324 research outputs found
Mini Review: Specificity in cytokine signal transduction: lessons learned from the IL-3:IL-5:GM-CSF receptor family
Cytokines mediate the transduction of proliferative, differentiation and survival signals in the hematopoietic system. Although
the cytokine family is large and diverse, many different cytokines display broadly overlapping functions. This can be explained by the fact that cytokine receptors often share multiple subunits. Specificity in signal transduction can however be achieved through several mechanisms. This review focuses on how signal specificity can be achieved within the IL-3, IL-5 and GM-CSF receptor family. This is discussed in terms of receptor expression, recent advances in our understanding of intracellular signalling components, and analysis of null mutant knock-out mice
Activation of RhoA and ROCK Are Essential for Detachment of Migrating Leukocytesh
Detachment of the rear of the cell from its substratum is an important aspect of locomotion. The
signaling routes involved in this adhesive release are largely unknown. One of the few candidate
proteins to play a role is RhoA, because activation of RhoA in many cell types leads to contraction,
a mechanism probably involved in detachment. To study the role of RhoA in detachment
regulation, we analyzed several subsets of expert migratory leukocytes by video microscopy. In
contrast to fast-migrating neutrophils, eosinophils do not detach the rear of the cell unless
stimulated with serum. When measuring the amount of active RhoA, with the use of a GSTRhotekin
pulldown assay, we found that serum is an excellent activator of RhoA in granulocytes.
Inhibition of RhoA or one of Rhos target proteins, the kinase ROCK, in neutrophils leads to the
phenotype seen in eosinophils: the rear of the cell is firmly attached to the substratum, whereas
the cell body is highly motile. ROCK-inhibition leads to impaired migration of granulocytes in
filters, on glass, and through endothelial monolayers. Also, the ROCK signaling pathway is
involved in changes of integrin-mediated adhesion. Eosinophil transduction by a tat-fusion
construct containing active RhoA resulted in detachment stimulation in the presence of chemoattractant.
From these results we conclude that activation of the RhoA-ROCK pathway is essential
for detachment of migratory leukocytes
Regulation of Proliferation, Differentiation and Survival by the IL-3/IL-5/GM-CSF Receptor Family
The receptors for the Il-3/IL-5/GM-CSF cytokine family are composed of a heterodimeric com-plex
of a cytokine-specific a chain and a common ß chain (ßc). Binding of IL-3/IL-5/GM-CSF to their respective
receptors rapidly induces activation of multiple intracellular signalling pathways, including the Ras-Raf-ERK, the
JAK/STAT, the phosphatidylinositol 3-kinase PKB, and the JNK/SAPK and p38 signalling pathways. This re-view
focuses on recent advancements in understanding how these different signalling pathways are activated by
IL-3/IL-5/GM-CSF receptors, and how the individual pathways contribute to the pleiotropic effects of IL-3/IL-5/
GM-CSF on their target cells, including proliferation, differentiation, survival, and effector functions
Analysis of Signal Transduction Pathways Regulating Cytokine-Mediated Fc Receptor Activation on Human Eosinophils
Igs can be potent stimulants of eosinophil activation since interaction with IgA or IgG-coated particles can lead to eosinophil
degranulation. We have investigated the comparative roles of mitogen-activated protein (MAP) kinases (MAPKs; ERK1/2 and
p38) and phosphatidylinositol-3 kinase (PI3K) in the priming and regulation of Fc receptor functioning on human eosinophils
utilizing a MAPK kinase (MEK) inhibitor (PD98059), a p38 inhibitor SB203580, and the widely used PI3K inhibitors wortmannin
and LY294002. We demonstrate that priming of human eosinophils with Th2-derived cytokines, IL-4 and IL-5, differentially
activate phosphotyrosine-associated PI3K and ERK and p38 MAP kinases. This activation can be inhibited by pre-incubation with
wortmannin or LY294002, PD98059, and SB203580, respectively. Analysis of the effects of the inhibitors on rosette formation
between human eosinophils and IgA- or IgG-coated beads revealed that activation of MEK was not required for IgA binding after
priming with IL-4 or IL-5. However, inhibition of MEK did inhibit IL-5-primed binding of IgG-beads. The rosette formation of
primed eosinophils with IgA-beads could be completely inhibited by wortmannin and LY294002 treatment, demonstrating a
critical role for PI3K. Interestingly, inhibition of the p38 pathway also resulted in a complete blockade of IgA rosette formation.
This work demonstrates regulatory control by inside-out signaling of Fc receptors by various cytokines on human eosinophils.
Thus in vivo the local production of Th2-derived cytokines will regulate the effector functions of Fc receptors
Cytokine-induced inside-out activation of FcaR (CD89) is mediated by a single serine residue (S263) in the intracellular domain of the receptor
Fc receptors play an important role in
leukocyte activation and the modulation
of ligand binding ("activation") is a criti-cal
point of regulation. Previous studies
demonstrated that the Fc receptor for IgA
(FcaRI/CD89) is regulated by cytokine
stimulation, switching it to a high-binding
state. To investigate the mechanism by
which cytokine-induced signal transduc-tion
pathways result in FcaRI activation,
cell lines expressing various receptor mu-tants
were generated. Binding studies
indicated that truncation of the C-termi-
nus of the FcaRI resulted in constitutive
IgA binding, removing the need for cyto-kine
stimulation. Furthermore, mutagen-esis
of a single C-terminal serine residue
(S263) to alanine (S>A) (single-letter
amino acid codes) also resulted in consti-tutive
IgA binding, whereas a serine to
aspartate (S>D) mutation was no longer
functional. The role of S263 might be in
regulating the interaction with the cy-toskeleton,
because disruption of the cy-toskeleton
results in reduced IgA binding
to both FcaRwt and FcaR_S>A. In addi-
tion, overexpression of a membrane-targeted
intracellular domain of FcaR,
and the introduction of cell-permeable
CD89 fusion proteins blocked IgA bind-ing,
implying a competition for endoge-nous
proteins. The proposal is made that
Fc receptors are activated by cytokines
via an inside-out mechanism converging
at the cytoplasmic tail of these receptors
Cytokine-mediated cPLA2 phosphorylation is regulated by multiple MAPK family members
Cytosolic phospholipase A2 (cPLA2) plays a critical
role in various neutrophil functions including the generation of
leukotrienes and platelet-activating factor release. Enzyme
activity is regulated both by translocation to the membrane in
a Ca^(2+) -dependent manner and serine phosphorylation by
members of the mitogen-activated protein kinase (MAPK)
family. In this report, we have investigated the role of
granulocyte/macrophage colony-stimulating factor (GM-CSF)-
mediated signalling pathways in the regulation of cPLA2. GM-
CSF-induced cPLA2 phosphorylation was not affected by
pharmacological inhibition of p38 MAPK, phosphatidylinositol
3-kinase or Src. However, inhibition of extracellular signal-
regulated kinase (ERK) MAPK activation resulted in a partial
inhibition of cPLA2 phosphorylation, revealed in a slower onset
of phosphorylation. A cell line stably transfected with the GM-
CSF receptor was used to further analyze GM-CSF-mediated
cPLA2 phosphorylation. Mutation of tyrosine residues 577 and
612 resulted in a delayed cPLA2 phosphorylation similar to the
pharmacological ERK inhibition. Furthermore, inhibition of p38
MAPK in cells bearing the double mutant ßc577/612 completely
abrogated GM-CSF-induced cPLA2 phosphorylation. We con-
clude that GM-CSF can mediate cPLA2 phosphorylation
through the redundant activation of both p38 and ERK MAP
kinases
Differential fMet-Leu-Phe- and Platelet-activating Factor-induced Signaling Toward Ral Activation in Primary Human Neutrophils
We have measured the activation of the small GTPase
Ral in human neutrophils after stimulation with fMet-
Leu-Phe (fMLP), platelet activating factor (PAF), and
granulocyte macrophage-colony stimulating factor and
compared it with the activation of two other small
GTPases, Ras and Rap1. We found that fMLP and PAF,
but not granulocyte macrophage-colony stimulating factor,
induce Ral activation. All three stimuli induce the
activation of both Ras and Rap1. Utilizing specific inhibitors
we demonstrate that fMLP-induced Ral activation
is mediated by pertussis toxin-sensitive G-proteins and
partially by Src-like kinases, whereas fMLP-induced
Ras activation is independent of Src-like kinases. PAFinduced
Ral activation is mediated by pertussis toxininsensitive
proteins, Src-like kinases and phosphatidylinositol
3-kinase. Phosphatidylinositol 3-kinase is not
involved in PAF-induced Ras activation. The calcium
ionophore ionomycin activates Ral, but calcium depletion
partially inhibits fMLP- and PAF-induced Ral activation,
whereas Ras activation was not affected. In addition,
12-O-tetradecanoylphorbol-13-acetate-induced
activation of Ral is completely abolished by inhibitors of
protein kinase C, whereas 12-O-tetradecanoylphorbol-
13-acetate-induced Ras activation is largely insensitive.
We conclude that in neutrophils Ral activation is mediated
by multiple pathways, and that fMLP and PAF induce
Ral activation differently
The personality characteristics of emergency nurses
Background: There are ever increasing demands on the emergency nursing workforce so it is necessary to consider how to enhance the recruitment and retention of emergency nurses. Personality is known to influence occupational choice, yet there is a lack of research exploring how personality may influence the workforce decisions of emergency nurses. Aims: To establish the personality profile of a sample of emergency nurses, and to explore whether any relationship exists between their personality characteristics and time spent working within emergency nursing. Methods: A standardised personality assessment instrument, the NEOâ„¢-PI-3, was used along with a demographic survey. Data were collected from 72 emergency nurses in an Australian Emergency Department between July and October 2012. Descriptive statistics were used to report demographics and the personality assessment results were compared against general population norms in each of the five personality domains and their 30 associated facets using a one-sample t-test. A two-sided alpha level of .01 was determined to indicate statistical significance. Results: Emergency nurse participants scored higher than the population norms in the domains of extraversion, openness to experience and agreeableness, and in twelve facets, including excitement seeking, vulnerability and competence. Conclusion: The personality profile of this sample of emergency nurses is different from the established population norms. Further research is required to establish whether these study results are applicable to the wider emergency nurse workforce and to establish any link with personality and other nursing specialty choice, which may assist in improving nursing workforce retention and recruitment
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