Literature DB >> 21693513

Neuropilin-2 promotes branching morphogenesis in the mouse mammary gland.

Hira Lal Goel1, Donggoo Bae, Bryan Pursell, Lindsey M Gouvin, Shaolei Lu, Arthur M Mercurio.   

Abstract

Although the neuropilins were characterized as semaphorin receptors that regulate axon guidance, they also function as vascular endothelial growth factor (VEGF) receptors and contribute to the development of other tissues. Here, we assessed the role of NRP2 in mouse mammary gland development based on our observation that NRP2 is expressed preferentially in the terminal end buds of developing glands. A floxed NRP2 mouse was bred with an MMTV-Cre strain to generate a mammary gland-specific knockout of NRP2. MMTV-Cre;NRP2(loxP/loxP) mice exhibited significant defects in branching morphogenesis and ductal outgrowth compared with either littermate MMTV-Cre;NRP2(+/loxP) or MMTV-Cre mice. Mechanistic insight into this morphological defect was obtained from a mouse mammary cell line in which we observed that VEGF(165), an NRP2 ligand, induces branching morphogenesis in 3D cultures and that branching is dependent upon NRP2 as shown using shRNAs and a function-blocking antibody. Epithelial cells in the mouse mammary gland express VEGF, supporting the hypothesis that this NRP2 ligand contributes to mammary gland morphogenesis. Importantly, we demonstrate that VEGF and NRP2 activate focal adhesion kinase (FAK) and promote FAK-dependent branching morphogenesis in vitro. The significance of this mechanism is substantiated by our finding that FAK activation is diminished significantly in developing MMTV-Cre;NRP2(loxP/loxP) mammary glands compared with control glands. Together, our data reveal a VEGF/NRP2/FAK signaling axis that is important for branching morphogenesis and mammary gland development. In a broader context, our data support an emerging hypothesis that directional outgrowth and branching morphogenesis in a variety of tissues are influenced by signals that were identified initially for their role in axon guidance.

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Year:  2011        PMID: 21693513      PMCID: PMC3119306          DOI: 10.1242/dev.051318

Source DB:  PubMed          Journal:  Development        ISSN: 0950-1991            Impact factor:   6.868


  45 in total

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Authors:  Lee Ann Cohen; Jun-Lin Guan
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2.  Neuropilin is a receptor for the axonal chemorepellent Semaphorin III.

Authors:  Z He; M Tessier-Lavigne
Journal:  Cell       Date:  1997-08-22       Impact factor: 41.582

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Authors:  S Soker; S Takashima; H Q Miao; G Neufeld; M Klagsbrun
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7.  Interactions of multiple heparin binding growth factors with neuropilin-1 and potentiation of the activity of fibroblast growth factor-2.

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10.  A peptide corresponding to the neuropilin-1-binding site on VEGF(165) induces apoptosis of neuropilin-1-expressing breast tumour cells.

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  10 in total

1.  Neuropilin-2 regulates α6β1 integrin in the formation of focal adhesions and signaling.

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2.  VEGF/neuropilin-2 regulation of Bmi-1 and consequent repression of IGF-IR define a novel mechanism of aggressive prostate cancer.

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Review 4.  Neuropilins: expression and roles in the epithelium.

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Review 6.  Enhancing integrin function by VEGF/neuropilin signaling: implications for tumor biology.

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Review 7.  Lymphangiogenesis and metastasis--a closer look at the neuropilin/semaphorin3 axis.

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8.  Balance between BDNF and Semaphorins gates the innervation of the mammary gland.

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10.  Neuropilin-1 is upregulated by Wnt/β-catenin signaling and is important for mammary stem cells.

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  10 in total

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