Activation of the Ancestral Polarity Regulator Protein Kinase Cζ at the Immunological Synapse Drives Polarization of Th Cell Secretory Machinery toward APCs

Bertrand, Florie; Esquerré, Michaël; Petit, Anne-Elisabeth; Rodrigues, Magda; Duchez, Sophie; Delon, Jérôme; Valitutti, Salvatore

doi:10.4049/jimmunol.1000739

Cited by 54 publications

(78 citation statements)

References 37 publications

(50 reference statements)

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“…S2C), p-PKCζ staining was increased at the IS where it paralleled phospho-tyrosine (p-Tyr) staining. These results indicated that in CTLs, similarly to T H cells (14), the PKCζ pathway is active at the IS. We thus treated CTLs with a selective pseudosubstrate inhibitor of PKCζ (PKCζ-PS) (16) to investigate the impact of PKCζ signaling blockade on MTOC polarization.…”

Section: Resultsmentioning

confidence: 53%

“…We also provide further evidence that lytic granule secretion might be, under certain circumstances, uncoupled from MTOC dynamics by blocking MTOC polarization with a selective inhibitor of the ancestral polarity protein PKCζ (14,15). Our results show that in conditions in which MTOC polarization is inhibited, no major effect on cytotoxicity and on the activation of caspase-3 in target cells could be detected.…”

Section: Discussionmentioning

confidence: 59%

“…To do so, we targeted protein kinase Cζ (PKCζ) function in CTLs. Indeed, we and others recently showed that the activation of this ancestral polarizing enzyme at the IS is required for MTOC polarization in CD4 + helper T cells interacting with dendritic cells (14,15). To test whether this pathway is also implicated in MTOC polarization in CTLs, we monitored PKCζ activation at the IS by staining CTL/target cell conjugates with antibodies directed against the phosphorylated form of PKCζ (p-PKCζ) (14).…”

Section: Resultsmentioning

confidence: 99%

“…We therefore asked whether CTLs treated with PKCζ-PS might elicit cytotoxicity. For this analysis, we took advantage of the observation that in helper T-cell/antigen-presenting cell (APC) conjugates, treatment with PKCζ-PS resulted in an inhibition of the secretory machinery toward the APC that lasted at least 6 h, a time longer than a standard cytotoxicity assay (14). In TSST-1-stimulated Vβ2 + CTLs, inhibition of MTOC polarization did not affect cytotoxicity at the different effector:target (E:T) ratios (Fig.…”

Section: Ctls Elicit Cytotoxicity In Conditions In Which Mtoc Polarizmentioning

confidence: 99%

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An initial and rapid step of lytic granule secretion precedes microtubule organizing center polarization at the cytotoxic T lymphocyte/target cell synapse

Bertrand

Müller

Roh

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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105

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It is presently assumed that lethal hit delivery by cytotoxic T lymphocytes (CTLs) is mechanistically linked to centrosome polarization toward target cells, leading to dedicated release of lytic granules within a confined secretory domain. Here we provide three lines of evidence showing that this mechanism might not apply as a general paradigm for lethal hit delivery. First, in CTLs stimulated with immobilized peptide-MHC complexes, lytic granules and microtubule organizing center localization into synaptic areas are spatio-temporally dissociated, as detected by total internal reflection fluorescence microscopy. Second, in many CTL/target cell conjugates, lytic granule secretion precedes microtubule polarization and can be detected during the first minute after cell-cell contact. Third, inhibition of microtubule organizing center and centrosome polarization impairs neither lytic granule release at the CTL synapse nor killing efficiency. Our results broaden current views of CTL biology by revealing an extremely rapid step of lytic granule secretion and by showing that microtubule organizing center polarization is dispensable for efficient lethal hit delivery.immunological synapse | T-cell antigen receptor | protein kinase Cζ | signal transduction

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Section: Resultsmentioning

confidence: 53%

Section: Discussionmentioning

confidence: 59%

Section: Resultsmentioning

confidence: 99%

Section: Ctls Elicit Cytotoxicity In Conditions In Which Mtoc Polarizmentioning

confidence: 99%

See 2 more Smart Citations

An initial and rapid step of lytic granule secretion precedes microtubule organizing center polarization at the cytotoxic T lymphocyte/target cell synapse

Bertrand

Müller

Roh

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

105

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“…Our results strongly suggest that L-plastin regulates lymphocyte polarity and migration by enabling cells to establish an axis of asymmetry in response to chemokine signaling, in particular, the localization of the F-actin cytoskeleton to the leading edge of the cell. We also uncovered a novel mechanistic link between PKC z, an established regulator of lymphocyte polarity (40)(41)(42)(43), and L-plastin in human T lymphocytes, specifically via PKC z-mediated phosphorylation of L-plastin on its Ser 5 residue. L-plastin expression also influenced the Rac1 activation cycle, Akt phosphorylation, and migration on the integrin ligand ICAM-1, but in a manner that was independent of LFA-1 activation or adhesion.…”

Section: Discussionmentioning

confidence: 99%

L-Plastin Regulates Polarization and Migration in Chemokine-Stimulated Human T Lymphocytes

Freeley

O’Dowd

Paul

et al. 2012

The Journal of Immunology

105

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Chemokines such as SDF-1α play a crucial role in orchestrating T lymphocyte polarity and migration via polymerization and reorganization of the F-actin cytoskeleton, but the role of actin-associated proteins in this process is not well characterized. In this study, we have investigated a role for L-plastin, a leukocyte-specific F-actin–bundling protein, in SDF-1α–stimulated human T lymphocyte polarization and migration. We found that L-plastin colocalized with F-actin at the leading edge of SDF-1α–stimulated T lymphocytes and was also phosphorylated at Ser5, a site that when phosphorylated regulates the ability of L-plastin to bundle F-actin. L-plastin phosphorylation was sensitive to pharmacological inhibitors of protein kinase C (PKC), and several PKC isoforms colocalized with L-plastin at the leading edge of SDF-1α–stimulated lymphocytes. However, PKC ζ, an established regulator of cell polarity, was the only isoform that regulated L-plastin phosphorylation. Knockdown of L-plastin expression with small interfering RNAs demonstrated that this protein regulated the localization of F-actin at the leading edge of chemokine-stimulated cells and was also required for polarization, lamellipodia formation, and chemotaxis. Knockdown of L-plastin expression also impaired the Rac1 activation cycle and Akt phosphorylation in response to SDF-1α stimulation. Furthermore, L-plastin also regulated SDF-1α–mediated lymphocyte migration on the integrin ligand ICAM-1 by influencing velocity and persistence, but in a manner that was independent of LFA-1 integrin activation or adhesion. This study, therefore, demonstrates an important role for L-plastin and the signaling pathways that regulate its phosphorylation in response to chemokines and adds L-plastin to a growing list of proteins implicated in T lymphocyte polarity and migration.

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Aurora‐A shines on T cell activation through the regulation of Lck

et al. 2016

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Different protein kinases control signaling emanating from the T cell receptor (TCR) during antigen-specific T cell activation. Mitotic kinases, e.g. Aurora-A, have been widely studied in the context of mitosis due to their role during microtubule (MT) nucleation, becoming critical regulators of cell cycle progression. We have recently described a specific role for Aurora-A kinase in antigenic T cell activation. Blockade of Aurora-A in T cells severely disrupts the dynamics of MTs and CD3z-bearing signaling vesicles during T cell activation. Furthermore, Aurora-A deletion impairs the activation of signaling molecules downstream of the TCR. Targeting Aurora-A disturbs the activation of Lck, which is one of the first signals that drive T cell activation in an antigen-dependent manner. This work describes possible models of regulation of Lck by Aurora-A during T cell activation. We also discuss possible roles for Aurora-A in other systems similar to the IS, and its putative functions in cell polarization.

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Activation of the Ancestral Polarity Regulator Protein Kinase Cζ at the Immunological Synapse Drives Polarization of Th Cell Secretory Machinery toward APCs

Cited by 54 publications

References 37 publications

An initial and rapid step of lytic granule secretion precedes microtubule organizing center polarization at the cytotoxic T lymphocyte/target cell synapse

An initial and rapid step of lytic granule secretion precedes microtubule organizing center polarization at the cytotoxic T lymphocyte/target cell synapse

L-Plastin Regulates Polarization and Migration in Chemokine-Stimulated Human T Lymphocytes

Aurora‐A shines on T cell activation through the regulation of Lck

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