ANZCTR - Registration

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Trial registered on ANZCTR

Registration number

ACTRN12618001965291

Ethics application status

Approved

Date submitted

21/11/2018

Date registered

5/12/2018

Date last updated

21/05/2024

Date data sharing statement initially provided

5/12/2018

Type of registration

Prospectively registered

Titles & IDs

Public title

Oral Ketamine Trial on Post-Traumatic Stress Disorder

Scientific title

An open-label, dose ranging, clinical trial of oral ketamine, an NMDA (N-methyl-D-aspartate) receptor antagonist, with weekly dosing over six weeks in patients who are experiencing post-traumatic stress disorder (PTSD)

Secondary ID [1]

CTN ID: CT-2018-CTN-03765-1 v1, Protocol: AU/1/7867310.

Universal Trial Number (UTN)

U1111-1224-3868

Trial acronym

OKTOP

Linked study record

Health condition

Health condition(s) or problem(s) studied:

Post-traumatic stress disorder

Condition category

Condition code

Mental Health

Other mental health disorders

Intervention/exposure

Study type

Interventional

Description of intervention(s) / exposure

This trial aims to determine the feasibility, tolerability, and safety of oral ketamine (OK) as a treatment for post-traumatic stress disorder (PTSD). In this 10-week trial, participants will undergo 6 weeks of active treatment followed by 2 follow-up assessments.

Participants will be administered a sub-anaesthetic oral dose of ketamine once a week for a period of 6 weeks. The initial dose will be 0.5mg per kilogram, after which dose amounts will be increased by between 0.1mg and 1mg/kg in each treatment, with a maximum dose of 3.0mg/kg. Upon reaching 3.0mg/kg, participants will continue at that level until the end of the treatment phase, provided they tolerate the dose, i.e. “endure the action of ketamine without any side effect or discomfort”.

Oral ketamine will be administered on-site by the psychiatrist as per the dosage protocol on routine basis but can be administered by the Mental Health Nurse Practitioner (MHNP) as directed by the psychiatrist. The participants will be observed at Thompson Institute for up to two hours after the drug administration. An accountability logbook and controlled drug register (as per Queensland Governmental regulations) for ketamine will be maintained throughout the trial. If a participant is unable to attend or misses a ketamine treatment, details of the deviation will be recorded in the source documentation. Participants will be withdrawn from the study if they miss more than 2 ketamine treatments.

Intervention code [1]

Treatment: Drugs

Comparator / control treatment

No control group

Control group

Uncontrolled

Outcomes

Primary outcome [1]

PTSD symptomology, as assessed by the PTSD Checklist for DSM-5 (PCL-5) between baseline (BAS) and Follow-up 1.

Timepoint [1]

The PCL-5 will be administered at the following time points:
• Baseline (week 0)
• 30-60 minutes pre-ketamine treatment
• 24-hours after ketamine treatment
• Follow-up 1 (1 week after final ketamine treatment) (primary endpoint)
• Follow-up 2 (4 weeks after final ketamine treatment)

Secondary outcome [1]

Change in PTSD symptomology, as determined by the PCL-5 between FUP1 and FUP2

Timepoint [1]

The PCL-5 will be administered at the following time points:
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-up 2 (4 weeks after final ketamine treatment)

Secondary outcome [2]

Clinical side effects, assessed using psychiatric safety scales: Clinician-Administered Dissociative States Scale (CADSS), Brief Psychiatric Rating Scale (BPRS), and Young Mania Rating Scale (YMRS). This is a composite secondary outcome.

Timepoint [2]

The CADSS, BPRS, YMRS will be administered at the following time points:
• Baseline (week 0)
• 30-60 minutes after receiving ketamine treatment
• 24-hours after ketamine treatment
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-up 2 (4 week after final ketamine treatment)

Secondary outcome [3]

Clinically rated suicidality as assessed by the Beck Scale for Suicide Ideation (BSS).

Timepoint [3]

The BSS will be administered at the following time points:
• Baseline (week 0)
• 30-60 minutes pre-ketamine treatment
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-up 2 (4 weeks after final ketamine treatment)

Secondary outcome [4]

Social and occupational functioning as assessed by Social and Occupational Assessment Scale (SOFAS).

Timepoint [4]

SOFAS will be administered at the following time points:
• Baseline (week 0)
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-up 2 (4 weeks after final ketamine treatment)

Secondary outcome [5]

Perceived pleasure as assessed by the Snaith Hamilton Pleasure Scale (SHAPS-C).

Timepoint [5]

The SHAPS-C will be administered at the following time points:
• Baseline (week 0)
• 30-60 minutes pre-ketamine treatment
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-up 2 (4 weeks after final ketamine treatment)

Secondary outcome [6]

Depression, as assessed by the Montgomery – Asberg Depression Rating Scale (MADRS).

Timepoint [6]

The MADRS will be administered at the following time points:
• Baseline (week 0)
• 30-60 minutes pre-ketamine treatment
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-up 2 (4 weeks after final ketamine treatment)

Secondary outcome [7]

Depression, assessed using the Depression subscale of the Depression, Anxiety and Stress Scale (DASS-21).

Timepoint [7]

The DASS-21 will be administered at the following time points:
• Baseline (week 0)
• 30-60 minutes pre-ketamine treatment
• 24 hours post-ketamine treatment
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-up 2 (4 weeks after final ketamine treatment)

Secondary outcome [8]

Self-rated stress, assessed through the use of the Perceived Stress Scale (PSS).

Timepoint [8]

The PSS will be administered at the following time points:
• Baseline (week 0)
• 24 hours after week 3 of ketamine treatment
• 24 hours after week 6 of ketamine treatment
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-Up 2 (4 weeks after final ketamine treatment)

Secondary outcome [9]

Global wellbeing, assessed using the World Health Organization Wellbeing Index (WHO-5).

Timepoint [9]

The WHO-5 will be administered at the following time points:
• Baseline (week 0)
• 30-60 minutes pre-ketamine treatment
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-Up 2 (4 weeks after final ketamine treatment)

Secondary outcome [10]

Sleep quality, assessed using the Pittsburgh Sleep Quality Index Addendum for PTSD (PSQI-A)

Timepoint [10]

The PSQI-A will be administered at the following time points:
• Baseline (week 0)
• 30-60 minutes pre-ketamine treatment
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-up 2 (4 weeks after final ketamine treatment)

Secondary outcome [11]

The relationship between glutamate and brain-derived neurotrophic factor (BDNF) will be assessed via research blood tests across 5 timepoints.

Timepoint [11]

Research blood tests will be conducted at 5 time points:
• Baseline (week 0)
• 24 hours after week 3 of ketamine treatment
• 24 hours after week 6 of ketamine treatment
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-up 2 (4 weeks after final ketamine)

Secondary outcome [12]

MRI will be utilized to examine a variety of neurobiological changes, including neuroanatomical changes in density, volume, and white matter tract connectivity

Timepoint [12]

MRI will be conducted at 5 time points:
• Baseline (week 0)
• 24 hours after week 3 of ketamine treatment
• 24 hours after week 6 of ketamine treatment
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-up 2 (4 weeks after final ketamine

Secondary outcome [13]

Electroencephalography (EEG) will be used to assess changes in neural network communication from BAS to FUP1 and FUP2.

Timepoint [13]

EEG will be administered at the following time points:
• Baseline (week 0)
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-up 2 (4 weeks after final ketamine treatment)

Secondary outcome [14]

Cambridge Neuropsychological Test Automated Battery (CANTAB) will be used to assess cognitive functioning such as attention, working memory, speed of processing, and executive functioning.

Timepoint [14]

The computerised cognitive battery will be administered at the following time points:
• Baseline (week 0)
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-Up 2 (4 weeks after final ketamine treatment)

Secondary outcome [15]

PTSD diagnosis, as assessed using the Clinician Administered PTSD Scale for DSM-5 (CAPS-5) between Baseline (Week 0) and Follow-up 1 (FUP1).

Timepoint [15]

Clinician Administered PTSD Scale for DSM-5 (CAPS-5) will be administered at the following time points:
• Baseline (week 0)
• Follow-up 1 (1 week after final ketamine treatment).

Secondary outcome [16]

PTSD diagnosis, as assessed using the Clinician Administered PTSD Scale for DSM-5 (CAPS-5) between Baseline (Week 0) and Follow-up 2 (FUP2).

Timepoint [16]

Clinician Administered PTSD Scale for DSM-5 (CAPS-5) will be administered at the following time points:
• Baseline (week 0)
• Follow-up 2 (4 weeks after final ketamine treatment).

Secondary outcome [17]

PTSD diagnosis, as assessed using the Clinician Administered PTSD Scale for DSM-5 (CAPS-5) between Follow-up 1 and Follow-up 2.

Timepoint [17]

Clinician Administered PTSD Scale for DSM-5 (CAPS-5) will be administered at the following time points:
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-up 2 (4 weeks after final ketamine treatment).

Secondary outcome [18]

Clinical side effects, assessed using the symptom tolerability scale: Frequency, Intensity, Burden of Side Effects Rating (FIBSER).

Timepoint [18]

The FIBSER will be administered at the following time points:
• Baseline (week 0)
• 24 hours post-ketamine treatment
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-up 2 (4 week after final ketamine treatment)

Secondary outcome [19]

Clinical side effects, assessed using the symptom tolerability scale: Patient Rated Inventory of Side Effects (PRISE).

Timepoint [19]

The PRISE will be administered at the following time points:
• Baseline (week 0)
• 30-60 minutes pre-ketamine treatment
• 24-hours after ketamine treatment
• Follow-up 1 (1 week after final ketamine treatment)
• Follow-up 2 (4 week after final ketamine treatment)

Secondary outcome [20]

Anxiety, assessed using the Anxiety subscale of the Depression, Anxiety and Stress Scale (DASS-21).

Timepoint [20]

Secondary outcome [21]

Self-rated stress, assessed through the stress subscale of the Depression, Anxiety and Stress Scale (DASS-21).

Timepoint [21]

Eligibility

Key inclusion criteria

•Current PTSD diagnosis
•Persons (male/female/other) aged over 18 years
•Participants must be able to understand and provide consent on the Participant Information and Consent Form (PICF).
•Participants must be able to tolerate the ketamine treatment, rating scales, blood testing and urinalysis in order to remain in the study and this will be monitored on an ongoing basis, as per the methodology.

Minimum age

18 Years

Maximum age

No limit

Sex

Both males and females

Can healthy volunteers participate?

Key exclusion criteria

Psychiatric conditions:
•Psychosis
•Mania/hypomania
•Acute suicidality requiring urgent psychiatric intervention
•History of ketamine use disorder

Physical conditions:
•Participants who have history of epilepsy or unexplained seizure history.
•Uncontrolled/severe symptomatic cardiovascular disease states including: recent myocardial infarction (within prior 6 months); history of stroke; and hypertension (resting blood pressure >150/100)
• Body weight of >150kg
•History of intracranial mass, intracranial haemorrhage/stroke, cerebral trauma/traumatic brain injury or increased intracranial pressure (as assessed by referring general practitioner)
•Liver function test (LFT) results out of normal range, as specified below:
•ALT: >135 U/L
•AST: >123 U/
•GAMMA GT (GGT) male participants: >210 U/L
•GAMMA GT (GGT) – female participants: >135 U/L
•TOTAL BILIRUBIN (BIT): >60 umol/L
•ALBUMIN (A): <25g/L and >150g/L
•ALK PHOS (ALP): >345 U/L
•Previous reaction to ketamine (as reported by referring general practitioner and participant)
•Participants who are pregnant, currently breastfeeding, or who are planning a pregnancy during the trial
•Participants who are simultaneously engaging in another clinical intervention trial while participating in OKTOP
•Participants with a history of substance use disorder (excluding ketamine use disorder), may be eligible to participate in the study if they abstain from alcohol or illicit substance use two weeks prior to participation in the trial and for the remainder of the trial.

Study design

Purpose of the study

Treatment

Allocation to intervention

Non-randomised trial

Procedure for enrolling a subject and allocating the treatment (allocation concealment procedures)

Allocation is not concealed

Methods used to generate the sequence in which subjects will be randomised (sequence generation)

Not applicable

Masking / blinding

Open (masking not used)

Who is / are masked / blinded?

Intervention assignment

Single group

Other design features

Phase

Phase 1 / Phase 2

Type of endpoint/s

Safety/efficacy

Statistical methods / analysis

Statistical Analyses will include generalised linear models (GLMs), analysis of the relative change index, Frequentist statistics, and Bayesian statistics. A significance level of .05 will be utilized where required. Data will be inspected for outliers and any spurious data will be corrected or removed prior to analysis.

Recruitment

Recruitment status

Suspended

Date of first participant enrolment

Anticipated

11/02/2021

Actual

8/07/2021

Date of last participant enrolment

Anticipated

28/02/2025

Actual

26/10/2023

Date of last data collection

Anticipated

1/05/2025

Actual

Sample size

Target

Accrual to date

Final

Recruitment in Australia

Recruitment state(s)

QLD

Recruitment postcode(s) [1]

4575 - Birtinya

Funding & Sponsors

Funding source category [1]

University

Name [1]

University of the Sunshine Coast, Thompson Institute

Address [1]

12 Innovation Parkway, Birtinya, Queensland, 4575

Country [1]

Australia

Primary sponsor type

University

Name

University of the Sunshine Coast Mind and Neuroscience Thompson Institute

Address

12 Innovation Parkway, Birtinya, Queensland, 4575

Country

Australia

Secondary sponsor category [1]

None

Name [1]

Address [1]

Country [1]

Ethics approval

Ethics application status

Approved

Ethics committee name [1]

Prince Charles Hospital Human Research Ethics Committee

Ethics committee address [1]

Building 14
Rode Road
CHERMSIDE QLD 4032

Ethics committee country [1]

Australia

Date submitted for ethics approval [1]

27/07/2018

Approval date [1]

06/09/2018

Ethics approval number [1]

Project ID: 42836. HREC/18/QPCH/288:

Summary

Brief summary

This open-label, dose-ranging clinical trial which aims to determine the feasibility, tolerability, and safety of oral ketamine (OK) for post-traumatic stress disorder. In this 10-week trial, participants will undergo 6 weeks of active treatment followed by 2 follow-up assessments (week 7; week 10)

Participants (N = 50) will be receive a sub-anaesthetic dose of OK once a week over a 6-week period (according to an established titration protocol; 6 ketamine treatments in total);

• All participants will be engaged with their treating doctors for the duration of the trial.
• Ketamine will be used as an adjunctive treatment, meaning that participants are able to maintain or modify their current treatments under guidance of their physician. Any changes to medication will be recorded by study staff.
 
Primary hypothesis: That a 6-week OK treatment will be efficacious in reducing PTSD symptom frequency and severity.

Secondary hypotheses: That a 6-week OK treatment will be efficacious in: reducing stress, anxiety, depression, suicidal ideation; Improving cognitive, social, and occupational functioning; Improving sleep quality; Improving overall wellbeing.

Additionally, this study aims to examine the cognitive, neurobiological, and neurophysiological effects of OK treatment in adult participants with PTSD.

All changes outlined in this ANZCTR have been approved prior by Princes Charles Hospital Human Research Ethics Committee.

Trial website

Trial related presentations / publications

Public notes

Contacts

Principal investigator

Name

Dr Adem Can

Address

University of the Sunshine Coast Thompson Institute 12 Innovation Parkway, Birtinya QLD, 4575

Country

Australia

Phone

+61 7 5430 1285

Fax

[email protected]

Contact person for public queries

Name

Trish Wilson

Address

University of the Sunshine Coast Thompson Institute 12 Innovation Parkway, Birtinya QLD, 4575

Country

Australia

Phone

+61 075456 3893

Fax

[email protected]

Contact person for scientific queries

Name

Dr Adem Can

Address

University of the Sunshine Coast Mind and Neuroscience Thompson Institute
12 Innovation Parkway, Birtinya QLD, 4575

Country

Australia

Phone

+61 07 5456 3893

Fax

[email protected]

Data sharing statement

Will individual participant data (IPD) for this trial be available (including data dictionaries)?

No/undecided IPD sharing reason/comment

What supporting documents are/will be available?

No Supporting Document Provided

Results publications and other study-related documents

Documents added manually

No documents have been uploaded by study researchers.

Documents added automatically

No additional documents have been identified.

Trial Review

Documents added manually

Documents added automatically