NANOMATERIALS-BASED SENSORS FOR PEROXYNITRITE DETECTION AND QUANTIFICATION

Kalil, Haitham Fawzy Mohamed

January 2017

No description available.

Chemistry

Peroxynitrite

Cyclic Voltammetry

Manganese functionalized graphene-hemin

Aniline selenide

Nanoanalytical Studies of Bacterial Adhesion to the Membrane of Endothelial Cells

Alhumaid, Haidar S.

January 2016

No description available.

Chemistry

Nanoanalytical study

Adhesion of bacteria

Endothelial cells

Nitric Oxide

Peroxynitrite

The Balance of Nitric Oxide and Peroxynitrite in the Heart Suring Organ Preservation

Kozak, Allyson Jill

January 2007

No description available.

Chemistry, Analytical

heart cold storage preservation

nitric oxide

peroxynitrite

Defense of Endothelial Cells Against Tumor Cell Adhesion-Crucial Role of Nitric Oxide and Peroxynitrite Balance

Liu, Feng

January 2007

No description available.

Chemistry, Analytical

nitric oxide

peroxynitrite

tumor cell adhesion

Macrophage Microbicidal Activity is Enhanced by Stressor-Exposure

Allen, Rebecca G.

06 January 2012

No description available.

Biomedical Research

Immunology

Stress

macrophage

bacterial killing

gut microbiota

peroxynitrite

Efeitos do tempol sobre a interação entre peroxinitrito/CO2 com albumina e macrófagos: inibição da nitração de tirosinas e da oxidação de cisteínas e amplificação da nitrosação de cisteínas / Effects of tempol on the interaction between peroxynitrite/CO2 with albumin and macrophages: Inhibition of the nitration of tyrosine and oxidation of cysteine and amplification of cysteine nitrosation

Fernandes, Denise de Castro

19 February 2004

O tempol (TP) tem se mostrado um eficiente protetor em modelos inflamatórios. Os mecanismos de proteção contra espécies reativas de oxigênio foi bastante estudado mas sua interação com espécies reativas de nitrogênio ainda permanece pouco explorada. Recentemente, propusemos que o TP re-direciona a nitração de fenol mediada por peroxintrito (PN)/CO2 para nitrosação, pela sua reação com o radical CO3•‾. O produto desta reação, o cátion oxamônio, oxidaria PN para O2 e •NO. Este último produziria uma espécie nitrosante (N2O3) pela reação com o radical derivado do PN, •NO2 [Bonini e col. (2002) Chem. Res. Tox. 15: 506]. Para examinar se este mecanismo poderia operar in vivo, estudamos os efeitos do TP na reatividade do PN/CO2 frente a albumina (BSA) e macrófagos. Os efeitos do TP se apresentaram dependentes de sua concentração e da concentração de Cys. Apesar do TP não se mostrar catalítico, ele inibiu a oxidação de Cys (20-50%) e nitração de Tyr (70-90%) da BSA e aumentou a nitrosação de Cys (200-400%). No caso dos macrófagos tratados com PN/CO2, o tempol também inibiu a nitração (90%) e aumentou a nitrosação (300%). Assim, em condições fisiológicas, concentrações sub-estequiométricas de TP seriam capazes de redirecionar a reatividade dos radicais derivados PN, de oxidação de Cys proteica e nitração de Tyr para nitrosação de Cys. Desta forma, o TP poderia inibir a injúria em inflamações. / Tempol has been shown to protect animals from oxidative stress conditions. Tempol\'s protective mechanisms against reactive oxygen species have been extensively studied but its interactions with reactive nitrogen species remain little explored. Recently, we proposed that tempol diverts peroxynitrite/CO2 mediated phenol nitration to nitrosation by reacting with CO3•‾ to produce tempol oxamonium cation that oxidizes peroxynitrite to O2 and •NO. The latter produces a nitrosating species by reacting with peroxynitrite-derived •NO2 [Bonini et al. (2002) Chem. Res. Toxicol. 15: 506]. To examine wether this mechanism operates in biological environments, we studied the effects of tempol on peroxynitrite/CO2 reactivity towards a protein, BSA, and cells, macrophages. Tempol\'s effects were dependent on its own and BSA-cys concentration. Although not a true catalyst, it inhibited BSA-cys oxydation (20-50%) and BSA-tyr nitration (70-90%) while increasing BSA-cys nitrosation (200-400%). In the case of macrophages treated with peroxynitrite/CO2, tempol also inhibited protein-tyr nitration (90%) and increased protein-cys nitrosation (300%). Then, under physiological conditions, a substoichiometric amount of tempol is able to divert peroxynitrite-derived radicais reactivity from protein-cys oxidation and protein-tyr nitration to protein-cys nitrosation. This may be the mechanism by wich tempol inhibits injury in inflammatory conditions.

Albumin (Interaction)

Albuminas (Interação)

Biochemistry

Bioquímica

BSA

BSA

Free radicals

Nitration

Nitration

Nitrosation

Nitrosation

Nitroxide

Nitroxide

Peroxynitrite

Peroxynitrite

Radicais livres

Tempol

Tempol

Efeitos do tempol sobre a interação entre peroxinitrito/CO2 com albumina e macrófagos: inibição da nitração de tirosinas e da oxidação de cisteínas e amplificação da nitrosação de cisteínas / Effects of tempol on the interaction between peroxynitrite/CO2 with albumin and macrophages: Inhibition of the nitration of tyrosine and oxidation of cysteine and amplification of cysteine nitrosation

Denise de Castro Fernandes

19 February 2004

O tempol (TP) tem se mostrado um eficiente protetor em modelos inflamatórios. Os mecanismos de proteção contra espécies reativas de oxigênio foi bastante estudado mas sua interação com espécies reativas de nitrogênio ainda permanece pouco explorada. Recentemente, propusemos que o TP re-direciona a nitração de fenol mediada por peroxintrito (PN)/CO2 para nitrosação, pela sua reação com o radical CO3•‾. O produto desta reação, o cátion oxamônio, oxidaria PN para O2 e •NO. Este último produziria uma espécie nitrosante (N2O3) pela reação com o radical derivado do PN, •NO2 [Bonini e col. (2002) Chem. Res. Tox. 15: 506]. Para examinar se este mecanismo poderia operar in vivo, estudamos os efeitos do TP na reatividade do PN/CO2 frente a albumina (BSA) e macrófagos. Os efeitos do TP se apresentaram dependentes de sua concentração e da concentração de Cys. Apesar do TP não se mostrar catalítico, ele inibiu a oxidação de Cys (20-50%) e nitração de Tyr (70-90%) da BSA e aumentou a nitrosação de Cys (200-400%). No caso dos macrófagos tratados com PN/CO2, o tempol também inibiu a nitração (90%) e aumentou a nitrosação (300%). Assim, em condições fisiológicas, concentrações sub-estequiométricas de TP seriam capazes de redirecionar a reatividade dos radicais derivados PN, de oxidação de Cys proteica e nitração de Tyr para nitrosação de Cys. Desta forma, o TP poderia inibir a injúria em inflamações. / Tempol has been shown to protect animals from oxidative stress conditions. Tempol\'s protective mechanisms against reactive oxygen species have been extensively studied but its interactions with reactive nitrogen species remain little explored. Recently, we proposed that tempol diverts peroxynitrite/CO2 mediated phenol nitration to nitrosation by reacting with CO3•‾ to produce tempol oxamonium cation that oxidizes peroxynitrite to O2 and •NO. The latter produces a nitrosating species by reacting with peroxynitrite-derived •NO2 [Bonini et al. (2002) Chem. Res. Toxicol. 15: 506]. To examine wether this mechanism operates in biological environments, we studied the effects of tempol on peroxynitrite/CO2 reactivity towards a protein, BSA, and cells, macrophages. Tempol\'s effects were dependent on its own and BSA-cys concentration. Although not a true catalyst, it inhibited BSA-cys oxydation (20-50%) and BSA-tyr nitration (70-90%) while increasing BSA-cys nitrosation (200-400%). In the case of macrophages treated with peroxynitrite/CO2, tempol also inhibited protein-tyr nitration (90%) and increased protein-cys nitrosation (300%). Then, under physiological conditions, a substoichiometric amount of tempol is able to divert peroxynitrite-derived radicais reactivity from protein-cys oxidation and protein-tyr nitration to protein-cys nitrosation. This may be the mechanism by wich tempol inhibits injury in inflammatory conditions.

Albuminas (Interação)

Bioquímica

BSA

Nitration

Nitrosation

Nitroxide

Peroxynitrite

Radicais livres

Tempol

Albumin (Interaction)

Biochemistry

BSA

Free radicals

Nitration

Nitrosation

Nitroxide

Peroxynitrite

Tempol

ROLE OF REACTIVE OXYGEN SPECIES PEROXYNITRITE IN TRAUMATIC SPINAL CORD INJURY

Xiong, Yiqin

01 January 2008

Peroxynitrite (PN, ONOO-), formed by nitric oxide radical (•NO) and superoxide radical (O2•-), plays an important role in post-traumatic oxidative damage. In the early work, we determined the temporal characteristics of PN-derived oxidative damage in a rat spinal cord injury (SCI) model. Our results showed 3-nitrotyrosine (3-NT), a specific marker for PN, rapidly accumulated at early time points (1 hr, 3 hrs), after when it plateaued and the high level was sustained to 1 week post injury. The co-localization of 3-NT and lipid peroxidation derived-4-HNE observed in immunohistochemistry indicates PN is involved in lipid peroxidative as well as protein nitrative damage. PN-oxidative damage exacerbates intracellular Ca2+ overload, which activates Ca2+ dependent calpain-mediated cytoskeletal protein (α-spectrin) degradation. The 145 kD fragments of α-spectrin (SBDP 145), which are specifically generated by calpain, increased dramatically as early as 1 hr after injury although the peak increase did not occur until 72 hrs post injury. The high level waned back toward sham level at one week post injury. We then carried out experiments to evaluate the beneficial effects of tempol, a scavenger of PN-derived radicals, following SCI. Three pathological events including PN-induced oxidative damage, mitochondrial dysfunction and cytoskeletal degradation were investigated. Immunoblotting and immunohistochemical studies indicated PN-mediated oxidative damage including protein nitration, protein oxidation and lipid peroxidation, were all reduced by a single dose of tempol (300mg/kg, i.p) after SCI. Spinal cord (SC) mitochondrial dysfunction in terms of the respiratory control ratio (RCR) significantly improved by both 150 mg/kg and 300 mg/kg tempol treatments. Moreover, calpain-mediated proteolysis was significantly decreased by tempol, with greater effects on calpain-specific SBDP 145 observed. Direct PN-scavenging effect of tempol was confirmed in vitro. Exposure of healthy SC mitochondria to SIN-1, a PN donor in vitro, impaired mitochondrial respiration in a dose-dependent manner. Tempol was able to protect mitochondria against SIN-1-induced damage by improving mitochondrial function and decreasing mitochondrial 3-NT formation. These findings strongly support the concept that PN is a crucial player in the secondary damage following SCI. And tempol, by scavenging PN-induced free radicals, provides a promising pharmocotherapeutic strategy for treating acute SCI.

Reactive Oxygen Species

Peroxynitrite

Tempol

Oxidative Damage

Spinal Cord Injury

Anatomy

Medical Neurobiology

Régulation de l'activation et de l'adhésion des leucocytes, des cellules endothéliales et des plaquettes par la protéine C-réactive

Khreiss, Tarek

January 2005

Thèse numérisée par la Direction des bibliothèques de l'Université de Montréal.

Protéine C-réactive

Neutrophile

Endothélium

Plaquette

Cytokines

Molécules d'adhésion

Peroxynitrite

Signal de transduction

Inflammation

Maladies coronaires aigües

Denitration in Colonic Smooth Muscle

Malick, Seemab

11 November 2009

Tyrosine nitration results in altered function of smooth muscle voltage-gated L-type calcium channel. We explored the possibility that smooth muscle contains denitrase activity to allow functional recovery of the calcium channel without requiring synthesis of new channel proteins. Following peroxynitrite treatment of mouse colonic smooth muscle strips, CaCl2 (1 mM)-induced smooth muscle contraction was significantly reduced by 67% (P ≤ 0.05), which reversed by approximately 86% upon periodic washing within 2 hr period (P ≤ 0.001). The effect of the c-Src kinase inhibitor, PP2, on muscle contraction was also restored after 2 hr post-peroxynitrite treatment consistent with the thesis that recovery from tyrosine nitration allows for tyrosine phosphorylation of the calcium channel. In addition, sodium orthovanadate prevented nitration-induced inhibition of muscle contraction by approximately 90%. Moreover, denitration of nitrated proteins was observed by western blots in smooth muscle cells over 2 hr. Since nitrotyrosine formation interferes with tyrosine kinase pathways involved in cell signaling, the presence of denitrase activity in smooth muscle cells may have profound and important effects in restoring the function of nitrated proteins involved in cell signaling processes.

L-type calcium channel

peroxynitrite

denitrase acitivity

Medical Pharmacology

Medical Sciences

Medicine and Health Sciences