首页> 外文期刊>Behavioural Brain Research: An International Journal >Cellular prion protein regulates the motor behaviour performance and anxiety-induced responses in genetically modified mice.
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Cellular prion protein regulates the motor behaviour performance and anxiety-induced responses in genetically modified mice.

机译:细胞病毒蛋白调节转基因小鼠的运动行为表现和焦虑诱导反应。

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摘要

The cellular prion protein (PrP(C)) is a sialoglycoprotein involved in neuroplasticity processes and synaptic transmission. This study investigated behavioural responses (balance in the rota-rod test at 24 rpm, motility in the open-field test, anxiety in the elevated plus-maze test) in Zurich developed wild-type adult mice (WT, controls of normal PrP(C) expression), in knockout (KO) mice (Prnp(0/0), with no PrP(C) expression), and in PrP(C) overexpressing Tg-20 mice. After 8 min in the rota-rod test, Tg-20 animals presented significantly fewer falls (1.08+/-1.56 falls) than both WT (7.27+/-4.36) and KO (7.6+/-6.15) mice (p<0.01). In the open field test, Tg-20 animals showed significantly increased motility [rearing=23.4+/-7.85, crossing=97.30+/-32.11) when compared with KO mice (rearing=5.45+/-3.69 and crossing=59.73+/-15.43) or WT mice (rearing=6.5+/-20.23 and crossing=45.18+/-20.33) (p<0.01). In the elevated plus-maze test, Tg-20 mice showed less anxiety (head projections=7.3+/-1.62) when compared with WT animals (3.38+/-0.67) (p<0.05). Moreover, KO mice spent more time in the centre of the plus maze (37.80+/-5.57 s) than did WT mice (22.57+/-3.82) (p<0.05). PrP(C) overexpressing mice evoked increased motility, less anxiety, and increased equilibrium when compared with WT control animals in the behavioural protocols used. KO animals also tended to evoke fewer anxiety-related responses in the elevated plus-maze test. These findings indicate that the levels of PrP(C) in adult life are associated with possible changes in motility, anxiety, and equilibrium.
机译:细胞病毒蛋白(PrP(C))是一种唾液酸糖蛋白,参与神经可塑性过程和突触传递。这项研究调查了苏黎世开发的野生型成年小鼠(WT,正常PrP()对照)的行为反应(在24 rpm的旋转棒测试中保持平衡,在开放视野测试中具有运动性,在高迷宫测试中具有焦虑) C)表达),敲除(KO)小鼠(Prnp(0/0),无PrP(C)表达)和PrP(C)过表达的Tg-20小鼠。在旋转棒试验中8分钟后,Tg-20动物的跌倒(1.08 +/- 1.56跌倒)次数明显少于WT(7.27 +/- 4.36)和KO(7.6 +/- 6.15)小鼠(p <0.01) )。在野外试验中,与KO小鼠(饲养= 5.45 +/- 3.69和杂交= 59.73 + /)相比,Tg-20动物显示出显着提高的运动力(饲养= 23.4 +/- 7.85,杂交= 97.30 +/- 32.11)。 -15.43)或WT小鼠(饲养= 6.5 +/- 20.23和杂交= 45.18 +/- 20.33)(p <0.01)。在高迷迷宫测试中,与野生动物(3.38 +/- 0.67)相比,Tg-20小鼠表现出更少的焦虑感(头部投射= 7.3 +/- 1.62)(p <0.05)。此外,KO小鼠在迷宫中心花费的时间更长(37.80 +/- 5.57 s),比WT小鼠(22.57 +/- 3.82)更多(p <0.05)。与所使用的行为方案中的WT对照动物相比,PrP(C)过表达的小鼠诱发了增加的运动性,更少的焦虑和增加的平衡。在高迷宫测试中,KO动物也倾向于引起较少的焦虑相关反应。这些发现表明,成人生活中的PrP(C)水平与运动,焦虑和平衡的可能变化有关。

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