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首页> 外文期刊>Neurobiology of Aging: Experimental and Clinical Research >Age-related defects in lifespan and learning ability in SAMP8 mice.
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Age-related defects in lifespan and learning ability in SAMP8 mice.

机译:SAMP8小鼠的寿命和学习能力与年龄有关的缺陷。

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Pertinent animal models of age-related learning deficiencies are required to elucidate the mechanism of age-related learning deficiencies and to develop novel therapeutic drugs for age-related diseases such as learning defects. Among many strains of accelerated senescence prone, senescence-accelerated mouse (SAM), SAMP8 mice have age-related defects in learning and cognitive abilities. We review recent findings on alterations in SAMP8 brain in neurochemical parameters related to neurotransmission and synaptic plasticity compared to those in SAMR1 brain as the control. In addition, we report the preventive effects of drugs on learning deficiencies in SAMP8 and discuss the usefulness of SAMP8 as an animal model of age-related learning deficiencies.
机译:需要与年龄相关的学习缺陷的相关动物模型,以阐明与年龄相关的学习缺陷的机制,并开发针对与年龄相关的疾病(例如学习缺陷)的新型治疗药物。在许多易于衰老的品系中,SAMP8小鼠在衰老和认知能力上具有与年龄相关的缺陷。我们回顾了最近的发现,与SAMR1脑作为对照相比,SAMP8脑中与神经传递和突触可塑性相关的神经化学参数发生了变化。此外,我们报告了药物对SAMP8学习缺陷的预防作用,并讨论了SAMP8作为与年龄相关的学习缺陷的动物模型的有用性。

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