Engel_2003_J.Neurocytol_32_1017

Reference

Title : Congenital myasthenic syndromes: A diverse array of molecular targets - Engel_2003_J.Neurocytol_32_1017
Author(s) : Engel AG , Ohno K , Sine SM
Ref : Journal of Neurocytology , 32 :1017 , 2003
Abstract :

The neuromuscular junction (NMJ) has served as a prototype for understanding mechanisms underlying synaptic transmission over the past 50 years. More recently, analysis of congenital myasthenic syndromes (CMS) revealed a diverse array of molecular targets and delineated their contributions to synaptic function. Clinical, electrophysiologic and morphologic studies have paved the way for detecting CMS-related mutations in proteins such as choline acetyltransferase acetylcholinesterase, the acetylcholine receptor, rapsyn, and the voltage-gated sodium channel of the Na(v)1.4 type. Further studies of the mutant proteins have allowed us to correlate the effects of the mutations with predicted alterations in protein structure. In this review, we focus on the symptomatology of the CMS, consider the factors that impair neuromuscular transmission, survey the mutations that have been uncovered in the different synaptic proteins, and consider the functional implications of the identified mutations.

PubMedSearch : Engel_2003_J.Neurocytol_32_1017
PubMedID: 15034283

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Citations formats

Engel AG, Ohno K, Sine SM (2003)
Congenital myasthenic syndromes: A diverse array of molecular targets
Journal of Neurocytology 32 :1017

Engel AG, Ohno K, Sine SM (2003)
Journal of Neurocytology 32 :1017