Therapeutic targets of formononetin for treating prostate cancer at the single-cell level

Jiawei Li, Zhaoquan Huang, Ping Wang, Rong Li, Li Gao, Keng Po Lai

Research output: Contribution to journalArticlepeer-review

2 Citations (Scopus)

Abstract

Prostate cancer is one of the serious health problems of older male, about 13% of male was affected by prostate cancer. Prostate cancer is highly heterogeneity disease with complex molecular and genetic alterations. So, targeting the gene candidates in prostate cancer in single-cell level can be a promising approach for treating prostate cancer. In the present study, we analyzed the single cell sequencing data obtained from 2 previous reports to determine the differential gene expression of prostate cancer in single-cell level. By using the network pharmacology analysis, we identified the therapeutic targets of formononetin in immune cells and tissue cells of prostate cancer. We then applied molecular docking to determine the possible direct binding of formononetin to its target proteins. Our result identified a cluster of differential gene expression in prostate cancer which can serve as novel biomarkers such as immunoglobulin kappa C for prostate cancer prognosis. The result of network pharmacology delineated the roles of formononetin’s targets such CD74 and THBS1 in immune cells’ function of prostate cancer. Also, formononetin targeted insulin receptor and zinc-alpha-2-glycoprotein which play important roles in metabolisms of tissue cells of prostate cancer. The result of molecular docking suggested the direct binding of formononetin to its target proteins including INSR, TNF, and CXCR4. Finally, we validated our findings by using formononetin-treated human prostate cancer cell DU145. For the first time, our result suggested the use of formononetin for treating prostate cancer through targeting different cell types in a single-cell level.

Original languageEnglish
Pages (from-to)10380-10401
Number of pages22
JournalAging-us
Volume16
Issue number12
DOIs
Publication statusPublished - 2024
Externally publishedYes

Keywords

  • formononetin
  • heterogeneity
  • immune response
  • network pharmacology
  • prostate cancer
  • single cell
  • therapeutic targets

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