Sex-dependent role of hippocampal BDNF and GSK-3β in mediating PTSD-like behaviors in both sexes of adolescent rats exposed to fear conditioning, extinction, and reinstatement.

IF 1.6 4区 医学 Q4 NEUROSCIENCES
Sepideh Khazaei, Arezu Jabbari, Reihaneh Nakhaei-Zadeh, Morteza Moradzadeh, Sayeneh Khodadadi, Anahita Najafi, Salar Vaseghi
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Abstract

Evidence has shown the role of brain-derived neurotrophic factor (BDNF) and glycogen synthase kinase-3 beta (GSK-3β) in the pathophysiology of posttraumatic stress disorder (PTSD). The present research explored the role of BDNF and GSK-3β activity in behavioral alterations in adolescent rats exposed to fear conditioning, extinction, and reinstatement. Three footshocks (0.8 mA for 3 s paired with sound 75 dB, 3 s) were delivered to rats. Extinction was done 1 min, or 1 h, or 1 day, or 5 days after conditioning (sound broadcasted for 20 times with no footshocks, 75 dB, 3 s). Reinstatement (one footshock, 0.8 mA, 3 s, with no sound) was done 1 h after extinction. The results showed extinction + reinstatement only in females decreased PTSD-like behaviors (darting was observed only in females). Fear conditioning decreased locomotion and rearing in both sexes, while extinction + reinstatement increased locomotion more effectively in females and rearing only in females. Fear conditioning decreased BDNF and increased GSK-3β more effectively in females, while extinction + reinstatement increased BDNF and decreased GSK-3β more effectively in females. In conclusion, we showed that BDNF and GSK-3β activity in the hippocampus may be involved in behavioral changes induced by fear conditioning and extinction + reinstatement sessions in females. However, it seems that behavioral changes in males may not be directly related to the function of BDNF and GSK-3β, although due to the absence of protein assessment, this conclusion is made with great caution. Additionally, reinstatement may induce a more powerful effect in males, counteracting the potential therapeutic effects of extinction session.

海马BDNF和GSK-3β在青春期大鼠暴露于恐惧条件反射、消退和恢复中介导ptsd样行为中的性别依赖作用
有证据表明脑源性神经营养因子(BDNF)和糖原合成酶激酶-3β (GSK-3β)在创伤后应激障碍(PTSD)的病理生理中的作用。本研究探讨了BDNF和GSK-3β活性在暴露于恐惧条件反射、消退和恢复的青春期大鼠行为改变中的作用。对大鼠进行3次足震(0.8 mA, 3 s, 75 dB, 3 s)。在调理后1分钟、1小时、1天或5天进行消光(声音广播20次,无足震,75 dB, 3 s)。消失后1 h恢复(1次足震,0.8 mA, 3 s,无声音)。结果显示,消退+恢复仅在女性中减少了ptsd样行为(仅在女性中观察到跳跃)。恐惧条件反射减少了两性的运动和繁殖,而灭绝+恢复在雌性中更有效地增加了运动,并且只在雌性中繁殖。在雌性动物中,恐惧调节更有效地降低BDNF和增加GSK-3β,而灭绝+恢复更有效地增加BDNF和降低GSK-3β。综上所述,我们发现海马中BDNF和GSK-3β活性可能参与了女性恐惧条件反射和消退+恢复过程引起的行为改变。然而,男性的行为改变似乎与BDNF和GSK-3β的功能没有直接关系,尽管由于缺乏蛋白质评估,这一结论是非常谨慎的。此外,恢复可能在雄性中诱导更强大的效果,抵消了灭绝过程的潜在治疗效果。
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来源期刊
CiteScore
3.60
自引率
5.00%
发文量
228
审稿时长
1 months
期刊介绍: Founded in 1966, Experimental Brain Research publishes original contributions on many aspects of experimental research of the central and peripheral nervous system. The focus is on molecular, physiology, behavior, neurochemistry, developmental, cellular and molecular neurobiology, and experimental pathology relevant to general problems of cerebral function. The journal publishes original papers, reviews, and mini-reviews.
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