AI Article Synopsis

  • Scientists have found a cool way to use a technique called surface-enhanced Raman spectroscopy (SERS) to see how small molecules, like the drug felodipine, attach to important proteins.
  • They showed that felodipine specifically binds to a protein called Aurora A kinase and can help slow down cancer growth in mice.
  • This research helps to identify special spots on proteins, which could lead to new medicines that target similar proteins in the body.

Article Abstract

We demonstrate the use of surface-enhanced Raman spectroscopy (SERS) as an excellent tool for identifying the binding site of small molecules on a therapeutically important protein. As an example, we show the specific binding of the common antihypertension drug felodipine to the oncogenic Aurora A kinase protein via hydrogen bonding interactions with Tyr-212 residue to specifically inhibit its activity. Based on SERS studies, molecular docking, molecular dynamics simulation, biochemical assays, and point mutation-based validation, we demonstrate the surface-binding mode of this molecule in two similar hydrophobic pockets in the Aurora A kinase. These binding pockets comprise the same unique hydrophobic patches that may aid in distinguishing human Aurora A versus human Aurora B kinase in vivo. The application of SERS to identify the specific interactions between small molecules and therapeutically important proteins by differentiating competitive and noncompetitive inhibition demonstrates its ability as a complementary technique. We also present felodipine as a specific inhibitor for oncogenic Aurora A kinase. Felodipine retards the rate of tumor progression in a xenografted nude mice model. This study reveals a potential surface pocket that may be useful for developing small molecules by selectively targeting the Aurora family kinases.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4115535PMC
http://dx.doi.org/10.1073/pnas.1402695111DOI Listing

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