School of Basic Medical Sciences, Peking University Health Science Center, Beijing, China.
PLoS One. 2011;6(6):e21568. doi: 10.1371/journal.pone.0021568. Epub 2011 Jun 29.
Late-phase long term potentiation (L-LTP) is thought to be the cellular basis for long-term memory (LTM). While LTM as well as L-LTP is known to depend on transcription and translation, it is unclear why brain-derived neurotrophic factor (BDNF) could sustain L-LTP when protein synthesis is inhibited. The persistently active protein kinase ζ (PKMζ) is the only molecule implicated in perpetuating L-LTP maintenance. Here, in mouse acute brain slices, we show that inhibition of PKMζ reversed BDNF-dependent form of L-LTP. While BDNF did not alter the steady-state level of PKMζ, BDNF together with the L-LTP inducing theta-burst stimulation (TBS) increased PKMζ level even without protein synthesis. Finally, in the absence of de novo protein synthesis, BDNF maintained TBS-induced PKMζ at a sufficient level. These results suggest that BDNF sustains L-LTP through PKMζ in a protein synthesis-independent manner, revealing an unexpected link between BDNF and PKMζ.
晚期长时程增强(L-LTP)被认为是长时记忆(LTM)的细胞基础。虽然已知 LTM 以及 L-LTP 依赖于转录和翻译,但不清楚为什么在蛋白质合成受到抑制时,脑源性神经营养因子(BDNF)能够维持 L-LTP。持续活跃的蛋白激酶 ζ(PKMζ)是唯一与持续维持 L-LTP 有关的分子。在这里,在小鼠急性脑片中,我们表明抑制 PKMζ 逆转了 BDNF 依赖性的 L-LTP 形式。虽然 BDNF 不会改变 PKMζ 的稳态水平,但 BDNF 与诱导 L-LTP 的θ爆发刺激(TBS)一起增加了 PKMζ 的水平,即使没有蛋白质合成也是如此。最后,在没有新蛋白质合成的情况下,BDNF 以足够的水平维持 TBS 诱导的 PKMζ。这些结果表明,BDNF 通过 PKMζ 以不依赖于蛋白质合成的方式维持 L-LTP,揭示了 BDNF 和 PKMζ 之间的意外联系。
Zotero 插件
