Deficiency of host CD96 and PD-1 or TIGIT enhances tumor immunity without significantly compromising immune homeostasis

Harjunpää, Heidi; Blake, Stephen J.; Ahern, Elizabeth; Allen, Stacey; Liu, Jing; Yan, Juming; Lutzky, Viviana P.; Takeda, Kazuyoshi; Aguilera, Amy Roman; Guillerey, Camille; Mittal, Deepak; Li, Xian Yang; Dougall, William C.; Smyth, Mark J.; Teng, Michele W.L.

doi:10.1080/2162402x.2018.1445949

Cited by 38 publications

(34 citation statements)

References 49 publications

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“…Five clinical trials are currently evaluating the safety of TIGIT/PD‐1 co‐blockade in cancer patients. Other promising combination targets for TIGIT include TIM‐3 , CD112R or CD96 . Interestingly, while most efforts are focused on blocking TIGIT inhibitory activity through mAbs, a recent study considered TIGIT in the context of T cell engineering .…”

Section: Discussionmentioning

confidence: 99%

“…The majority of patients treated with ipilimumab (anti‐CTLA‐4 mAb) showed irAEs with any grade, while patients treated with PD‐1 blockade showed fewer and less severe irAEs compared to CTLA‐4 blockade . Contrary to CTLA4 −/− mice or to Pdcd1 −/− mice, which develop severe autoimmune and lymphoproliferative syndromes , mice deficient for TIGIT show no signs of spontaneous autoimmunity nor defects in the development of haematopoietic cells . However, when TIGIT −/− mice are immunized or crossed with an autoimmune‐prone strain, they show enhanced development of autoimmune disease .…”

Section: Translating Tigit Blockade Into the Clinicsmentioning

confidence: 99%

“…TIGIT has emerged as a particularly attractive target for cancer therapy due to its seemingly central role in limiting anti‐tumour responses. Moreover, experiments using TIGIT −/− mice suggested that targeting TIGIT would be safe, and possibly trigger fewer irAEs than anti‐PD‐1 or anti‐CTLA‐4 mAbs . Here, we review our current knowledge on TIGIT, from its discovery in 2009 to its current status as a clinical target.…”

Section: Introductionmentioning

confidence: 99%

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TIGIT as an emerging immune checkpoint

Harjunpää

Guillerey

2019

Clinical and Experimental Immunology

364

311

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T cell immunoglobulin and ITIM domain (TIGIT) is an inhibitory receptor expressed on lymphocytes that was recently propelled under the spotlight as a major emerging target in cancer immunotherapy. TIGIT interacts with CD155 expressed on antigen-presenting cells or tumour cells to downregulate T cell and natural killer (NK) cell functions. TIGIT has emerged as a key inhibitor of anti-tumour responses that can hinder multiple steps of the cancer immunity cycle. Pre-clinical studies indicated that TIGIT blockade may protect against various solid and haematological cancers. Several monoclonal antibodies (mAbs) that block the inhibitory activity of human TIGIT have been developed. Clinical trials are ongoing, investigating TIGIT blockade as a monotherapy or in combination with anti-PD1/PD-L1 mAbs for the treatment of patients with advanced solid malignancies. In this review, we cover our current knowledge on TIGIT, from its discovery in 2009 to its current status as a clinical target.

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Section: Discussionmentioning

confidence: 99%

Section: Translating Tigit Blockade Into the Clinicsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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TIGIT as an emerging immune checkpoint

Harjunpää

Guillerey

2019

Clinical and Experimental Immunology

364

311

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“…Similar findings were recently confirmed in double knockout mice lacking both PD-1 and CD96. 145 Moreover, indirect evidence supporting the enhanced anti-tumor performance when both PVR receptors are targeted has been published. TIGIT knockout mice exhibit less metastasis when treated with an anti-CD96 mAb than equivalently treated wild-type mice, indicating that either distinct mechanism or different lymphocyte subsets are involved in this control, 48 although this finding was not confirmed in double knockout mice.…”

Section: Recombinant Oncolytic Poliovirusesmentioning

confidence: 99%

“…TIGIT knockout mice exhibit less metastasis when treated with an anti-CD96 mAb than equivalently treated wild-type mice, indicating that either distinct mechanism or different lymphocyte subsets are involved in this control, 48 although this finding was not confirmed in double knockout mice. 145 However, most of the studies did not adequately address the role of the CD96-PVR interaction and the mechanism of action of these antibodies. As shown in a recent study by Aquilera et al, 92 a specific anti-CD96 antibody that binds to second Ig domain of CD96 and does not prevent its interaction with PVR still retains NK cell-mediated antimetastatic activity in several murine melanoma models.…”

Section: Recombinant Oncolytic Poliovirusesmentioning

confidence: 99%

Targeting PVR (CD155) and its receptors in anti-tumor therapy

Brlić

Roviš

Cinamon³

et al. 2018

Cell Mol Immunol

122

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Poliovirus receptor (PVR, CD155) has recently been gaining scientific interest as a therapeutic target in the field of tumor immunology due to its prominent endogenous and immune functions. In contrast to healthy tissues, PVR is expressed at high levels in several human malignancies and seems to have protumorigenic and therapeutically attractive properties that are currently being investigated in the field of recombinant oncolytic virotherapy. More intriguingly, PVR participates in a considerable number of immunoregulatory functions through its interactions with activating and inhibitory immune cell receptors. These functions are often modified in the tumor microenvironment, contributing to tumor immunosuppression. Indeed, increasing evidence supports the rationale for developing strategies targeting these interactions, either in terms of checkpoint therapy (i.e., targeting inhibitory receptors) or in adoptive cell therapy, which targets PVR as a tumor marker.

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Human CD96 Correlates to Natural Killer Cell Exhaustion and Predicts the Prognosis of Human Hepatocellular Carcinoma

et al. 2019

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Immune checkpoint blockade has become a promising therapeutic approach to reverse immune cell exhaustion. Coinhibitory CD96 and T‐cell immunoglobulin and ITIM domain (TIGIT), together with costimulatory CD226, bind to common ligand CD155. The balancing between three receptors fine‐tunes immune responses against tumors. In this study, we investigated the expression of CD96, TIGIT, and CD226 in 55 fresh human hepatocellular carcinoma (HCC) samples, 236 paraffin‐embedded HCC samples, and 20 normal human livers. The cumulative percentage, absolute count, and mean fluorescence intensity (MFI) of CD96+ NK cells are significantly increased in the intratumoral tissues of HCC and break the balance between three receptors. Human CD96+ NK cells are functionally exhausted with impaired interferon‐gamma (IFN‐γ) and tumor necrosis factor‐alpha (TNF‐α) production, high gene expression of interleukin (IL)‐10 and transforming growth factor‐beta 1 (TGF‐β1), and low gene expression of T‐bet, IL‐15, perforin, and granzyme B. In addition, blocking CD96‐CD155 interaction specifically increases lysis of HepG2 cells by NK cells. HCC patients with a high level of CD96 or CD155 expression within tumor are strongly associated with deteriorating disease condition and shorter disease‐free survival (DFS) and overall survival times. Patients with a higher cumulative percentage of CD96+ NK cells within tumor also exhibit shorter DFS. High plasma level of TGF‐β1 in HCC patients up‐regulates CD96 expression and dynamically shifts the balance between CD96, TIGIT, and CD226 in NK cells. Blocking TGF‐β1 specifically restores normal CD96 expression and reverses the dysfunction of NK cells. Conclusion: These findings indicate that human intratumoral CD96+ NK cells are functionally exhausted and patients with higher intratumoral CD96 expression exhibit poorer clinical outcomes. Blocking CD96‐CD155 interaction or TGF‐β1 restores NK cell immunity against tumors by reversing NK cell exhaustion, suggesting a possible therapeutic role of CD96 in fighting liver cancer.

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Deficiency of host CD96 and PD-1 or TIGIT enhances tumor immunity without significantly compromising immune homeostasis

Cited by 38 publications

References 49 publications

TIGIT as an emerging immune checkpoint

TIGIT as an emerging immune checkpoint

Targeting PVR (CD155) and its receptors in anti-tumor therapy

Human CD96 Correlates to Natural Killer Cell Exhaustion and Predicts the Prognosis of Human Hepatocellular Carcinoma

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