成年 Fmr1 基因敲除小鼠的自发性癫痫发作:FVB.129P2-Pde6bTyrFmr1/J。
Spontaneous seizures in adult Fmr1 knockout mice: FVB.129P2-Pde6bTyrFmr1/J.
机构信息
Mercer University, College of Pharmacy, Department of Pharmaceutical Sciences, 3001 Mercer University Drive, Atlanta, GA 30341, USA.
Johns Hopkins University, Department of Chemical and Biomolecular Engineering, 3400 North Charles Street, Croft Hall B27, Baltimore, MD 21218, USA.
出版信息
Epilepsy Res. 2022 May;182:106891. doi: 10.1016/j.eplepsyres.2022.106891. Epub 2022 Mar 8.
The prevalence of seizures in individuals with fragile X syndrome (FXS) is ~25%; however, there are no reports of spontaneous seizures in the Fmr1 knockout mouse model of FXS. Herein, we report that 48% of adult (median age P96), Fmr1 knockout mice from our colony were found expired in their home cages. We observed and recorded adult Fmr1 knockout mice having spontaneous convulsions in their home cages. In addition, we captured by electroencephalography an adult Fmr1 knockout mouse having a spontaneous seizure-during preictal, ictal, and postictal phases-which confirmed the presence of a generalized seizure. We did not observe this phenotype in control conspecifics or in juvenile (age <P35) Fmr1 knockout mice. We hypothesized that chronic, random, noise perturbations during development caused the phenotype. We recorded decibels (dB) in our vivarium. The average was 61 dB, but operating the automatic door to the vivarium caused spikes to 95 dB. We modified the door to eliminate noise spikes, which reduced unexpected deaths to 33% in Fmr1 knockout mice raised from birth in this environment (P = 0.07). As the modifications did not eliminate unexpected deaths, we further hypothesized that building vibrations may also be a contributing factor. After installing anti-vibration pads underneath housing carts, unexpected deaths of Fmr1 knockout mice born and raised in this environment decreased to 29% (P < 0.01 compared to the original environment). We also observed significant sex effects, for example, after interventions to reduce sound and vibration, significantly fewer male, but not female, Fmr1 knockout mice died unexpectedly (P < 0.001). The spontaneous seizure phenotype in our Fmr1 knockout mice could serve as a model of seizures observed in individuals with FXS, potentially offering a new translationally-valid phenotype for FXS research. Finally, these observations, although anomalous, serve as a reminder to consider gene-environment interactions when interpreting data derived from Fmr1 knockout mice.
脆性 X 综合征 (FXS) 个体的癫痫发作患病率约为 25%;然而,在 FXS 的 Fmr1 基因敲除小鼠模型中尚无自发性癫痫发作的报道。在此,我们报告称,我们实验室中 48%的成年(中位数年龄 P96)Fmr1 基因敲除小鼠在其笼中死亡。我们观察并记录了成年 Fmr1 基因敲除小鼠在其笼中发生自发性惊厥。此外,我们通过脑电图捕捉到一只成年 Fmr1 基因敲除小鼠在发作前、发作中和发作后阶段发生自发性发作,这证实了全身性发作的存在。我们在对照组同窝仔鼠或幼年(<P35 年龄)Fmr1 基因敲除小鼠中未观察到这种表型。我们假设在发育过程中慢性、随机的噪声干扰导致了这种表型。我们在动物房中记录了分贝 (dB)。平均值为 61 dB,但打开动物房的自动门会导致噪声尖峰达到 95 dB。我们对门进行了修改以消除噪声尖峰,这使在这种环境中从出生起饲养的 Fmr1 基因敲除小鼠的意外死亡减少了 33%(P = 0.07)。由于这些修改并未消除意外死亡,我们进一步假设建筑物振动也可能是一个促成因素。在将防振垫安装在饲养箱下方后,在这种环境中出生和饲养的 Fmr1 基因敲除小鼠的意外死亡减少到 29%(与原始环境相比,P <0.01)。我们还观察到了显著的性别效应,例如,在减少声音和振动的干预措施后,明显减少了雄性但不是雌性 Fmr1 基因敲除小鼠的意外死亡(P <0.001)。我们的 Fmr1 基因敲除小鼠中自发性癫痫发作表型可作为 FXS 个体中观察到的癫痫发作的模型,可能为 FXS 研究提供新的具有转化意义的表型。最后,这些观察结果虽然异常,但提醒我们在解释源自 Fmr1 基因敲除小鼠的数据时要考虑基因-环境相互作用。
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