STING Agonists as Cancer Therapeutics

Amouzegar, Afsaneh; Chelvanambi, Manoj; Filderman, J; Storkus, Walter J.; Luke, Jason J.

doi:10.3390/cancers13112695

Cited by 223 publications

(197 citation statements)

References 123 publications

(146 reference statements)

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“…The activation of immune cells after DMXAA application is mainly related to the protein STING (stimulator of interferon genes). The pathway associated with the STING protein is a relatively new direction of research in cancer therapy [63]. It is well known that immune cells' activation using STING agonists mediates the innate immune response, which is responsible for the therapeutic effect [21,64].…”

Section: Discussionmentioning

confidence: 99%

The Proper Administration Sequence of Radiotherapy and Anti-Vascular Agent—DMXAA Is Essential to Inhibit the Growth of Melanoma Tumors

Drzyzga

Cichoń

Czapla

et al. 2021

Cancers

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Vascular disrupting agents (VDAs), such as DMXAA, effectively destroy tumor blood vessels and cause the formation of large areas of necrosis in the central parts of the tumors. However, the use of VDAs is associated with hypoxia activation and residues of rim cells on the edge of the tumor that are responsible for tumor regrowth. The aim of the study was to combine DMXAA with radiotherapy (brachytherapy) and find the appropriate administration sequence to obtain the maximum synergistic therapeutic effect. We show that the combination in which tumors were irradiated prior to VDAs administration is more effective in murine melanoma growth inhibition than in either of the agents individually or in reverse combination. For the first time, the significance of immune cells’ activation in such a combination is demonstrated. The inhibition of tumor growth is linked to the reduction of tumor blood vessels, the increased infiltration of CD8+ cytotoxic T lymphocytes and NK cells and the polarization of macrophages to the cytotoxic M1 phenotype. The reverse combination of therapeutic agents showed no therapeutic effect and even abolished the effect of DMXAA. The combination of brachytherapy and vascular disrupting agent effectively inhibits the growth of melanoma tumors but requires careful planning of the sequence of administration of the agents.

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Section: Discussionmentioning

confidence: 99%

The Proper Administration Sequence of Radiotherapy and Anti-Vascular Agent—DMXAA Is Essential to Inhibit the Growth of Melanoma Tumors

Drzyzga

Cichoń

Czapla

et al. 2021

Cancers

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“…The cGAS-STING signaling in cancer cells is an increasingly recognized and important mechanism connecting genome instability to immune cell infiltration and inflammation in neoplastic malignant tumors [ 210 ]. Subsequently, tumor cells frequently impair cGAS-STING signaling to evade immune surveillance [ 211 , 212 , 213 ]. Thus, agonists are being developed to restore and to enhance cGAS-STING activity and the subsequent antitumor immune response in cancer treatment [ 212 ].…”

Section: Cancermentioning

confidence: 99%

“…Subsequently, tumor cells frequently impair cGAS-STING signaling to evade immune surveillance [ 211 , 212 , 213 ]. Thus, agonists are being developed to restore and to enhance cGAS-STING activity and the subsequent antitumor immune response in cancer treatment [ 212 ]. It should be noted, however, that the immune response to cancer cells including the cGAS-STING signaling, is complex and an extensive review of the current state of the field is beyond the scope of this Review.…”

Section: Cancermentioning

confidence: 99%

Cytosolic Self-DNA—A Potential Source of Chronic Inflammation in Aging

Akbari

Shanley

Bohr

et al. 2021

Cells

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Aging is the consequence of a lifelong accumulation of stochastic damage to tissues and cellular components. Advancing age closely associates with elevated markers of innate immunity and low-grade chronic inflammation, probably reflecting steady increasing incidents of cellular and tissue damage over the life course. The DNA sensing cGAS-STING signaling pathway is activated by misplaced cytosolic self-DNA, which then initiates the innate immune responses. Here, we hypothesize that the stochastic release of various forms of DNA from the nucleus and mitochondria, e.g., because of DNA damage, altered nucleus integrity, and mitochondrial damage, can result in chronic activation of inflammatory responses that characterize the aging process. This cytosolic self-DNA-innate immunity axis may perturb tissue homeostasis and function that characterizes human aging and age-associated pathology. Proper techniques and experimental models are available to investigate this axis to develop therapeutic interventions.

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“…An increasing number of investigations have shown that STING is involved in various diseases; the activation of STING can develop as cancer therapeutics. However, the activation of STING can also induce inflammatory responses and lead to inflammatory injury ( Amouzegar et al, 2021 ; Decout et al, 2021 ). The activation of STING is associated with inflammatory diseases such as acute pancreatitis, sepsis, and rheumatoid arthritis ( Jeremiah et al, 2014 ; Heipertz et al, 2017 ; Zhao et al, 2018 ; Wang et al, 2019 ).…”

Section: Introductionmentioning

confidence: 99%

Tanreqing Inhibits LPS-Induced Acute Lung Injury In Vivo and In Vitro Through Downregulating STING Signaling Pathway

Zhou

Deng

et al. 2021

Front. Pharmacol.

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Acute lung injury (ALI) is a common life-threatening lung disease, which is mostly associated with severe inflammatory responses and oxidative stress. Tanreqing injection (TRQ), a Chinese patent medicine, is clinically used for respiratory-related diseases. However, the effects and action mechanism of TRQ on ALI are still unclear. Recently, STING as a cytoplasmic DNA sensor has been found to be related to the progress of ALI. Here, we showed that TRQ significantly inhibited LPS-induced lung histological change, lung edema, and inflammatory cell infiltration. Moreover, TRQ markedly reduced inflammatory mediators release (TNF-α, IL-6, IL-1β, and IFN-β). Furthermore, TRQ also alleviated oxidative stress, manifested by increased SOD and GSH activities and decreased 4-HNE, MDA, LDH, and ROS activities. In addition, we further found that TRQ significantly prevented cGAS, STING, P-TBK, P-P65, P-IRF3, and P-IκBα expression in ALI mice. And we also confirmed that TRQ could inhibit mtDNA release and suppress signaling pathway mediated by STING in vitro. Importantly, the addition of STING agonist DMXAA dramatically abolished the protective effects of TRQ. Taken together, this study indicated that TRQ alleviated LPS-induced ALI and inhibited inflammatory responses and oxidative stress through STING signaling pathway.

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STING Agonists as Cancer Therapeutics

Cited by 223 publications

References 123 publications

The Proper Administration Sequence of Radiotherapy and Anti-Vascular Agent—DMXAA Is Essential to Inhibit the Growth of Melanoma Tumors

The Proper Administration Sequence of Radiotherapy and Anti-Vascular Agent—DMXAA Is Essential to Inhibit the Growth of Melanoma Tumors

Cytosolic Self-DNA—A Potential Source of Chronic Inflammation in Aging

Tanreqing Inhibits LPS-Induced Acute Lung Injury In Vivo and In Vitro Through Downregulating STING Signaling Pathway

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