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去氧精胍菌素的骨髓保护活性:对小鼠脾集落形成细胞损伤的影响及与丝裂霉素C抗肿瘤活性的关系

Myeloprotective activity of deoxyspergualin: influence on splenic colony-forming cell injury and antitumor activity of mitomycin C in mice.

作者信息

Nemoto K, Sugawara Y, Ogino M, Mae T, Abe F, Takeuchi T

机构信息

Research Laboratories, Pharmaceuticals Group, Nippon Kayaku Co., Ltd., Tokyo.

出版信息

Jpn J Cancer Res. 1992 Jul;83(7):789-93. doi: 10.1111/j.1349-7006.1992.tb01981.x.

Abstract

We have examined the efficacy of deoxyspergualin (DSG) in protecting splenic colony-forming cells (CFU-S) from mitomycin C (MMC)-induced damage. The main findings of the study are as follows. (1) When DSG was administered at doses of 1.5 and 3 mg/kg for 7 days before the MMC injection, the decrease of the femoral CFU-S caused by MMC was diminished on the day after the MMC injection. The optimal dose was found to be 3 mg/kg. (2) In animals receiving 3 mg/kg DSG for at least 3 days preceding the MMC injection, the femoral CFU-S was more than 200% of that in the MMC alone group one day after the MMC injection. (3) The number of femoral CFU-S in the mice which received 3 mg/kg DSG for 3 days prior to MMC was significantly restored day by day and reached 70% of normal at 5 days after the MMC injection, while it was only 13% of normal in the MMC alone group. Moreover, the prior DSG administration significantly diminished the MMC toxicity to circulating platelets. (4) DSG administration (3 mg/kg) 3 days prior to MMC did not weaken the antitumor activity against colon 26 adenocarcinoma or P388 leukemia when compared with MMC alone. These findings have shown the ability of DSG specifically to protect the animals against bone marrow toxicity caused by MMC without interfering with the antitumor activity.

摘要

我们已经研究了去氧精胍菌素(DSG)在保护脾集落形成细胞(CFU-S)免受丝裂霉素C(MMC)诱导损伤方面的功效。该研究的主要发现如下。(1)在注射MMC前7天,以1.5和3mg/kg的剂量给予DSG,MMC注射后一天,MMC导致的股骨CFU-S减少量有所减轻。发现最佳剂量为3mg/kg。(2)在MMC注射前至少3天接受3mg/kg DSG的动物中,MMC注射后一天,股骨CFU-S是仅接受MMC组的200%以上。(3)在MMC注射前3天接受3mg/kg DSG的小鼠中,股骨CFU-S的数量逐日显著恢复,在MMC注射后5天达到正常水平的70%,而仅接受MMC组仅为正常水平的13%。此外,预先给予DSG可显著降低MMC对循环血小板的毒性。(4)与单独使用MMC相比,在MMC注射前3天给予DSG(3mg/kg)不会削弱对结肠26腺癌或P388白血病的抗肿瘤活性。这些发现表明DSG能够特异性地保护动物免受MMC引起的骨髓毒性,而不干扰抗肿瘤活性。

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