Highly stable and immunogenic CMV T cell vaccine candidate developed using a synthetic MVA platform

Author:

Yll-Pico MarcalORCID,Park Yoonsuh,Martinez Joy,Iniguez Angelina,Kha Mindy,Kim Taehyun,Medrano Leonard,Nguyen Vu H.,Kaltcheva Teodora,Dempsey Shannon,Chiuppesi FlaviaORCID,Wussow FelixORCID,Diamond Don J.ORCID

Abstract

AbstractHuman cytomegalovirus (CMV) is the most common infectious cause of complications post-transplantation, while a CMV vaccine for transplant recipients has yet to be licensed. Triplex, a multiantigen Modified Vaccinia Ankara (MVA)-vectored CMV vaccine candidate based on the immunodominant antigens phosphoprotein 65 (pp65) and immediate-early 1 and 2 (IE1/2), is in an advanced stage of clinical development. However, its limited genetic and expression stability restricts its potential for large-scale production. Using a recently developed fully synthetic MVA (sMVA) platform, we developed a new generation Triplex vaccine candidate, T10-F10, with different sequence modifications for enhanced vaccine stability. T10-F10 demonstrated genetic and expression stability during extensive virus passaging. In addition, we show that T10-F10 confers comparable immunogenicity to the original Triplex vaccine to elicit antigen-specific T cell responses in HLA-transgenic mice. These results demonstrate improvements in translational vaccine properties of an sMVA-based CMV vaccine candidate designed as a therapeutic treatment for transplant recipients.

Funder

This research was funded by the City of Hope internal funding.

Publisher

Springer Science and Business Media LLC

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