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33P 标记的抗人免疫缺陷病毒寡核苷酸(AR177)在大鼠单次和多次静脉给药后的药代动力学及分布情况。

Pharmacokinetics and distribution of a 33P-labeled anti-human immunodeficiency virus oligonucleotide (AR177) after single- and multiple-dose intravenous administration to rats.

作者信息

Wallace T L, Bazemore S A, Holm K, Markham P M, Shea J P, Chaudhary N, Cossum P A

机构信息

Aronex Pharmaceuticals, Inc., The Woodlands, Texas 77381, USA.

出版信息

J Pharmacol Exp Ther. 1997 Mar;280(3):1480-8.

PMID:9067338
Abstract

AR177 is a 17-mer oligonucleotide that has anti-human immunodeficiency virus activity in vitro. The disposition of internally labeled 33P-AR177 was studied after the tail vein injection of single and multiple doses (0.7 mg/kg) to rats. After a single dose, the terminal half-life of AR177 in the blood and plasma was 367 and 271 hr, respectively, significantly longer than values reported for other oligonucleotides. Analysis of the AR177 tissue distribution showed that the majority of the dose was distributed to the liver (40%), bone marrow (17%) and renal cortex (15%) at 8 hr after single dosing. Analysis of the AR177 concentrations in tissues showed that the highest concentrations were achieved in the renal cortex (15.0 microg-eq/g), liver (7.4 microg-eq/g), bone marrow (3.9 microg-eq/g), mesenteric lymph node (3.0 microg-eq/g) and spleen (2.4 microg-eq/g) at 8 hr after single dosing. The half-life in these tissues was 9.6, 7.7, 36.8, 10.0 and 30.8 days, respectively. Forty-eight hours after the last of seven i.v. doses given every other day, the concentrations in tissues were as follows: renal cortex, 39.9 microg-eq/g; liver, 33.9 microg-eq/g; bone marrow, 12.7 microg-eq/g; spleen, 9.3 microg-eq/g; mesenteric lymph node, 5.1 microg-eq/g. Twenty-one days after administration of the last dose, tissue concentrations were still high, as follows: renal cortex, 18.6 microg-eq/g; liver, 6.2 microg-eq/g; bone marrow, 12.5 microg-eq/g; mesenteric lymph node, 3.9 microg-eq/g; spleen, 8.1 microg-eq/g. There was low urinary and fecal excretion (urinary excretion of 12.8% and fecal excretion of 6.0% of the total dose over 21 days) after a single dose. Gel filtration and anion-exchange high-performance liquid chromatography and electrophoretic analysis of the radioactivity in tissues indicated that >90% of the radioactivity represented intact AR177 for at least 7 days after drug dosing. These results demonstrate that AR177 has an extended plasma, blood and tissue half-life, is widely distributed and achieves high concentrations in lymphoid and nonlymphoid tissues in rats.

摘要

AR177是一种17聚体寡核苷酸,在体外具有抗人类免疫缺陷病毒活性。在对大鼠单次和多次(0.7mg/kg)尾静脉注射后,研究了内部标记的33P-AR177的处置情况。单次给药后,AR177在血液和血浆中的末端半衰期分别为367小时和271小时,显著长于其他寡核苷酸报道的值。AR177组织分布分析表明,单次给药后8小时,大部分剂量分布于肝脏(40%)、骨髓(17%)和肾皮质(15%)。组织中AR177浓度分析表明,单次给药后8小时,肾皮质(15.0微克当量/克)、肝脏(7.4微克当量/克)、骨髓(3.9微克当量/克)、肠系膜淋巴结(3.0微克当量/克)和脾脏(2.4微克当量/克)达到最高浓度。这些组织中的半衰期分别为9.6天、7.7天、36.8天、10.0天和30.8天。在每隔一天静脉注射七次给药的最后一次给药后48小时,组织中的浓度如下:肾皮质,39.9微克当量/克;肝脏,33.9微克当量/克;骨髓,12.7微克当量/克;脾脏,9.3微克当量/克;肠系膜淋巴结,5.1微克当量/克。在最后一次给药后21天,组织浓度仍然很高,如下:肾皮质,18.6微克当量/克;肝脏,6.2微克当量/克;骨髓,12.5微克当量/克;肠系膜淋巴结,3.9微克当量/克;脾脏,8.1微克当量/克。单次给药后,尿液和粪便排泄量较低(21天内尿液排泄占总剂量的12.8%,粪便排泄占6.0%)。组织中放射性的凝胶过滤、阴离子交换高效液相色谱和电泳分析表明,给药后至少7天,>90%的放射性代表完整的AR177。这些结果表明,AR177在大鼠体内具有延长的血浆、血液和组织半衰期,分布广泛,并在淋巴组织和非淋巴组织中达到高浓度。

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