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磷酸雌莫司汀(癌腺治)在前列腺癌患者中的药代动力学。

Pharmacokinetics of estramustine phosphate (Estracyt) in prostatic cancer patients.

作者信息

Gunnarsson P O, Andersson S B, Johansson S A, Nilsson T, Plym-Forshell G

出版信息

Eur J Clin Pharmacol. 1984;26(1):113-9. doi: 10.1007/BF00546718.

Abstract

The pharmacokinetics of estramustine phosphate (EMP) was studied in five prostatic cancer patients given single i.v. and oral doses of EMP in a cross-over study. Plasma and urinary concentrations of parent drug, estramustine, estromustine (the estrone analogue), estradiol and estrone were followed by 32 h. The elimination of intravenous EMP from plasma was biphasic. The mean volumes of distribution were small, being 43 and 108 ml/kg for the central and peripheral compartments, respectively. The plasma clearance was 64 ml/kg/h, and the half-lives of the two phases were 0.16 and 1.27 h. Metabolism was the major route of elimination of EMP. It was readily dephosphorylated and oxidized to yield the cytotoxic metabolites estramustine and estromustine. Estromustine was the main metabolite in plasma. When given orally EMP underwent extensive presystemic dephosphorylation, which started in the gastrointestinal tract. The relative bioavailability of estromustine after administration of EMP-capsules was 44%, which reflects incomplete absorption of EMP rather than first-pass metabolism of estromustine. The terminal half-life of estromustine was 10-20 h, which suggests that EMP might be given once or twice a day.

摘要

在一项交叉研究中,对5例前列腺癌患者给予单剂量静脉注射和口服磷酸雌莫司汀(EMP)后,研究了其药代动力学。在32小时内监测母体药物、雌莫司汀、雌二醇氮芥(雌酮类似物)、雌二醇和雌酮的血浆及尿液浓度。静脉注射EMP后,其从血浆中的消除呈双相。分布容积均值较小,中央室和外周室分别为43和108 ml/kg。血浆清除率为64 ml/kg/h,两个相的半衰期分别为0.16和1.27小时。代谢是EMP消除的主要途径。它很容易去磷酸化并氧化生成细胞毒性代谢产物雌莫司汀和雌二醇氮芥。雌二醇氮芥是血浆中的主要代谢产物。口服EMP时,在胃肠道开始进行广泛的首过前体去磷酸化。服用EMP胶囊后,雌二醇氮芥的相对生物利用度为44%,这反映了EMP吸收不完全,而非雌二醇氮芥的首过代谢。雌二醇氮芥的终末半衰期为10 - 20小时,这表明EMP可能每天给药一次或两次。

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