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抽动秽语综合征纹状体去抑制大鼠模型中的频繁发声和深部脑刺激反应性运动障碍

Frequent vocalizations and deep brain stimulation-responsive hyperkinesia in a striatal disinhibition rat model for Tourette syndrome.

作者信息

Sagalajev Boriss, Lennartz Lina, Mokhtari Niloofar, Szpak Mikolaj, Uyar Meryem Sinem, Schüller Thomas, Baldermann Juan Carlos, Andrade Pablo, Visser-Vandewalle Veerle, Sesia Thibaut

机构信息

Department of Stereotactic and Functional Neurosurgery, Faculty of Medicine and University Hospital Cologne, University of Cologne, Cologne, Germany.

Mental Health and Neuroscience Research Institute (MHeNs), European Graduate School of Neuroscience (EURON), Maastricht University, Maastricht, Netherlands.

出版信息

Int J Neuropsychopharmacol. 2025 Jul 23;28(7). doi: 10.1093/ijnp/pyaf039.

Abstract

BACKGROUND

The lack of a rodent model for both motor and phonic tics hinders research on deep brain stimulation (DBS) for refractory Tourette syndrome (TS). Striatal disinhibition with a gamma-aminobutyric acid A antagonist (bicuculline) was previously shown to induce hyperkinesia and vocalizations in monkeys, indicating its potential as a TS model. In rats, however, only hyperkinesia was validated, prompting us to investigate whether they can also develop abnormal vocalizations and whether both conditions respond to thalamic DBS.

METHODS

Rats underwent surgical implantation of a unilateral guide cannula targeting the caudate putamen (CPu) or nucleus accumbens (NAc). Additionally, they were implanted with an ipsilateral stimulation electrode targeting the border between the central medial (CM) and ventrolateral (VL) thalamic nuclei. Motor changes and ultrasound vocalizations were recorded and characterized offline.

RESULTS

CPu bicuculline elicited arrhythmic shoulder jerks that tend to appear in fading bursts and sporadically alternate with sustained generalized hyperextension. Nucleus accumbens bicuculline elicited similar hyperkinesia, but at a much lower dose to prevent convulsions. DBS of CM/VL, but not adjacent regions, attenuated hyperkinesia with lower intensity showing stronger effects. In addition, bicuculline in NAc, but not CPu, elicited nonsensical vocalizations. However, the effect of CM/VL DBS on vocalizations remained inconclusive.

CONCLUSIONS

Hyperkinesia temporal features, co-development with vocalizations, and responsiveness to CM/VL DBS suggest striatal disinhibition may serve as a TS rat model. However, other movement disorders with vocal complications cannot be excluded, given the challenge of validating key tic indicators in animals, such as premonitory urge and suppressibility.

摘要

背景

缺乏一种同时具有运动性和发声性抽动的啮齿动物模型阻碍了对难治性抽动秽语综合征(TS)进行深部脑刺激(DBS)的研究。先前研究表明,用γ-氨基丁酸A拮抗剂(荷包牡丹碱)抑制纹状体可诱导猴子出现运动亢进和发声,这表明其有作为TS模型的潜力。然而,在大鼠中,仅证实了运动亢进,这促使我们研究它们是否也会出现异常发声,以及这两种情况是否对丘脑DBS有反应。

方法

大鼠接受手术,单侧植入靶向尾状壳核(CPu)或伏隔核(NAc)的引导套管。此外,它们还被同侧植入靶向中央内侧(CM)和腹外侧(VL)丘脑核边界的刺激电极。记录运动变化和超声发声,并在离线状态下进行特征分析。

结果

向CPu注射荷包牡丹碱会引发无节律的肩部抽搐,这些抽搐往往以逐渐减弱的阵发形式出现,并偶尔与持续的全身性过度伸展交替出现。向伏隔核注射荷包牡丹碱会引发类似的运动亢进,但剂量要低得多以防止惊厥。刺激CM/VL而非相邻区域可减轻运动亢进,强度较低时效果更强。此外,向NAc而非CPu注射荷包牡丹碱会引发无意义的发声。然而,CM/VL DBS对发声的影响仍无定论。

结论

运动亢进的时间特征、与发声的共同发展以及对CM/VL DBS的反应表明,纹状体抑制可能作为一种TS大鼠模型。然而,鉴于在动物中验证关键抽动指标(如预感冲动和可抑制性)具有挑战性,不能排除其他伴有发声并发症的运动障碍。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c0bf/12284881/76f4f13e40b5/pyaf039f1.jpg

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