Clonal analysis of cytotoxic and regulatory T cell responses against human melanoma.

Mukherji, Bijay; Guha, Amala; Chakraborty, Nitya G.; Muthukumaran, S.; Nashed, Amgad L.; Sporn, Jonathan; Ergin, M. T.

doi:10.1084/jem.169.6.1961

Cited by 119 publications

(49 citation statements)

References 29 publications

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“…Treg cells are known to suppress T-cell function (10,16,17) and are reported to be elevated in mRCC patients (34, 35). Four-color analysis of PBMC from patients in this study (n = 34) confirmed that mRCC patients have elevated levels of CD3 (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…The frequency of Treg cells is elevated in tumor sites and/or the peripheral blood of patients with advanced tumors (11 -15). Treg cells can impair induction of both antigen-specific and nonspecific T cells in melanoma patients (16,17) and predict reduced survival in multiple cancer cell types (13, 18 -20). Relevant to therapy, experimental models have shown that removal of Treg cells modifies the immune response to tumors.…”

Section: Discussionmentioning

confidence: 99%

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Sunitinib Reverses Type-1 Immune Suppression and Decreases T-Regulatory Cells in Renal Cell Carcinoma Patients

Finke

Rini²,

Ireland

et al. 2008

Clinical Cancer Research

450

364

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Purpose: Immune dysfunction is well documented in renal cell carcinoma (RCC) patients and likely contributes to tumor evasion. This dysfunction includes a shift from a type-1 to a type-2 T-cell cytokine response and enhanced T-regulatory (Treg) cell expression. Given the antitumor activity of select tyrosine kinase inhibitors such as sunitinib in metastatic RCC (mRCC) patients, it is relevant to assess their effect on the immune system. Experimental Design: Type-1 (IFNg) and type-2 (interleukin-4) responses were assessed in T cells at baseline and day 28 of treatment with sunitinib (50 mg/d) by measuring intracellular cytokines after in vitro stimulation with anti-CD3/anti-CD28 antibodies. Results: After one cycle of treatment, there was a significant increase in the percentage of IFNgproducingTcells (CD3 + , P < 0.001; CD3 + CD4 + , P = 0.001), a reduction in interleukin-4 production (CD3 + cells, P = 0.05), and a diminished type-2 bias (P = 0.005).The increase in type-1response may be partly related to modulation of Treg cells. The increased percentage of Treg cells noted in mRCC patients over healthy donors (P = 0.001) was reduced after treatment, although not reaching statistical significance. There was, however, an inverse correlation between the increase in type-1response after two cycles of treatment and a decrease in the percentage of Treg cells (r = -0.64, P = 0.01). In vitro studies suggest that the effects of sunitinib onTreg cells are indirect. Conclusions: The demonstration that sunitinib improved type-1 T-cell cytokine response in mRCC patients while reducingTreg function provides a basis for the rational combination of sunitinib and immunotherapy in mRCC.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Sunitinib Reverses Type-1 Immune Suppression and Decreases T-Regulatory Cells in Renal Cell Carcinoma Patients

Finke

Rini²,

Ireland

et al. 2008

Clinical Cancer Research

450

364

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“…In malignant melanoma, it has been shown that TIL are able to recognize tumour-associated antigens, and in some cases to lyse the malignant cells [16][17][18][19][20][21][22][23][24][25][26][27][28][29][30]. These findings provided a basis for the use of in vitro cultured TIL in adoptive immunotherapy in an effort to enhance the in vivo accumulation of tumour-lytic lymphocytes [29,31].…”

Section: Introductionmentioning

confidence: 99%

Studies of the mechanism of cytolysis by tumour-infiltrating lymphocytes

Hishii

Kurnick

Ramirez-Montagut

et al. 1999

Clinical and Experimental Immunology

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SUMMARYIn order to determine the mechanism of tumour destruction by tumour-infiltrating lymphocytes (TIL), we examined the ability of both CD4 þ and CD8 þ effector TIL, and TIL clones, to manifest granzymemediated and Fas-mediated destruction of tumour targets. In many in vitro studies TIL have been shown to manifest anti-tumour reactivity, yet many tumours escape immunological destruction. To investigate the role of Fas expression and the concomitant sensitivity to the inducibility of apoptotic death, we derived TIL from four melanomas and one glioma. The glioma, and all but one of the melanomas, expressed Fas, but Fas-mediated apoptosis could only be detected if the targets were treated with cyclohexamide. The melanomas and the glioma all expressed detectable cytoplasmic Bcl-2 protein, known to exert anti-apoptotic activity. Lysis of tumours by CD8-enriched cultures and CD8 þ clones was Ca 2þ -dependent and could not be modified by an anti-Fas MoAb. In CD4-enriched cultures or CD4 þ clones with cytotoxic potential against tumour cells, cytotoxicity was also Ca 2þ -dependent. As Ca 2þ -dependent cytotoxicity is usually the result of secretion of perforin/granzyme-B, we investigated the presence of perforin in cytotoxic CD4 þ clones and demonstrated the presence of granular deposits of this enzyme in some of the CD4 þ clones. Although an anti-Fas MoAb did not block the lysis of melanoma targets by CD4 þ clones, the examination of Fas-dependent targets demonstrated that these clones also had the potential to kill by the Fas/Fas ligand system. These data suggest that the predominant mechanism in tumour killing by TIL appears to be perforin-granzyme-dependent, and that the solid tumour cell lines we studied are less susceptible to Fas-mediated apoptosis. As non-apoptotic pathways may enhance tumour immunogenicity, exploitation of the perforin-granzyme-dependent cytotoxic T lymphocyte (CTL) pathways may be important for achieving successful anti-tumour responses.

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“…Cells were harvested in a Titertek semi-automatic cell harvester (Skattron, Sterling, VA, USA) and thymidine incorporation was estimated by a Beckman liquid scintillation counter (Beckman Instruments, Irvine, CA, USA). 6 …”

Section: Proliferation Of Peripheral Blood Mononuclear Cellsmentioning

confidence: 99%

Varicella zoster virus infection associated with high-dose chemotherapy and autologous stem-cell rescue

Bilgrami

Chakraborty

Rodriguez-Pinero

et al. 1999

Bone Marrow Transplant

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Summary:A retrospective evaluation of 215 consecutive recipients of high-dose chemotherapy (HDC) and autologous stem cell rescue (ASCR) was conducted to ascertain the incidence, temporal course, and outcome of varicella zoster virus (VZV) infection. Herpes zoster was identified in 40 individuals at a median of 69 days following ASCR. Six of these cases occurred at a median of 33 days prior to ASCR but following the initiation of high doses of stem cell mobilization chemotherapy. Twenty-five percent of patients demonstrated cutaneous or systemic dissemination and 32.5% required medical intervention for post-herpetic neuralgia. All except two individuals received antiviral chemotherapy. One patient with active VZV infection died of multiorgan failure 39 days after ASCR. Multivariate analysis of risk factors disclosed the significance of prophylactic acyclovir use in Herpes simplex virus seropositive individuals in reducing the risk of VZV infection. Moreover, the use of busulfan, thiotepa and carboplatin as the conditioning chemotherapy regimen was associated with an increased risk of subsequent VZV infection. The incidence of VZV reactivation after HDC and ASCR is similar to that observed following bone marrow transplantation but has an earlier onset. This may be related to an earlier induction of immunosuppression by stem cell mobilization chemotherapy administered prior to ASCR. We demonstrated a marked reduction in the proliferative and synthetic capacities of peripheral blood mononuclear cells obtained prior to and following stem cell mobilizing chemotherapy. Moreover, greater than 80% of VZV infections occurred within 6 months following ASCR and late cases were seldom observed compared to allogeneic and autologous bone marrow transplantation. The role of antiviral chemoprophylaxis during the period of maximum immunocompromise needs to be studied further in the HDC-ASCR setting.

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Clonal analysis of cytotoxic and regulatory T cell responses against human melanoma.

Cited by 119 publications

References 29 publications

Sunitinib Reverses Type-1 Immune Suppression and Decreases T-Regulatory Cells in Renal Cell Carcinoma Patients

Sunitinib Reverses Type-1 Immune Suppression and Decreases T-Regulatory Cells in Renal Cell Carcinoma Patients

Studies of the mechanism of cytolysis by tumour-infiltrating lymphocytes

Varicella zoster virus infection associated with high-dose chemotherapy and autologous stem-cell rescue

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