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对慢性受压马尾神经血流改善的影响:选择性前列腺素E受体(EP4)激动剂与前列腺素E1衍生物的比较。

Effects on improvement of blood flow in the chronically compressed cauda equina: comparison between a selective prostaglandin E receptor (EP4) agonist and a prostaglandin E1 derivate.

作者信息

Sekiguchi Miho, Konno Shin-ichi, Kikuchi Shin-ichi

机构信息

Department of Orthopaedic Surgery, Fukushima Medical University School of Medicine, Fukushima City, Fukushima, Japan.

出版信息

Spine (Phila Pa 1976). 2006 Apr 15;31(8):869-72. doi: 10.1097/01.brs.0000209256.96186.a7.

Abstract

STUDY DESIGN

Vasodilatation was studied in a model of experimental chronic cauda equina compression using measurements of vessel diameter on video recordings.

OBJECTIVE

The vasodilative effect was compared between a prostaglandin E2 receptor (EP) subtype agonists (EP4 agonist) and a prostaglandin E1 (PGE1) derivate.

SUMMARY AND BACKGROUND DATA

Reduction of blood flow is one important pathogenic factor of neurogenic intermittent claudication (NIC) for lumbar spinal canal stenosis. It is known that PGE1 improves the mean walking distance in patients with cauda equina compression type of NIC. There are four subtypes of EP: EP1, EP2, EP3, and EP4. EP4 is located in vessels of pigs and rabbits. A highly selective EP4 agonist, which has effects on dilatation of pig and rabbit vessels, has recently been developed. One may therefore assume that this agonist may improve blood flow in the chronically compressed cauda equina.

METHODS

A total of 25 dogs were used. A plastic balloon inflated to 10 mm Hg was placed under the lamina of the seventh lumbar vertebra for 1 week. OP-1206 cyclodextrin clathrate (OP-1206 CD: prostaglandin E1 derivate) and ONO-4819 CD (a highly selective EP4 agonist) were intravenously administrated. The following 5 experimental groups were assigned: animals in group OP (3) (n = 5) and Group OP (10) (n = 5) received 3 eta g/kg per minute and 10 eta g/kg per minute of OP-1206 CD, respectively; those in Group EP (3) (n = 5) and Group EP (10) (n = 5) received 3 eta g/kg per minute and 10 eta g/kg per minute of ONO-4819 CD, respectively; and those in the control group (n = 5) received saline. After 7 days, the cauda equina was exposed and blood vessels of the second or third sacral nerve root were identified using a specially designed operation microscope equipped with a video camera. The diameters of the observed blood vessels were measured on video-recordings every 10 minutes until 60 minutes after administrating OP-1206 CD or ONO-4819CD.

RESULTS

In the Groups OP (3), OP (10), and EP (10), the blood vessels were dilated and blood flow increased after injection of the agents. In the Group EP (10), the vessel diameter and blood flow increased significantly compared with that in the other four groups. In contrast, the blood vessels contracted and the blood flow was reduced in the Group EP (3).

CONCLUSIONS

Our results suggested that the EP4 agonist at high concentrations might be a potential therapeutic agent since it is expected to increase blood flow in nerve roots in patients with spinal canal stenosis.

摘要

研究设计

在实验性慢性马尾神经受压模型中,通过视频记录测量血管直径来研究血管舒张情况。

目的

比较前列腺素E2受体(EP)亚型激动剂(EP4激动剂)和前列腺素E1(PGE1)衍生物的血管舒张作用。

总结与背景数据

血流减少是腰椎管狭窄症神经源性间歇性跛行(NIC)的一个重要致病因素。已知PGE1可改善马尾神经受压型NIC患者的平均步行距离。EP有四种亚型:EP1、EP2、EP3和EP4。EP4存在于猪和兔的血管中。最近开发了一种对猪和兔血管舒张有作用的高选择性EP4激动剂。因此可以推测,这种激动剂可能改善慢性受压马尾神经的血流。

方法

共使用25只犬。将充气至10 mmHg的塑料球囊置于第七腰椎椎板下1周。静脉注射OP - 1206环糊精包合物(OP - 1206 CD:前列腺素E1衍生物)和ONO - 4819 CD(一种高选择性EP4激动剂)。分为以下5个实验组:OP(3)组(n = 5)和OP(10)组(n = 5)分别接受每分钟3 μg/kg和每分钟10 μg/kg的OP - 1206 CD;EP(3)组(n = 5)和EP(10)组(n = 5)分别接受每分钟3 μg/kg和每分钟10 μg/kg的ONO - 4819 CD;对照组(n = 5)接受生理盐水。7天后,暴露马尾神经,使用配备摄像机的特制手术显微镜识别第二或第三骶神经根的血管。在注射OP - 1206 CD或ONO - 4819 CD后,每隔10分钟在视频记录上测量观察到的血管直径,直至60分钟。

结果

在OP(3)组、OP(10)组和EP(10)组中,注射药物后血管扩张,血流增加。在EP(10)组中,血管直径和血流与其他四组相比显著增加。相比之下EP(3)组血管收缩且血流减少。

结论

我们的结果表明,高浓度的EP4激动剂可能是一种潜在的治疗药物,因为它有望增加椎管狭窄患者神经根的血流。

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