Transience in polarization of cytolytic effectors is required for efficient killing and controlled by Cdc42

Sinai, Parisa; Nguyen, Chau; Schatzle, John D.; Wülfing, Christoph

doi:10.1073/pnas.0913422107

Cited by 26 publications

(26 citation statements)

References 35 publications

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“…This is in contrast to the early increase in NK cell adhesion, which was evident already after 90 s cell contact. NK cells may therefore be much faster than T cells in establishing cellular adhesion, which is in line with their quick responses during innate immune reactions and that has been suggested to be essential for their effective cytotoxic activity (27). In T cells maximal adhesion forces of ∼14 nN were measured after 30 min contact time (26).…”

Section: Discussionmentioning

confidence: 86%

2B4 Engagement Mediates Rapid LFA-1 and Actin-Dependent NK Cell Adhesion to Tumor Cells as Measured by Single Cell Force Spectroscopy

Hoffmann

Cohnen

Ludwig

et al. 2011

The Journal of Immunology

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Adhesion to tumor target cells is essential for initiation and execution of cellular cytotoxicity. In this study, we use single cell force spectroscopy to determine the exact biophysical values of the interaction forces between NK cells and tumor cells. We show that engagement of the activating NK cell receptor 2B4 can rapidly mediate an increase in the force necessary to separate NK cells from tumor cells, starting from 1 nN and increasing to 3 nN after only 120 s tumor cell contact. This early adhesion was mediated by the integrin LFA-1 and dependent on the actin cytoskeleton. The ability of NK cells to rapidly adhere to tumor target cells is consistent with their function in innate immune responses. Our data further suggest that a killing decision is already made within 120– 300 s of tumor cell contact, supporting the essential function of cell adhesion during the early phase of cellular cytotoxicity.

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Section: Discussionmentioning

confidence: 86%

2B4 Engagement Mediates Rapid LFA-1 and Actin-Dependent NK Cell Adhesion to Tumor Cells as Measured by Single Cell Force Spectroscopy

Hoffmann

Cohnen

Ludwig

et al. 2011

The Journal of Immunology

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“…This dynamic remodeling of actin in the center of the IS would depend on Cdc42 in CD4 + T cells thus controlling cytokine release. This could be specific to CD4 + T cells or cytokine release, as Wülfing and colleagues (36) have shown that a dominant negative mutant of Cdc42 does not inhibit granule secretion by CD8 + cytotoxic T cells. What are the downstream regulators of Cdc42-dependent actin remodeling at the IS?…”

Section: Discussionmentioning

confidence: 99%

Cytokine Secretion by CD4+ T Cells at the Immunological Synapse Requires Cdc42-Dependent Local Actin Remodeling but Not Microtubule Organizing Center Polarity

Chemin

Bohineust²,

Dogniaux³

et al. 2012

The Journal of Immunology

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Cytokine secretion by T lymphocytes plays a central role in mounting adaptive immune responses. However, little is known about how newly synthesized cytokines, once produced, are routed within T cells and about the mechanisms involved in regulating their secretions. In this study, we investigated the role of cytoskeleton remodeling at the immunological synapse (IS) in cytokine secretion. We show that a key regulator of cytoskeleton remodeling, the Rho GTPase Cdc42, controls IFN-γ secretion by primary human CD4+ T lymphocytes. Surprisingly, microtubule organizing center polarity at the IS, which does not depend on Cdc42, is not required for cytokine secretion by T lymphocytes, whereas microtubule polymerization is required. In contrast, actin remodeling at the IS, which depends on Cdc42, controls the formation of the polymerized actin ring at the IS, the dynamic concentration of IFN-γ–containing vesicles inside this ring, and the secretion of these vesicles. These results reveal a previously unidentified role of Cdc42-dependent actin remodeling in cytokine exocytosis at the IS.

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“…While active Cdc42 is enriched selectively at the center of the CTL/target cell interface, it is spread out over the NK cell/target cell interface. 5 This becomes obvious when the amount of interface accumulation of active Cdc42 is normalized to its area. With such relation to accumulation area, CTLs are much more effective in generating a small area of intense Cdc42 accumulation than NK cells (Fig.…”

mentioning

confidence: 99%

“…Rapid execution of the killing interaction allows a cytolytic effector to kill several target cells sequentially, promoting effective population-wide killing. To maximize cytolytic efficacy, CTLs are fully polarized within seconds of target cell contact with accumulation of signaling intermediates, actin and the MTOC at the CTL/target cell interface, indicative of strong activating signaling 5,14 ( Fig. 1).…”

mentioning

confidence: 99%

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Tentative and transient natural killer cell polarization balances the requirements for discriminatory recognition and cytolytic efficacy

Sinai

Roybal

Wülfing

2010

Communicative & Integrative Biology

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Transience in polarization of cytolytic effectors is required for efficient killing and controlled by Cdc42

Cited by 26 publications

References 35 publications

2B4 Engagement Mediates Rapid LFA-1 and Actin-Dependent NK Cell Adhesion to Tumor Cells as Measured by Single Cell Force Spectroscopy

2B4 Engagement Mediates Rapid LFA-1 and Actin-Dependent NK Cell Adhesion to Tumor Cells as Measured by Single Cell Force Spectroscopy

Cytokine Secretion by CD4+ T Cells at the Immunological Synapse Requires Cdc42-Dependent Local Actin Remodeling but Not Microtubule Organizing Center Polarity

Tentative and transient natural killer cell polarization balances the requirements for discriminatory recognition and cytolytic efficacy

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