Clinical heterogeneity in lymphoedema-distichiasis with FOXC2 truncating mutations

Erickson, Robert P.; Dagenais, Susan L.; Caulder, Mark S; Downs, J. Crawford; Herman, Gail E.; Jones, Marilyn C.; Kerstjens-Frederikse, Wilhelmina S.; Lidral, Andrew C.; McDonald, Marie; Nelson, Christine C.; Witte, Marlys H.; Glover, Thomas W.

doi:10.1136/jmg.38.11.761

Cited by 94 publications

(88 citation statements)

References 21 publications

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“…The third was a missense mutation, and is only the second in FOXC2 so far identified as likely to give rise to LD, all the remainder being nonsense or frameshifts. [9][10][11][12] As the G362A (R121H) change is found in an isolated case of LD, it is impossible to prove that this is the causative mutation in this person. However, this is a highly conserved amino acid, being one of only 11 that are identical in 24 members of the forkhead family in the 100 amino acid DNA binding domain.…”

Section: Resultsmentioning

confidence: 99%

Analysis of the phenotypic abnormalities in lymphoedema-distichiasis syndrome in 74 patients with FOXC2 mutations or linkage to 16q24

Brice

2002

Journal of Medical Genetics

242

271

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Section: Resultsmentioning

confidence: 99%

Analysis of the phenotypic abnormalities in lymphoedema-distichiasis syndrome in 74 patients with FOXC2 mutations or linkage to 16q24

Brice

2002

Journal of Medical Genetics

242

271

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“…FOXC2, a Forkhead family transcription factor, is one of the few causative genes associated with human lymphatic disorder and malformation to date and is found to be responsible for lymphedema -distichiasis (double row of eye lashes) syndrome by multiple groups (Fang et al 2000;Erickson 2001;Erickson et al 2001;Finegold et al 2001;Bahuau et al 2002;Brice et al 2002;Traboulsi et al 2002;Kriederman et al 2003;Fabretto et al 2010). Foxc2 is expressed in both arterial and lymphatic endothelial cells and, along with Foxc1, is required for arterial specification and normal lymphatic sprouting from the vein during development (Dagenais et al 2004;Seo et al 2006;Kume 2009).…”

Section: Initial Steps For Lymphatic Specification and Differentiationmentioning

confidence: 99%

The New Era of the Lymphatic System: No Longer Secondary to the Blood Vascular System

Choi

Lee²,

Hong

2012

Cold Spring Harbor Perspectives in Medicine

117

106

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The blood and lymphatic systems are the two major circulatory systems in our body. Although the blood system has been studied extensively, the lymphatic system has received much less scientific and medical attention because of its elusive morphology and mysterious pathophysiology. However, a series of landmark discoveries made in the past decade has begun to change the previous misconception of the lymphatic system to be secondary to the more essential blood vascular system. In this article, we review the current understanding of the development and pathology of the lymphatic system. We hope to convince readers that the lymphatic system is no less essential than the blood circulatory system for human health and well-being.

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“…In humans, only three causative genes have been identified for disorders where lymphoedema is the primary phenotype; VEGFR3 in Milroy disease (Ferrell et al 1998, Irrthum et al 2000, FOXC2 for Lymphoedema distichiasis (Fang et al 2000, Bell et al 2001, Erickson et al 2001, Brice et al 2002) and mutations in SOX18 are responsible for causing the rare syndrome, hypotrichosislymphoedema-telangiectasia (Irrthum et al 2003). There are many other forms of primary lymphoedema where the genetic cause is unknown and the phenotype not well delineated.…”

Section: Introductionmentioning

confidence: 99%

Linkage and sequence analysis indicate that CCBE1 is mutated in recessively inherited generalised lymphatic dysplasia

et al. 2009

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Generalised lymphatic dysplasia (GLD) is chararacterised by extensive peripheral lymphoedema with visceral involvement. In some cases it presents in utero with hydrops fetalis. Autosomal dominant and recessive inheritance has been reported. A large, non-consanguineous family with three affected siblings with generalised lymphatic dysplasia is presented. One child died aged 5 months, one spontaneously miscarried at 17 weeks gestation, and the third has survived with extensive lymphoedema. All three presented with hydrops fetalis. There are seven other siblings who are clinically unaffected.Linkage analysis produced two loci on chromosome 18, covering 22Mb and containing 150 genes, one of which is CCBE1. A homozygous cysteine to serine change in CCBE1 has been identified in the proband, in exon 3, in a residue that is conserved across species. High density SNP analysis revealed homozygosity (a region of 900kb) around the locus for CCBE1 in all three affected cases. This indicates a likely ancestral mutation that is common to both parents; an example of a homozygous mutation representing Identity by Descent (IBD) in this pedigree. Recent studies in zebrafish have shown this gene to be required for lymphangiogenesis and venous sprouting and are therefore supportive of our findings. In view of the conserved nature of the cysteine, the nature of the amino acid change, the occurrence of a homozygous region around the locus, the segregation within the family, and the evidence from zebrafish, we propose that this mutation is causative for the generalised lymphatic dysplasia in this family, and may be of relevance in cases of non-immune hydrops fetalis.Introduction.

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Clinical heterogeneity in lymphoedema-distichiasis with FOXC2 truncating mutations

Cited by 94 publications

References 21 publications

Analysis of the phenotypic abnormalities in lymphoedema-distichiasis syndrome in 74 patients with FOXC2 mutations or linkage to 16q24

Analysis of the phenotypic abnormalities in lymphoedema-distichiasis syndrome in 74 patients with FOXC2 mutations or linkage to 16q24

The New Era of the Lymphatic System: No Longer Secondary to the Blood Vascular System

Linkage and sequence analysis indicate that CCBE1 is mutated in recessively inherited generalised lymphatic dysplasia

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