Zeliha Matur scite author profile

Inherited peripheral neuropathies are frequent neuromuscular disorders known for their clinical and genetic heterogeneity. In 33 families, we identified 8 mutations in HINT1 (encoding histidine triad nucleotide-binding protein 1) by combining linkage analyses with next-generation sequencing and subsequent cohort screening of affected individuals. Our study provides evidence that loss of functional HINT1 protein results in a distinct phenotype of autosomal recessive axonal neuropathy with neuromyotonia.

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Are Acquired Hepatocerebral Degeneration and Hepatic Myelopathy Reversible?

Pınarbaşı¹,

Kaymakoğlu²,

Matur

et al. 2009

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Iatrogenic Botulism After Botulinum Toxin Type A Injections

Çoban

Matur²,

Hanağası³

et al. 2010

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Therapeutic use of botulinum toxin type A (BT/A) is well known, effective, and safe. Iatrogenic botulism that presents with generalized weakness, dysphagia, and respiratory distress is a rare but significant complication in BT/A treatment. In this study, we report 4 patients who developed iatrogenic botulism after receiving therapeutic doses of BT/A for spasticity and blepharospasm. One patient was placed in intensive care unit, but consequently, every patient recovered fully. The cause of BT/A as an adverse effect is most likely hematological spread of the toxin.

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Autosomal Dominant Cortical Tremor, Myoclonus, and Epilepsy Syndrome Mimicking Juvenile Myoclonic Epilepsy

Özemir

Akarsu

Matur

et al. 2016

Arch Neuropsychiatr

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Exonic duplication CNV of NDRG1 associated with autosomal-recessive HMSN-Lom/CMT4D

Okamoto

Goksungur

Pehlivan

et al. 2014

Genetics in Medicine

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Purpose Copy-number variations as a mutational mechanism contribute significantly to human disease. Approximately one-half of the patients with Charcot–Marie–Tooth (CMT) disease have a 1.4 Mb duplication copy-number variation as the cause of their neuropathy. However, non-CMT1A neuropathy patients rarely have causative copy-number variations, and to date, autosomal-recessive CMT disease has not been associated with copy-number variation as a mutational mechanism. Methods We performed Agilent 8 × 60K array comparative genomic hybridization on DNA from 12 recessive Turkish families with CMT disease. Additional molecular studies were conducted to detect breakpoint junctions and to evaluate gene expression levels in a family in which we detected an intragenic duplication copy-number variation. Results We detected an ~6.25 kb homozygous intragenic duplication in NDRG1, a gene known to be causative for recessive HMSNL/CMT4D, in three individuals from a Turkish family with CMT neuropathy. Further studies showed that this intragenic copy-number variation resulted in a homozygous duplication of exons 6–8 that caused decreased mRNA expression of NDRG1. Conclusion Exon-focused high-resolution array comparative genomic hybridization enables the detection of copy-number variation carrier states in recessive genes, particularly small copy-number variations encompassing or disrupting single genes. In families for whom a molecular diagnosis has not been elucidated by conventional clinical assays, an assessment for copy-number variations in known CMT genes might be considered.

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Zeliha Matur

Loss-of-function mutations in HINT1 cause axonal neuropathy with neuromyotonia

Are Acquired Hepatocerebral Degeneration and Hepatic Myelopathy Reversible?

Iatrogenic Botulism After Botulinum Toxin Type A Injections

Autosomal Dominant Cortical Tremor, Myoclonus, and Epilepsy Syndrome Mimicking Juvenile Myoclonic Epilepsy

Exonic duplication CNV of NDRG1 associated with autosomal-recessive HMSN-Lom/CMT4D

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