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首页> 外文期刊>Frontiers in Pharmacology >A Fixed-Dose Combination, QXOH/Levobupivacaine, Produces Long-Acting Local Anesthesia in Rats Without Additional Toxicity
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A Fixed-Dose Combination, QXOH/Levobupivacaine, Produces Long-Acting Local Anesthesia in Rats Without Additional Toxicity

机译:固定剂量组合QXOH / Levobupivaine,在大鼠中产生长效的局部麻醉,而无需额外的毒性

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QXOH, a QX314 derivative with longer duration and lesser local toxicity, is a novel local anesthetic in preclinical drug development. Previous studies demonstrated that bupivacaine can prolong the effects of QX314. So, we attempted to combine QXOH with levobupivacaine to shorten the onset time and lengthen the duration. In this study, we investigated the efficacy, local and systemic toxicity in rats. In subcutaneous infiltration anesthesia, the inhibition of cutaneous trunci muscle reflex for QXOH-LB was greater than QXOH and levobupivacaine in the first 8 h (QXOH-LB vs. QXOH, P = 0.004; QXOH-LB vs. LB, P = 0.004). The completely recovery time for QXOH-LB (17.5 ± 2.5 h) was significantly longer than levobupivacaine (9.0 ± 1.3 h, P = 0.034) and QXOH (9.8 ± 0.9 h, P = 0.049). In sciatic nerve block, QXOH-LB produced a rapid onset time, which was obviously shorter than QXOH. For sensory, the time to recovery for QXOH-LB was 17.3 ± 2.6 h, which was statistically longer than 6.0 ± 1.8 h for QXOH (P = 0.027), and 4 h for levobupivacaine ( P = 0.001). Meanwhile, the time to motor recovery for QXOH-LB was 7.9 ± 2.8 h, significantly longer than 4 h for levobupivacaine ( P = 0.003) but similar to 6.0 ± 1.7 h for QXOH ( P = 0.061). In local toxicity, there was no significant difference of histological score regarding muscle and sciatic nerve in QXOH-LB, QXOH, levobupivacaine and saline ( P & 0.01). In the combination, the interaction index of LD _(50) was 1.39, indicating antagonistic interaction between QXOH and levobupivacaine in terms of systemic toxicity. In this study, we demonstrated that QXOH-LB produced cutaneous anesthesia which was 2-fold greater than that produced by QXOH or LB alone, and elicited sciatic nerve block with a potency that was 5- and 3-fold that of LB and QXOH, respectively. Local tissue inflammation by QXOH-LB was mild, similar to that induced by LB. This fixed-dose combination led to an antagonistic interaction between QXOH and LB in terms of systemic toxicity. These results suggested that QXOH-LB induced a long-lasting local anesthesia, likely, avoiding clinically important local and systemic toxicities.
机译:QXOH,QX314衍生物具有较长的持续时间和较小的局部毒性,是一种在临床前药发发中的新型局部麻醉药。以前的研究表明,Bupivacaine可以延长QX314的影响。因此,我们试图将QXOH与Levobupivacaine合并以缩短起始时间并延长持续时间。在这项研究中,我们研究了大鼠的疗效,局部和全身毒性。在皮下浸润麻醉中,在前8H(QXOH-LB对QXOH,P = 0.004; QXOH-LB对LB,P = 0.004)中,在QXOH-LB对QXOH-LB的抑制作用QXOH-LB的抑制大于QXOH和LEVOBivacaine 。 QXOH-LB(17.5±2.5小时)的完全恢复时间明显长于左旋素(9.0±1.3小时,P = 0.034)和QXOH(9.8±0.9小时,P = 0.049)。在坐骨神经嵌段中,QXOH-LB产生了快速发作时间,显着短于QXOH。对于感官,QXOH-LB的恢复时间为17.3±2.6小时,QXOH(P = 0.027)和4小时的统计学上长于6.0±1.8小时(P = 0.001)。同时,QXOH-LB的电动机恢复的时间为7.9±2.8小时,对于左旋眼盖(P = 0.003)显着长于4小时,但类似于QXOH的6.0±1.7小时(P = 0.061)。在局部毒性中,关于QXOH-LB,QXOH,Levobupivaina和盐水中的肌肉和坐骨神经的组织学分数没有显着差异(P <0.01)。在组合中,LD _(50)的相互作用指数为1.39,表明在全身毒性方面表明QXOH和LEVOBivacaine之间的拮抗相互作用。在这项研究中,我们证明了QXOH-LB产生的皮肤麻醉,其比QXOH或LB单独产生的2倍,并且引发坐骨神经嵌段,其效力为1B和3倍,分别。 QXOH-LB的局部组织炎症温和,类似于LB诱导的局部炎症。该固定剂量组合导致QXOH和LB之间的拮抗相互作用,在系统性毒性方面。这些结果表明,QXOH-LB可能诱导持久的局部麻醉,可能避免临床重要的局部和全身毒性。

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