Trial PaperAnxiety DisordersDepressive DisordersPalliative & End-of-Life DistressSafety & Risk ManagementPsilocybin

Psilocybin-assisted group therapy for demoralized older long-term AIDS survivor men: An open-label safety and feasibility pilot study

This open-label feasibility study (n=17) showed that psilocybin-assisted group therapy (21-25mg/70kg) was safe and effective for the treatment of demoralization in older long-term AIDS survivors.

Authors

  • Joshua Woolley
  • Gabrielle Agin-Liebes
  • Brian Anderson

Published

EClinicalMedicine
individual Study

Abstract

Background

Psilocybin therapy has shown promise as a rapid-acting treatment for depression, anxiety, and demoralization in patients with serious medical illness (e.g., cancer) when paired with individual psychotherapy. This study assessed the safety and feasibility of psilocybin-assisted group therapy for demoralization in older long-term AIDS survivor (OLTAS) men, a population with a high degree of demoralization and traumatic loss.

Methods

Self-identified gay men OLTAS with moderate-to-severe demoralization (Demoralization Scale-II ≥8) were recruited from the community of a major US city for a single-site open-label study of psilocybin-assisted group therapy comprising 8-10 group therapy visits and one psilocybin administration visit (0·3-0·36 mg/kg po). Primary outcomes were rate and severity of adverse events, and participant recruitment and retention. The primary clinical outcome was change in mean demoralization from baseline to end-of-treatment and to 3-month follow-up assessed with a two-way repeated measures ANOVA.

Findings

From 17 July 2017 to 16 January 2019, 18 participants (mean age 59·2 years (SD 4·4)) were enrolled, administered group therapy and psilocybin, and included in intent-to-treat analyses. We detected zero serious adverse reactions and two unexpected adverse reactions to psilocybin; seven participants experienced self-limited, severe expected adverse reactions. We detected a clinically meaningful change in demoralization from baseline to 3-month follow-up (mean difference -5·78 [SD 6·01], ηp2 = 0·47, 90% CI 0·21-0·60).

Interpretation

We demonstrated the feasibility, relative safety, and potential efficacy of psilocybin-assisted group therapy for demoralization in OLTAS. Groups may be an effective and efficient means of delivering psychotherapy pre- and post-psilocybin to patients with complex medical and psychiatric needs.

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Research Summary of 'Psilocybin-assisted group therapy for demoralized older long-term AIDS survivor men: An open-label safety and feasibility pilot study'

Editorial

βBlossom's Take

This pilot matters because it tests psilocybin in a group format and in a population marked by trauma, loss and age-related medical complexity, which sits a little outside the usual cancer-distress narrative. The open-label design keeps the claim modest, but it usefully extends the modern psilocybin literature into demoralisation and shows what delivery looks like when psychotherapy is shared rather than fully individual.

Introduction

Demoralization is described as existential suffering marked by helplessness, loss of meaning, and poor coping, and it is common among people with serious medical illnesses. Previous psychotherapies targeting demoralization have shown limited efficacy against active controls, and recent trials of psilocybin administered with adjunctive individual psychotherapy have demonstrated safety and durable symptomatic improvements for depression, anxiety and existential distress in patients with life-threatening illness. However, it is unknown whether psilocybin therapy can ameliorate demoralization in other clinical populations, or whether a group-based delivery model is feasible and safe. This pilot study sought to assess safety, feasibility, and preliminary clinical effects of psilocybin-assisted group therapy for demoralization in older long-term AIDS survivor (OLTAS) men, a population with substantial traumatic loss, social isolation and multimorbidity. Given the novelty of both the target population and the group-based approach, the investigators prioritised implementation outcomes (recruitment, tolerability, retention and protocol adherence) while treating clinical efficacy as exploratory.

Methods

Anderson and colleagues conducted a single-site, single-arm, open-label pilot study in an outpatient unit of an academic medical centre. The intervention combined preparatory individual sessions, a course of group psychotherapy, a single high-dose oral psilocybin administration session, and follow-up group and individual integration. Treatment spanned roughly seven weeks and comprised three hours of preparatory individual psychotherapy, 12–15 hours of group psychotherapy (90-minute sessions twice weekly), one eight-hour medication visit, and a two-hour individual integration session the day after drug administration. Three sequential cohorts were run, each with six participants and two therapists (total n = 18). Inclusion criteria required participants to be gay-identified, English-speaking cisgender men aged 50 or older who reported an HIV/AIDS diagnosis prior to the widespread availability of protease inhibitors (≈1996), and who scored ≥8 on the 16-item Demoralization Scale-II (DS-II). Standard exclusion criteria for psilocybin were adapted and applied, and cohort composition aimed to enhance homogeneity and rapid trust-building. Group therapy was adapted from Brief Supportive-Expressive Group Therapy (SEGT) with modifications for integration of the psilocybin session; sessions began and ended with brief breathing and guided mindfulness exercises. Crystalline psilocybin was dosed orally at 0.30 mg/kg for Cohort 1 and escalated to 0.36 mg/kg for Cohorts 2 and 3 after tolerability was established. Each participant had at least one of their group co-therapists act as a medication-session guide. Primary feasibility outcomes were recruitment and retention; safety was assessed via adverse event interviews at every visit, the Columbia-Suicide Severity Rating Scale (C-SSRS), the Challenging Experiences Questionnaire (ChEQ) after medication visits, and cardiovascular monitoring during sessions. The primary clinical outcome was change in mean demoralization (DS-II) from baseline to end-of-treatment and to 3-month follow-up. Secondary measures included PTSD symptoms (PCL-5), complicated grief (ICG-R), state anxiety, cognitive screening (MoCA), and substance use screens (AUDIT/DUDIT for later cohorts). Analyses were intent-to-treat with missing data handled by single imputation (baseline observation carried forward). Given the nested group design, two-way repeated measures ANOVAs with participants nested within cohorts were used, reporting partial eta squared (hp2) with 90% confidence intervals; a bias-corrected within-subject effect size (drm) with 95% CIs was also calculated for comparison with other studies.

Results

Eighteen participants were enrolled across three cohorts between July 2017 and August 2018; all 18 began the intervention, received psilocybin, completed the primary endpoint assessment and the 3-month safety follow-up, and were included in intent-to-treat analyses. Overall attendance at group therapy sessions was 95%. Absolute oral psilocybin doses ranged from 22 to 32 mg (mean 27.1 mg, SD 3.1). No psilocybin-related serious adverse events were reported. During medication sessions, 8 participants experienced moderate-to-severe anxiety reactions; four had paranoid reactions and one had a transient thought-disorder-like dissociation with repetitive self-talk. Hypertension was observed: four participants experienced self-limited severe, asymptomatic hypertension and eight had moderate hypertension; the two participants with severe hypertension met diagnostic criteria for borderline personality disorder (BPD). Fourteen participants had at least moderate expected adverse reactions to psilocybin, and seven experienced severe but self-limited expected reactions. Two unexpected post-medication reactions occurred: one participant had a moderate PTSD flashback two days later associated with nausea, tinnitus, panic and insomnia and was unable to work for two days; another participant reported severe anxiety ten days post-session, lapsed to methamphetamine use and subsequently withdrew from the intervention while completing most assessments. No change in suicidal ideation was detected on the C-SSRS and no suicidal behaviour occurred during the study. Participant-rated benefit at end-of-treatment averaged 6.61 (SD 0.6) on a 1–7 Likert scale, while perceived harm averaged 1.17 (SD 0.38). Mean ChEQ score was 37.11 (SD 26.0), approximately 28% of the maximum. Cognitive screening (MoCA) showed no meaningful change, and AUDIT/DUDIT scores (collected in Cohorts 2 and 3) did not worsen to 3-month follow-up. The pre-specified primary clinical outcome, demoralization (DS-II), showed robust pre–post improvement: mean difference baseline to end-of-treatment was −6.67 (SD 6.51), and baseline to 3-month follow-up was −5.78 (SD 6.01). Change across the three time points yielded a large effect (partial eta squared hp2 = 0.47, 90% CI 0.21–0.60). At end-of-treatment, 88.9% of participants had at least a 2-point reduction in DS-II; at 3 months this was 66.7%. Fifty percent and 33.3% of participants achieved >50% reduction in demoralization at end-of-treatment and 3 months, respectively. Most secondary clinical outcomes also improved over time except state anxiety (hp2 = 0.16, 90% CI 0.0–0.32) and antiretroviral adherence (hp2 = 0.08, 90% CI 0.0–0.22), the latter showing a ceiling effect with mean baseline adherence of 99%. Notable improvements were observed for PTSD symptoms (PCL-5, hp2 = 0.27, 90% CI 0.05–0.43) and complicated grief (ICG-R, hp2 = 0.45, 90% CI 0.19–0.58).

Discussion

The investigators conclude that psilocybin-assisted group therapy was feasible to deliver, relatively safe under the study conditions, and associated with preliminary improvements in demoralization and other measures of trauma-related distress in a sample of demoralized OLTAS men with substantial psychiatric comorbidity. Recruitment and retention were high and group attendance was excellent, although the sample was self-selected and many participants were highly motivated, retired or on disability, which may have facilitated participation. Compared with prior modern psilocybin trials that used individual psychotherapy, this cohort displayed greater clinical complexity and higher rates of non-serious adverse reactions; the authors attribute the elevated frequency and severity of expected adverse events in part to this complexity. Cardiovascular reactivity (moderate-to-severe hypertension) was more common than in some prior studies but generally resolved with non-pharmacological measures and clinician support; one participant with trauma history and BPD had prolonged severe hypertension that responded to environmental and interpersonal interventions. Two participants with BPD had challenging medication visits and difficulties integrating experiences in the group setting, although both reported short-term improvements post-treatment. The authors therefore recommend that high-complexity populations undergoing this protocol receive comparable levels of medical screening, preparatory work and post-drug psychotherapy. Effect-size estimates for demoralization compared favourably with effect sizes reported in pooled analyses of psilocybin trials for depression and with a large trial of non-psychedelic meaning-centred group psychotherapy for cancer patients. Nonetheless, the investigators acknowledge important limitations: small sample size, open-label uncontrolled design, potential selection bias (seven participants had substantial prior psychedelic experience), cohort differences in dose and number of group visits, and limited generalisability of findings beyond OLTAS men. The study team noted that stringent exclusion criteria needed for rigorous blinding (for example excluding individuals with any prior psychedelic use) would have been impractical for this population, which informed their decision not to include a placebo arm. Finally, the authors argue that group-based delivery may offer efficiency and therapeutic advantages for addressing social isolation and stigma, while emphasising the need for larger, randomised, well-blinded trials to determine efficacy and safety more definitively. They also highlight the unmet mental health needs of long-term AIDS survivors and call for further research into treatments for demoralization, complicated grief and trauma-related disorders in medically complex populations.

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RESULTS

Feasibility was assessed by rates of recruitment and retention of enrolled participants. Qualitative feedback on the tolerability of study procedures was also collected through a focus group that occurred after end-of-treatment. No prespecified criteria were used to judge whether to proceed to a future definitive trial. Safety was evaluated with multiple measures. Every study visit included an adverse events assessment interview and the Columbia Suicidality Severity Rating Scale (C-SSRS) interval interview. Adverse events assessments during the medication visit included spontaneous participant self-report, events observed by clinicians, and symptoms derived from the Challenging Experiences Questionnaire (ChEQ)administered the next day. During psilocybin sessions, blood pressure and heart rate were assessed at regular intervals of 30 min for the first two hours, and then 60 min thereafter. At end-oftreatment, participant perceptions of benefits and harms from the intervention were assessed by a 7-point Likert scale (1= none at all; 7=extremely). The Schedule of Attitudes towards Hastened Death (SAHD) was administered at baseline, end-of-treatment and 3-month follow-up. The Montreal Cognitive Assessment (MoCA) was performed at enrollment and end-of-treatment. Because they were added after Cohort 1 completed the study, only Cohorts 2 and 3 completed the Alcohol Use Disorder Identification Test (AUDIT) and Drug Use Disorders Identification Test (DUDIT) at baseline and at the 3-month follow-up with a 'last 3 month' recall period. The pre-specified primary clinical outcome measure was change in mean demoralization on the 16-item self-report DS-II with a 'last week' recall period. Data support using cut-off scores of 0À4 Low, 5À16 Medium and 17 High; and an improvement of 2/32 points is considered clinically meaningful in palliative care patients. Because the mental health needs of OLTAS are poorly characterized but likely multifaceted,we employed several secondary clinical outcome measures (see Supplemental Materials). Notably, because our OLTAS consultants identified treatments for trauma and unresolved grief as a key need, we included both PTSD Checklist-5 (PCL-5) and Inventory of Complicated Grief-Revised (ICG-R). The DS-II and all secondary clinical outcome self-report measures were administered at least at baseline, end-of-treatment, and 3-month follow-up.

CONCLUSION

Psilocybin therapy merits further research as a brief, rapid-acting intervention for demoralized patients with serious medical illness, including PLWH, but the literature remains immature. Larger, randomized, controlled and well-blinded trials are needed. Future trials and clinical treatments involving psilocybin may consider using group psychotherapy, particularly for socially isolated and marginalized populations seeking help with mood-and trauma-related disorders. session (Fig.). The study took place in an outpatient section of an urban academic medical center and was approved by the UCSF Institutional Review Board (CHR#15À17825), Food and Drug Administration, Research Advisory Panel of California, and Drug Enforcement Administration. Written informed consent was documented after the procedures had been fully explained, and the study was conducted according to Good Clinical Practices (NCT02950467).

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