Daiki Kajioka’s research while affiliated with University of Virginia and other places

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Publications (1)


Chimeric efferocytic receptors improve apoptotic cell clearance and alleviate inflammation
  • Article

December 2022

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110 Reads

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33 Citations

Cell

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Daiki Kajioka

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Yusuke Yamaoka

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[...]

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Our bodies turn over billions of cells daily via apoptosis and are in turn cleared by phagocytes via the process of "efferocytosis." Defects in efferocytosis are now linked to various inflammatory diseases. Here, we designed a strategy to boost efferocytosis, denoted "chimeric receptor for efferocytosis" (CHEF). We fused a specific signaling domain within the cytoplasmic adapter protein ELMO1 to the extracellular phosphatidylserine recognition domains of the efferocytic receptors BAI1 or TIM4, generating BELMO and TELMO, respectively. CHEF-expressing phagocytes display a striking increase in efferocytosis. In mouse models of inflammation, BELMO expression attenuates colitis, hepatotoxicity, and nephrotoxicity. In mechanistic studies, BELMO increases ER-resident enzymes and chaperones to overcome protein-folding-associated toxicity, which was further validated in a model of ER-stress-induced renal ischemia-reperfusion injury. Finally, TELMO introduction after onset of kidney injury significantly reduced fibrosis. Collectively, these data advance a concept of chimeric efferocytic receptors to boost efferocytosis and dampen inflammation.

Citations (1)


... A common feature of all forms of cell death is the loss of phospholipid asymmetry in the plasma membrane, leading to the exposure of PS on the cell surface, which facilitates the engulfment of dying cells. During apoptosis, PS, which is normally located on the inner leaflet of the membrane, translocates to the outer surface in the early stages [30]. ...

Reference:

Microglia efferocytosis: an emerging mechanism for the resolution of neuroinflammation in Alzheimer’s disease
Chimeric efferocytic receptors improve apoptotic cell clearance and alleviate inflammation
  • Citing Article
  • December 2022

Cell