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首页> 外文期刊>Pharmacology: International Journal of Experimental and Clinical Pharmacology >Effect of bradykinin receptor antagonists on vincristine- and streptozotocin-induced hyperalgesia in a rat model of chemotherapy-induced and diabetic neuropathy.
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Effect of bradykinin receptor antagonists on vincristine- and streptozotocin-induced hyperalgesia in a rat model of chemotherapy-induced and diabetic neuropathy.

机译:缓激肽受体拮抗剂对长春新碱和链脲佐菌素诱导的痛觉过敏的影响,该模型在化疗引起的糖尿病性神经病大鼠中。

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摘要

The role of bradykinin receptor blockade in the development of neuropathies caused by diabetes mellitus and vincristine was examined. The effects of a potent and selective B(1) receptor antagonist (des-Arg(10)-HOE 140) as well as a specific antagonist of B(2) receptors (HOE 140) were investigated. Both agents significantly decreased hyperalgesia caused otherwise by vincristine. In a diabetic neuropathy model, both agents almost completely suppressed hyperalgesia in the first 10 days of the study. However, from day 11 after administration of streptozotocin, the action of des-Arg(10)-HOE 140 was significantly weaker than that of HOE 140. The results of the study suggest involvement of both B(1) and B(2) receptors in transmission of nociceptive stimuli in the vincristine-induced as well as diabetic neuropathy model.
机译:检查了缓激肽受体阻滞在糖尿病和长春新碱引起的神经病发展中的作用。研究了有效和选择性的B(1)受体拮抗剂(des-Arg(10)-HOE 140)以及B(2)受体的特异性拮抗剂(HOE 140)的作用。两种药物均明显降低了长春新碱引起的痛觉过敏。在糖尿病性神经病模型中,两种药物在研究的前10天几乎都完全抑制了痛觉过敏。然而,从链脲佐菌素给药后的第11天起,des-Arg(10)-HOE 140的作用明显弱于HOE140。研究结果表明,B(1)和B(2)受体均参与其中。在长春新碱诱导的以及糖尿病性神经病模型中传递伤害性刺激。

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