Immunotherapy of Cytotoxic T Cell–resistant Tumors by T Helper 2 Cells

Mattes, Joërg; Hulett, Mark D.; Xie, Wei; Hogan, Simon P.; Rothenberg, Marc E.; Foster, Paul S.; Parish, Christopher R.

doi:10.1084/jem.20021683

Cited by 210 publications

(224 citation statements)

References 26 publications

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“…As discussed above, we did not observe any influence of STAT6 signaling on the differentiation of DCT-specific CD4 1 T cells, suggesting that STAT6 is also required downstream of the effector CD4 1 T cells. Consistent with our observation, Mattes et al [10] demonstrated that tumor regression mediated by transferred Th2 effector cells was dependent on the host expression of STAT6. Furthermore, there is ample evidence that STAT6 plays a critical role in the late phase of allergic asthma, in addition to its requirement in Th2 differentiation [32,33].…”

Section: Wt Vssupporting

confidence: 93%

“…More importantly, this anti-tumor mechanism did not evoke fulminant autoimmune pathology. The utility of Th2 cells or IL-4 as anti-tumor effectors has been reported by others, and in some cases Th2 cells were more effective than Th1 cells in the clearance of cytotoxic T lymphocyte-resistant tumors [10]. Furthermore, a human clinical trial of Canvaxin, a cell-based vaccine, found that the magnitude of vaccine-induced Th2 immunity correlated with overall survival, and anti-tumor Th2 cells can be identified in cancer patients supporting the possibility of generating such populations in humans [30,31].…”

Section: Wt Vsmentioning

confidence: 61%

“…Increasing evidence indicates that CD4 1 T cells are able to mediate tumor destruction without direct interaction with tumor cells and that CD4 1 T cells may provide even greater anti-tumor effect than CD8 1 T cells [5][6][7][8]. Furthermore, reports from various groups, including ours, have demonstrated the ability of CD4 1 T cells to reject cytotoxic T lymphocyte-resistant, MHC class II-negative tumors [7,9,10]. Therefore, understanding the potential for CD4 1 T cells as antitumor effectors is of broad value to both MHC class II-positive and -negative tumors.…”

Section: Introductionmentioning

confidence: 65%

“…With regard to MHC class II-negative tumors, it is believed that APC infiltrating the tumor bed process tumor antigen and present it to CD4 1 T cells. In turn, the tumor antigen-stimulated CD4 1 T cells can produce IFN-g (Th1) or IL-4 (Th2); both of these cytokines display anti-angiogenic properties and are able to recruit other tumoricidal cells such as NK, macrophages or eosinophils into the tumor [5,[10][11][12]. These indirect destructive mechanisms may prove advantageous over the direct effector functions mediated by CD8 1 T cells as the indirect mechanisms should not be affected by MHC expression levels on the tumor cell and consequently may deter the development of tumor escape variants due to antigen loss.…”

Section: Introductionmentioning

confidence: 99%

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CD4⁺ T‐cell‐mediated anti‐tumor immunity can be uncoupled from autoimmunity via the STAT4/STAT6 signaling axis

et al. 2009

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Previous reports have suggested that autoimmune sequelae may be an unavoidable consequence of successful immunization against tumor-associated antigens, which are typically non-mutated self-antigens. Using a melanoma model, we demonstrated that CD4 1 T-cell-mediated anti-tumor immunity and autoimmunity could be separated by modulating the STAT4/STAT6 signaling axis. Our results have revealed an unexpected dichotomy in the effector phase following cancer vaccination where anti-tumor immunity is mediated via a STAT6 and IL-4-dependent pathway, whereas autoimmune pathology is mediated via STAT4 through a mechanism that relies partially on IFN-c. Our results offer a possibility to elicit specific anti-tumor responses without triggering unwanted tissue autoimmune diseases.

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Section: Wt Vssupporting

confidence: 93%

Section: Wt Vsmentioning

confidence: 61%

Section: Introductionmentioning

confidence: 65%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

CD4⁺ T‐cell‐mediated anti‐tumor immunity can be uncoupled from autoimmunity via the STAT4/STAT6 signaling axis

et al. 2009

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“…Even though the beneficial effect of TATE remains controversial, the presence of eosinophils appears as an indicator of good prognosis indicator in some cancers, such as head and neck cancers (7)(8)(9) and gastrointestinal cancers (10), particularly in colorectal cancers, in which high eosinophil counts were associated to increased 5-y survival (11). Clinical observations that eosinophil accumulation in intestinal tumors was associated to a better prognosis have been recently supported by experimental data in murine models (12)(13)(14).…”

mentioning

confidence: 60%

Human Eosinophils Exert TNF-α and Granzyme A-Mediated Tumoricidal Activity toward Colon Carcinoma Cells

Legrand

Driss

Delbeke

et al. 2010

The Journal of Immunology

148

135

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Peripheral blood and tissue eosinophilia is a prominent feature in allergic diseases and helminth infections. In cancer patients, tumor-associated tissue eosinophilia is frequently observed. Tumor-associated tissue eosinophilia can be associated with a favorable prognosis, notably in colorectal carcinoma. However, underlying mechanisms of eosinophil contribution to antitumor responses are poorly understood. We have in this study investigated the direct interactions of human eosinophils with Colo-205, a colorectal carcinoma cell line, and show that eosinophils induce apoptosis and directly kill tumor cells. Using blocking Abs, we found that CD11a/CD18 complex is involved in the tumoricidal activity. Coculture of eosinophils with Colo-205 led to the release of eosinophil cationic protein and eosinophil-derived neurotoxin as well as TNF-α secretion. Moreover, eosinophils expressed granzyme A, which was released upon interaction with Colo-205, whereas cytotoxicity was partially inhibited by FUT-175, an inhibitor of trypsin-like enzymatic activity. Our data present the first demonstration, to our knowledge, that granzyme A is a cytotoxic mediator of the eosinophil protein arsenal, exerting eosinophil tumoricidal activity toward Colo-205, and provide mechanistic evidence for innate responses of eosinophil against tumor cells.

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NY‐CO‐58/KIF2C is overexpressed in a variety of solid tumors and induces frequent T cell responses in patients with colorectal cancer

Gnjatic

Cao

Reichelt

et al. 2010

Intl Journal of Cancer

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NY-CO-58/KIF2C has been identified as a tumor antigen by screening antibody responses in patients with colorectal cancer. However, expression had not consequently been examined, and nothing was known about its ability to induce spontaneous T cell responses, which have been suggested to play a role in the development of colorectal cancer. We analyzed 5 colorectal cancer cell lines, and tumor samples and adjacent healthy tissues from 176 patients with epithelial cancers for the expression of NY-CO-58/KIF2C by RT-PCR and Western Blot. T cell responses of 43 colorectal cancer patients and 35 healthy donors were evaluated by ELISpot following stimulation with 30mer peptides or full-length protein. All cell lines and tumor samples from colorectal cancer patients expressed NY-CO-58/KIF2C on the protein and RNA level, and expression levels correlated strongly with Ki-67 expression (r 5 0.69; p 5 0.0003). Investigating NY-CO-58/KIF2C-specific T cell responses, CD81 T cells directed against 1 or more peptides were found in less than 10% of patients, whereas specific CD4 1 T cells were detected in close to 50% of patients. These T cells were of high avidity, recognized the naturally processed antigen and secreted IFN-c and TNF-a. Depletion of CD4 1 CD25 1 T cells before stimulation significantly increased the intensity of the preexisting response. NY-CO-58/KIF2C is significantly overexpressed in colorectal and other epithelial cancers and expression levels correlate with the proliferative activity of the tumor. Importantly, NY-CO-58/KIF2C was able to induce spontaneous CD4 1 T cell responses of the Th1-type, which were tightly controlled by peripheral T regulatory cells.Colorectal cancer is the second leading cause of cancerrelated death in Western countries with $1 million new cases and over 500,000 deaths per year worldwide. 1 In locally advanced colorectal cancer, surgery combined with the selective application of adjuvant chemotherapy represents the treatment of choice providing cure in a significant number of cases. However, about 40% of patients whose primary tumor has surgically been removed will eventually relapse and ultimately die from the disease.2 Therefore, alternative therapeutic strategies, especially in the adjuvant setting, are needed to improve the prognosis of patients with this malignancy.In the case of colorectal carcinoma, there is strong evidence for a role of the T cell-mediated immune system in controlling the development and progression of the disease. Thus, it has convincingly been demonstrated that infiltration

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Immunotherapy of Cytotoxic T Cell–resistant Tumors by T Helper 2 Cells

Cited by 210 publications

References 26 publications

CD4⁺ T‐cell‐mediated anti‐tumor immunity can be uncoupled from autoimmunity via the STAT4/STAT6 signaling axis

CD4⁺ T‐cell‐mediated anti‐tumor immunity can be uncoupled from autoimmunity via the STAT4/STAT6 signaling axis

Human Eosinophils Exert TNF-α and Granzyme A-Mediated Tumoricidal Activity toward Colon Carcinoma Cells

NY‐CO‐58/KIF2C is overexpressed in a variety of solid tumors and induces frequent T cell responses in patients with colorectal cancer

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Immunotherapy of Cytotoxic T Cell–resistant Tumors by T Helper 2 Cells

Cited by 210 publications

References 26 publications

CD4+ T‐cell‐mediated anti‐tumor immunity can be uncoupled from autoimmunity via the STAT4/STAT6 signaling axis

CD4+ T‐cell‐mediated anti‐tumor immunity can be uncoupled from autoimmunity via the STAT4/STAT6 signaling axis

Human Eosinophils Exert TNF-α and Granzyme A-Mediated Tumoricidal Activity toward Colon Carcinoma Cells

NY‐CO‐58/KIF2C is overexpressed in a variety of solid tumors and induces frequent T cell responses in patients with colorectal cancer

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Resources

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CD4⁺ T‐cell‐mediated anti‐tumor immunity can be uncoupled from autoimmunity via the STAT4/STAT6 signaling axis

CD4⁺ T‐cell‐mediated anti‐tumor immunity can be uncoupled from autoimmunity via the STAT4/STAT6 signaling axis