Frontiers in Immunology (Mar 2018)

Centrosome- and Golgi-Localized Protein Kinase N-Associated Protein Serves As a Docking Platform for Protein Kinase A Signaling and Microtubule Nucleation in Migrating T-Cells

  • Seow Theng Ong,
  • Madhavi Latha Somaraju Chalasani,
  • M. H. U. Turabe Fazil,
  • Praseetha Prasannan,
  • Atish Kizhakeyil,
  • Graham D. Wright,
  • Dermot Kelleher,
  • Dermot Kelleher,
  • Dermot Kelleher,
  • Navin Kumar Verma,
  • Navin Kumar Verma

DOI
https://doi.org/10.3389/fimmu.2018.00397
Journal volume & issue
Vol. 9

Abstract

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Centrosome- and Golgi-localized protein kinase N-associated protein (CG-NAP), also known as AKAP450, is a cytosolic scaffolding protein involved in the targeted positioning of multiple signaling molecules, which are critical for cellular functioning. Here, we show that CG-NAP is predominantly expressed in human primary T-lymphocytes, localizes in close proximity (<0.2 μm) with centrosomal and Golgi structures and serves as a docking platform for Protein Kinase A (PKA). GapmeR-mediated knockdown of CG-NAP inhibits LFA-1-induced T-cell migration and impairs T-cell chemotaxis toward the chemokine SDF-1α. Depletion of CG-NAP dislocates PKARIIα, disrupts centrosomal and non-centrosomal microtubule nucleation, causes Golgi fragmentation, and impedes α-tubulin tyrosination and acetylation, which are important for microtubule dynamics and stability in migrating T-cells. Furthermore, we show that CG-NAP coordinates PKA-mediated phosphorylation of pericentrin and dynein in T-cells. Overall, our findings provide critical insights into the roles of CG-NAP in regulating cytoskeletal architecture and T-cell migration.

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