Enlightening the Path to Protein Engineering: Chemoselective Turn-On Probes for High-Throughput Screening of Enzymatic Activity

Hecko, Sebastian; Schiefer, Astrid; Badenhorst, Christoffel P. S.; Fink, Michael; Mihovilovič, Marko D.; Bornscheuer, Uwe T.; Rudroff, Florian

doi:10.1021/acs.chemrev.2c00304

Cited by 16 publications

(9 citation statements)

References 676 publications

(1,246 reference statements)

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“…Beim Screening auf neuartige Aktivitäten (die in den ersten Screening-Runden voraussichtlich gering sein werden) sind sowohl die Empfindlichkeit als auch die Fähigkeit, in Zelllysaten zu screenen, von entscheidender Bedeutung. [24] Ein von Tan et al beschriebener Homocystein-Assay ermöglicht den selektiven Nachweis von L-Homocystein gegenüber Cystein im Plasma über die Bildung von Schwefelwasserstoff durch eine Homocystein-α,γ-Lyase. [25] Der Fluoreszenznachweis mit N,N-Dibutylphenylendiamin…”

Section: Introductionunclassified

“…Aus diesem Grund führen andere biologische Thiole wie Glutathion und Cystein oder exogen zugesetzte Reduktionsmittel wie 2‐Mercaptoethanol zu einem hohen Hintergrund, was die Empfindlichkeit des Assays verringert und für die Verwendung mit Zelllysaten inkompatibel macht. Beim Screening auf neuartige Aktivitäten (die in den ersten Screening‐Runden voraussichtlich gering sein werden) sind sowohl die Empfindlichkeit als auch die Fähigkeit, in Zelllysaten zu screenen, von entscheidender Bedeutung [24] …”

Section: Introductionunclassified

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Ein universeller, kontinuierlicher Assay für SAM‐abhängige Methyltransferasen

Menke,

Schneider,

Badenhorst

et al. 2023

Angewandte Chemie

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Enzyme‐catalyzed late‐stage functionalization (LSF), such as methylation of drug molecules and lead structures, enables direct access to more potent active pharmaceutical ingredients (API). S‑adenosyl‐l‐methionine‐dependent methyltransferases (MTs) can play a key role in the development of new APIs, as they catalyze the chemo‐ and regioselective methylation of O‐, N‐, S‐ and C‐atoms, being superior to traditional chemical routes. To identify suitable MTs, we developed a continuous fluorescence‐based, high‐throughput assay for SAM‐dependent methyltransferases, which facilitates screening using E. coli cell lysates. This assay involves two enzymatic steps for the conversion of S‑adenosyl‐l‐homocysteine into l‑homocysteine and H2S to result in a selective fluorescence readout via reduction of a coumarin‐based sulfide probe. Investigation of two O‑MTs and an N‐MT confirmed that this assay is suitable for the determination of methyltransferase activity in E. coli cell lysates.

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Section: Introductionunclassified

Ein universeller, kontinuierlicher Assay für SAM‐abhängige Methyltransferasen

Menke,

Schneider,

Badenhorst

et al. 2023

Angewandte Chemie

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“…When screening for novel activities (which are expected to be low during initial rounds of screening), sensitivity and the ability to screen in cell lysates are both critically important. [24] One homocysteine assay reported by Tan et al features selective detection of L-homocysteine over cysteine in plasma through formation of hydrogen sulfide by a homocysteine-α,γ-lyase. [25] Fluorescent detection with N,N-dibutyl phenylene diamine (DBPDA) serves as the sensitive readout (Scheme 1E).…”

Section: Introductionmentioning

confidence: 99%

A Universal, Continuous Assay for SAM‐dependent Methyltransferases

Menke,

Schneider,

Badenhorst

et al. 2023

Angew Chem Int Ed

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“…In fluorescence bioimaging, the amine group is an extremely attractive target functional group because of its ubiquity and high reactivity. Many “turn-on type” amine-reactive fluorescent probes bearing active esters, isothiocyanates, and sulfonyl chlorides as amine-reactive groups have been reported for valid fluorescence labeling . The requirements of labeled reagents are fast and reliable chemical reactions and a compact molecular size for the exclusion of perturbations of the targeting biomolecules.…”

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confidence: 99%

“…Many "turn-on type" aminereactive fluorescent probes bearing active esters, isothiocyanates, and sulfonyl chlorides as amine-reactive groups have been reported for valid fluorescence labeling. 2 The requirements of labeled reagents are fast and reliable chemical reactions and a compact molecular size for the exclusion of perturbations of the targeting biomolecules. Bicyclic fluorophores, such as coumarin and 7-nitrobenzoxadiazole (NBD), are widely utilized as typical amine-reactive fluorophores with compact sizes.…”

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confidence: 99%

Naphthyridine-Based Electron Push–Pull-Type Amine-Reactive Fluorescent Probe for Sensing Amines and Proteins in Aqueous Media

Umeno,

Muroi,

Kayama

et al. 2023

Bioconjugate Chem.

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In bioengineering, fluorescent amine-reactive probes are invaluable for the detection of amine species. In particular, targeting probes for lysine, which has a free amino group in amino acids, are a valid method for protein detection. For this purpose, many fluorescent “turn-on type” probes with amine reactivity have been developed; however, they require improvements. In the typical florescence probes, BODIPY and NBD analogs have small Stokes shifts based on absorption and emission and lability in an aqueous environment, respectively. In this study, a new class of fluorescent probes, 1,8-Nap-F, based on the electron push–pull-type 1,8-naphthyridine framework, was designed and investigated as an amine-reactive probe. Generally, electron push–pull-type fluorophores exhibit a large Stokes shift at the expense of fluorescent enhancement in aqueous media; thus, there is a trade-off between possessing a large Stokes shift and intense emission. However, 1,8-Nap-F reacts with primary amines, yielding emissive amine products with a large Stokes shift (>70 nm) without fluorescence quenching and side products, even in an aqueous environment, thereby overcoming the disadvantages of electron push–pull-type fluorophores and lability in aqueous conditions. By applying the specific features of 1,8-Nap-F, we achieved selective lysine detection and fluorescence bioimaging, such as endoplasmic reticulum-selective protein labeling and organelle staining, in living cells by utilizing amine-substituted derivatives.

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Enlightening the Path to Protein Engineering: Chemoselective Turn-On Probes for High-Throughput Screening of Enzymatic Activity

Cited by 16 publications

References 676 publications

Ein universeller, kontinuierlicher Assay für SAM‐abhängige Methyltransferasen

Ein universeller, kontinuierlicher Assay für SAM‐abhängige Methyltransferasen

A Universal, Continuous Assay for SAM‐dependent Methyltransferases

Naphthyridine-Based Electron Push–Pull-Type Amine-Reactive Fluorescent Probe for Sensing Amines and Proteins in Aqueous Media

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