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二酰甘油激酶β在纹状体中等棘状神经元的突触周围位点积累。

Diacylglycerol kinase beta accumulates on the perisynaptic site of medium spiny neurons in the striatum.

作者信息

Hozumi Yasukazu, Fukaya Masahiro, Adachi Naoko, Saito Naoaki, Otani Koichi, Kondo Hisatake, Watanabe Masahiko, Goto Kaoru

机构信息

Department of Anatomy and Cell Biology, Yamagata University School of Medicine, Iida-nishi 2-2-2, Yamagata 990-9585, Japan.

出版信息

Eur J Neurosci. 2008 Dec;28(12):2409-22. doi: 10.1111/j.1460-9568.2008.06547.x.

Abstract

Following activation of Gq protein-coupled receptors, phospholipase C yields a pair of second messengers, i.e. diacylglycerol (DAG) and inositol 1,4,5-trisphosphate. The former activates protein kinase C and the latter mobilizes Ca(2+) from intracellular store. DAG kinase (DGK) then phosphorylates DAG to produce another second messenger (phosphatidic acid). Of 10 mammalian DGK isozymes, DGKbeta is expressed in dopaminergic projection fields with the highest level in the striatum and its particular splice variant is differentially expressed in patients with bipolar disorder. To gain molecular anatomical evidence for its signaling role, we investigated the cellular expression and subcellular localization of DGKbeta in the striatum of rat brain. DGKbeta was expressed in medium spiny neurons constituting the striatonigral and striatopallidal pathways, whereas striatal interneurons were below the detection threshold. DGKbeta was distributed in somatodendritic elements of medium spiny neurons and localized in association with the smooth endoplasmic reticulum and plasma membrane or in the narrow cytoplasmic space between them. In particular, DGKbeta exhibited dense accumulation at perisynaptic sites on dendritic spines forming asymmetrical synapses. The characteristic anatomical localization was consistent with exclusive enrichment of DGKbeta in the microsomal and postsynaptic density fractions. Intriguingly, DGKbeta was very similar in immunohistochemical and immunochemical distribution to Gq-coupled receptors, such as metabotropic glutamate receptors 1 and 5, and also to other downstream molecules involving DAG metabolism, such as phospholipase C beta and DAG lipase. These findings suggest that abundant DGKbeta is provided to perisynaptic sites of medium spiny neurons so that it can effectively produce phosphatidic acid upon activation of Gq-coupled receptors and modulate the cellular state of striatal output neurons.

摘要

Gq蛋白偶联受体激活后,磷脂酶C产生一对第二信使,即二酰基甘油(DAG)和肌醇1,4,5-三磷酸。前者激活蛋白激酶C,后者从细胞内储存库中释放Ca(2+)。然后二酰基甘油激酶(DGK)将DAG磷酸化以产生另一种第二信使(磷脂酸)。在10种哺乳动物DGK同工酶中,DGKβ在多巴胺能投射区域表达,在纹状体中水平最高,其特定的剪接变体在双相情感障碍患者中差异表达。为了获得其信号传导作用的分子解剖学证据,我们研究了大鼠脑纹状体中DGKβ的细胞表达和亚细胞定位。DGKβ在构成纹状体黑质和纹状体苍白球通路的中等棘状神经元中表达,而纹状体中间神经元低于检测阈值。DGKβ分布在中等棘状神经元的体树突成分中,并与光滑内质网和质膜相关联,或位于它们之间狭窄的细胞质空间中。特别是,DGKβ在形成不对称突触的树突棘的突触周围部位表现出密集积累。这种特征性的解剖定位与DGKβ在微粒体和突触后密度组分中的特异性富集一致。有趣的是,DGKβ在免疫组织化学和免疫化学分布上与Gq偶联受体(如代谢型谷氨酸受体1和5)以及其他涉及DAG代谢的下游分子(如磷脂酶Cβ和DAG脂肪酶)非常相似。这些发现表明,大量的DGKβ被提供给中等棘状神经元的突触周围部位,以便在Gq偶联受体激活时能够有效地产生磷脂酸并调节纹状体输出神经元的细胞状态。

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