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N-琥珀酰壳聚糖-丝裂霉素C偶联物和羧甲基几丁质-丝裂霉素C偶联物的药代动力学特征及抗肿瘤活性

Pharmacokinetic characteristics and antitumor activity of the N-succinyl-chitosan-mitomycin C conjugate and the carboxymethyl-chitin-mitomycin C conjugate.

作者信息

Song Y, Onishi H, Nagai T

机构信息

Faculty of Pharmaceutical Sciences, Hoshi University, Tokyo, Japan.

出版信息

Biol Pharm Bull. 1993 Jan;16(1):48-54. doi: 10.1248/bpb.16.48.

Abstract

The conjugate between N-succinyl-chitosan (Suc-chitosan) and mitomycin C (MMC), named Suc-chitosan-MMC, and that between carboxymethyl-chitin (CM-chitin) and MMC, named CM-chitin-MMC, were investigated in vivo. As for the intraperitoneal drug administration using rats, the order of the maximum blood concentration of MMC was unconjugated MMC > CM-chitin-MMC > Suc-chitosan-MMC. The plasma concentration of MMC for Suc-chitosan-MMC was maintained at an almost constant level over 24 h. Pharmacokinetic analysis of each plasma concentration indicated that for each conjugate, the in vitro drug release reported previously was useful for the approximate estimation of the in vivo regeneration of MMC. The chemotherapeutic effect of MMC and the conjugates was investigated using mice bearing L1210 leukemia or B16 melanoma. Concerning antitumor activity against L1210 leukemia, the conjugates exhibited a marked effect at higher doses, and their effect increased even in the dose range where the effect of MMC decreased. MMC and the conjugates exhibited a good growth-inhibitory effect against B16 melanoma. Complete inhibition of growth of B16 melanoma was observed at the dose of 10 mg eq MMC/kg for CM-chitin-MMC.

摘要

研究了N-琥珀酰壳聚糖(Suc-壳聚糖)与丝裂霉素C(MMC)的缀合物(命名为Suc-壳聚糖-MMC)以及羧甲基几丁质(CM-几丁质)与MMC的缀合物(命名为CM-几丁质-MMC)的体内情况。对于使用大鼠进行腹腔内给药,MMC的最大血药浓度顺序为游离MMC>CM-几丁质-MMC>Suc-壳聚糖-MMC。Suc-壳聚糖-MMC的MMC血浆浓度在24小时内几乎维持在恒定水平。对每个血浆浓度进行药代动力学分析表明,对于每种缀合物,先前报道的体外药物释放情况有助于近似估算MMC在体内的再生情况。使用携带L1210白血病或B16黑色素瘤的小鼠研究了MMC及其缀合物的化疗效果。关于对L1210白血病的抗肿瘤活性,缀合物在较高剂量时表现出显著效果,甚至在MMC效果降低的剂量范围内其效果仍有所增加。MMC及其缀合物对B16黑色素瘤表现出良好的生长抑制作用。对于CM-几丁质-MMC,在剂量为10 mg当量MMC/kg时观察到B16黑色素瘤的生长被完全抑制。

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