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μ、δ和κ阿片受体激动剂选择性调节雌性大鼠的性行为:对孕酮的不同依赖性。

Mu-, delta-, and kappa-opioid receptor agonists selectively modulate sexual behaviors in the female rat: differential dependence on progesterone.

作者信息

Pfaus J G, Pfaff D W

机构信息

Laboratory of Neurobiology and Behavior, Rockefeller University, New York, New York 10021.

出版信息

Horm Behav. 1992 Dec;26(4):457-73. doi: 10.1016/0018-506x(92)90014-m.

Abstract

Previous studies suggested that opioid receptor agonists infused into the lateral ventricles can inhibit (through mu receptors) or facilitate (through delta receptors) the lordosis behavior of ovariectomized (OVX) rats treated with estrogen and a low dose of progesterone. The present study investigated the behavioral and hormonal specificity of those effects using more selective opioid receptor agonists. Sexually experienced OVX rats were implanted stereotaxically with guide cannulae aimed at the right lateral ventricle. One group of rats was treated with estradiol benzoate (EB, 10 micrograms) 48 hr and progesterone (P, 250 micrograms) 4 hr before testing, whereas the other group was treated with EB alone. Rats were infused with different doses of the selective mu-receptor agonist DAMGO, the selective delta-receptor agonist DPDPE, or the selective kappa-receptor agonist U50-488. The females were placed with a sexually vigorous male in a bilevel chamber (Mendelson and Gorzalka, 1987) for three tests of sexual behavior, beginning 15, 30, and 60 min after each infusion. DAMGO reduced lordosis quotients and magnitudes significantly in rats treated with EB and P, but not in rats treated with EB alone. In contrast, DPDPE and U50-488H increased lordosis quotients and magnitudes significantly in both steroid-treatment groups. Surprisingly, measures of proceptivity, rejection responses, and level changes were not affected significantly by mu or kappa agonists, although proceptivity and rejection responses were affected by DPDPE treatment. These results suggest that the effects of lateral ventricular infusions of opioid receptor agonists on the sexual behavior of female rats are relatively specific to lordosis behavior. Moreover, the facilitation of lordosis behavior by delta- or kappa-receptor agonists is independent of progesterone treatment, whereas the inhibitory effect of mu-receptor agonists on lordosis behavior may require the presence of progesterone.

摘要

先前的研究表明,注入侧脑室的阿片受体激动剂可(通过μ受体)抑制或(通过δ受体)促进经雌激素和低剂量孕酮处理的去卵巢(OVX)大鼠的脊柱前凸行为。本研究使用更具选择性的阿片受体激动剂来研究这些作用的行为和激素特异性。对有性经验的OVX大鼠进行立体定位植入,将引导套管对准右侧脑室。一组大鼠在测试前48小时接受苯甲酸雌二醇(EB,10微克)处理,4小时前接受孕酮(P,250微克)处理,而另一组大鼠仅接受EB处理。给大鼠注入不同剂量的选择性μ受体激动剂DAMGO、选择性δ受体激动剂DPDPE或选择性κ受体激动剂U50-488。在每次注入后15、30和60分钟,将雌性大鼠与一只性活力旺盛的雄性大鼠置于双层笼舍中(Mendelson和Gorzalka,1987)进行三次性行为测试。DAMGO显著降低了接受EB和P处理的大鼠的脊柱前凸商数和幅度,但对仅接受EB处理的大鼠没有影响。相比之下,DPDPE和U50-488H在两个类固醇处理组中均显著提高了脊柱前凸商数和幅度。令人惊讶的是,尽管接受DPDPE处理会影响求偶行为和拒绝反应,但μ或κ激动剂对求偶行为、拒绝反应和水平变化的测量没有显著影响。这些结果表明,侧脑室注入阿片受体激动剂对雌性大鼠性行为的影响相对特定于脊柱前凸行为。此外,δ或κ受体激动剂对脊柱前凸行为的促进作用与孕酮处理无关,而μ受体激动剂对脊柱前凸行为的抑制作用可能需要孕酮的存在。

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