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Literature DB >> 19173070

myo-Inositol oxygenase: a radical new pathway for O(2) and C-H activation at a nonheme diiron cluster.

J Martin Bollinger¹, Yinghui Diao, Megan L Matthews, Gang Xing, Carsten Krebs.

Abstract

The enzyme myo-inositol oxygenase (MIOX) catalyzes conversion of myo-inositol (cyclohexan-1,2,3,5/4,6-hexa-ol or MI) to d-glucuronate (DG), initiating the only known pathway in humans for catabolism of the carbon skeleton of cell-signaling inositol (poly)phosphates and phosphoinositides. Recent kinetic, spectroscopic and crystallographic studies have shown that the enzyme activates its substrates, MI and O(2), at a carboxylate-bridged nonheme diiron(ii/iii) cluster, making it the first of many known nonheme diiron oxygenases to employ the mixed-valent form of its cofactor. Evidence suggests that: (1) the Fe(iii) site coordinates MI via its C1 and C6 hydroxyl groups; (2) the Fe(ii) site reversibly coordinates O(2) to produce a superoxo-diiron(iii/iii) intermediate; and (3) the pendant oxygen atom of the superoxide ligand abstracts hydrogen from C1 to initiate the unique C-C-bond-cleaving, four-electron oxidation reaction. This review recounts the studies leading to the recognition of the novel cofactor requirement and catalytic mechanism of MIOX and forecasts how remaining gaps in our understanding might be filled by additional experiments.

Entities: Chemical Disease Gene Mutation Species

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Year: 2008 PMID： 19173070 PMCID： PMC2788986 DOI： 10.1039/b811885j

Source DB: PubMed Journal: Dalton Trans ISSN： 1477-9226 Impact factor: 4.390

58 in total

1. Biochemical studies on inositol. V. Purification and properties of the enzyme that cleaves inositol to D-glucuronic acid.

Authors: F C CHARALAMPOUS
Journal: J Biol Chem Date: 1959-02 Impact factor: 5.157

2. Biochemical studies on inositol. IV. Conversion of inositol to glucuronic acid by rat kidney extracts.

Authors: F C CHARALAMPOUS; C LYRAS
Journal: J Biol Chem Date: 1957-09 Impact factor: 5.157

3. (Mu-1,2-peroxo)diiron(III/III) complex as a precursor to the diiron(III/IV) intermediate X in the assembly of the iron-radical cofactor of ribonucleotide reductase from mouse.

Authors: Danny Yun; Ricardo García-Serres; Brandon M Chicalese; Young H An; Boi Hanh Huynh; J Martin Bollinger
Journal: Biochemistry Date: 2007-01-27 Impact factor: 3.162

4. Dietary myo-inositol therapy in hyperglycemia-induced embryopathy.

Authors: M Khandelwal; E A Reece; Y K Wu; M Borenstein
Journal: Teratology Date: 1998-02

5. Enzymatic C-H activation by metal-superoxo intermediates.

Authors: J Martin Bollinger; Carsten Krebs
Journal: Curr Opin Chem Biol Date: 2007-03-19 Impact factor: 8.822

6. Dioxygen Activation and Methane Hydroxylation by Soluble Methane Monooxygenase: A Tale of Two Irons and Three Proteins A list of abbreviations can be found in Section 7.

Authors: Maarten Merkx; Daniel A. Kopp; Matthew H. Sazinsky; Jessica L. Blazyk; Jens Müller; Stephen J. Lippard
Journal: Angew Chem Int Ed Engl Date: 2001-08-03 Impact factor: 15.336

7. Evidence for C-H cleavage by an iron-superoxide complex in the glycol cleavage reaction catalyzed by myo-inositol oxygenase.

Authors: Gang Xing; Yinghui Diao; Lee M Hoffart; Eric W Barr; K Sandeep Prabhu; Ryan J Arner; C Channa Reddy; Carsten Krebs; J Martin Bollinger
Journal: Proc Natl Acad Sci U S A Date: 2006-04-10 Impact factor: 11.205

8. Use of a chemical trigger for electron transfer to characterize a precursor to cluster X in assembly of the iron-radical cofactor of Escherichia coli ribonucleotide reductase.

Authors: Lana Saleh; Carsten Krebs; Brenda A Ley; Sunail Naik; Boi Hanh Huynh; J Martin Bollinger
Journal: Biochemistry Date: 2004-05-25 Impact factor: 3.162

9. Evidence that dioxygen and substrate activation are tightly coupled in dopamine beta-monooxygenase. Implications for the reactive oxygen species.

Authors: John P Evans; Kyunghye Ahn; Judith P Klinman
Journal: J Biol Chem Date: 2003-09-09 Impact factor: 5.157

Review 10. Aldose reductase in the etiology of diabetic complications: 2. Nephropathy.

Authors: D Stribling; F M Armstrong; H E Harrison
Journal: J Diabet Complications Date: 1989 Apr-Jun

28 in total

1. O(2)-evolving chlorite dismutase as a tool for studying O(2)-utilizing enzymes.

Authors: Laura M K Dassama; Timothy H Yosca; Denise A Conner; Michael H Lee; Béatrice Blanc; Bennett R Streit; Michael T Green; Jennifer L DuBois; Carsten Krebs; J Martin Bollinger
Journal: Biochemistry Date: 2012-02-13 Impact factor: 3.162

2. Factors affecting the carboxylate shift upon formation of nonheme diiron-O2 adducts.

Authors: Jonathan R Frisch; Ryan McDonnell; Elena V Rybak-Akimova; Lawrence Que
Journal: Inorg Chem Date: 2013-02-22 Impact factor: 5.165

Review 3. Current challenges of modeling diiron enzyme active sites for dioxygen activation by biomimetic synthetic complexes.

Authors: Simone Friedle; Erwin Reisner; Stephen J Lippard
Journal: Chem Soc Rev Date: 2010-05-20 Impact factor: 54.564

myo-Inositol oxygenase: a radical new pathway for O(2) and C-H activation at a nonheme diiron cluster.

1. Biochemical studies on inositol. V. Purification and properties of the enzyme that cleaves inositol to D-glucuronic acid.

2. Biochemical studies on inositol. IV. Conversion of inositol to glucuronic acid by rat kidney extracts.

3. (Mu-1,2-peroxo)diiron(III/III) complex as a precursor to the diiron(III/IV) intermediate X in the assembly of the iron-radical cofactor of ribonucleotide reductase from mouse.

4. Dietary myo-inositol therapy in hyperglycemia-induced embryopathy.

5. Enzymatic C-H activation by metal-superoxo intermediates.

6. Dioxygen Activation and Methane Hydroxylation by Soluble Methane Monooxygenase: A Tale of Two Irons and Three Proteins A list of abbreviations can be found in Section 7.

7. Evidence for C-H cleavage by an iron-superoxide complex in the glycol cleavage reaction catalyzed by myo-inositol oxygenase.

8. Use of a chemical trigger for electron transfer to characterize a precursor to cluster X in assembly of the iron-radical cofactor of Escherichia coli ribonucleotide reductase.

9. Evidence that dioxygen and substrate activation are tightly coupled in dopamine beta-monooxygenase. Implications for the reactive oxygen species.

Review 10. Aldose reductase in the etiology of diabetic complications: 2. Nephropathy.

1. O(2)-evolving chlorite dismutase as a tool for studying O(2)-utilizing enzymes.

2. Factors affecting the carboxylate shift upon formation of nonheme diiron-O2 adducts.

Review 3. Current challenges of modeling diiron enzyme active sites for dioxygen activation by biomimetic synthetic complexes.

4. Oxygen activation at mononuclear nonheme iron centers: a superoxo perspective.

Review 5. Diiron monooxygenases in natural product biosynthesis.

Review 6. Anaerobic functionalization of unactivated C-H bonds.

7. Spectroscopic Evidence for the Two C-H-Cleaving Intermediates of Aspergillus nidulans Isopenicillin N Synthase.

8. Novel Approaches for the Accumulation of Oxygenated Intermediates to Multi-Millimolar Concentrations.

9. Characterization of two distinct adducts in the reaction of a nonheme diiron(II) complex with O2.

10. Organophosphonate-degrading PhnZ reveals an emerging family of HD domain mixed-valent diiron oxygenases.