Synergistic anti-tumor effects between oncolytic vaccinia virus and paclitaxel are mediated by the IFN response and HMGB1

Huang, Baocheng; Sikorski, Rachel; Kirn, David H.; Thorne, Steve H.

doi:10.1038/gt.2010.121

Cited by 59 publications

(46 citation statements)

References 33 publications

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“…113 Recent studies delineated that oncolytic viruses such as vaccinia, measles, HSV-2, and adenovirus cause the release of HMGB1. 64,65,114,115,116,117 Although HMGB1 interacts with viral components and may modulate viral replication, 117 the molecular mechanisms of how each oncolytic virus differentially produces these DAMPs remain largely elusive.…”

Section: Damps Induced By Infection With Oncolytic Virusesmentioning

confidence: 99%

Multimodal immunogenic cancer cell death as a consequence of anticancer cytotoxic treatments

2013

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Apoptotic cell death generally characterized by a morphologically homogenous entity has been considered to be essentially non-immunogenic. However, apoptotic cancer cell death, also known as type 1 programmed cell death (PCD), was recently found to be immunogenic after treatment with several chemotherapeutic agents and oncolytic viruses through the emission of various danger-associated molecular patterns (DAMPs). Extensive studies have revealed that two different types of immunogenic cell death (ICD) inducers, recently classified by their distinct actions in endoplasmic reticulum (ER) stress, can reinitiate immune responses suppressed by the tumor microenvironment. Indeed, recent clinical studies have shown that several immunotherapeutic modalities including therapeutic cancer vaccines and oncolytic viruses, but not conventional chemotherapies, culminate in beneficial outcomes, probably because of their different mechanisms of ICD induction. Furthermore, interests in PCD of cancer cells have shifted from its classical form to novel forms involving autophagic cell death (ACD), programmed necrotic cell death (necroptosis), and pyroptosis, some of which entail immunogenicity after anticancer treatments. In this review, we provide a brief outline of the well-characterized DAMPs such as calreticulin (CRT) exposure, high-mobility group protein B1 (HMGB1), and adenosine triphosphate (ATP) release, which are induced by the morphologically distinct types of cell death. In the latter part, our review focuses on how emerging oncolytic viruses induce different forms of cell death and the combinations of oncolytic virotherapies with further immunomodulation by cyclophosphamide and other immunotherapeutic modalities foster dendritic cell (DC)-mediated induction of antitumor immunity. Accordingly, it is increasingly important to fully understand how and which ICD inducers cause multimodal ICD, which should aid the design of reasonably multifaceted anticancer modalities to maximize ICD-triggered antitumor immunity and eliminate residual or metastasized tumors while sparing autoimmune diseases.

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Section: Damps Induced By Infection With Oncolytic Virusesmentioning

confidence: 99%

Multimodal immunogenic cancer cell death as a consequence of anticancer cytotoxic treatments

2013

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“…HMGB1 can function as a chemoattractant for immune cells, activating them upon binding to TLR2, TLR4, TLR9, and RAGE receptors, thereby initiating an adaptive immune response resulting in engagement of antigen-specific cytotoxic effectors (cytotoxic T lymphocytes [CTLs]) (67,72,82,83). Antitumor protection induced by oncolytic viruses also appears to rely on the release of HMGB1 (41,43). This is particularly the case for viruses enforced with immunostimulatory elements, as demonstrated by the ability of glycyrrhizin to completely block tumor regression induced by ganciclovir and adenoviral vectors encoding herpes simplex virus 1-thymidine kinase and cytokine Flt3L (Ad-TKϩGCV and Ad-Flt3L) in a glioblastoma model (84).…”

Section: Discussionmentioning

confidence: 99%

“…The release of ICD determinants upon infections in general, and by tumor cells infected with oncolytic viruses in particular, has started to draw attention (37)(38)(39)(40)(41)(42)(43). We hypothesized that triggering the adaptive anticancer activity by H-1PV-alone or in combination with gemcitabine-could be initiated by ICD determinants released from dying tumor cells.…”

mentioning

confidence: 99%

Complementary Induction of Immunogenic Cell Death by Oncolytic Parvovirus H-1PV and Gemcitabine in Pancreatic Cancer

Angelova

Grekova

Heller

et al. 2014

J Virol

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Pancreatic ductal adenocarcinoma (PDAC) is an extremely aggressive disease, with a median survival time of less than 9 months and a 5-year survival rate of Ͻ1%. Current advances in surgical, (neo)adjuvant, and palliative treatments have failed to prevent recurrence and ultimate metastasis (1-3).In order to be effective, chemotherapy must reduce the tumor burden, promote anticancer immunity, and alleviate intratumoral immunosuppression (4-6). Forced tumor cell death in an immunogenic manner (i.e., immunogenic cell death [ICD]) has been proposed as the best way to trigger an adaptive immune response, boosting the therapeutic efficacy of a cytoreductive treatment (7,8). Preapoptotic surface exposure of calreticulin (CRT) (as a result of the endoplasmic reticulum stress response), as well as release of ATP (autophagy) and high-mobility group box B1 protein (HMGB1) (late apoptosis/necrosis), is considered the optimal ICD combination for dying tumor cells to enable paracrine activation of dendritic cells and the consequent priming of cytotoxic effectors. The surface exposure of CRT promotes uptake of dying tumor cells by dendritic cells, and the release of HMGB1 engages

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“…VV kills cancer cells via a combination of necrosis and immunogenic apoptosis resulting in the release of damage associated molecular patterns [75][76][77][78] and pathogen associated molecular patterns [79][80][81] as well as the release of viral antigens into the tumor. This process leads to a strong inflammatory response that can overcome the immune suppression within the tumor microenvironment.…”

Section: Vaccinia Virus As Immunomodulatory Agentmentioning

confidence: 99%

Vaccinia Virus, a Promising New Therapeutic Agent for Pancreatic Cancer

et al. 2015

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The poor prognosis of pancreatic cancer patients signifies a need for radically new therapeutic strategies. Tumor-targeted oncolytic viruses have emerged as attractive therapeutic candidates for cancer treatment due to their inherent ability to specifically target and lyse tumor cells as well as induce antitumor effects by multiple action mechanisms. Vaccinia virus has several inherent features that make it particularly suitable for use as an oncolytic agent. In this review, we will discuss the potential of vaccinia virus in the management of pancreatic cancer in light of our increased understanding of cellular and immunological mechanisms involved in the disease process as well as our extending knowledge in the biology of vaccinia virus.

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Synergistic anti-tumor effects between oncolytic vaccinia virus and paclitaxel are mediated by the IFN response and HMGB1

Cited by 59 publications

References 33 publications

Multimodal immunogenic cancer cell death as a consequence of anticancer cytotoxic treatments

Multimodal immunogenic cancer cell death as a consequence of anticancer cytotoxic treatments

Complementary Induction of Immunogenic Cell Death by Oncolytic Parvovirus H-1PV and Gemcitabine in Pancreatic Cancer

Vaccinia Virus, a Promising New Therapeutic Agent for Pancreatic Cancer

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