Abstract:<p>In
our manuscript we outline an approach in which we convert a promiscuous
pyrimidine scaffold into narrowly selective, cell-active chemical leads for
several understudied kinases, including DRAK1, BMP2K, and MARK4. These chemical
tools will allow illumination of the function(s) of these poorly characterized
kinases for the first time. Several of the understudied kinases that we inhibit
with our pyrimidine-based compounds are also implicated in neurodegenerative
disease, pushing the utility of kinase … Show more
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