Stepwise Simulation of 3,5-Dihydro-5-methylidene-4<i>H-</i>imidazol-4-one (MIO) Biogenesis in Histidine Ammonia-lyase

Sánchez-Murcia, Pedro Alejandro Alejandro; Bueren-Calabuig, Juan A.; Camacho‐Artacho, Marta; Cortés-Cabrera, Álvaro; Gago, Federico

doi:10.1021/acs.biochem.6b00744

Cited by 11 publications

(6 citation statements)

References 51 publications

(113 reference statements)

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“…126 A very recent molecular dynamics simulation study provided great insight into the process of MIO formation in PpHAL, supporting the idea that mechanical compression from neighboring residues is required to prevent the formation of stabilizing hydrogen bonds and to enforce the correct alignment of donor and acceptor orbitals. 127 The crystal structure of PpHAL also showed for the first time the general structural features of arylalanine ammonia-lyases, homotetramers mainly built of α-helices of varying lengths 128 . Each subunit contains a globular N-terminal domain and an elongated C-terminal domain with five parallel α-helices, surrounded by six more (Figure 3).…”

Section: Arylalanine Ammonia-lyases (Pals Hals and Tals)mentioning

confidence: 94%

Synthetic and Therapeutic Applications of Ammonia-lyases and Aminomutases

et al. 2017

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Ammonia-lyases and aminomutases are mechanistically and structurally diverse enzymes which catalyze the deamination and/or isomerization of amino acids in nature by cleaving or shifting a C-N bond. Of the many protein families in which these enzyme activities are found, only a subset have been employed in the synthesis of optically pure fine chemicals or in medical applications. This review covers the natural diversity of these enzymes, highlighting particular enzyme classes that are used within industrial and medical biotechnology. These highlights detail the discovery and mechanistic investigations of these commercially relevant enzymes, along with comparisons of their various applications as stand-alone catalysts, components of artificial biosynthetic pathways and biocatalytic or chemoenzymatic cascades, and therapeutic tools for the potential treatment of various pathologies.

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Section: Arylalanine Ammonia-lyases (Pals Hals and Tals)mentioning

confidence: 94%

Synthetic and Therapeutic Applications of Ammonia-lyases and Aminomutases

et al. 2017

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“…These so-called MIOdependent aminomutases recruit an unusual highly electrophilic moiety MIO for catalyzing the 2,3-amine shift in aromatic amino acids and present outstanding enantioselectivity. The members from this enzyme family are frequently applied for an asymmetric synthesis route without cofactor recycling to produce the optically pure β-amino acids [30,31]. On the other hand, the enzymatic synthesis of optically pure β-amino acids has been considered as an attractive strategy, compared to the chemical processes, which are limited by low yield or enantiopurity, and high cost of the waste treatment.…”

Section: β-Amino Acids and Anticancer Drugsmentioning

confidence: 99%

Computational-Designed Enzyme for β-Tyrosine Production in Lignin Valorization

et al. 2021

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Lignin is an underutilized sustainable source of aromatic compounds. To valorize the low-value lignin monomers, we proposed an efficient strategy, involving enzymatic conversion from trans-p-hydroxycinnamic acids to generate valued-added canonical and non-canonical aromatic amino acids. Among them, β-amino acids are recognized as building blocks for bioactive natural products and pharmaceutical ingredients due to their attractive antitumor properties. Using computational enzyme design, the (R)-β-selective phenylalanine aminomutase from Taxus chinensis (TchPAM) was successfully mutated to accept β-tyrosine as the substrate, as well as to generate the (R)-β-tyrosine with excellent enantiopurity (ee > 99%) as the unique product from trans-p-hydroxycinnamic acid. Moreover, the kinetic parameters were determined for the reaction of four Y424 enzyme variants with the synthesis of different phenylalanine and tyrosine enantiomers. In the ammonia elimination reaction of (R)-β-tyrosine, the variants Y424N and Y424C displayed a two-fold increased catalytic efficiency of the wild type. In this work, a binding pocket in the active site, including Y424, K427, I431, and E455, was examined for its influence on the β-enantioselectivity of this enzyme family. Combining the upstream lignin depolymerization and downstream production, a sustainable value chain based on lignin is enabled. In summary, we report a β-tyrosine synthesis process from a monolignol component, offering a new way for lignin valorization by biocatalyst modification.

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“…Each complex foldamer: Li-TryR was immersed in a box of 27,000 TIP3P water molecules that extended 12 Å away from any solute atom and Na + ions were added to ensure electrical neutrality. The MD simulation protocol at 300 K and 1 atm (NPT ensemble) was carried out as described before [28] using the pmemd_cuda. SPFP module in AMBER16.…”

Section: Fitc-peg-pro-lys-β 3 Ile-ile-gln-β 3 Ser-val-gly-ile-β 3 Sermentioning

confidence: 99%

Improved proteolytic stability and potent activity against Leishmania infantum trypanothione reductase of α/β-peptide foldamers conjugated to cell-penetrating peptides

Lucio

Gamo

Ruiz-Santaquiteria

et al. 2017

European Journal of Medicinal Chemistry

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The objective of the current study was to enhance the proteolytic stability of peptide-based inhibitors that target critical protein-protein interactions at the dimerization interface of Leishmania infantum trypanothione reductase (Li-TryR) using a backbone modification strategy. To achieve this goal we carried out the synthesis, proteolytic stability studies and biological evaluation of a small library of α/β-peptide foldamers of different length (from 9-mers to 13-mers) and different α→β substitution patterns related to prototype linear α-peptides. We show that several 13-residue α/β-peptide foldamers retain inhibitory potency against the enzyme (in both activity and dimerization assays) while they are far less susceptible to proteolytic degradation than an analogous α-peptide. The strong dependence of the binding affinities for Li-TryR on the length of the α,β-peptides is supported by theoretical calculations on conformational ensembles of the resulting complexes. The conjugation of the most proteolytically stable α/β-peptide with oligoarginines results in a molecule with potent activity against L. infantum promastigotes and amastigotes.

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Stepwise Simulation of 3,5-Dihydro-5-methylidene-4H-imidazol-4-one (MIO) Biogenesis in Histidine Ammonia-lyase

Cited by 11 publications

References 51 publications

Synthetic and Therapeutic Applications of Ammonia-lyases and Aminomutases

Synthetic and Therapeutic Applications of Ammonia-lyases and Aminomutases

Computational-Designed Enzyme for β-Tyrosine Production in Lignin Valorization

Improved proteolytic stability and potent activity against Leishmania infantum trypanothione reductase of α/β-peptide foldamers conjugated to cell-penetrating peptides

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