青春期小白蛋白在左眼窝额叶皮层的表达影响雌性小鼠的社交能力

Yi-Seon Jeon, Daun Jeong, Hanseul Kweon, Jae-Hyun Kim, Choong Yeon Kim, Youngbin Oh, Young-Ho Lee, C. Kim, Sang-Gyu Kim, Jae-Woong Jeong, Eunjoon Kim, Seung-Hee Lee
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引用次数: 3

摘要

在哺乳动物中,青春期的社会经验对前额叶皮层的成熟至关重要。然而,仍然需要确定哪些皮质回路在这种经历中成熟,以及它如何以性别特定的方式塑造成人的社会行为。在这里,我们研究了雄性和雌性小鼠在断奶后的社会隔离(PWSI)后的社会接近行为,这种隔离剥夺了青春期的社会经验。我们发现,PWSI,特别是青春期后期的隔离,仅在雌性小鼠中导致社交方式(过度社交)的异常增加。我们进一步发现PWSI雌性小鼠左侧眶额皮质(OFCL)的小白蛋白(PV)表达降低。当我们测量雌性OFCL的神经活动时,大量的神经元在小鼠嗅闻其他小鼠(社交嗅闻)时比它们嗅闻物体(物体嗅闻)时表现出更高的活动。有趣的是,PWSI显著降低了雌性小鼠在社交嗅探过程中激活的神经元数量和活动水平。同样,在青春期后期,CRISPR/ cas9介导的OFCL中PV的下调通过降低PV+神经元的兴奋性和减少OFCL中的突触抑制,增强了成年雌性小鼠的社交能力,并减少了社交嗅觉诱导的活动。此外,光遗传学激活OFCL中的兴奋性神经元或光遗传学抑制PV+神经元可增强雌性小鼠的社交能力。我们的数据表明,青少年社会经验对OFCL中PV+抑制回路的成熟至关重要;这种成熟通过增强OFCL中的社会代表性来塑造女性的社会行为。在哺乳动物中,青春期的社会孤立常常改变成年后的社会行为。然而,我们并不完全了解社会隔离对性别的影响,以及调节这种变化的大脑区域和回路。在这里,我们发现青少年社会隔离导致雌性小鼠而非雄性小鼠出现三种异常表型:过度社交、左眼窝前额皮质(OFCL) PV+神经元减少和OFCL社交诱发活性降低。此外,体内OFCL中的小白蛋白(PV)缺失通过增加OFCL内的兴奋而不是抑制,在雌性小鼠中引起相同的表型。我们的数据表明,青春期的社会经验是OFCL中PV成熟所必需的,这对于激发塑造雌性小鼠社会行为的OFCL活动至关重要。
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Adolescent Parvalbumin Expression in the Left Orbitofrontal Cortex Shapes Sociability in Female Mice
The adolescent social experience is essential for the maturation of the prefrontal cortex in mammalian species. However, it still needs to be determined which cortical circuits mature with such experience and how it shapes adult social behaviors in a sex-specific manner. Here, we examined social-approaching behaviors in male and female mice after postweaning social isolation (PWSI), which deprives social experience during adolescence. We found that the PWSI, particularly isolation during late adolescence, caused an abnormal increase in social approaches (hypersociability) only in female mice. We further found that the PWSI female mice showed reduced parvalbumin (PV) expression in the left orbitofrontal cortex (OFCL). When we measured neural activity in the female OFCL, a substantial number of neurons showed higher activity when mice sniffed other mice (social sniffing) than when they sniffed an object (object sniffing). Interestingly, the PWSI significantly reduced both the number of activated neurons and the activity level during social sniffing in female mice. Similarly, the CRISPR/Cas9-mediated knockdown of PV in the OFCL during late adolescence enhanced sociability and reduced the social sniffing-induced activity in adult female mice via decreased excitability of PV+ neurons and reduced synaptic inhibition in the OFCL. Moreover, optogenetic activation of excitatory neurons or optogenetic inhibition of PV+ neurons in the OFCL enhanced sociability in female mice. Our data demonstrate that the adolescent social experience is critical for the maturation of PV+ inhibitory circuits in the OFCL; this maturation shapes female social behavior via enhancing social representation in the OFCL. SIGNIFICANCE STATEMENT Adolescent social isolation often changes adult social behaviors in mammals. Yet, we do not fully understand the sex-specific effects of social isolation and the brain areas and circuits that mediate such changes. Here, we found that adolescent social isolation causes three abnormal phenotypes in female but not male mice: hypersociability, decreased PV+ neurons in the left orbitofrontal cortex (OFCL), and decreased socially evoked activity in the OFCL. Moreover, parvalbumin (PV) deletion in the OFCL in vivo caused the same phenotypes in female mice by increasing excitation compared with inhibition within the OFCL. Our data suggest that adolescent social experience is required for PV maturation in the OFCL, which is critical for evoking OFCL activity that shapes social behaviors in female mice.
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