BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. Fluoxetine, rs7903146, PDX1, Coagulation, Inflammatory disorder, Lymphocyte)
Bookmark Forward

MERTK tyrosine kinase receptor together with TIM4 phosphatidylserine receptor mediates distinct signal transduction pathways for efferocytosis and cell proliferation.

Chihiro Nishi, Yuichi Yanagihashi, Katsumori Segawa, Shigekazu Nagata

The Journal of biological chemistry 2019 May 03


filter terms:
  • AKT (4)
  • apoptosis (1)
  • AXL (1)
  • cytoplasm (1)
  • IL 3 (1)
  • iκb (1)
  • macrophages (2)
  • MEK (1)
  • MERTK (13)
  • mice (2)
  • mitogen (1)
  • NF κB (1)
  • phagocytosis (1)
  • pro b cell (1)
  • receptor (8)
  • receptor t cell (1)
  • Ser (1)
  • signal (4)
  • STAT5 (2)
  • STAT6 (3)
  • TAM (4)
  • Thr (1)
  • TIM 4 (1)
  • TIM4 (4)
  • TYRO3 (1)
    • Sizes of these terms reflect their relevance to your search.

    Apoptotic cells expose phosphatidylserine (PtdSer) on their surface, leading to efferocytosis, i.e. their engulfment by resident macrophages that express the PtdSer receptor T cell immunoglobulin mucin receptor 4 (TIM4) and TAM family receptor tyrosine kinase receptors (MERTK, AXL, and TYRO3). TAM family receptors stimulate cell proliferation, and the many aspects of the growth signaling pathway downstream of TAM family receptors have been elucidated previously. However, the signaling cascade for TAM receptor-mediated efferocytosis has been elusive. Here we observed that efferocytosis by mouse-resident peritoneal macrophages was blocked by inhibitors against the MERTK, mitogen-activated protein kinase/extracellular signal-regulated kinase kinase (MEK), AKT Ser/Thr kinase (AKT), focal adhesion kinase (FAK), or STAT6 pathway. Accordingly, apoptotic cells stimulated the phosphorylation of MERTK, ERK, AKT, FAK, and STAT6, but not of IκB or STAT5. A reconstituted efferocytosis system using MERTK- and TIM4-expressing NIH3T3-derived cells revealed that the juxtamembrane and C-terminal regions of MERTK have redundant roles in efferocytosis. The transformation of murine IL-3-dependent Ba/F3 cells (a pro-B cell line) with MERTK and TIM4 enabled them to proliferate in response to apoptotic cells in a PtdSer-dependent manner. This apoptotic cell-induced MERTK-mediated proliferation required both MERTK's juxtamembrane and C-terminal regions and was blocked by inhibitors of not only ERK, AKT, FAK, and STAT6 but also of NF-κB and STAT5 signaling. These results suggest that apoptotic cells stimulate distinct sets of signal transduction pathways via MERTK to induce either efferocytosis or proliferation. © 2019 Nishi et al.

    Citation

    Chihiro Nishi, Yuichi Yanagihashi, Katsumori Segawa, Shigekazu Nagata. MERTK tyrosine kinase receptor together with TIM4 phosphatidylserine receptor mediates distinct signal transduction pathways for efferocytosis and cell proliferation. The Journal of biological chemistry. 2019 May 03;294(18):7221-7230

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 30846565

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.