TAAR1和5-HT1B受体激动剂可减轻产前暴露于丙戊酸的大鼠的自闭症样易怒性和攻击性。

IF 3.3 3区 心理学 Q1 BEHAVIORAL SCIENCES
Lien Wang , Erin A. Clark , Lynsey Hanratty , Kenneth S. Koblan , Andrew Foley , Nina Dedic , Linda J. Bristow
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引用次数: 0

摘要

尽管自闭症谱系障碍(ASD)的发病率不断上升,但针对其核心症状和相关症状的药物治疗仍有大量需求未得到满足。虽然一些非典型抗精神病药物已被批准用于控制相关的易激惹性和攻击性,但它们的使用受到大量副作用的限制。本研究首先旨在开发行为测量方法,以探索大鼠产前丙戊酸(VPA)ASD 模型中的挫折感、易激惹性和攻击性表型。此外,我们还研究了5-HT1B和TAAR1激动这两种新机制缓解这些行为的潜力。对暴露于产前 VPA 的雄性后代进行训练,使其在操作性任务中取得稳定的表现,然后在操作性挫折测试、刷瓶测试和常驻入侵者测试中进行药理评估。与对照组相比,暴露于 VPA 的大鼠表现出沮丧和易怒的行为,攻击性也有所增强。在操作试验过程中,先前经历过挫折事件的动物的易激惹行为和攻击性会进一步加剧。与车辆相比,单次给药 5-HT1B 激动剂 CP-94253 或 TAAR1 激动剂 RO5263397 可减轻挫折样行为。此外,这两种激动剂还能减少正常和挫折条件下的刺激样行为。CP-94253 在两种条件下都能减少常驻入侵者测试中的攻击行为,而 RO5263397 只对之前经历过挫折事件的大鼠产生影响。我们的研究描述了在大鼠产前 VPA ASD 模型中挫折感、易激惹性和攻击性这些以前未曾描述过的表型。给予选择性 TAAR1 或 5-HT1B 受体激动剂可减轻这些缺陷,因此有必要进一步探索这两种治疗 ASD 的靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
TAAR1 and 5-HT1B receptor agonists attenuate autism-like irritability and aggression in rats prenatally exposed to valproic acid

Despite the rising prevalence of autism spectrum disorder (ASD), there remains a significant unmet need for pharmacotherapies addressing its core and associative symptoms. While some atypical antipsychotics have been approved for managing associated irritability and aggression, their use is constrained by substantial side effects. This study aimed firstly to develop behavioral measures to explore frustration, irritability and aggression phenotypes in the rat prenatal valproic acid (VPA) model of ASD. Additionally, we investigated the potential of two novel mechanisms, 5-HT1B and TAAR1 agonism, to alleviate these behaviors. Male offspring exposed to prenatal VPA were trained to achieve stable performance on a cued operant task, followed by pharmacological assessment in an operant frustration test, bottle brush test and resident intruder test. VPA exposed rats demonstrated behaviors indicative of frustration and irritability, as well as increased aggression compared to controls. The irritability-like behavior and aggression were further exacerbated in animals previously experiencing a frustrative event during the operant test. Single administration of the 5-HT1B agonist CP-94253 or TAAR1 agonist RO5263397 attenuated the frustration-like behavior compared to vehicle. Additionally, both agonists reduced irritability-like behavior under both normal and frustrative conditions. While CP-94253 reduced aggression in the resident intruder test under both conditions, RO5263397 only produced effects in rats that previously experienced a frustrative event. Our study describes previously uncharacterized phenotypes of frustration, irritability, and aggression in the rat prenatal VPA model of ASD. Administration of selective TAAR1 or 5-HT1B receptor agonists alleviated these deficits, warranting further exploration of both targets in ASD treatment.

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来源期刊
CiteScore
6.40
自引率
2.80%
发文量
122
审稿时长
38 days
期刊介绍: Pharmacology Biochemistry & Behavior publishes original reports in the areas of pharmacology and biochemistry in which the primary emphasis and theoretical context are behavioral. Contributions may involve clinical, preclinical, or basic research. Purely biochemical or toxicology studies will not be published. Papers describing the behavioral effects of novel drugs in models of psychiatric, neurological and cognitive disorders, and central pain must include a positive control unless the paper is on a disease where such a drug is not available yet. Papers focusing on physiological processes (e.g., peripheral pain mechanisms, body temperature regulation, seizure activity) are not accepted as we would like to retain the focus of Pharmacology Biochemistry & Behavior on behavior and its interaction with the biochemistry and neurochemistry of the central nervous system. Papers describing the effects of plant materials are generally not considered, unless the active ingredients are studied, the extraction method is well described, the doses tested are known, and clear and definite experimental evidence on the mechanism of action of the active ingredients is provided.
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