Abstract 1773: Tumor cell-intrinsic STING pathway activation leads to robust induction of Type III Interferons and contributes to the anti-tumor activity elicited by STING agonism

Cetinbas, Naniye Mallı; Monnell, Travis E.; Catcott, Kalli C.; Lee, Winnie; Shaw, Pamela; Slocum, Kelly L.; Avocetien, Kenneth; Bentley, K. W.; Clardy, Susan; Jones, Bradley M.; Kelleher, Eoin; Mosher, Rebecca; Thomas, Joshua D.; Toader, Dorin; Duvall, Jeremy R.; Bukhalid, Raghida; Damelin, Marc; Lowinger, Timothy B.

doi:10.1158/1538-7445.am2021-1773

Cited by 3 publications

(3 citation statements)

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“…Notably, in addition to their potential therapeutic utility, ADCs may also be of use as a research tool for addressing these outstanding questions. Indeed, Cetinbas et al are pursuing such a strategy to dissect the importance of cell-specific STING pathway activation in tumors and have identified distinct differences in resultant immune profiles generated by nontargeted STING agonists and cancer cell-targeted STING agonists, which suggested that cancer cells can positively contribute to antitumor immunity in certain cases …”

Section: Summary Perspectives and Future Directionsmentioning

confidence: 99%

“…Indeed, Cetinbas et al and cancer cell-targeted STING agonists, which suggested that cancer cells can positively contribute to antitumor immunity in certain cases. 544 Another concern facing systemic administration of STING agonists, particularly non-nucleotide, small molecules, is the potential for inducing toxicity in T cells, which are important for therapeutic efficacy. 212 T cells express high levels of the STING protein and appear to be highly susceptible to STINGinduced apoptosis.…”

Section: Summary Perspectives and Futurementioning

confidence: 99%

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Chemical and Biomolecular Strategies for STING Pathway Activation in Cancer Immunotherapy

2022

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The stimulator of interferon genes (STING) cellular signaling pathway is a promising target for cancer immunotherapy. Activation of the intracellular STING protein triggers the production of a multifaceted array of immunostimulatory molecules, which, in the proper context, can drive dendritic cell maturation, antitumor macrophage polarization, T cell priming and activation, natural killer cell activation, vascular reprogramming, and/or cancer cell death, resulting in immune-mediated tumor elimination and generation of antitumor immune memory. Accordingly, there is a significant amount of ongoing preclinical and clinical research toward further understanding the role of the STING pathway in cancer immune surveillance as well as the development of modulators of the pathway as a strategy to stimulate antitumor immunity. Yet, the efficacy of STING pathway agonists is limited by many drug delivery and pharmacological challenges. Depending on the class of STING agonist and the desired administration route, these may include poor drug stability, immunocellular toxicity, immune-related adverse events, limited tumor or lymph node targeting and/or retention, low cellular uptake and intracellular delivery, and a complex dependence on the magnitude and kinetics of STING signaling. This review provides a concise summary of the STING pathway, highlighting recent biological developments, immunological consequences, and implications for drug delivery. This review also offers a critical analysis of an expanding arsenal of chemical strategies that are being employed to enhance the efficacy, safety, and/or clinical utility of STING pathway agonists and lastly draws attention to several opportunities for therapeutic advancements.

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Section: Summary Perspectives and Future Directionsmentioning

confidence: 99%

Section: Summary Perspectives and Futurementioning

confidence: 99%

Chemical and Biomolecular Strategies for STING Pathway Activation in Cancer Immunotherapy

2022

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“…In animal model studies, XMT‐2056 exhibited strong antitumor activity and pharmacokinetic properties, that can significantly induce type III interferon production and inhibit tumor growth. [ 57 ]…”

Section: Pattern Recognition Receptor Agonists As Payloadsmentioning

confidence: 99%

Antibody–Pattern Recognition Receptor Agonist Conjugates: A Promising Therapeutic Strategy for Cancer

Li²,

2022

Advanced Biology

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To date, 12 ADCs (gemtuzumab ozogamicin, brentuximab vedotin, trastuzumab emtansine, inotuzumab ozogamicin, moxetumomab pasudotox, polatuzumab vedotin, trastuzumab deruxtecan, enfortumab vedotin, sacituzumab govitecan, belantamab mafodotin, loncastuximab tesirine-lpyl, and tisotumab vedotin-tftv) have been approved by the FDA to treat various solid tumors and hematological malignancies. [3] An ADC is typically composed of a monoclonal antibody (mAb; recognizes a specific target) linked to a potent cytotoxic molecule (payload drug). In addition, a linker is required to connect these two components and maintain ADC stability. [4] Two types of linkers, namely cleavable [5] and noncleavable linkers, [6] have been developed, and these have met different requirements of preclinical and clinical studies. Cleavable linkers are designed to remain stable in the bloodstream and selectively release the payload drug in the target cell, whereas noncleavable linkers mainly rely on lysosomal degradation to release the payload drug after ADC internalization. [7] All components of an ADC can be distinctively designed to maximize its binding affinity and therapeutic effect (Figure 1).The ADC as a complex fully exerts biological effect of the two components and selectively delivers the payload drug to target tissues through the mAb. The ADC initially binds to cell surface antigens and enters tumor cells through clathrin-mediated endocytosis. [8] It is then transported to the early endosome, and it subsequently enters the lysosome where it is degraded by proteolytic enzymes to release the payload drug into the cytoplasm. [9] Ultimately, cytotoxic drugs induce tumor cell death or apoptosis via different mechanisms, such as by damaging DNA or inhibiting microtubule synthesis. [10] This process results in minimal systemic toxic effects, but it improves the treatment window of cytotoxic drugs, and the therapeutic efficacy is enhanced accordingly. [11] Development History of Antibody-Drug ConjugatesThe history of ADC drug development occurred in three stages and provided three generations of ADCs. For first-generation ADCs, cytotoxic drugs were mainly conjugated with mouse mAbs via non-cleavable linkers. This increased the possibility of inducing antidrug antibody effects. In addition, off-target Antibody-drug conjugates (ADCs) are composed of monoclonal antibodies linked to cytotoxic payload drugs, each of which can be diversely designed in accordance with pharmacological and clinical requirements. The use of ADCs is effective for the treatment of different diseases, including cancers, and is gaining widespread attention. To date, 12 ADCs have been approved by the U.S. Food and Drug Administration for treating cancer and improving the quality of life of patients. To expand the application of ADCs and improve their treatment efficiency, various formats have recently been manufactured, including pattern recognition receptor (PRR) agonist-based ADCs. The antibody has a unique structure that enables the specific delivery of PRR agonists ...

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Delivery of STING agonists for adjuvanting subunit vaccines

Herck

Feng

Tang

2021

Advanced Drug Delivery Reviews

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Abstract 1773: Tumor cell-intrinsic STING pathway activation leads to robust induction of Type III Interferons and contributes to the anti-tumor activity elicited by STING agonism

Cited by 3 publications

References 0 publications

Chemical and Biomolecular Strategies for STING Pathway Activation in Cancer Immunotherapy

Chemical and Biomolecular Strategies for STING Pathway Activation in Cancer Immunotherapy

Antibody–Pattern Recognition Receptor Agonist Conjugates: A Promising Therapeutic Strategy for Cancer

Delivery of STING agonists for adjuvanting subunit vaccines

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