Mechanisms of the growth inhibitory effects of the isoflavonoid biochanin A on LNCaP cells and xenografts

Lori Rice, Von G. Samedi, Theresa A. Medrano, Carol A. Sweeney, Henry V. Baker, Anne Stenstrom, Jaime Furman, Kathleen T. Shiverick

Resultado de la investigación: Articlerevisión exhaustiva

61 Citas (Scopus)

Resumen

BACKGROUND. Isoflavones inhibit the growth of some types of tumor cells, including prostate adenocarcinoma. This study used LNCaP cells and xenografts to investigate the mechanisms of the antiproliferative effects of biochanin A, a major isoflavone present in red clover but not soy-derived products. METHODS. LNCaP cells were exposed to varying doses of biochanin A to evaluate viability, DNA synthesis, and DNA fragmentation (TUNEL) analysis. Regulation of gene expression was determined by using Western immunoblotting and cDNA microarrays. Anti-tumorigenic effects were evaluated by using athymic mice with LNCaP flank tumors. RESULTS. Biochanin A induced a dose-dependent inhibition of proliferation and [3H]thymidine incorporation that correlated with increased DNA fragmentation, indicative of apoptosis. Western blot analyses of cell cycle regulatory proteins revealed that biochanin A significantly decreased expression of cyclin B and p21, whereas flow cytometry showed that cells were accumulating in the G0/G1 phase. cDNA microarray analyses identified 29 down-regulated genes with six reduced below assay detection limits. Eleven genes were up-regulated, including 9 that were undetectable in controls. In mice with LNCaP xenografts, biochanin A significantly reduced tumor size and incidence. CONCLUSION. These results indicate that biochanin A inhibits prostate cancer cell growth through induction of cell cycle arrest and apoptosis. Biochanin A-regulated genes suggest multiple pathways of action. Biochanin A inhibits the incidence and growth of LNCaP xenograft tumors in athymic mice.

Idioma originalEnglish (US)
Páginas (desde-hasta)201-212
Número de páginas12
PublicaciónProstate
Volumen52
N.º3
DOI
EstadoPublished - ago 1 2002
Publicado de forma externa

ASJC Scopus subject areas

  • Oncology
  • Urology

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