BMC Cancer (Apr 2008)

CD24 cross-linking induces apoptosis in, and inhibits migration of, MCF-7 breast cancer cells

  • Bae Ji-Yeon,
  • Cho Jihyoung,
  • Lee Jong,
  • Kim Sangmin,
  • Shin Incheol,
  • Lee Kyung-Min,
  • Lee Jeong,
  • Han Wonshik,
  • Ko Eunyoung,
  • Kim Jong,
  • Jee Hyeon-Gun,
  • Noh Dong-Young

DOI
https://doi.org/10.1186/1471-2407-8-118
Journal volume & issue
Vol. 8, no. 1
p. 118

Abstract

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Abstract Background The biological effects of CD24 (FL-80) cross-linking on breast cancer cells have not yet been established. We examined the impact of CD24 cross-linking on human breast cancer cell line MCF-7. Methods MCF-7 and MDA-MB-231 cells were treated with anti-rabbit polyclonal IgG or anti-human CD24 rabbit polyclonal antibodies to induce cross-linking, and then growth was studied. Changes in cell characteristics such as cell cycle modulation, cell death, survival in three-dimensional cultures, adhesion, and migration ability were assayed after CD24 cross-linking in MCF-7. Results Expression of CD24 was analyzed by flow cytometry in MDA-MB-231 and MCF-7 cells where 2% and 66% expression frequencies were observed, respectively. CD24 cross-linking resulted in time-dependent proliferation reduction in MCF-7 cells, but no reduction in MDA-MB-231 cells. MCF-7 cell survival was reduced by 15% in three-dimensional culture after CD24 cross-linking. Increased MCF-7 cell apoptosis was observed after CD24 cross-linking, but no cell cycle arrest was observed in that condition. The migration capacity of MCF-7 cells was diminished by 30% after CD24 cross-linking. Conclusion Our results showed that CD24 cross-linking induced apoptosis and inhibited migration in MCF-7 breast cancer cells. We conclude that CD24 may be considered as a novel therapeutic target for breast cancer.