Electrochemically Promoted Tyrosine-Click-Chemistry for Protein Labeling

Álvarez-Dorta, Dimitri; Thobie‐Gautier, Christine; Croyal, Mikaël; Bouzelha, Mohammed; Mével, Mathieu; Deniaud, David; Boujtita, Mohammed; Gouin, Sébastien G.

doi:10.1021/jacs.8b09372

Cited by 110 publications

(112 citation statements)

References 37 publications

(61 reference statements)

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“…We confirmed by 1 H NMR the reaction with a tyrosine analogue, 3-(4-hydroxyphenyl)propionic acid (Supplemental Spectra 1). We allowed PTAD to react with the tyrosine mimic for 15 minutes and observed conversion to labeled tyrosine, consistent with previous reports (Figure 1A) 16,17 . By repeated labeling up to four times, signals for the fully converted product exceeded those for the tyrosine analogue.…”

Section: Ptad Conjugation To Tyrosine or Peptides Can Yield Distinctisupporting

confidence: 88%

“…The most significant changes were found for Y180 and Y475 (p = 0.009 and 0.0034, respectively, for 8 M urea; Student's ttest). Phenylisocyanate (m/z = 121) conjugations were observed for sixteen lysine residues, twice as many as previously reported 16,19 . However, this enrichment was little changed in the unfolded protein (Supplemental Figure 3C).…”

Section: Ptad Labeling Is Distinct For Alternate Folded States In a Psupporting

confidence: 70%

“…We assessed the products of PTAD conjugation with tyrosine to determine products our experiment designs may produce. Previous reports noted such additional reactions as conjugates with amines, second additions to tyrosine phenols, and short-lived conjugations to cysteine residues 15,16 . We confirmed by 1 H NMR the reaction with a tyrosine analogue, 3-(4-hydroxyphenyl)propionic acid (Supplemental Spectra 1).…”

Section: Ptad Conjugation To Tyrosine or Peptides Can Yield Distinctimentioning

confidence: 98%

“…We could also observe a double-reacted product of two PTADs on the phenolic ring, Y (2) (m/z = 700, Supplemental Figure 1A). PTAD can decompose to an isocyanate that is reactive toward amines 16,18 . The third product we observed was the phenylisocyanate product conjugated with the primary amine of tyrosine, NH (urea) (m/z = 384, Supplemental Figure 1A).…”

Section: Ptad Conjugation To Tyrosine or Peptides Can Yield Distinctimentioning

confidence: 99%

“…Angiotensin II is an 8 amino acid long peptide, DRVYIHPF (m/z = 1046, Figure 1B). In this reaction, we incubated PTAD in aqueous buffer containing 100 mM 2-amino-2-hydroxymethyl-propane-1,3diol (Tris) to scavenge the isocyanate through its own primary amine 16,19 . Matrix-assisted laser desorption/ionization and time of flight (MALDI-TOF) mass spectrometry was used to detect the PTAD conjugate (m/z = 1221).…”

Section: Ptad Conjugation To Tyrosine or Peptides Can Yield Distinctimentioning

confidence: 99%

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Discriminating changes in protein structure using PTAD conjugation to tyrosine

Moinpour

Barker

Guzman

et al. 2020

Preprint

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Many proteins of high interest to biology and biomedical research have few options that can provide even simple insights into structure, such as whether the protein conformation has changed between two states. Tyrosine is an abundant amino acid that balances hydrophobic and hydrophilic properties such that it can be found at protein surfaces, binding interfaces, and buried in a protein core. The reactive compound 4-phenyl-3H-1,2,4-triazole-3,5(4H)-dione (PTAD) can conjugate the phenolic side chain of tyrosine. We hypothesized that individual protein conformations could be distinguished by changes induced to tyrosine reactivity with PTAD. We quantified for a wellfolded protein, bovine serum albumen (BSA), the complex distribution of PTAD labeling using LC-MS/MS. As a model conformational switch in BSA, we chose to label unfolded BSA using urea. We found that changes in PTAD reactivity for many tyrosine residues was easily quantified and several sites were highly sensitive to the changes produced by unfolding the protein. This study suggests that the reaction of PTAD to tyrosine may allow for the measurement of a covalent fingerprint that can discriminate conformational states in a protein.

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Section: Ptad Conjugation To Tyrosine or Peptides Can Yield Distinctisupporting

confidence: 88%

Section: Ptad Labeling Is Distinct For Alternate Folded States In a Psupporting

confidence: 70%

Section: Ptad Conjugation To Tyrosine or Peptides Can Yield Distinctimentioning

confidence: 98%

Section: Ptad Conjugation To Tyrosine or Peptides Can Yield Distinctimentioning

confidence: 99%

Section: Ptad Conjugation To Tyrosine or Peptides Can Yield Distinctimentioning

confidence: 99%

See 3 more Smart Citations

Discriminating changes in protein structure using PTAD conjugation to tyrosine

Moinpour

Barker

Guzman

et al. 2020

Preprint

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(Hetero)Aryl CH Amination via Organic Electrochemistry

Shah¹,

Ngai²

2022

Handbook of CH-Functionalization

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Aromatic amines are essential compounds found in various natural products, drugs, and materials. Their widespread presence has motivated scientists worldwide to explore new avenues for the development of aromatic CN bond formation methodologies. Since the turn of the century, there has been a growing impetus to develop sustainable molecular syntheses. Having been recognized as an effective tool to control the redox events and flow of electrons between reactive species, organic electrocatalysis has been revived after being somewhat dormant for decades in industry and academia. This article provides an overview of electrocatalyzed aromatic CN bond formation reactions, which involve dehydrogenative coupling between aromatic CH bonds and amines through electrocatalysis. We present mechanistic insights and the scope of the methodology in terms of various substrates. We also have provided an outlook for future synthetic applications and different technologies that can merge with electrosynthesis.

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Strategies for Making High‐Performance Artificial Spider Silk Fibers

Schmuck,

Greco,

Pessatti

et al. 2023

Adv Funct Materials

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Artificial spider silk is an attractive material for many technical applications since it is a biobased fiber that can be produced under ambient conditions but still outcompetes synthetic fibers (e.g., Kevlar) in terms of toughness. Industrial use of this material requires bulk‐scale production of recombinant spider silk proteins in heterologous host and replication of the pristine fiber's mechanical properties. High molecular weight spider silk proteins can be spun into fibers with impressive mechanical properties, but the production levels are too low to allow commercialization of the material. Small spider silk proteins, on the other hand, can be produced at yields that are compatible with industrial use, but the mechanical properties of such fibers need to be improved. Here, the literature on wet‐spinning of artificial spider silk fibers is summarized and analyzed with a focus on mechanical performance. Furthermore, several strategies for how to improve the properties of such fibers, including optimized protein composition, smarter spinning setups, innovative protein engineering, chemical and physical crosslinking as well as the incorporation of nanomaterials in composite fibers, are outlined and discussed.

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Electrochemically Promoted Tyrosine-Click-Chemistry for Protein Labeling

Cited by 110 publications

References 37 publications

Discriminating changes in protein structure using PTAD conjugation to tyrosine

Discriminating changes in protein structure using PTAD conjugation to tyrosine

(Hetero)Aryl CH Amination via Organic Electrochemistry

Strategies for Making High‐Performance Artificial Spider Silk Fibers

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