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Comprehensive behavioral analysis of voltage-gated calcium channel beta-anchoring and -regulatory protein knockout mice

机译:电压门控钙通道β锚定和调节蛋白敲除小鼠的综合行为分析

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Calcium (Ca2+) influx through voltage-gated Ca2+ channels (VGCCs) induces numerous intracellular events such as neuronal excitability, neurotransmitter release, synaptic plasticity, and gene regulation. It has been shown that genes related to Ca2+ signaling, such as the CACNA1C, CACNB2, and CACNA1I genes that encode VGCC subunits, are associated with schizophrenia and other psychiatric disorders. Recently, VGCC beta-anchoring and -regulatory protein (BARP) was identified as a novel regulator of VGCC activity via the interaction of VGCC β subunits. To examine the role of the BARP in higher brain functions, we generated BARP knockout (KO) mice and conducted a comprehensive battery of behavioral tests. BARP KO mice exhibited greatly reduced locomotor activity, as evidenced by decreased vertical activity, stereotypic counts in the open field test, and activity level in the home cage, and longer latency to complete a session in spontaneous T-maze alteration test, which reached “study-wide significance.” Acoustic startle response was also reduced in the mutants. Interestingly, they showed multiple behavioral phenotypes that are seemingly opposite to those seen in the mouse models of schizophrenia and its related disorders, including increased working memory, flexibility, prepulse inhibition, and social interaction, and decreased locomotor activity, though many of these phenotypes are statistically weak and require further replications. These results demonstrate that BARP is involved in the regulation of locomotor activity and, possibly, emotionality. The possibility was also suggested that BARP KO mice may serve as a unique tool for investigating the pathogenesis/pathophysiology of schizophrenia and related disorders. Further evaluation of the molecular and physiological phenotypes of the mutant mice would provide new insights into the role of BARP in higher brain functions.
机译:钙(Ca2 +)通过电压门控的Ca2 +通道(VGCC)流入会诱导许多细胞内事件,例如神经元兴奋性,神经递质释放,突触可塑性和基因调控。已经表明,与Ca 2+信号传导有关的基因,例如编码VGCC亚基的CACNA1C,CACNB2和CACNA1I基因与精神分裂症和其他精神疾病有关。最近,通过VGCCβ亚基的相互作用,VGCCβ锚定和调节蛋白(BARP)被确定为VGCC活性的新型调节剂。为了检查BARP在较高脑功能中的作用,我们生成了BARP基因敲除(KO)小鼠,并进行了一系列综合的行为测试。 BARP KO小鼠表现出极大的自发活动减少,这由垂直活动减少,开放视野测试中的刻板印象计数和家笼中的活动水平所证实,并且完成自发T迷宫改变测试的潜伏期更长,达到了“具有研究意义。”突变体中的惊吓声响应也降低了。有趣的是,他们表现出多种行为表型,似乎与精神分裂症及其相关疾病的小鼠模型相反,包括增加的工作记忆,柔韧性,前冲抑制和社交互动,以及运动能力下降,尽管这些表型中有许多是统计上较弱,需要进一步复制。这些结果表明,BARP参与了运动活动的调节,可能还参与了情绪调节。还提示了BARP KO小鼠可能是研究精神分裂症和相关疾病的发病机制/病理生理的独特工具。突变小鼠的分子和生理表型的进一步评估将提供新的见解BARP在更高的脑功能中的作用。

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