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Small molecule splicing modifiers with systemic HTT-lowering activity.

Authors :: Bhattacharyya A
Trotta CR
Narasimhan J
Wiedinger KJ
Li W
Effenberger KA
Woll MG
Jani MB
Risher N
Yeh S
Cheng Y
Sydorenko N
Moon YC
Karp GM
Weetall M
Dakka A
Gabbeta V
Naryshkin NA
Graci JD
Tripodi T Jr
Southwell A
Hayden M
Colacino JM
Peltz SW
Source :: Nature communications [Nat Commun] 2021 Dec 15; Vol. 12 (1), pp. 7299. Date of Electronic Publication: 2021 Dec 15.
Publication Year :: 2021
Abstract: Huntington's disease (HD) is a hereditary neurodegenerative disorder caused by expansion of cytosine-adenine-guanine (CAG) trinucleotide repeats in the huntingtin (HTT) gene. Consequently, the mutant protein is ubiquitously expressed and drives pathogenesis of HD through a toxic gain-of-function mechanism. Animal models of HD have demonstrated that reducing huntingtin (HTT) protein levels alleviates motor and neuropathological abnormalities. Investigational drugs aim to reduce HTT levels by repressing HTT transcription, stability or translation. These drugs require invasive procedures to reach the central nervous system (CNS) and do not achieve broad CNS distribution. Here, we describe the identification of orally bioavailable small molecules with broad distribution throughout the CNS, which lower HTT expression consistently throughout the CNS and periphery through selective modulation of pre-messenger RNA splicing. These compounds act by promoting the inclusion of a pseudoexon containing a premature termination codon (stop-codon psiExon), leading to HTT mRNA degradation and reduction of HTT levels.<br /> (© 2021. The Author(s).)