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Dlgap1基因敲除小鼠中强迫症样表型的晚期发展。

Late development of OCD-like phenotypes in Dlgap1 knockout mice.

作者信息

Minagawa Kimino, Hayakawa Takashi, Akimoto Hayato, Nagashima Takuya, Takahashi Yasuo, Asai Satoshi

机构信息

Division of Genomic Epidemiology and Clinical Trials, Clinical Trials Research Center, Nihon University School of Medicine, 30-1 Oyaguchi-Kamicho, Itabashi-ku, Tokyo, 173-8610, Japan.

Division of Pharmacology, Department of Biomedical Sciences, Nihon University School of Medicine, Tokyo, Japan.

出版信息

Psychopharmacology (Berl). 2025 Jan;242(1):215-231. doi: 10.1007/s00213-024-06668-9. Epub 2024 Aug 23.

Abstract

RATIONALE

Despite variants in the Dlgap1 gene having the two lowest p-value in a genome-wide association study of obsessive compulsive disorder (OCD), previous studies reported the absence of OCD-like phenotypes in Dlgap1 knockout (KO) mice. Since these studies observed behavioral phenotypes only for a short period, development of OCD-like phenotypes in these mice at older ages was still plausible.

OBJECTIVE

To examine the presence or absence of development of OCD-like phenotypes in Dlgap1 KO mice and their responsiveness to fluvoxamine.

METHODS AND RESULTS

Newly produced Dlgap1 KO mice were observed for a year. Modified SHIRPA primary screen in 2-month-old homozygous mutant mice showed only weak signs of anxiety, stress conditions and aggression. At older ages, however, these mutant mice exhibited excessive self-grooming characterized by increased scratching which led to skin lesions. A significant sex difference was observed in this scratching behavior. The penetrance of skin lesions reached 50% at 6-7 months of age and 90% at 12 months of age. In the open-field test performed just after the appearance of these lesions, homozygous mutant mice spent significantly less time in the center, an anxiety-like behavior, than did their wild-type and heterozygous littermates, none and less than 10% of which showed skin lesions at 1 year, respectively. The skin lesions and excessive self-grooming were significantly alleviated by two-week treatment with fluvoxamine.

CONCLUSION

Usefulness of Dlgap1 KO mice as a tool for investigating the pathogenesis of OCD-like phenotypes and its translational relevance was suggested.

摘要

理论依据

尽管在强迫症(OCD)的全基因组关联研究中,Dlgap1基因的变异具有两个最低的p值,但先前的研究报告称Dlgap1基因敲除(KO)小鼠不存在类似OCD的表型。由于这些研究仅在短时间内观察到行为表型,因此这些小鼠在老年时出现类似OCD的表型仍有可能。

目的

研究Dlgap1基因敲除小鼠是否会出现类似OCD的表型及其对氟伏沙明的反应。

方法与结果

对新产生的Dlgap1基因敲除小鼠进行了一年的观察。在2个月大的纯合突变小鼠中进行的改良SHIRPA初级筛查仅显示出轻微的焦虑、应激状态和攻击迹象。然而,在老年时,这些突变小鼠表现出过度的自我梳理行为,其特征是抓挠增加,导致皮肤损伤。在这种抓挠行为中观察到显著的性别差异。皮肤损伤的发生率在6 - 7个月龄时达到50%,在12个月龄时达到90%。在这些损伤出现后立即进行的旷场试验中,纯合突变小鼠在中央区域停留的时间明显少于野生型和杂合子同窝小鼠,这是一种类似焦虑的行为,野生型和杂合子同窝小鼠在1岁时分别没有和不到10%出现皮肤损伤。氟伏沙明治疗两周后,皮肤损伤和过度的自我梳理行为得到显著缓解。

结论

提示Dlgap1基因敲除小鼠作为研究类似OCD表型发病机制及其转化相关性的工具具有实用性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3c2c/11742909/6ab840e3e545/213_2024_6668_Figa_HTML.jpg

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