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2 záznamů v Medvik Filtry

Článek

Distinct patterns of complex rearrangements and a mutational signature of microhomeology are frequently observed in PLP1 copy number gain structural variants

Bahrambeigi, Vahid
Autor Bahrambeigi, Vahid Graduate Program in Diagnostic Genetics, School of Health Professions, The University of Texas MD Anderson Cancer Center, Houston, TX, USA. Present address: Graduate School of Biomedical Sciences, The University of Texas MD Anderson Cancer Center UTHealth, Houston, TX, USA
Song, Xiaofei
Autor Song, Xiaofei Department of Molecular and Human Genetics, Baylor College of Medicine, One Baylor Plaza, Room 604B, Houston, TX, USA
Sperle, Karen
Autor Sperle, Karen Nemours Biomedical Research, Nemours/Alfred I. DuPont Hospital for Children, 1600 Rockland Road, RC1, Wilmington, DE, USA
Beck, Christine R
Autor Beck, Christine R Department of Molecular and Human Genetics, Baylor College of Medicine, One Baylor Plaza, Room 604B, Houston, TX, USA. Present address: Department of Genetics and Genome Sciences, University of Connecticut Health Center and the Jackson Laboratory for Genomic Medicine, Farmington, CT, USA
Hijazi, Hadia
Autor Hijazi, Hadia Department of Molecular and Human Genetics, Baylor College of Medicine, One Baylor Plaza, Room 604B, Houston, TX, USA
Grochowski, Christopher M
Autor Grochowski, Christopher M Department of Molecular and Human Genetics, Baylor College of Medicine, One Baylor Plaza, Room 604B, Houston, TX, USA
Gu, Shen
Autor Gu, Shen School of Biomedical Sciences, Faculty of Medicine, The Chinese University of Hong Kong, Shatin, NT, Hong Kong SAR
Seeman, Pavel
Autor Seeman, Pavel DNA Laboratory, Department of Pediatric Neurology, 2nd Faculty of Medicine, Charles University in Prague and University Hospital Motol, 150 06, Prague, Czech Republic
Woodward, Karen J
Autor Woodward, Karen J Clinical and Molecular Genetics Unit, Institute of Child Health, London, UK. Present address: Diagnostic Genomics, PathWest Laboratory Medicine, Perth, WA, Australia. School of Biomedical Sciences, University of Western Australia, Perth, WA, Australia
Carvalho, Claudia M B
Autor Carvalho, Claudia M B Department of Molecular and Human Genetics, Baylor College of Medicine, One Baylor Plaza, Room 604B, Houston, TX, USA

Genome medicine. 2019 ; 11 (1) : 80. [pub] 20191209

Genome Med
ISSN 1756-994X
Medvik
Zdroj

BACKGROUND: We investigated the features of the genomic rearrangements in a cohort of 50 male individuals with proteolipid protein 1 (PLP1) copy number gain events who were ascertained with Pelizaeus-Merzbacher disease (PMD; MIM: 312080). We then compared our new data to previous structural variant mutagenesis studies involving the Xq22 region of the human genome. The aggregate data from 159 sequenced join-points (discontinuous sequences in the reference genome that are joined during the rearrangement process) were studied. Analysis of these data from 150 individuals enabled the spectrum and relative distribution of the underlying genomic mutational signatures to be delineated. METHODS: Genomic rearrangements in PMD individuals with PLP1 copy number gain events were investigated by high-density customized array or clinical chromosomal microarray analysis and breakpoint junction sequence analysis. RESULTS: High-density customized array showed that the majority of cases (33/50; ~ 66%) present with single duplications, although complex genomic rearrangements (CGRs) are also frequent (17/50; ~ 34%). Breakpoint mapping to nucleotide resolution revealed further previously unknown structural and sequence complexities, even in single duplications. Meta-analysis of all studied rearrangements that occur at the PLP1 locus showed that single duplications were found in ~ 54% of individuals and that, among all CGR cases, triplication flanked by duplications is the most frequent CGR array CGH pattern observed. Importantly, in ~ 32% of join-points, there is evidence for a mutational signature of microhomeology (highly similar yet imperfect sequence matches). CONCLUSIONS: These data reveal a high frequency of CGRs at the PLP1 locus and support the assertion that replication-based mechanisms are prominent contributors to the formation of CGRs at Xq22. We propose that microhomeology can facilitate template switching, by stabilizing strand annealing of the primer using W-C base complementarity, and is a mutational signature for replicative repair.

MeSH
body zlomu chromozomu MeSH
duplikace genu MeSH
genetická predispozice k nemoci MeSH
genetické asociační studie MeSH
genom lidský MeSH
genomika metody MeSH
genová přestavba * MeSH
jednonukleotidový polymorfismus MeSH
lidé MeSH
mutace * MeSH
myelinový proteolipidový protein genetika MeSH
nestabilita genomu MeSH
srovnávací genomová hybridizace MeSH
variabilita počtu kopií segmentů DNA * MeSH
Check Tag
lidé MeSH
Publikační typ
časopisecké články MeSH
práce podpořená grantem MeSH
Research Support, N.I.H., Extramural MeSH

Článek

Association of rare non-coding SNVs in the lung-specific FOXF1 enhancer with a mitigation of the lethal ACDMPV phenotype

Human genetics. 2019 ; 138 (11-12) : 1301-1311. [pub] 20191104

Hum. genet.
ISSN 1432-1203
Medvik
Zdroj

Haploinsufficiency of FOXF1 causes alveolar capillary dysplasia with misalignment of pulmonary veins (ACDMPV), a lethal neonatal lung developmental disorder. We describe two similar heterozygous CNV deletions involving the FOXF1 enhancer and re-analyze FOXF1 missense mutation, all associated with an unexpectedly mitigated disease phenotype. In one case, the deletion of the maternal allele of the FOXF1 enhancer caused pulmonary hypertension and histopathologically diagnosed MPV without the typical ACD features. In the second case, the deletion of the paternal enhancer resulted in ACDMPV rather than the expected neonatal lethality. In both cases, FOXF1 expression in lung tissue was higher than usually seen or expected in patients with similar deletions, suggesting an increased activity of the remaining allele of the enhancer. Sequencing of these alleles revealed two rare SNVs, rs150502618-A and rs79301423-T, mapping to the partially overlapping binding sites for TFAP2s and CTCF in the core region of the enhancer. Moreover, in a family with three histopathologically-diagnosed ACDMPV siblings whose missense FOXF1 mutation was inherited from the healthy non-mosaic carrier mother, we have identified a rare SNV rs28571077-A within 2-kb of the above-mentioned non-coding SNVs in the FOXF1 enhancer in the mother, that was absent in the affected newborns and 13 unrelated ACDMPV patients with CNV deletions of this genomic region. Based on the low population frequencies of these three variants, their absence in ACDMPV patients, the results of reporter assay, RNAi and EMSA experiments, and in silico predictions, we propose that the described SNVs might have acted on FOXF1 enhancer as hypermorphs.

MeSH
dítě MeSH
dospělí MeSH
fenotyp MeSH
forkhead transkripční faktory genetika MeSH
genomový imprinting MeSH
jednonukleotidový polymorfismus * MeSH
lidé MeSH
missense mutace * MeSH
novorozenec MeSH
prognóza MeSH
sekvenční delece * MeSH
syndrom přetrvávajícího fetálního oběhu genetika patologie prevence a kontrola MeSH
zesilovače transkripce * MeSH
Check Tag
dítě MeSH
dospělí MeSH
lidé MeSH
novorozenec MeSH
ženské pohlaví MeSH
Publikační typ
časopisecké články MeSH
kazuistiky MeSH

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