CU(II)-catalyzed oxidation of Alzheimer's disease beta-amyloid peptide and related sequences: remarkably different selectivities of neurotoxic betaAP1-40 and non-toxic betaAP40-1.

Schoneich C; Williams TD

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CU(II)-catalyzed oxidation of Alzheimer's disease beta-amyloid peptide and related sequences: remarkably different selectivities of neurotoxic betaAP1-40 and non-toxic betaAP40-1.

机译：CU（II）催化的阿尔茨海默氏病β-淀粉样蛋白肽和相关序列的氧化：神经毒性betaAP1-40和非毒性betaAP40-1的选择性显着不同。

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We investigated the CuII-catalyzed oxidation of beta-amyloid peptides betaAP10-20 and betaAP40-1 by tandem mass spectrometry and compared oxidation yields and selectivities to those for betaAP1-16, betaAP1-28 and betaAP1-40, which were obtained earlier (26). While betaAP1-16, betaAP1-28 and betaAP1-40 showed an almost exclusive oxidation of His residues to 2-oxo-histidine, the selectivity pattern is changed for betaAP10-20,which shows oxidation of His but also hydroxylation of Tyr and Phe. In contrast to betaAP1-40, the reverse sequence betaAP40-1 shows a strong selectivity for the hydroxylation of Tyr31 while only negligible His oxidation is observed at early time points. These selectivity patterns show the importance of the geometry of the metal-binding site for peptide/protein oxidation. The significantly different characteristic of betaAP1-40 and betaAP40-1 with regard to metal catalyzed processes may be related to the differences in the neurotoxic properties of these sequences.

机译：我们通过串联质谱研究了CuII催化的β-淀粉样肽betaAP10-20和betaAP40-1的氧化，并将氧化产率和选择性与较早获得的betaAP1-16，betaAP1-28和betaAP1-40的氧化产率和选择性进行了比较（26 ）。虽然betaAP1-16，betaAP1-28和betaAP1-40几乎将His残基氧化为2-氧代组氨酸，但betaAP10-20的选择性模式却发生了变化，既显示His的氧化，也显示了Tyr和Phe的羟基化。与betaAP1-40相比，反向序列betaAP40-1对Tyr31的羟基化表现出很强的选择性，而在早期时间点仅观察到了可忽略的His氧化。这些选择性模式显示出金属结合位点的几何结构对于肽/蛋白质氧化的重要性。关于金属催化过程，betaAP1-40和betaAP40-1的显着不同的特征可能与这些序列的神经毒性特性的差异有关。

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《Cellular and molecular biology》 |2003年第5期|共9页
作者
Schoneich C; Williams TD;
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正文语种 eng
中图分类细胞生物学;分子生物学;
关键词
Oxidation; Peptides; Amyloid; Toxic effect; Metals; 肽类; 淀粉样蛋白; 金属;

机译：Oxidation;Peptides;Amyloid;Toxic effect;Metals;肽类;淀粉样蛋白;金属;

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1. CU(II)-catalyzed oxidation of Alzheimer's disease beta-amyloid peptide and related sequences: remarkably different selectivities of neurotoxic betaAP1-40 and non-toxic betaAP40-1. [J] . Schoneich C, Williams TD Cellular and molecular biology . 2003,第5期

机译：CU（II）催化的阿尔茨海默氏病β-淀粉样蛋白肽和相关序列的氧化：神经毒性betaAP1-40和非毒性betaAP40-1的选择性显着不同。
2. Cu(II)-catalyzed oxidation of beta-amyloid peptide targets His13 and His14 over His6: Detection of 2-Oxo-histidine by HPLC-MS/MS. [J] . Schoneich C, Williams TD Chemical research in toxicology . 2002,第5期

机译：Cu（II）催化β淀粉样肽靶向His13和His14超过His6的氧化：通过HPLC-MS / MS检测2-氧代组氨酸。
3. Vitamin B6s inhibit oxidative stress caused by Alzheimer's disease-related Cu(II)-beta-amyloid complexes-cooperative action of phospho-moiety. [J] . Hashim A, Wang L, Juneja K, Bioorganic and Medicinal Chemistry Letters . 2011,第21期

机译：维生素B6抑制由阿尔茨海默氏病相关的Cu（II）-β-淀粉样蛋白复合物-磷酸部分的协同作用引起的氧化应激。
4. Selective oxidation of ethylbenzene catalyzed by N-hydroxyphthalimide (NHPI) and ZSM-5 supported Co(II), Mn(II), Cu(II), Zn(II), Fe(III) with molecular oxygen under mild conditions (PPT) [C] . Lei Chen, Bindong Li, Dabin Li AIChE Annual Meeting . 2014

机译：在温和条件下用分子氧（PPT）的N-羟基苯二甲酰亚胺（NHPI）和ZSM-5负载的CO（II），Mn（II），Cu（III），Zn（II），Fe（III），Mn（II），Fe（III）催化的选择性氧化氧化
5. Amyloid beta-peptide (1-42)-mediated oxidative stress and neurotoxicity: I. The role of methionine 35. II. Proteomic identification of specifically oxidized proteins in models of Alzheimer's disease. [D] . Boyd-Kimball, Debra Lynn. 2004

机译：淀粉样β-肽（1-42）介导的氧化应激和神经毒性：I.蛋氨酸的作用35. II。蛋白质组学鉴定阿尔茨海默病模型中特定氧化的蛋白质。
6. Evidence of oxidative stress and in vivo neurotoxicity of beta-amyloid in a transgenic mouse model of Alzheimers disease: a chronic oxidative paradigm for testing antioxidant therapies in vivo. [O] . M. A. Pappolla, Y. J. Chyan, R. A. Omar, 1998

机译：在阿尔茨海默氏病转基因小鼠模型中β-淀粉样蛋白的氧化应激和体内神经毒性的证据：用于测试体内抗氧化剂疗法的慢性氧化范例。
7. A model for beta-amyloid aggregation and neurotoxicity based on free radical generation by the peptide: relevance to Alzheimer disease. [O] . Hensley, K, Carney, J M, Mattson, M P, 1994

机译：基于肽自由基产生的β-淀粉样蛋白聚集和神经毒性模型：与阿尔茨海默氏病相关。

CU(II)-catalyzed oxidation of Alzheimer's disease beta-amyloid peptide and related sequences: remarkably different selectivities of neurotoxic betaAP1-40 and non-toxic betaAP40-1.

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