氧化蛋白的作用是在体外氧化压力下调节血液中的kaspasa -3淋巴细胞。

IF 0.2 Q4 MEDICINE, GENERAL & INTERNAL
O. L. Nosareva, Ye. A. Stepovaya, N. V. Ryazantseva, Ye. V. Shakhristova, O. N. Vesnina, V. V. Novitsky
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引用次数: 2

摘要

氧化应激的形成是许多常见和重要的社会疾病的核心。血液淋巴细胞是提供机体免疫控制的细胞。由于其功能的实现,血液淋巴细胞与不同的内源性和外源性因子接触,从而导致活性氧产生激活,大分子氧化修饰和细胞存活改变。目前,扩大和深化对血液淋巴细胞凋亡调控特性的基础认识是十分必要的。本研究旨在探讨体外氧化应激时血淋巴细胞谷胱甘肽系统状态、羰基化水平、蛋白谷胱甘肽酰化与caspase-3活性变化之间的相互作用。材料和方法。研究的材料是在最终浓度为0.5 mmol的双氧水和/或蛋白质sh基团抑制剂N-乙基马来酰亚胺- 5 mmol,保护剂- 5 mmol - 1,4-二硫代赤四糖醇的条件下培养的血液淋巴细胞。用分光光度法测定还原性、氧化性和蛋白结合性谷胱甘肽浓度,并估计还原性与氧化性硫醇组分的比值大小。用酶免疫法测定蛋白质羰基衍生物的水平;用荧光光谱法测定Caspase-3活性。结果。体外氧化应激时血淋巴细胞sh -组阻断,蛋白结合谷胱甘肽浓度迅速下降,蛋白羰基衍生物含量和caspase-3活性增加。体外氧化应激时血淋巴细胞中蛋白sh组的保护伴随着蛋白结合谷胱甘肽和蛋白羰基衍生物浓度的升高。结论。研究表明,caspase-3和蛋白结合的谷胱甘肽是选择性控制程序性细胞死亡的分子靶点。体外氧化应激时外周血淋巴细胞caspase-3活性变化和蛋白结合谷胱甘肽浓度变化等指标可用于制定细胞凋亡失调疾病的靶向治疗方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
РОЛЬ ОКИСЛИТЕЛЬНОЙ МОДИФИКАЦИИ БЕЛКОВ В РЕДОКС-РЕГУЛЯЦИИ АКТИВНОСТИ КАСПАЗЫ-3 В ЛИМФОЦИТАХ КРОВИ ПРИ ОКИСЛИТЕЛЬНОМ СТРЕССЕ IN VITRO
The formation of oxidative stress lies at the heart of many frequent and socially-important diseases. Blood lymphocytes are the cells which provide immunological control of our organism. As a result of their function implementation blood lymphocytes contact with different endogenic and exogenic factors, which can lead to active oxygen species production activation, macromolecules oxidative modification and to cell survival alteration. At the present time it is essential to expand and deepen the fundamental knowledge of blood lymphocytes apoptosis regulation peculiarities. The research objective was to establish the interaction among alterations of glutathione system condition, carbonylation level, protein glutathionylation and caspase-3 activity in blood lymphocytes during oxidative stress in vitro. Material and Methods. The material for research was blood lymphocytes cultivated with addition of hydrogen peroxide in final concentration of 0,5 mmol and/or protein SH-group inhibitor N- ethylmaleimide – 5 mmol, protector – 5 mmol – 1,4-dithioerythritol. Reduced, oxidized and protein-bound glutathione concentration was measured by method of spectropho-tometry, additionally, the ratio size of reduced to oxidized thiol fraction was estimated. With help of enzymoimmunoassay the level of protein carbonyl derivatives was evaluated; caspase-3 activity was registered by spectrofluorometric method. Results . Protein SH-group blocking in blood lymphocytes during oxidative stress in vitro was accompanied by protein-bound glutathione concentration rapid decrease in connection with increase of protein carbonyl derivatives content and caspase-3 activity. Protein SH-group protection in blood lymphocytes during oxidative stress in vitro was accompanied by concentration increase of protein-bound glutathione and protein carbonyl derivatives under comparable values of enzyme activity under study. Conclusion . The carried out research shows that caspase-3 and protein-bound glutathione are the molecular targets of selective control over programmed cell death. The received indices of caspase-3 activity change and protein-bound glutathione concentration alteration in blood lymphocytes during oxidative stress in vitro can be used when elaborating target therapy approaches to diseases accompanied by apoptosis disregulation.
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来源期刊
Byulleten Sibirskoy Meditsiny
Byulleten Sibirskoy Meditsiny MEDICINE, GENERAL & INTERNAL-
CiteScore
0.70
自引率
50.00%
发文量
102
审稿时长
8 weeks
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