单次腹腔内注入神经激肽-1受体拮抗剂在减少术后粘连形成方面的有效性具有时间依赖性。
The effectiveness of a single intraperitoneal infusion of a neurokinin-1 receptor antagonist in reducing postoperative adhesion formation is time dependent.
作者信息
Cohen Philip A, Aarons Cary B, Gower Adam C, Stucchi Arthur F, Leeman Susan E, Becker James M, Reed Karen L
机构信息
Department of Surgery, Boston University School of Medicine, Boston, MA 02118, USA.
出版信息
Surgery. 2007 Mar;141(3):368-75. doi: 10.1016/j.surg.2006.09.007. Epub 2007 Feb 6.
BACKGROUND
Current methods to prevent intraabdominal adhesions are not uniformly effective. We recently showed in rats that a neurokinin-1 receptor (NK-1R) antagonist is capable of reducing adhesion formation. To determine the clinical feasibility of using an NK-1R antagonist to reduce adhesions, this study examined the time dependence for the effectiveness of NK-1R antagonist administration and its effects on wound healing.
METHODS
Adhesions were surgically induced in rats receiving a single intraperitoneal infusion of the NK-1R antagonist, CJ-12,255, during or 1, 5, 12, or 24 hours after surgery. Adhesion formation was assessed 7 days later. In a subset of animals, tissue plasminogen activator (tPA) activity, which is a measure of peritoneal fibrinolytic activity, was determined in peritoneal fluid 24 hours after surgery (48 hours for animals infused at 24 hours). The tPA activity was also determined in nonoperated animals 24 hours after peritoneal injection of the NK-1R antagonist. Colonic burst pressures were measured 7 days after creation of anastomoses in rats that were administered the antagonist at surgery.
RESULTS
The NK-1R antagonist significantly reduced (P=.003) intraabdominal adhesions when administered during or 1 hour after surgery, only moderately reduced (P=.08) adhesions when administered at 5 hours, and had no effect at 12 or 24 hours. Peritoneal tPA activity was significantly increased (P<.05) in peritoneal fluid 24 hours after administration of the NK-1R antagonist regardless of the surgical procedure. The NK-1R antagonist did not alter colonic anastomotic healing.
CONCLUSIONS
These data show that some of the events critical to adhesion formation occur within the first 5 hours following an abdominal operation in this model. The fact that the NK-1R antagonist does not impair colonic anastomotic healing enhances its usefulness as a therapeutic agent to inhibit adhesion formation.
背景
目前预防腹腔内粘连的方法并非都有效。我们最近在大鼠实验中表明,神经激肽-1受体(NK-1R)拮抗剂能够减少粘连形成。为了确定使用NK-1R拮抗剂减少粘连的临床可行性,本研究检测了给予NK-1R拮抗剂的有效性的时间依赖性及其对伤口愈合的影响。
方法
在大鼠手术后即刻、术后1、5、12或24小时接受单次腹腔内输注NK-1R拮抗剂CJ-12,255,通过手术诱导粘连形成。7天后评估粘连形成情况。在一部分动物中,于术后24小时(术后24小时输注的动物为48小时)测定腹腔液中组织纤溶酶原激活物(tPA)活性,以此作为腹膜纤溶活性的指标。在腹腔注射NK-1R拮抗剂24小时后,也对未手术动物测定tPA活性。在手术时给予拮抗剂的大鼠中,于吻合口形成7天后测量结肠爆破压。
结果
当在手术期间或术后1小时给予NK-1R拮抗剂时,可显著减少(P = 0.003)腹腔内粘连;在术后5小时给予时,仅适度减少(P = 0.08)粘连;而在术后12或24小时给予则无效果。无论手术操作如何,给予NK-1R拮抗剂24小时后,腹腔液中的腹膜tPA活性均显著增加(P < 0.05)。NK-1R拮抗剂未改变结肠吻合口愈合情况。
结论
这些数据表明,在此模型中,腹腔手术后最初5小时内发生了一些对粘连形成至关重要的数据。NK-1R拮抗剂不损害结肠吻合口愈合这一事实,增强了其作为抑制粘连形成治疗药物的实用性。
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