Autosomal dominant HMSN with proximal involvement: new Brazilian cases

Patroclo, Cristiane Borges; Lino, Angelina Maria Martins; Marchiori, P E; Brotto, Mario Wilson Iervolino; Hirata, Mário H.

doi:10.1590/s0004-282x2009000500021

Cited by 11 publications

(8 citation statements)

References 11 publications

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“…Although the TFG was first reported to be a fusion partner of the NTRK1 gene, 13 the RNA-seq data revealed no TFG fusion with other genes, including NTRK. COMMENT In the literature, [6][7][8] HMSN-P has been described only in Japanese descendants; however, we could not find any record of a blood relationship between the present Korean family and the Japanese. Therefore, to our knowledge, this is the first report of a family with HMSN-P outside of Japan who are not Japanese descendants.…”

Section: Identification Of a P285l Mutation In Tfgcontrasting

confidence: 58%

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Proximal Dominant Hereditary Motor and Sensory Neuropathy With Proximal Dominance Association With Mutation in the TRK-Fused Gene

Lee¹,

Lee²,

Park³

et al. 2013

JAMA Neurol

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Section: Identification Of a P285l Mutation In Tfgcontrasting

confidence: 58%

“…6 Until now, HMSN-P has been reported only in Japan or in Japanese descendants. 7,8 Takashima et al 6 mapped the locus on chromosome 3q14.1-q13. Later, they suggested a narrowed locus on 3q13.1 within 3.1 cM.…”

Section: Conclusion and Relevancementioning

confidence: 99%

Proximal Dominant Hereditary Motor and Sensory Neuropathy With Proximal Dominance Association With Mutation in the TRK-Fused Gene

Lee¹,

Lee²,

Park³

et al. 2013

JAMA Neurol

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“…Its description emphasizes proximal dominant muscle weakness and atrophy, and also includes mild but obvious sensory dysfunction, fasciculation, decreased deep tendon reflexes, axonal degeneration in the peripheral nerves, and autosomal dominant inheritance. The disease appeared to be rare, and was originally reported only in patients of Japanese or Korean descent (Takashima et al, 1997;Takashima et al, 1999;Takahashi et al, 2007;Miura et al, 2008;Patroclo et al, 2009;Ishiura et al, 2012;Campellone, 2013;Lee et al, 2013). In 2015, we described a large Iranian HMSN-P affected pedigree and thus showed that the disease is not confined to individuals with Far East ancestry (Alavi et al, 2015).…”

Section: Introductionmentioning

confidence: 66%

“…A detailed comparison of phenotypic features of earlier described HMSN-P patients, all with the same p.Pro285Leu mutation in TFG, emphasized notable clinical variability within the framework of the original description of the disease (Takashima et al, 1997;Alavi et al, 2015 ). Some of the variable features were age at onset (from early 20's to late 60's), rate of disease progression, temporal order of upper and lower limb involvement, proximal only/ proximal and distal muscle weakness, and symmetric/ asymmetric onset (Maeda et al, 2007;Takahashi et al, 2007;Miura et al, 2008;Patroclo et al, 2009;Ishiura et al, 2012;Lee et al, 2013;Maeda, 2013;Alavi et al, 2015).…”

Section: Discussionmentioning

confidence: 99%

Identification of novel TFG mutation in HMSN-P pedigree: Emphasis on variable clinical presentations

Khani

Shamshiri

Alavi

et al. 2016

Journal of the Neurological Sciences

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We aimed to identify the genetic cause of neurological disease in an Iranian pedigree whose manifestations suggested hereditary motor and sensory neuropathy with proximal predominance (HMSN-P). Identification of a p.Gly269Val mutation in TFG, the known HMSN-P causative gene, provided supportive evidence. Subjective, biochemical, electrodiagnostic, and imaging data were compared with previously reported HMSN-P patients, including patients of an earlier described Iranian pedigree. Although notable clinical variability was found, comparable involvement of proximal and distal muscles was observed in both Iranian pedigrees. Interestingly, the same p.Gly269Val mutation was recently reported as cause of Charcot-Marie-Tooth disease type 2 in a Taiwanese pedigree. The likelihood that the two pedigrees with the p.Gly269Val mutation are not affected with different diseases is discussed. Identification of a second Iranian HMSN-P pedigree further confirms that HMSN-P is not confined to the Far East. Furthermore, p.Pro285Leu that has been the only TFG mutation thus far reported in HMSN-P patients is not the only mutation that can cause the disease. It is emphasized HMSN-P is a neuronopathy.

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“…Except for two recently described families from Iran, all reported HMSN‐P patients had Far East, usually Japanese, ancestry (Campellone, ; Ishiura et al, ; Lee et al, ; Miura et al, ; Patroclo, Lino, Marchiori, Brotto, & Hirata, ; Sarapura‐Castro et al, ; Takahashi et al, ; Takashima et al, ; Takashima et al, ). Clinical descriptions in the more recently diagnosed patients from Iran emphasized variability in presentations.…”

Section: Introductionmentioning

confidence: 99%

Continuum of phenotypes in hereditary motor and sensory neuropathy with proximal predominance and Charcot–Marie–Tooth patients with TFG mutation

Khani

Taheri

Shamshiri

et al. 2019

American J of Med Genetics Pt A

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Charcot-Marie-Tooth (CMT) is a common neuropathy, and hereditary motor and sensory neuropathy with proximal predominance (HMSN-P) is a recently described rare neuromuscular disease. Although many genes have been implicated for CMT, TFG is the only known HMSN-P-causing gene. Within the framework of diagnostic criteria, clinical variation is evident among CMT-diagnosed and also HMSN-P-diagnosed individuals. Mutations that cause p.(Pro285Leu) and p.(Gly269Val) in TFG were earlier reported as cause of HMSN-P in two Iranian pedigrees. Here, we report the identification of p.(Gly269Val) in TFG as cause of CMT in a large Iranian pedigree. The clinical features of patients of the three pedigrees are presented and critically compared. Similarities between the two HMSN-P-diagnosed pedigrees with different TFG mutations, and differences between the two differentially diagnosed pedigrees with the same p.(Gly269Val) mutation were evident. The clinical features of the HMSN-P pedigree with the p.(Pro285Leu) and the CMT pedigree with the p.(Gly269Val) mutation were clearly congruent with the respective diagnoses, whereas the features of the HMSN-P-diagnosed pedigree with the p.(Gly269Val) were intermediate between the other two pedigrees. It is therefore suggested that the clinical features of the three Iranian pedigrees with TFG mutations and diagnosed with HMSN-P or CMT represent a continuum.

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Autosomal dominant HMSN with proximal involvement: new Brazilian cases

Cited by 11 publications

References 11 publications

Proximal Dominant Hereditary Motor and Sensory Neuropathy With Proximal Dominance Association With Mutation in the TRK-Fused Gene

Proximal Dominant Hereditary Motor and Sensory Neuropathy With Proximal Dominance Association With Mutation in the TRK-Fused Gene

Identification of novel TFG mutation in HMSN-P pedigree: Emphasis on variable clinical presentations

Continuum of phenotypes in hereditary motor and sensory neuropathy with proximal predominance and Charcot–Marie–Tooth patients with TFG mutation

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