Epigenetic writers such as histone
acetyltransferases (HATs) control gene expression, which often goes awry in
cancer. The gene encoding the lysine acetyltransferase KAT6A, for example, is amplified
in multiple types of cancer, and its overexpression is associated with poor
clinical outcomes for patients with ER+ breast cancer. A recent
paper in Bioorg. Med. Chem. Lett. from Andrew Buesking and colleagues at
Prelude Therapeutics reports a new series of inhibitors.
The researchers started by considering
previously reported molecules such as PF-9363. Recognizing the importance of
the central sulfonamide, they generated a library of 150 fragments containing
this core and screened them in a biochemical assay. Taking a similar approach as
other researchers reporting on a different epigenetic target we discussed last year, the
Prelude team explicitly used ligand efficiency to call hits, setting the cutoff
at > 0.3 kcal per mol per heavy atom.
A direct deconstruction of PF-9363
led to compound 6, but, seeking something novel, the researchers were drawn to
compound 8, with similar ligand efficiency. Modifications were made to both of
the terminal aromatic groups, leading to compound 13, which was co-crystallized
with KAT6A. This led to further structure-guided modifications, with compound 25 being the most
potent.
Unfortunately, further improvements in potency were not forthcoming, and the ligand
efficiency had dropped steadily from both the initial fragment as well as PF-9363. The researchers conclude by stating that they “decided to pursue alternative
approaches.” Still, this paper is a nice, concise example of using metrics both
for pursuing a chemical series and, ultimately, discontinuing it.
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