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一种新型大麻素对大鼠丙戊酸自闭症模型的行为和转录组学影响。

Behavioral and transcriptomic effects of a novel cannabinoid on a rat valproic acid model of autism.

作者信息

Loomis Sally, Silva Diogo G, Savopoulos Ranjev, Cilia Jackie, Li Jennifer, Davis Mat D, Virley David, Foley Andrew, Loro Emanuele, McCreary Andrew C

机构信息

Jazz Pharmaceuticals Research UK Ltd., Cambridge, UK.

Jazz Pharmaceuticals Research UK Ltd., Cambridge, UK.

出版信息

Neuropharmacology. 2025 Aug 1;273:110450. doi: 10.1016/j.neuropharm.2025.110450. Epub 2025 Apr 3.

Abstract

Autism spectrum disorder (ASD) is a complex neurodevelopmental condition characterized by impaired social communication, restricted interests, repetitive behavior and irritability. Exposure to valproic acid (VPA) during pregnancy has been shown to increase the risk of autism in children and has led to the development of the in-utero VPA rat model that elicits neurodevelopmental autistic-like features. Offspring exhibit behavioral and neurobiological alterations modelling ASD symptoms. We performed a behavioral and molecular assessment in a rat in-utero VPA model treated with a novel botanical cannabinoid, JZP541. Male offspring from dams treated with VPA were tested acutely and sub-chronically with JZP541 (10, 30, or 100 mg/kg, intraperitoneally). A behavioral testing battery was performed, and brain frontal cortex and hippocampus used for RNA sequencing. In utero exposure to VPA resulted in progeny showing behavioral phenotypes characteristic of ASD. JZP541 attenuated these deficits in social, stereotypic, hyperactivity and irritability behavior in a dose-dependent fashion. VPA exposure was associated with a substantial transcriptional dysregulation impacting multiple key biological processes in a tissue-dependent manner. The expression profiles were integrated with publicly available datasets of autism-associated genes to support the validity of the model used and to focus on the effects of treatment on known autism-relevant transcriptional targets. This approach indicated a strong and dose-dependent reduction of the autism-associated gene expression signature in brain samples from animals dosed with JZP541. Our findings demonstrate JZP541 was able to ameliorate ASD associated behavioral deficits, and this was supported by improvements in putative transcriptional biomarkers of ASD.

摘要

自闭症谱系障碍(ASD)是一种复杂的神经发育疾病,其特征为社交沟通受损、兴趣受限、重复行为和易激惹。研究表明,孕期接触丙戊酸(VPA)会增加儿童患自闭症的风险,并由此建立了子宫内VPA大鼠模型,该模型可引发类似自闭症的神经发育特征。后代表现出模拟ASD症状的行为和神经生物学改变。我们在用新型植物大麻素JZP541治疗的子宫内VPA大鼠模型中进行了行为和分子评估。用VPA处理的母鼠所产雄性后代分别用JZP541(10、30或100mg/kg,腹腔注射)进行急性和亚慢性测试。进行了一系列行为测试,并将大脑额叶皮质和海马用于RNA测序。子宫内暴露于VPA导致后代出现ASD特征性的行为表型。JZP541以剂量依赖的方式减轻了社交、刻板、多动和易激惹行为方面的这些缺陷。VPA暴露与大量转录失调有关,这种失调以组织依赖的方式影响多个关键生物学过程。将表达谱与公开可用的自闭症相关基因数据集整合,以支持所用模型的有效性,并关注治疗对已知自闭症相关转录靶点的影响。这种方法表明,在给予JZP541的动物的脑样本中,自闭症相关基因表达特征有强烈且剂量依赖性的降低。我们的研究结果表明JZP541能够改善与ASD相关的行为缺陷,这得到了ASD假定转录生物标志物改善的支持。

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