Viruses (Apr 2024)

ML241 Antagonizes ERK 1/2 Activation and Inhibits Rotavirus Proliferation

  • Jinlan Wang,
  • Xiaoqing Hu,
  • Jinyuan Wu,
  • Xiaochen Lin,
  • Rong Chen,
  • Chenxing Lu,
  • Xiaopeng Song,
  • Qingmei Leng,
  • Yan Li,
  • Xiangjing Kuang,
  • Jinmei Li,
  • Lida Yao,
  • Xianqiong Tang,
  • Jun Ye,
  • Guangming Zhang,
  • Maosheng Sun,
  • Yan Zhou,
  • Hongjun Li

DOI
https://doi.org/10.3390/v16040623
Journal volume & issue
Vol. 16, no. 4
p. 623

Abstract

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Rotavirus (RV) is the main pathogen that causes severe diarrhea in infants and children under 5 years of age. No specific antiviral therapies or licensed anti-rotavirus drugs are available. It is crucial to develop effective and low-toxicity anti-rotavirus small-molecule drugs that act on novel host targets. In this study, a new anti-rotavirus compound was selected by ELISA, and cell activity was detected from 453 small-molecule compounds. The anti-RV effects and underlying mechanisms of the screened compounds were explored. In vitro experimental results showed that the small-molecule compound ML241 has a good effect on inhibiting rotavirus proliferation and has low cytotoxicity during the virus adsorption, cell entry, and replication stages. In addition to its in vitro effects, ML241 also exerted anti-RV effects in a suckling mouse model. Transcriptome sequencing was performed after adding ML241 to cells infected with RV. The results showed that ML241 inhibited the phosphorylation of ERK1/2 in the MAPK signaling pathway, thereby inhibiting IκBα, activating the NF-κB signaling pathway, and playing an anti-RV role. These results provide an experimental basis for specific anti-RV small-molecule compounds or compound combinations, which is beneficial for the development of anti-RV drugs.

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