Gemogenovatucel-T (Vigil): bi-shRNA plasmid-based targeted immunotherapy.
John J NemunaitisLaura StanberyAdam WalterGladice WallravenAlexander NemunaitisStaci HorvathErnest BognarDonald RaoSteven EngleScott BrunMaurizio GhisoliRodney P RocconiBradley J MonkRobert L ColemanPublished in: Future oncology (London, England) (2024)
We describe in this review the historical evidence leading up to the concept and design of Vigil and subsequent clinical applications including safety and efficacy in a randomized, controlled Phase IIB trial. Vigil (gemogenovatucel-T) is a unique triple function targeted immunotherapy that demonstrates preclinical and clinical systemic anticancer activity. Construction of Vigil involves harvest of autologous malignant tissue for neoantigen targeting (ideally containing clonal neoantigens) followed by a two-day process involving transfection with a plasmid to provide a permissive 'training environment' for the patient's immune system. Transfected plasmid components contain an expressive human GMCSF DNA segment to enhance anticancer immune functional response and a second component expressing bi-shRNA furin which reduces TGFβ isomers (TGFβ1 and TGFβ2) thereby reducing cancer inhibition of the targeted immune response. Results generated to date justify advancement to confirmatory clinical trials supporting product regulatory approval.
Keyphrases
- cancer therapy
- escherichia coli
- clinical trial
- transforming growth factor
- immune response
- crispr cas
- endothelial cells
- phase ii
- drug delivery
- cell therapy
- case report
- phase iii
- bone marrow
- study protocol
- stem cells
- randomized controlled trial
- cell free
- dendritic cells
- single molecule
- inflammatory response
- induced pluripotent stem cells
- signaling pathway
- childhood cancer