Department of Neurology/Neurosurgery and Montreal Neurological Institute, McGill University, Montreal, QC H3A 2B4 Canada.
Brain Res Bull. 2012 Aug 1;88(5):444-53. doi: 10.1016/j.brainresbull.2012.05.003. Epub 2012 May 14.
Charcot-Marie-Tooth disease (CMT) is one of the most common inherited neurological disorders. It comprises a group of diseases caused by mutations in genes involved in Schwann cells homeostasis and neuronal function that affect the peripheral nerves. So far mutations in more than 33 genes have been identified causing either the demyelinating form (CMT1) or the axonal form (CMT2). Genes involving a large variety of unrelated functions may lead to the same phenotype when mutated. Our review will focus on the common link between genes causing axonal phenotypes like MFN2, KIF1B, DYNC1H1, Rab7, TRPV4, ARSs, NEFL, HSPB1, MPZ, and HSPB8. While KIF1B and DYNC1H1, two genes coding for molecular motors, are directly linked to axonal transport, the involvement of the other CMT2-causing genes in this function is less obvious. However, the last years have seen a growing list of evidence demonstrating that intracellular trafficking and mitochondrial dynamics might be dysfunctional in CMT2, and these mechanisms might present a common link between dissimilar CMT2-causing genes. The involvement of impaired transport in the pathogenesis of other rare neurological diseases or recessive CMT2 is also discussed.
Charcot-Marie-Tooth 病(CMT)是最常见的遗传性神经疾病之一。它由一组由于参与雪旺细胞稳态和神经元功能的基因突变引起的疾病组成,这些疾病影响外周神经。到目前为止,已经发现超过 33 种基因突变导致脱髓鞘形式(CMT1)或轴突形式(CMT2)。涉及各种不同功能的基因突变可能导致相同的表型。我们的综述将重点关注导致轴突表型的基因之间的共同联系,如 MFN2、KIF1B、DYNC1H1、Rab7、TRPV4、ARSs、NEFL、HSPB1、MPZ 和 HSPB8。虽然编码分子马达的两个基因 KIF1B 和 DYNC1H1 与轴突运输直接相关,但其他 CMT2 致病基因在该功能中的参与则不那么明显。然而,近年来越来越多的证据表明,CMT2 中细胞内运输和线粒体动力学可能存在功能障碍,这些机制可能是不同的 CMT2 致病基因之间的共同联系。受损运输在其他罕见神经疾病或隐性 CMT2 发病机制中的作用也在讨论中。
