突触记忆和CaMKII。

IF 29.9 1区 医学 Q1 PHYSIOLOGY
Physiological reviews Pub Date : 2023-10-01 Epub Date: 2023-06-08 DOI:10.1152/physrev.00034.2022
Roger A Nicoll, Howard Schulman
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引用次数: 5

摘要

Ca2+/钙调蛋白依赖性蛋白激酶II(CaMKII)和长时程增强(LTP)是在十年内发现的,并且从那时起就密不可分。然而,就像许多婚姻一样,它也有起有落。基于CaMKII独特的生物化学性质,在与LTP形成任何生理连接之前,它被认为是一种记忆分子。然而,正如本文所述,CaMKII与突触生理和行为之间令人信服的联系花了几十年的时间。新技术在这一旅程中至关重要,包括体外脑切片、小鼠遗传学、单细胞分子遗传学、药理学试剂、蛋白质结构和双光子显微镜,以及被这一令人兴奋的挑战吸引的新研究人员。这篇综述追踪了这段旅程,并评估了40年后这段婚姻的状态。集体文献促使我们提出一个相对简单的突触记忆模型,包括以下驱动过程的步骤:1)Ca2+通过N-甲基-d-天冬氨酸(NMDA)受体进入激活CaMKII。2) CaMKII经历自身磷酸化,导致组成型、Ca2+非依赖性活性和NMDA受体亚基Glu22B结合位点的暴露。3) 活性CaMKII易位到突触后密度(PSD)并与GluN2B的细胞质C尾结合。4) CaMKII-GluN2B复合物引发PSD的结构重排,其可能涉及液-液相分离。5) 这种重排涉及PSD-95支架蛋白、α-氨基-3-羟基-5-甲基-4-异恶唑丙酸受体(AMPAR)及其跨膜AMPAR调节蛋白(TARP)辅助亚基,导致AMPAR在PSD中积累,这是突触增强的基础。6) 改性PSD的稳定性通过CaMKII-GluN2B复合物的稳定性来维持。7) 通过亚基交换或全酶间磷酸化的过程,CaMKII在面对CaMKII蛋白转换时保持突触增强。还有许多其他重要的蛋白质参与突触棘的扩大或驱动和维持增强的步骤的调节。在这篇综述中,我们批判性地讨论了每个步骤背后的数据。很明显,其中一些步骤比其他步骤更有根据,我们就如何加强或根据新数据替换支持这些步骤的证据提出了建议。尽管这是一段漫长的旅程,但对学习和记忆有详细的细胞和分子理解的前景就在眼前。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Synaptic memory and CaMKII.

Ca2+/calmodulin-dependent protein kinase II (CaMKII) and long-term potentiation (LTP) were discovered within a decade of each other and have been inextricably intertwined ever since. However, like many marriages, it has had its up and downs. Based on the unique biochemical properties of CaMKII, it was proposed as a memory molecule before any physiological linkage was made to LTP. However, as reviewed here, the convincing linkage of CaMKII to synaptic physiology and behavior took many decades. New technologies were critical in this journey, including in vitro brain slices, mouse genetics, single-cell molecular genetics, pharmacological reagents, protein structure, and two-photon microscopy, as were new investigators attracted by the exciting challenge. This review tracks this journey and assesses the state of this marriage 40 years on. The collective literature impels us to propose a relatively simple model for synaptic memory involving the following steps that drive the process: 1) Ca2+ entry through N-methyl-d-aspartate (NMDA) receptors activates CaMKII. 2) CaMKII undergoes autophosphorylation resulting in constitutive, Ca2+-independent activity and exposure of a binding site for the NMDA receptor subunit GluN2B. 3) Active CaMKII translocates to the postsynaptic density (PSD) and binds to the cytoplasmic C-tail of GluN2B. 4) The CaMKII-GluN2B complex initiates a structural rearrangement of the PSD that may involve liquid-liquid phase separation. 5) This rearrangement involves the PSD-95 scaffolding protein, α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptors (AMPARs), and their transmembrane AMPAR-regulatory protein (TARP) auxiliary subunits, resulting in an accumulation of AMPARs in the PSD that underlies synaptic potentiation. 6) The stability of the modified PSD is maintained by the stability of the CaMKII-GluN2B complex. 7) By a process of subunit exchange or interholoenzyme phosphorylation CaMKII maintains synaptic potentiation in the face of CaMKII protein turnover. There are many other important proteins that participate in enlargement of the synaptic spine or modulation of the steps that drive and maintain the potentiation. In this review we critically discuss the data underlying each of the steps. As will become clear, some of these steps are more firmly grounded than others, and we provide suggestions as to how the evidence supporting these steps can be strengthened or, based on the new data, be replaced. Although the journey has been a long one, the prospect of having a detailed cellular and molecular understanding of learning and memory is at hand.

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来源期刊
Physiological reviews
Physiological reviews 医学-生理学
CiteScore
56.50
自引率
0.90%
发文量
53
期刊介绍: Physiological Reviews is a highly regarded journal that covers timely issues in physiological and biomedical sciences. It is targeted towards physiologists, neuroscientists, cell biologists, biophysicists, and clinicians with a special interest in pathophysiology. The journal has an ISSN of 0031-9333 for print and 1522-1210 for online versions. It has a unique publishing frequency where articles are published individually, but regular quarterly issues are also released in January, April, July, and October. The articles in this journal provide state-of-the-art and comprehensive coverage of various topics. They are valuable for teaching and research purposes as they offer interesting and clearly written updates on important new developments. Physiological Reviews holds a prominent position in the scientific community and consistently ranks as the most impactful journal in the field of physiology.
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