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首页> 外文期刊>Developmental biology >Targeted disruption of the Pak5 and Pak6 genes in mice leads to deficits in learning and locomotion.
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Targeted disruption of the Pak5 and Pak6 genes in mice leads to deficits in learning and locomotion.

机译:小鼠中Pak5和Pak6基因的定向破坏会导致学习和运动能力下降。

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摘要

PAK6 is a member of the group B family of PAK serine/threonine kinases, and is highly expressed in the brain. The group B PAKs, including PAK4, PAK5, and PAK6, were first identified as effector proteins for the Rho GTPase Cdc42. They have important roles in filopodia formation, the extension of neurons, and cell survival. Pak4 knockout mice die in utero, and the embryos have several abnormalities, including a defect in the development of motor neurons. In contrast, Pak5 knockout mice do not have any noticeable abnormalities. So far nothing is known about the biological function of Pak6. To address this, we have deleted the Pak6 gene in mice. Since Pak6 and Pak5 are both expressed in the brain, we also generated Pak5/Pak6 double knockout mice. These mice were viable and fertile, but had several locomotor and behavioral deficits. Our results indicate that Pak5 and Pak6 together are not required for viability, but are required for a normal level of locomotion and activity as well as for learning and memory. This is consistent with a role for the group B PAKs in the nervous system.
机译:PAK6是PAK丝氨酸/苏氨酸激酶B组家族的成员,并在大脑中高度表达。首先将B组PAK(包括PAK4,PAK5和PAK6)鉴定为Rho GTPase Cdc42的效应蛋白。它们在丝状伪足形成,神经元扩展和细胞存活中具有重要作用。 Pak4基因敲除小鼠在子宫内死亡,胚胎有几种异常,包括运动神经元发育的缺陷。相比之下,Pak5基因敲除小鼠没有任何明显的异常。到目前为止,关于Pak6的生物学功能还一无所知。为了解决这个问题,我们删除了小鼠中的Pak6基因。由于Pak6和Pak5都在大脑中表达,因此我们还产生了Pak5 / Pak6双敲除小鼠。这些小鼠是活的和可育的,但是具有一些运动和行为缺陷。我们的结果表明,Pak5和Pak6在一起并不是生存力所必需的,但它们是正常水平的运动和活动以及学习和记忆所必需的。这与B组PAK在神经系统中的作用一致。

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