Monday, March 19, 2018
Ionis Pays to License TTR Drug
Sunday, March 11, 2018
Dicerna Supremely Confident About Clinical Pharmacology of its GalNAc Platform
Thursday, March 8, 2018
Commonly Used RNAi Trigger Modification Can Integrate into Genome and Cellular Transcripts
Saturday, March 3, 2018
Antisense Technology Produces Huntington’s Disease Breakthrough
It is widely thought that mutant huntingtin protein is harmful to the cell expressing it, ultimately resulting in neuronal death throughout the brain. This can be visualized by considerable, 30%-level atrophy of the brain over the course of the disease.
Although it is not possible to assess huntingtin levels directly in brain tissue in humans from biopsies, the experience in the preclinical animal models and human data from spinal muscular atrophy drug SPINRAZA allows one to model the correlation between ASO-dependent protein changes in the cerebrospinal fluid (CSF) and the various areas of the CNS quite well.
The future is bright
The study results therefore raise hopes that IONIS-HTTRx may halt or even reverse disease in manifest HD patients. As exciting and medically likely with the biggest bang for the buck is the prospect that the drug candidate may prevent disease symptoms to emerge in the first place when given early to those at risk of developing the disease (~1 in 2 with a parent having HD, 200,000 in the US alone).
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