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蛋白激酶 A 在嗅球中的增加可作为无条件刺激,并为并行记忆系统提供证据:将气味与增加的蛋白激酶 A 配对可产生中期和长期记忆,但不会产生短期记忆。

PKA increases in the olfactory bulb act as unconditioned stimuli and provide evidence for parallel memory systems: pairing odor with increased PKA creates intermediate- and long-term, but not short-term, memories.

机构信息

Division of BioMedical Sciences, Memorial University of Newfoundland, St. John's, NL, Canada A1B 3V6.

出版信息

Learn Mem. 2012 Feb 21;19(3):107-15. doi: 10.1101/lm.024489.111.

DOI:10.1101/lm.024489.111
PMID:22354948
Abstract

Neonatal odor-preference memory in rat pups is a well-defined associative mammalian memory model dependent on cAMP. Previous work from this laboratory demonstrates three phases of neonatal odor-preference memory: short-term (translation-independent), intermediate-term (translation-dependent), and long-term (transcription- and translation-dependent). Here, we use neonatal odor-preference learning to explore the role of olfactory bulb PKA in these three phases of mammalian memory. PKA activity increased normally in learning animals 10 min after a single training trial. Inhibition of PKA by Rp-cAMPs blocked intermediate-term and long-term memory, with no effect on short-term memory. PKA inhibition also prevented learning-associated CREB phosphorylation, a transcription factor implicated in long-term memory. When long-term memory was rescued through increased β-adrenoceptor activation, CREB phosphorylation was restored. Intermediate-term and long-term, but not short-term odor-preference memories were generated by pairing odor with direct PKA activation using intrabulbar Sp-cAMPs, which bypasses β-adrenoceptor activation. Higher levels of Sp-cAMPs enhanced memory by extending normal 24-h retention to 48-72 h. These results suggest that increased bulbar PKA is necessary and sufficient for the induction of intermediate-term and long-term odor-preference memory, and suggest that PKA activation levels also modulate memory duration. However, short-term memory appears to use molecular mechanisms other than the PKA/CREB pathway. These mechanisms, which are also recruited by β-adrenoceptor activation, must operate in parallel with PKA activation.

摘要

新生大鼠的气味偏好记忆是一种明确的依赖于 cAMP 的哺乳动物联想记忆模型。本实验室之前的工作表明,新生大鼠的气味偏好记忆有三个阶段:短期(不依赖翻译)、中期(依赖翻译)和长期(依赖转录和翻译)。在这里,我们使用新生大鼠的气味偏好学习来探索嗅球 PKA 在哺乳动物记忆的这三个阶段中的作用。在单次训练后 10 分钟,学习动物的 PKA 活性正常增加。用 Rp-cAMPs 抑制 PKA 会阻断中期和长期记忆,而对短期记忆没有影响。PKA 抑制也阻止了与学习相关的 CREB 磷酸化,这是一种与长期记忆有关的转录因子。当通过增加β-肾上腺素能受体激活来挽救长期记忆时,CREB 磷酸化得到恢复。通过在嗅球内使用 Sp-cAMPs 直接激活 PKA 来配对气味,可以产生中期和长期但不是短期的气味偏好记忆,Sp-cAMPs 绕过了β-肾上腺素能受体的激活。更高水平的 Sp-cAMPs 通过将正常的 24 小时保留时间延长至 48-72 小时,增强了记忆。这些结果表明,增加嗅球中的 PKA 对于诱导中期和长期气味偏好记忆是必要且充分的,并且表明 PKA 激活水平也调节记忆持续时间。然而,短期记忆似乎使用了不同于 PKA/CREB 途径的分子机制。这些机制也被β-肾上腺素能受体激活募集,必须与 PKA 激活并行运作。

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