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©The Author(s) 2020.
World J Clin Oncol. Aug 24, 2020; 11(8): 589-605
Published online Aug 24, 2020. doi: 10.5306/wjco.v11.i8.589
Published online Aug 24, 2020. doi: 10.5306/wjco.v11.i8.589
Table 1 Summary of current molecular targeted compounds under phase II/III clinical studies for the treatment of hepatocellular carcinoma
| Drug | Targets | Descriptions | Ref./ClinicalTrials.gov identifier |
| Phase II | |||
| Bevacizumab | VEGF | Monoclonal antibody | [116-118] |
| Inhibits tumour growth of HCC cell line or patient-derived HCC xenografts | |||
| Shows significant antitumour activity in patients with non-metastatic HCC, but serious bleeding complications occurs in 11% of patients. | |||
| Cediranib | VEGFR | Tyrosine kinase inhibitor | [119] |
| Shows high toxicity and ineffective for patients with unresectable or metastatic HCC | |||
| Cetuximab | EGFR | Human-mouse chimeric monoclonal antibody | [120] |
| Shows no obvious response in patients with advanced HCC | |||
| Dovitinib | c-KIT, Flt-3, FGFR, VEGFR | Multikinase inhibitor | [38,121] |
| Significantly prolongs survival and inhibits primary tumour growth and lung metastasis in HCC xenograft models | |||
| Shows less antitumour activity than sorafenib as a frontline systemic therapy for HCC | |||
| Erlotinib | EGFR | Tyrosine kinase inhibitor | [122,123] |
| Shows modest prolonged progression-free survival and overall survival in patients with unresectable HCC | |||
| Gefitinib | EGFR | Tyrosine kinase inhibitor | NCT00071994, [124] |
| Inhibits tumour growth of HCC xenografts in mouse model | |||
| Selumetinib | MEK1 | Tyrosine kinase inhibitor | [125,126] |
| Suppresses tumour growth of HCC xenografts in mouse model | |||
| Shows inadequate antitumour activity with no radiographic response and short progression-free survival in patients with locally advanced or metastatic HCC | |||
| Phase III | |||
| Brivanib | FGFR, VEGFR | Tyrosine kinase inhibitor | [127-129] |
| Inhibits tumour growth of patient-derived HCC xenografts by increasing apoptosis, reducing microvessel density and decreasing VEGFR phosphorylation | |||
| Shows promising antitumour activity in patients with advanced HCC | |||
| Linifanib | PDGFR, VEGFR | Receptor tyrosine kinase inhibitor | [39,130,131] |
| Inhibits tumour growth of HCC xenografts in mouse model | |||
| Shows similar overall survival in patients with advanced HCC as compared with sorafenib | |||
| Sunitinib | c-Kit, Flt-3, PDGFP, VEGFR | Multi-targeted receptor tyrosine kinase inhibitor | [132-134] |
| Inhibits tumour growth of patient-derived HCC xenografts by increasing apoptosis and reducing microvessel density | |||
| Shows significantly poorer overall survival than sorafenib in patients with advanced HCC, and shows more frequent and severe toxicity in treated patients | |||
| TSU-68 (Orantinib) | FGFR, PDGFR, VEGFR | Tyrosine kinase inhibitor | [135-137] |
| Suppresses the tumour growth of subcutaneously co-injected HCC cell lines (Huh7/WI-38) xenografts | |||
| Orantinib combined with TACE shows no improvement in overall survival in patients with unresectable HCC |
Table 2 Summary of potential pipeline compounds targeting novel molecular targets in several cancers
| Drug | Descriptions | Phase | Type of tumour | Ref./ClinicalTrials.gov identifier |
| Hh signaling pathway | ||||
| Erismodegib, (LDE-225) | Smo antagonist | 0 | Pancreatic cancer | NCT01694589 |
| In vitro and in vivo test results on HCC cells are not available | I | Advanced solid tumours | NCT00880308 | |
| I | SCLC | NCT01579929 | ||
| II | Advanced or metastatic basal cell carcinoma | NCT01327053 | ||
| I/II | Medulloblastoma | NCT01125800 | ||
| Vismodegib | Smo antagonist | I | HCC and lymphoma | NCT01546519 |
| Promotes regression of liver fibrosis and HCC tumour growth in a murine model of primary liver cancer[138] | I | Advanced or metastatic basal cell carcinoma | ||
| II | Ovarian cancer | NCT00739661 | ||
| Shows no obvious response in patients with hepatic impairment[139] | ||||
| Notch signaling pathway | ||||
| MK-0752 | γ-secretase inhibitor | I | Advanced solid tumour | [63] |
| In vitro and in vivo test results on HCC cells are not available | I | Brain and central nervous system tumours | [64] | |
| RO4929097 | γ-secretase inhibitor | I | Refractory metastatic or locally advanced solid tumours | [65] |
| Prevents tumour development and decreases liver fibrosis in mouse model[141] | ||||
| II | Metastatic colorectal cancer | [66] | ||
| Plk1 | ||||
| HMN-214 | Stilbene derivative interferes with the subcellular spatial distribution of Plk1 at centrosomes | I | Advanced solid tumours | [79] |
| In vitro and in vivo test results on HCC cells are not available | ||||
| GSK461364 | Reversible ATP-competitive Plk1 inhibitor | I | Advanced solid tumours and non-Hodgkin’s lymphoma | [81] |
| In vitro and in vivo test results on HCC cells are not available | ||||
| Arginine deprivation | ||||
| ADI-PEG-20 | Arginine deiminase | I | Pediatric ASS-deficient tumour | NCT01528384 |
| Shows its safe and efficacious in stabilizing the progression of advanced HCC in an Asian population | ||||
| II | SCLC | [142], NCT01266018 | ||
| II | Advanced melanoma | [143] | ||
| Shows no overall survival benefit in second line setting for patients with advanced HCC | ||||
| II | Malignant pleural mesothelioma | NCT01279967 | ||
| II/III | Advanced HCC | [87,144] | ||
| BCT100/ Peg-rhArg1 | Recombinant human arginase I | I | Leukemia and lymphoma | NCT01551628 |
| Inhibits tumour growth of HCC xenografts in mouse model[85] | ||||
| I/II | Advanced HCC | [90], NCT01092091 | ||
| HDACs | ||||
| Resminostat | HDACs (1, 3 & 6) inhibitor[145] | I/II | Advanced HCC | [146] |
| Combined with sorafenib shows no significant efficacy advantage over sorafenib monotherapy in patients with advanced HCC in East Asian populations | II | Hodgkin's lymphoma | NCT01037478 | |
| I/II | Advanced colorectal carcinoma | NCT01277406 | ||
| Chidamide | HDACs inhibitor (1, 2, 3 & 10)[147] | I | Advanced solid tumours and lymphomas | [148] |
| Inhibits proliferation of HCC cells in vitro[95] | ||||
| Panobinostat,(LBH-589) | Pan-HDAC inhibitor Inhibits tumour growth and lung metastasis of HCC xenografts in mouse model[149] | I | Prostate carcinoma | [150] |
| I | Advanced solid tumours | [151] | ||
| II | Refractory metastatic renal cell carcinoma | [152] | ||
| Glypican-3 | ||||
| Codrituzumab (GC33) | Anti-GPC3 monoclonal antibody | I | Advanced or metastatic HCC | [153] |
| Inhibits tumour growth of HCC xenografts in mouse model[102] | ||||
| Shows no clinical benefit in advanced HCC patients who has failed prior systemic therapy | ||||
Table 3 Clinical study of combined molecular targeted therapy based on sorafenib treatment for hepatocellular carcinoma
| Drug + Sorafenib | Phase | Ref./ClinicalTrials.gov identifier |
| VEGF inhibitors | ||
| Bevacizumab | I/II | NCT00867321 |
| Lenvatinib | I/II (HCC) | NCT01271504 |
| mTOR inhibitor | ||
| Everolimus (RAD001) | II | NCT01005199 |
| I/II | [154] | |
| Temsirolimus | I/II | NCT01335074, NCT01687673, NCT01008917 |
| HDAC inhibitors | ||
| Resminostat | II (Advanced HCC) | NCT00943449 |
| Panobinostat | I (HCC) | NCT00823290 |
| Anti-GPC3 antibody | ||
| GC33 | I | NCT00976170 |
| MEK1 inhibitor | ||
| Selumetinib (AZD6244) | I/II | NCT01029418 |
| HGFR inhibitor | ||
| Tivantinib (ARQ197) | I | NCT00827177 |
| TNF-α secretion inhibitor | ||
| Lenalidomide | I | NCT01348503 |
| TRAIL receptor 1 antibody | ||
| Mapatumumab | I/II | NCT00712855, NCT01258608 |
- Citation: Chow AKM, Yau SWL, Ng L. Novel molecular targets in hepatocellular carcinoma. World J Clin Oncol 2020; 11(8): 589-605
- URL: https://www.wjgnet.com/2218-4333/full/v11/i8/589.htm
- DOI: https://dx.doi.org/10.5306/wjco.v11.i8.589