2012
DOI: 10.1038/ejhg.2012.7
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Intragenic and large NIPBL rearrangements revealed by MLPA in Cornelia de Lange patients

Abstract: Cornelia de Lange syndrome (CdLS) is a rare multisystemic congenital anomaly disorder that is characterised by intellectual disability and growth retardation, congenital heart defects, intestinal anomalies, facial dysmorphism (including synophyris and high arched eyebrows) and limb reduction defects. Mutations in three cohesin-associated genes encoding a key regulator (NIPBL, chr 5p13.2) and one structural component of the cohesin ring (SMC1A, chr Xp11) occur in about 65% of CdLS patients. NIPBL is the major c… Show more

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Cited by 22 publications
(28 citation statements)
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“…Large-scale structural genomic rearrangements that disrupt the function of known CdLS genes have been reported as affecting NIPBL ,13 14 SMC1A ,15 HDAC8 12 and RAD21. 8 Rare copy number variants (CNVs) involving 1p36.23–36.22, 7p22.3, 17q24.2–25.3, 19p13.3 and 20q11.2-q12 have also been reported in association with CdLS-like features 16…”
Section: Introductionmentioning
confidence: 99%
“…Large-scale structural genomic rearrangements that disrupt the function of known CdLS genes have been reported as affecting NIPBL ,13 14 SMC1A ,15 HDAC8 12 and RAD21. 8 Rare copy number variants (CNVs) involving 1p36.23–36.22, 7p22.3, 17q24.2–25.3, 19p13.3 and 20q11.2-q12 have also been reported in association with CdLS-like features 16…”
Section: Introductionmentioning
confidence: 99%
“…Up to 60% of CdLS cases harbor mutations in NIPBL, which encodes a regulatory protein loading the cohesin complex onto the sister chromatids. Copy number variants (CNVs) in the NIPBL locus are found in approximately 5% of NIPBL point mutation-negative CdLS cases, while mosaic mutations in NIPBL are reported to account for an additional 23% (7)(8)(9)(10). SMC1A and SMC3 are core structural components of the cohesin complex.…”
Section: Introductionmentioning
confidence: 99%
“…In fact, a de novo balanced translocation involving chromosome 5 facilitated identification of the NIPBL gene (Tonkin et al 2004). Recently, a few reports have been published presenting several cases with sub-microscopic deletions encompassing the NIPBL gene, with the size of aberration ranging from 4.2 kb (a single exon) to 2 Mb deletion, including not only the NIPBL gene but also 14 adjacent genes (Bhuiyan et al 2007; Ratajska et al 2010; Oliver et al 2010, Murray et al 2012; Pehlivan et al 2012; Russo et al 2012). The incidence of genomic aberrations was estimated to be 4–5 % of CdLS patients negative for the NIPBL point mutation (Pehlivan et al 2012; Russo et al 2012).…”
Section: Discussionmentioning
confidence: 99%
“…Moreover, in a few cases, a large genomic rearrangement involving the NIPBL gene has been detected, indicating even higher complexity of the genetic background of the syndrome. Observed genomic alterations were mostly deletions, encompassing one or more of NIPBL exons; however, also, a few pathogenic duplications were reported (Bhuiyan et al 2007; Ratajska et al 2010; Oliver et al 2010; Murray et al 2012; Pehlivan et al 2012, Russo et al 2012). …”
Section: Introductionmentioning
confidence: 99%