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脑内核苷再循环的分子机制。

Molecular mechanisms of nucleoside recycling in the brain.

机构信息

Dipartimento di Biologia, Unità di Biochimica, Università di Pisa, Via San Zeno, 51, 56127 Pisa, Italy.

出版信息

Int J Biochem Cell Biol. 2011 Jan;43(1):140-5. doi: 10.1016/j.biocel.2010.10.007. Epub 2010 Oct 23.

Abstract

A major role of plasma membrane bound ectonucleotidases is the modulation of ATP, ADP, adenosine (the purinergic agonists), UTP, and UDP (the pyrimidinergic agonists) availability in the extracellular space at their respective receptors. We have recently shown that an ATP driven uridine-UTP cycle is operative in the brain, based on the strictly compartmentalized processes of uridine salvage to UTP and uridine generation from UTP, in which uptaken uridine is anabolized to UTP in the cytosol, and converted back to uridine in the extracellular space by the action of ectonucleotidases (Ipata et al. Int J Biochem Cell Biol 2010;42:932-7). In this paper we show that a similar cytidine-CTP cycle exists in rat brain. Since (i) brain relies on imported preformed nucleosides for the synthesis of nucleotides, RNA, nuclear and mitochondrial DNA, coenzymes, pyrimidine sugar- and lipid-conjugates and (ii) no specific pyrimidinergic receptors have been identified for cytidine and their nucleotides, our results, taken together with previous studies on the intra- and extracellular metabolic network of ATP, GTP, UTP, and their nucleosides in the brain (Barsotti and Ipata. Int J Biochem Cell Biol 2004;36:2214-25; Balestri et al. Neurochem Int 2007;50:517-23), strongly suggest that, apart from the modulation of ligand availability, ectonucleotidases may serve the process of local nucleoside recycling in the brain.

摘要

质膜结合的核苷酸外切酶的一个主要作用是调节细胞外空间中 ATP、ADP、腺苷(嘌呤能激动剂)、UTP 和 UDP(嘧啶能激动剂)在各自受体中的可用性。我们最近表明,基于尿苷回收至 UTP 和 UTP 生成尿苷的严格区室化过程,在脑中有一个由 ATP 驱动的尿苷-UTP 循环,其中摄取的尿苷在细胞质中被代谢为 UTP,并通过核苷酸外切酶的作用在细胞外空间中转化回尿苷(Ipata 等人,国际生化细胞生物学杂志 2010;42:932-7)。在本文中,我们表明类似的胞嘧啶-CMP 循环存在于大鼠脑中。由于 (i) 脑依赖于输入的预先形成的核苷来合成核苷酸、RNA、核和线粒体 DNA、辅酶、嘧啶糖和脂质缀合物,以及 (ii) 尚未为胞嘧啶及其核苷酸鉴定出特异性的嘧啶能受体,因此我们的结果与之前关于脑内 ATP、GTP、UTP 及其核苷的细胞内和细胞外代谢网络的研究相结合(Barsotti 和 Ipata,国际生化细胞生物学杂志 2004;36:2214-25;Balestri 等人,神经化学国际 2007;50:517-23),强烈表明除了调节配体的可用性外,核苷酸外切酶可能还服务于脑内局部核苷再循环的过程。

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