Antisense oligonucleotide therapy for neurodegenerative disease
Richard A. Smith, … , C. Frank Bennett, Don W. Cleveland
Richard A. Smith, … , C. Frank Bennett, Don W. Cleveland
Published August 1, 2006
Citation Information: J Clin Invest. 2006;116(8):2290-2296. https://doi.org/10.1172/JCI25424.
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Research Article Neuroscience

Antisense oligonucleotide therapy for neurodegenerative disease

Abstract

Neurotoxicity from accumulation of misfolded/mutant proteins is thought to drive pathogenesis in neurodegenerative diseases. Since decreasing levels of proteins responsible for such accumulations is likely to ameliorate disease, a therapeutic strategy has been developed to downregulate almost any gene in the CNS. Modified antisense oligonucleotides, continuously infused intraventricularly, have been demonstrated to distribute widely throughout the CNS of rodents and primates, including the regions affected in the major neurodegenerative diseases. Using this route of administration, we found that antisense oligonucleotides to superoxide dismutase 1 (SOD1), one of the most abundant brain proteins, reduced both SOD1 protein and mRNA levels throughout the brain and spinal cord. Treatment initiated near onset significantly slowed disease progression in a model of amyotrophic lateral sclerosis (ALS) caused by a mutation in SOD1. This suggests that direct delivery of antisense oligonucleotides could be an effective, dosage-regulatable means of treating neurodegenerative diseases, including ALS, where appropriate target proteins are known.

Authors

Richard A. Smith, Timothy M. Miller, Koji Yamanaka, Brett P. Monia, Thomas P. Condon, Gene Hung, Christian S. Lobsiger, Chris M. Ward, Melissa McAlonis-Downes, Hongbing Wei, Ed V. Wancewicz, C. Frank Bennett, Don W. Cleveland

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Figure 6

Infusion of oliogonucleotides complementary to humanSOD1 mRNA extends survival in SOD1G93A rats.

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Infusion of oliogonucleotides complementary to humanS...
(AC) Antisense oligonucleotides complementary to human SOD1 mRNA were infused into the right lateral ventricle of 65-day-old SOD1G93A rats at 100 μg/d for 28 days (n = 11 [saline-infused]; 12 [SODr/h333611]). Disease onset (A) was defined as the peak animal weight, early disease (B) was defined as the point at which the animals had lost 10% of their peak weight, and survival (C) was defined as the inability of the animal to right itself within 30 seconds of being placed on its side.