Pilot and Feasibility Studies (Oct 2023)

An open-label pilot trial assessing tolerability and feasibility of LSD microdosing in patients with major depressive disorder (LSDDEP1)

  • Carina Joy Donegan,
  • Dimitri Daldegan-Bueno,
  • Rachael Sumner,
  • David Menkes,
  • William Evans,
  • Nicholas Hoeh,
  • Frederick Sundram,
  • Lisa Reynolds,
  • Rhys Ponton,
  • Alana Cavadino,
  • Todd Smith,
  • Partha Roop,
  • Nathan Allen,
  • Binu Abeysinghe,
  • Darren Svirskis,
  • Anna Forsyth,
  • Mahima Bansal,
  • Suresh Muthukumaraswamy

DOI
https://doi.org/10.1186/s40814-023-01399-8
Journal volume & issue
Vol. 9, no. 1
pp. 1 – 16

Abstract

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Abstract Background Globally, an estimated 260 million people suffer from depression [1], and there is a clear need for the development of new, alternative antidepressant therapies. In light of problems with the tolerability and efficacy of available treatments [2], a global trend is emerging for patients to self-treat depression with microdoses of psychedelic drugs such as lysergic acid diethylamide (LSD) and psilocybin [3]. Beyond anecdotal reports from those who self-medicate in this way, few clinical trials have evaluated this practice. In our recently published phase 1 study in healthy volunteers [4], we determined that LSD microdosing was relatively safe and well tolerated in that cohort. Furthermore, the data demonstrated that conducting such microdosing trials is broadly feasible, with excellent adherence and compliance to the regimen observed. In this open-label pilot trial of patients with major depressive disorder (LSDDEP1), we will test the tolerability and feasibility of an 8-week regimen of LSD microdosing in this patient group prior to a larger subsequent randomised controlled trial (LSDDEP2). Methods Twenty patients meeting the DSM-5 criteria for major depressive disorder will receive an 8-week LSD microdosing treatment regimen. The treatment protocol will use a sublingual formulation of LSD (MB-22001) delivered twice per week under a titration schedule using a dose of 5–15 µg. Tolerability will be assessed by quantifying the percentage of participants who withdraw from the trial due to adverse events attributable to the treatment regimen, while feasibility will be assessed by quantifying the percentage of attended clinic visits once enrolled. To determine whether there is any antidepressant response to the LSD microdosing regimen, MADRS scores will be assessed at baseline and 2, 4, 6, and 8 weeks after the commencement of the regimen. Discussion The results of LSDDEP1 will provide valuable information regarding the tolerability and feasibility of a proposed LSD microdosing regimen in patients with MDD. Such information is critically important to optimise trial design prior to commencing a subsequent and more resource-intensive randomised controlled trial. Trial registration ANZCTR, ACTRN12623000486628. Registered on 12 May 2023.

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