Trials / Completed

CompletedNCT05924685

PREPARE-iVAC Trial

Prospective Randomized Trial of Everolimus Replacing MMF/MP Acid by the RECOVAC Consortium to Increase VACcine Response in Kidney Transplant Patients

Summary

Objective: To investigate whether replacement of MMF/MPA by everolimus in kidney transplant recipients results in superior immunogenicity of COVID-19 vaccination as measured by neutralizing antibody titer against the Omicron XBB.1.5 strain. Trial design: Multicentre, open-label randomized controlled clinical trial, for a duration of at least 10 weeks with an optional extension to 18 weeks. Trial population: Kidney transplant recipients, 18 years or older, who are at least 6 months after transplantation, with a functioning kidney transplant, using MMF/MPA in combination with at least one other immunosuppressant including a calcineurin inhibitor (CNI), with at least 3 previous COVID-19 vaccinations (=basic COVID-19 immunisation). Interventions: Patients will be randomized into one of two equally sized groups, with either continuation of their current immunosuppressive regimen including MMF/MPA or replacement of MMF/MPA by everolimus during at least six weeks before until four weeks after the last vaccination. Patients will receive a repeated COVID-19 vaccination with the monovalent Omicron XBB.1.5 vaccine, 28 days thereafter they can opt to also receive two herpes zoster vaccinations with the Recombinant Zoster Vaccine (RZV) with an interval between the first and second dose of 28 days. Main trial endpoints: The neutralizing antibody titer against the Omicron XBB.1.5. strain 28 days after monovalent Omicron XBB.1.5 COVID-19 vaccination in patients continuing MMF/MPA compared to patients who switched to everolimus. Secondary trial endpoints: * SARS-CoV-2 specific anti-S1 antibody level at 28 and 56 days after COVID-19 vaccination * Varicella zoster specific anti-gE antibody level 28 days after 1st and 2nd herpes zoster vaccination * SARS-CoV-2 specific T-cell response 28 days after COVID-19 vaccination * Varicella zoster specific T-cell response 28 days after 2nd herpes zoster vaccination * Safety in terms of incidence of acute rejection, kidney function decline, SAEs, AESIs and solicited local and systemic AEs after COVID-19 and herpes zoster vaccination

Detailed description

Rationale: The immunogenicity after vaccination against SARS-CoV-2 and other pathogens is diminished in kidney transplant recipients. This patient group therefore remains extremely vulnerable for viral infections despite vaccination. This impaired immune response is related to the use of immunosuppressive agents, especially Mycophenolate Mofetil/Mycophenolic Acid (MMF/MPA). Patients that use everolimus instead of MMF/MPA elicit a higher immune response after vaccination. Objective Primary objective: To investigate whether replacement of MMF/MPA by everolimus in kidney transplant recipients results in superior immunogenicity of COVID-19 vaccination as measured by neutralizing antibody titer against the Omicron XBB.1.5 strain. Secondary objectives: * To investigate whether replacement of MMF/MPA by everolimus in kidney transplant recipients results in superior humoral immunogenicity of * COVID-19 vaccination as measured by SARS-CoV-2 specific anti-S1 antibody levels * herpes zoster vaccination as measured by varicella zoster specific anti-gE antibody levels * To investigate whether replacement of MMF/MPA by everolimus in kidney transplant recipients results in superior cellular immunogenicity of * COVID-19 vaccination as measured by SARS-CoV-2 specific T-cell response * herpes zoster vaccination as measured by varicella zoster specific T-cell response * To evaluate safety of replacement of MMF/MPA by everolimus in terms of * incidence of treated acute rejection, kidney function decline, incidence of serious adverse events (SAEs) * incidence of adverse events of special interest (AESI) of immunosuppression * incidence of solicited adverse events (AEs) of COVID-19 vaccination * incidence of solicited AEs of herpes zoster vaccination This is a multicentre, open-label, controlled, randomized study to evaluate replacement of MMF/MPA by everolimus in KTR on immunogenicity and safety after vaccination. The seven participating study sites are Amsterdam UMC, Erasmus MC, Leiden UMC, Maastricht UMC+, Radboudumc, UMC Groningen and UMC Utrecht. At the first study visit, eligibility for study participation will be checked, blood will be drawn, and participants will subsequently be 1:1 randomised to: 1. Continue immunosuppressive therapy with MMF/MPA 2. Replace immunosuppressive therapy with MMF/MPA by everolimus After randomisation, the study will continue in 2 parts: Part 1 - Run-in and COVID-19 vaccination (≥6 weeks + 28 days) The aim of this phase is to first ensure complete washout of MMF/MPA and attaining optimal trough levels of everolimus in patients randomized to everolimus. To monitor tolerability, safety and trough levels, participants will be invited at week 1 and week 3 after randomisation for a blood withdrawal and spot urine collection. At least 6 weeks after randomisation, patients will receive the COVID-19 vaccination (=baseline visit). After 28 days patients will be invited for a study visit for blood withdrawal. Part 2 (optional) - Herpes zoster vaccination (+56 days) Patients that opted to participate in this part of the study will continue their randomised treatment for the next 56 days. During this period patients will receive 2 herpes zoster vaccinations with an interval of 28 days between each vaccination. At 28 days after the second vaccination patients will be invited for the last study visit for blood withdrawal. After completion of the study (either 28 days after COVID-19 vaccination or 28 days after the last herpes zoster vaccination) patients will be offered the option to continue everolimus instead of MMF/MPA as part of shared clinical decision making.

Conditions

• COVID-19 Vaccines
• Varicella Zoster Vaccine
• Vaccine Response
• Immunosuppression

Interventions

Timeline

Start date

2023-08-22

Primary completion

2023-12-29

Completion

2024-02-27

First posted

2023-06-29

Last updated

2024-03-04

Locations

7 sites across 1 country: Netherlands

Source: ClinicalTrials.gov record NCT05924685. Inclusion in this directory is not an endorsement.