Heat Shock Protein 90-Mediated Peptide-Selective Presentation of Cytosolic Tumor Antigen for Direct Recognition of Tumors by CD4+ T Cells

Tsuji, Takemasa; Matsuzaki, Junko; Caballero, Otávia L.; Jungbluth, Achim A.; Ritter, Gerd; Odunsi, Kunle; Old, Lloyd J.; Gnjatic, Sacha

doi:10.4049/jimmunol.1103269

Cited by 32 publications

(33 citation statements)

References 45 publications

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“…Indeed, as part of the classical endogenous pathway of antigen presentation, data from in vitro studies suggested that HSP90 may be required for the binding and delivery of chaperoned, antigenic peptides with MHC I molecules to the cell surface (29). More recently, it has been shown that HSP90 can also facilitate direct tumor recognition by CD4 þ T cells via a nonclassical, MHC IImediated mechanism for presentation of intracellular tumor antigens (30). HSP90 also plays pivotal roles in efficient antigen cross-presentation and priming by antigen donor cells (31,32), and in both the functional and phenotypic regulation of T lymphocytes (33).…”

Section: The Hsp90 Paradox For Modulating Tumor Immune Responsesmentioning

confidence: 99%

Targeting Heat-Shock Protein 90 (HSP90) as a Complementary Strategy to Immune Checkpoint Blockade for Cancer Therapy

Proia

Kaufmann

2015

Cancer Immunology Research

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The demonstration that immune checkpoint blockade can meaningfully improve outcomes for cancer patients has revolutionized the field of immuno-oncology. New biologic agents targeting specific checkpoints have shown remarkable durability in terms of patient response and, importantly, exhibit clinical activity across a range of human malignancies, including many that have traditionally proven refractory to other immunotherapies. In this rapidly evolving area, a key consideration relates to the identification of novel combinatorial strategies that exploit existing or investigational cancer therapies in order to optimize patient outcomes and the proportion of individuals able to derive benefit from this approach. In this regard, heat-shock protein 90 (HSP90) represents an important emerging target for cancer therapy because its inactivation results in the simultaneous blockade of multiple signaling pathways and can sensitize tumor cells to other anticancer agents. Within the context of immunology, HSP90 plays a dual regulatory role, with its functional inhibition resulting in both immunosuppressive and immunostimulatory effects. In this Cancer Immunology at the Crossroads overview, the anticancer activity profile of targeted HSP90 inhibitors is discussed along with their paradoxical roles in immunology. Overall, we explore the rationale for combining the modalities of HSP90 inhibition and immune checkpoint blockade in order to augment the antitumor immune response in cancer. Cancer Immunol Res; 3(6); 583-9. Ó2015 AACR.

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Section: The Hsp90 Paradox For Modulating Tumor Immune Responsesmentioning

confidence: 99%

Targeting Heat-Shock Protein 90 (HSP90) as a Complementary Strategy to Immune Checkpoint Blockade for Cancer Therapy

Proia

Kaufmann

2015

Cancer Immunology Research

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“…Melanoma cells, APCs and keratinocytes may contribute to MHC class II-restricted presentation in melanoma tumors. Melanoma cells may express MHC class II and are capable of presenting endogenous membrane bound and cytoplasmic antigens on MHC class II [14, 15]. Melanoma tumor cells directly presenting antigen are capable of activating naïve T cells [12].…”

Section: Introductionmentioning

confidence: 99%

Gamma-interferon-inducible lysosomal thiol reductase is upregulated in human melanoma

Nguyen

Bernert

et al. 2016

Melanoma Research

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T cell-mediated immunity has the ability to produce durable anti-melanoma responses resulting in improved survival of patients with advanced melanoma. Antigen presentation is a key determinant of T cell responses. Gamma-interferon-inducible lysosomal thiol reductase (GILT) is critical for MHC class II-restricted presentation of multiple melanoma antigens to CD4+ T cells. However, GILT expression in melanoma has not been defined. We evaluated GILT and MHC class II expression in human primary and metastatic melanomas and nevi using immunohistochemistry. GILT staining in melanocytes was observed in 70% of primary and 58% of metastatic melanomas versus 0% of nevi. When present, the GILT staining intensity in melanocytes was typically faint. Both GILT and MHC class II expression were increased in melanocytes of primary and metastatic melanomas compared with nevi. GILT staining in antigen presenting cells was detected in 100% of primary and metastatic melanomas versus 31% of nevi and was typically intense. GILT expression was increased in antigen presenting cells of primary and metastatic melanomas compared to nevi, whereas MHC class II had equivalent high expression in antigen presenting cells of all melanocytic lesions. GILT staining in keratinocytes was detected in 67% of primary melanomas versus 14% of nevi and 6% of metastatic melanomas. GILT, but not MHC class II, expression was increased in keratinocytes of primary melanomas compared to nevi and metastases. GILT expression is anticipated to result in improved presentation of melanoma antigens and more effective anti-melanoma T cell responses. GILT expression may be a biomarker of immune recognition of melanoma.

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“…As mentioned, targets of autoimmunity can be generated by chaperone-mediated autophagy [48] but endogenous processing has been reported for various autoantigens [64–68] and tumor antigens [69•,70]. If, as in the case of influenza, the majority of MHC-II-restricted self-peptides are produced by endogenous processing, systems that restrict candidate autoantigens to endosomal processing may miss opportunities for mechanistic insights and therapeutic strategies.…”

Section: Resultsmentioning

confidence: 99%

The elucidation of non-classical MHC class II antigen processing through the study of viral antigens

Ganesan

Eisenlohr

2017

Current Opinion in Virology

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By convention, CD4+ T cells are activated predominantly by Major Histocompatibility Complex class II-bound peptides derived from extracellular (exogenous) antigens. It has been known for decades that alternative sources of antigen, particularly those synthesized within the antigen-presenting cell, can also supply peptides but the impact on TCD4+ responses, sometimes considerable, has only recently become appreciated. This review focuses on the contributions that studies of viral antigen have made to this shift in perspective, concluding with discussions of relevance to rational vaccine design, autoimmunity and cancer immunotherapy.

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Heat Shock Protein 90-Mediated Peptide-Selective Presentation of Cytosolic Tumor Antigen for Direct Recognition of Tumors by CD4+ T Cells

Cited by 32 publications

References 45 publications

Targeting Heat-Shock Protein 90 (HSP90) as a Complementary Strategy to Immune Checkpoint Blockade for Cancer Therapy

Targeting Heat-Shock Protein 90 (HSP90) as a Complementary Strategy to Immune Checkpoint Blockade for Cancer Therapy

Gamma-interferon-inducible lysosomal thiol reductase is upregulated in human melanoma

The elucidation of non-classical MHC class II antigen processing through the study of viral antigens

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