Trial PaperDepressive DisordersMajor Depressive Disorder (MDD)Headache Disorders (Cluster & Migraine)Palliative & End-of-Life DistressChronic PainAnxiety DisordersKetamine

A Phase II, Open-Label Clinical Trial of Intranasal Ketamine for Depression in Patients with Cancer Receiving Palliative Care (INKeD-PC Study)

In an open‑label phase II trial of intranasal racemic ketamine (50–150 mg) given over one week to 20 advanced‑cancer palliative care patients with moderate–severe major depressive disorder, 70% achieved ≥50% MADRS response and 45% achieved remission by Day 8, with mean MADRS falling from 31 to 11 (p<0.001) and partial maintenance to Day 14. Treatment was feasible and generally well tolerated—adverse effects were mostly mild and transient—supporting larger randomised controlled trials.

1 linked clinical trial·1 cited-by link indexed in Blossom

Authors

  • Roger McIntyre
  • Jonathan Rosenblat
  • Zoe Doyle

Published

Cancers
individual Study

Abstract

Antidepressants require several weeks for the onset of action, a lag time that may exceed life expectancy in palliative care. Ketamine has demonstrated rapid antidepressant effects, but has been minimally studied in cancer and palliative care populations. Herein, the objective was to determine the feasibility, safety, tolerability and preliminary efficacy of intranasal racemic ketamine for major depressive disorder (MDD) in patients with advanced cancer. We conducted a single-arm, open-label phase II trial at the Princess Margaret Cancer Centre in Toronto, ON, Canada. Participants with advanced cancer with moderate to severe MDD received three flexible doses of intranasal (IN) ketamine (50–150 mg) over a one-week period. The primary efficacy outcome was an antidepressant response and remission rates as determined by the Montgomery–Åsberg Depression Rating Scale (MADRS) from baseline to the Day 8 primary endpoint. Twenty participants were enrolled in the trial, receiving at least one dose of IN ketamine, with fifteen participants receiving all three doses. The Day 8 antidepressant response (MADRS decreased by >50%) and remission (MADRS < 10 on Day 8) rates were high at 70% and 45%, respectively. Mean MADRS scores decreased significantly from baseline (mean MADRS of 31, standard deviation 7.6) to Day 8 (11 +/− 7.4) with an overall decrease of 20 points (p < 0.001). Antidepressant effects were partially sustained in the second week in the absence of additional ketamine doses, with a Day 14 mean MADRS score of 14 +/− 9.9. Common adverse effects included fatigue, dissociation, nausea, dysgeusia and headaches; almost all adverse effects were mild and transient, resolving within 2 h of each ketamine dose with one dropout related to adverse effects (negative dissociative episode). Given these promising findings, larger, controlled trials are merited.

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Research Summary of 'A Phase II, Open-Label Clinical Trial of Intranasal Ketamine for Depression in Patients with Cancer Receiving Palliative Care (INKeD-PC Study)'

Editorial

βBlossom's Take

This is a useful palliative-care ketamine paper because it tests whether rapid antidepressant effects can be delivered in the time available to patients with advanced cancer. The open-label design limits what can be concluded, but the feasibility, tolerability and short-term response signal make it a practical bridge between general TRD ketamine work and end-of-life distress.

Intranasal ketamine showed rapid antidepressant effects in advanced cancer palliative care

Sourced

Can a short intranasal ketamine course reduce depression quickly enough for patients with limited life expectancy?

70%
Day 8 antidepressant response
45%
Day 8 remission
31 to 11
Mean MADRS change by Day 8
20
Participants enrolled

Day 8 outcomes in the open-label phase II trial

Response
70%
Remission
45%
Study snapshot figure.

Single-arm, open-label phase II clinical trial in 20 patients with advanced cancer and major depressive disorder. The figures summarise short-term, within-study outcomes only, so they do not establish comparative efficacy against placebo or standard care, and the Day 14 score reflects partial maintenance without additional dosing.

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Study Details

Cited By (1)

Papers indexed in Blossom that reference this study.

Intranasal Ketamine for Existential Distress in Advanced Cancer

Aguiar, S., Makarious, M., Lipsitz, O. et al. · Journal of Pain and Symptom Management (2026)

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