Effect of Mitomycin-C on Rabbit Conjunctival Fibroblast Proliferation and Apoptosis

마이토마이신이 가토 결막섬유아세포의 증식 및 사멸에 미치는 효과

  • Kwon Young-Sam (School of Veterinary Medicine, University of Wisconsin-Madison) ;
  • Jang Kwang-Ho (College of Veterinary Medicine, Kyungpook National University)
  • 권영삼 (위스콘신-매디슨 대학교 수의과대학) ;
  • 장광호 (경북대학교 수의과대학)
  • Published : 2006.06.01

Abstract

The purpose of this study was to determine the effects of mitomycin C on conjunctival fibroblast proliferation and apoptosis. Rabbit conjunctival fibroblast mono layers were treated with 48 hours application of mitomycin-C. The viability of cells was evauated by MTT assay. To examine the effect of mitomycin-C on the cell proliferation, immunocytochemistry for BrdU staning was performed. Then, we investigated whether mitomycin-C induced cell's apoptosis by TUNEL staining. As a result of MTT assay, the viability of cells was gradually inhibited in a dose dependent manner by mitomycin-C. The BrdU staining showed that mitomycin-C significantly suppressed the proliferation of conjunctival fibroblast at concentrations of 0.02% or more. When TUNEL assays were performed, the number of apoptotic cells increased 5.6-, 18.5-, and 33.8-fold compared with the control at 0.01, 0.02, and 0.04%, respectively, of mitomycin-C at 48 hours of exposure. Therefore, mitomycin-C may be useful as a regulator in the treatment of corneal diseases that manifest with scar formation and tumor of fibroblast expansion.

Keywords

References

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