动情行为和中脑内 3α,5α-THP 水平被敲低动情前期大鼠中脑腹侧被盖区孕烷 X 受体表达所抑制。
Motivated behaviors and levels of 3α,5α-THP in the midbrain are attenuated by knocking down expression of pregnane xenobiotic receptor in the midbrain ventral tegmental area of proestrous rats.
机构信息
Department of Psychology, The University at Albany-SUNY, Albany, NY, USA.
出版信息
J Sex Med. 2013 Jul;10(7):1692-706. doi: 10.1111/jsm.12173. Epub 2013 May 1.
INTRODUCTION
Progesterone (P4 ) and its product, 5α-pregnan-3α-ol-20-one (3α,5α-THP), act in the midbrain ventral tegmental area (VTA) to alter motivated behaviors, such as mating, and motor and anxiety behavior. Of interest is whether 3α,5α-THP formation requires the pregnane xenobiotic receptor (PXR), which is expressed in the midbrain of rats.
AIM
The role of PXR in the midbrain for 3α,5α-THP formation, which precedes modulation of motivated behaviors, was investigated.
METHODS
Rats had estrous cycle phase determined and were assessed when they were in diestrus or proestrus. Diestrous and proestrous rats were infused with control or antisense oligodeoxyribonucleotides (AS-ODNs) targeted against PXR to the VTA.
MAIN OUTCOME MEASURES
In pilot studies, PXR gene and protein expression in the midbrain were determined with quantitative reverse transcriptase polymerase chain reaction and Western blotting, respectively. Diestrous and proestrous rats infused with control or AS-ODNs to the VTA were tested for anxiety (open field and plus maze), social (social interaction), and sexual (paced mating) behavior. Expression of PXR in the midbrain was verified with Western blotting. Plasma estradiol, P4 , dihydroprogesterone (DHP), and 3α,5α-THP levels, and brain P4 , DHP, and 3α,5α-THP levels were measured. We predicted that proestrous rats infused with PXR AS-ODNs would have decreased anti-anxiety, social, and sexual behavior, lower midbrain expression of PXR, and lower midbrain levels of 3α,5α-THP compared with controls.
RESULTS
Results supported the hypothesis that formation of 3α,5α-THP requires PXR and may be important for motivated behaviors. PXR AS-ODN, compared with control, infusions to the VTA reduced PXR expression and 3α,5α-THP levels in the midbrain and attenuated sexual receptivity of proestrous rats.
CONCLUSIONS
Knockdown of PXR in the midbrain reduces 3α,5α-THP levels and sexual receptivity of proestrous rats. Thus, PXR in the midbrain may be required for the observed increase in 3α-5α-THP during proestrus, which has subsequent effects on motivated, reproductive behaviors.
简介
孕激素(P4)及其产物 5α-孕烷-3α-醇-20-酮(3α,5α-THP)在中脑腹侧被盖区(VTA)发挥作用,改变动机行为,如交配、运动和焦虑行为。人们感兴趣的是,3α,5α-THP 的形成是否需要表达于大鼠中脑的孕烷 xenobiotic 受体(PXR)。
目的
研究 PXR 在中脑对于 3α,5α-THP 形成的作用,因为它先于动机行为的调节。
方法
确定大鼠动情周期阶段,并在它们处于动情前期或动情后期时进行评估。动情前期和动情后期大鼠接受 VTA 控制或针对 PXR 的反义寡核苷酸(AS-ODNs)输注。
主要观察指标
在初步研究中,使用定量逆转录聚合酶链反应和 Western blot 分别确定中脑的 PXR 基因和蛋白表达。接受 VTA 控制或 AS-ODNs 输注的动情前期和动情后期大鼠接受焦虑(旷场和加迷宫)、社交(社交互动)和性(定时交配)行为测试。用 Western blot 验证中脑 PXR 的表达。测量血浆雌二醇、P4、二氢孕酮(DHP)和 3α,5α-THP 水平,以及大脑 P4、DHP 和 3α,5α-THP 水平。我们预测,与对照组相比,接受 PXR AS-ODNs 输注的动情前期大鼠的抗焦虑、社交和性行为会减少,中脑 PXR 表达和中脑 3α,5α-THP 水平会降低。
结果
结果支持了 3α,5α-THP 的形成需要 PXR 并且可能对动机行为很重要的假设。与对照组相比,VTA 中的 PXR AS-ODN 输注降低了中脑的 PXR 表达和 3α,5α-THP 水平,并减弱了动情前期大鼠的性接受能力。
结论
中脑 PXR 的敲低降低了动情前期大鼠的 3α,5α-THP 水平和性接受能力。因此,中脑 PXR 可能是在动情前期观察到的 3α-5α-THP 增加所必需的,这对动机、生殖行为有后续影响。
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