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血清素作为与铜运输相关的生物还原剂的潜在作用。

Potential role of serotonin as a biological reductant associated with copper transportation.

机构信息

Department of Pharmaceutical Sciences, International University of Health and Welfare, Kitakanemaru 2600-1, Otawara, Tochigi 324-8501, Japan.

Department of Pharmaceutical Sciences, International University of Health and Welfare, Kitakanemaru 2600-1, Otawara, Tochigi 324-8501, Japan.

出版信息

J Inorg Biochem. 2019 Oct;199:110770. doi: 10.1016/j.jinorgbio.2019.110770. Epub 2019 Jul 11.

DOI:10.1016/j.jinorgbio.2019.110770
PMID:31336257
Abstract

Serotonin (5-HT) is a neurotransmitter that is derived from tryptophan. Owing to a hydroxyl group attached to the indole nucleus, 5-HT exhibits a considerably higher redox activity than tryptophan. To gain insight into the biological relevance of the redox activity of 5-HT, the effect of Cu(I)-binding ligands on the 5-HT-mediated copper reduction was investigated. The d-d transition band of Cu(II) complexed with glycine [Cu(II)-Gly] was not affected by addition of 5-HT alone but was diminished when a thioether-containing compound coexists with 5-HT. Concomitant with disappearance of the d-d transition band of Cu(II)-Gly, the π-π* transition band of 5-hydroxyindole of 5-HT exhibits a red-shift which is consistently explained by oxidation of 5-HT and subsequent formation of a dimeric species. The redox reactions between 5-HT and copper are also accelerated by a peptide composed of a methionine (Met)-rich region in the extracellular domain of an integral membrane protein, copper transporter 1 (Ctr1). Since Ctr1 transports copper across the plasma membrane with specificity for Cu(I), reduction of extracellular Cu(II) to Cu(I) is required for copper uptake by Ctr1. Metalloreductases that can donate Cu(I) for Ctr1 have been identified in yeast but not yet been found in mammals. The results of this study indicate that the Met-rich region in the N-terminal extracellular domain of Ctr1 promotes the 5-HT-mediated Cu(II) reduction in order to acquire Cu(I) via a non-enzymatic process.

摘要

血清素(5-HT)是一种由色氨酸衍生而来的神经递质。由于吲哚核上连接了一个羟基,5-HT 的氧化还原活性比色氨酸高得多。为了深入了解 5-HT 氧化还原活性的生物学意义,研究了 Cu(I)结合配体对 5-HT 介导的铜还原的影响。与 5-HT 单独存在相比,当含有硫醚的化合物与 5-HT 共存时,与甘氨酸[Cu(II)-Gly]络合的 Cu(II)的 d-d 跃迁带没有受到影响,但会减弱。随着 Cu(II)-Gly 的 d-d 跃迁带的消失,5-HT 的 5-羟吲哚的π-π*跃迁带发生红移,这可以用 5-HT 的氧化和随后形成二聚体来解释。5-HT 和铜之间的氧化还原反应也被完整膜蛋白细胞外结构域中富含蛋氨酸(Met)的区域组成的肽加速,该肽是铜转运蛋白 1(Ctr1)。由于 Ctr1 特异性地将铜从质膜外向质膜内转运,因此需要将细胞外的 Cu(II)还原为 Cu(I),才能被 Ctr1 摄取。已经在酵母中鉴定出可以为 Ctr1 提供 Cu(I)的金属还原酶,但在哺乳动物中尚未发现。这项研究的结果表明,Ctr1 细胞外结构域 N 端富含 Met 的区域促进了 5-HT 介导的 Cu(II)还原,以便通过非酶促过程获得 Cu(I)。

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