| Literature DB >> 30317566 |
Anna Lewinska1, Aleksandra Bocian2, Vladimir Petrilla3,4, Jagoda Adamczyk-Grochala1, Karolina Szymura1, Wiktoria Hendzel1, Edyta Kaleniuk5, Konrad K Hus2, Monika Petrillova6, Maciej Wnuk5.
Abstract
Snake venoms are widely studied in terms of their systemic toxicity and proteolytic, hemotoxic, neurotoxic, and cytotoxic activities. However, little is known about snake-venom-mediated effects when used at low, noncytotoxic concentrations. In the current study, two human fibroblast cell lines of different origin, namely WI-38 fetal lung fibroblasts and BJ foreskin fibroblasts were used to investigate snake-venom-induced adaptive response at a relatively noncytotoxic concentration (0.01 µg/ml). The venoms of Indochinese spitting cobra ( Naja siamensis), western green mamba ( Dendroaspis viridis), forest cobra ( Naja melanoleuca), and southern copperhead ( Agkistrodon contortrix) were considered. Snake venoms promoted FOXO3a-mediated oxidative stress response and to a lesser extent DNA damage response, which lead to changes in cell cycle regulators both at messenger RNA and protein levels, limited cell proliferation and migration, and induced cellular senescence. Taken together, we have shown for the first time that selected snake venoms may also exert adverse effects when used at relatively noncytotoxic concentrations.Entities:
Keywords: cellular senescence; fibroblasts; oxidative stress and DNA damage response (DDR); proliferation; snake venoms
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Year: 2018 PMID: 30317566 DOI: 10.1002/jcp.27382
Source DB: PubMed Journal: J Cell Physiol ISSN: 0021-9541 Impact factor: 6.384