Abstract

A 130-kDa receptor for VEGF165, neuropilin-1 (NRP1), has been purified and expression cloned. NRP1 is a cell surface glycoprotein previously shown to be a receptor for the semaphorins/ collapsins, a family of chemorepulsive proteins that mediate neuronal guidance. NRP1 is expressed by endothelial cells (EC) as are other VEGF receptors (e.g. KDR) but also abundantly by tumor cells, such as breast and prostate carcinoma, where it is the only receptor capable of binding VEGF. Co-expression of NRP1 and KDR in EC results in increased chemotaxis towards VEGF165 when compared to EC expressing KDR alone, suggesting that NRP1 may be a co-receptor for KDR in EC and contribute to angiogenesis. Tumor cells bind VEGF165 and respond by increased motility. Thus, VEGF165 may have a dual function in tumor growth as an angiogenesis factor and as a factor acting directly on tumor cells. While VEGF165 interactions with NRP1 enhance EC motility, collapsin/ semaphorin 111, an inhibitor of axon motility, inhibits EC motility via NRP1 suggesting that these two ligands have opposing effects acting on the same receptor. NRP1, a naturally occurring secreted 90 kDa NRP1 ectodomain (sNRP1) has been cloned which contains a unique intron sequence. Thus, the distribution of sNRP1 can determined by in situ hybridization independent of intact NRP1. SNRP1 is an antagonist of VEGF165 activity. A second gene, NRP2, with 47% homology to NRP1 has been cloned and its properties relative to NRP1 are being investigated. How NRP1 gene expression and activity is regulated is virtually unknown. The overall goals of this proposal are to define the structure, function and regulation of NRP1 as a novel receptor for VEGF165.
The aims of this proposal are: 1) to investigate VEGF165 and semaphorin/collapsin interactions with NRP1; 2) to investigate NRP1 expression and function in tumor cells; 3) to characterize the structure, function and distribution of a naturally occurring soluble NRP1 (sNRP1) receptor and 4) to investigate the regulation of NRP1 gene expression and activity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
3R37CA037392-20S1
Application #
6411175
Study Section
Pathology A Study Section (PTHA)
Program Officer
Mohla, Suresh
Project Start
1983-01-01
Project End
2001-12-31
Budget Start
2001-01-01
Budget End
2001-12-31
Support Year
20
Fiscal Year
2001
Total Cost
$45,610
Indirect Cost

  Institution

Name
Children's Hospital Boston
Department
Type
DUNS #
076593722
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Mucka, Patrick; Levonyak, Nicholas; Geretti, Elena et al. (2016) Inflammation and Lymphedema Are Exacerbated and Prolonged by Neuropilin 2 Deficiency. Am J Pathol 186:2803-2812
Panigrahy, Dipak; Adini, Irit; Mamluk, Roni et al. (2014) Regulation of soluble neuropilin 1, an endogenous angiogenesis inhibitor, in liver development and regeneration. Pathology 46:416-23
Akino, Tomoshige; Han, Xuezhe; Nakayama, Hironao et al. (2014) Netrin-1 promotes medulloblastoma cell invasiveness and angiogenesis, and demonstrates elevated expression in tumor tissue and urine of patients with pediatric medulloblastoma. Cancer Res 74:3716-26
Coma, Silvia; Allard-Ratick, Marc; Akino, Tomoshige et al. (2013) GATA2 and Lmo2 control angiogenesis and lymphangiogenesis via direct transcriptional regulation of neuropilin-2. Angiogenesis 16:939-52
Snuderl, Matija; Batista, Ana; Kirkpatrick, Nathaniel D et al. (2013) Targeting placental growth factor/neuropilin 1 pathway inhibits growth and spread of medulloblastoma. Cell 152:1065-76
Buehler, Anima; Sitaras, Nicholas; Favret, Sandra et al. (2013) Semaphorin 3F forms an anti-angiogenic barrier in outer retina. FEBS Lett 587:1650-5
Shimizu, Akio; Nakayama, Hironao; Wang, Priscilla et al. (2013) Netrin-1 promotes glioblastoma cell invasiveness and angiogenesis by multiple pathways including activation of RhoA, cathepsin B, and cAMP-response element-binding protein. J Biol Chem 288:2210-22
Wong, Hon-Kit; Shimizu, Akio; Kirkpatrick, Nathaniel D et al. (2012) Merlin/NF2 regulates angiogenesis in schwannomas through a Rac1/semaphorin 3F-dependent mechanism. Neoplasia 14:84-94
Coma, Silvia; Shimizu, Akio; Klagsbrun, Michael (2011) Hypoxia induces tumor and endothelial cell migration in a semaphorin 3F- and VEGF-dependent manner via transcriptional repression of their common receptor neuropilin 2. Cell Adh Migr 5:266-75
Coma, Silvia; Amin, Dhara N; Shimizu, Akio et al. (2010) Id2 promotes tumor cell migration and invasion through transcriptional repression of semaphorin 3F. Cancer Res 70:3823-32

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