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首页> 外文OA文献 >Effects of selective inhibitors of cyclo-oxygenase-1 (COX-1) and cyclo-oxygenase-2 (COX-2) on the spontaneous myogenic contractions in the upper urinary tract of the guinea-pig and rat
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Effects of selective inhibitors of cyclo-oxygenase-1 (COX-1) and cyclo-oxygenase-2 (COX-2) on the spontaneous myogenic contractions in the upper urinary tract of the guinea-pig and rat

机译:选择性环氧合酶-1(COX-1)和环氧合酶-2(COX-2)抑制剂对豚鼠和大鼠上尿路自发性肌源性收缩的影响

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The role of cyclo-oxygenase-1 (COX-1) and cyclo-oxygenase-2 (COX-2) in the upper urinary tract of the guinea-pig and rat was examined using simultaneous tension recordings of the proximal and distal regions of the renal pelvis and the ureter.The guinea-pig upper urinary tract contracted at a frequency (7.52±0.3 min−1 at 35°C) significantly lower than the frequency in the proximal renal pelvis (21.6±1.3 min−1) and in the distal renal pelvis and ureter (20.2±1.4 min−1) of the rat (at 30°C).Indomethacin (⩾1 μM for 60 min), decreased the motility index (amplitude×frequency) (MI) in all three regions of the guinea-pig upper urinary tract, an effect which mainly arose from a decrease in the frequency of contractions. In the rat, indomethacin (1–30 μM for 60 min) significantly decreased the MI calculated in the proximal renal pelvis (⩾30 μM indomethacin), and in the distal renal pelvis (⩾10 μM indomethacin), arising from a significant decrease in the amplitude of contractions.The COX-1 inhibitor, valeryl salicylate (VSA) (5–100 μM for 60 min), had no effect on either the amplitude or frequency of contractions in the guinea-pig upper urinary tract. In contrast, VSA increased the force of contractions in the proximal and distal renal pelvis of the rat, whilst having little effect on the frequency of contractions.The COX-2 inhibitor, NS-398 (10–100 nM for 60 min) reduced the MI in the guinea-pig upper urinary tract in a concentration-dependent manner. The MIs calculated for the proximal renal pelvis, distal renal pelvis and ureter, were decreased by 72, 64 and 72% respectively, in 100 nM NS-398. NS-398 (10–100 nM) had no effect on any of the three parameters measured in either the proximal or distal renal pelvis of the rat.These data suggest that endogenously-released prostaglandins (PGs) maintain the myogenic contractility of the upper urinary tract in both the guinea-pig and rat. Moreover COX-2 is the primary enzyme involved in synthesizing PGs in the guinea-pig upper urinary tract, while COX-1 appears to be the predominantly active enzyme in the rat.
机译:使用同时张力记录了豚鼠和大鼠上尿道中的环氧合酶1(COX-1)和环氧合酶2(COX-2)的作用。豚鼠上尿路的收缩频率(35°C下为7.52±0.3±min-1)显着低于近端肾盂的频率(21.6±1.3 min-1)和肾盂输尿管的收缩频率。大鼠的肾盂和输尿管远端(20.2±1.42min-1)(在30°C时)消炎痛(⩾1μM持续60 min)降低了大鼠所有三个区域的运动指数(幅度×频率)(MI)豚鼠上尿路,主要是由于收缩频率降低而引起的。在大鼠中,吲哚美辛(1–30μm,持续60μmin)可显着降低近端肾盂(⩾30μμM吲哚美辛)和远端肾盂(⩾10μμM吲哚美辛)的MI。 COX-1抑制剂戊酸水杨酸酯(VSA)(5–100μm,持续60μmin),对豚鼠上尿路的收缩幅度或频率均无影响。相比之下,VSA增加了大鼠近端和远端肾盂的收缩力,而对收缩频率的影响很小。COX-2抑制剂NS-398(10–100 nM持续60 min)减少了收缩力。豚鼠上尿路的MI呈浓度依赖性。在100 nM NS-398中,计算出的近端肾盂,远端肾盂和输尿管的MI分别降低了72%,64%和72%。 NS-398(10–100 nM)对大鼠近端或远端肾盂测量的三个参数均无影响。这些数据表明内源性释放的前列腺素(PGs)维持上尿的肌源性收缩力豚鼠和大鼠的呼吸道。此外,COX-2是参与豚鼠上尿路中PG合成的主要酶,而COX-1似乎是大鼠中的主要活性酶。

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    Davidson, M E; Lang, R J;

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  • 年度 2000
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