Cell cycle arrest and apoptosis induced by SART-1 gene transduction.

نویسندگان

  • Mami Hosokawa
  • Ritsuko Kadota
  • Shigeki Shichijo
  • Kyogo Itoh
  • Igor Dmitriev
  • Victor Krasnykh
  • David T Curiel
  • Yoichi Takue
  • Hiro Wakasugi
  • Shigemitsu Takashima
  • Yuji Heike
چکیده

UNLABELLED The biological function of the SART-1 gene product is demonstrated and its potential as a target for cancer gene therapy is discussed. MATERIALS AND METHODS The SART-1 gene was transduced by a recombinant adenovirus vector and its expression was promoted by a CMV promoter. RESULTS The transduction efficiency by recombinant adenoviruses in A549 and MCF-7 cells was determined using a vector expressing luciferase, which showed high expression in the cells. Cell count analysis using Trypan-Blue dye exclusion showed that SART-1 gene transduction inhibited cell growth. Flow cytometry analysis suggested that SART-1 gene transduction induced cell cycle arrest followed by apoptosis. Western blot analysis confirmed that the apoptosis pathway was activated by SART-1 gene transduction. CONCLUSION These results show that SART-1 gene transduction induces cell cycle arrest leading to apoptosis and suggest the possibility of gene therapy against cancer. In addition, SART-1 is known to be a tumor antigen in a range of cancers recognized by T cells, thus a potential strategy would be the combination of suicide gene therapy with immuno-gene therapy.

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عنوان ژورنال:
  • Anticancer research

دوره 25 3B  شماره 

صفحات  -

تاریخ انتشار 2005