Abstract

The complex genetic and biochemical programs that give rise to three- dimensional tree-like branching structures such as the lung, kidney and vascular systems have begun to be elucidated. The most well characterized of these branching systems is the Drosophila tracheal system and the mammalian lung, both of which require intact FGF signaling pathways for normal morphogenesis (1,2). For these branching events, the FGF signaling pathway establishes the initial pattern of branching which is subsequently modified by feedback mechanisms and other signals which result in increasingly more complex branching patterns. The evolutionary conservation of use of the FGF signaling pathway for branching morphogenesis of the fly and mammalian respiratory systems suggests a more general mechanism for branching of other organs such as the vasculature. An FGF antagonist called Sprouty (spr) was identified in a screen for mutations that affect branching of the Drosophila tracheal system (3). In flies that are null for spry, excessive tracheal branching occurs to branching of the Drosophila tracheal system (3). In flies that are null for spry, excessive tracheal branching occurs due to over-activity of the FGF signaling pathway Over-expression of spry results in an inhibition of FGF mediated tracheal branching. Spry expression was shown to be dependent upon FGF signaling, thus FGF induces expression of its own antagonist. Spry has also been shown to antagonize other receptor tyrosine kinase (RTK) pathways in Drosophila including the EGF receptor pathway (1). Three human and four mouse genes have been identified that have sequence similarity to Drosophila Spry (3,4). Recent investigations in the mouse and the chick embryo indicate that EGF regulates the expression of spry genes in a variety of tissues. Over-expression of spry in the chick limb bud results in reduced wing outgrowth which is consistent with a reduction in FGF signaling from the apical ectodermal ridge (4). Data from this laboratory revealed that spry 2 is expressed in endothelial cells and vascular smooth muscle cells in response to FGF or serum. This suggests that spry acts in the mammalian vasculature in a manner similar to the Drosophila tracheal system. We hypothesize that spry may play a role in the branching morphogenesis of the vascular system and that this regulatory pathway may become disrupted during vascular remodeling or angiogenesis. To address this we propose the following specific aims: 1) determine the mechanism by which spry inhibits FGF signaling in the vasculature using a variety of in vitro and in approaches and 2) to determine the phenotypic and molecular consequences of targeted over-expression of spry in the vasculature of transgenic animals. These studies may provide new insights in vascular homeostasis as well as a potential site for therapeutic intervention of vascular disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Center for Research Resources (NCRR)
Type
Exploratory Grants (P20)
Project #
5P20RR015555-02
Application #
6502116
Study Section
Special Emphasis Panel (ZRR1)
Project Start
2001-09-01
Project End
2002-08-31
Budget Start
Budget End
Support Year
2
Fiscal Year
2001
Total Cost
Indirect Cost

  Institution

Name
Maine Medical Center
Department
Type
DUNS #
City
Portland
State
ME
Country
United States
Zip Code
04102

  Publications

Soley, Luna; Falank, Carolyne; Reagan, Michaela R (2017) MicroRNA Transfer Between Bone Marrow Adipose and Multiple Myeloma Cells. Curr Osteoporos Rep 15:162-170
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Ames, Jacquelyn J; Contois, Liangru; Caron, Jennifer M et al. (2016) Identification of an Endogenously Generated Cryptic Collagen Epitope (XL313) That May Selectively Regulate Angiogenesis by an Integrin Yes-associated Protein (YAP) Mechano-transduction Pathway. J Biol Chem 291:2731-50
Contois, Liangru W; Akalu, Abebe; Caron, Jennifer M et al. (2015) Inhibition of tumor-associated ?v?3 integrin regulates the angiogenic switch by enhancing expression of IGFBP-4 leading to reduced melanoma growth and angiogenesis in vivo. Angiogenesis 18:31-46
Motyl, Katherine J; Bishop, Kathleen A; DeMambro, Victoria E et al. (2013) Altered thermogenesis and impaired bone remodeling in Misty mice. J Bone Miner Res 28:1885-97
Apra, Caroline; Richard, Laurence; Coulpier, Fanny et al. (2012) Cthrc1 is a negative regulator of myelination in Schwann cells. Glia 60:393-403
Contois, Liangru W; Nugent, Desiree P; Caron, Jennifer M et al. (2012) Insulin-like growth factor binding protein-4 differentially inhibits growth factor-induced angiogenesis. J Biol Chem 287:1779-89
Urs, Sumithra; Henderson, Terry; Le, Phuong et al. (2012) Tissue-specific expression of Sprouty1 in mice protects against high-fat diet-induced fat accumulation, bone loss and metabolic dysfunction. Br J Nutr 108:1025-33
Sathyanarayana, Pradeep; Dev, Arvind; Pradeep, Anamika et al. (2012) Spry1 as a novel regulator of erythropoiesis, EPO/EPOR target, and suppressor of JAK2. Blood 119:5522-31
Motyl, Katherine J; Dick-de-Paula, Ingrid; Maloney, Ann E et al. (2012) Trabecular bone loss after administration of the second-generation antipsychotic risperidone is independent of weight gain. Bone 50:490-8

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