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小剂量多巴胺输注对患病早产儿尿前列腺素E2排泄的影响。

Effect of low-dose dopamine infusion on urinary prostaglandin E2 excretion in sick, preterm infants.

作者信息

Seri I, Hajdu J, Kiszel J, Tulassay T, Aperia A

机构信息

Department of Developmental Physiology, Karolinska Institute, Stockholm, Sweden.

出版信息

Eur J Pediatr. 1988 Aug;147(6):616-20. doi: 10.1007/BF00442476.

Abstract

In pharmacological doses dopamine (DA) will interact with several endocrine systems and both inhibit (prolactin, thyrotropin) and enhance (renin, angiotensin) hormonal release. In this study we have examined whether DA given to preterm neonates will influence prostaglandin (PG) production. The question is of importance since vasodilator PGs play a role in postnatal adaptation. We determined the effect of low dose DA infusion on the 24 h urinary PGE2 excretion rate (an index of renal PGE2 synthesis) in preterm infants. Six preterm neonates, with a 24-h requirement of 2 micrograms/kg per min DA treatment for oedema, moderate oliguria, poor peripheral perfusion and/or mild systemic hypotension were studied on days 2 (Day 1), 3 (Day 2, the day of DA infusion), and 4 (Day 3, DA discontinued) of life. Six preterm infants (control group) that did not require DA infusion were also studied to monitor possible spontaneous changes in the renal PGE2 production on days 2, 3 and 4 of life. In the control group urine output (Uv) and PGE2 excretion rate remained unchanged during the study. In the study group DA administration resulted in nearly two-fold increases in both the Uv (194%) and PGE2 excretion (182%). Urinary PGE2 excretion was, however, closely related to urine flow in both the control infants (Day 1-3) and the study group infants (Day 1-2). Since increased diuresis stimulates renal PGE2 production, our data suggest that the increased PGE2 excretion on Day 2 in the study group was not due to a direct effect of DA on PGE2 synthesis.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

药理剂量的多巴胺(DA)会与多个内分泌系统相互作用,既能抑制(催乳素、促甲状腺素)又能增强(肾素、血管紧张素)激素释放。在本研究中,我们检验了给予早产儿DA是否会影响前列腺素(PG)的产生。这个问题很重要,因为血管舒张性PG在出生后适应过程中起作用。我们测定了低剂量DA输注对早产儿24小时尿PGE2排泄率(肾PGE2合成的指标)的影响。对6名因水肿、中度少尿、外周灌注不良和/或轻度全身性低血压而需要每分钟2微克/千克DA治疗24小时的早产儿,在出生第2天(第1天)、第3天(第2天,DA输注日)和第4天(第3天,停用DA)进行了研究。还研究了6名不需要DA输注的早产儿(对照组),以监测出生后第2、3和4天肾PGE2产生可能的自发变化。对照组在研究期间尿量(Uv)和PGE2排泄率保持不变。研究组给予DA后,Uv(194%)和PGE2排泄(182%)均增加了近两倍。然而,无论是对照组婴儿(第1 - 3天)还是研究组婴儿(第1 - 2天),尿PGE2排泄都与尿流量密切相关。由于利尿增加会刺激肾PGE2产生,我们的数据表明研究组第2天PGE2排泄增加并非DA对PGE2合成的直接作用所致。(摘要截短至250字)

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