Colon Cancer Liver Metastasis Clinical Trial
Official title:
Biospecimen Collection for:Prebiotic Effect of Eicosapentaenoic Acid Treatment for Colorectal Cancer Liver Metastases
A significant proportion of patients who undergo liver surgery to remove bowel cancer that has spread to the liver (metastases) develop disease recurrence and die from the disease. The EMT2 study (NCT03428477) is a clinical trial of the omega-3 fatty acid EPA, investigating whether patients who EPA ethyl ester remain free of disease recurrence for longer than those taking placebo. Recent data suggest that the anti-cancer effect of EPA may result from changes to the microbiota (gut bacteria) which lead to an improved anti-cancer response by the immune system. This study will collect biospecimens (stool, urine, blood, tumour tissue) from participants in the EMT2 trial in order to interrogate the microbiome and immune mechanisms associated with EPA treatment, in relation to participant survival. Insights from this study will identify those most likely to benefit from treatment, leading to more targeted, personalised use of EPA.
Status | Recruiting |
Enrollment | 250 |
Est. completion date | July 2025 |
Est. primary completion date | July 2024 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years and older |
Eligibility | Inclusion Criteria: - Only individuals who have already been enrolled in the EMT2 trial are eligible for inclusion in the biospecimen collection study. Exclusion Criteria: - There are NO exclusions for entry to the biospecimen collection study if an individual has already been recruited to the EMT2 trial. |
Country | Name | City | State |
---|---|---|---|
United Kingdom | St James's University Hospital | Leeds | |
United Kingdom | University of Liverpool | Liverpool |
Lead Sponsor | Collaborator |
---|---|
University of Leeds | Harvard School of Public Health (HSPH), Massachusetts General Hospital, Massachusetts Institute of Technology, National Cancer Institute (NCI), University of Bradford |
United Kingdom,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Abundance of individual bacterial taxa in the gut microbiome (eg. Bifidobacterium, Lactobacillus, and Fusobacterium) in stool samples. | 16S rRNA and metagenomic methods | A) Change between baseline (pre-treatment) and before liver surgery. B) Change between baseline (pre-treatment) and 6 months after liver surgery. C) Change between baseline (pre-treatment) and time points up to two years follow up. | |
Primary | Microbial gene expression in stool samples | Bacterial gene expression analysis | A) Change between baseline (pre-treatment) and before liver surgery. B) Change between baseline (pre-treatment) and 6 months after liver surgery. C) Change between baseline (pre-treatment) and time points up to two years follow up. | |
Primary | Levels of polyunsaturated fatty acids and lipid mediators in stool samples | Liquid chromatography-mass spectrometric measurement of lipids | A) Change between baseline (pre-treatment) and before liver surgery. B) Change between baseline (pre-treatment) and 6 months after liver surgery. C) Change between baseline (pre-treatment) and time points up to two years follow up. | |
Primary | Relationship between changes in the gut microbiome induced by EPA and survival of patients | 16S rRNA and metagenomic methods | A) Change between baseline (pre-treatment) and before liver surgery. B) Change between baseline (pre-treatment) and 6 months after liver surgery. C) Change between baseline (pre-treatment) and time points up to two years follow up. | |
Primary | Treg cells and myeloid-derived suppressor cells in colorectal cancer liver metastasis tissue | Immunohistochemistry and flow cytometry for immune cell populations | A) Change between baseline (pre-treatment) and before liver surgery. B) Change between baseline (pre-treatment) and 6 months after liver surgery. C) Change between baseline (pre-treatment) and time points up to two years follow up. | |
Primary | Levels of expression of immune checkpoint regulators in colorectal cancer liver metastasis tissue | Immunohistochemistry for CTLA-4, TIGIT, TIM-3, PD-1 in colorectal cancer liver metastasis tissue | A) Change between baseline (pre-treatment) and before liver surgery. B) Change between baseline (pre-treatment) and 6 months after liver surgery. C) Change between baseline (pre-treatment) and time points up to two years follow up. | |
Primary | Blood levels of chemokines and lipid mediators | Immunoassay and mass spectrometry of chemokines (plasma CCL2) and lipid metabolites (urinary PGE-M) | A) Change between baseline (pre-treatment) and before liver surgery. B) Change between baseline (pre-treatment) and 6 months after liver surgery. C) Change between baseline (pre-treatment) and time points up to two years follow up. | |
Primary | Effect of human faecal samples from patients treated with EPA or placebo on tumour burden in gnotobiotic mice with colorectal cancer liver metastasis | Liver tumour size | A) Change between baseline (pre-treatment) and before liver surgery. B) Change between baseline (pre-treatment) and 6 months after liver surgery. C) Change between baseline (pre-treatment) and time points up to two years follow up. | |
Primary | Effect of human faecal samples from patients treated with EPA or placebo on anti-tumour immune response in gnotobiotic mice with colorectal cancer liver metastasis | Flow cytometry and immunohistochemistry for immune cell populations and cytokine/chemokine levels | A) Change between baseline (pre-treatment) and before liver surgery. B) Change between baseline (pre-treatment) and 6 months after liver surgery. C) Change between baseline (pre-treatment) and time points up to two years follow up. |
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