Novel pathogenic mutations and copy number variations in the <i>VPS13A</i> Gene in patients with chorea‐acanthocytosis

Tomiyasu, Akiyuki; Nakamura, Masayuki; Ichiba, Mio; Ueno, Shu‐ichi; Saiki, Sachio; Morimoto, Masaharu; Kobal, Jan; Kageyama, Yasufumi; Inui, Toshio; Wakabayashi, Keiji; Yamada, Tatsuo; Kanemori, Yuji; Jung, Hans H.; Tanaka, Haruhiko; Orimo, Satoshi; Afawi, Zaid; Blatt, Ilan; Aasly, Jan; Ujike, Hiroshi; Babovic‐Vuksanovic, Dusica; Josephs, Keith A.; Tohge, Rie; Rodrigues, Guilherme; Dupré, Nicolas; Yamada, Hidetaka; Yokochi, Fusako; Kotschet, Katya; Takei, Takanobu; Rudzińska, Monika; Szczudlik, Andrzej; Penco, Silvana; Fujiwara, Masaki; Tojo, Koji; Sano, Akira

doi:10.1002/ajmg.b.31206

Cited by 62 publications

(67 citation statements)

References 23 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…This finding reveals key adaptive changes that participated in the genetic makeup of each equine species, with functions involved in cellular interactions (DSG1, NCAN, TBC1D2) and trafficking (MYO5C, ZW10), metabolism (ACCS, SLC9A4, HMGCR), development (SEMA5A, FAT2), olfaction (BPIFB4), and immunity (ITIH4, SIGLEC1). Interestingly, mountain zebras showed positive selection signatures at VPS13A, a gene associated with locomotory and behavioral disorders (23,24), possibly in relation to their high sociability. The antiporter SLC9A4, involved in pH regulation and countering of adverse environmental conditions, was found to be positively selected in plains zebras, which experience a wide range of environments throughout their geographical range.…”

Section: Resultsmentioning

confidence: 99%

Speciation with gene flow in equids despite extensive chromosomal plasticity

Jónsson

Schubert

Seguin-Orlando

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

190

186

View full text Add to dashboard Cite

Horses, asses, and zebras belong to a single genus, Equus, which emerged 4.0-4.5 Mya. Although the equine fossil record represents a textbook example of evolution, the succession of events that gave rise to the diversity of species existing today remains unclear. Here we present six genomes from each living species of asses and zebras. This completes the set of genomes available for all extant species in the genus, which was hitherto represented only by the horse and the domestic donkey. In addition, we used a museum specimen to characterize the genome of the quagga zebra, which was driven to extinction in the early 1900s. We scan the genomes for lineage-specific adaptations and identify 48 genes that have evolved under positive selection and are involved in olfaction, immune response, development, locomotion, and behavior. Our extensive genome dataset reveals a highly dynamic demographic history with synchronous expansions and collapses on different continents during the last 400 ky after major climatic events. We show that the earliest speciation occurred with gene flow in Northern America, and that the ancestor of present-day asses and zebras dispersed into the Old World 2.1-3.4 Mya. Strikingly, we also find evidence for gene flow involving three contemporary equine species despite chromosomal numbers varying from 16 pairs to 31 pairs. These findings challenge the claim that the accumulation of chromosomal rearrangements drive complete reproductive isolation, and promote equids as a fundamental model for understanding the interplay between chromosomal structure, gene flow, and, ultimately, speciation.equids | evolutionary genomics | speciation | admixture | chromosomal rearrangements

show abstract

Section: Resultsmentioning

confidence: 99%

Speciation with gene flow in equids despite extensive chromosomal plasticity

Jónsson

Schubert

Seguin-Orlando

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

190

186

View full text Add to dashboard Cite

show abstract

“…1 Concerning a pedigree with chorea-acanthocytosis in our previous reports, 1,[3][4][5]8 we would like to correct genetics materials associated with our pedigree already revised by Tomiyasu et al 7 In addition to a heterozygous splice site mutation (8035GϾA, transcript variant A [GenBank NM_033305.2]), which we had reported as 8295GϾA (using a different accession number) in the VPS13A genes of the patients (III-2 and III-3), we identified a novel nonsense mutation (1305GϾA, W435X) in the genes of the unaffected mother (II-4) and patients III-2 and III-3. 7 According to them, the inheritance pattern of the pedigree is actually autosomal recessive (pseudodominant).…”

mentioning

confidence: 98%

“…1 In their Correction, 1 Saiki et al mention with regret that "an error in sequencing occurred and the inheritance pattern should have been reported as autosomal recessive," with no reference to the recent publication of the full details of the mutations in this family. 7 This Correction effectively changes the impact of the original article and, even more so, its title message. We feel that it would be appropriate to retract the 2003 paper in order to reduce further confusion in the literature.…”

mentioning

confidence: 99%

Pilomotor seizure

Fisch¹,

Mégevand²,

Badoud³

et al. 2012

Neurology

View full text Add to dashboard Cite

A 68-year-old man complained of acute and recurrent episodes of diffuse gooseflesh variably accompanied by nonfluent aphasia, emotional distress, and focal myoclonic jerks (video 1 on the Neurology ® Web site at www.neurology.org), lasting about 2 minutes and occurring up to every 15 minutes. Contemporaneous EEG recording showed epileptic discharges over left temporal derivations (video 2). MRI showed a left temporal mass extending from the temporal pole to the pulvinar and involving amygdala and hippocampus (figure). Seizures were managed with valproate and levetiracetam. Partial lobectomy was performed demonstrating a grade III anaplastic astrocytoma. Pilomotor seizure 1,2 is a rare subtype of autonomic epilepsy related to temporal lesion of which it may be the presenting symptom, usually associated with other manifestations of temporal lobe epilepsy.L. Fisch, MD,* P. Mégevand, MD,* A. Badoud, PhD, M. Seeck, MD, P.R. Burkhard, MD, Geneva, Switzerland *These authors contributed equally to this work.Author contributions: Dr. Fisch: drafting and editing of the manuscript, acquisition, analysis, and interpretation of data. Dr. Mégevand: drafting and editing of the manuscript, acquisition, analysis, and interpretation of data. S. Badoud: drafting the manuscript, acquisition, analysis, and interpretation of data. Prof. Seeck: revision of the manuscript, acquisition, analysis, and interpretation of data. Prof. Burkhard: revision of the manuscript, acquisition, analysis and interpretation of data, study supervision and coordination.

show abstract

“…Tomiyasu et al 7 noted that the proband reported by Saiki et al is indeed compound heterozygous for mutations in the VPS13A (CHAC ) gene and, therefore, a typical recessive ChAc case. Subsequent to the publication of this report, we found the Correction only via PubMed but missed the original Correction in Neurology.…”

mentioning

confidence: 99%

Pilomotor seizure: When paroxysmal gooseflesh heralds brain tumor

Wilkins¹

2012

Neurology

View full text Add to dashboard Cite

Novel pathogenic mutations and copy number variations in the VPS13A Gene in patients with chorea‐acanthocytosis

Cited by 62 publications

References 23 publications

Speciation with gene flow in equids despite extensive chromosomal plasticity

Speciation with gene flow in equids despite extensive chromosomal plasticity

Pilomotor seizure

Pilomotor seizure: When paroxysmal gooseflesh heralds brain tumor

Contact Info

Product

Resources

About