Immune-checkpoint proteins VISTA and PD-1 nonredundantly regulate murine T-cell responses

Li, Jun; Yuan, Ying; Chen, Wenna; Putra, Juan; Suriawinata, Arief A.; Schenk, Austin D.; Miller, Halli E.; Guleria, Indira; Barth, Richard J.; Huang, Yina H.; Wang, Li

doi:10.1073/pnas.1420370112

Cited by 284 publications

(274 citation statements)

References 36 publications

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“…43 It has been shown that VISTA and PD-1 exert non-redundant immune regulatory functions and synergistically regulate T-cell responses. 17 Combined blockade using monoclonal antibodies specific for VISTA and PD-L1 achieved optimal tumor-clearing therapeutic efficacy in murine tumor models. 14 Our data indicate an involvement of both VISTA and PD-1 pathways in the immune evasion in AML, therefore combinational treatment targeting these two inhibitory pathways may lead to a successful leukemia control and improve the clinical outcome.…”

Section: Discussionmentioning

confidence: 99%

“…Combined inhibition of both VISTA and PD-1 pathways synergistically improves anti-tumor T cell activity. 14,17 These observations suggest a strong therapeutic potential of targeting VISTA for optimal tumor control. To investigate the effect of VISTA on anti-leukemia immune response in AML, we initiated a study using clinical samples collected from AML patients.…”

Section: Introductionmentioning

confidence: 98%

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VISTA is highly expressed on MDSCs and mediates an inhibition of T cell response in patients with AML

et al. 2018

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Treatment of acute myeloid leukemia (AML) remains challenging. Enhancement of anti-tumor responses by blocking negative immune regulators is a promising strategy for novel effective leukemia therapeutics. V-domain Ig suppressor of T-cell activation (VISTA) is a recently defined negative regulator mediating immune evasion in cancer. To investigate the effect of VISTA on anti-leukemia immune response in AML, we initiated a study using clinical samples collected from AML patients. Here we report that VISTA is highly expressed on myeloid-derived suppressor cells (MDSCs) in the peripheral blood of AML patients. Both the frequency and intensity of VISTA expression on MDSCs are significantly higher in newly diagnosed AML than in healthy controls. Importantly knockdown of VISTA by specific siRNA potently reduced the MDSCs-mediated inhibition of CD8 T cell activity in AML, suggesting a suppressive effect of VISTA on anti-leukemia T cell response. Furthermore, we observed a strong positive association between MDSC expression of VISTA and T cell expression of PD-1 in AML. These results support the strategy of VISTA-targeted treatment for AML and underscore the strong potential for combined blockade of VISTA and PD-1 pathways in effective leukemia control.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 98%

VISTA is highly expressed on MDSCs and mediates an inhibition of T cell response in patients with AML

et al. 2018

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“…Anti-VISTA monoclonal antibody also intensified EAE. Synergies between VISTA and PD-1 in regulating T cell tolerance are demonstrated by studies of VISTA/PD-1 and VISTA/PD-L1 double knockout mice, which developed increased frequencies of activated T cells and inflammation compared to single knockout mice, but no spontaneous autoimmunity (152). These findings suggest that combined VISTA and PD-1 blockade may have therapeutic benefits associated with limited adverse events.…”

Section: V-domain Immunoglobulin-containing Suppressor Of T Cell Actimentioning

confidence: 94%

Coinhibitory Pathways in Immunotherapy for Cancer

Baumeister

Freeman

Dranoff

et al. 2016

Annu. Rev. Immunol.

772

777

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The immune system is capable of recognizing tumors and eliminates many early malignant cells. However, tumors evolve to evade immune attack, and the tumor microenvironment is immunosuppressive. Immune responses are regulated by a number of immunological checkpoints that promote protective immunity and maintain tolerance. T cell coinhibitory pathways restrict the strength and duration of immune responses, thereby limiting immune-mediated tissue damage, controlling resolution of inflammation, and maintaining tolerance to prevent autoimmunity. Tumors exploit these coinhibitory pathways to evade immune eradication. Blockade of the PD-1 and CTLA-4 checkpoints is proving to be an effective and durable cancer immunotherapy in a subset of patients with a variety of tumor types, and additional combinations are further improving response rates. In this review we discuss the immunoregulatory functions of coinhibitory pathways and their translation to effective immunotherapies for cancer.

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“…Frozen sections are sometimes used for these sensitive Abs (26), but this results in distorted tissue architecture and artifacts that compromise morphological studies. For these reasons, flow cytometry has long been the gold standard for analysis of immune infiltrates in the tumor microenvironment (27). However, flow cytometry does not provide sufficient contextual information, which was shown, in murine and human studies, to be important in understanding the biological basis of diseases and for predicting outcome in various types of cancer (1,3).…”

Section: Discussionmentioning

confidence: 99%

“…pmel-1 TCR-transgenic mice were bred to Rag1 2/2 mice to generate pmel TCR/Rag1 2/2 mice. pmel TCR/Rag1 2/2 mice have CD8 + T cells expressing a transgenic TCR specific for mgp100 (25)(26)(27)(28)(29)(30)(31)(32)(33) peptide. TRP1 TCR/Rag1 2/2 -transgenic mice have CD4 + T cells expressing a transgenic TCR specific for mtyrp1 (113)(114)(115)(116)(117)(118)(119)(120)(121)(122)(123)(124)(125)(126)(127) peptide.…”

mentioning

confidence: 99%

Multispectral Imaging of T and B Cells in Murine Spleen and Tumor

Feng

Jensen

Messenheimer

et al. 2016

The Journal of Immunology

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Recent advances in multiplex immunohistochemistry techniques allow for quantitative, spatial identification of multiple immune parameters for enhanced diagnostic and prognostic insight. However, applying such techniques to murine fixed tissues, particularly sensitive epitopes, such as CD4, CD8α, and CD19, has been difficult. We compared different fixation protocols and Ag-retrieval techniques and validated the use of multiplex immunohistochemistry for detection of CD3+CD4+ and CD3+CD8+ T cell subsets in murine spleen and tumor. This allows for enumeration of these T cell subsets within immune environments, as well as the study of their spatial distribution.

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Immune-checkpoint proteins VISTA and PD-1 nonredundantly regulate murine T-cell responses

Cited by 284 publications

References 36 publications

VISTA is highly expressed on MDSCs and mediates an inhibition of T cell response in patients with AML

VISTA is highly expressed on MDSCs and mediates an inhibition of T cell response in patients with AML

Coinhibitory Pathways in Immunotherapy for Cancer

Multispectral Imaging of T and B Cells in Murine Spleen and Tumor

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