Suppression of <scp>T</scp>regs by anti‐glucocorticoid induced <scp>TNF</scp> receptor antibody enhances the antitumor immunity of interferon‐α gene therapy for pancreatic cancer

Aida, Kouichirou; Miyakawa, Reina; Suzuki, Kôji; Narumi, Kenta; Udagawa, Tsuyoshi; Yamamoto, Yoshiya; Chikaraishi, Tatsuya; Yoshida, Teruhiko; Aoki, Kazunori

doi:10.1111/cas.12332

Cited by 47 publications

(23 citation statements)

References 29 publications

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“…[139,140] Recently, antiglucocorticoid-induced TNF receptor monoclonal antibody has been introduced to suppress Tregs. Aida et al [47] showed this monoclonal antibody-induced suppression of Tregs infiltration in PC with down regulation of CCR5 and led to enhancement antitumor immunity of IFN-α gene therapy.…”

Section: Adaptive Immune Cells In Pcmentioning

confidence: 99%

Role of immune cells in pancreatic cancer from bench to clinical application

2016

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Background:Pancreatic cancer (PC) remains difficult to treat, despite the recent advances in various anticancer therapies. Immuno-inflammatory response is considered to be a major risk factor for the development of PC in addition to a combination of genetic background and environmental factors. Although patients with PC exhibit evidence of systemic immune dysfunction, the PC microenvironment is replete with immune cells.Methods:We searched PubMed for all relevant English language articles published up to March 2016. They included clinical trials, experimental studies, observational studies, and reviews. Trials enrolled at Clinical trial.gov were also searched.Results:PC induces an immunosuppressive microenvironment, and intratumoral activation of immunity in PC is attenuated by inhibitory signals that limit immune effector function. Multiple types of immune responses can promote an immunosuppressive microenvironment; key regulators of the host tumor immune response are dendritic cells, natural killer cells, macrophages, myeloid derived suppressor cells, and T cells. The function of these immune cells in PC is also influenced by chemotherapeutic agents and the components in tumor microenvironment such as pancreatic stellate cells. Immunotherapy of PC employs monoclonal antibodies/effector cells generated in vitro or vaccination to stimulate antitumor response. Immune therapy in PC has failed to improve overall survival; however, combination therapies comprising immune checkpoint inhibitors and vaccines have been attempted to increase the response.Conclusion:A number of studies have begun to elucidate the roles of immune cell subtypes and their capacity to function or dysfunction in the tumor microenvironment of PC. It will not be long before immune therapy for PC becomes a clinical reality.

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Section: Adaptive Immune Cells In Pcmentioning

confidence: 99%

Role of immune cells in pancreatic cancer from bench to clinical application

2016

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“…Importantly, the success of therapy was seen in several tumor models, independently of tumor cell line sensitivity to NDV-mediated lysis, highlighting the importance of the virus-induced antitumor immunity rather than direct oncolysis in the observed therapeutic efficacy . A similar study using systemic agonistic anti-GITR antibody together with intratumoral administration of adenovirus expressing IFNα also resulted in synergistic inhibition of the virus-injected and distant tumors (Aida et al, 2014). Taken together, these studies thus provide a strong rationale for further evaluation of oncolytic viruses as potentiators of immunotherapy with agents targeting immune costimulatory or coinhibitory receptors.…”

Section: Oncolytic Virusesmentioning

confidence: 71%

The New Era of Cancer Immunotherapy

Khalil¹,

Budhu²,

Gasmi³

et al. 2015

Advances in Cancer Research

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“…Kavanagh et al observed that CTLA-4 blockade expanded Treg at low doses, but expanded effector T cells only at high doses [116]. Some studies have reported that anti-CTLA-4 or anti-GITR made effector T cells resistant to the inhibitory effect of Treg [44,117,118]. …”

Section: Mechanisms Mediating the Efficacy Of Cancer Vaccines Combmentioning

confidence: 99%

Is There Still Room for Cancer Vaccines at the Era of Checkpoint Inhibitors

et al. 2016

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Checkpoint inhibitor (CPI) blockade is considered to be a revolution in cancer therapy, although most patients (70%–80%) remain resistant to this therapy. It has been hypothesized that only tumors with high mutation rates generate a natural antitumor T cell response, which could be revigorated by this therapy. In patients with no pre-existing antitumor T cells, a vaccine-induced T cell response is a rational option to counteract clinical resistance. This hypothesis has been validated in preclinical models using various cancer vaccines combined with inhibitory pathway blockade (PD-1-PDL1-2, CTLA-4-CD80-CD86). Enhanced T cell infiltration of various tumors has been demonstrated following this combination therapy. The timing of this combination appears to be critical to the success of this therapy and multiple combinations of immunomodulating antibodies (CPI antagonists or costimulatory pathway agonists) have reinforced the synergy with cancer vaccines. Only limited results are available in humans and this combined approach has yet to be validated. Comprehensive monitoring of the regulation of CPI and costimulatory molecules after administration of immunomodulatory antibodies (anti-PD1/PD-L1, anti-CTLA-4, anti-OX40, etc.) and cancer vaccines should help to guide the selection of the best combination and timing of this therapy.

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Suppression of Tregs by anti‐glucocorticoid induced TNF receptor antibody enhances the antitumor immunity of interferon‐α gene therapy for pancreatic cancer

Cited by 47 publications

References 29 publications

Role of immune cells in pancreatic cancer from bench to clinical application

Role of immune cells in pancreatic cancer from bench to clinical application

The New Era of Cancer Immunotherapy

Is There Still Room for Cancer Vaccines at the Era of Checkpoint Inhibitors

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