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Selective labelling of GBA2 in cells with fluorescent β-d-arabinofuranosyl cyclitol aziridines. | LitMetric

AI Article Synopsis

  • GBA2 is an enzyme that plays a critical role in breaking down glucosylceramide and has been linked to diseases like Sandhoff and Niemann-Pick type C, as well as parkinsonism.
  • Researchers have developed a specific activity-based probe (ABP) to study GBA2, which shows promise as a tool for visualizing and understanding this enzyme's function and location within cells.
  • The probe, β-d-arabinofuranosyl cyclitol aziridine, selectively binds to GBA2, allowing researchers to distinguish its subcellular localization from that of another enzyme, GBA1, and suggests a pathway for developing new GBA2 inhibitors for future clinical use.

Article Abstract

GBA2, the non-lysosomal β-glucosylceramidase, is an enzyme involved in glucosylceramide metabolism. Pharmacological inhibition of GBA2 by -alkyl iminosugars is well tolerated and benefits patients suffering from Sandhoff and Niemann-Pick type C diseases, and GBA2 inhibitors have been proposed as candidate-clinical drugs for the treatment of parkinsonism. With the ultimate goal to unravel the role of GBA2 in (patho)physiology, we sought to develop a GBA2-specific activity-based probe (ABP). A library of probes was tested for activity against GBA2 and the two other cellular retaining β-glucosidases, lysosomal GBA1 and cytosolic GBA3. We show that β-d-arabinofuranosyl cyclitol aziridine (β-d-Araf aziridine) reacts with the GBA2 active site nucleophile to form a covalent and irreversible bond. Fluorescent β-d-Araf aziridine probes potently and selectively label GBA2 both and , allowing for visualization of the localization of overexpressed GBA2 using fluorescence microscopy. Co-staining with an antibody selective for the lysosomal β-glucosylceramidase GBA1, shows distinct subcellular localization of the two enzymes. We proffer our ABP technology for further delineating the role and functioning of GBA2 in disease and propose the β-d-Araf aziridine scaffold as a good starting point for the development of GBA2-specific inhibitors for clinical development.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11375437PMC
http://dx.doi.org/10.1039/d3sc06146aDOI Listing

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