Selective Targeting of Myeloid-Derived Suppressor Cells in Cancer Patients Using DS-8273a, an Agonistic TRAIL-R2 Antibody

Dominguez, George A.; Condamine, Thomas; Mony, Sridevi; Hashimoto, Ayumi; Wang, Fang; Liu, Qin; Forero, Andres; Bendell, Johanna C.; Witt, Robert L.; Hockstein, Neil; Kumar, Prasanna; Gabrilovich, Dmitry I.

doi:10.1158/1078-0432.ccr-16-1784

Cited by 137 publications

(102 citation statements)

References 32 publications

(35 reference statements)

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“…Our study was focused on the analysis of DR networks in AML cells carrying FLT3‐ITD mutation. This type of analysis has a high clinical relevance, in particular, in view of recent reports that activation of TRAIL‐R2 may downregulate the myeloid‐derived suppressor cells in vivo . These findings increase the interest in the analysis of the DR network in AML cells, in particular focusing on specific mutations, as was done in our study.…”

Section: Discussionsupporting

confidence: 61%

Targeting RIPK1 in AML cells carrying FLT3‐ITD

Hillert

Bettermann‐Bethge

Nimmagadda

et al. 2019

Intl Journal of Cancer

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Mutations of fms-like tyrosine kinase 3 (FLT3) are the most frequent mutations in acute myeloid leukemia (AML). Furthermore, the internal tandem duplication (ITD) represents the most common mutation of FLT3 in AML. To explore therapeutic strategies for AML patients carrying FLT3-ITD, we analyzed death receptor (DR) signaling networks in AML cells comprising FLT3-ITD. We have started with murine myeloid progenitor 32D cells that ectopically express human FLT3-ITD (32D-FLT3-ITD) and found that RIPK1 is strongly upregulated in these cells. Subsequently, we have shown that combinatorial treatment of 32D-FLT3-ITD cells with the SMAC mimetic BV6 and CD95L sensitizes these cells toward apoptosis and necroptosis. Moreover, combinatorial treatment with death ligands (DLs), for example, CD95L or tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) and BV6 enhanced cell death in primary AML blasts from patients carrying FLT3-ITD mutation. Finally, pharmacological and genetic targeting of RIPK1 inhibited DL/BV6-mediated cell death in cells with FLT3-ITD mutations. Taken together, our study suggests a promising therapeutic opportunity for AML cancer cells harboring FLT3-ITD mutation via targeting RIPK1 pathways.

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Section: Discussionsupporting

confidence: 61%

Targeting RIPK1 in AML cells carrying FLT3‐ITD

Hillert

Bettermann‐Bethge

Nimmagadda

et al. 2019

Intl Journal of Cancer

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“…In another study, PMN‐MDSCs were demonstrated to have a shorter lifespan than normal neutrophils and this associated with Trail‐R2 receptor signaling . Importantly, targeting this receptor via an agonistic antibody approach resulted in relatively specific MDSC depletion in both tumor bearing animals and cancer patients …”

Section: Neutrophil Populations In Inflammatory Settingsmentioning

confidence: 99%

“…92 Importantly, targeting this receptor via an agonistic antibody approach resulted in relatively specific MDSC depletion in both tumor bearing animals and cancer patients. 92,93 A separate PMN-MDSC subset has also been characterized during endotoxemia challenge in humans. Pillay et al 10 demonstrated that following LPS stimulation a distinct mature neutrophil population that displays hypersegmented nuclear structure and CD16 hi CD62L lo expression can mediate T cell immunosuppression via ROS and an integrin Mac-1 dependent mechanism.…”

Section: Myeloid-derived Suppressor Cellsmentioning

confidence: 99%

Neutrophil heterogeneity: Bona fide subsets or polarization states?

Deniset

Kubes

2018

Journal of Leukocyte Biology

114

116

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Neutrophils are key components of the innate immune system that play important roles during infection, injury, and chronic disease. In recent years, neutrophil heterogeneity has become an emerging focus with accumulating evidence of neutrophil populations with distinct functions under both steady-state and pathologic conditions. Despite these advances, it remains unclear whether these different populations represent bona fide subsets or simply activation/polarization states in response to local cues. In this review, we summarize the varied neutrophils populations that have been described under both basal and during inflammation. We discuss the evidence that supports the existence of neutrophils subsets. Finally, we identify potential gaps in our knowledge that may further advance our current understanding of neutrophil heterogeneity.

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“…Numerous monoclonal antibody (mAb)-based therapies have shown promising efficacy as cancer therapeutics through the direct targeting of tumor antigens or tolerogenic molecules on immune cells (5,6). Although several mAb-based approaches have been developed to directly target exhausted or immunosuppressed T-cells in cancer patients, there are limited mAb-based therapies that could effectively inhibit MDSCs (7). …”

Section: Introductionmentioning

confidence: 99%

Anti-Jagged Immunotherapy Inhibits MDSCs and Overcomes Tumor-Induced Tolerance

et al. 2017

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Myeloid-derived suppressor cells (MDSCs) are a major obstacle to promising forms of cancer immunotherapy, but tools to broadly limit their immunoregulatory effects remain lacking. In this study, we assessed the therapeutic effect of the humanized anti-Jagged1/2 blocking antibody CTX014 on MDSC-mediated T cell suppression in tumor-bearing mice. CTX014 decreased tumor growth, impacted the accumulation and tolerogenic activity of MDSCs in tumors, and inhibited the expression of immunosuppressive factors arginase I and iNOS. Consequently, anti-Jagged therapy overcame tumor-induced T cell tolerance, increased the infiltration of reactive CD8+ T-cells into tumors, and enhanced the efficacy of T cell-based immunotherapy. Depletion of MDSC-like cells restored tumor growth in mice treated with anti-Jagged, whereas co-injection of MDSC-like cells from anti-Jagged-treated mice with cancer cells delayed tumor growth. Jagged1/2 was induced in MDSCs by tumor-derived factors via NFkB-p65 signaling, and conditional deletion of NFkB-p65 blocked MDSC function. Collectively, our results offer a preclinical proof of concept for the use of anti-Jagged1/2 to reprogram MDSC-mediated T cell suppression in tumors, with implications to broadly improve the efficacy of cancer therapy.

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Selective Targeting of Myeloid-Derived Suppressor Cells in Cancer Patients Using DS-8273a, an Agonistic TRAIL-R2 Antibody

Cited by 137 publications

References 32 publications

Targeting RIPK1 in AML cells carrying FLT3‐ITD

Targeting RIPK1 in AML cells carrying FLT3‐ITD

Neutrophil heterogeneity: Bona fide subsets or polarization states?

Anti-Jagged Immunotherapy Inhibits MDSCs and Overcomes Tumor-Induced Tolerance

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