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Merck

TIM-1 and TIM-4 glycoproteins bind phosphatidylserine and mediate uptake of apoptotic cells.

Immunity (2007-12-18)
Norimoto Kobayashi, Piia Karisola, Victor Peña-Cruz, David M Dorfman, Masahisa Jinushi, Sarah E Umetsu, Manish J Butte, Haruo Nagumo, Irene Chernova, Baogong Zhu, Arlene H Sharpe, Susumu Ito, Glenn Dranoff, Gerardo G Kaplan, Jose M Casasnovas, Dale T Umetsu, Rosemarie H Dekruyff, Gordon J Freeman
ABSTRACT

The T cell immunoglobulin mucin (TIM) proteins regulate T cell activation and tolerance. Here we showed that TIM-4 is expressed on human and mouse macrophages and dendritic cells, and both TIM-4 and TIM-1 specifically bound phosphatidylserine (PS) on the surface of apoptotic cells but not any other phospholipid tested. TIM-4(+) peritoneal macrophages, TIM-1(+) kidney cells, and TIM-4- or TIM-1-transfected cells efficiently phagocytosed apoptotic cells, and phagocytosis could be blocked by TIM-4 or TIM-1 monoclonal antibodies. Mutations in the unique cavity of TIM-4 eliminated PS binding and phagocytosis. TIM-4 mAbs that blocked PS binding and phagocytosis mapped to epitopes in this binding cavity. These results show that TIM-4 and TIM-1 are immunologically restricted members of the group of receptors whose recognition of PS is critical for the efficient clearance of apoptotic cells and prevention of autoimmunity.

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Sigma-Aldrich
Anticorpo anti-fosfatidilserina, clone 1H6, clone 1H6, Upstate®, from mouse