Abstract:Monopolar spindle kinase 1 (MPS1/TTK) is a key element
of the mitotic checkpoint securing proper chromosome segregation. It is being
evaluated as a target in the treatment of aggressive tumors such as triple-negative
breast cancer with several reversible inhibitors currently undergoing clinical
trials. While long drug–target residence times have been suggested to be
beneficial in the context of therapeutic MPS1 inhibition, no irreversible
inhibitors are known. Here we present the design and characterization of… Show more
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