梗阻会改变前列腺素E2对输尿管收缩性的影响。

Obstruction alters the effect of prostaglandin E2 on ureteral contractility.

作者信息

Lowry Patrick S, Jerde Travis J, Bjorling Dale E, Maskel Jennifer L, Nakada Stephen Y

机构信息

Department of Surgery, Division of Urology, University of Wisconsin Medical School, Madison, Wisconsin 53792-3236, USA.

出版信息

J Endourol. 2005 Mar;19(2):183-7. doi: 10.1089/end.2005.19.183.

DOI:10.1089/end.2005.19.183

PMID:15798415

Abstract

BACKGROUND AND PURPOSE

Although our understanding of ureteral physiology during acute obstruction remains limited, we believe that prostanoids (prostaglandins [PGs], thromboxanes, prostacyclins) play a major role in modulation of ureteral contractility and that inhibition of prostanoid synthesis causes substantial reduction in in-vitro and in-vivo ureteral contractility rates. The purpose of this study was to determine the in-vitro effects of PGE2 on chronically obstructed human and acutely obstructed porcine ureters.

MATERIALS AND METHODS

Female pigs underwent unilateral laparoscopic ureteral obstruction. Following 1, 2, 6, 24, and 48 hours of obstruction (n = 3 at all points), animals were euthanized, and obstructed, contralateral nonobstructed, and normal (from unobstructed pigs) ureters were harvested. Chronically obstructed human ureter was obtained from subjects who underwent nephrectomy to remove nonfunctioning kidneys. Normal human ureter was obtained from the discarded portion of excess distal ureter in patients undergoing elective donor nephrectomy. Rings 4 to 5 mm long were suspended in aerated Krebs buffer, and their spontaneous contractions and contraction in response to various concentrations of PGE2 were recorded.

RESULTS

Prostaglandin E2 increased contractility in chronically obstructed human ureters. In acutely obstructed porcine ureteral segments, low concentrations of PGE2 inhibited ureteral contractility in a dose-dependent fashion, similar to controls. At higher concentrations of PGE2, contractility was increased. This increase was more pronounced with longer intervals of obstruction in a time-dependent manner.

CONCLUSION

Prostaglandin E2 increased contractility in obstructed ureters while relaxing normal and nonobstructed ureters. The response to PGE2 was accentuated by a longer duration of obstruction. Prostaglandin E2 may be a unique target for pharmacologic modulation in the treatment of symptoms associated with acute urinary obstruction.

摘要

背景与目的

尽管我们对急性梗阻期间输尿管生理的理解仍然有限，但我们认为前列腺素（前列腺素[PGs]、血栓素、前列环素）在调节输尿管收缩性方面起主要作用，并且抑制前列腺素合成会导致体外和体内输尿管收缩率大幅降低。本研究的目的是确定前列腺素E2对慢性梗阻的人类输尿管和急性梗阻的猪输尿管的体外作用。

材料与方法

雌性猪接受单侧腹腔镜输尿管梗阻。在梗阻1、2、6、24和48小时后（各时间点n = 3），对动物实施安乐死，并获取梗阻侧、对侧未梗阻以及正常（来自未梗阻猪）的输尿管。慢性梗阻的人类输尿管取自接受肾切除术以切除无功能肾脏的受试者。正常人类输尿管取自接受择期供体肾切除术患者多余远端输尿管的废弃部分。将4至5毫米长的输尿管环悬挂在充氧的 Krebs 缓冲液中，记录其自发收缩以及对不同浓度前列腺素E2的收缩反应。