Oxalyl‐CoA Decarboxylase Enables Nucleophilic One‐Carbon Extension of Aldehydes to Chiral α‐Hydroxy Acids

Burgener, Simon; Cortina, Niña Socorro; Erb, Tobias J.

doi:10.1002/anie.201915155

Cited by 25 publications

(33 citation statements)

References 35 publications

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“…Considering the abundance of the enzyme in 2-HIBA-grown cells (Table 1), a specific activity of about 250 nmol min −1 mg −1 (corresponding to a k cat of 0.26 s −1 ) can be deduced, indicating that enzyme preparation and assay protocols still need to be optimized. In addition, a significant overexpression in E. coli could not be established, likely due to insufficient soluble expression as previously observed for human HACL1 and other 2-hydroxyacyl-CoA lyases from prokaryotic origin (Chou et al, 2019;Burgener et al, 2020). In order to purify the enzyme from strain DSM 45062 for kinetic and structural characterization, production of the recombinant protein has to be improved, for example, by employing an actinobacterial expression system such as M. smegmatis (Bashiri and Baker, 2015).…”

Section: Discussionmentioning

confidence: 99%

“…The human peroxisomal 2hydroxyphytanoyl-CoA lyase HACL1 (NP_036392.2), for example, catalyzes the decomposition of 2-hydroxyphytanoyl-CoA (2-hydroxy-3,7,11,15-tetramethylhexadecanoyl-CoA) to the aldehyde pristanal (2,6,10,14-tetramethylpentadecanal) and formyl-CoA (Foulon et al, 1999(Foulon et al, , 2005. In addition, it has recently been demonstrated that HACL1 and related prokaryotic TPP-dependent enzymes can even catalyze the reversible acyloin condensation of formyl-CoA with shortand medium-chain carbonyl compounds (Chou et al, 2019;Burgener et al, 2020). Although these 2-hydroxyacyl-CoA lyases and the putative lyase from DSM 45062 are only distantly related (<30% sequence identity at about 90% query coverage), this provisional, only sequence-based functional assignment of WP_018331913.1 let us speculate about a mutase-independent pathway for the degradation of MPD and 2-HIBA proceeding via the decomposition of 2-hydroxyisobutyryl-CoA to acetone and formyl-CoA ( Figure 1A).…”

Section: Organization Of the Lyase-hcl Gene Cluster In A Chiangmaienmentioning

confidence: 99%

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Actinobacterial Degradation of 2-Hydroxyisobutyric Acid Proceeds via Acetone and Formyl-CoA by Employing a Thiamine-Dependent Lyase Reaction

et al. 2020

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The tertiary branched short-chain 2-hydroxyisobutyric acid (2-HIBA) has been associated with several metabolic diseases and lysine 2-hydroxyisobutyrylation seems to be a common eukaryotic as well as prokaryotic post-translational modification in proteins. In contrast, the underlying 2-HIBA metabolism has thus far only been detected in a few microorganisms, such as the betaproteobacterium Aquincola tertiaricarbonis L108 and the Bacillus group bacterium Kyrpidia tusciae DSM 2912. In these strains, 2-HIBA can be specifically activated to the corresponding CoA thioester by the 2-HIBA-CoA ligase (HCL) and is then isomerized to 3-hydroxybutyryl-CoA in a reversible and B 12-dependent mutase reaction. Here, we demonstrate that the actinobacterial strain Actinomycetospora chiangmaiensis DSM 45062 degrades 2-HIBA and also its precursor 2-methylpropane-1,2-diol via acetone and formic acid by employing a thiamine pyrophosphate-dependent lyase. The corresponding gene is located directly upstream of hcl, which has previously been found only in operonic association with the 2-hydroxyisobutyryl-CoA mutase genes in other bacteria. Heterologous expression of the lyase gene from DSM 45062 in E. coli established a 2-hydroxyisobutyryl-CoA lyase activity in the latter. In line with this, analysis of the DSM 45062 proteome reveals a strong induction of the lyase-HCL gene cluster on 2-HIBA. Acetone is likely degraded via hydroxylation to acetol catalyzed by a MimABCD-related binuclear iron monooxygenase and formic acid appears to be oxidized to CO 2 by selenium-dependent dehydrogenases. The presence of the lyase-HCL gene cluster in isoprene-degrading Rhodococcus strains and Pseudonocardia associated with tropical leafcutter ant species points to a role in degradation of biogenic short-chain ketones and highly branched organic compounds.

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Section: Discussionmentioning

confidence: 99%

Section: Organization Of the Lyase-hcl Gene Cluster In A Chiangmaienmentioning

confidence: 99%

Actinobacterial Degradation of 2-Hydroxyisobutyric Acid Proceeds via Acetone and Formyl-CoA by Employing a Thiamine-Dependent Lyase Reaction

et al. 2020

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“…Moreover, strategies for enzymatic production of high added value alcohols from aminoacids have also been developed [54,55].…”

Section: Cascade Enzymes In Aminoacid Chemistrymentioning

confidence: 99%

“…The methylated R-α-ketoacid obtained recovers its amino group from pyridoxamine (PMP) contained in the enzymes L-TA (IIvE) or D-TA to form L-β-Me-α-amino acids or D-β-Me-α-amino acids, respectively. The third enzyme in the cascade is a halide methyltransferase from Burkholderia xenovorans (HMT), used for SAM regeneration by stereoselective S-methylation of S-adenosylhomocysteine (SAH), through the use of methyl iodide as a methyl donor (Figure8).Moreover, strategies for enzymatic production of high added value alcohols from aminoacids have also been developed[54,55].…”

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confidence: 99%

Recent Advances in Enzymatic and Chemoenzymatic Cascade Processes

et al. 2020

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Cascade reactions have been described as efficient and universal tools, and are of substantial interest in synthetic organic chemistry. This review article provides an overview of the novel and recent achievements in enzyme cascade processes catalyzed by multi-enzymatic or chemoenzymatic systems. The examples here selected collect the advances related to the application of the sequential use of enzymes in natural or genetically modified combination; second, the important combination of enzymes and metal complex systems, and finally we described the application of biocatalytic biohybrid systems on in situ catalytic solid-phase as a novel strategy. Examples of efficient and interesting enzymatic catalytic cascade processes in organic chemistry, in the production of important industrial products, such as the designing of novel biosensors or bio-chemocatalytic systems for medicinal chemistry application, are discussed

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“…For example, the formolase enzyme can convert formaldehyde into dihydroxyacetone (8) or glycolaldehyde (13), which can be assimilated by either natural or engineered enzymes (14). An engineered enzyme can convert formyl-CoA and formaldehyde into glycolyl-CoA and then glycolate, which can be assimilated naturally (15,16). The common advance needed to enable all of these pathways is the reduction of formate to formaldehyde.…”

Section: Introductionmentioning

confidence: 99%

Enzyme engineering andin vivotesting of a formate-reduction pathway

Wang

Anderson

Yang

et al. 2021

Preprint

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Formate is an attractive feedstock for sustainable microbial production of fuels and chemicals, but its potential is limited by the lack of efficient assimilation pathways. The reduction of formate to formaldehyde would allow efficient downstream assimilation, but no efficient enzymes are known for this transformation. To develop a 2-step formate-reduction pathway, we screened natural variants of acyl-CoA synthetase (ACS) and acylating aldehyde dehydrogenase (ACDH) for activity on one-carbon substrates and identified active and highly expressed homologs of both enzymes. We then performed directed evolution, increasing ACDH specific activity by 2.5-fold and ACS lysate activity by 5-fold. To test for in vivo activity of our pathway, we expressed it in a methylotroph which can natively assimilate formaldehyde. Although the enzymes were active in cell extracts, we could not detect formate assimilation into biomass, indicating that further improvement will be required for formatotrophy. Our work provides a foundation for further development of a versatile pathway for formate assimilation.

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Oxalyl‐CoA Decarboxylase Enables Nucleophilic One‐Carbon Extension of Aldehydes to Chiral α‐Hydroxy Acids

Cited by 25 publications

References 35 publications

Actinobacterial Degradation of 2-Hydroxyisobutyric Acid Proceeds via Acetone and Formyl-CoA by Employing a Thiamine-Dependent Lyase Reaction

Actinobacterial Degradation of 2-Hydroxyisobutyric Acid Proceeds via Acetone and Formyl-CoA by Employing a Thiamine-Dependent Lyase Reaction

Recent Advances in Enzymatic and Chemoenzymatic Cascade Processes

Enzyme engineering andin vivotesting of a formate-reduction pathway

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