Zhang Guo-Rong, Liu Meng, Cao Haiyan, Kong Lingxin, Wang Xiaodan, O'Brien Jennifer A, Wu Shuo-Chieh, Cook Robert G, Geller Alfred I
Department of Neurology, West Roxbury VA Hospital/Harvard Medical School, West Roxbury, MA 02132, USA.
Hippocampus. 2009 May;19(5):413-23. doi: 10.1002/hipo.20506.
Age-related decline in human cognition is well known, and there are correlative changes in the function of neocortical and hippocampal neurons. Similarly, age-related decline in learning has been observed in rodents, including deficits in a hippocampal-dependent learning paradigm, the Morris water maze. Furthermore, there are correlative deficits in specific signaling pathways, including protein kinase C (PKC) pathways, in cerebellar, hippocampal, or neocortical neurons. PKC pathways are strong candidates for mediating the molecular changes that underlie spatial learning, as they play critical roles in neurotransmitter release and synaptic plasticity, including long-term potentiation (LTP) and long-term depression (LTD), and deletion of specific PKC genes results in deficits in learning. Conversely, genetic activation of PKC pathways in small groups of hippocampal or cortical neurons enhances learning in specific paradigms. In this study, the authors delivered a constitutively active PKC into small groups of hippocampal dentate granule neurons in aged rats (using a herpes simplex virus-1 vector). Aged 2-year-old rats that received the constitutively active PKC displayed improved performance in the Morris water maze relative to controls in three different measures. These results indicate that PKC pathways play an important role in mediating spatial learning in aged rats. Additionally, these results represent a system for studying the neural mechanisms underlying aging-related learning deficits, and potentially developing gene therapies for cognitive and age-related deficits.
人类认知能力随年龄增长而下降是众所周知的,新皮质和海马体神经元的功能也会发生相应变化。同样,在啮齿动物中也观察到了与年龄相关的学习能力下降,包括在依赖海马体的学习范式——莫里斯水迷宫中的缺陷。此外,在小脑、海马体或新皮质神经元中,特定信号通路,包括蛋白激酶C(PKC)通路,也存在相应缺陷。PKC通路很可能介导了空间学习背后的分子变化,因为它们在神经递质释放和突触可塑性(包括长时程增强效应(LTP)和长时程抑制效应(LTD))中发挥着关键作用,而且特定PKC基因的缺失会导致学习缺陷。相反,在小群海马体或皮质神经元中对PKC通路进行基因激活可增强特定范式下的学习能力。在本研究中,作者(使用单纯疱疹病毒-1载体)将组成型活性PKC导入老年大鼠的小群海马齿状颗粒神经元中。接受组成型活性PKC的2岁老年大鼠在莫里斯水迷宫中的表现相对于对照组在三种不同测量指标上均有所改善。这些结果表明,PKC通路在介导老年大鼠的空间学习中起重要作用。此外,这些结果代表了一个用于研究衰老相关学习缺陷背后神经机制的系统,并且有可能开发针对认知和与年龄相关缺陷的基因疗法。