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Spir-1肌动蛋白组织者突变小鼠中恐惧表达增强。

Enhanced fear expression in Spir-1 actin organizer mutant mice.

作者信息

Pleiser Sandra, Banchaabouchi Mumna Al, Samol-Wolf Annette, Farley Dominika, Welz Tobias, Wellbourne-Wood Joel, Gehring Isabell, Linkner Jörn, Faix Jan, Riemenschneider Markus J, Dietrich Susanne, Kerkhoff Eugen

机构信息

University Hospital Regensburg, Department of Neurology, Molecular Cell Biology Laboratory, Franz-Josef-Strauß-Allee 11, 93053 Regensburg, Germany.

European Molecular Biology Laboratory (EMBL), Mouse Biology Unit, Via Ramarini 32, 00015 Monterotondo, Italy; Campus Vienna Biocenter, CSF - Campus Science Support Facilities GmbH, Dr. Bohr-Gasse 7, 1020 Vienna, Austria.

出版信息

Eur J Cell Biol. 2014 May-Jun;93(5-6):225-37. doi: 10.1016/j.ejcb.2013.11.001. Epub 2013 Nov 20.

Abstract

Spir proteins nucleate actin filaments at vesicle membranes and facilitate intracellular transport processes. The mammalian genome encodes two Spir proteins, namely Spir-1 and Spir-2. While the mouse spir-2 gene has a rather broad expression pattern, high levels of spir-1 expression are restricted to the nervous system, oocytes, and testis. Spir-1 mutant mice generated by a gene trap method have been employed to address Spir-1 function during mouse development and in adult mouse tissues, with a specific emphasis on viability, reproduction, and the nervous system. The gene trap cassette disrupts Spir-1 expression between the N-terminal KIND domain and the WH2 domain cluster. Spir-1 mutant mice are viable and were born in a Mendelian ratio. In accordance with the redundant function of Spir-1 and Spir-2 in oocyte maturation, spir-1 mutant mice are fertile. The overall brain anatomy of spir-1 mutant mice is not altered and visual and motor functions of the mice remain normal. Microscopic analysis shows a slight reduction in the number of dendritic spines on cortical neurons. Detailed behavioral studies of the spir-1 mutant mice, however, unveiled a very specific and highly significant phenotype in terms of fear learning in male mice. In contextual and cued fear conditioning experiments the male spir-1 mutant mice display increased fear memory when compared to their control littermates. Our data point toward a particular function of the vesicle associated Spir-1 actin organizer in neuronal circuits determining fear behavior.

摘要

Spir蛋白在囊泡膜上使肌动蛋白丝成核,并促进细胞内运输过程。哺乳动物基因组编码两种Spir蛋白,即Spir-1和Spir-2。虽然小鼠spir-2基因具有相当广泛的表达模式,但spir-1的高表达水平仅限于神经系统、卵母细胞和睾丸。通过基因捕获方法产生的Spir-1突变小鼠已被用于研究Spir-1在小鼠发育过程中和成年小鼠组织中的功能,特别关注生存能力、繁殖和神经系统。基因捕获盒破坏了Spir-1在N端KIND结构域和WH2结构域簇之间的表达。Spir-1突变小鼠能够存活,并以孟德尔比例出生。鉴于Spir-1和Spir-2在卵母细胞成熟中具有冗余功能,Spir-1突变小鼠是可育的。Spir-1突变小鼠的整体脑解剖结构没有改变,其视觉和运动功能保持正常。显微镜分析显示皮质神经元上的树突棘数量略有减少。然而,对Spir-1突变小鼠的详细行为研究揭示,在雄性小鼠的恐惧学习方面存在一种非常特殊且高度显著的表型。在情境性和线索性恐惧条件反射实验中,与对照同窝小鼠相比,雄性Spir-1突变小鼠表现出增强的恐惧记忆。我们的数据表明,与囊泡相关的Spir-1肌动蛋白组织者在决定恐惧行为的神经回路中具有特定功能。

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