NIPBL Mutational Analysis in 120 Individuals with Cornelia de Lange Syndrome and Evaluation of Genotype-Phenotype Correlations

Gillis, Lynette A.; McCallum, Jennifer; Kaur, Maninder; DeScipio, Cheryl; Yaeger, Dinah; Mariani, Allison; Kline, Antonie D.; Li, Hui Hua; Devoto, Marcella; Jackson, Laird G.; Krantz, Ian D.

doi:10.1086/424698

Cited by 284 publications

(354 citation statements)

References 33 publications

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“…A deletion removing the NIPBL region, however, was seen in a severe case of CdLS, supporting the idea that loss-offunction mutations cause CdLS (Hulinsky et al 2003). Many of the less severe cases of CdLS are associated with mutations that cause amino acid substitutions, although the general correlation of milder CdLS cases with missense mutations and more severe forms with truncations has exceptions (Bhuiyan et al 2005;Gillis et al 2004). Many polymorphisms are found in unaffected parents, and in addition to numerous other genetic differences between individuals, these polymorphisms could contribute to the phenotypic variability of the syndrome.…”

Section: Cornelia De Lange Syndrome (Cdls)mentioning

confidence: 71%

“…The first CdLS gene was mapped by linkage exclusion analysis and a de novo balanced translocation affecting the 5p13.1 region, which is one of the five non-excluded regions Tonkin et al 2004). Subsequent analysis revealed mutations in the NIPBL gene in 5p13.1 in many of the patients, and now several studies have identified a variety of NIPBL mutations in CdLS patients (Borck et al 2004;Bhuiyan et al 2005;Gillis et al 2004;Krantz et al 2004;Miyake et al 2005;Tonkin et al 2004). …”

Section: Cornelia De Lange Syndrome (Cdls)mentioning

confidence: 99%

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Roles of the sister chromatid cohesion apparatus in gene expression, development, and human syndromes

2006

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The sister chromatid cohesion apparatus mediates physical pairing of duplicated chromosomes. This pairing is essential for appropriate distribution of chromosomes into the daughter cells upon cell division. Recent evidence shows that the cohesion apparatus, which is a significant structural component of chromosomes during interphase, also affects gene expression and development. The Cornelia de Lange (CdLS) and Roberts/SC phocomelia (RBS/SC) genetic syndromes in humans are caused by mutations affecting components of the cohesion apparatus. Studies in Drosophila suggest that effects on gene expression are most likely responsible for developmental alterations in CdLS. Effects on chromatid cohesion are apparent in RBS/SC syndrome, but data from yeast and Drosophila point to the likelihood that changes in expression of genes located in heterochromatin could contribute to the developmental deficits.

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Section: Cornelia De Lange Syndrome (Cdls)mentioning

confidence: 71%

Section: Cornelia De Lange Syndrome (Cdls)mentioning

confidence: 99%

Roles of the sister chromatid cohesion apparatus in gene expression, development, and human syndromes

2006

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“…Each missense mutation affects a residue conserved in human NIPBL, and all are close to conserved residues altered by CdLScausing missense NIPBL mutations ( Fig. 2; Gillis et al 2004;Miyake et al 2005;Schoumans et al 2007). Two other Nipped-B mutations, Nipped-B NC7 and Nipped-B NC59 , truncate the encoded protein in the C-terminal region after the HEAT repeats, and four, Nipped-B NC6 , Nipped-B NC23 , Nipped-B NC41 , and Nipped-B NC77 , truncate the protein in the N-terminal region before the HEAT repeats.…”

Section: And 4)mentioning

confidence: 97%

Functional links between Drosophila Nipped-B and cohesin in somatic and meiotic cells

et al. 2007

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Drosophila Nipped-B is an essential protein that has multiple functions. It facilitates expression of homeobox genes and is also required for sister chromatid cohesion. Nipped-B is conserved from yeast to man, and its orthologs also play roles in deoxyribonucleic acid repair and meiosis. Mutation of the human ortholog, Nipped-B-Like (NIPBL), causes Cornelia de Lange syndrome (CdLS), associated with multiple developmental defects. The Nipped-B protein family is required for the cohesin complex that mediates sister chromatid cohesion to bind to chromosomes. A key question, therefore, is whether the Nipped-B family regulates gene expression, meiosis, and development by controlling cohesin. To gain insights into Nipped-B's functions, we compared the effects of several Nipped-B mutations on gene expression, sister chromatid cohesion, and meiosis. We also examined association of Nipped-B and cohesin with somatic and meiotic chromosomes by immunostaining. Missense Nipped-B alleles affecting the same HEAT repeat motifs as CdLS-causing NIPBL mutations have intermediate effects on both gene expression and mitotic chromatid cohesion, linking these two functions and the role of NIPBL in human development. Nipped-B colocalizes extensively with cohesin on chromosomes in both somatic and meiotic cells and is present in soluble complexes

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“…NIPBL maps to chromosome 5p13.2 and encodes delangin, the mammalian ortholog of Drosophila Nipped-B and yeast Scc2 which are both involved in sister chromatid cohesion by loading cohesin complexes onto chromatin (Strachan, 2005;Dorsett, 2006). CdLS-causing mutations are scattered throughout this large gene and include nonsense, frameshift, splice site, and missense DOI: 10.1002/humu.9478 mutations, as well as a mutation in the 5'untranslated region (5'UTR) and small in-frame deletions (Borck et al, 2004;Gillis et al, 2004;Krantz et al, 2004;Tonkin et al, 2004;Miyake et al, 2005;Bhuiyan et al, 2006;Borck et al, 2006;Yan et al, 2006). Absence of NIPBL mutations in half of affected persons suggested genetic heterogeneity in CdLS.…”

Section: Introductionmentioning

confidence: 99%

Incidence and clinical features of X-linked Cornelia de Lange syndrome due toSMC1L1 mutations

et al. 2007

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NIPBL Mutational Analysis in 120 Individuals with Cornelia de Lange Syndrome and Evaluation of Genotype-Phenotype Correlations

Cited by 284 publications

References 33 publications

Roles of the sister chromatid cohesion apparatus in gene expression, development, and human syndromes

Roles of the sister chromatid cohesion apparatus in gene expression, development, and human syndromes

Functional links between Drosophila Nipped-B and cohesin in somatic and meiotic cells

Incidence and clinical features of X-linked Cornelia de Lange syndrome due toSMC1L1 mutations

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