Chemical engineering of therapeutic siRNAs for allele-specific gene silencing in Huntington’s disease models

Author:

Conroy Faith,Miller RachaelORCID,Alterman Julia F.,Hassler Matthew R.,Echeverria Dimas,Godinho Bruno M. D. C.ORCID,Knox Emily G.,Sapp Ellen,Sousa Jaquelyn,Yamada Ken,Mahmood Farah,Boudi Adel,Kegel-Gleason Kimberly,DiFiglia Marian,Aronin Neil,Khvorova AnastasiaORCID,Pfister Edith L.ORCID

Abstract

AbstractSmall interfering RNAs are a new class of drugs, exhibiting sequence-driven, potent, and sustained silencing of gene expression in vivo. We recently demonstrated that siRNA chemical architectures can be optimized to provide efficient delivery to the CNS, enabling development of CNS-targeted therapeutics. Many genetically-defined neurodegenerative disorders are dominant, favoring selective silencing of the mutant allele. In some cases, successfully targeting the mutant allele requires targeting single nucleotide polymorphism (SNP) heterozygosities. Here, we use Huntington’s disease (HD) as a model. The optimized compound exhibits selective silencing of mutant huntingtin protein in patient-derived cells and throughout the HD mouse brain, demonstrating SNP-based allele-specific RNAi silencing of gene expression in vivo in the CNS. Targeting a disease-causing allele using RNAi-based therapies could be helpful in a range of dominant CNS disorders where maintaining wild-type expression is essential.

Funder

CHDI Foundation

U.S. Department of Health & Human Services | NIH | National Institute of Neurological Disorders and Stroke

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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