2015
DOI: 10.1111/cmi.12519
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cAMP signalling ofBordetellaadenylate cyclase toxin through the SHP‐1 phosphatase activates the BimEL‐Bax pro‐apoptotic cascade in phagocytes

Abstract: The adenylate cyclase toxin-hemolysin (CyaA, ACT or AC-Hly) plays a key role in virulence of Bordetella pertussis. CyaA penetrates myeloid cells expressing the complement receptor 3 (αM β2 integrin CD11b/CD18) and subverts bactericidal capacities of neutrophils and macrophages by catalysing unregulated conversion of cytosolic ATP to the key signalling molecule adenosine 3',5'-cyclic monophosphate (cAMP). We show that the signalling of CyaA-produced cAMP hijacks, by an as yet unknown mechanism, the activity of … Show more

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Cited by 34 publications
(39 citation statements)
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“…4C) that the contribution of PKA activation to the inhibition of ROS production in response to fMLF could be indirect and might potentially result from inhibition of MAPK (ERK and p38) signaling toward NADPH complex assembly. This would be in line with our previous reports that activation of PKA signaling by CyaA-generated cAMP activates, by an as yet unknown mechanism, the tyrosine phosphatase SHP-1, which is known to deactivate ERK by dephosphorylation of its Thr 202 and Tyr 204 residues (13,39,54). We have measured fMLF-stimulated phosphorylation of ERK on these two sites and found it to be significantly reduced by incubation with active CyaA toxin (Fig.…”
Section: Discussionsupporting
confidence: 92%
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“…4C) that the contribution of PKA activation to the inhibition of ROS production in response to fMLF could be indirect and might potentially result from inhibition of MAPK (ERK and p38) signaling toward NADPH complex assembly. This would be in line with our previous reports that activation of PKA signaling by CyaA-generated cAMP activates, by an as yet unknown mechanism, the tyrosine phosphatase SHP-1, which is known to deactivate ERK by dephosphorylation of its Thr 202 and Tyr 204 residues (13,39,54). We have measured fMLF-stimulated phosphorylation of ERK on these two sites and found it to be significantly reduced by incubation with active CyaA toxin (Fig.…”
Section: Discussionsupporting
confidence: 92%
“…4C, but it remains to be conclusively demonstrated. Intriguingly, we found previously that the CyaA/cAMP-elicited activation of SHP-1 and inhibition of ERK in monocytes was mediated by the cAMP-triggered activity of PKA and not by Epac (13,39,55). The involvement of cAMP-activated PKA signaling in promoting dephosphorylation of ERK and p38 has previously been reported in human neutrophils (56,57 [58] would actually have been Epacspecific if it was modified by a methyl group at the 29 position [63]).…”
Section: Discussionsupporting
confidence: 50%
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“…In macrophages, inactivation of the GTPase RhoA by CyaA toxin leads to actin cytoskeleton rearrangements including membrane ruffling and alterations of phagocytic functions (Kamanova et al., ). In addition, CyaA can induce apoptosis associated with caspase activation and thus promote the activation of cell death cascade in macrophages cells (Gueirard et al., ; Ahmad et al., ). However, CyaA toxin also invades a broad range of cells that do not express CD11b/CD18, although the functional and patho‐physiological consequences of CyaA cytotoxicity are not fully understood.…”
Section: Introductionmentioning
confidence: 99%
“…High levels of cAMP cause a transient inactivation of RhoA inducing massive actin rearrangements that dramatically decrease macropinocytosis, block complement-mediated phagocytosis ( Kamanova et al, 2008 ) and possibly impair the chemotactic properties of primary monocytes. Recently, ACT-induced cAMP synthesis was shown to trigger pro-apoptotic signaling in phagocytes through the activity of tyrosine phosphatase SHP-1, the accumulation of cytosolic BimEL and the consequent activation of Bax, permeabilisation of the outer mitochondrial membrane and activation of programmed cell death ( Ahmad et al, 2015 ; Cerny et al, 2015 ). Besides the immediate action of ACT on the ablation of bactericidal functions of phagocytes, ACT activity was also reported to block the release of TNFα and the production of ROS in human monocytes ( Njamkepo et al, 2000 ), to promote incomplete or aberrant maturation of DCs ( Skinner et al, 2004 ; Boyd et al, 2005 ) and to impair T-cell activation by interfering with immunological synapse signaling ( Paccani et al, 2011 ).…”
Section: Bordetella Pertussis : Two Toxins Are Better Than Omentioning
confidence: 99%