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一种新型抗肿瘤半合成醚磷脂,即14C标记的浆膜酰基-(N-酰基)乙醇胺,在患有肉瘤Mc11的小鼠体内的药代动力学和代谢情况。

Pharmacokinetics and metabolism of a new antitumor semisynthetic ether phospholipid, 14C-labeled plasmanyl-(N-acyl)ethanolamine, in mice bearing sarcoma Mc11.

作者信息

Kára J, Zimakova N I, Serebryakova E A, Dĕdková V, Zolotaryov A E

机构信息

Laboratory of Evolutionary Biology, Czech Academy of Sciences Prague 4.

出版信息

J Cancer Res Clin Oncol. 1994;120(11):662-7. doi: 10.1007/BF01245378.

Abstract

New natural and semisynthetic antitumor ether phospholipids PNAE and PNAE(s) [plasmanyl-(N-acyl)ethanolamines] and their selective antitumor activity in vivo have been described previously. We are now presenting the pharmacokinetics, in vivo metabolism and distribution of a [14C]PNAE(s) preparation (1-O-octadecyl-2-oleoyl-sn-glycero-3-phospho-(N-[U-14C]palmitoyl) ethanolamine in the intact or Mc11-tumor-bearing BDF1 mice. Only partial degradation (about 50%-60%) of [14C]PNAE(s) was observed in vivo 24 h after i.v. administration, as detected by TLC analysis of phospholipids extracted from the blood, liver, tumor and brain of animals. Pharmacokinetic curves of [14C]PNAE(s) and its metabolites were fitted with a two-compartment model (t alpha 1/2 = 2.5 h, t beta 1/2 = 61.6 h). After repeated i.v. doses of [14C]PNAE(s) (administered on days 1, 2, 3, 4, and 5) accumulation of [14C]PNAE(s) and lyso-[14C]PNAE(s) in tumor tissue was detected. High levels of [14C]PNAE(s) were also detected in the liver, lung and spleen of animals. After i.v. administration of [14C]PNAE(s) the ether phospholipid was also detected in the brain tissue. The parmacokinetic data indicate that repeated parenteral doses of PNAE(s) are necessary to attain therapeutic concentrations in tumor tissue. The very high accumulation of [14C]PNAE(s) in the liver of animals after repeated i.v. doses, and the absence of toxic side-effects in vivo indicate a possible clinical therapeutic use of PNAE(s), especially in the treatment of tumor metastases in liver as well as in the prophylaxis of liver metastases after surgical removal of primary tumors.

摘要

新型天然和半合成抗肿瘤醚磷脂PNAE和PNAE(s) [质酰基-(N-酰基)乙醇胺]及其在体内的选择性抗肿瘤活性此前已有报道。我们现在展示一种[14C]PNAE(s)制剂(1-O-十八烷基-2-油酰基-sn-甘油-3-磷酸-(N-[U-14C]棕榈酰)乙醇胺)在完整或携带Mc11肿瘤的BDF1小鼠体内的药代动力学、体内代谢和分布情况。静脉注射后24小时,通过对从动物血液、肝脏、肿瘤和脑组织中提取的磷脂进行薄层色谱分析检测到,体内仅观察到[14C]PNAE(s)的部分降解(约50%-60%)。[14C]PNAE(s)及其代谢产物的药代动力学曲线用二室模型拟合(tα1/2 = 2.5小时,tβ1/2 = 61.6小时)。在重复静脉注射[14C]PNAE(s)(在第1、2、3、4和5天给药)后,检测到肿瘤组织中[14C]PNAE(s)和溶血-[14C]PNAE(s)的蓄积。在动物的肝脏、肺和脾脏中也检测到高水平的[14C]PNAE(s)。静脉注射[14C]PNAE(s)后,在脑组织中也检测到了醚磷脂。药代动力学数据表明,需要重复肠胃外给药PNAE(s)才能在肿瘤组织中达到治疗浓度。重复静脉注射后,动物肝脏中[14C]PNAE(s)的极高蓄积以及体内无毒性副作用表明PNAE(s)可能具有临床治疗用途,特别是在治疗肝脏肿瘤转移以及在手术切除原发性肿瘤后预防肝脏转移方面。

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