G Protein-Coupled Receptors at the Crossroad between Physiologic and Pathologic Angiogenesis: Old Paradigms and Emerging Concepts
G protein-coupled receptors (GPCRs) have been implicated in transmitting signals across the extra- and intra-cellular compartments, thus allowing environmental stimuli to elicit critical biological responses. As GPCRs can be activated by an extensive range of factors including hormones, neurotransmi...
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doaj-58f5227a58044ce1b2eb791b7c82608b2020-11-24T22:14:26ZengMDPI AGInternational Journal of Molecular Sciences1422-00672017-12-011812271310.3390/ijms18122713ijms18122713G Protein-Coupled Receptors at the Crossroad between Physiologic and Pathologic Angiogenesis: Old Paradigms and Emerging ConceptsErnestina M. De Francesco0Federica Sotgia1Robert B. Clarke2Michael P. Lisanti3Marcello Maggiolini4Department of Pharmacy, Health and Nutrition Sciences, University of Calabria via Savinio, 87036 Rende, ItalyTranslational Medicine, School of Environment and Life Sciences, Biomedical Research Centre, University of Salford, Greater Manchester M5 4WT, UKBreast Cancer Now Research Unit, Division of Cancer Sciences, Manchester Cancer Research Centre, University of Manchester, Wilmslow Road, Manchester M20 4GJ, UKTranslational Medicine, School of Environment and Life Sciences, Biomedical Research Centre, University of Salford, Greater Manchester M5 4WT, UKDepartment of Pharmacy, Health and Nutrition Sciences, University of Calabria via Savinio, 87036 Rende, ItalyG protein-coupled receptors (GPCRs) have been implicated in transmitting signals across the extra- and intra-cellular compartments, thus allowing environmental stimuli to elicit critical biological responses. As GPCRs can be activated by an extensive range of factors including hormones, neurotransmitters, phospholipids and other stimuli, their involvement in a plethora of physiological functions is not surprising. Aberrant GPCR signaling has been regarded as a major contributor to diverse pathologic conditions, such as inflammatory, cardiovascular and neoplastic diseases. In this regard, solid tumors have been demonstrated to activate an angiogenic program that relies on GPCR action to support cancer growth and metastatic dissemination. Therefore, the manipulation of aberrant GPCR signaling could represent a promising target in anticancer therapy. Here, we highlight the GPCR-mediated angiogenic function focusing on the molecular mechanisms and transduction effectors driving the patho-physiological vasculogenesis. Specifically, we describe evidence for the role of heptahelic receptors and associated G proteins in promoting angiogenic responses in pathologic conditions, especially tumor angiogenesis and progression. Likewise, we discuss opportunities to manipulate aberrant GPCR-mediated angiogenic signaling for therapeutic benefit using innovative GPCR-targeted and patient-tailored pharmacological strategies.https://www.mdpi.com/1422-0067/18/12/2713GPCRtumor angiogenesistumor microenvironmentVEGFHIF-1GPERSDF-1sphingosine-1P |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Ernestina M. De Francesco Federica Sotgia Robert B. Clarke Michael P. Lisanti Marcello Maggiolini |
spellingShingle |
Ernestina M. De Francesco Federica Sotgia Robert B. Clarke Michael P. Lisanti Marcello Maggiolini G Protein-Coupled Receptors at the Crossroad between Physiologic and Pathologic Angiogenesis: Old Paradigms and Emerging Concepts International Journal of Molecular Sciences GPCR tumor angiogenesis tumor microenvironment VEGF HIF-1 GPER SDF-1 sphingosine-1P |
author_facet |
Ernestina M. De Francesco Federica Sotgia Robert B. Clarke Michael P. Lisanti Marcello Maggiolini |
author_sort |
Ernestina M. De Francesco |
title |
G Protein-Coupled Receptors at the Crossroad between Physiologic and Pathologic Angiogenesis: Old Paradigms and Emerging Concepts |
title_short |
G Protein-Coupled Receptors at the Crossroad between Physiologic and Pathologic Angiogenesis: Old Paradigms and Emerging Concepts |
title_full |
G Protein-Coupled Receptors at the Crossroad between Physiologic and Pathologic Angiogenesis: Old Paradigms and Emerging Concepts |
title_fullStr |
G Protein-Coupled Receptors at the Crossroad between Physiologic and Pathologic Angiogenesis: Old Paradigms and Emerging Concepts |
title_full_unstemmed |
G Protein-Coupled Receptors at the Crossroad between Physiologic and Pathologic Angiogenesis: Old Paradigms and Emerging Concepts |
title_sort |
g protein-coupled receptors at the crossroad between physiologic and pathologic angiogenesis: old paradigms and emerging concepts |
publisher |
MDPI AG |
series |
International Journal of Molecular Sciences |
issn |
1422-0067 |
publishDate |
2017-12-01 |
description |
G protein-coupled receptors (GPCRs) have been implicated in transmitting signals across the extra- and intra-cellular compartments, thus allowing environmental stimuli to elicit critical biological responses. As GPCRs can be activated by an extensive range of factors including hormones, neurotransmitters, phospholipids and other stimuli, their involvement in a plethora of physiological functions is not surprising. Aberrant GPCR signaling has been regarded as a major contributor to diverse pathologic conditions, such as inflammatory, cardiovascular and neoplastic diseases. In this regard, solid tumors have been demonstrated to activate an angiogenic program that relies on GPCR action to support cancer growth and metastatic dissemination. Therefore, the manipulation of aberrant GPCR signaling could represent a promising target in anticancer therapy. Here, we highlight the GPCR-mediated angiogenic function focusing on the molecular mechanisms and transduction effectors driving the patho-physiological vasculogenesis. Specifically, we describe evidence for the role of heptahelic receptors and associated G proteins in promoting angiogenic responses in pathologic conditions, especially tumor angiogenesis and progression. Likewise, we discuss opportunities to manipulate aberrant GPCR-mediated angiogenic signaling for therapeutic benefit using innovative GPCR-targeted and patient-tailored pharmacological strategies. |
topic |
GPCR tumor angiogenesis tumor microenvironment VEGF HIF-1 GPER SDF-1 sphingosine-1P |
url |
https://www.mdpi.com/1422-0067/18/12/2713 |
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