Publications by authors named "B Solhonne"

Individuals with impaired immune responses, such as ventilated and cystic fibrosis patients are often infected with () bacteria, and a co-infection with the virus (IAV) is often present. It has been known for many years that infection with IAV predisposes the host to secondary bacterial infections (such as or ), and there is an abundance of mechanistic studies, including those studying the role of desensitization of TLR signaling, type I IFN- mediated impairment of neutrophil chemokines and antimicrobial production, attenuation of IL1β production etc., showing this.

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Silver nanoparticles (AgNPs) are microbicidal agents which could be potentially used as an alternative to antivirals to treat human infectious diseases, especially influenza virus infections where antivirals have generally proven unsuccessful. However, concerns about the use of AgNPs on humans arise from their potential toxicity, although mechanisms are not well-understood. We show here, in the context of an influenza virus infection of lung epithelial cells, that AgNPs down-regulated influenza induced CCL-5 and -IFN-β release (two cytokines important in antiviral immunity) through RIG-I inhibition, while enhancing IL-8 production, a cytokine important for mobilizing host antibacterial responses.

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Idiopathic pulmonary fibrosis (IPF) is characterized by the deposition of excessive extracellular matrix and the destruction of lung parenchyma, resulting from an aberrant wound-healing response. Although IPF is often associated with an imbalance in protease activity, the mechanisms underlying the sustained repair mechanisms are not fully understood. Here, we addressed the role of the recently identified, membrane-anchored serine protease human airway trypsin-like protease (HAT).

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Article Synopsis
  • FGF9 is crucial for fetal lung development and is expressed in both epithelium and mesothelium, leading to research on its impact during pleural injury caused by adenoviruses.
  • In experiments, injecting an adenovirus with FGF9 into mice showed it could prevent harmful changes in pleura cells, such as thickening and fibrosis.
  • In lab tests, FGF9 inhibited mesothelial cell migration and reduced differentiation induced by another growth factor, suggesting it may have protective effects against fibrosis.
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According to the WHO, and despite reduction in mortality rates, there were an estimated 438 000 malaria deaths in 2015. Therefore new antimalarials capable of limiting organ damage are still required. We show that systemic and lung adenovirus (Ad)-mediated over-expression of trappin-2 (T-2) an antibacterial molecule with anti-inflammatory activity, increased mice survival following infection with the cerebral malaria-inducing Plasmodium berghei ANKA (PbANKA) strain.

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