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年龄依赖性的孤啡肽/阿片生长因子对脑损伤后低血压性脑血流动力学受损的作用

Age-dependent NOC/oFQ contribution to impaired hypotensive cerebral hemodynamics after brain injury.

作者信息

Armstead William M

机构信息

Department of Anesthesia and Pharmacology, University of Pennsylvania, Philadelphia 19104, USA.

出版信息

J Neurotrauma. 2002 Oct;19(10):1193-202. doi: 10.1089/08977150260337994.

Abstract

Previous studies have observed that the newly described opioid, nociceptin/orphanin FQ (NOC/oFQ), contributed to age dependent reductions in cerebral blood flow (CBF) and pial artery diameter after fluid percussion brain injury (FPI). Unrelated studies have noted a similar age dependency in impaired hypotensive cerebral autoregulation after FPI. This study was designed to compare the role of NOC/oFQ in impaired hypotensive cerebral autoregulation after FPI in newborn and juvenile pigs equipped with a closed cranial window. Ten minutes of hemorrhagic hypotension (10-15 mL blood/kg) decreased mean arterial blood pressure uniformly in both groups ( approximately 44%). In the newborn, hypotensive pial artery dilation was blunted within 1 h of FPI but partially protected by pretreatment with the NOC/oFQ antagonist, [F/G] NOC/oFQ (1-13) NH(2) (1 mg/kg, i.v.) (34 +/- 1 vs. 8 +/- 1 vs. 20 +/- 2% for sham control, FPI, and FPI-[F/G] NOC/oFQ (1-13) NH(2), respectively). CBF was reduced during normotension by FPI, further reduced by hypotension, but both were partially protected by this antagonist in the newborn (63 +/- 4, 34 +/- 2, and 20 +/- 2 vs. 65 +/- 4, 47 +/- 2, and 29 +/- 2 mL/min.100 g for normotension, normotension-FPI and hypotension-FPI in the absence and presence of [F/G] NOC/oFQ (1-13) NH(2), respectively). In contrast, blunted hypotensive pial artery dilation was protected significantly less by this NOC/oFQ antagonist in the juvenile (32 +/- 2 vs. 7 +/- 2 vs. 13 +/- 2% for sham control, FPI and FPI-NOC/oFQ antagonist, respectively). Similarly, [F/G] NOC/oFQ (1-13) NH(2) had less protective effect on normotensive and hypotensive CBF values post FPI in the juvenile. These data indicate that NOC/oFQ contributes to impaired hypotensive cerebral hemodynamics following brain injury in an age-dependent manner.

摘要

先前的研究观察到,新描述的阿片样物质——孤啡肽/痛敏肽(NOC/oFQ),在流体冲击脑损伤(FPI)后导致脑血流量(CBF)和软脑膜动脉直径出现年龄依赖性降低。无关研究指出,FPI后低血压性脑自动调节受损也存在类似的年龄依赖性。本研究旨在比较NOC/oFQ在配备闭合颅骨视窗的新生猪和幼年猪FPI后低血压性脑自动调节受损中的作用。两组均出现10分钟的出血性低血压(10 - 15 mL/kg血液),平均动脉血压均一性降低(约44%)。在新生猪中,FPI后1小时内低血压性软脑膜动脉扩张减弱,但用NOC/oFQ拮抗剂[F/G]NOC/oFQ(1 - 13)NH₂(1 mg/kg,静脉注射)预处理可部分保护(假手术对照组、FPI组和FPI - [F/G]NOC/oFQ(1 - 13)NH₂组分别为34±1%、8±1%和20±2%)。FPI使新生猪在正常血压时CBF降低,低血压使其进一步降低,但该拮抗剂在新生猪中对二者均有部分保护作用(正常血压、正常血压 - FPI和低血压 - FPI时,在不存在和存在[F/G]NOC/oFQ(1 - 13)NH₂的情况下,分别为63±4、34±2和20±2 vs. 65±4、47±2和29±2 mL/min·100g)。相比之下,在幼年猪中,该NOC/oFQ拮抗剂对减弱的低血压性软脑膜动脉扩张的保护作用明显较小(假手术对照组、FPI组和FPI - NOC/oFQ拮抗剂组分别为32±2%、7±2%和13±2%)。同样,[F/G]NOC/oFQ(1 - 13)NH₂对幼年猪FPI后正常血压和低血压时的CBF值的保护作用较小。这些数据表明,NOC/oFQ以年龄依赖性方式导致脑损伤后低血压性脑血流动力学受损。

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