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色胺酮,一种内源性非肽生物因子:综述其分子靶点、作用机制及对生物医学的影响。

Isatin, an endogenous nonpeptide biofactor: A review of its molecular targets, mechanisms of actions, and their biomedical implications.

机构信息

Department of Proteomic Research and Mass Spectrometry, Institute of Biomedical Chemistry, Moscow, Russia.

出版信息

Biofactors. 2018 Mar;44(2):95-108. doi: 10.1002/biof.1408. Epub 2018 Jan 16.

DOI:10.1002/biof.1408
PMID:29336068
Abstract

Isatin (indole-2,3-dione) is an oxidized indole. It is widely distributed in mammalian tissues and body fluids, where isatin concentrations vary significantly from <0.1 to > 10 µM. Isatin output is increased under conditions of stress. Exogenously administered isatin is characterized by low toxicity, mutagenicity, and genotoxicity in vivo. Cytotoxic effects of isatin on various cell cultures are usually observed at concentrations exceeding 100 µM. Binding of [ H]isatin to rat brain sections is consistent with its physiological concentrations. Proteomic analysis of mouse and rat brain isatin-binding proteins revealed about 90 individual proteins, which demonstrated significant interspecies differences (rat versus mouse). Certain evidence exist that redox state(s) and possibly other types of posttranslational modifications regulate affinity of target proteins to isatin. Recent data suggest that interacting with numerous intracellular isatin binding proteins, isatin can act as a regulator of complex protein networks in norm and pathology. Physiological concentrations of isatin in vitro inhibit monoamine oxidase B and natriuretic peptide receptor guanylate cyclase, higher (neuroprotective) concentrations (50-400 μM) cause apoptosis of various (including malignant tumor) cell lines and influence expression of certain apoptosis-related genes. Being administered in vivo, isatin exhibits various behavioral effects; it attenuates manifestations of MPTP-induced parkinsonism and tumor growth in experimental animal models. © 2017 BioFactors, 44(2):95-108, 2018.

摘要

色胺酮(吲哚-2,3-二酮)是一种氧化的吲哚。它广泛分布于哺乳动物组织和体液中,其浓度在<0.1 至>10 μM 之间变化显著。在应激条件下,色胺酮的产量会增加。外源性给予的色胺酮在体内具有低毒性、致突变性和遗传毒性。色胺酮对各种细胞培养物的细胞毒性作用通常在浓度超过 100 μM 时才会观察到。[H]色胺酮与大鼠脑切片的结合与其生理浓度一致。对小鼠和大鼠脑色胺酮结合蛋白的蛋白质组学分析显示,约有 90 种单一蛋白,这些蛋白显示出明显的种间差异(大鼠与小鼠)。有一定证据表明,氧化还原状态(和可能的其他类型的翻译后修饰)调节靶蛋白与色胺酮的亲和力。最近的数据表明,与许多细胞内色胺酮结合蛋白相互作用,色胺酮可以作为正常和病理条件下复杂蛋白质网络的调节剂。体外生理浓度的色胺酮抑制单胺氧化酶 B 和利钠肽受体鸟苷酸环化酶,更高浓度(神经保护作用,50-400 μM)会导致各种(包括恶性肿瘤)细胞系的凋亡,并影响某些与凋亡相关基因的表达。体内给予色胺酮后,可表现出多种行为效应;它可减轻 MPTP 诱导的帕金森病和实验动物模型中肿瘤生长的症状。

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