Generation of New Artificial Metalloproteins by Cofactor Modification of Native Hemoproteins

Hayashi, Takashi; Sano, Yohei; Onoda, Akira

doi:10.1002/ijch.201400123

Cited by 33 publications

(26 citation statements)

References 56 publications

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“…Our group has been engaged in engineering of myoglobin (Mb), another representative hemoprotein ( Fig. 1) [38][39][40][41][42][43] which has not yet been explored as a possible NPMC precursor. Herein, we report the characterization of NPMCs prepared from Mb by heat treatment and an investigation of the ORR activity of these NPMCs under acidic conditions.…”

Section: Introductionmentioning

confidence: 99%

Myoglobin-based non-precious metal carbon catalysts for an oxygen reduction reaction

Onoda

Tanaka

Ono

et al. 2015

J. Porphyrins Phthalocyanines

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A non-precious metal catalyst (NPMC) promoting a four-electron oxygen reduction reaction (ORR) was synthesized by heat treatment of myoglobin (Mb) containing a heme (iron protoporphyrin IX) as a source of iron, nitrogen, and carbon atoms. Samples of the mixture of Mb and carbon black (Vulcan XC72R: VC) were pyrolyzed at 740, 840, 940, 1040 or 1140 °C under N 2 flow. The microstructures of the carbonized Mb catalysts were characterized by XRD, Raman spectroscopy, XPS, and TEM. Results indicate that the iron-containing active site is embedded within the surface structure in an amorphous domain of the carbon materials. The catalyst ink in a 0.05 wt% Nafion solution in isopropanol was coated onto a glassy carbon electrode and the ORR activity of Mb-based NPMCs was evaluated in a rotating disk electrode experiment in an O 2 -saturated 0.1 M HClO 4 solution at 25 °C. The catalyst synthesized at 940 °C has the highest ORR activity in terms of the onset potential and the current density. In contrast, pyrolytic temperatures above 940 °C decrease the activity, suggesting that the active structure of the catalyst apparently decomposes at higher temperatures. The Koutecky-Levich plots indicate that the Mb-based catalyst prepared at 940 °C catalyzes four-electron ORR (n = ca. 4). The catalysts prepared at other temperatures have n values of 3.6 at 740 °C, 3.7 at 840 °C, and 2.9 at 1040 °C. The ORR of Mb/VC is diffusion-controlled at potentials lower than 0.3 V (vs. RHE) and the onset potential is 0.84 ± 0.01 V.

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Section: Introductionmentioning

confidence: 99%

Myoglobin-based non-precious metal carbon catalysts for an oxygen reduction reaction

Onoda

Tanaka

Ono

et al. 2015

J. Porphyrins Phthalocyanines

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“…Teale described a simple acidification and heme extraction technique which allowed for generations of hemoprotein researchers to easily exchange cofactors and explore new possibilities for functionalities as shown in Figure 2 [1]. Many decades later the utility of replacing the native heme cofactor with heme analogs has emerged as a strategy to produce synthetic metalloenzymes to function as robust biocatalysts [2][3][4][5][6][7][8][9][10].…”

Section: Introductionmentioning

confidence: 99%

“…Watanabe, Lu, and colleagues have spent a considerable effort in exploring the potential of these types of substitutions particularly in myoglobin where enantioselective sulfoxidation of thioanisole is shown with Watanabe's Cr III (Schiff-base)-myoglobin enhancing the oxidation rates by up to 15-fold comparatively to Cr III (Schiff-base) alone [8,10,22,[24][25][26]. These examples did show promising improved functionality in some cases, but others have proven to be difficult to isolate in high yields and/or require protein modification or some form of covalent anchor in order to handle efficiently.…”

Section: Introductionmentioning

confidence: 99%

Advances in Engineered Hemoproteins that Promote Biocatalysis

Stone

Ahmed

2016

Inorganics

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Some hemoproteins have the structural robustness to withstand extraction of the heme cofactor and replacement with a heme analog. Recent reports have reignited interest and exploration in this field by demonstrating the versatility of these systems. Heme binding proteins can be utilized as protein scaffolds to support heme analogs that can facilitate new reactivity by noncovalent bonding at the heme-binding site utilizing the proximal ligand for support. These substituted hemoproteins have the capability to enhance catalytic reactivity and functionality comparatively to their native forms. This review will focus on progress and recent advances of artificially engineered hemoproteins utilized as a new target for the development of biocatalysts.

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“…In fact, this can be done by making mutations to existing proteins (Hu et al 2014; Nakajima, et al 2008), adding cofactors to systems that previously did not include such catalytic functionality (Dürrenberger et al 2014; Miner et al 2014), making protein fusions that provide photoaddressable proteins that localize in membranes (Hallett et al 2016), altering cofactors to serve a different purpose or attaching side chains (Hayashi et al 2015) or metal binding sites to confer new protein-protein interactions (PPIs) (Speltz et al 2015) or added stability (Salgado et al 2007; Schoene et al 2014). These PPIs are critical for molecular recognition, but often are difficult to measure in their native environments so that new methodologies have been developed to quantify these interactions in vivo (Cherf and Cochran 2015).…”

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confidence: 99%

“…In terms of systems investigated, many design studies attempt to mimic or reproduce electron transfer (Zhang et al 2011,; Plegaria et al 2015b; Roy et al, 2014), structural (Lombardi et al 2000; Plegaria et al 2015a; Fragoso et al 2015; Mocny and Pecoraro 2015) or catalytic function (Cangelosi et al 2014; Durrenberger and Ward 2014; Miner et al 2014; Nakajima, et al 2008; Reig et al 2012; Tegoni et al 2012; Zastrow et al 2012). However, this field is not restricted to biomimics as new catalysis is explored by building unique cofactors (Dürrenberger and Ward 2014; Hayashi et al 2015; Popp and Ball 2010). Another area of great interest is the ability of a protein to recognize another protein or an inanimate surface.…”

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confidence: 99%

Preface

Pecoraro¹

2016

Methods in Enzymology

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Generation of New Artificial Metalloproteins by Cofactor Modification of Native Hemoproteins

Cited by 33 publications

References 56 publications

Myoglobin-based non-precious metal carbon catalysts for an oxygen reduction reaction

Myoglobin-based non-precious metal carbon catalysts for an oxygen reduction reaction

Advances in Engineered Hemoproteins that Promote Biocatalysis

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