Domínguez-Salazar Emilio, Portillo Wendy, Baum Michael J, Bakker Julie, Paredes Raúl G
Centro de Neurobiologia, Universidad Nacional Autónoma de México, Qro. 76230, Querétaro, Mexico.
Physiol Behav. 2002 Mar;75(3):337-46. doi: 10.1016/s0031-9384(01)00674-6.
Many socially relevant odors are detected in rodent species by the vomeronasal organ and subsequently processed by the accessory olfactory system (AOS). We previously found that gonadectomized male and female rats treated in adulthood with testosterone propionate (TP) showed equivalent Fos responses in the AOS to odors derived from estrous females. Likewise, in contrast with numerous other mammalian species, gonadectomized female rats show surprisingly high levels of male-typical mounting behavior in response to adult TP. We tested the hypothesis that prenatal testosterone (T) exposure, acting via androgen receptors (ARs) or via estrogen receptors, masculinizes the AOS in rats of both sexes. Pregnant dams were treated with either the AR blocker, Flutamide, the aromatase inhibitor, 1,4,6-androstatriene-3,17-dione (ATD), or nothing (control) to assess the role of prenatal androgen and estradiol receptor activation, respectively, in this masculinization. Beginning at birth, male and female offspring were injected subcutaneously (sc) every other day with either ATD (pre- and neonatal ATD group) or oil vehicle (Flutamide and control groups) until postnatal Day 12. Subjects were gonadectomized as adults, hormonally treated and tested for different behaviors before having their AOS Fos responses to estrous female odors assessed. Prenatal treatment with Flutamide (but not ATD) significantly decreased anogenital distance and severely impaired intromissive and ejaculatory behaviors in males tested after TP replacement without disrupting mounting capacity in either sex. Pre- and neonatal treatment with ATD (but not Flutamide) enhanced lordosis responsiveness in males tested after sc injections of estradiol and progesterone, whereas these perinatal treatments had no effect on any aspect of masculine coital performance in either sex. After TP treatment, male and female control subjects preferred to approach a tethered stimulus female as opposed to a male, and prenatal Flutamide or perinatal ATD treatments did not modify this pattern of partner preference. Neuronal Fos responses to estrous odors were (as in previous studies) identical in the AOS of gonadectomized TP-treated control males and females. Prenatal Flutamide or perinatal ATD treatments failed to disrupt consistently this profile of Fos responses to estrous odors in the AOS of rats of either sex. These behavioral and neuroanatomical findings raise the possibility that the similar level of male-typical responsiveness to social odors that occurs in male and female rats after adult TP treatment results from nonsteroid-hormone-dependent, species-specific factors that act perinatally in the brains of rats of both sexes.
许多与社会行为相关的气味在啮齿动物中是由犁鼻器检测到的,随后由副嗅觉系统(AOS)进行处理。我们之前发现,成年后用丙酸睾酮(TP)处理的去势雄性和雌性大鼠,其AOS对来自发情期雌性的气味表现出同等的Fos反应。同样,与许多其他哺乳动物物种不同,去势雌性大鼠对成年TP会表现出令人惊讶的高水平雄性典型骑跨行为。我们测试了这样一个假设:产前睾酮(T)通过雄激素受体(ARs)或雌激素受体起作用,使两性大鼠的AOS雄性化。给怀孕的母鼠分别注射AR阻断剂氟他胺、芳香化酶抑制剂1,4,6 - 雄甾三烯 - 3,17 - 二酮(ATD)或不做处理(对照组),以分别评估产前雄激素和雌二醇受体激活在这种雄性化过程中的作用。从出生开始,雄性和雌性后代每隔一天皮下注射(sc)ATD(产前和新生儿期ATD组)或油剂载体(氟他胺和对照组),直到出生后第12天。成年后对实验对象进行去势,给予激素处理并测试不同行为,然后评估其AOS对发情期雌性气味的Fos反应。产前用氟他胺处理(而不是ATD)显著缩短了雄性的肛门与生殖器之间的距离,并严重损害了TP替代后测试的雄性的插入和射精行为,而对两性的骑跨能力均无影响。产前和新生儿期用ATD处理(而不是氟他胺)增强了皮下注射雌二醇和孕酮后测试的雄性的脊柱前凸反应性,而这些围产期处理对两性的雄性交配行为的任何方面均无影响。TP处理后,雄性和雌性对照实验对象更倾向于接近被拴住的雌性刺激物而非雄性,产前氟他胺或围产期ATD处理并未改变这种伴侣偏好模式。去势后经TP处理的对照雄性和雌性大鼠的AOS中,对发情期气味的神经元Fos反应(如先前研究)是相同的。产前氟他胺或围产期ATD处理未能持续破坏两性大鼠AOS中对发情期气味的这种Fos反应模式。这些行为和神经解剖学发现提出了一种可能性,即成年TP处理后雄性和雌性大鼠对社会气味的类似水平的雄性典型反应性,是由非甾体激素依赖性、物种特异性因素导致的,这些因素在两性大鼠出生时就已在其大脑中起作用。
