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Trial registered on ANZCTR

Registration number

ACTRN12622000015741

Ethics application status

Approved

Date submitted

8/09/2021

Date registered

11/01/2022

Date last updated

8/03/2023

Date data sharing statement initially provided

11/01/2022

Type of registration

Prospectively registered

Titles & IDs

Public title

The impact of faecal microbiome transfer on gut health in autistic adolescents and young adults

Scientific title

Faecal microbiome transfer for the treatment of gastrointestinal symptoms in autistic adolescents and young adults: A double-blinded randomised placebo-controlled trial

Secondary ID [1]

Nil known

Universal Trial Number (UTN)

U1111-1261-0104

Trial acronym

Linked study record

Health condition

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

Autism

Functional gastrointestinal disorders

Condition category

Condition code

Mental Health

Autistic spectrum disorders

Oral and Gastrointestinal

Other diseases of the mouth, teeth, oesophagus, digestive system including liver and colon

Intervention/exposure

Study type

Interventional

Description of intervention(s) / exposure

All participants will undergo bowel cleansing on the day before treatment using an oral solution containing 70 g of Glycoprep-O (active ingredient macrogol 3350) (Fresenius Kabi Australia, Mount Kuring-gai, Australia). After bowel cleansing, participants will fast overnight for at least 8 hours; in the morning at clinic, participants will take the first dose of either encapsulated faecal microbiome transfer (FMT) or placebo (saline), 10 capsules each swallowed with water or diluted juice. Following another 8-hour overnight fast, in the next morning, participants will receive a second dose of 10 capsules of the same treatment. After each dose, participants will need to remain fasted for another 2 hours.

The FMT treatment will be extracted from donor stools and be doubly encapsulated using delayed release hydroxypropyl methylcellulose capsules (DRCaps, Capsugel Inc, Sydney, Australia). The DRCaps mask taste, odour, and visual appearance; importantly, they are designed to remain intact during passage from the stomach to the intestine, ensuring FMT delivery to the proximal bowel. Thus, the use of invasive techniques (i.e. endoscopy) for FMT will not be required.

Methods for faecal microbiome isolation, preparation, and double encapsulation will be carried out as detailed in the Gut Bugs Trial study protocol (Leong et al. BMJ Open 2019). Briefly, immediately after donation, stools are placed in normal saline, blended, and sieved to remove particulate matter. Samples are then differentially centrifuged to isolate the microbiota pellet. The use of low-speed centrifugation to pellet the microbiota cells is a feature of this methodology that reduces the risk of having free viruses included into the treatment capsules. The pellet is suspended in normal saline (containing 15% glycerol – a cryoprotectant) at 1 g wet weight/ml before being dispensed into size 0 DRcaps capsules. These capsules are closed and secondarily sealed within size 00 DRcaps capsules. Each capsule will contain 0.5 ml of faecal suspension corresponding to approximately 0.5 g of microbiota, so that our treatment dose of 20 capsules will administer approximately 10 g of microbiota. Capsules will be stored frozen at -80°C and will remain viable for at least 6 months.

Intervention code [1]

Treatment: Other

Comparator / control treatment

The control treatment are the placebo capsules containing only saline.

Control group

Placebo

Outcomes

Primary outcome [1]

Gastrointestinal symptoms using the Gastrointestinal Symptoms Rating Scale (GSRS) overall score

Timepoint [1]

6 weeks post-intervention

Secondary outcome [1]

Gastrointestinal symptoms using the GSRS overall score

Timepoint [1]

12, 20, and 26 weeks post-intervention

Secondary outcome [2]

Total score from the Patient Health Questionnaire-9 (PHQ-9)

Timepoint [2]

6, 12, and 26 weeks post-intervention

Secondary outcome [3]

Total score from the Generalised Anxiety Disorder Assessment (GAD-7)

Timepoint [3]

6, 12, and 26 weeks post-intervention

Secondary outcome [4]

Total score from the Short Warwick-Edinburgh Mental Well-being Scale (SWEMWBS)

Timepoint [4]

6, 12, and 26 weeks post-intervention

Secondary outcome [5]

Total score from the the 10-item Perceived Stress Scale (PSS-10)

Timepoint [5]

6, 12, and 26 weeks post-intervention

Secondary outcome [6]

Total score from the Sleep Quality Scale (SQS)

Timepoint [6]

6, 12, and 26 weeks post-intervention

Secondary outcome [7]

Diet quality score assessed with the short food-frequency questionnaire (FFQ)

Timepoint [7]

6, 12, and 26 weeks post-intervention

Secondary outcome [8]

BMI standard deviation score (BMI SDS) (height determined by stadiometer, and weight determined using weighing scale)

Timepoint [8]

6, 12, and 26 weeks post-intervention

Secondary outcome [9]

Waist-to-hip ratio (waist and hip circumference determined using a tape measure)

Timepoint [9]

6, 12, and 26 weeks post-intervention

Secondary outcome [10]

Waist-to-height ratio (waist circumference determined using a tape measure, height determined using a stadiometer)

Timepoint [10]

6, 12, and 26 weeks post-intervention

Secondary outcome [11]

Percentage of fat mass from bioelectrical impedance analysis

Timepoint [11]

26 weeks post-intervention

Secondary outcome [12]

Percentage of fat-free mass from bioelectrical impedance analysis

Timepoint [12]

26 weeks post-intervention

Secondary outcome [13]

Hair cortisol levels

Timepoint [13]

6, 12 and 26 weeks post-intervention

Secondary outcome [14]

Gastrointestinal inflammation and permeability by measuring faecal markers including calprotectin, lactoferrin, M2-pyruvate kinase, S100A12, and zonulin (composite outcome)

Timepoint [14]

6, 12, and 26 weeks post-intervention

Secondary outcome [15]

Recipient gut microbiome diversity (assessed with faecal samples using taxonomic profiling methods)

Timepoint [15]

6, 12 and 26 weeks post-intervention

Secondary outcome [16]

Recipient gut microbiome composition (assessed with faecal samples using taxonomic profiling methods)

Timepoint [16]

6, 12 and 26 weeks post-intervention

Secondary outcome [17]

Donor strain engraftment (assessed with faecal samples using strain profiling methods)

Timepoint [17]

6, 12 and 26 weeks post-intervention

Secondary outcome [18]

Bacteriophage diversity (assessed with faecal samples using shotgun metagenomic sequencing)

Timepoint [18]

6, 12 and 26 weeks post-intervention

Secondary outcome [19]

Changes in gut metabolites detectable in serum/urine using LC-MS/MS

Timepoint [19]

6, 12 and 26 weeks post-intervention

Eligibility

Key inclusion criteria

Aged 16-30 years inclusive at time of enrolment recruitment
Previous formal diagnosis of autism (including ASD, Asperger's Syndrome, Autistic Disorder, and PDD-NOS) as characterised in DSM-4, DSM-5, or ICD-10-AM
Moderate to severe gastrointestinal symptoms with mean overall GSRS score =2.0
Believe they are able to swallow treatment capsules
Willing to comply with the clinical assessments at baseline and follow-up visits

Minimum age

16 Years

Maximum age

30 Years

Sex

Both males and females

Can healthy volunteers participate?

Key exclusion criteria

Systemic antibiotic use within the preceding month
Intake of probiotic supplements within the preceding month
Regular steroid treatment
Dependence upon tube feeding
Serious medical problems that require specific treatment
Moderate to severe depression and/or suicidal ideation as per PHQ-9
Pregnancy
Known allergy to any medications or foods and/or to macrogol

Study design

Purpose of the study

Treatment

Allocation to intervention

Randomised controlled trial

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

Allocation concealment will be done using the REDCap electronic database based on a computer-generated randomisation list.

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

Participants will be randomised in a 1:1 ratio to either FMT or placebo, stratified by sex,
using block randomisation with variable block sizes of 2 and 4, based on a computer-generated randomisation sequence.

Masking / blinding

Blinded (masking used)

Who is / are masked / blinded?

The people receiving the treatment/s
The people administering the treatment/s
The people assessing the outcomes
The people analysing the results/data

Intervention assignment

Parallel

Other design features

Phase

Not Applicable

Type of endpoint/s

Efficacy

Statistical methods / analysis

The power calculation was based on a mean and standard deviation of 2.44 and 0.47, respectively, for GSRS overall scores at baseline among 18 children and adolescents (aged 7-16 years) diagnosed with ASD (Kang et al. 2017). We aim to recruit 50 participants per group, which will allow us to detect a statistically significance difference in GSRS overall scores of 0.31 (approximately 12.7%) between groups, based on a two-tailed t-test with 90% power and a=0.05. In the event of a 20% loss to follow-up, with 40 participants per group our study would still be powered to detect a statistically significance difference in GSRS overall scores of 0.35 (approximately 14%) between groups.

The primary outcome analysis will be based on intention-to-treat with multiple imputations on missing data. For all continuous outcomes, linear mixed models with repeated measures will be used to control for correlated data collected from the same participants. Binary outcomes will be assessed using generalized linear models with a logit link. Models will be adjusted for the baseline outcome value and sex (stratification factor). Model-adjusted estimates and differences between groups will be calculated with 95% confidence intervals. Planned subgroup analyses by sex will be conducted on primary and secondary outcomes to evaluate the consistency of main treatment effects among male and female participants.

Recruitment

Recruitment status

Recruiting

Date of first participant enrolment

Anticipated

13/02/2023

Actual

Date of last participant enrolment

Anticipated

31/12/2024

Actual

Date of last data collection

Anticipated

30/06/2025

Actual

Sample size

Target

100

Accrual to date

Final

Recruitment outside Australia

Country [1]

New Zealand

State/province [1]

Auckland

Country [2]

New Zealand

State/province [2]

Wellington

Country [3]

New Zealand

State/province [3]

Hamilton

Funding & Sponsors

Funding source category [1]

Charities/Societies/Foundations

Name [1]

Rockfield Trust

Address [1]

Castle Drive
Epsom
Auckland 1023
New Zealand

Country [1]

New Zealand

Primary sponsor type

University

Name

University of Auckland

Address

Liggins Institute
University of Auckland
85 Park Road
Grafton 1023
Auckland
New Zealand

Country

New Zealand

Secondary sponsor category [1]

None

Name [1]

None

Address [1]

None

Country [1]

Ethics approval

Ethics application status

Approved

Ethics committee name [1]

Central Health and Disability Ethics Committee

Ethics committee address [1]

Health and Disability Ethics Committees
Ministry of Health
133 Molesworth Street
PO Box 5013
Wellington
6011

Ethics committee country [1]

New Zealand

Date submitted for ethics approval [1]

04/08/2021

Approval date [1]

24/08/2021

Ethics approval number [1]

21/CEN/211

Summary

Brief summary

Background
Many autistic children and adults have chronic gastrointestinal symptoms that adversely affect their quality of life. These symptoms have been associated with a disordered gut microbiome.

Aims
To evaluate the efficacy of oral encapsulated faecal microbiome transfer (FMT) in improving gastrointestinal symptoms and well-being among autistic adolescents and young adults.

Study design
Randomised double-blind placebo-controlled trial.

Participants
100 autistic adolescents and young adults aged 16-30 years with moderate to severe gastrointestinal symptoms.

Intervention
Participants will be randomised to either FMT or placebo (saline). FMT treatment will be extracted from stools of healthy donors, and will be doubly encapsulated. Treatment consists of 20 capsules taken over two days (10 per day).

Assessments
Questionnaires to assess gastrointestinal symptoms, well-being, sleep quality, and food selectivity will be administered. Stool and hair samples will be collected to monitor changes to the gut microbiome profile, gut inflammation and permeability, and stress hormone levels (cortisol). We will also take anthropometric measurements and assess body composition using bioelectrical impedance analysis.

Significance
The findings could lead to novel therapies for improving gastrointestinal health among autistic individuals.

Trial website

Trial related presentations / publications

Public notes

Contacts

Principal investigator

Name

Prof Wayne Cutfield

Address

Liggins Institute,
Building 505,
Level 2, 85 Park Road,
Auckland, 1023
New Zealand

Country

New Zealand

Phone

+64 9 923 4476

Fax

[email protected]

Contact person for public queries

Name

Wayne Cutfield

Address

Liggins Institute,
Building 505,
Level 2, 85 Park Road,
Auckland, 1023
New Zealand

Country

New Zealand

Phone

+64 9 923 4476

Fax

[email protected]

Contact person for scientific queries

Name

Wayne Cutfield

Address

Liggins Institute,
Building 505,
Level 2, 85 Park Road,
Auckland, 1023
New Zealand

Country

New Zealand

Phone

+64 9 923 4476

Fax

[email protected]

Data sharing statement

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

Yes

What data in particular will be shared?

Coded and anonymised health information may be shared with researchers outside of this study for future research deemed appropriate by the Data Access Committee from the Liggins Institute's Clinical Data Research Hub. Anonymised gut microbiome data will be deposited in an international sequence database where it may be used for future microbiome research outside of this study.

When will data be available (start and end dates)?

Immediately following publication; beginning 3 months to 5 years

Available to whom?

Researchers outside of this study for future research deemed appropriate by the Data Access Committee from the Liggins Institute's Clinical Data Research Hub.

Available for what types of analyses?

Any purpose deemed appropriate by the Data Access Committee from the Liggins Institute's Clinical Data Research Hub, except that no clinical data collected in this trial will be used in any studies seeking a cure for autism.

How or where can data be obtained?

For queries, contact Professor Wayne Cutfield ([email protected]) or Professor Justin O'Sullivan ([email protected]). Requests to access clinical data will be forwarded to the Data Access Committee from the Liggins Institute's Clinical Data Research Hub.

Metagenomic sequencing data will be shared on NCBI's Sequence Read Archive (SRA)

What supporting documents are/will be available?

Doc. No.	Type	Citation	Link	Email	Other Details	Attachment
13100	Study protocol			[email protected]	The study protocol will be made available once it ... [More Details]
14461	Statistical analysis plan	The statistical analysis plan will be made available once the study protocol has been published.		[email protected]

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

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