This is an open label randomized trial to evaluate the efficacy and treatment duration with vedolizumab to patients with immune mediated colitis. The trial will include 82 patients randomized into two arms, either standard treatment with prednisolone (plus infliximab in severe cases) or vedolizumab treatment up front.
Background information Immune check point inhibitors (ICPI) have revolutionized the treatment of a growing number of cancer forms resulting in a rapidly increasing number of patients treated with these drugs within the very recent years. The aim is to allow and boost an immune response towards the neoantigens of neoplastic cells, but the blockage of inhibitory signals might also interfere with normal barriers against the development of autoimmunity or autoimmune-like reactions and thus lead to a number of immune-related adverse events (IrAEs). Gastrointestinal inflammation - typically colitis - is the most common IrAE among ICPI treated patients. Vedolizumab, a integrin antibody, has been shown to be highly effective in treating ICPI induced colitis with remission rates of 85%. Vedolizumab has a better safety profile than anti-tumor necrosis factor antibodies, including infliximab, with lower risk of infections and tumor development in inflammatory bowel disease patients. Moreover, vedolizumab does not seem to inhibit tumor specific T cell responses in vitro, suggesting that this treatment is also beneficial with regards to tumor response. The hypothesis Vedolizumab induction and maintenance treatment of patients with ICPI related intestinal symptoms and evidence of colitis: 1. Is effective in inducing remission of the colitis 2. Reduces the risk of progression from grade 2 to grade 3 or 4 colitis 3. Reduces the need of systemic corticosteroid 4. Is not associated with increased risk of tumor progression or other serious adverse events including serious infections 5. Allows reintroduction/continuation of ICPI treatment. Further it is hypothesized that ICPI induced colitis can be diagnosed and monitored by intestinal bowel ultrasound and treatment response is associated with multi-omics changes in intestinal tissue, tumor tissue, feces, blood, and urine, e.g. peripheral blood mononuclear cells (PBMCs) RNAseq profiles, profiles of single cell RNAseq from isolated immune cells from standard pinch biopsies from the inflamed colon and composition of the microbiota. Lastly, it is hypothesized, that anti-tumor T-cell function is affected in vivo by the medication used to treat ICPI induced colitis, and that this can be assessed by changes in single cell RNAseq profiles of tumor resident T-cells (isolated from tumor biopsies).
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
NONE
Enrollment
82
Repeatedly vedolizumab infusion at week 0, 2, 6, 14, 22
tablet prednisolone plus infliximab in severe cases.
Herlev University Hospital
Herlev, Denmark
RECRUITINGdose of prednisolone
The cumulative dose of corticosteroids (tablets and IV) due to IrAE colitis at week 30
Time frame: Week 30
clinical remission
Clinical remission at week 2, 10 and 30\*, defined as a partial Mayo score ≤ 2.
Time frame: week 2
clinical remission
Clinical remission at week 2, 10 and 30\*, defined as a partial Mayo score ≤ 2.
Time frame: week 10
clinical remission
Clinical remission at week 2, 10 and 30\*, defined as a partial Mayo score ≤ 2.
Time frame: week 30
time to response
Time to clinical remission and eventual relapse of GI symptoms (measured by patient reported stool chart registered the first 30 days).
Time frame: 30 days
partial Mayo score
Response defined as decrease in partial Mayo score ≥ 30 % at week 2, 10 and 30
Time frame: week 2
partial Mayo score
Response defined as decrease in partial Mayo score ≥ 30 % at week 2, 10 and 30
Time frame: week 10
partial Mayo score
Response defined as decrease in partial Mayo score ≥ 30 % at week 2, 10 and 30
Time frame: week 30
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change in scores
change between clinical scores
Time frame: change from week 0 and 10 and 30
fecal calprotectin
change between fecal-calprotectin
Time frame: change from week 0 and 10 and 30
IUS
Intestinal ultrasound
Time frame: change from week 0 and 10 and 30
endoscopy
endoscopy
Time frame: change from week 0 and 30
change in scores
biochemistry
Time frame: change from week 0 and 10 and 30
Life qualtity
Changes in quality of life
Time frame: change from week 0 and 10 and 30
steroid use for other reasons
Corticosteroid use for non-intestinal indications.
Time frame: During the 30 weeks period
ICPI treatment
The proportion of patients able to continue ICPI treatment at any time after inclusion and until week 30\*.
Time frame: Week 30
steroid free remission
Proportion of patients in corticosteroid (tablets or IV) free remission at week 10 and 30\* and the cumulative dose corticosteroid at week 10
Time frame: week 10
steroid free remission
Proportion of patients in corticosteroid (tablets or IV) free remission at week 10 and 30\*
Time frame: week 30
ICPI treatment
Proportion of patients able to continue ICPI treatment at any time after inclusion and until week 30
Time frame: week 30