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  2. Multiplex imaging and cellular target identification of kinase inhibitors via an affinity-based proteome profiling approach

Multiplex imaging and cellular target identification of kinase inhibitors via an affinity-based proteome profiling approach

  • Sci Rep. 2015 Jan 12;5:7724. doi: 10.1038/srep07724.
Ying Su 1 Sijun Pan 1 Zhengqiu Li 1 Lin Li 1 Xiaoyuan Wu 1 Piliang Hao 2 Siu Kwan Sze 2 Shao Q Yao 1
Affiliations

Affiliations

  • 1 Department of Chemistry, National University of Singapore, 3 Science Drive 3, Singapore 117543.
  • 2 School of Biological Sciences, Nanyang Technological University, 60 Nanyang Drive, Singapore 637551.
Abstract

MLN8237 is a highly potent and presumably selective inhibitor of Aurora Kinase A (AKA) and has shown promising antitumor activities. Like other kinase inhibitors which target the ATP-binding site of kinases, MLN8237 might be expected to have potential cellular off-targets. Herein, we report the first photoaffinity-based, small molecule AKA probe capable of both live-cell imaging of AKA activities and in situ proteome profiling of potential off-targets of MLN8237 (including AKA-associating proteins). By using two mutually compatible, bioorthogonal reactions (copper-catalyzed azide-alkyne cycloaddition chemistry and TCO-tetrazine ligation), we demostrate small molecule-based multiplex bioimaging for simultaneous in situ monitoring of two important cell-cycle regulating kinases (AKA and CDK1). A broad range of proteins, as potential off-targets of MLN8237 and AKA's-interacting partners, is subsequently identified by affinity-based proteome profiling coupled with large-scale LC-MS/MS analysis. From these studies, we discover novel AKA interactions which were further validated by cell-based immunoprecipitation (IP) experiments.

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