A Novel Visible Range FRET Probe for Monitoring Acid Sphingomyelinase Activity in Living Cells

Kappe, C. Oliver; Mohamed, Zainelabdeen H.; Naser, Eyad; Carpinteiro, Alexander

doi:10.1002/chem.202000133

Cited by 13 publications

(12 citation statements)

References 21 publications

(26 reference statements)

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“…We therefore aimed at developing as creening assayt hat should be as realistic as possible in order to be able to detect compounds with completely new binding modes. We reasoned that in anyc ase, at ransfer assay would be more predictive than ab inding assay.B eing inspiredb yo ur recent success in developing assayso fs phingolipid metabolizing enzymes based on Fçrster Resonance Energy Transfer (FRET), [18] we wanted to apply this principle to aC ERT-mediated lipid transfer assay.T he goal was to monitort he activity of CERT in ah omogeneous assay system in multi-well format and making use of the inherentn ormalization of fluorescenceb yd ual wavelength readout. [19] The idea wast hat perhaps ab i-directional transfer of dye-labelled ceramides coulda chieve the necessary transfer rate.…”

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confidence: 99%

Liposomal FRET Assay Identifies Potent Drug‐Like Inhibitors of the Ceramide Transport Protein (CERT)

Samaha

Hamdo

Cong

et al. 2020

Chemistry A European J

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Ceramide transfer protein (CERT) mediates non‐vesicular transfer of ceramide from endoplasmic reticulum to Golgi apparatus and thus catalyzes the rate‐limiting step of sphingomyelin biosynthesis. Usually, CERT ligands are evaluated in tedious binding assays or non‐homogenous transfer assays using radiolabeled ceramides. Herein, a facile and sensitive assay for CERT, based on Förster resonance energy transfer (FRET), is presented. To this end, we mixed donor and acceptor vesicles, each containing a different fluorescent ceramide species. By CERT‐mediated transfer of fluorescent ceramide, a FRET system was established, which allows readout in 96‐well plate format, despite the high hydrophobicity of the components. Screening of a 2 000 compound library resulted in two new potent CERT inhibitors. One is approved for use in humans and one is approved for use in animals. Evaluation of cellular activity by quantitative mass spectrometry and confocal microscopy showed inhibition of ceramide trafficking and sphingomyelin biosynthesis.

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confidence: 99%

Liposomal FRET Assay Identifies Potent Drug‐Like Inhibitors of the Ceramide Transport Protein (CERT)

Samaha

Hamdo

Cong

et al. 2020

Chemistry A European J

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“…Bioluminescence resonance energy transfer (BRET) [2][3][4][5] and fluorescence resonance energy transfer (FRET) [6][7][8] have been frequently used for this purpose. However, despite numerous examples, these techniques are limited by low brightness and different maturation speed of RET donors and acceptors [9], poor spectral overlap [10], and a low dynamic range of resonance energy transfer (RET) from a donor to an acceptor within a distance of 2−10 nm [11].…”

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confidence: 99%

BRED: bioluminescence energy transfer to dye for monitoring ceramide trafficking in cell

Naseri

2021

Preprint

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Bioluminescence resonance energy transfer (BRET) is a genetically encoded proximity-based tool to study biomolecular interactions. However, conventional BRET is usually restricted to only a few types of interactions like protein-protein or protein-ligand interactions. We here developed a spatially unbiased resonance energy transfer system, so-called BRED - bioluminescence resonance energy transfer to dye. BRED allows transferring energy from a genetically encoded bright human optimized luciferase to a fluorophore-labelled small molecule. The high efficiency of the system allows RET without specific interaction of donor and acceptor. Here, we applied BRED to monitor the trafficking of the signalling lipid ceramide, to the Golgi. This was enabled by an engineered Golgi-resident luciferase, which was used to sense the influx of BODIPY-labeled ceramide into the surrounding membrane. We demonstrated the implementation of the method via flow cytometry, thereby combining the sensitivity of bulk cell methods with the advantages of single-cell analysis. This toolbox enables simple and robust live-cell analysis of inhibitors of CERT-mediated ceramide transport. The design principle of our optogenetic tool can be applied to study intracellular trafficking of metabolites and screen for inhibitors of their key enzymes.

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“…A ligand-binding peptide is sandwiched between a pair of donor and acceptor fluorophores, and ligand binding is observed via the FRET change. A set of FRET biosensors, based on three pairs of donor/acceptor, carboxyfluorescein (FAM)/Boron dipyrromethene (BODIPY) 85 , Nitrobenzoxadiazole (NBD)/nonsteroidal dye (Nile red) 86 , and coumarine/NBD 86 , was developed for real time monitoring of acid sphingomyelinase at high sensitivity and with high spatial resolution. The FRET biosensor is selectively cleaved by sphingomyelinase that leads to significant increase in fluorescence of the fluorescein FRET donor 85 .…”

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confidence: 99%

Application of combinatorial optimization strategies in synthetic biology

Naseri¹,

Koffas²

2020

Nat Commun

105

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In the first wave of synthetic biology, genetic elements, combined into simple circuits, are used to control individual cellular functions. In the second wave of synthetic biology, the simple circuits, combined into complex circuits, form systems-level functions. However, efforts to construct complex circuits are often impeded by our limited knowledge of the optimal combination of individual circuits. For example, a fundamental question in most metabolic engineering projects is the optimal level of enzymes for maximizing the output. To address this point, combinatorial optimization approaches have been established, allowing automatic optimization without prior knowledge of the best combination of expression levels of individual genes. This review focuses on current combinatorial optimization methods and emerging technologies facilitating their applications.

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A Novel Visible Range FRET Probe for Monitoring Acid Sphingomyelinase Activity in Living Cells

Cited by 13 publications

References 21 publications

Liposomal FRET Assay Identifies Potent Drug‐Like Inhibitors of the Ceramide Transport Protein (CERT)

Liposomal FRET Assay Identifies Potent Drug‐Like Inhibitors of the Ceramide Transport Protein (CERT)

BRED: bioluminescence energy transfer to dye for monitoring ceramide trafficking in cell

Application of combinatorial optimization strategies in synthetic biology

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