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Macrophages discriminate glycosylation patterns of apoptotic cell-derived microparticles
Authors:Bilyy Rostyslav O  Shkandina Tanya  Tomin Andriy  Muñoz Luis E  Franz Sandra  Antonyuk Volodymyr  Kit Yuriy Ya  Zirngibl Matthias  Fürnrohr Barbara G  Janko Christina  Lauber Kirsten  Schiller Martin  Schett Georg  Stoika Rostyslav S  Herrmann Martin
Institution:Institute of Cell Biology, National Academy of Sciences of Ukraine, 79005-Lviv, Ukraine.
Abstract:Inappropriate clearance of apoptotic remnants is considered to be the primary cause of systemic autoimmune diseases, like systemic lupus erythematosus. Here we demonstrate that apoptotic cells release distinct types of subcellular membranous particles (scMP) derived from the endoplasmic reticulum (ER) or the plasma membrane. Both types of scMP exhibit desialylated glycotopes resulting from surface exposure of immature ER-derived glycoproteins or from surface-borne sialidase activity, respectively. Sialidase activity is activated by caspase-dependent mechanisms during apoptosis. Cleavage of sialidase Neu1 by caspase 3 was shown to be directly involved in apoptosis-related increase of surface sialidase activity. ER-derived blebs possess immature mannosidic glycoepitopes and are prioritized by macrophages during clearance. Plasma membrane-derived blebs contain nuclear chromatin (DNA and histones) but not components of the nuclear envelope. Existence of two immunologically distinct types of apoptotic blebs may provide new insights into clearance-related diseases.
Keywords:Apoptosis  Glycosylation  Macrophages  Phagocytosis  Sialic Acid  Blebs  Clearance  Glycopattern  SLE  Sialidase
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