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Basic Sciences

Host-mediated Therapeutic Effects Produced by Appropriately Timed Administration of Bleomycin on a Rat Fibrosarcoma

Kiyoshi Morikawa, Masuo Hosokawa, Jun-ichi Hamada, Michio Sugawara and Hiroshi Kobayashi
Kiyoshi Morikawa
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Masuo Hosokawa
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Jun-ichi Hamada
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Michio Sugawara
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Hiroshi Kobayashi
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DOI:  Published April 1985
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Abstract

The timing of bleomycin (BLM) administration after KMT-17 tumor inoculation was found to be important for optimizing its therapeutic effect on tumor-bearing rats. A remarkable therapeutic effect was observed when BLM (5 mg/kg/day) was administered i.p. for 5 days from the eighth day after tumor inoculation (Day 8 to Day 12) rather than when BLM was administered i.p. for 5 days during the days immediately following tumor inoculation (Day 1 and Day 5)(cured rats/treated rats: 10/21 and 2/16, respectively). By means of a Winn assay, stronger tumor-neutralizing activities were observed in spleen cells from BLM (Day 8 to Day 12)-treated tumor-bearing rats than were observed in spleen cells from BLM (Day 1 to Day 5)-treated tumor-bearing rats (% Inhibition: 70.9 and 49.3%, respectively). These therapeutic effects were thus found to be consistent with the antitumor immunity against KMT-17. The enhanced tumor-neutralizing activities of spleen cells from BLM-treated tumor-bearing rats were suppressed by adding spleen cells from nontreated tumor-bearing rats. In cell transfer experiments, an antitumor transplantation resistance in rats immunized with irradiated KMT-17 cells was abrogated by an adoptive transfer of spleen cells from untreated tumor-bearing rats or BLM (Day 1 to Day 5)-treated tumor-bearing rats but not from BLM (Day 8 to Day 12)-treated tumor-bearing rats. These results suggest that, when BLM is administered during a late stage of tumor growth, it is effective in eliminating suppressor cells and that this leads to an improvement in the therapeutic effects of the drug.

Footnotes

  • ↵1 Supported in part by a Grant-in-Aid for Cancer Research from the Japanese Ministry of Education, Science, and Culture, and by a grant from the Japanese Foundation for Multidisciplinary Treatment of Cancer, Tokyo, Japan.

  • ↵2 To whom requests for reprints should be addressed.

  • Received April 24, 1984.
  • Revision received December 6, 1984.
  • Accepted December 27, 1984.
  • ©1985 American Association for Cancer Research.
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April 1985
Volume 45, Issue 4
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Host-mediated Therapeutic Effects Produced by Appropriately Timed Administration of Bleomycin on a Rat Fibrosarcoma
Kiyoshi Morikawa, Masuo Hosokawa, Jun-ichi Hamada, Michio Sugawara and Hiroshi Kobayashi
Cancer Res April 1 1985 (45) (4) 1502-1506;

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Host-mediated Therapeutic Effects Produced by Appropriately Timed Administration of Bleomycin on a Rat Fibrosarcoma
Kiyoshi Morikawa, Masuo Hosokawa, Jun-ichi Hamada, Michio Sugawara and Hiroshi Kobayashi
Cancer Res April 1 1985 (45) (4) 1502-1506;
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