首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >3'-azido-3'-deoxythymidine (AZT) transplacental perfusion kinetics and DNA incorporation in normal human placentas perfused with AZT
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3'-azido-3'-deoxythymidine (AZT) transplacental perfusion kinetics and DNA incorporation in normal human placentas perfused with AZT

机译:3'-azido-3'-deoxythymidine(AZT)经胎盘灌注动力学和DNA掺入正常人胎盘中的AZT

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摘要

Vertical transmission of the human immunodeficiency virus 1 (HIV-1) is reduced from similar to 25% to similar to 7% as a result of 3'-azido-3'-deoxythymidine (AZT) therapy given during pregnancy; however, the consequences of transplacental AZT exposure to the fetus remain unknown. To address the extent and kinetics of AZT transfer across the human placenta, perfusion studies have been performed with fresh uninfected human placentas perfused with 0.5, 1.0 and 5.0 mg AZT/ml for 2 h using a dual recirculating single cotyledon perfusion apparatus [T.I. Ala-Kokko, P. Pienimaki, R. Herva, A.I. Hollmen, O. Pelkonen, K. V a h a kangas, Transfer of lidocaine and bupivacaine across the isolated perfused human placenta, Pharmacol. Toxicol. 77 (1995) 142-148]. For two placentas, samples of perfusion effluent were taken every 15 min from the maternal and fetal sides of the apparatus and AZT levels were determined by AZT radioimmunoassay (RIA). At the end of the perfusion, AZT-DNA incorporation into placental DNA was determined by AZT-RIA. The concentration of AZT in the fetal perfusate increased with time, along with a concomitant slow decrease in the concentration of AZT in the maternal perfusates. For three different placentas, at 2 h after the start of perfusion, AZT-DNA incorporation values (molecules of AZT/10 super(6) nucleotides) were 11.8 for the 0.5 mg AZT/ml perfusate, 13.7 for the 1.0 mg AZT/ml perfusion, and 42.0 for the 5 mg AZT/ml perfusion. An additional placenta perfused with 1 mg AZT/ml did not have detectable values of AZT incorporated into DNA (data not shown). The data show that AZT crosses the human placenta and becomes rapidly incorporated into DNA of placental tissue in a dose-dependent fashion, suggesting that even short exposures to this drug might induce fetal genotoxicity and might also inhibit maternal-fetal viral transmission.
机译:由于怀孕期间进行3'-叠氮基3'-脱氧胸苷(AZT)治疗,人类免疫缺陷病毒1(HIV-1)的垂直传播从相似的25%降低到相似的7%;然而,经胎盘AZT暴露于胎儿的后果仍然未知。为了解决AZT在整个人胎盘上转移的程度和动力学问题,已经使用双循环单子叶灌注设备对新鲜未感染的人胎盘分别灌注0.5、1.0和5.0 mg AZT / ml进行了2小时的灌注研究。 Ala-Kokko,P.Pienimaki,R.Herva,A.I。 Hollmen,O。Pelkonen,K。V a kangas,利多卡因和布比卡因在分离的灌注人胎盘Pharmacol中的转移。毒药。 77(1995)142-148]。对于两个胎盘,每15分钟从设备的母胎和胎侧取一次灌注液样品,并通过AZT放射免疫测定(RIA)测定AZT水平。在灌注结束时,通过AZT-RIA确定AZT-DNA掺入胎盘DNA中。胎儿灌洗液中AZT的浓度随时间增加,而孕产妇灌洗液中AZT的浓度随之缓慢降低。对于三种不同的胎盘,灌注开始后2小时,0.5 mg AZT / ml灌注液的AZT-DNA掺入值(AZT / 10 super(6)核苷酸分子)为11.8,1.0 mg AZT / ml的为13.7。灌注,对于5 mg AZT / ml灌注为42.0。灌注了1 mg AZT / ml的其他胎盘没有掺入DNA的可检测到的AZT值(数据未显示)。数据显示,AZT可以穿越人类胎盘,并以剂量​​依赖的方式迅速整合到胎盘组织的DNA中,这表明即使短时间接触该药物也可能引起胎儿遗传毒性,也可能抑制母体-胎儿的病毒传播。

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