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向血容量正常和血容量不足的猴子脑内注射阿片受体药物的效果。

Effects of opiate receptor drugs injected intracerebrally into the normovolemic and hypovolemic monkey.

作者信息

Kregel K C, Reynolds D G, Gurll N J, Gisolfi C V

出版信息

Peptides. 1985 Nov-Dec;6(6):1161-6. doi: 10.1016/0196-9781(85)90444-9.

Abstract

Systemic injection of naloxone (NAL), an opioid-receptor antagonist, significantly elevates systolic blood pressure (SBP) in anesthetized hypovolemic monkeys, providing indirect evidence that endogenous opioids contribute to cardiovascular depression during shock. The purpose of this study was to identify specific centrally located opioid receptor sites that participate in SBP regulation under normovolemic and hypovolemic conditions. In 6 monkeys, bilateral guide cannulae were stereotaxically implanted above areas ranging from the diencephalon to the lower medulla. Microinjections (1 microliter) of D- Ala2-Met-enkephalinamide (DAME) (3.4-27.2 nM) into normovolemic unanesthetized monkeys reduced SBP by 10-65 mm Hg in a dose-related fashion. Subsequent injection of NAL (12.2 nM) attenuated this hypotensive response. Heart rate fell 20-40 bpm with DAME, but not in response to dose. In the anesthetized animal rendered hypotensive (SBP = 45 mm Hg) by hemorrhage. NAL injected into predetermined DAME-sensitive sites failed to increase SBP more than 5 mm Hg. Even consecutive injections into multiple sites elevated SBP only 20 mm Hg. We conclude that the centrally located opioid-sensitive sites tested exert only a mild influence in mediating hemorrhagic hypotension.

摘要

全身性注射阿片受体拮抗剂纳洛酮(NAL)可显著提高麻醉状态下低血容量猴子的收缩压(SBP),这间接证明内源性阿片类物质在休克期间会导致心血管抑制。本研究的目的是确定在血容量正常和低血容量条件下参与SBP调节的特定中枢性阿片受体位点。在6只猴子中,通过立体定位将双侧引导套管植入从间脑到延髓下部的区域上方。向血容量正常的未麻醉猴子微量注射(1微升)D-丙氨酸2-甲硫氨酸脑啡肽酰胺(DAME)(3.4 - 27.2 nM),SBP以剂量相关的方式降低了10 - 65 mmHg。随后注射NAL(12.2 nM)减弱了这种降压反应。DAME使心率下降20 - 40次/分钟,但对剂量无反应。在因出血而血压降低(SBP = 45 mmHg)的麻醉动物中,向预先确定的对DAME敏感的位点注射NAL,SBP升高不超过5 mmHg。即使连续向多个位点注射,SBP也仅升高20 mmHg。我们得出结论,所测试的中枢性阿片敏感位点在介导出血性低血压方面仅发挥轻微作用。

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