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Mertk Interacts with Tim-4 to Enhance Tim-4-Mediated Efferocytosis

Byeongjin Moon, Juyeon Lee, Sang-Ah Lee, Chanhyuk Min, Hyunji Moon, Deokhwan Kim, Susumin Yang, Heera Moon, Jaeseon Jeon, Young‐Eun Joo, Daeho Park

2020Cells32 citationsDOIOpen Access PDF

Abstract

Apoptotic cells expressing phosphatidylserine (PS) on their cell surface are directly or indirectly recognized by phagocytes through PS-binding proteins. The PS-binding protein Tim-4 secures apoptotic cells to phagocytes to facilitate the engulfment of apoptotic cells. However, the molecular mechanism by which Tim-4 transduces signals to phagocytes during Tim-4-mediated efferocytosis is incompletely understood. Here, we report that Tim-4 collaborates with Mertk during efferocytosis through a biochemical interaction with Mertk. Proximal localization between the two proteins in phagocytes was observed by immunofluorescence and proximal ligation assays. Physical association between Tim-4 and Mertk, which was mediated by an interaction between the IgV domain of Tim-4 and the fibronectin type-III domain of Mertk, was also detected with immunoprecipitation. Furthermore, the effect of Mertk on Tim-4-mediated efferocytosis was abolished by GST-MertkFnIII, a soluble form of the fibronectin type-III domain of Mertk that disrupts the interaction between Tim-4 and Mertk. Taken together, the results from our study suggest that a physical interaction between Tim-4 and Mertk is necessary for Mertk to enhance efferocytosis mediated by Tim-4.

Topics & Concepts

MERTKEfferocytosisCell biologyPhosphatidylserineImmunoprecipitationApoptosisChemistryPhagocytosisBiologyImmunologyBiochemistrySignal transductionMacrophagePhospholipidAntibodyIn vitroReceptor tyrosine kinaseMembranePhagocytosis and Immune RegulationErythrocyte Function and Pathophysiology