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Potential molecular metabolic mechanisms underlying the effects of cimifugin in gastric cancer through single-cell and bulk RNA sequencing combined with network pharmacology.

Ziming ZhuYinbiao ZhangXinyue ZhangQiaoling ChenShanneng TangXuan ZhouXiao LiJieying WenYang BaiTao Zhang
Published in: Journal of gastrointestinal oncology (2024)
We verified the pharmacological effects of cimifugin on GC cell proliferation, invasion, and migration. AKR1C2, MAOB, and PDE2A were identified as the key targets of cimifugin in GC-related metabolic reprogramming and pathogenesis. Our research provides preliminary insights into the potential therapeutic effects of cimifugin, which could be considered for future exploration in the context of GC treatment.
Keyphrases
  • single cell
  • cell proliferation
  • rna seq
  • gas chromatography
  • human health
  • high throughput
  • cell cycle
  • cell migration
  • mass spectrometry
  • risk assessment
  • high resolution
  • climate change