MiR-155 regulates neutrophil extracellular trap formation and lung injury in abdominal sepsis

Hawez, Avin; Taha, Dler; Algaber, Anwar; Madhi, Raed; Rahman, Milladur; Thorlacius, Henrik

doi:10.1002/jlb.3a1220-789rr

Cited by 19 publications

(12 citation statements)

References 45 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…24 , 39 , 40 Furthermore, preclinical studies have shown a great potential for anti-NET strategies in limiting inflammation-associated collateral damage in sepsis models. 23 , 38 , 41 – 43 Our study confirms these earlier reports, in that we found that NET inhibition or NET degradation significantly improved outcomes in a mouse model of neonatal peritonitis. Targeting NETs reduced the levels of inflammatory cytokines in the peritoneal cavity and reduced circulating platelet–neutrophil aggregates, a sensitive marker for systemic platelet activation.…”

Section: Discussionsupporting

confidence: 90%

Neutrophil extracellular trap inhibition improves survival in neonatal mouse infectious peritonitis

et al. 2022

View full text Add to dashboard Cite

Background Treatment of neonatal peritonitis and sepsis is challenging. Following infection, neutrophils elaborate neutrophil extracellular traps (NETs)—extracellular lattices of decondensed chromatin decorated with antimicrobial proteins. NETs, however, can augment pathogenic inflammation causing collateral damage. We hypothesized that NET inhibition would improve survival in experimental neonatal infectious peritonitis. Methods We induced peritonitis in 7 to 10-day-old mice by intraperitoneal injection with cecal slurry. We targeted NETs by treating mice with neonatal NET-Inhibitory Factor (nNIF), an endogenous NET-inhibitor; Cl-amidine, a PAD4 inhibitor; DNase I, a NET degrading enzyme, or meropenem (an antibiotic). We determined peritoneal NET and cytokine levels and circulating platelet–neutrophil aggregates. Survival from peritonitis was followed for 6 days. Results nNIF, Cl-amidine, and DNase I decreased peritoneal NET formation and inflammatory cytokine levels at 24 h compared to controls. nNIF, Cl-amidine, and DNase I decreased circulating platelet–neutrophil aggregates, and NET-targeting treatments significantly increased survival from infectious peritonitis compared to controls. Finally, nNIF administration significantly improved survival in mice treated with sub-optimal doses of meropenem even when treatment was delayed until 2 h after peritonitis induction. Conclusions NET inhibition improves survival in experimental neonatal infectious peritonitis, suggesting that NETs participate pathogenically in neonatal peritonitis and sepsis. Impact Neutrophil extracellular trap formation participates pathogenically in experimental neonatal infectious peritonitis. NET-targeting strategies improve outcomes in a translational model of neonatal infectious peritonitis. NET inhibition represents a potential target for drug development in neonatal sepsis and infectious peritonitis.

show abstract

Section: Discussionsupporting

confidence: 90%

Neutrophil extracellular trap inhibition improves survival in neonatal mouse infectious peritonitis

et al. 2022

View full text Add to dashboard Cite

show abstract

“…Moreover, Wu et al reported that overexpression of miR-155 promoted the chronic intermittent hypoxia-induced NLRP3 inflammasome activation in renal tubular cells [ 34 ]. Additionally, Hawez et al revealed that miR-155 regulates the pulmonary formation of neutrophil extracellular traps in abdominal sepsis [ 35 ]. More importantly, miR-155 has been noted to be highly expressed in COPD, while miR-155 deficiency notably suppressed CSE-mediated lung inflammation [ 36 ].…”

Section: Discussionmentioning

confidence: 99%

Wenshen Yiqi Keli Mitigates the Proliferation and Migration of Cigarette Smoke Extract-Induced Human Airway Smooth Muscle Cells through miR-155/FoxO3a Axis

Dong

Liu

et al. 2022

Evidence-Based Complementary and Alternative Medicine

View full text Add to dashboard Cite

Some domestic scholars revealed the effectiveness of Wenshen Yiqi Keli (WSYQKL) on chronic obstructive pulmonary disease (COPD). However, the exact mechanism of WSYQKL on COPD is fuzzy and needs further research. We adopted UPLC-Q/TOF-MS to analyze the chemical components of WSYQKL. In in vitro experiments, human airway smooth muscle cells (hASMCs) were intervened with 2.5% cigarette smoke extract (CSE), medicine serum of WSYQKL, miR-155 mimic, and FoxO3a silencing. Cell viability, proliferation, migration, and the expressions of miR-155, PCNA, Ki67, p21, p27, and FoxO3a were examined by cell counting kit-8, EdU staining, Transwell assay, scarification assay, qRT-PCR, immunol cytochemistry, and western blot, respectively. The association between miR-155 and FoxO3a was assessed by database and luciferase reporter gene analysis. We identified 47 kinds of chemical compositions of WSYQKL in ESI+ mode and 42 kinds of components of WSYQKL in ESI− mode. The medicine serum of WSYQKL strongly alleviated the proliferation and migration of hASMCs induced by CSE in a concentration-dependent manner. The medicine serum of WSYQKL enhanced the levels of p21, p27, and FoxO3a and weakened PCNA and Ki67 levels in hASMCs induced by CSE with the increase of concentration. MiR-155 mimic or FoxO3a silencing notably advanced CSE-treated HASMC viability, proliferation, migration, and the levels of PCNA and Ki67 and downregulated the levels of p21, p27, and FoxO3a in CSE-triggered hASMCs, which was reversed by WSYQKL-containing serum. Our results described that WSYQKL alleviated the proliferation and migration of hASMCs induced by CSE by modulating the miR-155/FoxO3a axis.

show abstract

“…Thus, these authors showed that miR-155/ PAD4 interaction after transfection of human neutrophils with miR-155 mimic or inhibitor correlated with NET formation capacity in vitro [50]. Furthermore, miR-155 deficiency in a murine model of abdominal sepsis decreased the intrinsic capacity of neutrophils to generate NETs and attenuated the levels of NETs in the lungs [51 ▪ ].…”

Section: Do Mirnas Regulate Cells Involved In Thrombo-inflammation?mentioning

confidence: 94%

microRNAs and thrombo-inflammation: relationship in sight

Águila,

González-Conejero,

Martínez

2024

Current Opinion in Hematology

View full text Add to dashboard Cite

Purpose of review Thrombo-inflammation is a multifaceted pathologic process involving various cells such as platelets, neutrophils, and monocytes. In recent years, microRNAs have been consistently implicated as regulators of these cells. Recent findings MicroRNAs play a regulatory role in several platelet receptors that have recently been identified as contributing to thrombo-inflammation and neutrophil extracellular trap (NET) formation. In addition, a growing body of evidence has shown that several intracellular and extracellular microRNAs directly promote NET formation. Summary Targeting microRNAs is a promising therapeutic approach to control thrombosis in patients with both infectious and noninfectious inflammatory diseases. Future research efforts should focus on elucidating the specific roles of microRNAs in thrombo-inflammation and translating these findings into tangible benefits for patients.

show abstract

MiR-155 regulates neutrophil extracellular trap formation and lung injury in abdominal sepsis

Cited by 19 publications

References 45 publications

Neutrophil extracellular trap inhibition improves survival in neonatal mouse infectious peritonitis

Neutrophil extracellular trap inhibition improves survival in neonatal mouse infectious peritonitis

Wenshen Yiqi Keli Mitigates the Proliferation and Migration of Cigarette Smoke Extract-Induced Human Airway Smooth Muscle Cells through miR-155/FoxO3a Axis

microRNAs and thrombo-inflammation: relationship in sight

Contact Info

Product

Resources

About