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异环磷酰胺立体异构体在大鼠体内乳腺癌模型中的疗效与毒性

Efficacy and toxicity of ifosfamide stereoisomers in an in vivo rat mammary carcinoma model.

作者信息

Wainer I W, Granvil C P, Wang T, Batist G

机构信息

Experimental Pharmacology Program, Lady Davis Institute for Medical Research, Jewish General Hospital, Montreal, Quebec, Canada.

出版信息

Cancer Res. 1994 Aug 15;54(16):4393-7.

PMID:8044787
Abstract

Ifosfamide (IFF) is a nitrogen mustard with significant activity against a number of tumors. Since it is a chiral molecule, it has been suggested that enantioselective metabolism could result in different efficacy and toxicity profiles for (R)- and (S)-ifosfamide. Both experimental animal and clinical data suggest that N-dechloroethyl metabolites of (S)-IFF are more significantly associated with neurological toxicity, which may limit therapeutic use of IFF. We have used purified ifosfamide enantiomers to examine the pharmacokinetics; spectrum of toxicity including lethality, weight loss, and myelosuppression; and antitumor effects of the mixture compared to each of the purified enantiomers. In the MatB mammary carcinoma grown in female Fischer rats we demonstrated that the antitumor efficacy appears to be the same for (R)-IFF and (S)-IFF, while the (R)-IFF has greater myelotoxicity. Pharmacokinetic analysis of plasma concentration-time confirms that the (R)-IFF is metabolized to a greater extent than (S)-IFF via the activation pathway. These data suggest that purified (R)-IFF may be an effective way to delivery active cytotoxic drug while limiting the generation of neurotoxic metabolites.

摘要

异环磷酰胺(IFF)是一种对多种肿瘤具有显著活性的氮芥。由于它是一种手性分子,有人提出对映体选择性代谢可能导致(R)-异环磷酰胺和(S)-异环磷酰胺具有不同的疗效和毒性特征。实验动物和临床数据均表明,(S)-IFF的N-去氯乙基代谢产物与神经毒性的关联更为显著,这可能会限制IFF的治疗应用。我们使用纯化的异环磷酰胺对映体来研究其药代动力学;包括致死率、体重减轻和骨髓抑制在内的毒性谱;以及与每种纯化对映体相比混合物的抗肿瘤作用。在雌性Fischer大鼠体内生长的MatB乳腺癌模型中,我们证明(R)-IFF和(S)-IFF的抗肿瘤疗效似乎相同,但(R)-IFF具有更大的骨髓毒性。血浆浓度-时间的药代动力学分析证实,(R)-IFF通过活化途径的代谢程度比(S)-IFF更大。这些数据表明,纯化的(R)-IFF可能是一种有效递送活性细胞毒性药物同时限制神经毒性代谢产物生成的方法。

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