| Literature DB >> 31769427 |
Kenya Kamimura1, Takeshi Yokoo1, Hiroyuki Abe1, Shuji Terai1.
Abstract
The liver is a key organ for metabolism, protein synthesis, detoxification, and endocrine function, and among liver diseases, including hepatitis, cirrhosis, malignant tumors, and congenital disease, liver cancer is one of the leading causes of cancer-related deaths worldwide. Conventional therapeutic options such as embolization and chemotherapy are not effective against advanced-stage liver cancer; therefore, continuous efforts focus on the development of novel therapeutic options, including molecular targeted agents and gene therapy. In this review, we will summarize the progress toward the development of gene therapies for liver cancer, with an emphasis on recent clinical trials and preclinical studies.Entities:
Keywords: cancer; gene therapy; hepatocellular carcinoma; liver; metastatic liver tumors
Year: 2019 PMID: 31769427 PMCID: PMC6966544 DOI: 10.3390/cancers11121865
Source DB: PubMed Journal: Cancers (Basel) ISSN: 2072-6694 Impact factor: 6.639
Gene delivery methods used in clinical and preclinical stages.
| Gene Transfer Methods | Genetic Materials (Cloning Capacity)/ Functional Component | Advantages | Disadvantages | |
|---|---|---|---|---|
| Viral Vectors | ||||
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| Oncoretrovirus | Single stranded RNA (8 kb) | High transduction efficiency | Infect to dividing cells | Random integration Low efficiency of purification |
| Lentivirus | Single stranded RNA (8 kb) | High transduction efficiency Sustained gene expression Low immune response | Infect to dividing and non-dividing cells | Random integration Low efficiency of purification |
| Foamy virus | Single stranded RNA (9.2 kb) | High transduction efficiency Sustained gene expression No expression of viral proteins Low immune response | Infect to dividing cells Form a stable transduction intermediate in non-dividing cells | Random integration Low efficiency of purification |
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| First generation adenovirus (FGAd) | Double stranded DNA (8–10 kb) | High transduction efficiency | Infect to dividing and non-dividing cells | Transient expression Host innate immune response Complicated vector production |
| Helper-dependent adenovirus (HDAd) | Double stranded DNA (~37 kb) | Large insert size Essentially no integration | Infect to dividing and non-dividing cells | Transient expression Host innate immune response Complicated vector production |
|
| Single stranded DNA (4–5 kb) | Non pathogenic Sustained gene expression Mainly no integration Low immune response | Infect to dividing and non-dividing cells | Integration may occur Small capacity of transgene Transient expression Complicated vector production |
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| Double stranded DNA (~30 kb) | Large insert size No integration Sustained gene expression | Infectivity to nervous system | Transient expression Low transduction efficiency |
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| Cationic charge, hydrophobic domain | High efficiency in vitro, ease to prepare | Low efficiency in vivo, acute immune response | |
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| Cationic charge, polymer | Highly effective in vitro, ease to prepare | Toxic to cells, acute immune response | |
|
| Natural or chemically modified proteins in cationic nature | Highly effective in vitro, less toxic, can be target specific | Low activity in vivo | |
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| Lysine or arginine residues in peptides | Highly effective in vitro, less toxic, can be target specific | Low activity in vivo | |
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| Mechanic force | Simple | Low efficiency, expression limited to needle track | |
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| Pressure | Ease, Good efficiency | Limited to target area, need surgical procedure for internal organ | |
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| Electric pulse | High efficiency | Tissue damage, limited target area, need surgical procedure for internal organ | |
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| Ultrasound | Simple, can be site-specific | Low efficiency, tissue damage | |
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| Magnetic field | Site specific | Low efficiency, limited target area, need surgical procedure for internal organ | |
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| Hydrodynamic pressure | Simple, high efficiency in vivo, site specific | Need catheter insertion technique in large animals | |
|
| CAR-T, T cells | Antigen-specific | Require ex vivo cell culture Poorly effective for solid tumors | |
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| Antigen-pulsed dendritic cells | Ease to prepare less toxic, ease to administer | Low efficacy | |
Figure 1Schematic summary of gene therapy strategies for liver cancers. siRNA: small interfering RNA, miRNA: microRNA, ncRNA: non-coding RNA, CAR-T: chimeric antigen receptor-T-cell.
Summary of ongoing clinical trials for gene therapy for liver cancers.
| No | NCT Number | Types of Liver Tumors | Gene/Antigen | Types of Gene | Vectors or Cells | Intervention | Route of Administration | Phase | Current Status and Results | Ref. |
|---|---|---|---|---|---|---|---|---|---|---|
| 1 | NCT00003147 | HCC | p53 | Adenoviral Vector | Ad5CMV-p53 gene | Percutaneous injection | 1 | Terminated No results available | ||
| 2 | NCT01071941 | Primary Liver Cancers | Oncolytic Virus | Oncolytic Virus | Herpes simplex virus 1 | rRp450 | Hepatic arterial injection | 1 | Recruiting No results available Estimated Completion Date: July, 2020 | |
| Metastatic Liver Tumors | ||||||||||
| 3 | NCT00844623 | HCC | HSVtk | Suicide | Adenoviral vector | TK99UN (adenoviral vector containing TK) | Intratumoral injection | 1 | Completed Results partly reported. | [ |
| 4 | NCT02202564 | HCC | HSVtk | Suicide | Adenoviral vector | LT ADV-TK ganciclovir | Intravenous infusion | 2 | Completed No results reported to date | |
| 5 | NCT02561546 | HCC | p53 | Tumor suppressor | Recombinant adenoviral vector | p53 gene therapy TAE | Hepatic arterial injection following TAE | 2 | Not yet recruiting | |
| 6 | NCT00300521 | HCC | HSVtk | Suicide | Adenoviral vector | ADV-TK | Intravenous infusion | 2 | Completed No results reported to date | |
| 7 | NCT00004178 | Primary Liver Cancers Metastatic Liver Tumors | CEA | Tumor-related Protein Coding | T Cells Modified with Chimeric Anti-CEA Immunoglobulin-T Cell Receptors (IgTCR) in Adenocarcinoma | Therapeutic autologous lymphocytes | Intravenous infusion | 1 | Completed No results reported to date | |
| 8 | NCT03313596 | HCC | HSVtk | Suicide | Adenoviral vector | ADV-TK LT | Intravenous infusion | 3 | Recruiting No results available Estimated Completion Date: Dec, 2019 | |
| 9 | NCT03480152 | Primary Liver Cancers | mRNA containing epitopes from immunogenic neoantigens | Tumor-related Protein Coding | mRNA vaccine | NCI-4650, a mRNA-based, Personalized Cancer Vaccine | Intramuscular injection | 1/2 | Terminated Related results partly reported | [ |
| Metastatic Liver Tumors | mRNA containing epitopes from immunogenic predicted neoantigens | |||||||||
| mRNA containing epitopes from immunogenic mutations in tumor suppressor or driver genes | ||||||||||
| 10 | NCT01967823 | HCC Metastatic Liver Tumors | NY-ESO-1 | Tumor-related Protein Coding | Anti-NY ESO-1 Murine TCR-Gene Engineered Lymphocytes | Anti-NY ESO-1 mTCR PBL Cyclophosphamide Fludarabine Aldesleukin | Intravenous infusion | 2 | Recruiting No results available Estimated Completion Date: July, 2028 | [ |
| 11 | NCT02509169 | HCC | p53 | Tumor suppressor | Recombinant adenoviral vector | TAE plus P53 gene TAE | Hepatic arterial injection following TAE | 2 | Recruiting No results available | |
| 12 | NCT02932956 | Pediatric Primary Liver Cancers | GPC-3 | Tumor-related Protein Coding | CAR T cells | GAP T cells Cytoxan Fludara | 1 | Recruiting No results available Estimated Completion Date: Feb, 2037 | ||
| 13 | NCT00012155 | Metastatic Liver Tumors | Oncoytic Virus | Oncoytic Virus | oncolytic herpes simplex virus type-1(HSV-1) | NV1020, oncolytic herpes simplex virus type-1 (HSV-1) | Hepatic arterial injection | 1 | Completed Results partly reported | [ |
| 14 | NCT00066404 | Metastatic Liver Tumors | Interferon-beta | Genetic Immunotherapy | Adenoviral vector | recombinant adenovirus-hIFN-beta | Intrapleural injection | 1 | Active, not recruiting Results partly reported | [ |
| 15 | NCT00035919 | Metastatic Liver Tumors | Dominant Negative Cyclin G1 | Tumor suppressor | Retroviral Vector | Mx-dnG1 Retroviral Vector | Hepatic arterial infusion | 1/2 | Withdrawn | |
| 16 | NCT00005629 | Primary Liver Cancers Metastatic Liver Tumors | AFP | Tumor-related Protein Coding | AFP peptide | AFP gene hepatocellular carcinoma vaccine | Intradermal injection | 1/2 | Completed No results reported to date | |
| 17 | NCT02905188 | HCC | GPC-3 | Tumor-related Protein Coding | CAR T cells | GLYCAR T cells | Intravenous infusion | 1 | Recruiting No results available Estimated Completion Date: Oct, 2036 | |
| 18 | NCT00093548 | HCC | AFP, GM-CSF | Tumor-related Protein Coding | Adenoviral vector | Vaccination AFP plasmid DNA vaccine GM-CSF plasmid DNA hepatocellular carcinoma vaccine adjuvant | Intramuscular injection/Intradermal injection | 1/2 | Withdrawn | [ |
| 19 | NCT01628640 | Primary Liver Cancers Metastatic Liver Tumors | Interferon-beta | Genetic Immunotherapy | Vesicular Stomatitis Virus | Recombinant Vesicular Stomatitis Virus-expressing Interferon-beta | Intratumoral Injection | 1 | Active, not recruiting Estimated Completion Date: June, 2025 | |
| 20 | NCT03602079 | HCC CCC Metastatic Liver Tumors | HER-2 | Tumor-related Protein Coding | Antibody Drug Conjugate (ADC) | A166, an Antibody Drug Conjugate (ADC) targeting HER2 expressing cancer cells. | Intravenous infusion | 1/2 | Recruiting No results available Estimated Completion Date: May, 2021 | |
| 21 | NCT02416466 | Metastatic Liver Tumors | CEA | Tumor-related Protein Coding | CAR-T cells | anti-CEA CAR-T cells | Hepatic arterial infusion | 1 | Completed No results reported to date | |
| 22 | NCT02869217 | NY-ESO-1 Expressing Liver Cancers in HLA-A2 Positive Patients Metastatic Liver Tumors | NY-ESO-1 | Tumor-related Protein Coding | NY-ESO-1 Specific TCR Gene Transduced Autologous T Lymphocytes | TBI-1301 (NY-ESO-1 Specific TCR Gene Transduced Autologous T Lymphocytes) Cyclophosphamide | Infusion | 1 | Recruiting No results available Estimated Completion Date: June, 2020 | |
| 23 | NCT01061840 | Primary Liver Cancers Metastatic Liver Tumors | rhGMCSF and bi-shRNAfurin from the Vigil™ plasmid | Tumor-related Protein Coding | plasmid | Vaccination | Intradermal injection | 1 | Completed Results partly reported | [ |
| 24 | NCT01437007 | Metastatic Liver Tumors from Colorectal, Pancreas, Gastric, Breast, and Ovarian Cancers | siRNA Against the PLK1 | Oncogene suppression | Lipid Nanoparticles | TKM-080301 | Hepatic arterial infusion | 1 | Completed Results partly reported | [ |
| 25 | NCT03971747 | HCC | AFP | Tumor-related Protein Coding | T Cell | AFP Specific T Cell Receptor T Cells | Intravenous infusion | 1 | Not yet recruiting | |
| 26 | NCT02418988 | HCC | p53 | Tumor suppressor | Recombinant adenoviral vector | TACE plus rAd-p53 artery injection TACE | Injected into the embolization artery. | 2 | Recruiting No results available | |
| 27 | NCT02850536 | Metastatic Liver Tumors from Colorectal, Pancreas, Gastric, Breast, and Ovarian Cancers | CEA | Tumor-related Protein Coding | CAR-T cells | anti-CEA CAR-T cells | Hepatic arterial infusion or splenic vein | 1 | Active, not recruiting Estimated Completion Date: Dec, 2019 | |
| 28 | NCT01373047 | Metastatic Liver Tumors from Colorectal, Pancreas, Gastric, Breast, and Ovarian Cancers | CEA | Tumor-related Protein Coding | T cell | anti-CEA 2nd generation designer T cells | Hepatic arterial infusion or splenic vein | 1 | Completed No results reported to date | |
| 29 | NCT02432963 | Adult Solid Neoplasm | p53 | Tumor suppressor | Modified vaccinia virus | Vaccination | 1 | Active, not recruiting Estimated Completion Date: Feb, 2020 | ||
| 30 | NCT02715362 | HCC | GPC3 | Tumor-related Protein Coding | CAR-T cells | TAI-GPC3-CART cells | Hepatic arterial infusion | 1/2 | Recruiting No results available | |
| 31 | NCT00301106 | Metastatic Liver Tumors from Colorectal, Pancreas, Gastric, Breast, and Ovarian Cancers | Interleukin-12 | Genetic Immunotherapy | Adenoviral Vector | adenovirus-mediated human interleukin-12 | Intratumoral Injection | 1 | Terminated No results available | |
| 32 | NCT00072098 | Metastatic Liver Tumors from Colorectal, Pancreas, Gastric, Breast, and Ovarian Cancers | Interleukin-12 | Genetic Immunotherapy | Adenoviral Vector | adenoviral vector-delivered interleukin-12 | Intratumoral Injection | 1 | Terminated No results available | |
| 33 | NCT03198546 | HCC | GPC3 | Tumor-related Protein Coding | CAR-T cells | GPC3 targeting CAR-T cells | Systemic or local injections | 1 | Recruiting No results available Estimated Completion Date: Aug, 2022 | [ |
| 34 | NCT00103142 | Metastatic Liver Tumors from Colorectal, Pancreas, Gastric, Breast, and Ovarian Cancers | Vaccinia-Carcinoembryonic antigen (CEA)-mucin 1 (MUC-1)- Triad of costimulatory molecules TRICOM vaccine (PANVAC-V) | Tumor-related Protein Coding | Autologous dendritic cells | Vaccination | 2 | Completed Results available | [ |
HCC, hepatocellular carcinoma; CCC, cholangiocellular carcinoma; TACE, transarterial chemoembolization; TAE, transarterial embolization; HSVtk, thymidine kinase of herpes simplex virus; NY-ESO-1, New York esophageal squamous cell carcinoma 1; GPC-3, Glypican-3; LT, liver transplantation.
Summary of ongoing clinical trials for gene-based diagnosis.
| No | NCT Number | Official Title | Brief Summary | Types of Liver Tumors | Phase | Enrollment | Current Status and Results | Ref. |
|---|---|---|---|---|---|---|---|---|
| 1 | NCT00373737 | Microarray Analysis of Gene Expression in Liver Tumors | This study aims to study the gene expression profiles of liver tumors to help us understand their biology, and to find new tumor and treatment markers for liver cancer. | Liver Cancer | Not Applicable | 300 | Completed No results reported to date | |
| 2 | NCT01786980 | The Methylation Phenotype Screening and Determination Mode Study of Liver Cancer Prognosis Related Gene | This study aimed to obtain the important factors affecting liver cancer prognosis, survival, recurrence and metastasis in order to be able to find and establish the effective prognostic evaluation method by analyzing clinical information combining the information of gene chip, methylation chip and flow cytometry to carry out comprehensive researches on liver cancer cell genetics, epigenetics, stem cells and tumor microenvironment changes. | HCC | Not Applicable | 300 | Completed No results reported to date | |
| 3 | NCT00160940 | Differential Gene Expression in Liver Tissue and Blood From Individuals With Chronic Viral Hepatitis With or Without a Complicating Hepatoma or Autoimmune Liver Disease | This study aimed to find the genes that are expressed in both the circulating white blood cells and the liver of patients, using differential gene expression analysis, with varying degrees of liver damage of different causes with or without liver cancers. | Primary Liver Cancers Metastatic Liver Tumors | Not Applicable | 200 | Recruiting No results available | |
| 4 | NCT01643499 | A Genotype-guided Dosing Study of mFOLFIRINOX in Previously Untreated Patients With Advanced Gastrointestinal Malignancies | This study aimed to determine the dose of a chemotherapy drug (irinotecan) in 1st cycle in each of two UGT1A1 genotype groups (*1*1, *1*28) using genotype-guided dosing, that can be tolerated as part of a combination of drugs. | HCC CCC Metastatic Liver Tumors | 1 | 79 | Active, not recruiting Estimated Completion Date: Apr, 2019 | |
| 5 | NCT02465060 | Molecular Analysis for Therapy Choice (MATCH) | This phase II MATCH trial aimed to study how well treatment that is directed by genetic testing works in patients with solid tumors or lymphomas that have progressed following at least one line of standard treatment or for which no agreed upon treatment approach exists. | Primary Liver Cancers Metastatic Liver Tumors | 2 | 6452 | Recruiting No results available Estimated Primary Completion Date: June, 2022 | |
| 6 | NCT02733809 | Mechanism of Sorafenib Resistance in Patients With Advanced Hepatocellular Carcinoma | This study aimed to clarify the hypothesis that resistant tumor may be due to genetic mutations and/or other alternative pathways that could be the reason to overcome the SOR and still proliferate by analyzing the gene expression profiling signature (a set of dysregulated genes) for molecular classification, diagnosis, and prognosis of several types of cancers. | HCC | 4 | 40 | Recruiting No results available Estimated Completion Date: Dec, 2024 | [ |
| 7 | NCT01752920 | A Phase 1/2 Study of ARQ 087 in Adult Subjects With Advanced Solid Tumors With FGFR Genetic Alterations, Including Intrahepatic Cholangiocarcinoma With FGFR2 Gene Fusion | This open-label, Phase 1/2, dose escalation and signal finding study aimed to clarify the effect of Derazantinib (ARQ 087), multi-kinase inhibitor designed to preferentially inhibit the FGFR family of kinases, in the cases with cholangiocarcinoma with FGFR2 gene alterations. | CCC | 1/2 | 119 | Completed Results partly reported | [ |
| 8 | NCT03993873 | A Phase 1, Open-Label, Multi-Center, First-in-Human Study of the Safety, Tolerability, Pharmacokinetics, and Anti-Tumor Activity of TPX-0022, a Novel MET/CSF1R/SRC Inhibitor, in Patients With Advanced Solid Tumors Harboring Genetic Alterations in MET | A phase 1, first-in-human, open-label study to determine the safety, tolerability, PK, and preliminary efficacy of the novel MET/CSF1R/SRC inhibitor TPX-0022 in adult subjects with advanced solid tumors harboring genetic alterations in MET. The study will proceed in three parts: a dose-escalation, a food effect, and dose-expansion. | Advanced Solid Tumor Metastatic Solid Tumors | 1 | 120 | Recruiting No results available Estimated Completion Date: Nov, 2023 | |
| 9 | NCT01892072 | VEGF Signaling Promotes Cell Growth and Metastasis in Hepatocellular Carcinoma in a VEGF Receptor Mediated Pathway | This study aimed to examine the VEGF signaling in HCC cell lines and its mechanism in HCC growth, proliferation and apoptosis. | HCC | Not Applicable | 50 | Active, not recruiting | |
| 10 | NCT02507882 | Impact of IL-28B rs12979860 and rs4803217 Gene Polymorphisms Associated With miRNAs Deregulation on HCV-related Hepatocellular Carcinoma | This study aimed to determine through investigating a cohort of 405 patients, whether IL28B rs12979860 and rs4803217 polymorphisms are associated to the risk of HCC in chronic hepatitis C patients. | HCC | Not Applicable | 405 | Not yet recruiting | |
| 11 | NCT00858000 | Analysis of the Incidence of Expression of a Specific Set of Genes and of Tumor Antigens in Cancer Tissue From Patients With Hepatocellular Carcinoma | This study aimed to analyze the expression of specific markers in HCC and tumor-related antigens to develop new approaches to treat this type of cancer with genetic immunotherapy. | HCC | Not Applicable | 30 | Completed No results reported to date | |
| 12 | NCT03722628 | The Assessment of Matrix Metalloproteinase-1 Genotypes Polymorphism as a Risk Factor for Hepatocellular Carcinoma in Chronic Hepatitis C Patients With Liver Cirrhosis | This study aimed to assess whether the Matrix Metalloproteinase-1 genotypes polymorphism can be a risk factor for HCC in chronic hepatitis C patients with liver cirrhosis. | HCC | Not Applicable | 200 | Not yet recruiting | [ |
| 13 | NCT01930383 | Circulating Tumor Cells as Biomarkers of Prognosis and Predictors of Efficacy of Drug Therapy for Patients With Hepatocellular Carcinoma | This study aimed to explore the clinical value of correlation between circulating tumor cells numbers and other clinical characteristics in HCC patients with different stages. | HCC | Not Applicable | 150 | Recruiting No results available | |
| 14 | NCT00619541 | Phase II Study of Sorafenib (Bay 43-9006) and Infusional 5-Fluorouracil in Advanced Hepatocellular Carcinoma. | The purpose of this study is to use SOR + 5-FU to evaluate activity, efficacy, safety, pharmacodynamics and pharmacokinetics in patients with advanced HCC. | HCC | 2 | 46 | Completed Results partly reported | [ |
HCC, hepatocellular carcinoma; FOLFIRINOX regimen A regimen consisting of leucovorin calcium, fluorouracil, irinotecan hydrochloride, and oxaliplatin; SOR, sorafenib; FGFR, fibroblast growth factor receptor; CCC, cholangiocellular carcinoma.