SURF1 deficiency causes demyelinating Charcot-Marie-Tooth disease

Echaniz‐Laguna, Andoni; Ghezzi, Daniele; Chassagne, Maïté; Mayençon, Martine; Padet, Sylvie; Melchionda, Laura; Rouvet, Isabelle; Lannes, Béatrice; Bozon, Dominique; Latour, Philippe; Zeviani, Massimo; Camaret, Bénédicte Mousson de

doi:10.1212/wnl.0b013e3182a4a518

Cited by 57 publications

(34 citation statements)

References 27 publications

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“…Compound heterozygous truncating mutations in SURF1 were identified in a proband with demyelinating CMT. Loss of function mutations in SURF1 were recently described in patients with autosomal recessive severe demyelinating neuropathy of childhood onset [Echaniz-Laguna, 2013], consistent with this patient’s clinical and molecular findings.…”

Section: Resultssupporting

confidence: 84%

Exome Sequence Analysis Suggests that Genetic Burden Contributes to Phenotypic Variability and Complex Neuropathy

et al. 2015

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Charcot-Marie-Tooth (CMT) disease is a clinically and genetically heterogeneous distal symmetric polyneuropathy. Whole-exome sequencing (WES) of 40 individuals from 37 unrelated families with CMT-like peripheral neuropathy refractory to molecular diagnosis identified apparent causal mutations in ~45% (17/37) of families. Three candidate disease genes are proposed, supported by a combination of genetic and in vivo studies. Aggregate analysis of mutation data revealed a significantly increased number of rare variants across 58 neuropathy associated genes in subjects versus controls; confirmed in a second ethnically discrete neuropathy cohort, suggesting mutation burden potentially contributes to phenotypic variability. Neuropathy genes shown to have highly penetrant Mendelizing variants (HMPVs) and implicated by burden in families were shown to interact genetically in a zebrafish assay exacerbating the phenotype established by the suppression of single genes. Our findings suggest that the combinatorial effect of rare variants contributes to disease burden and variable expressivity.

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Section: Resultssupporting

confidence: 84%

Exome Sequence Analysis Suggests that Genetic Burden Contributes to Phenotypic Variability and Complex Neuropathy

et al. 2015

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“…Interestingly, mutations of proteins involved in alternative splicing, such as the RNA‐binding protein quaking I (QKI; MIM #609590), result in severe central and peripheral dys/demyelination [Mandler et al., ]. Indeed, mutations and genetic rearrangements occurring in CMT neuropathies disrupt alternative splicing and several myelin genes are alternatively spliced, including myelin basic protein (MBP), proteolipid protein (PLP), myelin‐associated glycoprotein MAG [Regis et al., ; Lassuthova et al., ; Padhi and Pelletier, ; Park et al., ; Echaniz‐Laguna et al., ; Zearfoss et al., ; Tamiya et al., ]. PMP22 has three known variants arising from three distinct primary transcripts.…”

Section: Introductionmentioning

confidence: 99%

Alternative Splicing in the HumanPMP22Gene: Implications in CMT1A Neuropathy

et al. 2015

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CMT1A patients commonly share PMP22 genetic overloading but they show phenotypic heterogeneity and variability in PMP22 mRNA and protein expression. Moreover, PMP22 mRNA levels do not correlate with clinical outcome measures in these patients, suggesting their uselessness as a disease biomarker. Thus, in-depth analysis of PMP22 transcription and translation might help to define its pathogenic role in CMT1A. We focused on the alternative splicing of PMP22 gene to verify whether mRNA processing is altered in CMT1A. We identified three new PMP22 transcripts enriched in human sural nerve biopsies. One of them was an untranslated variant, whereas the other two originated from a PMP22 undescribed exon and encoded for a new putative protein localized in the endoplasmic reticulum. As splicing events in the PMP22 gene are differently regulated in tissues and during development, we analyzed the levels of PMP22 transcripts and their splicing pattern in human and experimental CMT1A. We found an altered PMP22 splicing ratio in the CMT1A rat. In addition, we showed a remarkable derangement in rat QKI expression, which is a critical regulator of splicing during myelination. Overall, our data suggest that an alteration of mRNA processing could be a pathogenic mechanism in CMT1A.

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“…In these patients, nerve conduction velocities are decreased and nerve biopsy is suggestive of a myelinopathy, with disproportionately thin myelinated fibers and loss of large myelinated fibers [20]. In some patients, the CNS dysfunction is very limited, appears later than the PNP [21], and lifespan is much longer, two of the three patients reported to date being older than 40 years of age. In one patient, nerve biopsy showed features of chronic demyelinating neuropathy, with moderate axonal loss, presence of onion bulbs, and hypomyelinated fibers [21].…”

Section: Mitochondrial Dna Depletionmentioning

confidence: 94%

“…In some patients, the CNS dysfunction is very limited, appears later than the PNP [21], and lifespan is much longer, two of the three patients reported to date being older than 40 years of age. In one patient, nerve biopsy showed features of chronic demyelinating neuropathy, with moderate axonal loss, presence of onion bulbs, and hypomyelinated fibers [21].…”

Section: Mitochondrial Dna Depletionmentioning

confidence: 99%

Peripheral neuropathies in mitochondrial disorders

Funalot

2014

Peripheral Nerve Disorders

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SURF1 deficiency causes demyelinating Charcot-Marie-Tooth disease

Cited by 57 publications

References 27 publications

Exome Sequence Analysis Suggests that Genetic Burden Contributes to Phenotypic Variability and Complex Neuropathy

Exome Sequence Analysis Suggests that Genetic Burden Contributes to Phenotypic Variability and Complex Neuropathy

Alternative Splicing in the HumanPMP22Gene: Implications in CMT1A Neuropathy

Peripheral neuropathies in mitochondrial disorders

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