Instituto de Investigaciones Médicas Mercedes y Martín Ferreyra (INIMEC-CONICET-Universidad Nacional de Córdoba), Cordoba, Argentina.
Facultad de Psicología, Universidad Nacional de Córdoba, Cordoba, Argentina.
Psychopharmacology (Berl). 2022 Oct;239(10):3355-3366. doi: 10.1007/s00213-022-06228-z. Epub 2022 Sep 5.
Serotonin (5-HT) is a monoamine neuromodulator that plays a key role in the organization of the central nervous system. 5-HT alterations may be associated to the emergence of social deficits and psychiatric disorders, including anxiety, depression, and substance abuse disorders. Notably, disruption of the 5-HT system during sensitive periods of development seems to exert long-term consequences, including altered anxiety responses and problematic use of alcohol.
We analyzed, in mice, the effects of transient 5-HT depletion at gestation (a developmental stage when medial prefrontal cortex (mPFC) 5-HT levels depend exclusively on placental 5-HT availability) on 5-HT central synthesis and reuptake at weaning. We also explored if 5-HT disruption at the embryonic stage influences behavioral outcomes that may serve as a proxy for autistic- or anxiety-like phenotypes.
C57/BL6 male and female mice, born from dams treated with a 5-HT synthesis inhibitor (PCPA; 4-Chloro-DL-phenylalanine methyl ester hydrochloride) at gestational days (G)13.5-16.5, were subjected to a behavioral battery that assesses social preference and novelty, compulsive behavior, stereotypies, and ethanol's anti-anxiety effects, at postnatal days (P) 21-28. Afterwards, expression of the genes that encode for 5-HT synthesis (Tph2) and SERT (5-HT transporter) were analyzed in mPFC via real-time RT-PCR. Dopamine 2 receptor (D2R) expression was also analyzed via RT-PCR to further explore possible effects of PCPA on dopaminergic transmission.
Transient 5-HT disruption at G13.5-16.5 reduced Tph2 expression of both male and female mice in mPFC at P23. Notably, female mice also exhibited higher SERT expression and reduced D2R expression in mPFC. Mice derived from 5-HT depleted dams displayed heightened compulsive behavior at P21, when compared to control mice. Alcohol anti-anxiety effects at early adolescence (P28) were exhibited by mice derived from 5-HT depleted dams, but not by control counterparts. No social deficits or stereotyped behaviors were observed.
Transient 5-HT inhibition at gestation resulted in altered expression of genes involved in 5-HT synthesis and reuptake in mPFC at weaning, a period in which the 5-HT system is still developing. These alterations may exert lingering effects, which translate to significant compulsivity and heightened sensitivity to the anxiolytic effects of alcohol at early adolescence.
血清素(5-HT)是一种单胺类神经调质,在中枢神经系统的组织中起着关键作用。5-HT 的改变可能与社会缺陷和精神疾病的出现有关,包括焦虑、抑郁和物质滥用障碍。值得注意的是,5-HT 系统在发育敏感时期的中断似乎会产生长期后果,包括焦虑反应改变和酒精使用问题。
我们在小鼠中分析了妊娠期间(即中前额皮质(mPFC)5-HT 水平完全依赖胎盘 5-HT 可用性的发育阶段)短暂 5-HT 耗竭对断奶时中枢 5-HT 合成和再摄取的影响。我们还探讨了胚胎期 5-HT 中断是否会影响可能作为自闭症或焦虑样表型替代物的行为结果。
用 5-HT 合成抑制剂(PCPA;4-氯-DL-苯丙氨酸甲酯盐酸盐)处理妊娠第 13.5-16.5 天的母鼠所生的 C57/BL6 雄性和雌性小鼠,在出生后第 21-28 天进行行为测试,评估社交偏好和新奇感、强迫行为、刻板行为和乙醇的抗焦虑作用。之后,通过实时 RT-PCR 分析 5-HT 合成(Tph2)和 SERT(5-HT 转运体)基因的表达。通过 RT-PCR 还分析了多巴胺 2 受体(D2R)的表达,以进一步探索 PCPA 对多巴胺能传递的可能影响。
妊娠第 13.5-16.5 天短暂的 5-HT 耗竭减少了 P23 时雄性和雌性小鼠 mPFC 中的 Tph2 表达。值得注意的是,雌性小鼠的 SERT 表达也较高,mPFC 中的 D2R 表达降低。与对照小鼠相比,来自 5-HT 耗竭母鼠的小鼠在 P21 时表现出更高的强迫行为。在青春期早期(P28),来自 5-HT 耗竭母鼠的小鼠表现出酒精的抗焦虑作用,但对照母鼠没有。没有观察到社交缺陷或刻板行为。
妊娠期间短暂的 5-HT 抑制导致断奶时 mPFC 中 5-HT 合成和再摄取相关基因表达改变,此时 5-HT 系统仍在发育中。这些改变可能会产生持久的影响,导致青春期早期强迫行为显著增加和对酒精抗焦虑作用的敏感性增加。
