In vivo dilatation of the fetal and postnatal ductus arteriosus by inhibition of phosphodiesterase 3 in rats.

Biology of the neonate Pub Date : 2006-01-01 Epub Date: 2005-11-24 DOI:10.1159/000089954
Katsuaki Toyoshima, Kazuo Momma, Shinichiro Imamura, Toshio Nakanishi
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引用次数: 27

Abstract

Background: Clinically, it appears that phosphodiesterase 3 (PDE 3) inhibitors, which are used for acute cardiac failure in premature infants, dilate the ductus arteriosus (DA).

Objectives: To clarify the ductus-dilating effects of PDE 3 inhibitors in near-term rat pups and their differential effects in near-term and preterm fetal rats, in in vivo studies.

Methods: The in vivo ductal diameter of rat pups and fetuses was measured using a rapid whole-body freezing method, by cutting on a freezing microtome and measuring with a microscope and micrometer. Eight to twenty pups and fetuses were studied in each group. Milrinone and amrinone (specific inhibitors of PDE 3) were injected into 1-hour-old pups and the DA was studied 0.5 and 1 h later. The differential effects of these PDE 3 inhibitors on the near-term and preterm ductus were studied by injecting indomethacin (10 mg/kg) and PDE 3 inhibitors into 21D (21st day of pregnancy: term-21.5 days) and 19D dams and studying the fetal ductus 4 and 8 h later.

Results: Milrinone and amrinone dilated the postnatal ductus dose-dependently. Large doses of these drugs dilated it completely, and clinically equivalent doses dilated it minimally. Milrinone and amrinone prevented constriction of the fetal ductus by indomethacin. Their ductus-dilating effects were more potent in the preterm than in the near-term fetuses, and clinically equivalent doses of these PDE 3 inhibitors dilated preterm ductus completely.

Conclusion: In rats, PDE 3 inhibitors reopen the constricted postnatal DA slightly. PDE 3 inhibitors dilate the fetal DA constricted with indomethacin effectively and more sensitively in preterm than in near-term fetuses.

抑制磷酸二酯酶3对大鼠胎儿和出生后动脉导管的体内扩张作用。
背景:临床上,磷酸二酯酶3 (PDE 3)抑制剂用于早产儿急性心力衰竭,似乎会扩张动脉导管(DA)。目的:通过体内研究,阐明pde3抑制剂对近期大鼠幼鼠的导管扩张作用,以及它们对近期和早产胎鼠的不同作用。方法:采用快速全身冷冻法,在冷冻切片机上切割,显微镜和千分尺测量大鼠幼仔和胎儿的体内导管直径。每组研究8 ~ 20只幼犬和胎儿。将pde3特异性抑制剂Milrinone和amrinone注射到1 h龄幼犬体内,0.5 h和1 h后观察DA的变化。通过在21D(妊娠第21天:足月-21.5天)和19D胎体注射吲哚美辛(10 mg/kg)和PDE 3抑制剂,并在4和8 h后对胎儿导管进行观察,研究PDE 3抑制剂对近期和早产儿导管的不同影响。结果:米力农和氨力农均呈剂量依赖性地扩张产后导管。大剂量的这些药物完全使其扩张,而临床上同等剂量的药物使其最小限度地扩张。米力农和氨力农可防止吲哚美辛对胎儿导管的收缩。它们的导管扩张作用在早产儿中比在近期胎儿中更有效,临床上相同剂量的PDE - 3抑制剂可以完全扩张早产儿导管。结论:在大鼠中,pde3抑制剂可使产后缩窄的DA略微打开。pde3抑制剂能有效地扩张因吲哚美辛收缩的胎儿DA,并且在早产儿中比在近期胎儿中更敏感。
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