Literature DB >> 27384937

Imaging Spatiotemporal Activities of ZAP-70 in Live T Cells Using a FRET-Based Biosensor.

Kaitao Li1, Xue Xiang1,2,3, Jie Sun4,5, Hai-Tao He6, Jianhua Wu2,7, Yingxiao Wang4,8, Cheng Zhu9.   

Abstract

The zeta-chain-associated protein kinase 70 kDa (ZAP-70), a member of the spleen tyrosine kinase (Syk) family, plays an essential role in early T cell receptor (TCR) signaling. Defects in ZAP-70 lead to impaired thymocyte development and peripheral T cell activation. To better understand its activation dynamics and regulation, we visualized ZAP-70 activities in single live T cells with a Förster resonance energy transfer (FRET)-based biosensor, which was designed for probing kinase activities of the Syk family. We observed in Jurkat E6.1 T cells rapid and specific FRET changes following anti-CD3 stimulation and subsequent piceatannol inhibition. The initiation of ZAP-70 activation was prompt (within 10 s) and correlates with the accompanied intracellular calcium elevation, as revealed by simultaneous imaging of the biosensor and calcium. Different from the previously reported ZAP-70 activation in the immunological synapse and the opposite pole (anti-synapse), we have observed rapid and sustained ZAP-70 activation only at the synapse with superantigen-pulsed Raji B cells. Furthermore, ZAP-70 signaling was impaired by cholesterol depletion, further supporting the importance of membrane organization in TCR signaling. Together our results provide a direct characterization of the spatiotemporal features of ZAP-70 activity in real time at subcellular levels.

Entities:  

Keywords:  Immunological synapse; Membrane microdomains; Syk family kinase; TCR signaling

Mesh:

Substances:

Year:  2016        PMID: 27384937      PMCID: PMC5114152          DOI: 10.1007/s10439-016-1683-6

Source DB:  PubMed          Journal:  Ann Biomed Eng        ISSN: 0090-6964            Impact factor:   3.934


  41 in total

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2.  Genetically encoded fluorescent reporters of protein tyrosine kinase activities in living cells.

Authors:  A Y Ting; K H Kain; R L Klemke; R Y Tsien
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Review 5.  T-cell antigen receptor triggering and lipid rafts: a matter of space and time scales. Talking Point on the involvement of lipid rafts in T-cell activation.

Authors:  Hai-Tao He; Didier Marguet
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6.  Syk mutation in Jurkat E6-derived clones results in lack of p72syk expression.

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Journal:  J Biol Chem       Date:  1995-11-03       Impact factor: 5.157

Review 7.  The SYK tyrosine kinase: a crucial player in diverse biological functions.

Authors:  Attila Mócsai; Jürgen Ruland; Victor L J Tybulewicz
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Review 8.  The kinetic-segregation model: TCR triggering and beyond.

Authors:  Simon J Davis; P Anton van der Merwe
Journal:  Nat Immunol       Date:  2006-08       Impact factor: 25.606

9.  Recruitment of SLP-76 to the membrane and glycolipid-enriched membrane microdomains replaces the requirement for linker for activation of T cells in T cell receptor signaling.

Authors:  N J Boerth; J J Sadler; D E Bauer; J L Clements; S M Gheith; G A Koretzky
Journal:  J Exp Med       Date:  2000-10-02       Impact factor: 14.307

10.  The spatiotemporal pattern of Src activation at lipid rafts revealed by diffusion-corrected FRET imaging.

Authors:  Shaoying Lu; Mingxing Ouyang; Jihye Seong; Jin Zhang; Shu Chien; Yingxiao Wang
Journal:  PLoS Comput Biol       Date:  2008-07-25       Impact factor: 4.475

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2.  Imaging Membrane Order and Dynamic Interactions in Living Cells with a DNA Zipper Probe.

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4.  Integration of FRET and sequencing to engineer kinase biosensors from mammalian cell libraries.

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5.  Sensitive FRET Biosensor Reveals Fyn Kinase Regulation by Submembrane Localization.

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6.  Biophysical basis underlying dynamic Lck activation visualized by ZapLck FRET biosensor.

Authors:  Rongxue Wan; Jenny Wu; Mingxing Ouyang; Lei Lei; Jiaming Wei; Qin Peng; Reed Harrison; Yiqian Wu; Binbin Cheng; Kaitao Li; Cheng Zhu; Liling Tang; Yingxiao Wang; Shaoying Lu
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7.  Signaling Dynamics of TSHR-Specific CAR-T Cells Revealed by FRET-Based Biosensors.

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Review 9.  Ca2+ Microdomains in T-Lymphocytes.

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