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From heavy cannabis use to psychosis: is it time to take action?

Published online by Cambridge University Press:  27 May 2021

L. Johnson-Ferguson*
Affiliation:
Jacobs Center for Productive Youth Development, University of Zurich, Zurich, Switzerland Psychiatric University Hospital, Zurich, Switzerland Department of Psychosis Studies, Institute of Psychiatry, King’s College London, London, UK
M. Di Forti
Affiliation:
Social, Genetic and Developmental Psychiatry Centre, Institute of Psychiatry, King’s College London, London, UK South London and Maudsley NHS Mental Health Foundation Trust, London, UK
*
*Address for correspondence: L. Johnson-Ferguson, Jacobs Center for Productive Youth Development, Andreasstrasse 15, 8050 Zurich, Switzerland. (Email: [email protected])
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Abstract

Cannabis is one of the most widely used recreational drugs among people with clinical psychosis, after nicotine and alcohol. There has been a debate in psychiatry about whether or not we can infer a cause-and-effect relationship between the use of cannabis and psychotic disorders. In this editorial, we first present and critically discuss the evidence to date of the association between heavy cannabis use and psychosis. We argue that while the biological mechanisms underlying individual susceptibility to develop a psychotic disorder following heavy cannabis use are still unknown, heavy cannabis use remains the most modifiable risk factor for the onset of psychotic disorders and for its clinical and functional outcome. This demands a clear move towards both primary and secondary prevention intervention to reduce the impact of heavy cannabis use on the incidence and prevalence of psychotic disorders.

Type
Editorial
Copyright
© The Author(s), 2021. Published by Cambridge University Press on behalf of The College of Psychiatrists of Ireland

Psychosis

Epidemiology

Psychotic disorders are prevalent in 0.7% of the UK population (Department of Health, 2016). A multi-site incidence rate (IR) study investigating six countries and a total of 17 catchment areas of people with first-episode psychosis found that IRs for psychotic disorders vary widely across Europe, with, for example, an eightfold variation of IRs found between Santiago in Spain and Paris in France (Jongsma et al., Reference Jongsma, Gayer-Anderson, Lasalvia, Quattrone, Mulè, Szöke, Selten, Turner, Arango, Tarricone and Berardi2018).

A wide range of genetic and environmental risk factors for psychotic disorders have been documented. Early-life risk factors include obstetric complications at birth and child abuse, and later-life risk factors include migration, childhood adversity, social disadvantage and urban living (Stilo et al., Reference Stilo, Di Forti and Murray2011). Cannabis use is the most consistently replicated environmental risk factor for psychotic disorders (Marconi et al., Reference Marconi, Di Forti, Lewis, Murray and Vassos2016).

Schizophrenia and psychotic disorders are highly heritable (Hilker et al., Reference Hilker, Helenius, Fagerlund, Skytthe, Christensen, Werge, Nordentoft and Glenthøj2018), and genome-wide association studies (GWAS) have found a number of genetic risk variants for psychosis (Ripke et al., Reference Ripke, Neale, Corvin, Walters, Farh, Holmans, Lee, Bulik-Sullivan, Collier, Huang and Pers2014). The genetic risk variants associated to psychosis can be summarised into polygenic risk scores (PRS) (Murray et al., Reference Murray, Lin, Austin, McGrath, Hickie and Wray2021) which are believed to mediate the effects of environmental risk factors (Murray et al., Reference Murray, Englund, Abi-Dargham, Lewis, Di Forti, Davies, Sherif, McGuire and D’Souza2017).

Cannabis-associated psychosis

Scepticism

One argument is that people experiencing early symptoms of psychosis self-medicate with cannabis as they experience negative symptoms of schizophrenia spectrum disorders such as anhedonia, and that cannabis use is indeed a prodromal or precursory sign of psychosis, a theory disputed by Murray et al. (Reference Murray, Englund, Abi-Dargham, Lewis, Di Forti, Davies, Sherif, McGuire and D’Souza2017). Indeed, similar reasons for using cannabis have been described by people with and without first-episode psychosis (Bianconi et al., Reference Bianconi, Bonomo, Marconi, Kolliakou, Stilo, Iyegbe, Muñoz, Homayoun, Mondelli, Luzi and Dazzan2016; Santacana & Pérez-Sola, Reference Santacana and Pérez-Solá2014; Green et al., Reference Green, Kavanagh and Young2004).

More recently, and consistently, GWAS have indicated a positive and strong correlation between both cannabis use initiation and cannabis use disorder (CUD) with schizophrenia (Johnson et al., Reference Johnson, Demontis, Thorgeirsson, Walters, Polimanti, Hatoum, Sanchez-Roige, Paul, Wendt, Clarke and Lai2020). This has led to question whether the association between cannabis use and psychotic disorders described by epidemiological studies might be confounded by genetic effects and indeed reverse causation.

Mendelian randomization (MR) studies have used the available genetic data from both schizophrenia and cannabis initiation GWAS, to test for a) a genetic causal association between cannabis use and schizophrenia and b) its direction: whether it is from cannabis use initiation to schizophrenia or vice versa. While MR findings have been mixed and the jury is still out, as discussed by Johnson et al. (Reference Johnson, Demontis, Thorgeirsson, Walters, Polimanti, Hatoum, Sanchez-Roige, Paul, Wendt, Clarke and Lai2020), genetic factors are likely to play an important role in the association between cannabis use and psychotic disorder (Giordano et al., Reference Giordano, Ohlsson, Sundquist, Sundquist and Kendler2015).

In contrast, data from the EU-GEI multisite case–control study, a European collaboration study including 10 sites plus one from Brazil, reported that frequent use of high-potency cannabis was associated with a fivefold increase in the risk for psychotic disorders, compared to never having used cannabis, independent of the genetic load for schizophrenia measured as PRS (Di Forti et al., Reference Di Forti, Wu-Choi, Quattrone, Richards, Freeman, Tripoli, Gayer-Anderson, Rodriguez, Jongsma, Ferraro and La Cascia2019a).

Epidemiological evidence

The first longitudinal case–control study investigating the association between cannabis use and psychosis was conducted on 45 570 Swedish military conscripts over 15 years (Andréasson et al., Reference Andréasson, Engström, Allebeck and Rydberg1987) following concerns of psychiatrists in Sweden about cannabis use in their patients with psychosis (Hamilton, Reference Hamilton2017). Frequent use of cannabis was defined as having consumed it more than 50 times in a lifetime. They found an adjusted odds ratio of 2.41 (95% confidence interval = 1.72–3.30) of schizophrenia among frequent users of cannabis at follow-up compared to non-users. Interestingly, 7% of conscripts refused to disclose their cannabis consumption, which may have been due to stigma associated to cannabis use and could have been a limiting factor in this study (Hamilton, Reference Hamilton2017).

A systematic review and meta-analysis of 11 cohort and case–control studies conducted in 2005 (Semple et al., Reference Semple, McIntosh and Lawrie2005) found an odds ratio of 2.9 (95% confidence interval = 2.4–3.6) of schizophrenia or schizophrenia-like psychotic illness associated with cannabis use. The dose–response relationship was found in some included studies that, similarly to the Swedish conscript study, had dichotomous categories for high and low use of cannabis (e.g., past and current use) and abuse and dependence as defined by the DSM-IV. A review published in 2007 of seven studies found similar results (Moore et al., Reference Moore, Zammit, Lingford-Hughes, Barnes, Jones, Burke and Lewis2007), with all studies included showing a dose–response effect of duration of use and frequency. A limitation of these meta-analyses is that they used only both extreme categories (e.g., highest level of use compared to no use of cannabis) to measure the overall effect sizes (Marconi et al., Reference Marconi, Di Forti, Lewis, Murray and Vassos2016).

A 2016 review of 18 studies and meta-analysis of 10 studies showed a dose–response effect of frequency of cannabis use and long-lasting psychotic disorders, with a 3.90 (95% confidence interval = 2.84 to 5.34) increase in risk for the heaviest users compared to non-users and a twofold increase in risk between the average cannabis-users and non-users (Marconi et al., Reference Marconi, Di Forti, Lewis, Murray and Vassos2016). An important strength of this study was that it re-examined raw data from studies included in order to use an exposure continuum of cannabis use as opposed to binary categories of cannabis use to measure the magnitude of effect. This revealed that the magnitude of effect was higher than that documented in previous meta-analyses that had only compared two extreme categories. In addition, studies that included participants suffering from psychosis symptoms at baseline were excluded, which the authors argue means that results are unlikely to be explained by psychosis symptoms leading to cannabis use. These data support a causal role of cannabis use on psychosis, whereby consuming higher amounts of cannabis leads to a higher risk of psychosis.

While this meta-analysis provides insights into the role of cannabis exposure, the role of the potency of the cannabis used was not accounted for. The potency of a type of cannabis here refers to its levels of delta-9-tetrahydrocannabinol (THC), to which the psychosis-inducing effects are attributed (Di Forti et al., Reference Di Forti, Morgan, Dazzan, Pariante, Mondelli, Marques, Handley, Luzi, Russo, Paparelli and Butt2009).

Clear evidence has shown that daily use of high-potency cannabis carries a fivefold increased risk for psychotic disorders (Di Forti et al., Reference Di Forti, Marconi, Carra, Fraietta, Trotta, Bonomo, Bianconi, Gardner-Sood, O’Connor, Russo and Stilo2015, Reference Di Forti, Quattrone, Freeman, Tripoli, Gayer-Anderson, Quigley, Rodriguez, Jongsma, Ferraro, La Cascia and La Barbera2019b); a risk that reached a ninefold increase in Amsterdam, where types of cannabis highly concentrated in THC are widely available (Di Forti et al., Reference Di Forti, Quattrone, Freeman, Tripoli, Gayer-Anderson, Quigley, Rodriguez, Jongsma, Ferraro, La Cascia and La Barbera2019b). Furthermore, findings from the EUGEI study indicated that the prevalence of use of high potency cannabis (THC ≥10%) and separately of daily use of cannabis among the population controls, representative of each site catchment area, contributed to explain the reported significant variations in rates of psychotic disorders across the study sites, even after controlling for age, gender and migration (Di Forti et al., Reference Di Forti, Quattrone, Freeman, Tripoli, Gayer-Anderson, Quigley, Rodriguez, Jongsma, Ferraro, La Cascia and La Barbera2019b). Moreover, this study calculated that 30% of the first-episode psychosis cases presenting to the South London site Mental Health services and 50% of those presenting to services in Amsterdam could have been prevented if high-potency forms of cannabis, such as ‘skunk’ had not been available to consumers. These findings support the view that for this significant proportion of people, who are likely to carry many other risk factors for psychosis, the use of high-potency cannabis represented the final risk factor that tipped them over the threshold into frank clinical psychosis.

Further evidence from this multisite study shows that patients in their first episode of psychosis who report having used high-potency cannabis daily presented with more positive symptoms compared to those who never used cannabis or used low-potency types (Quattrone et al., Reference Quattrone, Ferraro, Tripoli, La Cascia, Quigley, Quattrone, Jongsma, Del Peschio, Gatto, Gayer-Anderson and Jones2020).

These findings have public health implications because the potency of cannabis has increased in the UK and beyond in the last 40 years, from 5% THC or less in the 1970s to levels averaging 16–20% reported in by Freeman et al. (Reference Freeman, Craft, Wilson, Stylianou, ElSohly, Di Forti and Lynskey2020). Recent evidence report that in Denmark the incidence of dual diagnoses of schizophrenia and CUD rose in conjunction with the rise in cannabis use and of its THC content between 1994 and 2006 (Hjorthøj et al., Reference Hjorthøj, Larsen, Starzer and Nordentoft2019). Furthermore, forms of street cannabis containing cannabidiol (CBD) are becoming increasingly rare, while CBD-only products are now popular on the shelves of many UK health shops, advertised for their anxiolytic effects but without any evidence about the efficacy and safety (Chesney et al., Reference Chesney, McGuire, Freeman, Strang and Englund2020). The fact that potency is not measured in most of the epidemiological literature is an important research gap, and future studies need to measure potency as well as frequency of cannabis use.

Experimental studies

Cannabis contains more than 500 components, of which around 100 cannabinoids have been identified, the two most studied being THC and CBD (Pertwee, Reference Pertwee2014). These act on the endocannabinoid system of which the most important cannabinoid receptors are CB-1 and CB-2 (Lu and MacKie, Reference Lu and Mackie2016). Human laboratory studies have demonstrated that the administration of THC induces psychotic-like symptoms such as paranoia and cognitive impairment, which is mediated by action on the CB1 receptor (D’Souza et al., Reference D’Souza, Abi-Saab, Madonick, Forselius-Bielen, Doersch, Braley, Gueorguieva, Cooper and Krystal2005), while CBD counters this effect (Englund et al., Reference Englund, Morrison, Nottage, Hague, Kane, Bonaccorso, Stone, Reichenberg, Brenneisen, Holt and Feilding2013). Indeed functional magnetic resonance imaging data show that THC and CBD have opposite effects on regional brain function (Bhattacharyya et al., Reference Bhattacharyya, Morrison, Fusar-Poli, Martin-Santos, Borgwardt, Winton-Brown, Nosarti, O’Carroll, Seal, Allen and Mehta2010). The strength of laboratory studies is that they allow for causal inference to be made about the effect of different cannabinoids on psychotic symptoms in a controlled environment. However, while these studies demonstrate acute short-term effects of cannabinoids, they cannot explain the association between cannabis use and lasting psychosis. Neuroimaging evidence on this topic is mixed (Murray et al., Reference Murray, Englund, Abi-Dargham, Lewis, Di Forti, Davies, Sherif, McGuire and D’Souza2017), and more evidence is needed in order to make any claims about how cannabis may induce long-lasting psychosis.

It is important to note that new evidence from animal and human studies suggests that the CBD to THC ratio in cannabis plays an important role in its psychoactive properties, as CBD has been found to potentiate the effects of THC in certain doses (Freeman et al., Reference Freeman, Petrilli, Lees, Hindocha, Mokrysz, Curran, Saunders and Freeman2019). Future studies should aim to clarify the exact impact of different CBD doses on the effects of THC.

Adverse outcomes associated with continued cannabis use in people with psychosis

A meta-analysis found that patients who continue to use cannabis, and in particular those who use daily high potency cannabis after their first episode of psychosis, show a longer time spent in hospital, have higher rates of psychosis relapse and show more severe psychotic symptoms (Schoeler et al., Reference Schoeler, Monk, Sami, Klamerus, Foglia, Brown, Camuri, Altamura, Murray and Bhattacharyya2016). A 10-year follow-up study conducted in Spain found that patients who stop using cannabis after their first psychosis episode had similar remission rates to people who had never consumed cannabis (Setién-Suero et al., Reference Setién-Suero, Neergaard, Ortiz-García de la Foz, Suárez-Pinilla, Martínez-García, Crespo-Facorro and Ayesa-Arriola2019). These data show the importance of interventions reducing cannabis use in patients presenting with first-episode psychosis in order to improve their prognosis.

Cannabis withdrawal syndrome and cannabis dependence

Substance use disorders are characterised by dependence, which occurs when an individual experiences craving for the substance, withdrawal when they stop consuming it and show failed attempts to reduce consumption (American Psychiatric Association, 2013). Cannabis withdrawal symptoms include anxiety, disturbed sleep and decreases in appetite (Bonnet & Preuss, Reference Bonnet and Preuss2017). A review found that cannabis withdrawal syndrome (CWS) is prevalent in the majority of daily users of cannabis upon abrupt cessation (Budney et al., Reference Budney, Hughes, Moore and Vandrey2004). One study conducted in the United States found that 94.2% of 120 chronic cannabis users with schizophrenia reported withdrawal symptoms (Boggs et al., Reference Boggs, Kelly, Liu, Linthicum, Turner, Schroeder, McMahon and Gorelick2013).

On top of an association between cannabis potency and psychosis risk, there is evidence of an association between the potency of cannabis and cannabis dependence severity. A 16-year observational study in the Netherlands found a positive association between increases in cannabis potency and first-time cannabis admissions to specialist drug treatment (Freeman et al., Reference Freeman, van der Pol, Kuijpers, Wisselink, Das, Rigter, van Laar, Griffiths, Swift, Niesink and Lynskey2018). Furthermore, a study of 410 participants found that THC exposure was associated with cannabis dependence measured via self-report and clinician ratings of dependency (Curran et al., Reference Curran, Hindocha, Morgan, Shaban, Das and Freeman2019).

Treatments for cannabis use disorder in patients with psychotic disorders

While there are currently no recommended psychological interventions for cannabis use reduction and/or cessation and CWS in patients with co-morbid psychosis, some recent evidence suggests the possible effectiveness of cannabinoids agonists (Lintzeris et al., Reference Lintzeris, Bhardwaj, Mills, Dunlop, Copeland, McGregor, Bruno, Gugusheff, Phung, Montebello and Chan2019) or compounds able to modulate the endocannabinoid system (D’Souza et al., Reference D’Souza, Cortes-Briones, Creatura, Bluez, Thurnauer, Deaso, Bielen, Surti, Radhakrishnan, Gupta and Gupta2019) in patients with CUD. Harm reduction measures for non-medicinal cannabis use have been published, notably in Canada (Fischer et al., Reference Fischer, Jeffries, Hall, Room, Goldner and Rehm2011), encouraging, for example, people to opt for lower-potency cannabis forms and to reduce the frequency of consumption. However, for these guidelines to be effective, especially in a sample of people with psychosis and cannabis use who have been shown to struggle with engagement, they need to be turned into targeted interventions. Indeed, while we are able to offer several intervention strategies for tobacco smoking cessation, we still expect patients with psychotic disorders to stop their heavy cannabis use just because, we, psychiatrists and mental health professionals say so, ignoring their degree of dependence, as well as the withdrawal symptoms and craving that they are likely to experience.

The Circle Trial was the first to test whether combining contingency management with a psychoeducation package was more effective in the treatment of CUD in patients with first-episode psychosis than psychoeducation alone (Rains et al., Reference Rains, Marston, Hinton, Marwaha, Craig, Fowler, King, Omar, McCrone, Spencer and Taylor2019). Although the overall findings failed to show an advantage of the new intervention, the latter led to better outcomes in those who engaged throughout the trial. This underlines the importance of developing interventions able to successfully engage patients with first-episode psychosis.

Recently, in south London, thanks to the funding of the Maudsley Charity (https://maudsleycharity.org/), a new clinical service was developed to deliver an intervention for cannabis use reduction/cessation to young adults suffering their first episode of psychosis. The Cannabis Clinic for patients with Psychosis (CCP) (https://maudsleycharity.org/case-studies/cannabis-clinic/) is the first service in UK that combines the expertise of Early Intervention (EI) services in engaging patients at their first episode of psychosis with established addiction models. These encompass motivational interviewing, contingency management, psychoeducation, nicotine replacement therapy for the frequent co-morbid tobacco smoking and medications reviews when appropriate. The CCP has also developed a Peer group, currently running online because of the COVID19 pandemic, where patients referred to the CCP can attend small educational talks on cannabis dependence, on the effects of cannabis on mental health and overall well-being and share their lived experience of both psychosis and cannabis dependence. The Peer group is co-run by peer mentors who have recovered from cannabis-induced psychosis and stopped their cannabis use. By sharing their experience, they play a central role in this service. While it is too early to make conclusions about the effectiveness of the CCP, preliminary observations are encouraging. Given the robust evidence that indicate cannabis use as the most modifiable risk factor for poor clinical and functional outcome in psychosis, the work of the CCP should prompt us mental health professionals to bring together the existing recourses and expertise to provide support to patients with psychosis who are smoking cannabis and wish to stop.

Conclusion and future directions

Epidemiological studies consistently support heavy cannabis use as a component cause for developing psychosis and provide convincing evidence that both frequency of use and potency play important roles in this association.

Challenging social norms and widespread misconceptions such as the notion that cannabis cannot be harmful or addictive will be a crucial step forwards. As people who start using cannabis from a young age are more likely to develop CUD (Leung et.al, Reference Leung, Chan, Hides and Hall2020), which will make it harder for them to reduce their consumption if confronted with psychiatric illness, we need to address young people with the message that certain forms of cannabis can be harmful and cause dependence.

Therefore, while the underlying biological mechanisms of this association are still unclear and while we are still exploring the role of genetic variants in shaping individual susceptibility to the psychotogenic effects of heavy cannabis use, there is enough evidence to justify the development 1) of a public education campaign using engaging dissemination tools (e.g. social media platforms, school seminars, short movies) tailored to reach adolescents to inform them about the hazards of the frequent use of high potency cannabis on mental health and 2) of targeted interventions for people with first-episode psychosis who continue to use cannabis after the onset of their illness.

Conflict of interest

M Di Forti reports personal fees from Janssen, outside the submitted work.

Ethical standards

The authors assert that all procedures contributing to this work comply with the ethical standards of the relevant national and institutional committee on human experimentation with the Helsinki Declaration of 1975, as revised in 2008.

Financial support

This research received no specific grant from any funding agency, commercial or not-for-profit sectors.

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