Vascular endothelial growth factor C is required for sprouting of the first lymphatic vessels from embryonic veins

Karkkainen, Marika J.; Haiko, Paula; Sainio, Kirsi; Partanen, Juha; Taipale, Jussi; Petrova, Tatiana V.; Jeltsch, Michael; Jackson, David G.; Talikka, Marja; Rauvala, Heikki; Betsholtz, Christer; Alitalo, Kari

doi:10.1038/ni1013

Cited by 1,224 publications

(1,180 citation statements)

References 41 publications

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“…4 This budding and migration of lymphatic endothelial progenitor cells is mediated by VEGF-C signals and is critically modulated by collagen-and calcium-binding EGF domain 1 protein. 6,7 COUP-TFII and Prox-1 are essential for the maintenance of the identity of the lymphatic endothelial cells following their differentiation. 8 The primary lymphatic networks then enlarge by sprouting lymphangiogenesis induced by the VEGFR-3 ligand VEGF-C. By upregulation of VEGFR-3 expression independently of Prox-1, T-box transcription factor 1 supports the growth and maintenance of the gastrointestinal lymphatic vessel network.…”

Section: Lymphatic Vessel Developmentmentioning

confidence: 99%

Interaction of tumor cells and lymphatic vessels in cancer progression

2011

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Section: Lymphatic Vessel Developmentmentioning

confidence: 99%

Interaction of tumor cells and lymphatic vessels in cancer progression

2011

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“…Recently, regulators were also pipetted directly onto the early chicken CAM at E5 (Melkonian et al, 2002), and CAM assays were reviewed in thorough helpful detail (Richardson and Singh, 2003). In avian and mammalian embryos, it is becoming clear that lymphangiogenesis follows earlier development of the blood vascular system in a complex, rather intertwined fashion (Wigle and Oliver, 1999;Karkkainen et al, 2004;Wilting et al, 2004).…”

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confidence: 99%

Lymphangiogenesis by blind‐ended vessel sprouting is concurrent with hemangiogenesis by vascular splitting

et al. 2006

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Development of effective vascular therapies requires the understanding of all modes of vessel formation involved in angiogenesis (here termed "hemangiogenesis") and lymphangiogenesis. Two major modes of vessel morphogenesis include sprouting of a new vessel from a preexisting vessel and splitting of a preexisting parent vessel into two offspring vessels. In the quail chorioallantoic membrane (CAM) during mid-development (embryonic days E6 -E9), lymphangiogenesis progressed primarily via blind-ended vessel sprouting. Isolated lymphatic endothelial progenitor cells were recruited to the tips of growing vessels. During concurrent hemangiogenesis, parent blood vessels expanded from the capillary network and split into offspring vessels, accompanied by transient capillary expression of alpha smooth muscle actin (␣SMA) and recruitment of polarized mural progenitor cells. Lymphatics and blood vessels were identified by confocal/fluorescence microscopy of vascular endothelial growth factor (VEGF) receptor VEGFR-2, ␣SMA (specific to CAM blood vessels), homeobox transcription factor Prox1 (specific to lymphatics), and the quail hematopoetic marker, QH-1. VEGFR-2 was expressed intensely in isolated cells and lymphatics, and moderately in blood vessels. Prox1 was absent from isolated progenitor cells prior to lymphatic recruitment. Exogenous vascular endothelial growth factor-165 (VEGF 165 ) increased blood vessel density and anastomotic frequency without changing endogenous modes of vascular/lymphatic vessel formation or marker expression. Although VEGF 165 is a key cellular regulator of hemangiogenesis and vasculogenesis, the role of VEGF 165 in lymphangiogenesis is less clear. Interestingly, VEGF 165 increased lymphatic vessel diameter and density as measured by novel Euclidean distance mapping, and the antimaturational dissociation of lymphatics from blood vessels, accompanied by lymphatic reassociation into homogeneous networks. Published 2006 Wiley-Liss, Inc. †

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“…Although the expression of Prox1 in the lymphatically specified venous endothelial cells of the cardinal vein was not inhibited in VEGF-C-deficient mice, Prox1-positive cells were unable to migrate out to form the initial lymph sacs, indicating that lymphatic endothelial cell specification and subsequent cell migration are two separate events, possibly controlled by distinct signaling pathways. Importantly, the sprouting defect of the committed LEC progenitors was rescued by application of VEGF-C or VEGF-D, but not VEGF-A, indicating the necessity of VEGFR-3-mediated signaling for the initial lymphatic vessel formation (Karkkainen et al, 2004). Because VEGFR-3 is expressed by all venous endothelial cells at mouse E8.5, additional autocrine or paracrine signals likely induce lymphatic cell fate among the VEGFR-3-positive cells by activating Prox1 expression.…”

Section: Vegf-c and Vegf-dmentioning

confidence: 97%

“…VEGF-C is expressed by a multitude of cell types, including mesenchymal cells around embryonic veins, activated macrophages, skeletal muscle cells, and smooth muscle cells surrounding large arteries Kukk et al, 1996;Eichmann et al, 1998;Karkkainen et al, 2004). Of interest, blood vascular endothelial cells also express VEGF-C , suggesting possible paracrine mechanisms by which the blood vascular system may control lymphatic vessel growth and/or maintenance.…”

Section: Vegf-c and Vegf-dmentioning

confidence: 99%

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Development of the lymphatic vascular system: A mystery unravels

Hong

Shin

Detmar

2004

Developmental Dynamics

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The blood vascular and the lymphatic system play complementary roles in tissue perfusion and fluid reabsorption. Despite its critical role in mediating tissue fluid homeostasis, intestinal lipid absorption, and the immune response, the lymphatic system has not received as much attention as the blood vascular system, largely due to a lack of lymphatic-specific markers and to the dearth of knowledge about the molecular regulation of lymphatic development and function. A series of recent landmark studies now significantly has advanced our understanding of the lymphatic system. Based upon the discovery and characterization of lymphatic-specific growth factors, receptors, and transcriptional regulators, the mystery of lymphatic vascular system development begins to be unraveled. The successful isolation and cultivation of blood vascular and lymphatic endothelial cells has enabled comparative molecular and cellular analyses of these two genetically and developmentally closely related cell lineages. Moreover, studies of several genetic mouse models have set the framework for a new molecular model of embryonic lymphatic vascular development and have identified molecular pathways whose mutational inactivation leads to human diseases associated with lymphedema. Although these rapid advances already have led to development of the first lymphatic-targeted molecular therapies, there still remain many unanswered questions regarding almost every aspect of lymphatic vascular biology, making the lymphatic system a highly exciting and rewarding field of study.

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Vascular endothelial growth factor C is required for sprouting of the first lymphatic vessels from embryonic veins

Cited by 1,224 publications

References 41 publications

Interaction of tumor cells and lymphatic vessels in cancer progression

Interaction of tumor cells and lymphatic vessels in cancer progression

Lymphangiogenesis by blind‐ended vessel sprouting is concurrent with hemangiogenesis by vascular splitting

Development of the lymphatic vascular system: A mystery unravels

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