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Neutrophil extracellular traps sequester circulating tumor cells and promote metastasis

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TLDR
It is reported that circulating tumor cells become trapped within NETs in vitro under static and dynamic conditions and NETs are identified as potential therapeutic targets in the context of systemic infection.
Abstract
The majority of patients with cancer undergo at least one surgical procedure as part of their treatment. Severe postsurgical infection is associated with adverse oncologic outcomes; however, the mechanisms underlying this phenomenon are unclear. Emerging evidence suggests that neutrophils, which function as the first line of defense during infections, facilitate cancer progression. Neutrophil extracellular traps (NETs) are extracellular neutrophil-derived DNA webs released in response to inflammatory cues that trap and kill invading pathogens. The role of NETs in cancer progression is entirely unknown. We report that circulating tumor cells become trapped within NETs in vitro under static and dynamic conditions. In a murine model of infection using cecal ligation and puncture, we demonstrated microvascular NET deposition and consequent trapping of circulating lung carcinoma cells within DNA webs. NET trapping was associated with increased formation of hepatic micrometastases at 48 hours and gross metastatic disease burden at 2 weeks following tumor cell injection. These effects were abrogated by NET inhibition with DNAse or a neutrophil elastase inhibitor. These findings implicate NETs in the process of cancer metastasis in the context of systemic infection and identify NETs as potential therapeutic targets.

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EDIL3 deficiency ameliorates adverse cardiac remodeling by neutrophil extracellular traps (NET)-mediated macrophage polarization.

TL;DR: In this paper, the role of EDIL3 in post-MI adverse remodeling after myocardial infarction (MI) was defined, and it was shown that EDIL-3 deficiency ameliorated adverse cardiac healing via NET-mediated pro-inflammatory macrophage polarization and discovered a new crosstalk between neutrophil and macrophages after MI.
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Mast cells co-expressing CD68 and inorganic polyphosphate are linked with colorectal cancer.

TL;DR: Surgical specimens from CRC were examined to investigate the presence of polyP, as a possible NET inducer, and the detection of CD68+ polyP-expressing mast cells could represent a potential prognostic marker in colorectal adenomas and/or carcinomas.
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Mechanistic insights into the interplays between neutrophils and other immune cells in cancer development and progression

TL;DR: Understanding the detailed mechanisms of neutrophil-tumor cell interactions and the concomitant roles of other immune cells will substantially improve the clinical utility of neutophils in cancer and eventually may aid in the identification of biomarkers for cancer prognosis and the development of novel therapeutic approaches for cancer treatment.
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Bioinspired nucleic acid structures for immune modulation.

TL;DR: This review highlights recent advances in biomaterials inspired by the various interactions of nucleic acids and the immune system, and discusses key advances in self-assembled structures based on exogenous nucleic acid and engineering approaches to apply endogenousucleic acids as found in immunogenic cell death and extracellular traps.
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PAMPs and DAMPs as the Bridge Between Periodontitis and Atherosclerosis: The Potential Therapeutic Targets

TL;DR: This review summarized the research progress of some representative PAMPs and DAMPs as the molecular pathological mechanism bridging periodontitis and atherosclerosis and discussed possible ways to prevent serious cardiovascular events in patients with periodont diseases by targeting molecular patterns.
References
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TL;DR: Analysis of a collected database representing all clinical, surgical-pathologic, and follow-up information for 5,319 patients treated for primary lung cancer confirmed the validity of the TNM and stage grouping classification schema.
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TL;DR: Preoperative chemoradiotherapy improved survival among patients with potentially curable esophageal or esophagogastric-junction cancer and the regimen was associated with acceptable adverse-event rates.
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