Distinct Mechanisms Regulate Lck Spatial Organization in Activated T Cells

dc.contributor.authorKapoor-Kaushik, Natasha
dc.contributor.authorHinde, Elizabeth
dc.contributor.authorCompeer, Ewoud B.
dc.contributor.authorYamamoto, Yui
dc.contributor.authorKraus, Felix
dc.contributor.authorYang, Zhengmin
dc.contributor.authorLou, Jieqiong
dc.contributor.authorPageon, Sophie V.
dc.contributor.authorGaus, Katharina
dc.contributor.authorRossy, Jérémie
dc.date.accessioned2018-08-07T12:03:08Z
dc.date.available2018-08-07T12:03:08Z
dc.date.issued2016eng
dc.description.abstractPhosphorylation of the T cell receptor (TCR) by the kinase Lck is the first detectable signaling event upon antigen engagement. The distribution of Lck within the plasma membrane, its conformational state, kinase activity, and protein-protein interactions all contribute to determine how efficiently Lck phosphorylates the engaged TCR. Here, we used cross-correlation raster image correlation spectroscopy and photoactivated localization microscopy to identify two mechanisms of Lck clustering: an intrinsic mechanism of Lck clustering induced by locking Lck in its open conformation and an extrinsic mechanism of clustering controlled by the phosphorylation of tyrosine 192, which regulates the affinity of Lck SH2 domain. Both mechanisms of clustering were differently affected by the absence of the kinase Zap70 or the adaptor Lat. We further observed that the adaptor TSAd bound to and promoted the diffusion of Lck when it is phosphorylated on tyrosine 192. Our data suggest that while Lck open conformation drives aggregation and clustering, the spatial organization of Lck is further controlled by signaling events downstream of TCR phosphorylation.eng
dc.description.versionpublishedeng
dc.identifier.doi10.3389/fimmu.2016.00083eng
dc.identifier.pmid27014263eng
dc.identifier.ppn508528569
dc.identifier.urihttps://kops.uni-konstanz.de/handle/123456789/42995
dc.language.isoengeng
dc.rightsAttribution 4.0 International
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/
dc.subjectLck, T cell signaling, assembly of signaling complexes, membrane organization, super-resolution fluorescence microscopy, image correlation spectroscopyeng
dc.subject.ddc570eng
dc.titleDistinct Mechanisms Regulate Lck Spatial Organization in Activated T Cellseng
dc.typeJOURNAL_ARTICLEeng
dspace.entity.typePublication
kops.citation.bibtex
@article{KapoorKaushik2016Disti-42995,
  year={2016},
  doi={10.3389/fimmu.2016.00083},
  title={Distinct Mechanisms Regulate Lck Spatial Organization in Activated T Cells},
  volume={7},
  journal={Frontiers in Immunology},
  author={Kapoor-Kaushik, Natasha and Hinde, Elizabeth and Compeer, Ewoud B. and Yamamoto, Yui and Kraus, Felix and Yang, Zhengmin and Lou, Jieqiong and Pageon, Sophie V. and Gaus, Katharina and Rossy, Jérémie},
  note={Article Number: 83}
}
kops.citation.iso690KAPOOR-KAUSHIK, Natasha, Elizabeth HINDE, Ewoud B. COMPEER, Yui YAMAMOTO, Felix KRAUS, Zhengmin YANG, Jieqiong LOU, Sophie V. PAGEON, Katharina GAUS, Jérémie ROSSY, 2016. Distinct Mechanisms Regulate Lck Spatial Organization in Activated T Cells. In: Frontiers in Immunology. 2016, 7, 83. eISSN 1664-3224. Available under: doi: 10.3389/fimmu.2016.00083deu
kops.citation.iso690KAPOOR-KAUSHIK, Natasha, Elizabeth HINDE, Ewoud B. COMPEER, Yui YAMAMOTO, Felix KRAUS, Zhengmin YANG, Jieqiong LOU, Sophie V. PAGEON, Katharina GAUS, Jérémie ROSSY, 2016. Distinct Mechanisms Regulate Lck Spatial Organization in Activated T Cells. In: Frontiers in Immunology. 2016, 7, 83. eISSN 1664-3224. Available under: doi: 10.3389/fimmu.2016.00083eng
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