电邮这篇文章 The Production of Reactive Oxygen and Halogen Species by Neutrophils in Response to Monomeric Forms of Myeloperoxidase
- 作者: Gorudko I.V.1, Mikhalchik E.V.2, Sokolov A.V.2,3,4,5, Grigorieva D.V.1, Kostevich V.A.2,3, Vasilyev V.B.3,4, Cherenkevich S.N.1, Panasenko O.M.2
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隶属关系:
- Belarusian State University
- Federal Research and Clinical Center of Physical-Chemical Medicine
- Institute of Experimental Medicine
- St. Petersburg State University
- Center of Preclinical Translational Research
- 期: 卷 62, 编号 6 (2017)
- 页面: 919-925
- 栏目: Cell Biophysics
- URL: https://ogarev-online.ru/0006-3509/article/view/152447
- DOI: https://doi.org/10.1134/S0006350917060069
- ID: 152447
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详细
It was shown for the first time that myeloperoxidase, a homodimer that consists of two disulfidebonded identical protomers and catalyzes the formation of hypochlorous acid (HOCl), is decomposed by HOCl into monomers (MPO-Cl). Dimeric myeloperoxidase can also be converted into monomers (hemimyeloperoxidase) by reduction of the disulfide bond. In this study, the effects of two monomeric forms of myeloperoxidase, MPO-Cl and hemi-myeloperoxidase, and native dimeric myeloperoxidase on the production of reactive oxygen (•O2− and H2O2) and halogen (HOCl) species by neutrophils were compared. Neutrophil production of these species was monitored after addition of hemi-myeloperoxidase, MPO-Cl, or dimeric myeloperoxidase and also after the subsequent addition of activators, phorbol-12-myristate-13-acetate or N-formyl-Met-Leu-Phe. HOCl production was assessed by chemiluminescence in the presence of luminol; •O2− production was assessed by chemiluminescence in the presence of lucigenin and by cytochrome c reduction determined spectrophotometrically, and H2O2 production was measured using fluorimetry with scopoletin. The results indicate that MPO-Cl and hemi-myeloperoxidase, which can occur in blood under halogenative stress, do not prime neutrophil NADPH oxidase, and do not enhance the production of reactive oxygen (•O2− and H2O2) and halogen (HOCl) species.
作者简介
I. Gorudko
Belarusian State University
Email: o-panas@mail.ru
白俄罗斯, Minsk, 220030
E. Mikhalchik
Federal Research and Clinical Center of Physical-Chemical Medicine
Email: o-panas@mail.ru
俄罗斯联邦, Moscow, 119435
A. Sokolov
Federal Research and Clinical Center of Physical-Chemical Medicine; Institute of Experimental Medicine; St. Petersburg State University; Center of Preclinical Translational Research
Email: o-panas@mail.ru
俄罗斯联邦, Moscow, 119435; St. Petersburg, 197376; St. Petersburg, 199034; St. Petersburg, 197371
D. Grigorieva
Belarusian State University
Email: o-panas@mail.ru
白俄罗斯, Minsk, 220030
V. Kostevich
Federal Research and Clinical Center of Physical-Chemical Medicine; Institute of Experimental Medicine
Email: o-panas@mail.ru
俄罗斯联邦, Moscow, 119435; St. Petersburg, 197376
V. Vasilyev
Institute of Experimental Medicine; St. Petersburg State University
Email: o-panas@mail.ru
俄罗斯联邦, St. Petersburg, 197376; St. Petersburg, 199034
S. Cherenkevich
Belarusian State University
Email: o-panas@mail.ru
白俄罗斯, Minsk, 220030
O. Panasenko
Federal Research and Clinical Center of Physical-Chemical Medicine
编辑信件的主要联系方式.
Email: o-panas@mail.ru
俄罗斯联邦, Moscow, 119435
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