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Multitarget affinity/specificity screening of natural products: finding and characterizing high-affinity ligands from complex mixtures by using high-performance mass spectrometry. | LitMetric

AI Article Synopsis

  • - This study presents a high-throughput screening method using electrospray ionization-Fourier transform ion cyclotron resonance mass spectrometry (ESI-FTICR) to investigate noncovalent interactions between RNA drug targets and components from a bacterial natural product library.
  • - The screening identifies molecules that bind to a synthetic RNA mimic of the prokaryotic 16S rRNA A-site, measuring both binding affinity and specificity by using a control RNA without the key structural feature.
  • - The results confirmed the expected binding of paromomycin and revealed a new molecule with specific binding to the A-site RNA, characterized as an aminoglycoside with modifications, showcasing the effectiveness of this multitarget affinity/specificity screening

Article Abstract

In this work we describe a high-throughput screening approach based on electrospray ionization-Fourier transform ion cyclotron resonance mass spectrometry (ESI-FTICR) that rapidly interrogates the noncovalent interaction between RNA-based drug targets and components derived from a bacterial natural product library. The screening process detects molecules present in the natural product library that bind to a synthetic RNA target that mimics the prokaryotic 16S rRNA A-site, while simultaneously measuring specificity for the synthetic A-site target using a control RNA target that lacks the critical structural element of the A-site construct. This screening approach known as multitarget affinity/specificity screening (MASS) demonstrated the expected binding of paromomycin from a fractionated natural product library derived from Streptomyces rimosus sp. paromomycinus. A new molecule was observed to bind with specificity to the 16S A-site RNA construct. MS/MS characterization of this species yielded partial structural information suggesting it is an aminoglycoside consisting of a paromomycin core with one or more modified rings. This work demonstrates the tremendous utility of MASS for screening natural product fractions against macromolecular targets.

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Source
http://dx.doi.org/10.1021/np0301137DOI Listing

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