Identification and Optimization of RNA-Splicing Modulators as Huntingtin Protein-Lowering Agents for the Treatment of Huntington's Disease.
Longbin LiuKarine MalaguAlan F HaughanVinod KhetarpalAndrew J StottWilliam EsmieuHuw D VaterStephen J WebsterAmanda J Van de PoëlCole ClissoldBrett CosgroveBenjamin SuttonJonathan A SpencerPerla BrecciaEmanuela GanciaSilvia BonomoTammy LadduwahettyOvadia LazariHiral PatelHelen C AttonSteve CliftonDaniel M MotaDario MagnaniAmy O'NeillMarta StebbedsNatsuko MacabuagDaniel ToddMaria E HervaPhilip MitchellMijke VisserSara Compte SancerniLaure Grand MourselMarta da SilvaEva KritikouTaneli T HeikkinenTamuna BolkvadzeValentina FodaleDebora SpadaforaManuel DaldinAlberto BrescianiJohn E MangetteElizabeth M DohertyMatthew R LeeTodd HerbstEdith MonteagudoDouglas MacdonaldNikolay V PlotnikovMark ChambersGeorge McAllisterIgnacio Muňoz-SanjuanCelia DominguezPublished in: Journal of medicinal chemistry (2023)
Huntington's disease (HD) is caused by an expanded CAG trinucleotide repeat in exon 1 of the huntingtin ( HTT ) gene. We report the design of a series of HTT pre-mRNA splicing modulators that lower huntingtin (HTT) protein, including the toxic mutant huntingtin (mHTT), by promoting insertion of a pseudoexon containing a premature termination codon at the exon 49-50 junction. The resulting transcript undergoes nonsense-mediated decay, leading to a reduction of HTT mRNA transcripts and protein levels. The starting benzamide core was modified to pyrazine amide and further optimized to give a potent, CNS-penetrant, and orally bioavailable HTT -splicing modulator 27 . This compound reduced canonical splicing of the HTT RNA exon 49-50 and demonstrated significant HTT-lowering in both human HD stem cells and mouse BACHD models. Compound 27 is a structurally diverse HTT -splicing modulator that may help understand the mechanism of adverse effects such as peripheral neuropathy associated with branaplam.