Chapter 38 Spinal muscular atrophy

Publication date: 2018 Source:Handbook of Clinical Neurology, Volume 148 Author(s): Eveline S. Arnold, Kenneth H. Fischbeck Autosomal-recessive proximal spinal muscular atrophy (Werdnig–Hoffmann, Kugelberg–Welander) is caused by mutation of the SMN1 gene, and the clinical severity correlates with the number of copies of a nearly identical gene, SMN2. The SMN protein plays a critical role in spliceosome assembly and may have other cellular functions, such as mRNA transport. Cell culture and animal models have helped to define the disease mechanism and to identify targets for therapeutic intervention. The main focus for developing treatment has been to increase SMN levels, and accomplishing this with small molecules, oligonucleotides, and gene replacement has been quite. An oligonucleotide, nusinersen, was recently approved for treatment in patients, and confirmatory studies of other agents are now under way.
Source: Handbook of Clinical Neurology - Category: Neurology Source Type: research