TLR8-Mediated Metabolic Control of Human Treg Function: A Mechanistic Target for Cancer Immunotherapy

Li, Lingyun; Liu, Xia; Sanders, Katherine L.; Edwards, John A.; Ye, Jian; Si, Fusheng; Gao, Aiqin; Huang, Lan; Hsueh, Eddy C.; Ford, David A.; Hoft, Daniel F.; Peng, Guangyong

doi:10.1016/j.cmet.2018.09.020

Cited by 154 publications

(195 citation statements)

References 77 publications

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“…3B). Similar result was observed in the immunecompetent EMT6 mouse syngeneic breast cancer model in which DN052 markedly 19 suppressed tumor growth as a single agent and resulted in complete tumor regression in 1/8, 2/8 and 3/8 tumor-bearing mice at 40, 80 and 160 mg/kg, respectively (Fig. 3C, 3D).…”

Section: Dn052 Strongly Inhibited Tumor Growth As a Single Agent Or Isupporting

confidence: 85%

“…TLR8 was chosen because it is one of the most important molecules of the innate immunity (42,(44)(45)(46). Accumulating evidence indicated that activation of TLR8 could reverse Treg and MDSC mediated immune suppression resulting in strong tumor inhibition (16,(19)(20)(21). One of the major causes of cancer immunotherapy failure is potent suppression of immune response by Treg or MDSC cells (21)(22)(23).…”

Section: Discussionmentioning

confidence: 99%

“…We reasoned that among different TLRs amenable to small molecule modality, specific targeting TLR8 would be advantageous. First, from the efficacy perspective, TLR8 has been shown to be necessary and sufficient to reverse the immune suppressive 4 function of Treg cells leading to strong tumor inhibition (16)(17)(18)(19)(20). TLR8 activation has also been shown to induce apoptosis of MDSCs (21).…”

Section: Introductionmentioning

confidence: 99%

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Development of A Novel Highly Selective TLR8 Agonist for Cancer Immunotherapy

Wang¹,

Yang²,

H³

et al. 2020

Preprint

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Toll-like receptors (TLRs) are a family of proteins that recognize pathogen associated molecular patterns (PAMPs). Their primary function is to activate innate immune responses while also involved in facilitating adaptive immune responses. Different TLRs exert distinct functions by activating varied immune cascades. Several TLRs are being pursued as cancer drug targets. We discovered a novel, highly potent and selective small molecule TLR8 agonist DN052. DN052 exhibited strong in vitro cellular activity with EC50 at 6.7 nM and was highly selective for TLR8 over other TLRs including TLR4, 7 and 9. The selectivity profile distinguished DN052 from all other TLR agonists currently in clinical development. DN052 displayed excellent in vitro ADMET and in vivo PK profiles. DN052 potently inhibited tumor growth as a single agent. Moreover, combination of DN052 with the immune checkpoint inhibitor, selected targeted therapeutics or chemotherapeutic drugs further enhanced efficacy of single agents. Mechanistically, treatment with DN052 resulted in strong induction of pro-inflammatory cytokines in ex vivo human PBMC assay and in vivo monkey study. GLP toxicity studies in rats and monkeys demonstrated favorable safety profile. This led to the advancement of DN052 into phase I clinical trials.

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Section: Dn052 Strongly Inhibited Tumor Growth As a Single Agent Or Isupporting

confidence: 85%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Development of A Novel Highly Selective TLR8 Agonist for Cancer Immunotherapy

Wang¹,

Yang²,

H³

et al. 2020

Preprint

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“…TLR8 stimulation with poly-G reversed the ability of regulatory T cells to suppress T cell proliferation 40 , whereas stimulation with the TLR7/8 ligand R848 in conjunction with TCR activation enhanced proliferation, IFN-γ, IL-8, and IL-10 secretion in memory CD4+ T cells 39 . A recent study reported TLR8-mediated reversal of Treg suppressive functions through inhibition of glucose uptake and glycolysis 96 . Our data show that TLR8 and TLR7 stimulation enhanced TCR activation by increasing the level of phosphorylated proteins involved in TCR signaling such as ribosomal protein S6 and, MAPK signaling (p38, ERK1/2) and NFκB p65.…”

Section: Discussionmentioning

confidence: 99%

Sensing of HIV-1 by TLR8 activates human T cells and reverses latency

et al. 2020

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During HIV infection, cell-to-cell transmission results in endosomal uptake of the virus by target CD4+ T cells and potential exposure of the viral ssRNA genome to endosomal Toll-like receptors (TLRs). TLRs are instrumental in activating inflammatory responses in innate immune cells, but their function in adaptive immune cells is less well understood. Here we show that synthetic ligands of TLR8 boosted T cell receptor signaling, resulting in increased cytokine production and upregulation of surface activation markers. Adjuvant TLR8 stimulation, but not TLR7 or TLR9, further promoted T helper cell differentiation towards Th1 and Th17. In addition, we found that endosomal HIV induced cytokine secretion from CD4+ T cells in a TLR8-specific manner. TLR8 engagement also enhanced HIV-1 replication and potentiated the reversal of latency in patient-derived T cells. The adjuvant TLR8 activity in T cells can contribute to viral dissemination in the lymph node and low-grade inflammation in HIV patients. In addition, it can potentially be exploited for therapeutic targeting and vaccine development.

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“…In multiple murine tumour models, TI‐Tregs have proven to be less vulnerable to glucose restriction than other effector T‐cells . However, in some settings, inhibition of glycolysis in TI‐Tregs reversed Treg suppressive function and promoted anti‐tumour immunity . This may be due to the capacity of Tregs to preferentially convert pyruvate into mitochondrial acetyl‐CoA, which would further support OXPHOS but, more likely, this reflects a requirement for some glycolytic activity in Tregs despite their increased utilization of OXPHOS compared with effector T‐cells.…”

Section: Metabolism In Ti‐tregsmentioning

confidence: 99%

Treg programming and therapeutic reprogramming in cancer

Ayala

DuPage

2019

Immunology

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Summary Overcoming the immunosuppressive tumour microenvironment is the major challenge impeding cancer immunotherapy today. Regulatory T‐cells (Tregs) are prevalent in nearly all cancers and, as immunosuppressive regulators of immune responses, they are the principal opponents of cancer immunotherapy. However, disabling Tregs systemically causes severe autoimmune toxicity, hastening the need for more selective methods to target intratumoural Tregs. In this review, we discuss a burgeoning new modality to specifically target tumour‐infiltrating Tregs (TI‐Tregs) by reprogramming their functionality from immunosuppressive to immune stimulatory within tumours. As the basis for therapeutic selectivity of TI‐Tregs, we will focus on the defining features of Tregs within cancer: their highly activated state controlled by the engagement of key surface receptors, their distinct metabolic programme, and their unique transcriptional programme. By identifying proteins and pathways that distinguish TI‐Tregs from other Tregs in the body, as well as from the beneficial antitumour effector T‐cells within tumours, we highlight mechanisms to selectively reprogramme TI‐Tregs for the treatment of cancer.

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TLR8-Mediated Metabolic Control of Human Treg Function: A Mechanistic Target for Cancer Immunotherapy

Cited by 154 publications

References 77 publications

Development of A Novel Highly Selective TLR8 Agonist for Cancer Immunotherapy

Development of A Novel Highly Selective TLR8 Agonist for Cancer Immunotherapy

Sensing of HIV-1 by TLR8 activates human T cells and reverses latency

Treg programming and therapeutic reprogramming in cancer

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