Literature DB >> 18673379

Human fetal placental endothelial cells have a mature arterial and a juvenile venous phenotype with adipogenic and osteogenic differentiation potential.

Ingrid Lang1, Angela Schweizer, Ursula Hiden, Nassim Ghaffari-Tabrizi, Gabriele Hagendorfer, Martin Bilban, Maria A Pabst, Emin T Korgun, Gottfried Dohr, Gernot Desoye.   

Abstract

Growing interest in the sources of origin of blood vessel related diseases has led to an increasing knowledge about the heterogeneity and plasticity of endothelial cells lining arteries and veins. So far, most of these studies were performed on animal models. Here, we hypothesized that the plasticity of human fetal endothelial cells depends on their vascular bed of origin i.e. vein or artery and further that the differences between arterial and venous endothelial cells would extend to phenotype and genotype. We established a method for the isolation of fetal arterial and venous endothelial cells from the human placenta and studied the characteristics of both cell types. Human placental arterial endothelial cells (HPAEC) and human placental venous endothelial cells (HPVEC) express classical endothelial markers and differ in their phenotypic, genotypic, and functional characteristics: HPAEC are polygonal cells with a smooth surface growing in loose arrangements and forming monolayers with classical endothelial cobblestone morphology. They express artery-related genes (hey-2, connexin 40, depp) and more endothelial-associated genes than HPVEC. Functional testing demonstrated that vascular endothelial growth factors (VEGFs) induce a higher proliferative response on HPAEC, whereas placental growth factors (PlGFs) are only effective on HPVEC. HPVEC are spindle-shaped cells with numerous microvilli at their surface. They grow closely apposed to each other, form fibroblastoid swirling patterns at confluence and have shorter generation and population doubling times than HPAEC. HPVEC overexpress development-associated genes (gremlin, mesenchyme homeobox 2, stem cell protein DSC54) and show an enhanced differentiation potential into adipocytes and osteoblasts in contrast to HPAEC. These data provide collective evidence for a juvenile venous and a more mature arterial phenotype of human fetal endothelial cells. The high plasticity of the fetal venous endothelial cells may reflect their role as tissue-resident endothelial progenitors during embryonic development with a possible benefit for regenerative cell therapy.

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Year:  2008        PMID: 18673379     DOI: 10.1111/j.1432-0436.2008.00302.x

Source DB:  PubMed          Journal:  Differentiation        ISSN: 0301-4681            Impact factor:   3.880


  40 in total

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2.  Post-transcriptional down regulation of ICAM-1 in feto-placental endothelium in GDM.

Authors:  Francisca Isidora Díaz-Pérez; Ursula Hiden; Martin Gauster; Ingrid Lang; Viktoria Konya; Akos Heinemann; Jelena Lögl; Richard Saffery; Gernot Desoye; Silvija Cvitic
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Review 3.  Cord blood--an alternative source for bone regeneration.

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4.  GDM alters paracrine regulation of feto-placental angiogenesis via the trophoblast.

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6.  Placental mesenchymal stromal cells derived from blood vessels or avascular tissues: what is the better choice to support endothelial cell function?

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7.  The role of endothelial cells in myofiber differentiation and the vascularization and innervation of bioengineered muscle tissue in vivo.

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9.  Differential response of arterial and venous endothelial cells to extracellular matrix is modulated by oxygen.

Authors:  Luciana Lassance; Heidi Miedl; Viktoria Konya; Akos Heinemann; Birgit Ebner; Hubert Hackl; Gernot Desoye; Ursula Hiden
Journal:  Histochem Cell Biol       Date:  2012-02-01       Impact factor: 4.304

Review 10.  Role of the fetoplacental endothelium in fetal growth restriction with abnormal umbilical artery Doppler velocimetry.

Authors:  Emily J Su
Journal:  Am J Obstet Gynecol       Date:  2015-10       Impact factor: 8.661

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