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. 2017 Nov 16;98(12):2895–2911. doi: 10.1099/jgv.0.000980

Table 1. Novel VSV recombinants used as oncolytic agents against cancer (reported 2012–2017).

VSV recombinants used as oncolytic agents against cancer designed before 2012 can be found in Table 1 of our previous review [8]. * Designed to prevent premature clearance of VSV.

Novel oncolytic VSV Virus description Ref Designed to improve:
Oncolselectivity Safety Direct oncotoxicity VSV survival* Tumour immunity
WT and miscellaneous
VSV-12'GFP VSV expressing GFP reporter gene at position 1 and 2. Attenuated because all VSV genes are moved downward, to positions 3–7. Safe and still effective as an OV. [36] X
VSVFMDV and VSVHRV Insertion of foot-and-mouth disease virus IRES and human rhinovirus type 2 IRES elements before the start codon of the M gene. Controlled the translation of VSV-M. [55] X X
Foreign glycoprotein
VSV-αRGD, -αEchi, -αHER2 and -αEGFR VSV encoding a modified VSV-G displaying tumour vasculature-targeting ligands (cyclic RGD and echistatin) and single-chain antibodies (scFv) against tumour-specific antigens (human epidermal growth factor receptor-2 and epidermal growth factor receptor) [37] X X
VSVFH with H mutations Chimeric VSV (lacks VSV-G) encoding the MV F and H. Different mutations were made to H to disrupt attachment to nectin-4, SLAM and CD46. [44] X X
VSVFH-αHER2 Chimeric VSV (lacks VSV-G) encoding the MV F and H displaying single-chain antibodies (scFv) specific for human epidermal growth factor receptor-2. Retargeted VSV to cells that expressed the targeted receptor. [42] X X
VSV-CD133 Chimeric VSV (lacks VSV-G) encoding the MV F and H displaying single-chain antibodies (scFv) specific for CD133. Retargeted VSV to cells that expressed the targeted receptor. [43] X X
rVSV(GP) Chimeric VSV (lacks VSV-G) encoding the non-neurotropic glycoprotein of LMCV. [46] X X X
VSV-gp160G Chimeric VSV (lacks full-length VSV-G) encoding a hybrid fusion protein, combining domains from gp160 of HIV-1 and VSV-G. Retargeted VSV to human T-cell lymphotropic virus type 1-associated adult T-cell leukemia. [47] X X
VSV-RABV-G, VSV-LASV-GPC, VSV-LCMV-GPC, VSV-EBOV-GP, VSV-MARV-GP Chimeric VSV (lacks VSV-G) encoding the G of rabies virus, Lassa virus, LCMV, Ebola virus or Marburg virus. [48] X X
VSVΔG-CHICKV, VSVΔG-H5N1, VSVΔG-Nipah F, VSVΔG-Nipah G, VLV Chimeric VSV (lacks VSV-G) encoding the G of chikungunya virus, influenza virus H5N1, and Nipah virus F and G. For VLV only VSV-G is used and all other VSV genes are deleted and replaced by the Semliki Forest virus non-structural protein genes. [49] X X
VSV/Maraba G VSV-G is deleted and replaced by the glycoprotein genes from Maraba virus. Resistant to non-immune human serum. [112] X
Cancer suppressors
VSVΔM51eqFP650-p53wt, -p53CC, -p53CC/fs VSV expressing the human p53 gene. [98] X X X X
Immunomodulation
VSV-mIFNbeta-/hIFNbeta-NIS VSV expressing the murine (m) or human (h) IFNβ gene and the thyroidal NIS. [31] X X X X
VSV28.1 and VSV28.2 VSV expressing IL-28, a member of the type III IFN (IFN-λ) family, at position 1 and 5. [34] X X X
VSVΔ51-IFNγ VSV expressing the murine IFN-γ gene. [116] X X X X
VSV-NRAS, VSV-TYRP1 and VSV-CYC1 VSV expressing neuroblastoma-Ras, cytochrome c and tyrosinase-related protein 1. [117] X X
VSV-HIF-2α, VSV-Sox-10, and VSV-c-Myc VSV expressing hypoxia-inducible factor [HIF]–2α, Sox-10, c-Myc. [118] X X