Neutrophils as immune effector cells in antibody therapy in cancer

Behrens, Leonie M; Egmond, Marjolein van; Berg, Timo K. van den

doi:10.1111/imr.13159

Cited by 24 publications

(12 citation statements)

References 246 publications

(633 reference statements)

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“…43 We also observed polymer-diABZI uptake by DCs, professional antigen presenting cells that can prime antitumor T cell responses, as well as granulocytes that may also promote antitumor immunity in response to STING activation (Figure 4F-H, S14). 44,45,46 Consistent with their relatively poor capacity for endocytosis, we did not observe uptake by T cells; this may reflect an additional advantage of SAPCon over free diABZI since T cells are susceptible to STING-induced apoptosis.…”

Section: Evaluation Of Sapcon Pharmacokinetics Biodistribution and Ce...supporting

confidence: 66%

STING-Activating Polymer-Drug Conjugates for Cancer Immunotherapy

Sheehy,

Kwiatkowski,

Arora

et al. 2024

Preprint

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The stimulator of interferon genes (STING) pathway links innate and adaptive antitumor immunity and therefore plays an important role in cancer immune surveillance. This has prompted widespread development of STING agonists for cancer immunotherapy, but pharmacological barriers continue to limit the clinical impact of STING agonists and motivate the development of drug delivery systems to improve their efficacy and/or safety. To address this challenge, we developed SAPCon, a STING-activating polymer-drug conjugate platform based on strain-promoted azide-alkyne cycloaddition of dimeric-amidobenzimidazole (diABZI) STING agonists to hydrophilic polymer chains through an enzyme-responsive chemical linker. To synthesize a first-generation SAPCon, we designed a diABZI prodrug modified with a DBCO reactive handle a cathepsin B-cleavable spacer for intracellular drug release and conjugated this to pendant azide groups on a 100 kDa poly(dimethyla acrylamide-co-azide methacrylate) copolymer backbone to increase circulation time and enable passive tumor accumulation. We found that intravenously administered SAPCon accumulated at tumor sites where they it was endocytosed by tumor-associated myeloid cells, resulting in increased STING activation in tumor tissue compared to a free diABZI STING agonist. Consequently, SAPCon promoted an immunogenic tumor microenvironment, characterized by increased frequency of activated macrophages and dendritic cells and improved infiltration of CD8+ T cells, resulting in inhibition of tumor growth, prolonged survival, and increased response to anti-PD-1 immune checkpoint blockade in orthotopic models of breast cancer. Collectively, these studies position SAPCon as a modular and programmable platform for improving the efficacy of systemically administered STING agonists for cancer immunotherapy.

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Section: Evaluation Of Sapcon Pharmacokinetics Biodistribution and Ce...supporting

confidence: 66%

STING-Activating Polymer-Drug Conjugates for Cancer Immunotherapy

Sheehy,

Kwiatkowski,

Arora

et al. 2024

Preprint

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“…Additionally, GO and KEGG gene enrichment analyses suggested that IMPDH1 was associated with neutrophil-related innate immunity and FC gamma R mediated phagocytosis in HCC. As innate immune cells, neutrophils promotes tumor progression by regulating the expression of various inflammatory factors and influencing phagocytosis ( 53 ). Targeting or manipulating neutrophils may gain clinical benefits and are expected to be combined with immunotherapy ( 54 , 55 ).…”

Section: Discussionmentioning

confidence: 99%

IMPDH1, a prognostic biomarker and immunotherapy target that correlates with tumor immune microenvironment in pan-cancer and hepatocellular carcinoma

et al. 2022

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BackgroundsIMPDH1, a rate-limiting enzyme in de novos synthesis of guanine nucleotides, plays an essential role in the growth and progression of certain tumors. However, there is still a lack of study on IMPDH1 evaluating its role in the tumor immune microenvironment, the potential mechanisms, and its potential as a promising tumor therapeutic target.MethodsThe Cancer Genome Atlas (TCGA), Gene Expression Omnibus (GEO), Genotype-Tissue Expression (GTEx), TIMER2.0, KM-Plotter, University of Alabama at Birmingham Cancer data analysis Portal (UALCAN), cbioportal, The Human Protein Atlas (HPA), and Gene Expression Profiling Interactive Analysis 2 (GEPIA2) were used to perform the systematic analysis of IMPDH1, including mRNA expression, protein expression, prognostic value, Enrichment analysis, DNA methylation, immune cell infiltration in pan-cancer, Then, we conducted qRT-PCR and immunohistochemistry to analyze the expression level of IMPDH1 in cancer tissues and non-cancer tissues of patients with primary hepatocellular carcinoma (HCC), and performed the same verification at cellular level.ResultsWe discovered that IMPDH1 was highly expressed in a variety of tumors and was associated with poor prognosis. IMPDH1 not only had the potential as a tumor prognostic marker and therapeutic target, but also was closely related to immune cells, immune checkpoints and immune-related genes and pathways in the tumor immune microenvironment (TIME). Meanwhile, IMPDH1 expression influenced the efficacy and prognosis of tumor patients treated with immune checkpoint inhibitors.ConclusionsIMPDH1 may be as a potential combined target of immunotherapy.

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Section: Neutrophil S In the S E T Ting Of Malig Nan C Ymentioning

confidence: 99%

“…The ability to harness the activity of neutrophils to halt tumor progression, promote elimination of cancer cells, or both could provide clinicians with potent therapies with fewer toxicities than those associated with current interventions. Behrens et al 17 review how neutrophils and monoclonal antibodies can support antibody‐directed cellular cytotoxicity. With tumor cells covered by tumor‐specific monoclonal antibodies, neutrophils can drive tumor killing.…”

Section: Neutrophils In the Setting Of Malignancymentioning

confidence: 99%

“…Critical for this intervention to yield results is formation of the neutrophil cytotoxic synapse: a tight cellular structure dependent on conformational changes that follow binding by Mac‐1 (aka complement receptor 3, α m β 2 , CD11b CD18). Firmly associated with antibody‐targeted tumor cells, neutrophils exert tumor cytotoxicity in a variety of different ways, including trogocytosis, as discussed in detail 17 …”

Section: Neutrophils In the Setting Of Malignancymentioning

confidence: 99%

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