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

Connell, Fiona; Kalidas, Kamini; Østergaard, Pia; Brice, Glen; Homfray, Tessa; Roberts, Lesley; Bunyan, David J.; Mitton, Sally G.; Mansour, Sahar; Mortimer, Peter; Jeffery, Steve

doi:10.1007/s00439-009-0766-y

Cited by 87 publications

(84 citation statements)

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“…Moreover, the detection of mCcbe1 protein near Prox1 + LECs further supports the previously raised hypothesis that Ccbe1 protein might act as an extracellular guidance molecule regulating the budding and migration of lymphangioblasts from the anterior cardinal vein . In humans, homozygous and compound heterozygous mutations of hCCBE1 gene have also been shown to result in generalized lymphatic dysplasia associated with the very debilitating and highly deadly Hennekam syndrome (Connell et al, 2009;Alders et al, 2009). Despite the above mentioned and more preeminent defects in sues followed by absence of expression at later stages of heart development suggests that expression of mCcbe1 is limited to multipotent and highly proliferative progenitors and downregulated upon cellular commitment into more specific cardiac phenotypes.…”

Section: Discussionmentioning

confidence: 99%

“…lymphangiogenesis, cysteine to serine mutation of hCCBE1 gene (C75S) has also been shown to be associated with in hypertrofic cardiomyopathy and congenital heart defects (Connell et al, 2009;Alders et al, 2009). This raises the possibility of a role of Ccbe1 in the organogenesis of the heart from cardiac progenitors of the FHF, SHF and proepicardium where mCcbe1 is now reported to be expressed.…”

Section: A B Cmentioning

confidence: 99%

“…In humans, CCBE1 gene has also been associated with Hennekam syndrome, a disorder characterized by abnormal lymphatic system development causing generalized lymphedema, intestinal lymphangiectasias and mild to moderate levels of growth and mental retardation. Homozygous cysteine to serine mutation in a human CCBE1 (hCCBE1) gene region (exon 3) highly conserved across vertebrates has been shown to result in a generalized lymphatic dysplasia leading to significant morbidity and high mortality prevalence (Connell et al, 2009;Alders et al, 2009). While the importance of mCcbe1 for the development of the lymphatic system appears to be indisputable, its role in cardiac development has not been investigated despite the increasing evidence of a potential function in cardiogenesis.…”

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confidence: 99%

“…5 (Bos et al, 2011). Furthermore, some of the Hennekam syndrome patients carrying a mutated hCCBE1 gene were shown to possess congenital heart defects including hypertrophic cardiomyopathy and ventricular septal defects (Connell et al, 2009;Alders et al, 2009).…”

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Ccbe1 expression marks the cardiac and lymphatic progenitor lineages during early stages of mouse development

Facucho-Oliveira¹,

Bento²,

Belo³

2011

Int. J. Dev. Biol.

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The mammalian heart is a complex organ composed of diverse components and various cell types. Heart organogenesis requires the contribution of distinct pools of heart progenitors positioned in separate embryonic regions and subject to particular developmental signals. Moreover, these embryonic heart lineages have different transcriptional profiles expressing specific genes which activate pathways involved in heart lineage specification. Understanding the molecular control of heart organogenesis has major implications for treating congenital and adult heart diseases since specific heart lineages have been associated with particular human cardiovascular malformations. Collagen and calcium-binding EGF-like domain 1 (Ccbe1) was identified in our laboratory using an Affymetrix GeneChip system approach to identify the transcriptome of chick heart/hemangioblast precursor cells. Here, we present a detailed and systematic analysis of the expression of Ccbe1 during early mouse development using whole-mount in situ hybridization (WISH), immunohistochemistry and histological techniques. Ccbe1 mRNA was initially detected in the early cardiac progenitors of the two bilateral cardiogenic fields (E7.0) and in the cardiogenic mesoderm (E7.5 to E8.0). Ccbe1 mRNA was then persistently detected in the pericardium and transiently expressed in the myocardial tissue of the primitive heart tube (E8.25), being later expressed in the proepicardium. By E9.5, the Ccbe1 and Prox1 proteins were found to be expressed in common regions, including the septum transversum and in the proximity of the anterior cardinal vein. Here, it is shown that Ccbe1 is expressed in the FHF, SHF and proepicardium during heart organogenesis (E7.0 to E8.75). Later in development, Ccbe1 expression is localized in the septum transversum and in the vicinity of the anterior cardinal vein, embryonic structures related to hepatic and lymphatic development, respectively. KEY WORDS: Ccbe1, cardiogenic mesoderm, proepicardium, cardiogenesis, lymphangiogenesisCardiogenesis is dependent on three major pools of embryonic heart progenitors that are spatially and temporally segregated in the developing embryo and give rise to distinct cardiac structures (Harvey, 2002;Laugwitz et al., 2008). The cardiogenic mesoderm is the first major source of heart cell precursors to be identified during heart development (embryonic day (E) 7.0) and consists of two different population of heart progenitors, the first heart field (FHF) and the second heart field (SHF). The FHF is derived from the anterior splanchnic mesoderm and gives rise to the primitive heart tube that ultimately generates the bulk of the atrial chambers and the left ventriculum (Laugwitz et al., 2008;Vincent and Buckingham, 2010). The SHF is derived from the pharyngeal mesoderm and contributes to the outflow tract, the right ventricular Int.

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Section: Discussionmentioning

confidence: 99%

Section: A B Cmentioning

confidence: 99%

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confidence: 99%

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Ccbe1 expression marks the cardiac and lymphatic progenitor lineages during early stages of mouse development

Facucho-Oliveira¹,

Bento²,

Belo³

2011

Int. J. Dev. Biol.

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“…CCBE1 is essential for embryonic lymphangiogenesis in both zebrafish and mice (Hogan et al, 2009a;Bos et al, 2011) and is mutated in the human primary lymphoedema syndrome, Hennekam syndrome (Alders et al, 2009;Connell et al, 2010) (see also Table 1). CCBE1 is a secreted protein and loss-of-function phenotypes closely resemble those of Vegfc and Vegfr3 in zebrafish and VEGFC in mice (Hogan et al, 2009a;Bos et al, 2011).…”

Section: Reviewmentioning

confidence: 99%

Getting out and about: the emergence and morphogenesis of the vertebrate lymphatic vasculature

et al. 2013

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SummaryThe lymphatic vascular system develops from the pre-existing blood vasculature of the vertebrate embryo. New insights into lymphatic vascular development have recently been achieved with the use of alternative model systems, new molecular tools, novel imaging technologies and growing interest in the role of lymphatic vessels in human disorders. The signals and cellular mechanisms that facilitate the emergence of lymphatic endothelial cells from veins, guide migration through the embryonic environment, mediate interactions with neighbouring tissues and control vessel maturation are beginning to emerge. Here, we review the most recent advances in lymphatic vascular development, with a major focus on mouse and zebrafish model systems.

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Disorders Affecting Cutaneous Vasculature

Dompmartin

Revençu

Boon

et al. 2016

Rook's Textbook of Dermatology, Ninth Edition

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Skin is rich in blood and lymphatic vessels. These can undergo abnormal development generating localized lesions, which are called vascular anomalies. On the basis of clinical and biological criteria, they are divided into vascular tumours and vascular malformations. This classification has been adopted by the International Society for the Study of Vascular Anomalies and used to cover all reported entities. The identification of disease‐causing genes associated with precise clinical delineation of the phenotypes has become the foundation for better management of these diseases. It has been established that the rare familial forms follow a paradominant inheritance with a combination of a germinal mutation and a local somatic second‐hit, whereas somatic/mosaic genetic defects cause the more common sporadic vascular malformations. Links between phenotypes and genotypes have been unravelled for several vascular malformations.

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

Cited by 87 publications

References 28 publications

Ccbe1 expression marks the cardiac and lymphatic progenitor lineages during early stages of mouse development

Ccbe1 expression marks the cardiac and lymphatic progenitor lineages during early stages of mouse development

Getting out and about: the emergence and morphogenesis of the vertebrate lymphatic vasculature

Disorders Affecting Cutaneous Vasculature

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