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Therapeutic strategies for Huntington's disease

Carlos Estevez‐Fraga, Michael Flower, Sarah J. Tabrizi

2020Current Opinion in Neurology30 citationsDOIOpen Access PDF

Abstract

PURPOSE OF REVIEW: Huntington's disease is a fatal autosomal dominant neurodegenerative disorder caused by a trinucleotide expansion in the HTT gene, and current therapies focus on symptomatic treatment. This review explores therapeutic approaches that directly target the pathogenic mutation, disrupt HTT mRNA or its translation. RECENT FINDINGS: Zinc-finger transcription repressors and CRISPR-Cas9 therapies target HTT DNA, thereby preventing all downstream pathogenic mechanisms. These therapies, together with RNA interference (RNAi), require intraparenchymal delivery to the brain in viral vectors, with only a single delivery potentially required, though they may carry the risk of irreversible side-effects.Along with RNAi, antisense oligonucleotides (ASOs) target mRNA, but are delivered periodically and intrathecally. ASOs have safely decreased mutant huntingtin protein (mHTT) levels in the central nervous system of patients, and a phase 3 clinical trial is currently underway.Finally, orally available small molecules, acting on splicing or posttranslational modification, have recently been shown to decrease mHTT in animal models. SUMMARY: Huntingtin-lowering approaches act upstream of pathogenic mechanisms and therefore have a high a priori likelihood of modifying disease course. ASOs are already in late-stage clinical development, whereas other strategies are progressing rapidly toward human studies.

Topics & Concepts

HuntingtinRNA interferenceCRISPRBiologyMedicineHuntington's diseaseDiseaseBioinformaticsRNANeuroscienceGeneticsGeneMutantPathologyGenetic Neurodegenerative DiseasesCRISPR and Genetic EngineeringAmyotrophic Lateral Sclerosis Research
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