IBD Clinical Trial
Official title:
Immunogenicity of COVID-19 Vaccine in Patients With Inflammatory Bowel Disease
Verified date | December 2022 |
Source | University of Wisconsin, Madison |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Observational |
The overall objective of this proposal is to evaluate the safety and immunogenicity of a COVID-19 vaccine in patients with Inflammatory Bowel Disease (IBD). This will help determine if immunosuppressive regimens impact COVID-19 vaccine response. The investigators will determine if certain groups may need more doses of a vaccine, with future adjuvanted vaccines or require a booster to maintain immunity. 260 participants with IBD and scheduled to get a COVID-19 vaccine will be recruited and can expect to be on study for 18 months.
Status | Completed |
Enrollment | 222 |
Est. completion date | November 11, 2022 |
Est. primary completion date | November 11, 2022 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years to 85 Years |
Eligibility | Inclusion Criteria: For mRNA cohort: - Participant has a history of ulcerative colitis (UC) or Crohn's disease diagnosed by standard clinical, radiographic, endoscopic, and histopathologic criteria. - On one of the following treatment regimens: - Group A: Non-systemic immunosuppressive Group at least 75 participants - Mesalamine monotherapy or no therapy for IBD - Vedolizumab Therapy Group: on either vedolizumab monotherapy or combination therapy with methotrexate or azathioprine - Group B: Systemic immunosuppressive Group at least 75 participants - Thiopurine Therapy Group: on azathioprine at least 2.0mg/kg or 6MP 1.0mg/kg - Anti-TNF Therapy Group: on maintenance therapy infliximab (at least 8 every 8 weeks), golimumab (at least monthly), adalimumab (at least every 2 weeks), or certolizumab (at least monthly) - Anti-TNF Combination Therapy Group: on anti-TNF therapy as described above along with either 15mg of methotrexate or azathioprine at least 1.0mg/kg or 6MP 0.5mg/kg - Ustekinumab Therapy Group: on either ustekinumab monotherapy or combination therapy with methotrexate or azathioprine. - Tofacitinib Therapy Group: on tofacitinib at least 5mg PO BID - Corticosteroid Therapy Group: on any one of the systemic immunosuppressive groups and any dose of corticosteroids - Participant has been on the same IBD treatment for at least two months. - Participant is receiving an mRNA COVID-19 vaccine per standard of care recommended by their clinical provider or has started the COVID-19 series or finished the mRNA COVID-19 vaccine series within the past six months and would qualify for six month study visits or has received a third dose of the vaccine as standard of care. - Participants entering in the study at the six month study visit must have been on same treatment at their time of immunization. For Viral vector cohort: - Participant has a history of ulcerative colitis (UC) or Crohn's disease diagnosed by standard clinical, radiographic, endoscopic, and histopathologic criteria. - On one of the following treatment regimens: - Group A: Non-systemic immunosuppressive Group at least 15 participants - Mesalamine monotherapy or no therapy for IBD - Vedolizumab Therapy Group: on vedolizumab monotherapy - Group B: Systemic immunosuppressive Group at least 15 participants - Thiopurine Therapy Group: on azathioprine at least 2.0mg/kg or 6MP 1.0mg/kg - Anti-TNF Therapy Group: on maintenance therapy infliximab (at least 8 every 8 weeks), golimumab (at least monthly), adalimumab (at least every 2 weeks), or certolizumab (at least monthly) - Anti-TNF Combination Therapy Group: on anti-TNF therapy as described above along with either 15mg of methotrexate or azathioprine at least 1.0mg/kg or 6MP 0.5mg/kg - Ustekinumab Therapy Group: on either ustekinumab monotherapy or combination therapy with methotrexate or azathioprine. - Tofacitinib Therapy Group: on tofacitinib at least 5mg PO BID - Corticosteroid Therapy Group: on any one of the systemic immunosuppressive groups and any dose of corticosteroids - Participant has been on the same IBD treatment for at least two months. - Participant is receiving a viral vector COVID-19 vaccine per standard of care or has started or finished the viral vector series within the past 6 months. If participant entering at six months and would qualify for six month study visits and has received an additional one or two dose of viral vector of mRNA for a total of two -three COVID vaccines as standard of care. - Participants entering in the study at the six month study visit must have been on same treatment at their time of immunization. Exclusion Criteria: For mRNA cohort: - Allergy to COVID-19 vaccine or a component of it - Participant cannot or will not provide written informed consent - Unable to provide appropriate informed consent due to being illiterate or impairment in decision-making capacity For Viral vector cohort: - Allergy to COVID-19 vaccine or a component of it - Participant cannot or will not provide written informed consent. - Unable to provide appropriate informed consent due to being illiterate or impairment in decision-making capacity. |
Country | Name | City | State |
---|---|---|---|
United States | University of Wisconsin | Madison | Wisconsin |
Lead Sponsor | Collaborator |
---|---|
University of Wisconsin, Madison |
United States,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Change in Geometric Mean Titers (GMT) of SARS-CoV-2 Antibody Concentrations following mRNA COVID-19 vaccine series | The primary endpoint will be evaluating the change in humoral immunity between the immunosuppressive and non-immunosuppressive IBD treatment regimens following the recommended doses mRNA COVID-19 vaccine series. | baseline to 18 months post-2nd dose, 12 months post-3rd dose, or 6 months post-4th dose | |
Primary | Sustained antibody concentrations of mRNA COVID-19 vaccines | The investigators will evaluate sustained antibody concentrations of mRNA COVID-19 vaccines by using a quantitative assay from LabCorp that is currently being used by the CDC to evaluate seroprevalence. | 18 months post-2nd dose | |
Primary | Sustained antibody concentrations of mRNA COVID-19 vaccines | The investigators will evaluate sustained antibody concentrations of mRNA COVID-19 vaccines by using a quantitative assay from LabCorp that is currently being used by the CDC to evaluate seroprevalence. | 12 months post-3rd dose | |
Primary | Sustained antibody concentrations of mRNA COVID-19 vaccines | The investigators will evaluate sustained antibody concentrations of mRNA COVID-19 vaccines by using a quantitative assay from LabCorp that is currently being used by the CDC to evaluate seroprevalence. | 6 months post-4th dose | |
Primary | Change in level of T-cell response after mRNA COVID-19 vaccine | Investigators will evaluate sustained cell mediated immunity against Covid-spike proteins after completing the vaccine schedule of a mRNA COVID-19 vaccine. | 18 months post-2nd dose, 12 months post-3rd dose, or 6 months post-4th dose | |
Primary | Percentage of participants with detectable level of T-cell response after mRNA COVID-19 vaccine | For each patient, peripheral blood monocytes (PBMCs) will be isolated. IFN-? ELISpot, which detects both CD4 and CD8 T cell effectors, will be used to detect T-cell immunity to the Covid-spike protein or peptides. The plates will be read on an AID ELISpot reader (Cell Technology, Inc., Columbia MD, reader software v.3.1.1.). A positive response to antigen will be defined as a frequency that was significantly (p < 0.05, two-tailed t test) greater than the mean of control no-antigen wells and detectable (i.e., >1:100,000). T cell responses will be correlated to Covid-19 neutralizing antibody responses. | 18 months post-2nd dose, 12 months post-3rd dose, or 6 months post-4th dose | |
Secondary | Incidence of Adverse Events | Safety will be assessed by the incidence of adverse events (AEs and SAEs) related to the vaccine. | up to 1 month post final immunization | |
Secondary | Patient reported outcome 3 (PRO3) score | Safety will be assessed by monitoring the PRO3 scores at baseline and 1 month post-vaccination. PRO-3 is a measure of overall well-being as well as specific symptoms and complications of CD, such as stool frequency, abdominal pain and general well being. Greater PRO3 scores indicate more severe CD symptoms. | baseline, 18 months post-2nd dose, 12 months post-3rd dose, or 6 months post-4th dose | |
Secondary | Simple Colitis Activity Index (SCAI) Questionnaire Score | For participants with Ulcerative Colitis (UC), safety will be assessed by monitoring the SCAI score at baseline and 1 month post-vaccination. SCAI is a measure of overall well-being as well as specific symptoms and complications of UC, such as stool frequency and abdominal pain. The total possible range of scores is 0-21, with higher scores indicative of increased symptoms. | baseline, 18 months post-2nd dose, 12 months post-3rd dose, or 6 months post-4th dose | |
Secondary | Seroconversion: assessed by percentages of participants with =4-fold rise in antibody titer | Percentages (and 2-sided 95% CIs) of participants with =4-fold rise will be assessed for the COVID-19 vaccine within each group. | 1 month post-immunization | |
Secondary | Change in Geometric Mean Titers (GMT) of SARS-CoV-2 Antibody Concentrations following two doses of viral vector COVID-19 vaccine series | The primary endpoint will be evaluating the change in humoral immunity between the immunosuppressive and non-immunosuppressive IBD treatment regimens following the two doses viral vector COVID-19 vaccine series. | baseline,18 months post-2nd dose, 12 months post-3rd dose, or 6 months post-4th dose | |
Secondary | Sustained antibody concentration of viral vector COVID-19 vaccines | The investigators will evaluate sustained antibody concentrations of viral vector COVID-19 vaccines by using a quantitative assay from LabCorp that is currently being used by the CDC to evaluate seroprevalence. | 18 months post-2nd dose, 12 months post-3rd dose, or 6 months post-4th dose | |
Secondary | Percentage of participants with detectable level of T-cell response after viral vector COVID-19 vaccine | For each patient, peripheral blood monocytes (PBMCs) will be isolated. IFN-? ELISpot, which detects both CD4 and CD8 T cell effectors, will be used to detect T-cell immunity to the Covid-spike protein or peptides. The plates will be read on an AID ELISpot reader (Cell Technology, Inc., Columbia MD, reader software v.3.1.1.). A positive response to antigen will be defined as a frequency that was significantly (p < 0.05, two-tailed t test) greater than the mean of control no-antigen wells and detectable (i.e., >1:100,000). T cell responses will be correlated to Covid-19 neutralizing antibody responses. | 18 months post-2nd dose, 12 months post-3rd dose, or 6 months post-4th dose | |
Secondary | Change in level of T-cell response after viral vector COVID-19 vaccine | Investigators will evaluate sustained cell mediated immunity against Covid-spike protein after completing the vaccine schedule of a viral vectors vaccine. | 18 months post-2nd dose, 12 months post-3rd dose, or 6 months post-4th dose | |
Secondary | Presence of SARS-CoV2 anti-nucleocapside antibody : Yes/No | To evaluate the rate of asymptomatic COVID-19 infections in patients with IBD, investigators will evaluate the presence for anti-nucleocapside antibody in participants at baseline and/or 1 month visit after immunization to evaluate the rate of asymptomatic infection in our cohort. A SARS-CoV2 anti-nucleocapside antibody is not induced by vaccine so it's presence means there was a presence of a previous infection. | baseline, 18 months post-2nd dose, 12 months post-3rd dose, or 6 months post-4th dose |
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