A Dictyostelium Secreted Factor Requires a PTEN-Like Phosphatase to Slow Proliferation and Induce Chemorepulsion

Herlihy, Sarah E.; Tang, Yaxun; Gomer, Richard H.

doi:10.1371/journal.pone.0059365

Cited by 13 publications

(16 citation statements)

References 37 publications

(103 reference statements)

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“…Other studies (Henry et al 1984 ) employed the checkerboard assay described by Zigmond & Hirsch ( 1973 ). The use of the Insall chamber has recently expanded (Phillips & Gomer 2012 , Choi et al 2013 , Herlihy et al 2013a , b , Kaul et al 2013 ) and opened up new research questions, which informed the present study. Here, we report on speed, velocity and chemotactic accuracy.…”

Section: Discussionmentioning

confidence: 99%

Impaired neutrophil directional chemotactic accuracy in chronic periodontitis patients

Roberts

Ling

Insall

et al. 2015

J Clinic Periodontology

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AimTo investigate the chemotactic accuracy of peripheral blood neutrophils from patients with chronic periodontitis compared with matched healthy controls, before and after non-surgical periodontal therapy.Material & MethodsNeutrophils were isolated from patients and controls (n = 18) by density centrifugation. Using the Insall chamber and video microscopy, neutrophils were analysed for directional chemotaxis towards N-formyl-methionyl-leucyl-phenylalanine [fMLP (10 nM), or CXCL8 (200 ng/ml)]. Circular statistics were utilized for the analysis of cell movement.ResultsPrior to treatment, neutrophils from patients with chronic periodontitis had significantly reduced speed, velocity and chemotactic accuracy compared to healthy controls for both chemoattractants. Following periodontal treatment, patient neutrophils continued to display reduced speed in response to both chemoattractants. However, velocity and accuracy were normalized for the weak chemoattractant CXCL8 while they remained significantly reduced for fMLP.ConclusionsChronic periodontitis is associated with reduced neutrophil chemotaxis, and this is only partially restored by successful treatment. Dysfunctional neutrophil chemotaxis may predispose patients with periodontitis to their disease by increasing tissue transit times, thus exacerbating neutrophil-mediated collateral host tissue damage.

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Section: Discussionmentioning

confidence: 99%

Impaired neutrophil directional chemotactic accuracy in chronic periodontitis patients

Roberts

Ling

Insall

et al. 2015

J Clinic Periodontology

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“…Both AprA and CfaD are necessary for proliferation inhibition, as recombinant AprA (rAprA) cannot rescue the cfaD¯ phenotype and recombinant CfaD (rCfaD) cannot rescue the aprA¯ phenotype ( 7 , 8 ). Several components of the AprA-induced and/or CfaD-induced proliferation inhibition signaling pathway have been identified, including the ROCO kinase QkgA, the p21-activated kinase (PAK) family member PakD, the PTEN-like phosphatase CnrN, and the tumor suppressor RblA ( 9 , 10 , 11 , 13 , 18 ). Additionally, AprA functions to chemorepel D. discoideum cells, causing cells to move in a biased direction away from a source of AprA ( 12 ).…”

Section: Introductionmentioning

confidence: 99%

“…Additionally, AprA functions to chemorepel D. discoideum cells, causing cells to move in a biased direction away from a source of AprA ( 12 ). QkgA, PakD, CnrN, and RblA are also involved in the AprA-induced-chemorepulsion signaling pathway ( 9 – 13 , 18 ). Both AprA inhibition of proliferation and AprA induction of chemorepulsion require the G proteins Gβ and Gα subunit Gα8, and the binding of AprA to cell membrane is inhibited by GTPγS, suggesting that AprA functions through binding to a G protein-coupled receptor (GPCR) ( 8 , 12 ).…”

Section: Introductionmentioning

confidence: 99%

An Autocrine Proliferation Repressor Regulates Dictyostelium discoideum Proliferation and Chemorepulsion Using the G Protein-Coupled Receptor GrlH

Tang

Herlihy

et al. 2018

mBio

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In eukaryotic microbes, little is known about signals that inhibit the proliferation of the cells that secrete the signal, and little is known about signals (chemorepellents) that cause cells to move away from the source of the signal. Autocrine proliferation repressor protein A (AprA) is a protein secreted by the eukaryotic microbe Dictyostelium discoideum. AprA is a chemorepellent for and inhibits the proliferation of D. discoideum. We previously found that cells sense AprA using G proteins, suggesting the existence of a G protein-coupled AprA receptor. To identify the AprA receptor, we screened mutants lacking putative G protein-coupled receptors. We found that, compared to the wild-type strain, cells lacking putative receptor GrlH (grlH¯ cells) show rapid proliferation, do not have large numbers of cells moving away from the edges of colonies, are insensitive to AprA-induced proliferation inhibition and chemorepulsion, and have decreased AprA binding. Expression of GrlH in grlH¯ cells (grlH¯/grlHOE) rescues the phenotypes described above. These data indicate that AprA signaling may be mediated by GrlH in D. discoideum.

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“…The chemorepellent AprA increased the directness of Dictyostelium cells, while DPPIV and the PAR2 agonists induced chemorepulsion without increasing directness. This suggests a difference in the chemorepulsion mechanisms used by AprA compared to the DPPIV and PAR2 agonists.…”

Section: Discussionmentioning

confidence: 94%

Protease activated-receptor 2 is necessary for neutrophil chemorepulsion induced by trypsin, tryptase, or dipeptidyl peptidase IV

White

Chinea

Pilling

2017

Journal of Leukocyte Biology

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Compared to neutrophil chemoattractants, relatively little is known about the mechanism neutrophils use to respond to chemorepellents. We previously found that the soluble extracellular protein dipeptidyl peptidase IV (DPPIV) is a neutrophil chemorepellent. In this report, we show that an inhibitor of the protease activated receptor 2 (PAR2) blocks DPPIV-induced human neutrophil chemorepulsion, and that PAR2 agonists such as trypsin, tryptase, 2f-LIGRL, SLIGKV, and AC55541 induce human neutrophil chemorepulsion. Several PAR2 agonists in turn block the ability of the chemoattractant fMLP to attract neutrophils. Compared to neutrophils from male and female C57BL/6 mice, neutrophils from male and female mice lacking PAR2 are insensitive to the chemorepulsive effects of DPPIV or PAR2 agonists. Acute respiratory distress syndrome (ARDS) involves an insult-mediated influx of neutrophils into the lungs. In a mouse model of ARDS, aspiration of PAR2 agonists starting 24 h after an insult reduce neutrophil numbers in the bronchoalveolar lavage (BAL) fluid, as well as the post-BAL lung tissue. Together, these results indicate that the PAR2 receptor mediates DPPIV-induced chemorepulsion, and that PAR2 agonists might be useful to induce neutrophil chemorepulsion.

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A Dictyostelium Secreted Factor Requires a PTEN-Like Phosphatase to Slow Proliferation and Induce Chemorepulsion

Cited by 13 publications

References 37 publications

Impaired neutrophil directional chemotactic accuracy in chronic periodontitis patients

Impaired neutrophil directional chemotactic accuracy in chronic periodontitis patients

An Autocrine Proliferation Repressor Regulates Dictyostelium discoideum Proliferation and Chemorepulsion Using the G Protein-Coupled Receptor GrlH

Protease activated-receptor 2 is necessary for neutrophil chemorepulsion induced by trypsin, tryptase, or dipeptidyl peptidase IV

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