Adoptive Transfer of Tumor-Reactive Transforming Growth Factor-β–Insensitive CD8+ T Cells: Eradication of Autologous Mouse Prostate Cancer

Zhang, Qiang; Yang, Ximing J.; Pins, Michael; Javonovic, Borko; Kuzel, Timothy M.; Kim, Seong‐Jin; Parijs, Luk Van; Greenberg, Norman M.; Liu, Victoria; Guo, Yinglu; Lee, Chung

doi:10.1158/0008-5472.can-04-3169

Cited by 138 publications

(100 citation statements)

References 30 publications

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“…Reasons for the lack of in vitro CTL activity are unclear but could include: (a) no TRAMP-C2 -specific CTLs were generated in this model system. A recent study reported that TRAMP-C2 cells secrete large amounts of the potent immunosuppressant transforming growth factor-h, which could prevent CD8 + cells from infiltrating into metastatic lung tumors (36). Based on this report, we did in vitro stimulation of splenocytes with TRAMP-C2 cells in the presence of antitransforming growth factor-h antibodies; however, the CTL assay was again unsuccessful.…”

Section: Discussionmentioning

confidence: 99%

Systemic Oncolytic Herpes Virus Therapy of Poorly Immunogenic Prostate Cancer Metastatic to Lung

Varghese

Rabkin

Nielsen

et al. 2006

Clinical Cancer Research

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Purpose: Our goal was to evaluate whether systemic administration of NV1042, an interleukin-12 (IL-12)^expressing oncolytic herpes simplex virus, and its noncytokine parental vector NV1023 are effective against preexisting metastatic prostate cancer in an immunocompetent mice model. Experimental Design: MetastaticTRAMP-C2 lung tumors established in C57Bl/6 or nude mice were treated on day 21with four i.v. administrations of NV1042 or NV1023 and sacrificed on day 42 to assess virus efficacy and the potential mechanism of efficacy. Results: NV1042 or NV1023 treatment was similarly effective in eliminating extrapleural and hemorrhagic tumors present in mock-treated mice. However, NV1042 was further effective compared with NV1023 in controlling the growth of lung tumors (as determined by mean surface tumor nodule number, lung weights, and surface tumor burden) and in extending survival. NV1042-treated mice exhibited a transient increase of serum IL-12 1 day posttreatment, whereas IL-12 levels in tumor bearing lungs persisted a further 2 days at least. Only splenocytes from NV1042-treated mice secreted IFN-g in response to TRAMP-C2 stimulation and displayed natural killer activity. The IL-12-mediated enhancement observed with NV1042 in the syngeneic model was abrogated in athymic mice treated in a similar manner, thus indicating a role forTcells in the augmented efficacy of NV1042 virus. Conclusions: Systemic administration of the IL-12-expressing NV1042 virus is more effective than its noncytokine parent, NV1023, against preestablished metastatic lung tumors. Given the clinical safety profile of NV1020, the parental vector of NV1023, and NV1042's enhanced efficacy and ability to activate the host immune system, NV1042 merits clinical consideration for treating metastatic prostate cancers.Prostate cancer is the most commonly diagnosed cancer in men in the United States, accounting for 33% of all cancers and claiming the life of one in eight men with this diagnosis (1). Early diagnosis facilitated by screening high-risk populations using prostate-specific antigen and imaging techniques have aided in lowering the mortality rates of patients with localized, early-stage cancer. However, about one third will bear regional or metastatic tumors at the time of diagnosis with another 25% progressively developing metastatic disease during the course of the disease (2). Bone is the primary site of metastasis in 85% of cases followed by lymph nodes, lung, liver, and adrenals, in f45% of cases.Currently, there are no curative treatment options available for patients with advanced prostate cancer. Although organconfined cancer responds well to surgery and radiation therapy, with 5-year survival rates for such patients being 89%, the survival rates for patients with metastatic cancer decreases to 31% (2). Hormonal therapy (androgen ablation) has been the primary treatment of choice since the 1960s for patients with advanced disease. Unfortunately, the effectiveness of hormonal therapy is limited by the inevitable developme...

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Section: Discussionmentioning

confidence: 99%

Systemic Oncolytic Herpes Virus Therapy of Poorly Immunogenic Prostate Cancer Metastatic to Lung

Varghese

Rabkin

Nielsen

et al. 2006

Clinical Cancer Research

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“…Indeed, tumors have been shown to escape the anti-tumor immune responses by generating an immunosuppressed tumor microenvironment. Tumors often produce soluble immunosuppressive factors, such as TGFβ [13,68,69], VEGF [69,70], IL-10 [69,71], iNOS [72,73], PGE 2 [74,75], and gangliosides [76,77], that act on neutrophils and other tumor infiltrating immune cells. Often, progressive immunosuppression is observed at advanced tumor stages, which is partially mediated by tumor-infiltrating immunosuppressive immune cells such as regulatory T (Treg) cells, Th17 cells, regulatory dendritic cells, TAMs, TANs and MDSCs.…”

Section: Immunosuppression In the Tumor Microenvironmentmentioning

confidence: 99%

“…These ex vivo expanded TGFβ-insensitive CD8 + T cells infiltrated the tumor and mediated apoptosis in tumor cells [68]. Fridlender et al [13] showed that inhibition of TGFβ signaling using the small molecule inhibitor SM16 conferred anti-tumorigenic activity to neutrophils.…”

Section: Tgfβmentioning

confidence: 99%

The Multifaceted Roles Neutrophils Play in the Tumor Microenvironment

Sionov

Fridlender

Granot

2014

Cancer Microenvironment

342

261

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Neutrophils are myeloid cells that constitute 50-70 % of all white blood cells in the human circulation. Traditionally, neutrophils are viewed as the first line of defense against infections and as a major component of the inflammatory process. In addition, accumulating evidence suggest that neutrophils may also play a key role in multiple aspects of cancer biology. The possible involvement of neutrophils in cancer prevention and promotion was already suggested more than half a century ago, however, despite being the major component of the immune system, their contribution has often been overshadowed by other immune components such as lymphocytes and macrophages. Neutrophils seem to have conflicting functions in cancer and can be classified into anti-tumor (N1) and pro-tumor (N2) sub-populations. The aim of this review is to discuss the varying nature of neutrophil function in the cancer microenvironment with a specific emphasis on the mechanisms that regulate neutrophil mobilization, recruitment and activation.

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“…While active TGF-β does not inhibit lysis by CTLs, it can inhibit maturation of T cells to that effector state [79]. This explains, at least in part, how CD8 + T cells resistant to TGF-β1 can mediate tumor rejection [80].…”

Section: The Immunosuppressive Environment Inside Tumorsmentioning

confidence: 99%

Targeting tumors with LIGHT to generate metastasis-clearing immunity

Yü¹,

Fu²

2008

Cytokine & Growth Factor Reviews

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Metastastic diseases cause the majority of morbidity and mortality of cancer patients. Established tumors form both physical and immunological barriers to limit immune detection and destruction. Current immunotherapy of vaccination and adoptive transfer shows limited effect at least in part due to the existing barriers in the tumors and depending on the knowledge of tumor antigens. Tumor necrosis factor superfamily member 14 (TNFSF14) LIGHT interacts with stromal cells, dendritic cells, NK cells, naïve and activated T cells and tumor cells inside the tumor tissues via its two functional receptors, HVEM and lymphotoxin β receptor (LTβR). Targeting tumor tissues with LIGHT leads to augmentation of priming, recruitment, and retention of effector cells at tumor sites, directly or indirectly, to induce strong anti-tumor immunity to inhibit the growth of primary tumors as well as eradicate metastases. Intratumor treatment would break tumor barriers and allow strong immunity against various tumors without defining tumor antigens. This review summarizes recent findings to support that LIGHT is a promising candidate for an effective cancer immunotherapy.

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Adoptive Transfer of Tumor-Reactive Transforming Growth Factor-β–Insensitive CD8+ T Cells: Eradication of Autologous Mouse Prostate Cancer

Cited by 138 publications

References 30 publications

Systemic Oncolytic Herpes Virus Therapy of Poorly Immunogenic Prostate Cancer Metastatic to Lung

Systemic Oncolytic Herpes Virus Therapy of Poorly Immunogenic Prostate Cancer Metastatic to Lung

The Multifaceted Roles Neutrophils Play in the Tumor Microenvironment

Targeting tumors with LIGHT to generate metastasis-clearing immunity

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