effect of the inhibitor to membrane-bound enzyme on the growth of invasion of cancer cells

1995 Fiscal Year Final Research Report Summary

• Project/Area Number: 06671642
• Research Category: Grant-in-Aid for General Scientific Research (C)
• Allocation Type: Single-year Grants
• Research Field: Obstetrics and gynecology
• Research Institution: Nagoya University
• Principal Investigator: GOTO Setsuko Nagoya Univ., College of medical Technology, Professor, 医療技術短期大学部, 教授 (80111847)
• Co-Investigator(Kenkyū-buntansha): KATO Noriko Nagoya Univ., School of Med., Medical Staff (Senior Resident), 医学部, 医員 ; WAKAHARA Yasunori Nagoya Univ., School of Med., Medical Staff (Senior Resident), 医学部, 医員 ; SUZUKI Takanobu Nagoya Univ., School of Med., Medical Staff (Senior Resident), 医学部, 医員 ; INO Kazuhiko Nagoya Univ., School of Med., Medical Staff (Senior Resident), 医学部, 医員
• Project Period (FY): 1994 – 1995
• Keywords: Ubenimex (bestatin) / cell-growth suppression / aminopeptidase N / Monoclonal antibody / Immunoblotting / MTT assay / bestatin uptake / flow cytometry

Research Abstract

We previously found that ubenimex (bestatin), an aminopeptidase inhibitor, had a growth-suppressive effect on cancer cells. To clarify the mechanism of the growth-suppressive effect, we investigated the expression of aminopeptidase N (AP-N/CD13) on choriocarcinoma cells and other human tumor cells.
1) Two choriocarcinoma cell lines, NaUCC-4 and BeWo, had higher AP-N activity than other cell lines, as did the human myeloid leukemia cell line, IIL-60.2) These choriocarcinoma and leukemia cell lines with aboundunt AP-N activity showed much higher sensitivity to bestatin than the other cell lines. 3) By immunoblotting and immunocytochemical staining, AP-N was detected as an approximately 165-kDa protein and localized on the cell membrane in choriocarcinoma cells. 4) We examined the effects of three anti-CD13 monoclonal antibodies (WM15, MCS2, and MY7) on the growth of NaUCC-4 cells. Of the three MABs, only WM15, which is able to inhibit AP-N activity, suppressed cell growth in a dose-dependent manner.
These results indicate that AP-N inhibitors show a growth-suppressive effect, presumably through inhibition of the enzyme activity of AP-N on carcinoma cells.
5) we examined bestatin uptake using 3H-bestatin in choriocarcinoma cells and other cells. A higher upake of 3H-bestatin was resulted in NaUCC-4 cells, which showed the highest sensitivity bestatin. 6) In DNA histogram, NaUCC-4 cells treated with bestatin were not blocked at any cell-cycle phases as studied by flow fluorocytometry.

Research Products

• [Publications] Kazuhiko Ino: "Experssion of Aminopeptidase N on Human Choriocarcinoma Cells and Cell Growth Supression by the Inhibition of Aminopeptidase N Activity" Jpn.J.Cancer Res.85. 927-933 (1994)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] Kazuhiko Ino, Setsuko Goto, Tomomitu Okamoto, Seiji Nomura, Akihiro Nawa, Ken-ichi Isobe, Shigehiko Mizutani, Yutaka Tomoda.: "Expression of Aminopeptidase N on Human Choriocarcinoma Cells and Cell Growth Suppression by the Inhibition of Aminopeptidase N Activity" Japanese Journal of Cancer Research. 85. 927-933 (1994)
  • Description: 「研究成果報告書概要(欧文)」より