including this last case, the outcome was reported as recovery with or without minor symptoms in 13 cases (18, 19, 21, 22, 23, 24, 25, 27, 28, 29, 31, 32, 33), or improvement in 3 cases (26, 30, 34).

Two patients who developed depression also experienced flashbacks, but there was little to suggest that these played a causal role: case 27 had had only four flashbacks and in case 26, flashbacks were only discovered on questioning and appeared to be independent of the mood symptoms.

Other psychiatric disorders

There were three cases of anxiety disorders precipitated by psychedelic use, two with LSD (McGennis, Reference McGennis1979; Shick & Smith, Reference Shick and Smith1970) and one with psilocybin (Benjamin, Reference Benjamin1979). All three cases took the form of generalized anxiety, accompanied by panic attacks in one of them. The state occurred after taking the drug three times, ‘a number of times’ or (probably) many times. There were few details concerning duration or degree of recovery.

There was one case of depersonalization and derealization (Abraham & Mamen, Reference Abraham and Mamen1996). This developed in an 18-year-old male a week after he took the last of 6–8 doses of LSD. The symptoms developed in association with flashbacks but then became persistent. The state persisted for 20 years, at which point he developed depression and anxiety. Drug treatment brought about only at most minor improvement.

One case could not be classified (Harley-Mason et al., Reference Harley-Mason, Laird and Smythies1958): two weeks after taking mescaline for research purposes, a man had a five-day period of continuously experiencing patterned visual experiences, only this time muddy rather than bright as previously. The state was accompanied by generally dulled perception, unease, loss of appetite and a feeling of physical and mental exhaustion.

Flashbacks/HPPD

Twenty-nine includable case reports were found. They were mainly reported in association with LSD use (21 cases), with the remaining drugs being psilocybin (2 cases), mescaline (2 cases) and multiple/unspecified psychedelic drugs (4 cases). Cannabis was also used in 9 cases, and alcohol use was recorded in 5.

In 7 cases flashbacks began occurring after only a single dose of the drug was taken, in 1 after two doses were taken, in 2 after use that was sporadic (‘occasional’ or ‘several times’); in the remainder the drug was taken from 6 to 180 times. In over half (15 of 23 cases where information was provided or implied) the symptom resolved within a year after stopping taking psychedelics, with or without treatment. However, cases were also reported with durations of 2, 3, 8, 14, 22, 23 and 25 years.

Details of the features of the flashbacks are given in Table 3. It can be seen that visual afterimages (also referred to as trailing and palinopsia) was the most common perceptual experience, with other elementary visual changes and distortions, such as patterns, flashes of light and color, shimmering and halos round objects occurring less frequently. Unexpectedly, there were descriptions of formed images, including of animals, human figures, and inanimate objects in ten cases. Auditory experiences, ranging from distortions of real sounds to elementary sounds to unintelligible whispers, were described in four cases, and somatosensory disturbances in two. Experiences of unreality and/or depersonalization were reported in 6 cases.

Table 3. Flashback phenomena as described in 29 case reports

1. Kawasaki and Purvin (Reference Kawasaki and Purvin1996); 2. Lerner, Oyefe, Isaacs, and Sigal (Reference Lerner, Oyefe, Isaacs and Sigal1997); 3. Anderson and O'Malley (Reference Anderson and O'Malley1972); 4. Horowitz (Reference Horowitz1964); 5. Haslacher, Novkovic, Buthut, Heinz, and Soekadar (Reference Haslacher, Novkovic, Buthut, Heinz and Soekadar2022); 6. Abraham and Mamen (Reference Abraham and Mamen1996); 7. Kaminer and Hrecznyj (Reference Kaminer and Hrecznyj1991); 8. Noushad, Al Hillawi, Siram, and Arif (Reference Noushad, Al Hillawi, Siram and Arif2015); 9. Twemlow and Bowen (Reference Twemlow and Bowen1979); 10. Cohen and Ditman (Reference Cohen and Ditman1963); 11. Espiard, Lecardeur, Abadie, Halbecq, and Dollfus (Reference Espiard, Lecardeur, Abadie, Halbecq and Dollfus2005); 12. Young (Reference Young1997); 13. Smith and Seymour (Reference Smith and Seymour1985); 14. Rosenthal (Reference Rosenthal1964); 15. Kleber (Reference Kleber1967); 16. Markel et al. (Reference Markel, Lee, Holmes and Domino1994); 17. Charre et al. (Reference Charre, Herrero, Martelli and Benyamina2020); 18. Lerner and Ran (Reference Lerner and Ran2015); 19. Harley-Mason et al. (Reference Harley-Mason, Laird and Smythies1958); 20. Scott (Reference Scott1971); 21.Skryabin, Vinnikova, Nenastieva, and Alekseyuk (Reference Skryabin, Vinnikova, Nenastieva and Alekseyuk2018); 22. Horowitz (Reference Horowitz1970); 23. Lerner, Skladman, Kodesh, Sigal, and Shufman (Reference Lerner, Skladman, Kodesh, Sigal and Shufman2001).

Twelve of the 29 cases showed associated psychiatric symptomatology that persisted beyond the flashbacks. Anxiety outlasting or occurring outside flashback periods were present in five cases, usually but not always related to fear of having an attack. Eight patients developed persistent depressive symptoms in response to flashbacks. One patient developed hypochondriasis, becoming convinced he had Creutzfeldt-Jakob disease because of his flashback symptoms (Charre, Herrero, Martelli, & Benyamina, Reference Charre, Herrero, Martelli and Benyamina2020). This patient also experienced depersonalization/derealization that probably outlasted the flashbacks. In one case (Lerner & Ran, Reference Lerner and Ran2015) the only associated psychiatric symptom was worry.

In a further 6 cases anxiety was only experienced during the flashbacks themselves. In 3 cases it was unclear when the anxiety occurred. One further case (Abraham & Mamen, Reference Abraham and Mamen1996, also reported in the ‘other psychiatric disorders section) developed persistent depersonalization/derealization with persistent flashbacks after taking LSD 6–8 times; 20 years later he also developed depression and anxiety.

Among the remaining 11 cases no associated psychiatric symptomatology was noted. Three of these cases were in an ophthalmological journal, and the others more gave few details of any kind, leaving open the question of whether psychiatric symptoms were simply not reported.

Discussion

This systematic review found credible case reports of an association between use of psychedelic drugs and schizophrenia spectrum psychosis, and similar case reports of an association with affective disorder, including both depression and bipolar disorder. Both types of disorder were seen in individuals without a previous psychiatric history and were not, or at least were not wholly, attributable to concurrent use of other drugs, since we excluded cases where there was co-existent substance use apart from alcohol and cannabis.

Our ability to find only 17 case reports of psychosis in individuals who used psychedelic drugs contrasts with a relatively entrenched view in psychiatry and society as a whole that such drugs are strongly associated with this form of psychiatric disorder. For example, several well-known rock musicians who developed schizophrenia are widely considered to be ‘acid casualties’. It also contrasts with a previous study: Smart and Bateman (Reference Smart and Bateman1967) reported that they had been able to trace reports of 225 adverse reactions to LSD, of which 142 took the form of prolonged psychotic reactions. However, how this number was arrived at was not explained by the authors, and it seems probable that they included sources beyond case reports, e.g. counting patients who had participated in clinical studies of LSD psychosis. One possible reason for the relative paucity of case reports we found is that we were strict about excluding cases where other drugs (apart from cannabis) were also used. Another could be that interest in psychosis as a complication of psychedelic use was at its highest at a time when the concept of schizophrenia was broad, i.e. before the introduction of DSM-III in 1980. However, it has to be said we did not have to exclude many cases for this latter reason.

As noted in the introduction, a longstanding view has been that affective disorder is not a significant complication of psychedelic drug use. When such states have been commented on, they have mostly been considered to take the form of depression, with one review documenting only a single case of a ‘motor excitatory’ state (Smart & Bateman, Reference Smart and Bateman1967). In contrast we found as many case reports of affective disorder as of schizophrenia spectrum disorder. Such a finding is arguably not unexpected, given that psychedelics exert their effect on the serotonin system, which has been implicated, and continues to be implicated, in depression for over 50 years (Jauhar, Cowen, & Browning, Reference Jauhar, Cowen and Browning2023). Serotonin has also been implicated in bipolar disorder, albeit with less consistent findings (Mahmood & Silverstone, Reference Mahmood and Silverstone2001), and with little investigation in recent years. Nevertheless, the ‘bidirectionality’ of the association, i.e. the existence of case reports of both depression and mania after psychedelic drug use, goes against any simplistic conceptualization of the link with serotonin, if there is one.

Could it be that the major psychiatric association of psychedelic drug use is actually with affective disorder, with cases of schizophrenia spectrum disorder being largely or wholly the result of misdiagnosis? While in some ways attractive, this is probably not a tenable position, for two reasons. Firstly, while affective symptoms were present in a proportion of the schizophrenia spectrum cases we found, there were other cases where no affective component was discernible from the descriptions given. Secondly, psychedelic drugs are capable of inducing psychotic symptoms during intoxication itself. Thus, Klee and Weintraub (Reference Klee, Weintraub, Bradley, Deniker and Radouco-Thomas1959) reported four healthy volunteers who developed sometimes quite elaborate persecutory and referential delusions, and in one case auditory hallucinations, when given LSD under experimental conditions. There is also contemporary evidence to the same effect: Griffiths et al. (Reference Griffiths, Johnson, Richards, Richards, McCann and Jesse2011) described the occurrence of delusions or paranoid thinking in 8 of 18 volunteers while taking psilocybin; examples included believing that a person close to the participant had died, or that the experimenters were malevolently manipulating them. It also seems probable that at least some of the (fortunately rare) cases of individuals who jumped to their deaths, otherwise harmed themselves or committed murder while taking psychedelic drugs (e.g. Asselborn, Wennig, & Yegles, Reference Asselborn, Wennig and Yegles2000; Blacha et al., Reference Blacha, Schmid, Gahr, Freudenmann, Plener, Finter and Schonfeldt-Lecuona2013; Le Dare, Gicquel, Baert, Morel, & Bouvet, Reference Le Dare, Gicquel, Baert, Morel and Bouvet2020; Reich & Hepps, Reference Reich and Hepps1972) did so in response to delusions and/or hallucinations.

Two contemporary population surveys (Johansen & Krebs, Reference Johansen and Krebs2015; Krebs & Johansen, Reference Krebs and Johansen2013) found no evidence that recreational use of psychedelics was associated with increased rates of poor mental health, as indexed in various ways. Similarly, a 2020 meta-analysis of 24 studies that examined post-acute effects of psilocybin, ayahuasca and LSD given in clinical or experimental settings (Goldberg et al., Reference Goldberg, Shechet, Nicholas, Ng, Deole, Chen and Raison2020) found no evidence of any more than transient adverse effects. Our findings, whilst not directly comparable in terms of methodology, paint a different picture: psychedelic drugs, even when taken only one or a few times, can be followed by major psychiatric adverse events. A recent study using a different methodology from ours also had findings that could be seen as pointing in the same direction. Bremler, Katati, Shergill, Erritzoe, and Carhart-Harris (Reference Bremler, Katati, Shergill, Erritzoe and Carhart-Harris2023) advertised on social media for individuals who had experienced negative psychological effects after taking psychedelics or MDMA lasting for longer than 72 hours. Those who reported the most severe adverse effects were then invited for an in-person interview. Fifteen participants took part in this second phase, of whom seven took psychedelics only (i.e. not MDMA), and had no previous history of major psychiatric illness. The symptoms they described included anxiety/panic, depression, loss of the ability to experience pleasure, suicidal thoughts, intrusive or obsessive thoughts and behaviors, as well as paranoia/delusional thinking, derealization, distractibility and elevated mood in one case. Two users were diagnosed with bipolar disorder after taking LSD, although both reported experiencing similar symptoms prior to consumption.

Our review of case reports adds detail to the existing, rather sparse descriptive literature on flashbacks. Notably, the experiences described went beyond the conventional view that they take the form simply of ‘psychedelic’ visual phenomena like geometric patterns, distortions and afterimages, but instead could sometimes include formed and sometimes complex images, as well as auditory and occasionally somatosensory experiences. Our findings here are in line with those of Vis, Goudriaan, Ter Meulen, and Blom (Reference Vis, Goudriaan, Ter Meulen and Blom2021) who systematically reviewed case reports of HPPD/flashbacks, employing a similar but broader strategy than ours, including MDMA- and cannabis-related experiences and not excluding cases where there was comorbid major psychiatric illness or a history of other drug use. They found formed visual hallucinations, such as faces, skulls, and animals in 9.3% of cases.

We additionally found that flashbacks were not only a consequence of prolonged use of psychedelics but, as with psychosis and major affective disorder, could sometimes develop after taking such drugs only one or a few times. This finding contrasts with those of a questionnaire survey of healthy subjects who took psilocybin between 1 and 4 times as part of a series of experimental studies (Studerus, Kometer, Hasler, & Vollenweider, Reference Studerus, Kometer, Hasler and Vollenweider2011), which found that only 1 of 90 participants reported the occurrence of flashback-like visual phenomena, and that these were infrequent, brief, and ceased within three days after taking the drug. Rates were higher in another study (Muller et al., Reference Muller, Kraus, Holze, Becker, Ley, Schmid and Borgwardt2022), which found that 13 of 142 healthy volunteers who took part in clinical trials of LSD or psilocybin and who had used illicit drugs apart from cannabis no more than 10 times reported flashbacks after participating. The experiences were mostly pleasant or neutral in this study.

The case report literature supports the view that flashbacks are commonly associated with psychiatric symptomatology, and this mostly takes the form of anxiety and depression. Depression, in particular, could sometimes become persistent. Anxiety could accompany the flashbacks themselves, but sometimes extended beyond them to a fear of developing an attack. Our findings remain open on the issue of whether flashbacks are ever ‘benign’, i.e. that they occur without the distress or interference with functioning that would lead to a diagnosis of HPPD: we found 11 out of 29 case reports where no associated psychiatric symptomatology was reported (and one more where the only symptom was worry). However, there are grounds for suspecting that relevant psychiatric description was simply lacking in some of these cases.

In conclusion, this systematic review of case studies supports the view that both psychosis and major affective disorder subsequent to psychedelic drug use exist, highlighting a potential risk in the therapeutic application of these drugs if they are ever approved, and more generally in recreational use. The major limitation of a review of this type is that, while it can say something about the nature of the individual psychiatric complications encountered, it cannot establish rates for their occurrence. Another limitation is that we were unable to apply diagnostic criteria to the case material; because of the wide variation in the richness of the clinical detail provided, this would have resulted in an unacceptably high number of unclassifiable diagnoses. Finally, due to the vagaries of reporting, it is possible that some of the cases included may have been in individuals who used other drugs besides psychedelics. Social and psychological factors contributing to the emergence of psychiatric disorders in response to psychedelic use would also be likely to have been under-reported, if they were reported at all.

Supplementary material

The supplementary material for this article can be found at https://doi.org/10.1017/S0033291724002496.

Acknowledgements

We thank Sui McKenna and Martin Lepage for their translation of articles. James Rucker's contribution represents independent research part-funded by the National Institute for Health Research (NIHR) Biomedical Research Centre at South London and Maudsley NHS Foundation Trust and King's College London. Funding was provided by Ministerio de Salud, Plan Nacional de Drogas proj. 2021|066 and 2020|065.

Competing interests

J. R. has undertaken paid advisory boards for Clerkenwell Health (Past), Beckley PsyTech (Past), Delica Therapeutics (Past), paid articles for Janssen, received assistance for attendance at conferences from Compass Pathways (past) and Janssen, and received grant funding (managed by King's College London) from Compass Pathfinder, Beckley PsyTech, Multidisciplinary Association for Psychedelic Studies, National Institute for Health Research, Wellcome Trust, Biomedical Research Centre at the South London and Maudsley NHS Foundation Trust. J. R. is co-director for the Centre for Mental Health Research & Innovation, a research collaboration between King's College London, the South London & Maudsley NHS Foundation Trust and Compass Pathways investigating the safety and efficacy of psilocybin treatment. J. R. has no shareholdings in pharmaceutical companies and no shareholdings in companies developing psychedelics. The views expressed are those of this author and not necessarily those of the NHS, the NIHR, or the Department of Health. No award/grant number is applicable. For the purposes of open access, the author has applied a Creative Commons Attribution (CC BY) license to any Accepted Author Manuscript version arising from this submission. S. J. has received honoraria for educational talks given for Lundbeck, Sunovian, Boehringer-Ingelheim, and Janssen. He is a Council Member (unpaid) of the British Association for Psychopharmacology. He has sat as an advisor on panels for the Wellcome Trust and NICE. He has consulted for LB Pharmaceuticals. The remaining authors declare no conflicts of interest.

Footnotes

*

These authors contributed equally to this work.

References

Abraham, H. D., & Mamen, A. (1996). LSD-like panic from risperidone in post-LSD visual disorder. Journal of Clinical Psychopharmacology, 16, 238241.CrossRefGoogle ScholarPubMed
Alcantarilla, L., García-Alcarria, E., & Almonacid, C. (2022). Episodios psicóticos inducidos por ayahuasca: Revisión sistemática a partir de un caso. Revista de Neuro-Psiquiatría, 85, 224234.CrossRefGoogle Scholar
Alper, K. R. (2001). Ibogaine: A review. The Alkaloids: Chemistry and Biology, 56, 249281.Google ScholarPubMed
Anderson, W. H., & O'Malley, J. E. (1972). Trifluoperazine for the ‘trailing’ phenomenon. Journal of the American Medical Association, 220, 12441245.Google ScholarPubMed
Asselborn, G., Wennig, R., & Yegles, M. (2000). Tragic flying attempt under the influence of ‘magic mushrooms’. Problems of Forensic Sciences, XLII, 4146.Google Scholar
Benjamin, C. (1979). Persistent psychiatric symptoms after eating psilocybin mushrooms. British Medical Journal, 1, 13191320.CrossRefGoogle ScholarPubMed
Blacha, C., Schmid, M. M., Gahr, M., Freudenmann, R. W., Plener, P. L., Finter, F., … Schonfeldt-Lecuona, C. (2013). Self-inflicted testicular amputation in first lysergic acid diethylamide use. Journal of Addiction Medicine, 7, 8384.CrossRefGoogle ScholarPubMed
Braconnier, A., & Schmit, G. (1979). [Acute psychoses and LSD in adolescents]. Psychiatrie de l' Enfant, 22, 431472.Google ScholarPubMed
Bremler, R., Katati, N., Shergill, P., Erritzoe, D., & Carhart-Harris, R. L. (2023). Case analysis of long-term negative psychological responses to psychedelics. Scientific Reports, 13, 15998.CrossRefGoogle ScholarPubMed
Carhart-Harris, R., Giribaldi, B., Watts, R., Baker-Jones, M., Murphy-Beiner, A., Murphy, R., … Nutt, D. J. (2021). Trial of psilocybin versus escitalopram for depression. New England Journal of Medicine, 384, 14021411.CrossRefGoogle ScholarPubMed
Charre, M., Herrero, H., Martelli, C., & Benyamina, A. (2020). [Hallucinogen perception persisting disorder: Discussion about a clinic situation]. L'Encephale, 46, 408409.CrossRefGoogle ScholarPubMed
Ching, T. H. W., Amoroso, L., Bohner, C., D'Amico, E., Eilbott, J., Entezar, T., … Kelmendi, B. (2023a). Safety, feasibility, tolerability, and clinical effects of repeated psilocybin dosing combined with non-directive support in the treatment of obsessive-compulsive disorder: Protocol for a randomized, waitlist-controlled trial with blinded ratings. Frontiers in Psychiatry, 14, 1278823.CrossRefGoogle ScholarPubMed
Ching, T. H. W., Grazioplene, R., Bohner, C., Kichuk, S. A., DePalmer, G., D'Amico, E., … Kelmendi, B. (2023b). Safety, tolerability, and clinical and neural effects of single-dose psilocybin in obsessive-compulsive disorder: Protocol for a randomized, double-blind, placebo-controlled, non-crossover trial. Frontiers in Psychiatry, 14, 1178529.CrossRefGoogle ScholarPubMed
Cohen, S. (1960). Lysergic acid diethylamide: Side effects and complications. Journal of Nervous and Mental Disease, 130, 3040.CrossRefGoogle ScholarPubMed
Cohen, S. (1964). Suicide following morning glory seed ingestion. American Journal of Psychiatry, 120, 10241025.CrossRefGoogle ScholarPubMed
Cohen, S. (1966). A classification of LSD complications. Psychosomatics, 7, 182186.CrossRefGoogle ScholarPubMed
Cohen, S. (1985). LSD: The varieties of psychotic experience. Journal of Psychoactive Drugs, 17, 291296.CrossRefGoogle ScholarPubMed
Cohen, S., & Ditman, K. S. (1963). Prolonged adverse reactions to lysergic acid diethylamide. Archives of General Psychiatry, 8, 475480.CrossRefGoogle ScholarPubMed
Cooper, H. A. (1955). Hallucinogenic drugs. Lancet, 268, 10781079.CrossRefGoogle ScholarPubMed
Dos Santos, R. G. (2011). Ayahuasca and psychosis. In dos Santos, R. G. (Ed.), The ethnopharmacology of ayahuasca (pp. 9799). Trivandrum, Kerala: Transworld Research Network.Google Scholar
Espiard, M. L., Lecardeur, L., Abadie, P., Halbecq, I., & Dollfus, S. (2005). Hallucinogen persisting perception disorder after psilocybin consumption: A case study. European Psychiatry, 20, 458460.CrossRefGoogle ScholarPubMed
Fink, P. J., Goldman, M. J., & Lyons, I. (1966). Morning glory seed psychosis. Archives of General Psychiatry, 15, 209213.CrossRefGoogle Scholar
Flach, C. (1967). [A case of morning-glory-(ipomoea)-seed psychosis]. Nordisk Psykiatrisk Tidsskrift (Nordic Journal of Psychiatry), 21, 313321.CrossRefGoogle ScholarPubMed
Fookes, B. H. (1972). Psychosis after L.S.D. Lancet, 1, 10741075.CrossRefGoogle ScholarPubMed
Glass, G. S. (1973). Psychedelic drugs, stress, and the ego. The differential diagnosis of psychosis associated with psychotomimetic drug use. Journal of Nervous and Mental Disease, 156, 232241.CrossRefGoogle ScholarPubMed
Glass, G. S., & Bowers, M. B. Jr. (1970). Chronic psychosis associated with long-term psychotomimetic drug abuse. Archives of General Psychiatry, 23, 97103.CrossRefGoogle ScholarPubMed
Goldberg, S. B., Shechet, B., Nicholas, C. R., Ng, C. W., Deole, G., Chen, Z., & Raison, C. L. (2020). Post-acute psychological effects of classical serotonergic psychedelics: A systematic review and meta-analysis. Psychological Medicine, 50, 26552666.CrossRefGoogle ScholarPubMed
Goodwin, G. M., Aaronson, S. T., Alvarez, O., Arden, P. C., Baker, A., Bennett, J. C., … Malievskaia, E. (2022). Single-dose psilocybin for a treatment-resistant episode of major depression. New England Journal of Medicine, 387, 16371648.CrossRefGoogle ScholarPubMed
Griffiths, R. R., Johnson, M. W., Richards, W. A., Richards, B. D., McCann, U., & Jesse, R. (2011). Psilocybin occasioned mystical-type experiences: Immediate and persisting dose-related effects. Psychopharmacology (Berlin), 218, 649665.CrossRefGoogle ScholarPubMed
Harley-Mason, J., Laird, A. H., & Smythies, J. R. (1958). The metabolism of mescalin in the human; delayed clinical reactions to mescalin. Confinia Neurologica, 18, 152155.CrossRefGoogle Scholar
Haslacher, D., Novkovic, N., Buthut, M., Heinz, A., & Soekadar, S. R. (2022). Pathological delta oscillations in hallucinogen persisting perception disorder: A case report. Frontiers in Psychiatry, 13, 867314.CrossRefGoogle ScholarPubMed
Hatrick, J. A., & Dewhurst, K. (1970). Delayed psychosis due to L.S.D. Lancet, 2, 742744.CrossRefGoogle ScholarPubMed
Hoffer, A., & Callbeck, M. J. (1960). Drug-induced schizophrenia. Journal of Mental Science, 106, 138159.CrossRefGoogle ScholarPubMed
Holze, F., Gasser, P., Muller, F., Dolder, P. C., & Liechti, M. E. (2023). Lysergic acid diethylamide-assisted therapy in patients with anxiety with and without a life-threatening illness: A randomized, double-blind, placebo-controlled phase ii study. Biological Psychiatry, 93, 215223.CrossRefGoogle Scholar
Horowitz, M. J. (1964). The imagery of visual hallucinations. Journal of Nervous and Mental Disease, 138, 513523.CrossRefGoogle ScholarPubMed
Horowitz, M. J. (1970). Image formation and cognition. London: Butterworths/Appleton-Century-Crofts.Google Scholar
Hyde, C., Glancy, G., Omerod, P., Hall, D., & Taylor, G. S. (1978). Abuse of indigenous psilocybin mushrooms: A new fashion and some psychiatric complications. British Journal of Psychiatry, 132, 602604.CrossRefGoogle ScholarPubMed
Iversen, L. (2008). Speed, ecstasy, ritalin: The science of amphetamines. Oxford: Oxford University Press.CrossRefGoogle Scholar
Jauhar, S., Cowen, P. J., & Browning, M. (2023). Fifty years on: Serotonin and depression. Journal of Psychopharmacology, 37, 237241.CrossRefGoogle ScholarPubMed
Johansen, P. O., & Krebs, T. S. (2015). Psychedelics not linked to mental health problems or suicidal behavior: A population study. Journal of Psychopharmacology, 29, 270279.CrossRefGoogle ScholarPubMed
Jørgensen, F. (1968). Psykotiske reaktioner ved LSD-misbrug. Nordisk Psykiatrisk Tidsskrift, 22, 2031.CrossRefGoogle Scholar
Kaminer, Y., & Hrecznyj, B. (1991). Lysergic acid diethylamide-induced chronic visual disturbances in an adolescent. Journal of Nervous and Mental Disease, 179, 173174.CrossRefGoogle ScholarPubMed
Kawasaki, A., & Purvin, V. (1996). Persistent palinopsia following ingestion of lysergic acid diethylamide (LSD). Archives of Ophthalmology, 114, 4750.CrossRefGoogle ScholarPubMed
Klawans, H. L., Tanner, C. M., & Goetz, C. G. (1979). Psychiatric reaction to ergot derivatives. In Fuxe, K., & Calne, D. B. (Eds.), Dopaminergic ergot derivatives and motor function (pp. 405414). Oxford: Pergamon.CrossRefGoogle Scholar
Kleber, H. (1967). Prolonged adverse reactions from unsupervised use of hallucinogenic drugs. Journal of Nervous and Mental Disease, 144, 308319.CrossRefGoogle Scholar
Klee, G. D., & Weintraub, W. (1959). Paranoid reactions following lysergic acid diethylamide (LSD-25). In Bradley, P. B., Deniker, P., & Radouco-Thomas, C. (Eds.), Neuro-psychopharmacology: Proceedings of the first international congress of neuro-psychopharmacology, Rome, September 1958 (pp. 457460). Amsterdam: Elsevier.Google Scholar
Krebs, T. S., & Johansen, P. O. (2013). Psychedelics and mental health: A population study. PLoS One, 8, e63972.CrossRefGoogle ScholarPubMed
Lake, C. R., Stirba, A. L., Kinneman, R. E. Jr., Carlson, B., & Holloway, H. C. (1981). Mania associated with LSD ingestion. American Journal of Psychiatry, 138, 15081509.Google ScholarPubMed
Le Dare, B., Gicquel, T., Baert, A., Morel, I., & Bouvet, R. (2020). Self-inflicted neck wounds under influence of lysergic acid diethylamide: A case report and literature review. Medicine (Baltimore), 99, e20868.CrossRefGoogle ScholarPubMed
Lerner, A. G., & Ran, S. L. (2015). LSD-associated ‘alice in wonderland syndrome’ (AIWS): A hallucinogen persisting perception disorder (HPPD) case report. Israel Journal of Psychiatry and Related Sciences, 52, 6769.Google Scholar
Lerner, A. G., Oyefe, I., Isaacs, G., & Sigal, M. (1997). Naltrexone treatment of hallucinogen persisting perception disorder. American Journal of Psychiatry, 154, 437.Google ScholarPubMed
Lerner, A. G., Skladman, I., Kodesh, A., Sigal, M., & Shufman, E. (2001). LSD-induced hallucinogen persisting perception disorder treated with clonazepam: Two case reports. Israel Journal of Psychiatry and Related Sciences, 38, 133136.Google ScholarPubMed
Lieberman, J. A. (2021). Back to the future – the therapeutic potential of psychedelic drugs. New England Journal of Medicine, 384, 14601461.CrossRefGoogle Scholar
Linken, A. (1971). Propranolol for L.S.D.-induced anxiety states. Lancet, 2, 10391040.CrossRefGoogle ScholarPubMed
Lu, B. Y., Woofter, C., & Escalona, R. (2004). A case of prolonged peyote-induced psychosis resolved by sleep. Journal of Clinical Psychiatry, 65, 14331434.CrossRefGoogle ScholarPubMed
Lyttle, T., Goldstein, D., & Gartz, J. (1996). Bufo toads and bufotenine: Fact and fiction surrounding an alleged psychedelic. Journal of Psychoactive Drugs, 28, 267290.CrossRefGoogle ScholarPubMed
Mahmood, T., & Silverstone, T. (2001). Serotonin and bipolar disorder. Journal of Affective Disorder, 66, 111.CrossRefGoogle ScholarPubMed
Markel, H., Lee, A., Holmes, R. D., & Domino, E. F. (1994). LSD flashback syndrome exacerbated by selective serotonin reuptake inhibitor antidepressants in adolescents. Journal of Pediatrics, 125, 817819.CrossRefGoogle ScholarPubMed
Mash, D. C. (2023). Iuphar – invited review – ibogaine – a legacy within the current renaissance of psychedelic therapy. Pharmacological Research, 190, 106620.CrossRefGoogle ScholarPubMed
McGennis, A. (1979). Psychiatric symptoms and hallucinogenic compounds. British Medical Journal, 2, 797.CrossRefGoogle ScholarPubMed
Metzner, R. (1979). A note on the treatment of LSD psychosis: A case report. Psychotherapy: Theory, Research and Practice, 6, 201205.CrossRefGoogle Scholar
Muller, F., Kraus, E., Holze, F., Becker, A., Ley, L., Schmid, Y., … Borgwardt, S. (2022). Flashback phenomena after administration of LSD and psilocybin in controlled studies with healthy participants. Psychopharmacology (Berlin), 239, 19331943.CrossRefGoogle ScholarPubMed
Neu, P. (2020). [Ayahuasca – religion, life-style or drug?]. Fortschritte der Neurologie Psychiatrie, 88, 669673.Google ScholarPubMed
Neyra-Ontaneda, D. (2017). Psicosis inducida por ayahuasca: Reporte de un caso. Revista de Neuro-Psiquiatría, 80, 265272.CrossRefGoogle Scholar
Nichols, D. E. (2016). Psychedelics. Pharmacological Reviews, 68, 264355.CrossRefGoogle ScholarPubMed
Noushad, F., Al Hillawi, Q., Siram, V., & Arif, M. (2015). 25 years of hallucinogen persisting perception disorder – a diagnostic challenge. British Journal of Medical Practitioners, 8, a805.Google Scholar
Opitz, E. (1963). Die klinische Therapie seelischer Störungen mit Lysergsäure. Psychiatrie, Neurologie und medizinische Psychologie, 15, 366372.Google Scholar
Raison, C. L., Sanacora, G., Woolley, J., Heinzerling, K., Dunlop, B. W., Brown, R. T., … Griffiths, R. R. (2023). Single-dose psilocybin treatment for major depressive disorder: A randomized clinical trial. Journal of the American Medical Association, 330, 843853.CrossRefGoogle ScholarPubMed
Reich, P., & Hepps, R. B. (1972). Homicide during a psychosis induced by LSD. Journal of the American Medical Association, 219, 869871.CrossRefGoogle ScholarPubMed
Reiff, C. M., Richman, E. E., Nemeroff, C. B., Carpenter, L. L., Widge, A. S., Rodriguez, C. I., … McDonald, W. M. (2020). Psychedelics and psychedelic-assisted psychotherapy. American Journal of Psychiatry, 177, 391410.CrossRefGoogle ScholarPubMed
Rosen, D. H., & Hoffman, A. M. (1972). Focal suicide: Self-enucleation by two young psychotic individuals. American Journal of Psychiatry, 128, 10091012.CrossRefGoogle ScholarPubMed
Rosenberg, C. M., & Eldred, B. (1968). L.S.D. Psychosis. Medical Journal of Australia, 1, 129131.CrossRefGoogle ScholarPubMed
Rosenthal, S. H. (1964). Persistent hallucinosis following repeated administration of hallucinogenic drugs. American Journal of Psychiatry, 121, 238244.CrossRefGoogle ScholarPubMed
Rucker, J. J. H., Iliff, J., & Nutt, D. J. (2018). Psychiatry & the psychedelic drugs. Past, present & future. Neuropharmacology, 142, 200218.CrossRefGoogle ScholarPubMed
Sandison, R. A., & Whitelaw, J. D. (1957). Further studies in the therapeutic value of lysergic acid diethylamide in mental illness. Journal of Mental Science, 103, 332343.CrossRefGoogle ScholarPubMed
Scarella, T. M., & Teslyar, P. (2019). Prolonged psychosis with catatonia due to 2,5-dimethoxy-4-bromoamphetamine: Case report and literature review. Psychosomatics, 60, 599602.CrossRefGoogle ScholarPubMed
Schwarz, C. J. (1968). The complications of LSD: A review of the literature. Journal of Nervous and Mental Disease, 146, 174186.CrossRefGoogle ScholarPubMed
Scott, M. E. (1971). The flashback phenomenon. Virginia Medical Monthly, 98, 317320.Google ScholarPubMed
Shick, J. F. E., & Smith, D. E. (1970). Analysis of the LSD flashback. Journal of Psychedelic Drugs, 3, 1319.CrossRefGoogle Scholar
Skryabin, V. Y., Vinnikova, M., Nenastieva, A., & Alekseyuk, V. (2018). Hallucinogen persisting perception disorder: A literature review and three case reports. Journal of Addictive Diseases, 37, 268278.CrossRefGoogle ScholarPubMed
Smart, R. G., & Bateman, K. (1967). Unfavourable reactions to LSD: A review and analysis of the available case reports. Canadian Medical Association Journal, 97, 12141221.Google ScholarPubMed
Smith, D. E., & Seymour, R. B. (1985). Dream becomes nightmare: Adverse reactions to LSD. Journal of Psychoactive Drugs, 17, 297303.CrossRefGoogle ScholarPubMed
Sobanski, E., Dalm, S., Sievers, L., Kulzer, T., Liesenfeld, H., Schmidt-Kittler, H., & Huss, M. (2021). Herbal high: Substance-induced psychosis after consumption of seeds of the hawaiian baby woodrose. Zeitschrift fur Kinder- und Jugendpsychiatrie und Psychotherapie, 49, 307311.CrossRefGoogle ScholarPubMed
Strassman, R. J. (1984). Adverse reactions to psychedelic drugs. A review of the literature. Journal of Nervous and Mental Disease, 172, 577595.CrossRefGoogle ScholarPubMed
Studerus, E., Kometer, M., Hasler, F., & Vollenweider, F. X. (2011). Acute, subacute and long-term subjective effects of psilocybin in healthy humans: A pooled analysis of experimental studies. Journal of Psychopharmacology, 25, 14341452.CrossRefGoogle ScholarPubMed
Suleiman, M., Basu, A., Belal, S., & Jacob, T. (2022). From mushrooms to myolysis: A case of rhabdo in psilocybin-induced mood and psychotic disorder. Journal of Nervous and Mental Disease, 210, 638639.CrossRefGoogle ScholarPubMed
Twemlow, S. W., & Bowen, W. T. (1979). Psychedelic drug-induced psychological crises: Attitudes of the ‘crisis therapist’. Journal of Psychedelic Drugs, 11, 331335.CrossRefGoogle ScholarPubMed
Vis, P. J., Goudriaan, A. E., Ter Meulen, B. C., & Blom, J. D. (2021). On perception and consciousness in HPPD: A systematic review. Frontiers in Neuroscience, 15, 675768.CrossRefGoogle ScholarPubMed
von Rotz, R., Schindowski, E. M., Jungwirth, J., Schuldt, A., Rieser, N. M., Zahoranszky, K., … Vollenweider, F. X. (2023). Single-dose psilocybin-assisted therapy in major depressive disorder: A placebo-controlled, double-blind, randomised clinical trial. EClinicalMedicine, 56, 101809.CrossRefGoogle ScholarPubMed
Wing, J. K., Cooper, J. E., & Sartorius, N. (1974). The measurement and classification of psychiatric symptoms. Cambridge: Cambridge University Press.Google Scholar
Young, C. R. (1997). Sertraline treatment of hallucinogen persisting perception disorder. Journal of Clinical Psychiatry, 58, 85.CrossRefGoogle ScholarPubMed
Figure 0

Figure 1. Flow chart of the results of the search process.

Figure 1

Table 1. PSE syndromes in 17 case reports of psychosis

Figure 2

Table 2. PSE syndromes in 17 cases of affective disorder

Figure 3

Table 3. Flashback phenomena as described in 29 case reports

Supplementary material: File

Yildirim et al. supplementary material

Yildirim et al. supplementary material
Download Yildirim et al. supplementary material(File)
File 138.3 KB