Selective Targeting of the TPX2 Site of Importin‐α Using Fragment‐Based Ligand Design |
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| Authors: | Dr. Rhian S. Holvey Dr. Eugene Valkov Prof. David Neal Dr. Murray Stewart Prof. Chris Abell |
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| Affiliation: | 1. Department of Chemistry, University of Cambridge, Lensfield Road, Cambridge, CB2?1EW (UK);2. MRC Laboratory of Molecular Biology, Francis Crick Avenue, Cambridge, CB2?0QH (UK);3. University of Cambridge, Department of Oncology, Box 279, Addenbrooke's Hospital, Hills Road, Cambridge, CB2?0QQ (UK) |
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| Abstract: | Protein–protein interactions are difficult therapeutic targets, and inhibiting pathologically relevant interactions without disrupting other essential ones presents an additional challenge. Herein we report how this might be achieved for the potential anticancer target, the TPX2–importin‐α interaction. Importin‐α is a nuclear transport protein that regulates the spindle assembly protein TPX2. It has two binding sites—major and minor—to which partners bind. Most nuclear transport cargoes use the major site, whereas TPX2 binds principally to the minor site. Fragment‐based approaches were used to identify small molecules that bind importin‐α, and crystallographic studies identified a lead series that was observed to bind specifically to the minor site, representing the first ligands specific for this site. Structure‐guided synthesis informed the elaboration of these fragments to explore the source of ligand selectivity between the minor and major sites. These ligands are starting points for the development of inhibitors of this protein–protein interaction. |
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| Keywords: | cancer fragment‐based ligand design nuclear transporters protein– protein interactions structure‐guided ligand design |
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