Recurrent central nervous system white matter changes in charcot–Marie–Tooth type X disease

Introduction: X‐linked Charcot–Marie–Tooth (CMT1X) disease is caused by mutations in the GJB1 gene. We describe a young man who presented with recurrent central nervous symptoms and transient white matter changes in the setting of a novel mutation in the GJB1 gene. Methods: Evaluation included clinical examination, neuroimaging, electrophysiological, and molecular genetic studies. Results: Clinical examination on 2 admissions 5 years apart demonstrated hemiparesis with findings of underlying peripheral neuropathy. Electrophysiologic studies revealed a sensorimotor polyneuropathy. MRI studies from both admissions revealed white matter changes, with improvement on an intervening study. Mutation analysis showed a novel mutation (c.98T>A; p.Ile33Asn) in the GJB1 gene. Conclusions: Mutations in GJB1 can result in recurrent central nervous system symptoms with transient white matter signal changes on MRI. In patients presenting with hemiparesis, the presence of signs of a peripheral neuropathy may facilitate identification of CMT1X, and is likely to affect clinical management. Muscle Nerve 49:451–454, 2014

[1]  S. Scherer,et al.  How do mutations in GJB1 cause X-linked Charcot–Marie–Tooth disease? , 2012, Brain Research.

[2]  S. Scherer,et al.  Gap junctions in inherited human disorders of the central nervous system. , 2012, Biochimica et biophysica acta.

[3]  M. S. van der Knaap,et al.  X‐linked hereditary motor sensory neuropathy (type 1) presenting with a stroke‐like episode , 2010, Developmental medicine and child neurology.

[4]  A. Panigrahy,et al.  Transient Leukoencephalopathy Associated With X-Linked Charcot-Marie-Tooth Disease , 2010, Journal of child neurology.

[5]  M. Shy,et al.  Persistent CNS dysfunction in a boy with CMT1X , 2009, Journal of the Neurological Sciences.

[6]  S. Henikoff,et al.  Predicting the effects of coding non-synonymous variants on protein function using the SIFT algorithm , 2009, Nature Protocols.

[7]  R. Reynolds,et al.  Human oligodendrocytes express Cx31.3: Function and interactions with Cx32 mutants , 2008, Neurobiology of Disease.

[8]  S. Scherer,et al.  CMT1X phenotypes represent loss of GJB1 gene function , 2007, Neurology.

[9]  H. Sasaki,et al.  X-linked Charcot-Marie-Tooth disease (CMTX) in a severely affected female patient with scattered lesions in cerebral white matter. , 2007, Internal medicine.

[10]  K. Zerres,et al.  Transient, recurrent, white matter lesions in X-linked Charcot-Marie-Tooth disease with novel connexin 32 mutation. , 2003, Archives of neurology.

[11]  K. Fischbeck,et al.  Transient central nervous system white matter abnormality in X‐linked Charcot‐Marie‐Tooth disease , 2002, Annals of neurology.

[12]  D. Paul,et al.  Connexin32 is a myelin-related protein in the PNS and CNS , 1995, The Journal of neuroscience : the official journal of the Society for Neuroscience.

[13]  K. Fischbeck,et al.  New connexin32 mutations associated with X-linked Charcot-Marie-Tooth disease , 1995, Neurology.