Jochen Fesseler scite author profile

Organohalide-respiring microorganisms can use a variety of persistent pollutants, including trichloroethene (TCE), as terminal electron acceptors. The final two-electron transfer step in organohalide respiration is catalyzed by reductive dehalogenases. Here we report the x-ray crystal structure of PceA, an archetypal dehalogenase from Sulfurospirillum multivorans, as well as structures of PceA in complex with TCE and product analogs. The active site harbors a deeply buried norpseudo-B12 cofactor within a nitroreductase fold, also found in a mammalian B12 chaperone. The structures of PceA reveal how a cobalamin supports a reductive haloelimination exploiting a conserved B12-binding scaffold capped by a highly variable substrate-capturing region.

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How the [NiFe₄S₄] Cluster of CO Dehydrogenase Activates CO₂ and NCO⁻

Fesseler

2015

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Ni,Fe-containing CO dehydrogenases (CODHs) use a [NiFe4S4] cluster, termed cluster C, to reversibly reduce CO2 to CO with high turnover number. Binding to Ni and Fe activates CO2, but current crystal structures have insufficient resolution to analyze the geometry of bound CO2 and reveal the extent and nature of its activation. The crystal structures of CODH in complex with CO2 and the isoelectronic inhibitor NCO(-) are reported at true atomic resolution (dmin ≤1.1 Å). Like CO2, NCO(-) is a μ2,η(2) ligand of the cluster and acts as a mechanism-based inhibitor. While bound CO2 has the geometry of a carboxylate group, NCO(-) is transformed into a carbamoyl group, thus indicating that both molecules undergo a formal two-electron reduction after binding and are stabilized by substantial π backbonding. The structures reveal the combination of stable μ2,η(2) coordination by Ni and Fe2 with reductive activation as the basis for both the turnover of CO2 and inhibition by NCO(-).

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Carbon Monoxide. Toxic Gas and Fuel for Anaerobes and Aerobes: Carbon Monoxide Dehydrogenases

Jeoung¹,

Fesseler²,

Goetzl³

et al. 2014

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Carbon monoxide (CO) pollutes the atmosphere and is toxic for respiring organisms including man. But CO is also an energy and carbon source for phylogenetically diverse microbes living under aerobic and anaerobic conditions. Use of CO as metabolic fuel for microbes relies on enzymes like carbon monoxide dehydrogenase (CODH) and acetyl-CoA synthase (ACS), which catalyze conversions resembling processes that eventually initiated the dawn of life.CODHs catalyze the (reversible) oxidation of CO with water to CO2 and come in two different flavors with unprecedented active site architectures. Aerobic bacteria employ a Cu- and Mo-containing CODH in which Cu activates CO and Mo activates water and takes up the two electrons generated in the reaction. Anaerobic bacteria and archaea use a Ni- and Fe-containing CODH, where Ni activates CO and Fe provides the nucleophilic water. Ni- and Fe-containing CODHs are frequently associated with ACS, where the CODH component reduces CO2 to CO and ACS condenses CO with a methyl group and CoA to acetyl-CoA.Our current state of knowledge on how the three enzymes catalyze these reactions will be summarized and the different strategies of CODHs to achieve the same task within different active site architectures compared.

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When the inhibitor tells more than the substrate: the cyanide-bound state of a carbon monoxide dehydrogenase

et al. 2016

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The extended reductive acetyl-CoA pathway: ATPases in metal cluster maturation and reductive activation

Jeoung

Goetzl

Hennig

et al. 2014

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The reductive acetyl-coenzyme A (acetyl-CoA) pathway, also known as the Wood-Ljungdahl pathway, allows reduction and condensation of two molecules of carbon dioxide (CO2) to build the acetyl-group of acetyl-CoA. Productive utilization of CO2 relies on a set of oxygen sensitive metalloenzymes exploiting the metal organic chemistry of nickel and cobalt to synthesize acetyl-CoA from activated one-carbon compounds. In addition to the central catalysts, CO dehydrogenase and acetyl-CoA synthase, ATPases are needed in the pathway. This allows the coupling of ATP binding and hydrolysis to electron transfer against a redox potential gradient and metal incorporation to (re)activate one of the central players of the pathway. This review gives an overview about our current knowledge on how these ATPases achieve their tasks of maturation and reductive activation.

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A Morphing [4Fe‐3S‐nO]‐Cluster within a Carbon Monoxide Dehydrogenase Scaffold

et al. 2022

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Ni,Fe‐containing carbon monoxide dehydrogenases (CODHs) catalyze the reversible reduction of CO2 to CO. Several anaerobic microorganisms encode multiple CODHs in their genome, of which some, despite being annotated as CODHs, lack a cysteine of the canonical binding motif for the active site Ni,Fe‐cluster. Here, we report on the structure and reactivity of such a deviant enzyme, termed CooS‐VCh. Its structure reveals the typical CODH scaffold, but contains an iron‐sulfur‐oxo hybrid‐cluster. Although closely related to true CODHs, CooS‐VCh catalyzes neither CO oxidation, nor CO2 reduction. The active site of CooS‐VCh undergoes a redox‐dependent restructuring between a reduced [4Fe‐3S]‐cluster and an oxidized [4Fe‐2S‐S*‐2O‐2(H2O)]‐cluster. Hydroxylamine, a slow‐turnover substrate of CooS‐VCh, oxidizes the hybrid‐cluster in two structurally distinct steps. Overall, minor changes in CODHs are sufficient to accommodate a Fe/S/O‐cluster in place of the Ni,Fe‐heterocubane‐cluster of CODHs.

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Wie der [NiFe₄S₄]‐Cluster der CO‐Dehydrogenase CO₂ und NCO⁻ aktiviert

2015

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Recombinant portal protein fromStaphylococcus epidermidisbacteriophage CNPH82 is a 13-subunit oligomer

et al. 2012

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The portal protein cn3 of bacteriophage CNPH82 is predicted to serve as a gateway for translocation of viral genome into preformed pro-capsid, like portal proteins from other double-stranded DNA tailed bacteriophages. The host of bacteriophage CNPH82 is the opportunistic human pathogenic bacterium Staphylococcus epidermidis, a major cause of nosocomial infections. The portal protein of this phage has been cloned, overexpressed and purified. Sizeexclusion chromatography-multi-angle laser light scattering analysis has indicated that the portal protein contains $13 subunits. Crystals of the portal protein, diffracting to 4.2 Å , have been obtained. These crystals belong to the space group C222 1 with the unit-cell parameters of a = 252.4, b = 367.0, c = 175.5 Å . The self-rotation function revealed the presence of a single 13-subunit oligomer in the asymmetric unit.

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Jochen Fesseler

Structural basis for organohalide respiration

How the [NiFe₄S₄] Cluster of CO Dehydrogenase Activates CO₂ and NCO⁻

Carbon Monoxide. Toxic Gas and Fuel for Anaerobes and Aerobes: Carbon Monoxide Dehydrogenases

When the inhibitor tells more than the substrate: the cyanide-bound state of a carbon monoxide dehydrogenase

The extended reductive acetyl-CoA pathway: ATPases in metal cluster maturation and reductive activation

A Morphing [4Fe‐3S‐nO]‐Cluster within a Carbon Monoxide Dehydrogenase Scaffold

Wie der [NiFe₄S₄]‐Cluster der CO‐Dehydrogenase CO₂ und NCO⁻ aktiviert

Recombinant portal protein fromStaphylococcus epidermidisbacteriophage CNPH82 is a 13-subunit oligomer

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Jochen Fesseler

Structural basis for organohalide respiration

How the [NiFe4S4] Cluster of CO Dehydrogenase Activates CO2 and NCO−

Carbon Monoxide. Toxic Gas and Fuel for Anaerobes and Aerobes: Carbon Monoxide Dehydrogenases

When the inhibitor tells more than the substrate: the cyanide-bound state of a carbon monoxide dehydrogenase

The extended reductive acetyl-CoA pathway: ATPases in metal cluster maturation and reductive activation

A Morphing [4Fe‐3S‐nO]‐Cluster within a Carbon Monoxide Dehydrogenase Scaffold

Wie der [NiFe4S4]‐Cluster der CO‐Dehydrogenase CO2 und NCO− aktiviert

Recombinant portal protein fromStaphylococcus epidermidisbacteriophage CNPH82 is a 13-subunit oligomer

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Resources

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How the [NiFe₄S₄] Cluster of CO Dehydrogenase Activates CO₂ and NCO⁻

Wie der [NiFe₄S₄]‐Cluster der CO‐Dehydrogenase CO₂ und NCO⁻ aktiviert