Effect of the administration of prostaglandins (PGE2) in the early postnatal period on closure of the ductus arteriosus in the laboratory rat.

Physiologia Bohemoslovaca Pub Date : 1989-01-01
T Janatová, D Jarkovská, J Hruda, M Samánek, B Ostádal
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Abstract

Maintenance of a patent ductus arteriosus by means of prostaglandins enables the surgical correction of a congenital heart defect in infants to be postponed until a phase of development when the operation hazards are smaller. We investigated the pathophysiological consequences of this therapeutic measure in an experimental model in which E2 prostaglandin was administered to newborn laboratory rats. It was found that, physiologically, the ductus arteriosus (DA) closed progressively within 180 min after birth. The repeated administration of PGE2 (subcutaneously, 15 micrograms.kg-1 every 30 min from the 5th min after birth) blocked closure of the DA, which was still fully patent 300 min after birth. Histological tests showed no significant differences in the structure of the tunica media of the physiologically patent and the PGE2-treated DA. The results show that PGE2 also inhibit physiological closure of the DA in newborn rats. Long-term study of this pathophysiological process is at present impeded by the need for the continuous administration of prostaglandins.

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产后早期给予前列腺素(PGE2)对实验大鼠动脉导管闭合的影响。
通过前列腺素维持动脉导管未闭,可以将婴儿先天性心脏缺陷的手术矫正推迟到手术危害较小的发育阶段。我们在一个实验模型中研究了这种治疗措施的病理生理后果,该模型将E2前列腺素给予新生实验室大鼠。生理上发现,出生后180分钟内,动脉导管(DA)逐渐闭合。重复给药PGE2(皮下注射,15微克。从出生后第5分钟起每30分钟1公斤)阻断DA闭合,出生后300分钟仍完全通畅。组织学检查显示生理性专利和pge2处理的DA的中膜结构无显著差异。结果表明,PGE2对新生大鼠DA的生理闭合也有抑制作用。这种病理生理过程的长期研究目前由于需要持续使用前列腺素而受到阻碍。
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