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米诺环素治疗可逆转脆性 X 综合征小鼠模型的超声发声产生缺陷。

Minocycline treatment reverses ultrasonic vocalization production deficit in a mouse model of Fragile X Syndrome.

机构信息

Neuroscience Graduate Program, University of California, Riverside, CA-92521, USA.

出版信息

Brain Res. 2012 Feb 23;1439:7-14. doi: 10.1016/j.brainres.2011.12.041. Epub 2011 Dec 31.

DOI:10.1016/j.brainres.2011.12.041
PMID:22265702
Abstract

Fragile X Syndrome (FXS) is the most common inherited form of intellectual disability, with behaviors characteristic of autism. Symptoms include abnormal social behavior, repetitive behavior, communication disorders, and seizures. Many symptoms of FXS have been replicated in the Fmr1 knockout (KO) mice. Whether Fmr1 KO mice exhibit vocal communication deficits is not known. By recording ultrasonic vocalizations (USV) produced by adult male mice during mating, we show that USV calling rate (number of calls/second) is reduced in Fmr1 KO mice compared to WT controls. The WT control and Fmr1 KO groups did not differ in other aspects of mating behavior such as time spent sniffing, mounting, rooting and without contact. Acoustic properties of calls such as mean frequency (in kHz), duration and dynamic range of frequencies were not different. This indicates a specific deficit in USV calling rate in Fmr1 KO mice. Previous studies have shown that treatment of Fmr1 KO mice with minocycline for 4weeks from birth can alleviate some behavioral symptoms. Here we tested if minocycline also reversed vocalization deficits in these mice. Calling rate increased and was similar to WT controls in adult Fmr1 KO mice treated with minocycline for four weeks from birth (P0-P28). All acoustic properties measured were similar in treated and untreated WT control mice indicating minocycline effects were specific to vocalizations in the Fmr1 KO mice. These data suggest that mating-related USVs are robust and relevant biomarkers of FXS, and that minocycline treatment is a promising avenue for treatment of FXS symptoms.

摘要

脆性 X 综合征 (FXS) 是最常见的遗传性智力障碍,其行为特征具有自闭症的特点。症状包括异常的社交行为、重复行为、沟通障碍和癫痫发作。许多 FXS 的症状在 Fmr1 敲除 (KO) 小鼠中得到了复制。Fmr1 KO 小鼠是否表现出声音沟通缺陷尚不清楚。通过记录成年雄性小鼠交配期间产生的超声发声 (USV),我们发现与 WT 对照组相比,Fmr1 KO 小鼠的 USV 发声率 (每秒叫声数) 降低。WT 对照组和 Fmr1 KO 组在其他交配行为方面没有差异,例如嗅探、交配、挖掘和无接触的时间。叫声的声学特性,如平均频率 (kHz)、持续时间和频率动态范围没有差异。这表明 Fmr1 KO 小鼠的 USV 发声率存在特定缺陷。先前的研究表明,从出生开始用米诺环素治疗 Fmr1 KO 小鼠 4 周可以缓解一些行为症状。在这里,我们测试了米诺环素是否也能逆转这些小鼠的发声缺陷。从出生到 28 天 (P0-P28) 接受米诺环素治疗的成年 Fmr1 KO 小鼠的发声率增加且与 WT 对照组相似。所有测量的声学特性在未经处理的 WT 对照组和经处理的 WT 对照组中均相似,表明米诺环素的作用是针对 Fmr1 KO 小鼠的发声。这些数据表明,与交配相关的 USV 是 FXS 的强大且相关的生物标志物,米诺环素治疗是治疗 FXS 症状的有前途的途径。

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