2018
DOI: 10.3389/fgene.2018.00255
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Mosaic Intronic NIPBL Variant in a Family With Cornelia de Lange Syndrome

Abstract: Cornelia de Lange Syndrome (CdLS) is a well described multiple malformation syndrome caused by alterations in genes encoding subunits or regulators of the cohesin complex. In approximately 70% of CdLS patients, pathogenic NIPBL variants are detected and 15% of them are predicted to affect splicing. Moreover, a large portion of genetic variants in NIPBL was shown to be somatic mosaicism. Here we report two family members with different expression of the CdLS phenotype. In both individuals, a c.869-2A>G (r.869_1… Show more

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Cited by 7 publications
(13 citation statements)
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“…Interestingly despite only a tiny fraction of the total NIPBL mRNA seems represented by the alternative transcripts, likely undergoing degradation, their occurrence is sufficient for recognition of the CdLS phenotype. In conclusion, our data corroborates the previously reported case with the same branch site pathogenic variant ( 11 ) highlighting the significance and diagnostic impact of non-canonical intronic variants of NIPBL gene in CdLS patients and the graded clinical presentation of CdLS with detection of extremely mild adult cases through their progeny ( 10 ). It is well-known that the approximate detection rate of NIPBL pathogenic variants (~70%) also implemented by the recent widespread application of multigene panel and WES NGS ( 9 ), underestimates the fraction of cases with mild phenotype.…”
Section: Discussionsupporting
confidence: 91%
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“…Interestingly despite only a tiny fraction of the total NIPBL mRNA seems represented by the alternative transcripts, likely undergoing degradation, their occurrence is sufficient for recognition of the CdLS phenotype. In conclusion, our data corroborates the previously reported case with the same branch site pathogenic variant ( 11 ) highlighting the significance and diagnostic impact of non-canonical intronic variants of NIPBL gene in CdLS patients and the graded clinical presentation of CdLS with detection of extremely mild adult cases through their progeny ( 10 ). It is well-known that the approximate detection rate of NIPBL pathogenic variants (~70%) also implemented by the recent widespread application of multigene panel and WES NGS ( 9 ), underestimates the fraction of cases with mild phenotype.…”
Section: Discussionsupporting
confidence: 91%
“…Although the estimated frequency of NIPBL splicing defects is consistent ( 9 , 10 ), only two non-canonical splice variants are recorded in HGMD database: NM_133433:c.459-9G>A which effect is only predicted ( 4 ) and the branch site variant NM_133433:c.5329-15A>G, recurring in our patients and the previously described case ( 11 ). Sequencing of the proband's cDNA showed two aberrant transcripts a-Tr1 and a-Tr2, a finding consistent with the frequent detection of multiple mRNA species, widely reported for variants deeply located within an intron as those affecting the branch point ( 15 ).…”
Section: Discussionsupporting
confidence: 54%
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“…Unfortunately, the blood sample of this patient was not available for the study. In the patient CdLS02M, substitution (c.869-2A>G, p.Gly290_Lys498del) was detected in 23% (251/1115) and 51% (74/148) of reads in DNA extracted from blood and buccal swab samples, respectively (13). Finally, a novel intronic and mosaic variant of KMT2A (c.4012+1G>A) was found in 48% (349/823) of reads of DNA extracted from buccal swab sample of patient CdLS09.…”
Section: Resultsmentioning
confidence: 99%