4.4 Article

Nuclear localization of vasoactive intestinal peptide (VIP) receptors in human breast cancer

Journal

PEPTIDES
Volume 31, Issue 11, Pages 2035-2045

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.peptides.2010.07.024

Keywords

VIP receptors; Nuclear VPAC receptors; Human breast cancer; cAMP

Funding

  1. Ministerio de Educacion y Ciencia [SAF2007-63794]
  2. Comunidad de Madrid/Universidad de Alcala [CCG08-UAH/BIO-3782]

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Vasoactive intestinal peptide (VIP) and its receptors (VPACs) are involved in proliferation survival and differentiation in human breast cancer cells Its mechanism of action is traditionally thought to be through specific plasma membrane receptors There is compelling evidence for a novel intracrine mode of genomic regulation by G-protein-coupled receptors (GPCRs) that implies both endocytosis and nuclear translocation of peripheral GPCR and/or the activation of nuclear-located GPCRs by endogenously-produced non-secreted ligands Regarding to VPAC receptors which are GPCRs there is only a report suggesting them as a dynamic system for signaling from plasma membrane and nuclear membrane complex In this study we show that VPAC(1) receptor is localized in cell nuclear fraction whereas VPAC(2) receptor presents an extranuclear localization and its protein expression is lower than that of VPAC(1) receptor in human breast tissue samples Both receptors as well as VIP are overexpressed in breast cancer as compared to non-tumor tissue Moreover we report the markedly nuclear localization of VPAC(1) receptors in estrogen-dependent (T47D) and independent (MDA-MB-468) human breast cancer cell lines VPAC(1) receptors are functional in plasma membrane and nucleus as shown by VIP stimulation of cAMP production in both cell lines In addition VIP increases its own intracellular and extracellular levels and could be involved in the regulation of VPAC(1)-receptor traffic from the plasma membrane to the nucleus These results support new concepts on function and regulation of nuclear GPCRs which could have an impact on development of new therapeutic drugs (C) 2010 Elsevier Inc All rights reserved

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