AI Article Synopsis

  • Animal models are commonly used for toxicity studies, but there's a growing demand for in vitro methods, leading to a focus on EGR1 expression changes during toxic injuries in drug discovery.
  • In experiments, EGR1 mRNA and protein levels increased in the liver, kidney, and corneal cells after exposure to certain irritants, confirming injury-related EGR1 induction in both in vivo and in vitro studies.
  • This study suggests that EGR1 could serve as a valuable biomarker in a promoter-luciferase gene reporter system, enhancing the accuracy of predicting ocular irritation in future toxicity assessments.

Article Abstract

Animal models are used for preclinical toxicity studies, and the need for in vitro alternative methods has been strongly raised. Our study aims to elucidate the potential mechanism of change in EGR1 expression under situations of toxic injury and to develop an promoter-luciferase gene reporter assay for an in vitro alternative method for toxicity prediction in drug discovery. We first found an increase in early growth response-1 (EGR1) mRNA/protein expressions in the liver and kidney of cisplatin-treated injured rats. Additionally, the EGR1 protein level was also elevated under situations of ocular injury after sodium lauryl sulfate (SLS) eye drops. These in vivo observations on injury-related EGR1 induction were confirmed by in vitro studies, where human corneal epithelial cells were treated with representative irritants (SLS and benzalkonium chloride) and 17 chemicals having different UN GHS irritant categories. Additionally, our results suggest the involvement of ERK, JNK, p38 MAPK pathways in EGR1 elevation in response to gamma-butyrolactone-induced injury. As EGR1 is considered to be a pivotal factor in proliferation and regeneration, siRNA-mediated knockdown of promoted cytotoxic potential through a delay of injury-related recovery. More importantly, the elevation of promoter activities was observed by various irritants in cells transfected with promoter-reporter vector. In conclusion, can be a potential biomarker in a promoter-reporter system to improve the accuracy of in vitro predictions for ocular irritation.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8537669PMC
http://dx.doi.org/10.3390/pharmaceutics13101584DOI Listing

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