Enhanced antitumor efficacy of a novel oncolytic vaccinia virus encoding a fully monoclonal antibody against T-cell immunoglobulin and ITIM domain (TIGIT)

Zuo, Shuguang; Wei, Min; He, Bohao; Chen, Anxian; Wang, Shiqun; Kong, Long; Zhang, Yenan; Ma, Gang; Xu, Tiancheng; Wu, Jingyi; Yang, Fengxia; Zhang, Hailin; Wang, Shibing; Guo, Ciliang; Wu, Junhua; Dong, Jie; Wei, Jiwu

doi:10.1016/j.ebiom.2021.103240

Cited by 26 publications

(21 citation statements)

References 33 publications

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“… 106 Furthermore, OVs encoding an anti-murine PD-1, CTLA-4 or TIGIT antibody enabled tumor growth inhibition and survival superior to parental virus and for the PD-1 virus similar to combined parental virus with repeated high dose systemic mAb. 103 , 105 , 117 Similar results were obtained for an oncolytic HSV-2 encoding an anti-human PD-1 antibody in a mouse model with humanized PD-1. 92 …”

Section: Therapeutic Antibody-encoding Ovs: Antibody Formats Targets and Therapeutic Strategiessupporting

confidence: 69%

“…These studies included a model antibody to demonstrate proof-of-principle, 117 an experimental therapeutic antibody targeting the tumor vascular antigen fibronectin extradomain B, 121 IgGs with specificity for tumor targets (CD147), 122 or targets of approved mAbs (CTLA-4, PD-1, VEGF), 92 , 103 , 106 , 111 and the approved antibody trastuzumab. 108 Overall, the reports established that the genetic delivery of full-length IgGs is feasible for both RNA viruses, as reported for NDV 121 , 122 and influenza A, 117 and for DNA viruses, reported for Ad, 106–108 , 111 VV, 103 , 105 and HSV. 92 Strategies for the required co-expression of IgG heavy and light chains were the insertion of two separate transcription units for NDV and VV, fusion to two viral ORFs of different gene segments using viral 2A sequences for influenza A virus or co-expression via an IRES or a 2A sequence for Ads.…”

Section: Therapeutic Antibody-encoding Ovs: Antibody Formats Targets and Therapeutic Strategiesmentioning

confidence: 52%

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Viro-antibody therapy: engineering oncolytic viruses for genetic delivery of diverse antibody-based biotherapeutics

Kontermann

Ungerechts

Nettelbeck

2021

mAbs

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Section: Therapeutic Antibody-encoding Ovs: Antibody Formats Targets and Therapeutic Strategiessupporting

confidence: 69%

Section: Therapeutic Antibody-encoding Ovs: Antibody Formats Targets and Therapeutic Strategiesmentioning

confidence: 52%

Viro-antibody therapy: engineering oncolytic viruses for genetic delivery of diverse antibody-based biotherapeutics

Kontermann

Ungerechts

Nettelbeck

2021

mAbs

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“…Treatment stimulated a CD8 T cell-mediated anti-tumour response with evidence of immune memory and protection from re-challenge. High levels of anti-TIGIT mAb were seen in tumour tissue, but not in blood from treated mice ( 66 ). A TK-gene deleted oVV expressing anti-PD-1 and an anti-4-1BB co-stimulatory receptor agonist was also shown to suppress tumour growth in mouse models of liver and pancreatic cancer ( 67 ).…”

Section: Oncolytic Virotherapymentioning

confidence: 99%

Kickstarting Immunity in Cold Tumours: Localised Tumour Therapy Combinations With Immune Checkpoint Blockade

et al. 2021

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Cancer patients with low or absent pre-existing anti-tumour immunity (“cold” tumours) respond poorly to treatment with immune checkpoint inhibitors (ICPI). In order to render these patients susceptible to ICPI, initiation of de novo tumour-targeted immune responses is required. This involves triggering of inflammatory signalling, innate immune activation including recruitment and stimulation of dendritic cells (DCs), and ultimately priming of tumour-specific T cells. The ability of tumour localised therapies to trigger these pathways and act as in situ tumour vaccines is being increasingly explored, with the aspiration of developing combination strategies with ICPI that could generate long-lasting responses. In this effort, it is crucial to consider how therapy-induced changes in the tumour microenvironment (TME) act both as immune stimulants but also, in some cases, exacerbate immune resistance mechanisms. Increasingly refined immune monitoring in pre-clinical studies and analysis of on-treatment biopsies from clinical trials have provided insight into therapy-induced biomarkers of response, as well as actionable targets for optimal synergy between localised therapies and ICB. Here, we review studies on the immunomodulatory effects of novel and experimental localised therapies, as well as the re-evaluation of established therapies, such as radiotherapy, as immune adjuvants with a focus on ICPI combinations.

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“…Arming HSV with secreted chimeric molecules to induce innate immune cell killing of infected tumours has also been explored [ 79 ]. In contrast, as NK cells were shown to augment oncolytic vaccinia virus activities [ 4 ], engineering expression of a monoclonal antibody against TIGIT was able to enhance preclinical effectiveness [ 80 ]. Similarly, an adenovirus expressing fusion protein PD-1/CD137L demonstrated anti-tumoural response in murine hepatocellular carcinoma [ 81 ].…”

Section: Strategies That Exploit Nk Cell Response To Improve Ov Efficaciesmentioning

confidence: 99%

Strategies to Optimise Oncolytic Viral Therapies: The Role of Natural Killer Cells

Leung

McNeish

2021

Viruses

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Oncolytic viruses (OVs) are an emerging class of anti-cancer agents that replicate selectively within malignant cells and generate potent immune responses. Their potential efficacy has been shown in clinical trials, with talimogene laherparepvec (T-VEC or IMLYGIC®) now approved both in the United States and Europe. In healthy individuals, NK cells provide effective surveillance against cancer and viral infections. In oncolytic viral therapy, NK cells may render OV ineffective by rapid elimination of the propagating virus but could also improve therapeutic efficacy by preferential killing of OV-infected malignant cells. Existing evidence suggests that the overall effect of NK cells against OV is context dependent. In the past decade, the understanding of cancer and OV biology has improved significantly, which helped refine this class of treatments in early-phase clinical trials. In this review, we summarised different strategies that have been evaluated to modulate NK activities for improving OV therapeutic benefits. Further development of OVs will require a systematic approach to overcome the challenges of the production and delivery of complex gene and cell-based therapies in clinical settings.

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Enhanced antitumor efficacy of a novel oncolytic vaccinia virus encoding a fully monoclonal antibody against T-cell immunoglobulin and ITIM domain (TIGIT)

Cited by 26 publications

References 33 publications

Viro-antibody therapy: engineering oncolytic viruses for genetic delivery of diverse antibody-based biotherapeutics

Viro-antibody therapy: engineering oncolytic viruses for genetic delivery of diverse antibody-based biotherapeutics

Kickstarting Immunity in Cold Tumours: Localised Tumour Therapy Combinations With Immune Checkpoint Blockade

Strategies to Optimise Oncolytic Viral Therapies: The Role of Natural Killer Cells

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