G-protein signaling modulator-3, a gene linked to autoimmune diseases, regulates monocyte function and its deficiency protects from inflammatory arthritis

Giguère, Patrick M.; Billard, Matthew J.; Laroche, Geneviève; Buckley, Brian K.; Timoshchenko, Roman G.; McGinnis, Marcus W.; Esserman, Denise; Foreman, Oded; Liu, Peng; Siderovski, David P.; Tarrant, Teresa K.

doi:10.1016/j.molimm.2012.12.001

Cited by 25 publications

(42 citation statements)

References 18 publications

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“…The location of the Gpsm3 gene within the class III major histocompatibility class locus suggested that AGS4/Gpsm3 is expressed primarily in the immune system, and initial observations from us and others indicated this was indeed the case (Cao et al, 2004;Kimple et al, 2004;Zhao et al, 2010;Schmidt et al, 2012;Giguère et al, 2013). We also discovered AGS4 expression in primary bone marrow-derived dendritic cells and splenocytes (Fig.…”

Section: Resultssupporting

confidence: 64%

“…A growing number of cellular and physiologic roles have been ascribed to GPR proteins in systems where signal modulation and adaptation are critical for system responsiveness (Bowers et al, 2004(Bowers et al, , 2008Yao et al, 2005Yao et al, , 2006Blumer et al, 2008;Nadella et al, 2010;Regner et al, 2011;Chauhan et al, 2012;Kwon et al, 2012;Giguère et al, 2013;Kamakura et al, 2013;Branham-O'Connor et al, 2014;Singh et al, 2014). The immune system is certainly an area rich in signaling modulation and adaptation and requires dynamic signal processing and spatially integrated G-protein signaling (Cho and Kehrl, 2009;Kehrl et al, 2009).…”

Section: Discussionmentioning

confidence: 99%

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Regulation of Chemokine Signal Integration by Activator of G-Protein Signaling 4 (AGS4)

Robichaux

Branham‐O'Connor

Hwang

et al. 2017

J Pharmacol Exp Ther

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Activator of G-protein signaling 4 (AGS4)/G-protein signaling modulator 3 (Gpsm3) contains three G-protein regulatory (GPR) motifs, each of which can bind Gai-GDP free of Gbg. We previously demonstrated that the AGS4-Gai interaction is regulated by seven transmembrane-spanning receptors (7-TMR), which may reflect direct coupling of the GPR-Gai module to the receptor analogous to canonical Gabg heterotrimer. We have demonstrated that the AGS4-Gai complex is regulated by chemokine receptors in an agonist-dependent manner that is receptor-proximal. As an initial approach to investigate the functional role(s) of this regulated interaction in vivo, we analyzed leukocytes, in which AGS4/Gpsm3 is predominantly expressed, from AGS4/Gpsm3-null mice. Loss of AGS4/Gpsm3 resulted in mild but significant neutropenia and leukocytosis. Dendritic cells, T lymphocytes, and neutrophils from AGS4/Gpsm3-null mice also exhibited significant defects in chemoattractantdirected chemotaxis and extracellular signal-regulated kinase activation. An in vivo peritonitis model revealed a dramatic reduction in the ability of AGS4/Gpsm3-null neutrophils to migrate to primary sites of inflammation. Taken together, these data suggest that AGS4/Gpsm3 is required for proper chemokine signal processing in leukocytes and provide further evidence for the importance of the GPR-Gai module in the regulation of leukocyte function.

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Section: Resultssupporting

confidence: 64%

Section: Discussionmentioning

confidence: 99%

Regulation of Chemokine Signal Integration by Activator of G-Protein Signaling 4 (AGS4)

Robichaux

Branham‐O'Connor

Hwang

et al. 2017

J Pharmacol Exp Ther

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“…We are currently testing whether reducing the expression of these proteins impacts phagocytosis. Suggesting that they may have functional roles, myeloid cells from Gpsm3 Ϫ/Ϫ mice migrate less efficiently to Ccl2 and Cx3cl1 than do wild-type mouse myeloid cells (45). Importantly, many of these proteins have additional domains that can interact with other relevant proteins.…”

Section: Discussionmentioning

confidence: 99%

Canonical and Noncanonical G-Protein Signaling Helps Coordinate Actin Dynamics To Promote Macrophage Phagocytosis of Zymosan

Huang

Becker

Boularan

et al. 2014

Molecular and Cellular Biology

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Both chemotaxis and phagocytosis depend upon actin-driven cell protrusions and cell membrane remodeling. While chemoattractant receptors rely upon canonical G-protein signaling to activate downstream effectors, whether such signaling pathways affect phagocytosis is contentious. Here, we report that G␣ i nucleotide exchange and signaling helps macrophages coordinate the recognition, capture, and engulfment of zymosan bioparticles. We show that zymosan exposure recruits F-actin, G␣ i proteins, and Elmo1 to phagocytic cups and early phagosomes. Zymosan triggered an increase in intracellular Ca 2؉ that was partially sensitive to G␣ i nucleotide exchange inhibition and expression of GTP-bound G␣ i recruited Elmo1 to the plasma membrane. Reducing GDP-G␣ i nucleotide exchange, decreasing G␣ i expression, pharmacologically interrupting G␤␥ signaling, or reducing Elmo1 expression all impaired phagocytosis, while favoring the duration that G␣ i remained GTP bound promoted it. Our studies demonstrate that targeting heterotrimeric G-protein signaling offers opportunities to enhance or retard macrophage engulfment of phagocytic targets such as zymosan.

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“…Some of us have recently described functional studies of G protein signaling modulator-3 (GPSM3), a newly identified signaling regulator with prominent expression in myeloid lineage cells and lower relative expression levels in other hematopoietic lineages as well as non-hematopoietic tissues (16). GPSM3 (a.k.a.…”

mentioning

confidence: 99%

“…AGS4 or G18; Ref. 17,18) possesses two functional "GoLoco motifs" (18) for binding heterotrimeric G protein G␣ i subunits and additionally binds to G␤ subunits during their synthetic pathway toward forming mature G␤␥ dimers (19); these interactions with heterotrimeric G protein subunits are thought to underlie the effects of GPSM3 on chemokine receptor signaling that is critical to the development of inflammatory arthritis (16). More recently, we have described GPSM3 as also interacting directly with the adaptor protein 14-3-3 (20).…”

mentioning

confidence: 99%

G Protein Signaling Modulator-3 Inhibits the Inflammasome Activity of NLRP3

Giguère¹,

Gall

Ezekwe³

et al. 2014

Journal of Biological Chemistry

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Background: NLRP3 is a key regulator of innate inflammation and is linked to inflammatory diseases. Results: GPSM3 associates with NLRP3 and inhibits its function. Conclusion: GPSM3 specifically inhibits NLRP3-dependent inflammasome activity by interacting with its leucine-rich repeat domain. Significance: This association uncovers a putative new mechanism of NLRP3 control, linking a G protein modulator to NLRP3-dependent inflammatory diseases.

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G-protein signaling modulator-3, a gene linked to autoimmune diseases, regulates monocyte function and its deficiency protects from inflammatory arthritis

Cited by 25 publications

References 18 publications

Regulation of Chemokine Signal Integration by Activator of G-Protein Signaling 4 (AGS4)

Regulation of Chemokine Signal Integration by Activator of G-Protein Signaling 4 (AGS4)

Canonical and Noncanonical G-Protein Signaling Helps Coordinate Actin Dynamics To Promote Macrophage Phagocytosis of Zymosan

G Protein Signaling Modulator-3 Inhibits the Inflammasome Activity of NLRP3

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