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抑制4型磷酸二酯酶可减少大鼠和小鼠应激诱导的排便。

Inhibition of phosphodiesterase type 4 decreases stress-induced defecation in rats and mice.

作者信息

Barone Frank C, Barton Matthew E, White Ray F, Legos Jeffrey J, Kikkawa Hideo, Shimamura Midori, Kuratani Kazuyoshi, Kinoshita Mine

机构信息

Discovery Research, High Throughput Biology, GlaxoSmithKline, King of Prussia, PA 19406, USA.

出版信息

Pharmacology. 2008;81(1):11-7. doi: 10.1159/000107662. Epub 2007 Aug 28.

Abstract

BACKGROUND/AIMS: Phosphodiesterase type 4 (PDE4) has been previously shown to regulate colonic contractile activity in vitro. In this study, the effects of PDE4 inhibition were assessed in a model of stress-induced defecation previously demonstrated to be due to increased colonic transit/evacuation.

METHODS

Rats were individually placed in a mild restraint cage and placed into a 12 degrees C environment (cold-restraint stress) for 60 min. Mice received restraint (only) stress at room temperature for 30 min. Loperamide (positive control compound) or two different PDE4 inhibitors (rolipram and roflumilast) were administered orally at several doses to the rodents 1 h before stress began. Vehicle alone was administered for comparison. The number of fecal pellets expelled during stress (fecal pellet output), total fecal pellet wet weight and total fecal water content were measured.

RESULTS

Loperamide produced a dose-related decrease (ID(50)s in mg/kg) in fecal pellet output (rat = 7.4, mouse = 0.7) and significantly decreased fecal wet weight (72.9%) and decreased fecal percent water content (9.4%). The two PDE4 inhibitors produced a similar dose-related inhibition of fecal pellet output. Rolipram exhibited ID(50)s in rat and mouse of 14.1 and 27.1, respectively. Rolipram significantly decreased fecal wet weight (58.8%) but increased fecal percent water content (15.0%). For roflumilast, ID(50)s were 24.2 mg/kg and 12.4 in the rat and mouse, respectively. Although roflumilast also significantly (p < 0.05) decreased fecal wet weight (47.2%), it did not significantly increase fecal percent water content.

CONCLUSIONS

These data indicate that PDE4 inhibition is effective in reducing rodent stress-induced defecation, provides the first functional data on a potential role for PDE4 activity in the colonic evacuation response to stress, and indicates the potential utility of PDE4 inhibitors in functional bowel disease such as irritable bowel syndrome requires further evaluation.

摘要

背景/目的:先前已证明4型磷酸二酯酶(PDE4)可在体外调节结肠收缩活性。在本研究中,在先前已证明由结肠转运/排空增加所致的应激性排便模型中评估了PDE4抑制的作用。

方法

将大鼠单独置于轻度束缚笼中,并放入12℃环境(冷束缚应激)中60分钟。小鼠在室温下接受束缚(仅)应激30分钟。在应激开始前1小时,以几种剂量给啮齿动物口服洛哌丁胺(阳性对照化合物)或两种不同的PDE4抑制剂(咯利普兰和罗氟司特)。仅给予赋形剂作为对照。测量应激期间排出的粪便颗粒数量(粪便颗粒排出量)、粪便颗粒总湿重和粪便总含水量。

结果

洛哌丁胺使粪便颗粒排出量呈剂量相关减少(大鼠的半数抑制剂量(ID50)以mg/kg计为7.4,小鼠为0.7),并显著降低粪便湿重(72.9%)和粪便含水量百分比(9.4%)。两种PDE4抑制剂对粪便颗粒排出量产生了类似的剂量相关抑制作用。咯利普兰在大鼠和小鼠中的ID50分别为14.1和27.1。咯利普兰显著降低粪便湿重(58.8%),但增加粪便含水量百分比(15.0%)。对于罗氟司特,大鼠和小鼠的ID50分别为24.2mg/kg和12.4。尽管罗氟司特也显著(p<0.05)降低了粪便湿重(47.2%),但未显著增加粪便含水量百分比。

结论

这些数据表明PDE4抑制可有效减少啮齿动物应激性排便,提供了关于PDE4活性在结肠对应激的排空反应中的潜在作用的首个功能数据,并表明PDE4抑制剂在诸如肠易激综合征等功能性肠病中的潜在效用需要进一步评估。

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