Synthesis and Evaluation of a Library of Fluorescent Dipeptidomimetic Analogues as Substrates for Modified Bacterial Ribosomes

Chowdhury, Sandipan; Chauhan, Pradeep S.; Dedkova, Larisa M.; Bai, Xiaoguang; Chen, Shengxi; Talukder, Poulami; Hecht, Sidney M.

doi:10.1021/acs.biochem.6b00102

Cited by 14 publications

(20 citation statements)

References 40 publications

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“…For example, Hecht introduced 6-cyano tryptophan as a FRET pair to study the binding of several proteins to DNA labeled with fluorescent nucleobases [26]. Using the dipeptidyl-tRNA tolerant ribosomes, he incorporated aryl oxazole and thiazole dipeptide mimics into the GFP structure, leading to the formation of modified fluorophores and fluorescent proteins [27]. Introduction of ncAAs has also made its mark in the synthesis of radiolabeled proteins for PET imaging.…”

Section: In Vitro Synthesis Of Modified Proteinsmentioning

confidence: 99%

In vitro genetic code reprogramming and expansion to study protein function and discover macrocyclic peptide ligands

Richardson

Dods

Abrigo

et al. 2018

Current Opinion in Chemical Biology

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The ability to introduce non-canonical amino acids into peptides and proteins is facilitated by working within in vitro translation systems. Non-canonical amino acids can be introduced into these systems using sense codon reprogramming, stop codon suppression, and by breaking codon degeneracy. Here, we review how these techniques have been used to create proteins with novel properties and how they facilitate sophisticated studies of protein function. We also discuss how researchers are using in vitro translation experiments with non-canonical amino acids to explore the tolerance of the translation apparatus to artificial building blocks. Finally, we give several examples of how non-canonical amino acids can be combined with mRNA-displayed peptide libraries for the creation of protease-stable, macrocyclic peptide libraries for ligand discovery.

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Section: In Vitro Synthesis Of Modified Proteinsmentioning

confidence: 99%

In vitro genetic code reprogramming and expansion to study protein function and discover macrocyclic peptide ligands

Richardson

Dods

Abrigo

et al. 2018

Current Opinion in Chemical Biology

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“…In addition, ongoing studies show the potential of amino and amido-oxazoles to act as fluorescent dipeptidomimetics ( Fig. 1 ) [ 9 ]. Due to their diene character, oxazoles find also use as intermediates in the synthesis of other organic scaffolds such as furans and pyridines, via cycloaddition/retro-cycloaddition tandem processes ( Fig.…”

Section: Introductionmentioning

confidence: 99%

Continuous multistep synthesis of 2-(azidomethyl)oxazoles

Rossa¹,

Suveges²,

Sá³

et al. 2018

Beilstein J. Org. Chem.

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An efficient three-step protocol was developed to produce 2-(azidomethyl)oxazoles from vinyl azides in a continuous-flow process. The general synthetic strategy involves a thermolysis of vinyl azides to generate azirines, which react with bromoacetyl bromide to provide 2-(bromomethyl)oxazoles. The latter compounds are versatile building blocks for nucleophilic displacement reactions as demonstrated by their subsequent treatment with NaN3 in aqueous medium to give azido oxazoles in good selectivity. Process integration enabled the synthesis of this useful moiety in short overall residence times (7 to 9 min) and in good overall yields.

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“…To the best of our knowledge, the only adequate approach reported in the literature is the use of a mutated ribosome that incorporates azolecontaining dipeptide units into the nascent peptide chain [30][31][32][33][34] . Unfortunately, the incorporation of such azole-containing dipeptide units into the nascent peptide chain was very modest where only 1-7% efficiency was observed for the expression of green fluorescent protein (GFP) mutants compared to the wildtype GFP expression even using the dedicated mutant ribosome (i.e., the conventional wildtype ribosome could not do the job at all) 31,32 . This implies that direct incorporation of azole moiety via such a peptidyl-transfer reaction is yet an arduous task.…”

mentioning

confidence: 99%

Posttranslational chemical installation of azoles into translated peptides

et al. 2021

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Azoles are five-membered heterocycles often found in the backbones of peptidic natural products and synthetic peptidomimetics. Here, we report a method of ribosomal synthesis of azole-containing peptides involving specific ribosomal incorporation of a bromovinylglycine derivative into the nascent peptide chain and its chemoselective conversion to a unique azole structure. The chemoselective conversion was achieved by posttranslational dehydrobromination of the bromovinyl group and isomerization in aqueous media under fairly mild conditions. This method enables us to install exotic azole groups, oxazole and thiazole, at designated positions in the peptide chain with both linear and macrocyclic scaffolds and thereby expand the repertoire of building blocks in the mRNA-templated synthesis of designer peptides.

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Synthesis and Evaluation of a Library of Fluorescent Dipeptidomimetic Analogues as Substrates for Modified Bacterial Ribosomes

Cited by 14 publications

References 40 publications

In vitro genetic code reprogramming and expansion to study protein function and discover macrocyclic peptide ligands

In vitro genetic code reprogramming and expansion to study protein function and discover macrocyclic peptide ligands

Continuous multistep synthesis of 2-(azidomethyl)oxazoles

Posttranslational chemical installation of azoles into translated peptides

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