Neuroimmunology
Multiple sclerosis: biological differences in children and adults
Apr. 30, 2024
MedLink®, LLC
3525 Del Mar Heights Rd, Ste 304
San Diego, CA 92130-2122
Toll Free (U.S. + Canada): 800-452-2400
US Number: +1-619-640-4660
Support: service@medlink.com
Editor: editor@medlink.com
ISSN: 2831-9125
Toll Free (U.S. + Canada): 800-452-2400
US Number: +1-619-640-4660
Support: service@medlink.com
Editor: editor@medlink.com
ISSN: 2831-9125
Nearly 3,000 illustrations, including video clips of neurologic disorders.
Every article is reviewed by our esteemed Editorial Board for accuracy and currency.
Full spectrum of neurology in 1,200 comprehensive articles.
Listen to MedLink on the go with Audio versions of each article.
The upper panel of the schematic shows all pathogenic variants in patients in whom a congenital myasthenic syndrome was the main feature, whereas the mutations in the lower panel are the pathogenic variants in patients diagnosed with D/L-2-HGA. (Source: Li W, Zhang M, Zhang L, et al. A case report of an intermediate phenotype between congenital myasthenic syndrome and D-2- and L-2-hydroxyglutaric aciduria due to novel SLC25A1 variants. BMC Neurol 2020;20[1]:278. Creative Commons Attribution 4.0 License, https://creativecommons.org/licenses/by/4.0. The figure has been modified by Dr. Douglas J Lanska.)