Limbic oxytocin receptor expression alters molecular signaling and social avoidance behavior in female prairie voles (Microtus ochrogaster)

Lina K. Nerio-Morales, A. J. Boender, L. J. Young, Marisol R. Lamprea, Adam S. Smith
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Abstract

The social defeat paradigm is the most representative animal model to study social anxiety disorder (SAD) and its underlying neuronal mechanisms. We have previously reported that defeat progressively reduces oxytocin receptors (OXTR) in limbic regions of the brain over an eight-week period in female prairie voles (Microtus ochrogaster). Oxytocin receptors activate the mitogen-activated protein kinase (MAPK) pathway, which has been previously associated with the anxiolytic effects of oxytocin. Here, we assessed the functional significance of OXTR in stress-induced social avoidance and the response of the MAPK signaling pathway in the nucleus accumbens (NAc), anterior cingulate cortex (ACC), and basolateral amygdala (BLA) of female prairie voles.In experiment 1, Sexually naïve adult female prairie voles were defeated for three consecutive days and tested a week after for social preference/avoidance (SPA) test. Control subjects were similarly handled without defeat conditioning. In experiment 2, sexually and stress naïve adult female prairie voles were bilaterally injected into the NAc, ACC, or the BLA with a CRISPR/Cas9 virus targeting the Oxtr coding sequence to induce OXTR knockdown. Two weeks post-surgery, subjects were tested for SPA behavior. Viral control groups were similarly handled but injected with a control virus. A subgroup of animals from each condition in both experiments were similarly treated and euthanized without being tested for SPA behavior. Brains were harvested for OXTR autoradiography, western blot analysis of MAPK proteins and quantification of local oxytocin content in the NAc, BLA, ACC, and PVN through ELISA.Social defeat reduced OXTR binding in the NAc and affected MAPK pathway activity and oxytocin availability. These results were region-specific and sensitive to exposure to the SPA test. Additionally, OXTR knockdown in the NAc, ACC, and BLA induced social avoidance and decreased basal MAPK activity in the NAc. Finally, we found that OXTR knockdown in these regions was associated with less availability of oxytocin in the PVN.Dysregulation of the oxytocin system and MAPK signaling pathway in the NAc, ACC, and BLA are important in social behavior disruptions in female voles. This dysregulation could, therefore, play an important role in the etiology of SAD in women.
肢端催产素受体的表达改变了雌性草原田鼠(Microtus ochrogaster)的分子信号传递和社会回避行为
社交失败范例是研究社交焦虑症(SAD)及其潜在神经元机制的最具代表性的动物模型。我们以前曾报道过,在为期八周的时间里,失败会逐渐减少雌性草原田鼠(Microtus ochrogaster)大脑边缘区域的催产素受体(OXTR)。催产素受体会激活丝裂原活化蛋白激酶(MAPK)通路,这与催产素的抗焦虑作用有关。在实验1中,我们评估了催产素受体在应激诱导的社交回避中的功能意义,以及MAPK信号通路在雌性草原田鼠的伏隔核(NAc)、前扣带回皮层(ACC)和基底外侧杏仁核(BLA)中的反应。对照组受试者的处理方法与此类似,但未进行失败条件反射。在实验 2 中,向性和应激均未受影响的成年雌性草原田鼠的 NAc、ACC 或 BLA 双侧注射靶向 Oxtr 编码序列的 CRISPR/Cas9 病毒,以诱导 OXTR 基因敲除。手术后两周,受试者接受 SPA 行为测试。病毒对照组的处理方法类似,但注射的是对照病毒。两项实验中每种情况下都有一个动物子组接受了类似的处理,并在未进行 SPA 行为测试的情况下安乐死。采集大脑进行 OXTR 自显影、MAPK 蛋白 Western 印迹分析,并通过 ELISA 对 NAc、BLA、ACC 和 PVN 中的催产素含量进行定量。这些结果具有区域特异性,并且对暴露于SPA测试很敏感。此外,在NAc、ACC和BLA中敲除OXTR会诱发社交回避,并降低NAc中MAPK的基础活性。最后,我们发现这些区域的 OXTR 基因敲除与 PVN 中催产素的可用性降低有关。因此,这种失调可能在女性 SAD 的病因中扮演重要角色。
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