Extensive Nitration of Protein Tyrosines in Human Atherosclerosis Detected by Immunohistochemistry

Beckmann, Jacques S.; Ye, Yao Zu; Anderson, Peter G.; Accavitti, Mary Ann; Tarpey, Margaret M.; White, C. Roger

doi:10.1515/bchm3.1994.375.2.81

Cited by 1,086 publications

(666 citation statements)

References 17 publications

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“…Peroxynitrite generation in vivo is being implicated in a wide range of human diseases, including atherosclerosis [13], lung disease [12], neurodegenerative disorders [9] and chronic inflammation [14,21]. Hence agents able to protect against ONOO--dependent damage may be therapeutically useful.…”

Section: Discussionmentioning

confidence: 99%

“…When tyrosine is exposed to ONOO-at physiological pH, nitration occurs [10,12,13,16,17]. compounds (GSH, DHLA and penicillamine) could prevent this nitration whereas the disulphides GSSG and penicillamine were much less effective.…”

Section: Inhibition Of Tyrosine Nitrationmentioning

confidence: 99%

“…Although nitric oxide (NO') has many important physiological functions [11], its production in excess may contribute to the pathology of neurodegenerative disease, chronic inflammation, acute respiratory distress syndrome, atherosclerosis and septic shock [9][10][11][12][13][14]. Part of the toxicity of NO" involves its reaction with superoxide radical (02 °-) to give peroxynitrite, ONOO-…”

Section: Introductionmentioning

confidence: 99%

“…In particular, addition of peroxynitrite to biological fluids leads to nitration of tyrosine residues, and the presence of these appears to be a 'marker' of peroxynitrite-dependent damage in vivo [10,[12][13][14][15][16]. Tyrosine nitration can interfere with signal transduction mechanisms involving phosphorylation/dephosphorylation [17].…”

Section: Introductionmentioning

confidence: 99%

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Protection against peroxynitrite‐dependent tyrosine nitration and α₁‐antiproteinase inactivation by oxidized and reduced lipoic acid

Whiteman

Tritschler²,

Halliwell

1996

FEBS Letters

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Peroxynitrite, formed by combination of superoxide radical with nitric oxide, is a reactive tissue-damaging species apparently involved in the pathology of several human diseases. Peroxynitrite nitrates tyrosine residues and inactivates vq-antiproteinase. We show that both lipoic acid and dihydrolipoic acid efficiently protect against damage by peroxynitrite. By contrast, other disulphides tested did not. The biological antioxidant effects of lipoateldihydrolipoate may involve scavenging of reactive nitrogen species as well as reactive oxygen species.

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Section: Discussionmentioning

confidence: 99%

Section: Inhibition Of Tyrosine Nitrationmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Protection against peroxynitrite‐dependent tyrosine nitration and α₁‐antiproteinase inactivation by oxidized and reduced lipoic acid

Whiteman

Tritschler²,

Halliwell

1996

FEBS Letters

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“…We therefore analyzed the aortic sections for nitrotyrosine expression by immunohistochemistry. 8,19 There was a significant increase in nitrotyrosine immunopositivity in the AAV/Neo-treated LDLR KO mice on HCD (vs ND-fed animals) ( Figure 7a). In sharp contrast, mice injected with AAV/hNetrin-1 showed only very low level of nitrotyrosine staining despite the HCD.…”

Section: Hnetrin-1 Delivery Is Associated With Lower Inflammationmentioning

confidence: 98%

Systemic human Netrin-1 gene delivery by adeno-associated virus type 8 alters leukocyte accumulation and atherogenesis in vivo

et al. 2010

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Atherosclerosis is an inflammatory disorder of arteries. Atherosclerotic plaque, in its early to intermediate stages, is composed largely of lipid-engorged foam cells. These foam cells are derived from the trafficking of monocytes (Mo) into the arterial intima, attracted to the site by chemoattractants. Given that foam cells are derived from the trafficking of Mo, the use of Netrin-1, an Mo chemorepellent, may be useful in limiting Mo accumulation and subsequent plaque formation. To investigate the potential of Netrin-1 for limiting atherosclerosis, we systemically delivered its human (h) cDNA by adeno-associated virus type 8 (AAV8, single-stranded structure) delivery into low-density lipoprotein receptor knockout (LDLRÀ/À) mice and placed the animals on a high cholesterol diet (HCD). Compared with control neomycin resistance (Neo) gene delivery/HCD, hNetrin-1 delivery resulted in a significant reduction in plaque formation, as determined by larger aortic lumen size, thinner intima-media thickness and lower blood velocity than the Neo/HCD control (all statistically significant). Indices of monocyte/macrophage (Mo/MF) accumulation, CD68, integrin, alpha M (ITGAM) and egf-like module containing, mucin-like, hormone receptor-like 1 (EMR-1), were reduced in hNetrin-1/HCD-treated animal's aortas and spleens compared with Neo/HCD-treated animals. Unexpectedly, CD25 and foxp3 (regulatory T cells (Tregs)) in the aorta were strongly upregulated. This is the first time the Mo/MF chemorepellent approach, and specific Netrin-1 gene delivery, has been performed for the reduction of Mo/MF burden and atherosclerosis. In addition, Netrin-1 has never before been linked to altered Treg levels. These data strongly suggest that hNetrin-1 gene delivery can reduce Mo/MF accumulation, inflammation and subsequent plaque formation.

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Association of Increased Immunostaining for Inducible Nitric Oxide Synthase and Nitrotyrosine With Fibroblast Growth Factor Transformation in Pancreatic Cancer

Vickers

MacMillan-Crow²,

Green³

et al. 1999

Arch Surg

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Extensive Nitration of Protein Tyrosines in Human Atherosclerosis Detected by Immunohistochemistry

Cited by 1,086 publications

References 17 publications

Protection against peroxynitrite‐dependent tyrosine nitration and α₁‐antiproteinase inactivation by oxidized and reduced lipoic acid

Protection against peroxynitrite‐dependent tyrosine nitration and α₁‐antiproteinase inactivation by oxidized and reduced lipoic acid

Systemic human Netrin-1 gene delivery by adeno-associated virus type 8 alters leukocyte accumulation and atherogenesis in vivo

Association of Increased Immunostaining for Inducible Nitric Oxide Synthase and Nitrotyrosine With Fibroblast Growth Factor Transformation in Pancreatic Cancer

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Extensive Nitration of Protein Tyrosines in Human Atherosclerosis Detected by Immunohistochemistry

Cited by 1,086 publications

References 17 publications

Protection against peroxynitrite‐dependent tyrosine nitration and α1‐antiproteinase inactivation by oxidized and reduced lipoic acid

Protection against peroxynitrite‐dependent tyrosine nitration and α1‐antiproteinase inactivation by oxidized and reduced lipoic acid

Systemic human Netrin-1 gene delivery by adeno-associated virus type 8 alters leukocyte accumulation and atherogenesis in vivo

Association of Increased Immunostaining for Inducible Nitric Oxide Synthase and Nitrotyrosine With Fibroblast Growth Factor Transformation in Pancreatic Cancer

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Resources

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Protection against peroxynitrite‐dependent tyrosine nitration and α₁‐antiproteinase inactivation by oxidized and reduced lipoic acid

Protection against peroxynitrite‐dependent tyrosine nitration and α₁‐antiproteinase inactivation by oxidized and reduced lipoic acid