LSD to Improve Cluster Headache Impact Trial

Phase 2

Recruiting

• Conditions: Chronic Cluster Headache
• Interventions: Drug: LSD tartrate; Drug: Placebo

• Registration Number: NCT05477459
• Lead Sponsor: Radboud University Medical Center

Brief Summary

This study aims to investigate the efficacy and safety of LSD 25μg every 3 days for 3 weeks versus placebo in the treatment of chronic cluster headache (cCH).

It is a 3-week double-blind placebo-controlled intervention study, preceded by a 4-week baseline observation period and followed by a 5-week post-treatment observation period.

Primary objective: to evaluate the efficacy of LSD 25μg every 3 days for 3 weeks in cCH.

Additional objectives:

* To evaluate the safety of LSD 25μg every 3 days for 3 weeks in cCH.

* To explore the exposure-response relationship of 25μg LSD in cCH.

* To explore cost-effectiveness of treatment with LSD in cCH.

* To evaluate the efficacy of LSD on health-related quality of life.

Detailed Description

Treatment of cluster headache consists of acute remedies for attacks (mainly 100% O2, sumatriptan), transitional treatment for temporary frequency reduction (subcutaneous steroid injection at the greater occipital nerve (GON block), oral steroids or frovatriptan) and prolonged prophylaxis (e.g. verapamil, lithium, topiramate). Although the latter compounds have shown some efficacy in reducing the attack frequency, the evidence for their effect is weak. All current prophylactics are prescribed off-label and are limited in their utility due to associated side effects. Despite treatment, many (notably chronic) cluster headache patients continue suffering headache attacks.

Invasive, expensive treatments like hypothalamic deep brain stimulation, occipital nerve stimulation and sphenopalatine ganglion stimulation are last resort options. Recently, a monoclonal antibody targeting calcitonin gene related peptide (CGRP) received FDA approval for episodic cluster headache, but was shown to be ineffective in cCH. Thus, there is a considerable unmet need for effective treatments that are better tolerated, safe and affordable.

In this study, the investigators will assess the efficacy of prophylactic treatment with LSD in cCH. The evidence for the efficacy of LSD is limited, with the majority of data originating from case reports or uncontrolled and retrospective (internet) surveys. Nevertheless, these studies do provide indications that LSD may hold potential as a cluster headache prophylaxis.

The primary objective of this randomized double-blind placebo-controlled trial is to compare the efficacy of LSD 25μg every 3 days for 3 weeks versus placebo in cCH. The investigators aim to show that, at the end of treatment, verum is more efficacious than placebo with comparable tolerability in an ambulatory setting. To explore the sustainability of benefit the investigators will also assess the (sustained) response at 5 weeks post-treatment (8 weeks postrandomization).

If the study findings are positive, LSD should be further studied before use in routine clinical practice. Non-hallucinogenic low-dosed LSD may provide an alternative or adjunctive option for patients who do not respond to or cannot tolerate currently available treatments.

Study Timeline

• Study First Submitted: 2022-07-05
• Study First Submitted QC: 2022-07-25
• Study First Posted: 2022-07-28
• Status Verified: 2025-03
• Last Update Submitted: 2025-04-10
• Last Update Posted: 2025-04-15
• Study Start: 2025-04-16
• Primary Completion: 2027-04
• Study Completion: 2027-04

Recruitment & Eligibility

• Status: RECRUITING
• Sex: All
• Target Recruitment: 65

Inclusion Criteria

• CCH according to the International Classification of Headache Disorders version 3 (ICHD-3)
• At screening: stable weekly attack frequency in the 4 weeks prior to screening (assessed retrospectively), averaging at least 8 per week and each week within a 40% window around the average
• At randomization: average of at least 8 attacks per week and no absence of attacks on more than two consecutive days during baseline

Exclusion Criteria

• Use of excluded concomitant treatment at screening (lithium; other prophylactics if not on a stable dose for less than one month; steroids/GON block within 2 months before screening; sphenopalatinum block, neurostimulation (changed setting within 3 months before screening) or botulinum toxin within 3 months before screening) and during the double-blind phase
• Use of LSD(-derivatives) (other than investigational drug), psilocybin, ketamine or cannabis within 3 months prior to screening and throughout the study
• Lifetime and/or family history (first degree relatives) of psychotic or bipolar disorder, suicidal intention or attempt
• A score of 6 or more on the 'Ervaringenlijst' (PQ-16) to exclude subclinical susceptibility to psychosis
• Actual abuse of alcohol and/or recreational drugs
• Lifetime history of cardiac valvular disease
• History or evidence of cognitive disorder at screening
• Positive urine drug screen at screening
• Females: Pregnancy, lactation, no acceptable contraceptive use

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Verum	LSD tartrate	Lysergic diethylamide tartrate (equivalent to 25 microgram LSD base), one dose every 3 days for 3 weeks (totalling 7 vials)
Placebo	Placebo	Placebo vial looking like verum vial, one vial every 3 days for 3 weeks (totalling 7 vials)

Primary Outcome Measures

Name	Time	Method
Mean change in weekly attack frequency, across treatments groups.	week 3 of treatment	In week 3 post-randomization, compared to the 4-week baseline average per week

Secondary Outcome Measures

Name	Time	Method
Mean change in weekly attack frequency across weeks 4-8 compared to the 4-week baseline and for each week separately.	week 8 post-randomization
100% reduction (remission rate) in number of weekly attacks in the third treatment week, compared to the 4-week baseline, across treatment groups.	week 3 post-randomization	Rate of subjects with 100% reduction in weekly attack frequency compared to baseline
≥50% reduction (50% responder rate) in number of weekly attacks in the third treatment week, compared to the 4-week baseline, across treatment groups.	week 3 post-randomization	Rate of subjects with more than 50% reduction in weekly attack frequency compared to baseline
≥30% reduction (30% responder rate) in number of weekly attacks in the third treatment week, compared to the 4-week baseline, across treatment groups.	week 3 post-randomization	Rate of subjects with more than 30% reduction in weekly attack frequency compared to baseline
100% reduction (remission rate) in number of weekly attacks across weeks 4-8 compared to the 4-week baseline and for each week separately.	week 8 post-randomization	Rate of subjects with 100% reduction in weekly attack frequency compared to baseline
≥50% reduction (50% responder rate) in number of weekly attacks across weeks 4-8 compared to the 4-week baseline and for each week separately.	week 8 post-randomization	Rate of subjects with 50% reduction in weekly attack frequency compared to baseline
Mean change in weekly attack frequency in the entire 3 week treatment period compared to the 4-week baseline.	week 3 post-randomization
Mean change in mean headache attack duration (minutes) per week, across treatment groups	week 8 post-randomization	Across weeks 4-8 compared to the 4-week baseline and for each week separately.
≥30% reduction (30% responder rate) in number of weekly attacks across weeks 4-8 compared to the 4-week baseline and for each week separately.	week 8 post-randomization	Rate of subjects with 30% reduction in weekly attack frequency compared to baseline
Mean change in mean headache attack severity (VAS 1-10), across treatment groups	week 8 post-randomization	Across weeks 4-8 compared to the 4-week baseline and for each week separately.
Mean change in number of abortive medication use, across treatment groups	week 8 post-randomization	Across weeks 4-8 compared to the 4-week baseline
Failure of sustained response'	Weeks 4-8 post-randomization	Time to initiation of additional prophylactic treatment and/or GON-block during weeks 4-8, across treatment groups
Patient Global Impression of Change (PGIC)	weeks 3 and 8	Patient Global Impression of Change at week 8 post-randomization; scale 0-7, higher scores representing better improvement
Health-related quality of life	weeks 3 and 8	Change from baseline in EQ-5D-5L Visual Analogue Scale (VAS) at weeks 3 and 8.
Hospital Anxiety and Depression Score (HADS)	weeks 3 and 8.	Change from baseline in Hospital Anxiety and Depression Scale (HADS) at weeks 3 and 8.
Pharmacokinetic (PK)-pharmacodynamic (PD) modelling	Day 18 post-randomization	Plasma LSD concentrations on day 18 post-randomization frequency
Cost-effectiveness analysis (CEA) from a societal perspective comparing the LSD intervention with usual care.	Week 1, 3 and 8	Healthcare use and productivity losses will be measured by patient questionnaires (iMCQ, and iPCQ)
Efficacy of treatment masking	Week 1 and 3 post-randomization	measured as perceived treatment assignment on a 5-point scale (likely verum/possibly verum/don't know/possibly placebo/likely placebo).

Trial Locations

Locations (2)

Leiden University Medical Center (LUMC); 🇳🇱 Leiden, Netherlands

Canisius-Wilhelmina Ziekenhuis (CWZ); 🇳🇱 Nijmegen, Netherlands