Metal-catalyzed Oxidation of Histidine in Human Growth Hormone

Zhao, Fang; Ghezzo-Schöneich, Elena; Aced, Gaby; Hong, Jinyang; Milby, Terry; Schöneich, Christian

doi:10.1074/jbc.272.14.9019

Cited by 109 publications

(61 citation statements)

References 47 publications

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“…This system was chosen because it generates both superoxide anions and hydroxyl radicals. The reaction mechanism has been described previously (27,28). The reaction proceeds faster at alkaline pH, but was carried out at pH 7.4 to lower the reaction rate.…”

Section: Binding Of Mouse Ec-sod To Hyaluronan Eah-sepharose-mentioning

confidence: 99%

Extracellular Superoxide Dismutase Inhibits Inflammation by Preventing Oxidative Fragmentation of Hyaluronan

Gao

Koenitzer

Tobolewski

et al. 2008

Journal of Biological Chemistry

162

133

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Extracellular superoxide dismutase (EC-SOD) is expressed at high levels in lungs. EC-SOD has a polycationic matrix-binding domain that binds to polyanionic constituents in the matrix. Previous studies indicate that EC-SOD protects the lung in both bleomycin-and asbestos-induced models of pulmonary fibrosis. Although the mechanism of EC-SOD protection is not fully understood, these studies indicate that EC-SOD plays an important role in regulating inflammatory responses to pulmonary injury. Hyaluronan is a polyanionic high molecular mass polysaccharide found in the extracellular matrix that is sensitive to oxidant-mediated fragmentation. Recent studies found that elevated levels of low molecular mass hyaluronan are associated with inflammatory conditions. We hypothesize that EC-SOD may inhibit pulmonary inflammation in part by preventing superoxide-mediated fragmentation of hyaluronan to low molecular mass fragments. We found that EC-SOD directly binds to hyaluronan and significantly inhibits oxidant-induced degradation of this glycosaminoglycan. In vitro human polymorphic neutrophil chemotaxis studies indicate that oxidative fragmentation of hyaluronan results in polymorphic neutrophil chemotaxis and that EC-SOD can completely prevent this response. Intratracheal injection of crocidolite asbestos in mice leads to pulmonary inflammation and injury that is enhanced in EC-SOD knock-out mice. Notably, hyaluronan levels are increased in the bronchoalveolar lavage fluid after asbestos-induced pulmonary injury, and this response is markedly enhanced in EC-SOD knock-out mice. These data indicate that inhibition of oxidative hyaluronan fragmentation probably represents one mechanism by which EC-SOD inhibits inflammation in response to lung injury.

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Section: Binding Of Mouse Ec-sod To Hyaluronan Eah-sepharose-mentioning

confidence: 99%

Extracellular Superoxide Dismutase Inhibits Inflammation by Preventing Oxidative Fragmentation of Hyaluronan

Gao

Koenitzer

Tobolewski

et al. 2008

Journal of Biological Chemistry

162

133

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“…Representative UV traces of peptide maps of native, NaOCl-and MPO-modified lipid-free apo A-I are shown in Figure 4. To identify tryptic fragments of native apo A-I, RP-HPLC separation was followed by online ESI-MS analyses in a first set of experiments, an analytical tool successfully applied to the identification of tryptic peptides obtained from digests of different proteins [35]. The residue number, sequence and observed molecular masses for the corresponding tryptic peptides of native apo A-I ( Figure 4A) are summarized in Table 2.…”

Section: Peptide Map and Ms Analyses Of Tryptic Fragments Of Native mentioning

confidence: 99%

Reagent or myeloperoxidase-generated hypochlorite affects discrete regions in lipid-free and lipid-associated human apolipoprotein A-I

Bergt

OETTL²,

Keller

et al. 2000

Biochem. J.

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“…It became known that the cytosolic SOD, Cu,ZnSOD (also known as SOD1) suffers oxidative modification by its product, hydrogen peroxide, a reaction potentially involving site-specifically formed hydroxyl radicals at the active site containing redox-active Cu II (Uchida & Kawakishi, 1994). This process leads to the formation of 2-oxo-His (structure 5), a characteristic product identified also for the in vitro metalcatalyzed oxidation of other proteins (Lewisch & Levine, 1995;Zhao et al, 1997). Interestingly, recent tandem mass spectrometry data show that for Cu,ZnSOD not the His residue bridging the redox-active Cu II and the structurally important Zn II ion is oxidized, but His residues only binding Cu II represent the predominant oxidation targets (Kurahashi et al, 2001).…”

Section: Cuzn Superoxide Dismutasementioning

confidence: 99%

Mass spectrometry in aging research

Schöneich

2004

Mass Spectrometry Reviews

Self Cite

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This review covers the application of mass spectrometric techniques to aging research. Modern proteomic strategies will be discussed as well as the targeted analysis of specific proteins for the correlation of post-translational modifications with protein function. Selected examples will show both the power and also current limitations of the respective techniques. Experimental results and strategies are discussed in view of current theories of the aging process. # 2004 Wiley Periodicals, Inc., Mass Spec Rev 24: [701][702][703][704][705][706][707][708][709][710][711][712][713][714][715][716][717][718] 2005

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Metal-catalyzed Oxidation of Histidine in Human Growth Hormone

Cited by 109 publications

References 47 publications

Extracellular Superoxide Dismutase Inhibits Inflammation by Preventing Oxidative Fragmentation of Hyaluronan

Extracellular Superoxide Dismutase Inhibits Inflammation by Preventing Oxidative Fragmentation of Hyaluronan

Reagent or myeloperoxidase-generated hypochlorite affects discrete regions in lipid-free and lipid-associated human apolipoprotein A-I

Mass spectrometry in aging research

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