Inflammatory Bowel Diseases (IBD) Cannabis Registry

NCT ID: NCT05578313

Last Updated: 2022-10-13

Basic Information

• Recruitment Status: UNKNOWN
• Total Enrollment: 1000 participants
• Study Classification: OBSERVATIONAL
• Study Start Date: 2019-07-10
• Study Completion Date: 2024-07-10

Brief Summary

The inflammatory bowel diseases (IBDs), ulcerative colitis (UC) and Crohn's disease (CD), are characterized by lifelong relapsing-remitting gastrointestinal inflammation, with symptoms of abdominal pain, diarrhea, and rectal bleeding during active disease. Medical therapy reduces intestinal inflammation and ameliorates symptoms. Medical cannabis has recently been added to the arsenal of symptom-reducing measures in IBD. Though the efficacy of THC and CBD have been established as the two most dominant ingredients of cannabis, the rest of the plant phytochemicals are unknown, and effects on patients are not yet determined.

Detailed Description

Hypothesis (es) and Aims:

Prospectively follow IBD patients receiving medical cannabis as treatment of their disease (group 1) in comparison to the following control groups:

2) Healthy patients who do not use cannabis; 3) IBD patients who experience pain and do not use cannabis; 4) IBD patients who do not experience pain and do not use cannabis; 5) IBD patients previously prescribed cannabis and were identified to have positive effect on their disease

• Specific aims: a prospective trial to determine whether cannabis can induce remission in patients with IBD.

• To identify treatment regimens associated with treatment success in IBD patients.
• To identify treatment regimens associated with treatment side effects in IBD patients.
• To analyze the optimal drug level for disease management in various IBD patient types.

• Study design:

• A prospective cohort study
• Setting: prospectively collect clinical, behavioral, dietary and environmental data of IBD patients receiving medical cannabis as treatment of their disease. Data will be collected according to a uniform standardized protocol specifically adapted to the needs of the study.
• Study population:

Eligible IBD patients treated at the IBD clinic in the Tel Aviv Medical Center participating in the study, which have signed an informed consent form and answered to all the study inclusion criteria. Patients will be informed of the study by their treating physician, recruited and followed throughout the follow-up period by study coordinators.

This study will include five patient groups:

• Group 1 (study group): IBD patients prescribed cannabis as treatment for their bowel disease.
• Group 2 (Control group): One hundred healthy patients who do not use cannabis and are not eligible or not interested to commence this intervention.
• Group 3 (control group): Up to 100 IBD patient who experience pain and do not use cannabis
• Group 4 (control group): Up to 100 IBD patient who do not experience pain and do not use cannabis
• Group 5 (Cannabis responders group): up to 100 IBD patients previously prescribed cannabis and were identified to have positive effect on their disease

*Study plan:

• Among the study group :

At baseline, demographic characteristics, medical history, concomitant medication assessment, disease related therapy and failed therapy will be documented.

Study visits:

Among the study group: recruitment at time 0, after one month (±14 days) of treatment, at three months (±21 days) and at 6 months (±30 days) of therapy (end of study), will be conducted, in which patients will be asked to fill in questionnaires, give biologic samples, undergo clinical, anthropometric and nutritional evaluation and physician assessment and monitoring of therapy, safety and adverse events. The cannabis producing company, composition, quantity and way of consumption will be documented.

•Among control group and Cannabis responders group: Healthy controls will be samples once at baseline. All IBD control groups (groups 3-5) will be followed up similarly as the study group and will undergo all sampling and questionnaires, at times 0, 3, 6 months (excluding the 1 month cannabis dose adjustment meeting).

Patients will be asked to inform in case of relapse during the follow up period and provide stool and blood samples before therapy is changed. At relapse time point, disease activity index will be recorded and questionnaires will be completed.

*Sample collection: Baseline and follow up study visits will include biologic samples collection (blood, feces) from which blood levels of complete blood count (CBC), Albumin, Liver enzymes (ALT, AST, ALP), lipid panel (Total cholesterol, LDL, HDL, triglycerides), creatinine, fasting glucose, C-reactive protein (CRP), drug levels and antibodies (for patients treated with thiopurines and biologics), and fecal levels of Calprotectin will be measured.

White blood cells will be separated and stored for m RNA analysis of cannabinoid metabolism. Only RNA fractions will be extracted and analyzed, no DNA will be assessed and no genetic sequencing will be performed . In addition, 10 ml of blood will be drawn for analysis of Th17 cells. CD4 T cells will be purified from peripheral blood of IBD patients by RosetteSep™ Human CD4+ T Cell Enrichment Cocktail kit. STAT3 and IL-17 levels will be analyzed. The samples analysis will be done at Dedi Meiri's lab at the Technion-IIT. Serum, and fecal samples will be stored at -80◦C for future analysis after being authorized by the IRB and by law including cannabis phytochemical analysis (10ml of each) on WBC and on biopsies when available and for fecal microbiome analysis. In appendix A- a detailed list of all tests in each visit.

*Endoscopic evaluation: In patients who will undergo a standard of care endoscopic examination for clinical reasons: these will include mucosal and histologic assessment for disease severity (SES-CD and MAYO score for CD and UC patients respectively, PDAI for Pouchitis patients).

Mucosal biopsies will be collected from inflamed and healthy areas, and from standard areas of the GI track (table 1), sent for histology assessment and stored for future analysis after being authorized by the IRB and by law. These samples will be stored in RNA Later snapped frozen and stored at -80◦c until analysis. No more than 10 samples will be collected during endoscopy including samples for clinical assessment. Samples from recto-sigmoid junction (20 cm from anus) will be taken in every colonoscopy, regardless of the status of inflammation.

*Biologic sample handling: Samples will be stored at -80◦c while coded with no identifying information; access to samples will be restricted to the study staff only. Samples will be stored up to 10 years from final data collection.

In this study, serum and fecal samples analyzed will include those gathered from protocol number 0276-19 and from protocol number 0250-17 in patients using medical cannabis only. In the later group, samples will be used only if the patient had agreed for use of samples in other studies other than 0250-17. To both studies, Professor Nitsan Maharshak is PI.

*Questionnaires:

Baseline and follow up study visits will include data collection from the following:

• Documentation of cannabis therapy: consumption method, quantity, THC/CBD concentration and cannabis strain/ barcode of preparation
• Food frequency questionnaire
• Food diary from last 3 days
• Lifestyle questionnaire
• Medical management questionnaire (IBD SES- self efficacy scale questionnaire)
• Patient reported outcomes (PROMIS) questionnaires
• Medical cannabis treatment evaluation questionnaire and Adverse events
• Big Five personality traits

Anthropometric and nutritional evaluation:

• Patients weight (kg), height (m), waist circumference (cm) will be documented at each study visit, and body mass index (BMI) will be calculated.
• Nutritional status will be evaluated by a MUST questionnaire

*Study endpoints: the study will follow patients throughout 6 months of treatment and follow disease remission (clinical/biochemical) or exacerbation.

• Disease remission:

• Reduction in appropriate clinical scores
• Decrease in serum CRP or fecal CLP
• Endoscopic remission
• Disease exacerbation:

• Increase in appropriate clinical score
• Increase in fecal calprotectin levels (>250mg/gr OR 100 units higher than baseline levels)
• Emergency room visit due to disease symptoms, hospitalization, non-elective surgery.
• Diagnosis of active disease by endoscopy or imaging
• Medical treatment change by treating physician

• Statistical analysis:

Statistical analyses will be performed using SPSS version 23.0 for Windows. Patients who adhere to the study's protocol (defined as preforming ≥ 80% of exercises) will be included in data analysis. An intention-to-treat analysis will include patients excluded because of non-adherence to the intervention.

Descriptive statistics will be used to describe the distribution of variables associated with characteristics of the study sample. Continuous variables will be presented as means± SD and dichotomous/categorical variables as proportions. The normality of the distribution of continuous variables will be tested by the Kolmogorov-Smirnov test. If normality is rejected, non-parametric tests will be used.

Univariate analysis: To test the association between continuous variables with normal distribution, the Pearson correlation coefficient will be performed. To test associations between continuous variables which do not distribute normally or for ordinal variable, the spearman correlation coefficient will be used. To test differences in continuous variables between the treatments arms the t-test for independent groups (or Mann-Whitney test for non-normally distributed variables) will be performed. For comparison of dichotomous or categorical variables the Chi-square test will be performed.

To compare baseline to end of treatment parameters within arms for continuous variables the t-test for dependent groups will be performed (or Wilcoxson test for non-normally distributed variables), in dichotomous/categorical variables the McNemar Test will be performed.

To test differences in continuous variables between the treatment groups in numbers of time points the Mix model for repeated measures will be performed. To test differences in dichotomous/categorical variables between the treatment groups in numbers of time points Generalized estimating equation will be performed.

Conditions

Crohn Disease; Ulcerative Colitis; Pouchitis; Healthy

Study Design

• Observational Model Type: COHORT
• Study Time Perspective: PROSPECTIVE

Study Groups

• Group 1 (study group)

IBD patients prescribed cannabis as treatment of their bowel disease.

Medical Cannabis

Intervention Type: DRUG

Patients will be observed throughout their treatment with medical cannabis, prescribed to them by for clinically treating their disease (treatment is not an intervention of the study).

• Group 2 (Control group)

One hundred healthy patients who do not use cannabis and are not eligible or not interested to commence this intervention.

No interventions assigned to this group

• Group 3 (control group)

Up to 100 IBD patient who experience pain and do not use cannabis

No interventions assigned to this group

• Group 4 (control group)

Up to 100 IBD patient who do not experience pain and do not use cannabis

No interventions assigned to this group

• Group 5 (Cannabis responders group)

up to 100 IBD patients previously prescribed cannabis and were identified to have positive effect on their disease

No interventions assigned to this group

Interventions

Medical Cannabis

Patients will be observed throughout their treatment with medical cannabis, prescribed to them by for clinically treating their disease (treatment is not an intervention of the study).

Intervention Type: DRUG

Eligibility Criteria

Inclusion Criteria

Patients (male and female, age 18-80 years) diagnosed with Crohn's disease (CD), ulcerative colitis (UC) or pouchitis, and healthy volunteers.

All patients will sign an informed consent form. IBD patients who are recruited to group 3 will be included if they report mild-severe abdominal pain in clinical questioning of clinical activity (Harvey-Bradshaw index).

Healthy participants recruited to group 2 will be healthy volunteers with no prior/current use of medical cannabis

Exclusion Criteria

• Inability to sign an informed consent and complete the study protocol
• Unstable or uncontrolled medical disorder, or severe systemic disease (other than IBD)
• Participating in clinical interventional trial unrelated to cannabis derived preparations
• Ileostomy/ colostomy
• Pregnancy or intent to become pregnant in the next 6 month or breast feeding during the study

• Minimum Eligible Age: 18 Years
• Maximum Eligible Age: 80 Years
• Eligible Sex: ALL
• Accepts Healthy Volunteers: Yes

Sponsors

Eli Sprecher, MD

OTHER_GOV

Sponsor Role: lead

Responsible Party

Eli Sprecher, MD

PI

Responsibility Role: SPONSOR_INVESTIGATOR

Locations

Dep. of Gastroenterology, Tel Aviv Sourasky Medical Center

Tel Aviv, , Israel

Site Status: RECRUITING

Countries

Israel

Central Contacts

Nitsanm Maharshak, Professor

Role: CONTACT

nitsanm@tlvmc.gov.il

+972527360384

Naomi Fliss, Doctor

Role: CONTACT

naomifl@tlvmc.gov.il

+972524626445

Facility Contacts

Nitsan Maharshak, MD

Role: primary

nitsanm@tlvmc.gov.il

972527360384

Naomi Fliss, PhD

Role: backup

naomifl@tlvmc.gov.il

972524626445

Other Identifiers

TLV_0276-19

Identifier Type: -

Identifier Source: org_study_id