Two Novel Myelin Protein Zero Mutations in a Group of Chinese Patients

Chen, Bin; Zhang, Zaiqiang; Chen, Na; Li, Wei; Pan, Hua; Wang, Xingao; Ren, Yuting; Shi, Yuzhi; Tai, Hongfei; Niu, Songtao

doi:10.3389/fneur.2021.734515

Cited by 3 publications

(9 citation statements)

References 27 publications

(50 reference statements)

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“…However, some scholars have suggested that adult‐onset neuropathy does not necessarily imply that the disease will be mild [27,41]. In our study, although the average CMTNS of adult‐onset patients was lower than that of infantile‐onset patients, no statistically significant difference was observed, possibly because the sample size was insufficient; the infantile patients had a younger age at onset and relatively slower progression, whilst adult patients had an older age at onset and rapid progression [11,42]. The percentage of hearing loss in our study (5.4%) was lower than that reported by Sanmaneechai et al (20.4%) in the USA and was similar to that reported by Taniguchi et al in Japan, indicating that the occurrence of hearing loss might be less frequent in east Asia [24,29].…”

Section: Discussioncontrasting

confidence: 81%

Genotype–phenotype characteristics and baseline natural history of Chinese myelin protein zero gene related neuropathy patients

Liu

Lin

et al. 2023

Euro J of Neurology

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Background and purpose:The aim was to characterize the phenotypic and genotypic features of myelin protein zero (MPZ) related neuropathy and provide baseline data for longitudinal natural history studies or drug clinical trials. Method: Clinical, neurophysiological and genetic data of 37 neuropathy patients with MPZ mutations were retrospectively collected. Results: Nineteen different MPZ mutations in 23 unrelated neuropathy families were detected, and the frequency of MPZ mutations was 5.84% in total. Mutations c.103_104InsTGGTTTACACCG, c.513dupG, c.521_557del and c.696_699delCAGT had not been reported previously. Hot spot mutation p.Thr124Met was detected in four unrelated families, and seven patients carried de novo mutations. The onset age indicated a bimodal distribution: prominent clustering in the first and fourth decades. The infantile-onset group included 12 families, the childhood-onset group consisted of two families and the adult-onset group included nine families. The Charcot-Marie-Tooth Disease Neuropathy Score ranged from 3 to 25 with a mean value of 15.85 ± 5.88. Mutations that changed the cysteine residue (p.Arg98Cys, p.Cys127Trp, p.Ser140Cys and p.Cys127Arg) in the extracellular region were more likely to cause severe early-onset Charcot-Marie-Tooth disease type 1B (CMT1B) or Dejerine-Sottas syndrome. Nonsense-mediated mRNA decay mutations p.Asp35delInsVVYTD, p.Leu174Argfs*66 and p.Leu172Alafs*63 were related to severe infantile-onset CMT1B or Dejerine-Sottas syndrome; however, mutation p.Val232Valfs*19was associated with a relatively milder childhood-onset CMT1 phenotype. Conclusion:Four novel MPZ mutations are reported that expand the genetic spectrum.De novo mutations accounted for 30.4% and were most related to a severe infantileonset phenotype. Genetic and clinical data from this cohort will provide the baseline data necessary for clinical trials and natural history studies.

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Section: Discussioncontrasting

confidence: 81%

Genotype–phenotype characteristics and baseline natural history of Chinese myelin protein zero gene related neuropathy patients

Liu

Lin

et al. 2023

Euro J of Neurology

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“…More than 300 MPZ gene mutations have been identified as the cause of inherited peripheral neuropathy, exhibiting a wide range of phenotypes with varying severity of clinical symptoms [ 7 , 9 , 13 ]. The early-onset infantile and childhood phenotypes developmentally impair myelination, while the adult-onset phenotypes are characterized by axonal degeneration without prior demyelination [ 7 , 14 ]. Sanmaneechai and colleagues provided detailed descriptions of phenotypes of MPZ mutations from a cohort of 103 patients from 71 families with 47 different mutations [ 15 ].…”

Section: Discussionmentioning

confidence: 99%

“…Genetic studies confirmed a heterozygous identical variant of MPZ in Exon 2.c109G>A (p.Glu37Lys) for both patients 1 and 2. Inherited in an autosomal dominant fashion, this single-nucleotide variant has a cytogenetic location on chromosome 1q23.3 [ 7 , 12 ]. The variant was deemed to be of uncertain clinical significance by the lab as it has not been reported before.…”

Section: Case Presentationmentioning

confidence: 99%

“…While the PMP22 gene mutation is most frequently confirmed in CMT disease, greater than 100 gene mutations are known to cause CMT phenotypes which may be inherited in an autosomal dominant, autosomal recessive, or X-linked manner [ 1 , 7 ]. A type I transmembrane protein consisting of 248 amino acids and a member of the immunoglobulin supergene family, myelin protein zero (MPZ), is the most abundant structural protein in the peripheral nervous system myelin [ 8 , 9 ].…”

Section: Introductionmentioning

confidence: 99%

“…MPZ gene mutations are being increasingly recognized as causes of certain forms of hereditary peripheral neuropathy including CMT disease and early-onset Dejerine-Sottas disease [ 9 , 10 ]. Affecting 4.1-5% of all CMT patients, MPZ mutations are associated with the autosomal dominant demyelinating neuropathy CMT1B and axonal neuropathy CMT2I/J [ 7 , 9 ]. Additionally, point mutations in the MPZ gene account for 10-12% of all dominant demyelinating CMT type 1 cases [ 10 ].…”

Section: Introductionmentioning

confidence: 99%

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Clinical Features of a Newly Described Mutation of Myelin Protein Zero in a Family

Iyer¹,

Shields²,

Shields³

2023

Cureus

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Charcot-Marie-Tooth (CMT) disease is the most common hereditary neuropathy. Duplication of the peripheral myelin protein-22 ( PMP22 ) gene is the most frequent genetic abnormality in CMT disease. Although rare compared to PMP22 gene mutations, many different myelin protein zero ( MPZ ) gene mutations have been described in patients with CMT disease. MPZ gene mutations are known to cause hereditary neuropathies with heterogenous phenotypes ranging from early-onset severe demyelinating to adult-onset axonal forms. MPZ, the major protein component of peripheral nerve myelin, is important for myelin compaction. We report a family in which a mother and her son, both with adult-onset CMT disease, showed a newly described mutation p.Glu37Lys of the MPZ gene. The clinical features of the mother provided insight into the progression of the disease over decades, while features in the early stage of the disease could be studied in the son. Clinical, electrodiagnostic, and sonographic findings are described in the early and late stages of the disease. The MPZ gene mutation p.Glu37Lys is associated with clinical features of a progressive axonal type of adult-onset CMT disease.

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Structural bases for the Charcot-Marie-Tooth disease induced by single amino acid substitutions of myelin protein zero

Sakakura,

Tanabe,

Mori

et al. 2023

Structure

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Two Novel Myelin Protein Zero Mutations in a Group of Chinese Patients

Cited by 3 publications

References 27 publications

Genotype–phenotype characteristics and baseline natural history of Chinese myelin protein zero gene related neuropathy patients

Genotype–phenotype characteristics and baseline natural history of Chinese myelin protein zero gene related neuropathy patients

Clinical Features of a Newly Described Mutation of Myelin Protein Zero in a Family

Structural bases for the Charcot-Marie-Tooth disease induced by single amino acid substitutions of myelin protein zero

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