Periaxin mutation in Japanese patients with Charcot-Marie-Tooth disease

AbstractPeriaxin (PRX) plays an important role in the myelination of the peripheral nerve and consequently in the pathogenesis of Charcot-Marie-Tooth disease (CMT). To date, nine nonsense or frameshift PRX mutations have been reported in eight families with CMT. The patients with PRX mutations appeared to show characteristic clinical features with early onset but slow or no progression, a common result of mutations that lead to missing a C-terminal acidic domain. Here, we report a Japanese CMT patient with these characteristic clinical features, who was a compound heterozygote for PRX R1070X and L132FsX153 mutations. We previously reported that three Japanese isolated families also had the homozygous R1070X mutation. To examine the potential founder effect of the R1070X mutation in the Japanese population, we performed haplotype analysis and found that each R1070X allele lay on a different haplotype background in these four families. Therefore, the high frequency of the R1070X mutation among the Japanese population is not likely the consequence of a founder effect, but probably a result of a mutation hot spot.

[1]  I. Nonaka,et al.  Congenital hypomyelination neuropathy: decreased expression of the P2 protein in peripheral nerve with normal DNA sequence of the coding region , 1995, Journal of the Neurological Sciences.

[2]  S M Leber,et al.  Periaxin mutations cause recessive Dejerine-Sottas neuropathy. , 2001, American journal of human genetics.

[3]  D. Sherman,et al.  Periaxin expression in myelinating Schwann cells: modulation by axon-glial interactions and polarized localization during development. , 1995, Development.

[4]  J. Lupski,et al.  Periaxin mutations cause a broad spectrum of demyelinating neuropathies , 2002, Annals of neurology.

[5]  J. Lupski,et al.  Novel missense mutation in the early growth response 2 gene associated with Dejerine–Sottas syndrome phenotype , 1999, Neurology.

[6]  U. Suter,et al.  The causes of Charcot-Marie-Tooth disease , 2003, Cellular and Molecular Life Sciences CMLS.

[7]  D. Sherman,et al.  A Tripartite Nuclear Localization Signal in the PDZ-domain Protein L-periaxin* , 2000, The Journal of Biological Chemistry.

[8]  J. Lupski,et al.  Dejerine–Sottas syndrome associated with point mutation in the peripheral myelin protein 22 (PMP22) gene , 1993, Nature Genetics.

[9]  P. Brophy,et al.  Clinicopathological and genetic study of early-onset demyelinating neuropathy. , 2004, Brain : a journal of neurology.

[10]  D. Sherman,et al.  Specific Disruption of a Schwann Cell Dystrophin-Related Protein Complex in a Demyelinating Neuropathy , 2001, Neuron.

[11]  A. Mégarbané,et al.  A mutation in periaxin is responsible for CMT4F, an autosomal recessive form of Charcot-Marie-Tooth disease. , 2001, Human molecular genetics.

[12]  E. Shirahata,et al.  Periaxin mutation causes early-onset but slow-progressive Charcot-Marie-Tooth disease , 2004, Journal of Human Genetics.

[13]  Peter J. Brophy,et al.  Periaxin, a novel protein of myelinating schwann cells with a possible role in axonal ensheathment , 1994, Neuron.

[14]  N. Tachi,et al.  De novo mutation of the myelin Po gene in Dejerine–Sottas disease (hereditary motor and sensory neuropathy type III) , 1993, Nature Genetics.