A solid-phase DNA-encoded library (DEL) was studied for
binding
the RNA repeat expansion r(CUG)exp, the
causative agent of the most common form of adult-onset muscular dystrophy,
myotonic dystrophy type 1 (DM1). A variety of uncharged and novel
RNA binders were identified to selectively bind r(CUG)exp by using a two-color flow cytometry screen. The cellular
activity of one binder was augmented by attaching it with a module
that directly cleaves r(CUG)exp. In DM1
patient-derived muscle cells, the compound specifically bound r(CUG)exp and allele-specifically eliminated r(CUG)exp, improving disease-associated defects.
The approaches herein can be used to identify and optimize ligands
and bind RNA that can be further augmented for functionality including
degradation.
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