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Research ArticleMinireview—A Latin American Perspective On G Protein-Coupled Receptors

Gβγ Pathways in Cell Polarity and Migration Linked to Oncogenic GPCR Signaling: Potential Relevance in Tumor Microenvironment

José Vázquez-Prado, Ismael Bracho-Valdés, Rodolfo Daniel Cervantes-Villagrana and Guadalupe Reyes-Cruz
Molecular Pharmacology November 2016, 90 (5) 573-586; DOI: https://doi.org/10.1124/mol.116.105338
José Vázquez-Prado
Departments of Pharmacology (J.V.-P., R.D.C.-V.) and Cell Biology (G.R.-C.). CINVESTAV-IPN, Mexico City, and Department of Pharmacology (I.B.-V.), School of Medicine, UABC, Mexicali, B.C., Mexico
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Ismael Bracho-Valdés
Departments of Pharmacology (J.V.-P., R.D.C.-V.) and Cell Biology (G.R.-C.). CINVESTAV-IPN, Mexico City, and Department of Pharmacology (I.B.-V.), School of Medicine, UABC, Mexicali, B.C., Mexico
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Rodolfo Daniel Cervantes-Villagrana
Departments of Pharmacology (J.V.-P., R.D.C.-V.) and Cell Biology (G.R.-C.). CINVESTAV-IPN, Mexico City, and Department of Pharmacology (I.B.-V.), School of Medicine, UABC, Mexicali, B.C., Mexico
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Guadalupe Reyes-Cruz
Departments of Pharmacology (J.V.-P., R.D.C.-V.) and Cell Biology (G.R.-C.). CINVESTAV-IPN, Mexico City, and Department of Pharmacology (I.B.-V.), School of Medicine, UABC, Mexicali, B.C., Mexico
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Abstract

Cancer cells and stroma cells in tumors secrete chemotactic agonists that exacerbate invasive behavior, promote tumor-induced angiogenesis, and recruit protumoral bone marrow–derived cells. In response to shallow gradients of chemotactic stimuli recognized by G protein–coupled receptors (GPCRs), Gβγ-dependent signaling cascades contribute to specifying the spatiotemporal assembly of cytoskeletal structures that can dynamically alter cell morphology. This sophisticated process is intrinsically linked to the activation of Rho GTPases and their cytoskeletal-remodeling effectors. Thus, Rho guanine nucleotide exchange factors, the activators of these molecular switches, and their upstream signaling partners are considered participants of tumor progression. Specifically, phosphoinositide-3 kinases (class I PI3Ks, β and γ) and P-Rex1, a Rac-specific guanine nucleotide exchange factor, are fundamental Gβγ effectors in the pathways controlling directionally persistent motility. In addition, GPCR-dependent chemotactic responses often involve endosomal trafficking of signaling proteins; coincidently, endosomes serve as signaling platforms for Gβγ. In preclinical murine models of cancer, inhibition of Gβγ attenuates tumor growth, whereas in cancer patients, aberrant overexpression of chemotactic Gβγ effectors and recently identified mutations in Gβ correlate with poor clinical outcome. Here we discuss emerging paradigms of Gβγ signaling in cancer, which are essential for chemotactic cell migration and represent novel opportunities to develop pathway-specific pharmacologic treatments.

Footnotes

    • Received May 25, 2016.
    • Accepted September 14, 2016.
  • This work was supported by Consejo Nacional de Ciencia y Tecnología (CONACyT) grants [Grant 152434] and [Grant 24011] to JVP and GRC, respectively.

  • dx.doi.org/10.1124/mol.116.105338.

  • Copyright © 2016 by The American Society for Pharmacology and Experimental Therapeutics
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Molecular Pharmacology: 90 (5)
Molecular Pharmacology
Vol. 90, Issue 5
1 Nov 2016
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Research ArticleMinireview—A Latin American Perspective On G Protein-Coupled Receptors

Gβγ Pathways in Oncogenic GPCR Signaling

José Vázquez-Prado, Ismael Bracho-Valdés, Rodolfo Daniel Cervantes-Villagrana and Guadalupe Reyes-Cruz
Molecular Pharmacology November 1, 2016, 90 (5) 573-586; DOI: https://doi.org/10.1124/mol.116.105338

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Research ArticleMinireview—A Latin American Perspective On G Protein-Coupled Receptors

Gβγ Pathways in Oncogenic GPCR Signaling

José Vázquez-Prado, Ismael Bracho-Valdés, Rodolfo Daniel Cervantes-Villagrana and Guadalupe Reyes-Cruz
Molecular Pharmacology November 1, 2016, 90 (5) 573-586; DOI: https://doi.org/10.1124/mol.116.105338
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  • Article
    • Visual Overview
    • Abstract
    • Introduction
    • Protumoral Chemotactic Agonists
    • Availability of Gβγ for Chemotactic Signaling
    • P-Rex1 as a Potential Chemotactic Scaffold
    • Gβγ/PI3K/mTORC2/P-Rex1 Axis in Oncogenesis
    • Endosomes as Platforms of Gβγ Signaling
    • Gβγ Activates ERK-Signaling Cascades
    • Inhibition of Gβγ Signaling Offers Pharmacologic Potential in Cancer Treatment
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