PERFORM Publications

Keyword search (4,163 papers available)

Title		Authors	PubMed ID
1	Modeling CH sub 3 /sub SOH-aromatic complexes to probe cysteine sulfenic acid-aromatic interactions in proteins	Orabi EA; English AM;	40994121 CHEMBIOCHEM
2	Modeling predicts facile release of nitrite but not nitric oxide from the thionitrate CH3SNO2 with relevance to nitroglycerin bioactivation	Parmar V; Orabi EA; English AM; Peslherbe GH;	39738238 CERMM
3	Theoretical evidence that Cu(I) complexation promotes degradation of S-nitrosothiols	Toubin C; Yeung DY; English AM; Peslherbe GH;	12475301 CERMM
4	Effective simulations of gas diffusion through kinetically accessible tunnels in multisubunit proteins: O2 pathways and escape routes in T-state deoxyhemoglobin	Shadrina MS; English AM; Peslherbe GH;	22690872 CERMM
5	Structural determination and anticholinesterase assay of C-glycosidic ellagitannins from Lawsonia inermis leaves: A study supported by DFT calculations and molecular docking	Orabi MAA; Orabi EA; Abdel-Sattar ES; English AM; Hatano T; Elimam H;	36423882 CHEMBIOCHEM
6	Modeling Shows that Rotation about the Peroxide O-O Bond Assists Protein and Lipid Functional Groups in Discriminating between H2O2 and H2O	Orabi EA; English AM;	33356279 CHEMBIOCHEM
7	Sublethal Paraquat Confers Multidrug Tolerance in Pseudomonas aeruginosa by Inducing Superoxide Dismutase Activity and Lowering Envelope Permeability.	Martins D, McKay GA, English AM, Nguyen D	33101252 CHEMBIOCHEM
8	Ctt1 catalase activity potentiates antifungal azoles in the emerging opportunistic pathogen Saccharomyces cerevisiae.	Martins D, Nguyen D, English AM	31235707 CHEMBIOCHEM
9	Derivatization of yeast cytochrome c peroxidase with pentaammineruthenium(III).	Fox T, English AM, Gibbs BF	8199229 CHEMBIOCHEM
10	Mass spectral analysis of protein-based radicals using DBNBS. Nonradical adduct formation versus spin trapping.	Filosa A, English AM	11262405 CHEMBIOCHEM
11	Heme nitrosylation of deoxyhemoglobin by s-nitrosoglutathione requires copper.	Romeo AA, Capobianco JA, English AM	11970954 CHEMBIOCHEM
12	S-nitrosation of Ca(2+)-loaded and Ca(2+)-free recombinant calbindin D(28K) from human brain.	Tao L, Murphy ME, English AM	11994015 CHEMBIOCHEM
13	Different pathways of radical translocation in yeast cytochrome c peroxidase and its W191F mutant on reaction with H(2)O(2) suggest an antioxidant role.	Tsaprailis G, English AM	12589560 CHEMBIOCHEM
14	Mechanism of S-nitrosation of recombinant human brain calbindin D28K.	Tao L, English AM	12641465 CHEMBIOCHEM
15	Quantitative analysis of the yeast proteome by incorporation of isotopically labeled leucine.	Jiang H, English AM	12645890 CHEMBIOCHEM
16	Scavenging with TEMPO* to identify peptide- and protein-based radicals by mass spectrometry: advantages of spin scavenging over spin trapping.	Wright PJ, English AM	12848573 CHEMBIOCHEM
17	ESI-MS and FTIR studies of the interaction between the second PDZ domain of hPTP1E and target peptides.	Papp R, Ekiel I, English AM	12870871 CHEMBIOCHEM
18	Superoxide dismutase targets NO from GSNO to Cysbeta93 of oxyhemoglobin in concentrated but not dilute solutions of the protein.	Romeo AA, Capobianco JA, English AM	14624585 CHEMBIOCHEM
19	Protein S-glutathiolation triggered by decomposed S-nitrosoglutathione.	Tao L, English AM	15049710 CHEMBIOCHEM
20	Mass spectrometric analysis of nitroxyl-mediated protein modification: comparison of products formed with free and protein-based cysteines.	Shen B, English AM	16229492 CHEMBIOCHEM
21	Hemoglobin S-nitrosation on oxygenation of nitrite/deoxyhemoglobin incubations is attenuated by methemoglobin.	Laterreur J, English AM	17889368 CHEMBIOCHEM
22	ESI-MS quantitation of iron as its 4-(2-pyridylazo)resorcinol (PAR) complex: application to pharmaceutical tablets containing iron oxide pigment.	Susanto D, English AM, Sharma R, Kwong E	21520348 CHEMBIOCHEM
23	SOD1 oxidation and formation of soluble aggregates in yeast: relevance to sporadic ALS development.	Martins D, English AM	24936435 CHEMBIOCHEM
24	Targeted proteomics identify metabolism-dependent interactors of yeast cytochrome c peroxidase: implications in stress response and heme trafficking.	Kathiresan M, English AM	26980054 CHEMBIOCHEM
25	Expanding the range of binding energies and oxidizability of biologically relevant S-aromatic interactions: imidazolium and phenolate binding to sulfoxide and sulfone	Orabi EA; English AM;	31214677 CHEMBIOCHEM
26	Evaluation of D10-Leu metabolic labeling coupled with MALDI-MS analysis in studying the response of the yeast proteome to H2O2 challenge	Jiang H; English AM;	17022625 CBAMS
27	Reduction and S-nitrosation of the neuropeptide oxytocin: implications for its biological function	Roy JF; Chrétien MN; Woodside B; English AM;	17692543 CBAMS
28	LC-MS/MS suggests that hole hopping in cytochrome c peroxidase protects its heme from oxidative modification by excess H2O2.	Kathiresan M, English AM	28451256 CHEMBIOCHEM
29	LC-MS/MS Proteoform Profiling Exposes Cytochrome c Peroxidase Self-Oxidation in Mitochondria and Functionally Important Hole Hopping from Its Heme	Kathiresan M; English AM;	30145880 CHEMBIOCHEM
30	Predicting structural and energetic changes in Met-aromatic motifs on methionine oxidation to the sulfoxide and sulfone	Orabi EA; English AM;	30168822 CHEMBIOCHEM
31	Superoxide dismutase activity confers (p)ppGpp-mediated antibiotic tolerance to stationary-phase Pseudomonas aeruginosa.	Martins D, McKay G, Sampathkumar G, Khakimova M, English AM, Nguyen D	30201715 CHEMBIOCHEM

Title:	LC-MS/MS Proteoform Profiling Exposes Cytochrome c Peroxidase Self-Oxidation in Mitochondria and Functionally Important Hole Hopping from Its Heme
Authors:	Kathiresan M, English AM
Link:	https://pubmed.ncbi.nlm.nih.gov/30145880/
DOI:	10.1021/jacs.8b05966
Publication:	Journal of the American Chemical Society
Keywords:
PMID:	30145880	Category:	J Am Chem Soc	Date Added:	2019-05-31
Dept Affiliation:	CHEMBIOCHEM 1 Quebec Network for Research on Protein Function, Structure and Engineering (PROTEO), and Department of Chemistry and Biochemistry , Concordia University , Montreal , QC H4B 1R6 , Canada.

Description:

LC-MS/MS profiling reveals that the proteoforms of cytochrome c peroxidase (Ccp1) isolated from respiring yeast mitochondria are oxidized at numerous Met, Trp, and Tyr residues. In vitro oxidation of recombinant Ccp1 by H₂O₂ in the absence of its reducing substrate, ferrocytochrome c, gives rise to similar proteoforms, indicating uncoupling of Ccp1 oxidation and reduction in mitochondria. The oxidative modifications found in the Ccp1 proteoforms are consistent with radical transfer (hole hopping) from the heme along several chains of redox-active residues (Trp, Met, Tyr). These modifications delineate likely hole-hopping pathways to novel substrate-binding sites. Moreover, a decrease in recombinant Ccp1 oxidation by H₂O₂ in vitro in the presence of glutathione supports a protective role for hole hopping to this antioxidant. Isolation and characterization of extramitochondrial Ccp1 proteoforms reveals that hole hopping from the heme in these proteoforms results in selective oxidation of the proximal heme ligand (H175) and heme labilization. Previously, we demonstrated that this labilized heme is recruited for catalase maturation (Kathiresan, M.; Martins, D.; English, A. M. Respiration triggers heme transfer from cytochrome c peroxidase to catalase in yeast mitochondria. Proc. Natl. Acad. Sci. U. S. A. 2014, 111, 17468-17473; DOI: 10.1073/pnas.1409692111 ). Following heme release, apoCcp1 exits mitochondria, yielding the extramitochondrial proteoforms that we characterize here. The targeting of Ccp1 for selective H175 oxidation may be linked to the phosphorylation status of Y153 close to the heme since pY153 is abundant in certain proteoforms. In sum, when insufficient electrons from ferrocytochrome c are available to Ccp1 in mitochondria, hole hopping from its heme expands its physiological functions. Specifically, we observe an unprecedented hole-hopping sequence for heme labilization and identify hole-hopping pathways from the heme to novel substrates and to glutathione at Ccp1's surface. Furthermore, our results underscore the power of proteoform profiling by LC-MS/MS in exploring the cellular roles of oxidoreductases.

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