| Literature DB >> 30832256 |
Abstract
RNA viruses have been subjected to substantial engineering efforts to support gene therapy applications and vaccine development. Typically, retroviruses, lentiviruses, alphaviruses, flaviviruses rhabdoviruses, measles viruses, Newcastle disease viruses, and picornaviruses have been employed as expression vectors for treatment of various diseases including different types of cancers, hemophilia, and infectious diseases. Moreover, vaccination with viral vectors has evaluated immunogenicity against infectious agents and protection against challenges with pathogenic organisms. Several preclinical studies in animal models have confirmed both immune responses and protection against lethal challenges. Similarly, administration of RNA viral vectors in animals implanted with tumor xenografts resulted in tumor regression and prolonged survival, and in some cases complete tumor clearance. Based on preclinical results, clinical trials have been conducted to establish the safety of RNA virus delivery. Moreover, stem cell-based lentiviral therapy provided life-long production of factor VIII potentially generating a cure for hemophilia A. Several clinical trials on cancer patients have generated anti-tumor activity, prolonged survival, and even progression-free survival.Entities:
Keywords: RNA viruses; animal models; cancer therapy; clinical trials; gene therapy; immunogenicity; prolonged survival; protection; vaccine
Mesh:
Substances:
Year: 2019 PMID: 30832256 PMCID: PMC6471356 DOI: 10.3390/genes10030189
Source DB: PubMed Journal: Genes (Basel) ISSN: 2073-4425 Impact factor: 4.096
Characteristics of RNA viruses.
| Virus | Genome | Insert Size | Features | Ref |
|---|---|---|---|---|
| Retroviruses | ssRNA | 8 kb | Transduction uniquely of dividing cells | [ |
| Lentiviruses | ssRNA | 8 kb | Broad host range (non-dividing cells) | [ |
| Alphaviruses | ssRNA | 8 kb | Broad host range including neurons | [ |
| Flaviviruses | ssRNA | 6 kb | Relatively broad host range | [ |
| Rhabdoviruses | ssRNA | 6 kb | Relatively broad host range | [ |
| Measles viruses | ssRNA | 6 kb | Self-amplifying RNA replicon | [ |
| NDV | ssRNA | 6 kb | Replication in tumor cells | [ |
| Picornaviruses | ssRNA | 6 kb | Oncolytic strains | [ |
HIV, human immunodeficiency virus; KUN, Kunjin virus; MMLV, Moloney murine leukemia virus; MMSV, Moloney murine sarcoma virus; MSCV, murine stem cell virus; NDV, Newcastle disease virus; SFV, Semliki Forest virus; SIN, Sindbis virus; ssRNA, single-stranded RNA; VEE, Venezuelan equine encephalitis virus; VSV, vesicular stomatitis virus; VV, vaccinia virus; YFV, yellow fever virus.
Examples of preclinical studies on RNA viral-based gene therapy and vaccines.
| Viral Vector | Disease | Target | Response | Ref |
|---|---|---|---|---|
|
| ||||
| RRV/Toca511+5-FC | Glioma | CD | Prolonged survival in mice | [ |
| GRV | X-CGD | SINfes.gp91s | Protection against | [ |
| RV | Cancer | NK cells | Support for GMP grade production | [ |
| COL7A1 | RDEB | Collagen VII | Reversed RDEB in mice | [ |
| RV | XP | XPC | Skin regeneration in mouse model | [ |
|
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| HIV-1 | PD | RNAi | Down-regulation of α-synuclein | [ |
| HIV-1 | PD | GAD67 | Normalized neuronal activity | [ |
| HIV-1 | AD | RNAi | Reduction in neurodegeneration | [ |
| HIV-1 | AD | siRNA | Reduction in tau phosphorylation | [ |
| HIV-1 | SCI | AQP4-RNAi | Accelerated motor function | [ |
| HIV-1 | PKD | PKLR | Corrected hematological phenotype | [ |
| HIV-1 | β-thalassemia | β-globin | Therapeutic efficacy, no toxicity | [ |
| HIV (BB305) | SCID-X1 | IL2RG | Restoration of T, B, and NK cell counts | [ |
| HIV-CAR-T | AML | CD123 | Rapid elimination of leukemia in mice | [ |
| HIV-CAR-T | Ovarian CA | TAA | Potential ovarian cancer treatment | [ |
| HIV-CAR-T | SHIV | CD46-CD4 | Protection against SHIV | [ |
| Cal-1 anti-HIV | SHIV | Cal-1 | Safe integration | [ |
|
| ||||
| SFV | Lung CA | EGFP | Prolonged survival | [ |
| SFV | Glioma | IL-12 | Tumor regression, prolonged survival | [ |
| SFV | Glioma | miRNAs | Tumor targeting, prolonged survival | [ |
| M1 | Liver CA | oncolytic M1 | Tumor growth inhibition | [ |
| VEE | EBOV | EBOV NP | Protection against Ebola virus | [ |
| VEE | EBOV | EBOV GP, NP | Protection against Ebola virus | [ |
| SFV | EBOV | EBOVGP, VP40 | Neutralizing antibodies | [ |
| SFV | HIV | Env | Humoral response | [ |
| SFV | HIV | Env/Gag/Pol | Antigen-specific immune response | [ |
| VEE | Influenza | HA | Protection against influenza in chicken | [ |
| SFV | Influenza | HA, NP | Protection against influenza in mice | [ |
| VEE | Influenza | HA | Protection against influenza in mice | [ |
| VEE | Lassa | GP | Protection against Lassa in mice | [ |
|
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| KUN | Colon CA | G-CSF | Tumor regression | [ |
| KUN | Melanoma | G-CSF | Tumor regression | [ |
| Zika virus | Glioblastoma | Glioma cells | Specific killing of GSCs | [ |
| KUN | SIV | SIV gag-pol | Protection against SIV | [ |
|
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| VSV | EBOV | EBOV-GP | Protection against EBOV in macaques | [ |
| VSV | EBOV | EBOV-GP | Protection against EBOV in primates | [ |
| VSV | MARV | MARV-GP | Protection against EBOV in primates | [ |
| VSV | Melanoma | VSV-GP | Prolonged survival in mice | [ |
| VSV + ruxilitinib | Ovarian CA | VSV-GP | Oncolytic activity | [ |
| VSV | Prostate CA | VSV-GP | Long-term remission in mice | [ |
|
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| MV | Dengue | Dengue DV2 | Neutralizing antibodies in mice | [ |
| MV | Dengue | Dengue DV1-4 | Protection against Dengue in mice | [ |
| MV | HBV | HBsAg | Humoral response in mice, primates | [ |
| MV | Brain CA | SLAM, EGFR | Tumor regression in mice | [ |
| MV | Breast CA | CEA | Prolonged survival in mice | [ |
| MV | Lung CA | SLAM | Tumor suppression in mice | [ |
| MV | Pancreatic CA | SLAM | Tumor suppression in mice | [ |
| MV | Prostate CA | CEA | Prolonged survival in mice | [ |
|
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| NDV TS09-C | NDV | NDV-GFP | Protection against NDV in chicken | [ |
| NDV | Neuroblastoma | NDV 73-T | Complete tumor regression in mice | [ |
| NDV-F | Colon CA | IL-2 | Long-term remission in mice | [ |
| NDV LaSota | Melanoma | IL-15 | Suppression of tumor growth in mice | [ |
| NDV D90 | Lung CA | NDV D90, GFP | Suppression of tumor growth in mice | [ |
| NDV | Melanoma | IL-2 + TRAIL | Prolonged survival in mice | [ |
| NDV | HCC | IL-2 + TRAIL | Prolonged survival in mice | [ |
| NDV Anhinga | HCC | TRAIL | Cure and protection against re-challenges | [ |
| VSV-NDV | HCC | VSV-NDF | Prolonged survival in mice | [ |
|
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| CVB3 | IN | FGF2 | Protection against ischemic necrosis | [ |
| CAV21 | Melanoma | ICAM1, DAF | Tumor regression, also in metastases | [ |
| CAV21 | Breast CA | ICAM1, DAF | Improved tumor regression | [ |
| CAV21 + DH | Breast CA | ICAM1. DAF1 | Tumor regression, dose dependence | [ |
| CAV21, EV1 | Prostate CA | DAFv | Superior tumor regression | [ |
| CVB3 | Coxsackievirus | CVB3-IFN-γ | Protection against Coxsackievirus | [ |
5-FC, 5-fluorocytosine; AD, Alzheimer’s disease; AML, acute myeloid leukemia; AQP4, Aquaporin-4; CA, carcinoma; CAR-T, chimeric antigen receptor T cell; CAV21, Coxsackievirus A21; CEA, carcinoembryonic antigen; CD, cytosine deaminase; CVB3, Coxsackievirus B3; DAF, decay-accelerating factor; DH, doxorubicin hydrochloride; EBOV, Ebola virus; G-CSF, Granulocyte-Colony Stimulating Factor; GP, glycoprotein; GRV, gammaretrovirus; EGFR, epidermal growth factor receptor; FGF2, fibroblast growth factor-2; GSCs, glioblastoma stem cells; HA, hemagglutinin; HBV, hepatitis B virus; HBsAg, hepatitis B surface antigen; HCC, hepatocellular carcinoma; HIV, human immunodeficiency virus; ICAM-1, intercellular adhesion molecule-1; IL2RG, interleukin-2 receptor γ gene; IL, interleukin; IN, ischemic necrosis; KUN, Kunjin virus; MARB, Marburg virus; miRNAs, micro-RNAs; MV, measles virus; NDV, Newcastle disease virus; NP, nucleoprotein; PD, Parkinson’s disease; PKD, pyruvate kinase deficiency; PKLR, pyruvate kinase isoenzymes L/R; RDEB, Recessive Dystrophic Epidermolysis Bullosa; RNAi, RNA interference; RV, retroviral vector; RRV, retroviral replicating vector; SCI, spinal cord injury; SCID, severe combined immunodeficiency; SHIV, Simian/Human Immunodeficiency Virus; SFV, Semliki Forest virus; siRNA, small interfering RNA; SLAM, signaling lymphocyte activation molecule; TAA, tumor associated antigen; TRAIL, tumor necrosis factor-related apoptosis inducing ligand; VEE, Venezuelan equine encephalitis virus; VSV, vesicular stomatitis virus; VSV-GP, VSV pseudotyped with lymphocytic choriomeningitis virus glycoprotein; X-CGD, X-linked chronic granulomatous disease; XP, Xeroderma pigmentosium.
Examples of Clinical Trials Conducted with RNA Viral Vectors.
| Viral Vector | Disease | Phase | Response | Ref |
|---|---|---|---|---|
| Toca 511 RV | HGG | Phase I | Prolonged survival | [ |
| Toca 511 RV | HGG | Phase II/III | Study in progress | [ |
| GRV | CGD | Phase I/II | Resolved bacterial & fungal infections | [ |
| LV hCEF-CT | CT | Phase 0 | Established parameters for Phase I CT trial | [ |
| LentiGlobin BB305 | β-thalassemia | Phase I/II | Reversion of need of red-blood cell transfusions | [ |
| LV pELPs 19-BB-z | CLL | Case report | CLL remission for 10 months | [ |
| LV CTL019 | ALL | Phase I | Sustained ALL remission, prolonged survival | [ |
| LV CTL019 | ALL | Approved | FDA approval for refractory/relapsed ALL | [ |
| LV-FVIII | Hemophilia A | Phase 0 | Potential cure, life-long production of FVIII | [ |
| LV-FIX | Hemophilia B | Phase 0 | High level expression of | [ |
| LV ProSavin® | PD | Phase I/II | Improvements in motor behavior | [ |
| LVsh5/C46 | HIV | Phase I | Safe, protection of the immune system | [ |
| VEE-gB/pp65 | CMV | Phase I | CMV-specific antibodies | [ |
| VEE-gag | HIV | Phase I | Low-level antibody responses | [ |
| VEE-CEA | Breast, colorectal, pancreatic CA | Phase I | Prolonged survival | [ |
| VEE-PSMA | CRPC | Phase I | Neutralizing antibodies | [ |
| LipoVIL12 | Melanoma, kidney CA | Phase I | Safe delivery, tumor targeting | [ |
| VSV-ZEBOV | EBOV | Phase I | Safe administration, antibody responses | [ |
| VSVΔG-ZEBOV | EBOV | Phase I | Safe administration, sustainable IgG responses | [ |
| VSV-ZEBOV | EBOV | Phase I/II | Better tolerability, reduced antibody responses | [ |
| VSVΔG-ZEBOV | EBOV | Phase III | Better immune response than for Ad vector | [ |
| VSV-ZEBOV | EBOV | Phase III | Safe administration, protection against EBOV | [ |
| VSV-ZEBOV | EBOV | Phase III | Safe administration, protection against EBOV | [ |
| VSV-ZEBOV | EBOV | Phase II/III | Safe administration, no EBOV cases | [ |
| MV-EZ | CTCL | Phase I | Regression of CTCL lesions | [ |
| MV-CEA | Ovarian CA | Phase I | Stable disease | [ |
| MV-CEA | Glioblastoma | Phase I | No dose-related toxicity in initial patients | [ |
| MV-NIS | Myeloma | Phase I | Complete response in one patient | [ |
| NDV-TAA | Prostate CA | Phase II | Prolonged survival | [ |
| NDV PV701 | Solid tumors | Phase II | Progression-free survival | [ |
| NDV | Melanoma | Phase II/III | Failure to provide superiority to controls | [ |
| NDV | Colorectal CA | Phase II | Prolonged survival | [ |
| CVA21 | Melanoma | Phase I/II | Good tolerance, anti-tumor activity | [ |
| CVA2 1 + ICB | Melanoma | Phase II | Enhanced anti-tumor activity | [ |
| CVA21 + PLMAb | Melanoma | Phase 1b | Stable disease | [ |
Ad, adenovirus; ALL, Acute lymphocytic leukemia; CA, carcinoma; CAV21, Coxsackievirus A21; CEA, carcinoembryonic antigen; CGD, chronic granulomatous disease; CMV, cytomegalovirus; CRPC, castration resistant metastatic prostate cancer; CT, cystic fibrosis; CLL, chronic lymphocytic leukemia; CTCL, cutaneous T cell lymphoma; EBOV, Ebola virus; GRV, gammaretrovirus; HGG, high-grade glioma; HIV, human immunodeficiency virus; ICL, immune checkpoint blockade; IL, interleukin; LipoVIL-12; liposome-encapsulated SFV-IL-12; LV, lentivirus; MV, measles virus; NDV, Newcastle disease virus; NIS, sodium iodide symporter; PD, Parkinson’s disease; PLMab, pembrolizumab; PSMA, prostate-specific membrane antigen; RV, retroviral vector; TAA, tumor-associated antigen; VEE, Venezuelan equine encephalitis virus; VSV, vesicular stomatitis virus; ZEBOV, Ebola virus Zaire strain.