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The loss of RGS protein-G?(i2) interactions results in markedly impaired mouse neutrophil trafficking to inflammatory sites.


ABSTRACT: Neutrophils are first responders rapidly mobilized to inflammatory sites by a tightly regulated, nonredundant hierarchy of chemoattractants. These chemoattractants engage neutrophil cell surface receptors triggering heterotrimeric G-protein G?(i) subunits to exchange GDP for GTP. By limiting the duration that G?(i) subunits remain GTP bound, RGS proteins modulate chemoattractant receptor signaling. Here, we show that neutrophils with a genomic knock in of a mutation that disables regulator of G-protein signaling (RGS)-G?(i2) interactions accumulate in the bone marrow and mobilize poorly to inflammatory sites. These defects are attributable to enhanced sensitivity to background signals, prolonged chemoattractant receptor signaling, and inappropriate CXCR2 downregulation. Intravital imaging revealed a failure of the mutant neutrophils to accumulate at and stabilize sites of sterile inflammation. Furthermore, these mice could not control a nonlethal Staphylococcus aureus infection. Neutrophil RGS proteins establish a threshold for G?(i) activation, helping to coordinate desensitization mechanisms. Their loss renders neutrophils functionally incompetent.

SUBMITTER: Cho H 

PROVIDER: S-EPMC3486189 | biostudies-literature | 2012 Nov

REPOSITORIES: biostudies-literature

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The loss of RGS protein-Gα(i2) interactions results in markedly impaired mouse neutrophil trafficking to inflammatory sites.

Cho Hyeseon H   Kamenyeva Olena O   Yung Sunny S   Gao Ji-Liang JL   Hwang Il-Young IY   Park Chung C   Murphy Philip M PM   Neubig Richard R RR   Kehrl John H JH  

Molecular and cellular biology 20120910 22


Neutrophils are first responders rapidly mobilized to inflammatory sites by a tightly regulated, nonredundant hierarchy of chemoattractants. These chemoattractants engage neutrophil cell surface receptors triggering heterotrimeric G-protein Gα(i) subunits to exchange GDP for GTP. By limiting the duration that Gα(i) subunits remain GTP bound, RGS proteins modulate chemoattractant receptor signaling. Here, we show that neutrophils with a genomic knock in of a mutation that disables regulator of G-  ...[more]

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