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Phase II Trial to Evaluate an EBV-derived Dendritic Cell Vaccine in Autologous Stem Cell Transplant

Hodgkin Lymphoma Clinical Trial

Official title:
A Randomized Phase II Trial to Evaluate an EBV Derived Dendritic Cell (DC) Vaccine When Administered Alone or Co-administered With the TLR9 Agonist, DUK-CPG-001, in EBV+ Lymphoma in the Setting of Autologous Stem Cell Transplant

Clinical Trial Summary

This is a non-blinded, not placebo controlled, randomized, parallel phase 2 pilot study to evaluate the immunological response and the safety of Epstein Barr Virus (EBV)-derived tumor antigen, Latent Membrane Protein-2 (LMP2)-loaded dendritic cell (DC) vaccines alone or co-administered with the TLR9 ligand, DUK-CPG-001, in patients with EBV+ lymphoma in the setting of autologous stem cell transplant with infusion of mature T cells. Patients will be randomized to receive vaccine alone or vaccine co-administered with the TLR9 ligand, DUK-CPG-001. Randomization will be stratified by 2 disease types: Hodgkin lymphoma and non-Hodgkin lymphoma.

Clinical Trial Description

Objectives

The primary objectives of this study are to:

1. To assess the ability of an Epstein-Barr virus (EBV) derived tumor antigen, LMP2 loaded DC vaccine co-administered with a Toll-like receptor 9 (TLR9) ligand, DUK-CPG-001, to induce EBV derived tumor antigen specific CD8+ T cell response in patients with EBV+ lymphoma in the setting of autologous stem cell transplant

2. To assess the ability of an Epstein-Barr virus (EBV) derived tumor antigen, LMP2 loaded DC vaccine administered alone to induce EBV derived tumor antigen specific CD8+ T cell response in patients with EBV+ lymphoma in the setting of autologous stem cell transplant

3. To evaluate the safety of using LMP2- loaded DC vaccine alone or co-administered with the TLR9 ligand, DUK-CPG-001, in patients with EBV+ lymphoma in the setting of autologous stem cell transplant

The secondary objectives of this study are to:

1. Evaluate duration of the presence of long term memory cells after administration of an LMP2 loaded DC vaccine alone or co-administered with the TLR9 ligand, DUK-CPG-001.

2. Evaluate duration of multi-functional CD8 T cell responses after administration of an LMP2 loaded DC vaccine alone or co-administered with the TLR9 ligand, DUK-CPG-001.

3. Evaluate duration of Th1, Th2 and Th17 CD4 T cell responses as well as CD4+CD25+Foxp3+ regulatory T cell (Treg) responses after administration of an LMP2 loaded DC vaccine alone or co-administered with the TLR9 ligand, DUK-CPG-001.

4. Evaluate the disease free survival (DFS) of patients with EBV+ lymphoma in the setting of autologous stem cell transplant who receive LMP2-loaded DC vaccines alone or co-administered with DUK-CPG-001.

Patient population Patients with EBV+ lymphoma who are in a complete remission (CR) after salvage therapy with plans to proceed to autologous peripheral stem cell transplant .

Immune response will be defined as an increase in number of spots to 25-fold more than at baseline, or at least 200 spots per 105 CD8+ T cells, by Day 7 post 2nd vaccination (i.e., a patient with a baseline of 1 spot/105 CD8+ T cells who achieved 25 spots/million would not be counted as a response).

1. Leukapheresis #1: The first pheresis will be performed after that patient has obtained a complete remission, but prior to transplant. Complete remission will be determined based on Cheson Criteria100. No special preparative regimen is required prior to pheresis but it must occur at least 2 weeks after most recent chemotherapy and most recent granulocytic growth factor.

Pheresis will last approximately 4 hours to collect a goal of 1 x 108 nucleated cells/kg. This will follow standard stem cell transplant Standard Operating Procedures (SOPs). The cells will be transferred to John Sampson's GMP facility (Duke Brain Tumor Immunotherapy Processing Laboratory) where the sample will be divided into DC cell product for making vaccine, T cells for re-infusion during transplant, and research sample that will go to Yiping Yang's lab.

As described below, they will subsequently be defrosted and the T cells will be infused at the time of the autologous stem cell transplant. This will follow standard stem cell transplant Standard Operating Procedures (SOPs).Please see appendix 8.6 Cell collection: removal of PBMCs by leukapheresis.

2. Leukapheresis # 2: This is a standard-of-care pheresis to collect cells for the autologous stem cell transplant and will be performed as per the usual stem cell transplant and pheresis SOP.

Leukapheresis will follow institutional norms.

3. Stem Cell Transplant will follow institutional norms. The standard minimum infusion of CD34+ PBSC cells required for autologous stem cell transplant is 2 x 106 cd34+ cells/kg (range 2-7). The standard transplant preparative regimens used are BEAM or BCV.

4. T Cell Infusion: T cells will be thawed and infused through an IV after the autologous stem cell graft infusion has been completed. This will be infused following the stem cell transplant Standard Operating Procedure (SOP) for re-infusion of thawed transplant products (SOP ABMT-GEN-017).

5. Post Transplant Vaccine #1: Nine -13 weeks status PBSC transplant, patients will receive their first post-transplant vaccination. At the time of vaccination, ANC must be > 1.5. Delays beyond 13 weeks may be allowed after discussion with the PI. Delays beyond the 13 weeks will be decided on by the PI on a case by case basis but will only be allowed if delay is due to a slow ANC recovery that has been attributed to a medication or if the delay was for a non-medical reason.

6. Post Transplant Vaccine #2: Four weeks +/- 7 days after post-transplant vaccine #1, a second Boost vaccination will be administered. At the time of vaccination ANC must be > 1.5.

1. Subjects who are randomized to the CPG arm will receive CPG immediately after vaccine #1 and vaccine #2.

7) Blood samples for evaluation of immune response will be collected throughout the study procedures. Specifically, blood samples will be obtained within 7 days prior to initial leukapheresis. Blood will also be collected prior to receiving vaccine # 1 and #2 on the day on which vaccine is administered or up to 2 days before hand. In addition, blood will be drawn 7 days after each vaccination and at one, three and six months after the second vaccination. These blood samples will be used for analyzing T cell responses as detailed in section 3.7. The day 7 draws must be drawn +/- 2 day. The one, three and six month draws may occur +/- 1 week. ;

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment

Related Conditions & MeSH terms

Clinical Trial Details
NCT number NCT02115126
Study type Interventional
Source Duke University
Contact
Status Withdrawn
Phase Phase 2
Start date December 2016
Completion date January 2025
View Details
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