Pedersen C A, Boccia M L
Department of Psychiatry, CB# 7160, University of North Carolina at Chapel Hill, Chapel Hill, NC 27599, USA.
Neuroscience. 2006;139(3):843-51. doi: 10.1016/j.neuroscience.2006.01.002. Epub 2006 Feb 20.
Previous studies have found that central administration of arginine vasopressin and arginine vasopressin receptor V1a antagonists respectively inhibited and stimulated receptivity but did not examine effects on other aspects of female sexual behavior. Central oxytocin facilitates both proceptive and receptive components of sexual behavior and diminishes male-directed agonistic behavior. The present study examined i.c.v.-administered arginine vasopressin and V1a antagonist effects on proceptive, receptive and agonistic behaviors, and interactions with oxytocin. In experiment 1, rats were primed s.c. with 2 microg estradiol benzoate x 2 days and with 500 microg of progesterone on day 3. Arginine vasopressin (0.2, 0.4 microg) or normal saline vehicle was administered 5 h after progesterone treatment and sexual and agonistic behavior measured 30, 60 and 90 min later. Compared with saline, both doses of arginine vasopressin significantly decreased lordosis responses to mounting and hop-dart proceptive behavior and trended toward significantly increasing agonistic behaviors. In experiment 2, oxytocin (2 microg) infusion just after arginine vasopressin (0.4 microg) significantly increased lordoses and decreased agonistic behaviors but did not affect hopping and darting. In experiment 3, conducted in ovariectomized rats primed with estradiol benzoate (1 microg/day s.c. x 2 days), i.c.v. infusion of 0.5 and 1.0 microg of the selective V1a antagonist, d(CH2)5Tyr-(Me)arginine vasopressin on day 3 significantly increased lordoses and trended toward increasing hopping and darting 4 and 6 h after i.c.v. treatment. In experiment 4, 1 microg of the selective oxytocin antagonist, d(CH2)5[Tyr(Me)2, Thr4, Tyr-NH2(9)]OVT given 1 h before d(CH2)5Tyr-(Me)arginine vasopressin (1 microg) significantly decreased lordoses. Previous studies indicate that arginine vasopressin contributes to light phase inhibition of female sexual behavior. Our findings suggest that arginine vasopressin may exert this effect through interactions that decrease oxytocin stimulation of sexual behavior and raise the question whether sex steroid conditions that stimulate sexual behavior may suppress central arginine vasopressin and V1a receptor activity.
以往的研究发现,中枢给予精氨酸加压素和精氨酸加压素受体V1a拮抗剂分别抑制和刺激接受性,但未研究对雌性性行为其他方面的影响。中枢催产素可促进性行为的求偶和接受成分,并减少针对雄性的攻击行为。本研究检测了脑室内给予精氨酸加压素和V1a拮抗剂对求偶、接受和攻击行为的影响,以及与催产素的相互作用。在实验1中,大鼠于第1、2天皮下注射2μg苯甲酸雌二醇,第3天注射500μg孕酮进行预处理。在孕酮处理后5小时给予精氨酸加压素(0.2、0.4μg)或生理盐水载体,并于30、60和90分钟后测量性行为和攻击行为。与生理盐水相比,两种剂量的精氨酸加压素均显著降低了对爬跨的脊柱前凸反应和跳跃-冲刺求偶行为,并呈现出显著增加攻击行为的趋势。在实验2中,在精氨酸加压素(0.4μg)注射后立即输注催产素(2μg)可显著增加脊柱前凸并减少攻击行为,但不影响跳跃和冲刺行为。在实验3中,对皮下注射苯甲酸雌二醇(1μg/天×2天)预处理的去卵巢大鼠,于第3天脑室内输注0.5和1.0μg选择性V1a拮抗剂d(CH2)5Tyr-(Me)精氨酸加压素,在脑室内给药后4和6小时显著增加了脊柱前凸,并呈现出增加跳跃和冲刺行为的趋势。在实验4中,在d(CH2)5Tyr-(Me)精氨酸加压素(1μg)给药前1小时给予1μg选择性催产素拮抗剂d(CH2)5[Tyr(Me)2, Thr4, Tyr-NH2(9)]OVT可显著降低脊柱前凸。以往的研究表明,精氨酸加压素有助于对雌性性行为的明相抑制。我们的研究结果表明,精氨酸加压素可能通过减少催产素对性行为的刺激的相互作用来发挥这种作用,并提出了刺激性行为的性类固醇条件是否可能抑制中枢精氨酸加压素和V1a受体活性的问题。
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