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CD24 is a marker of exosomes secreted into urine and amniotic fluid
Author(s) -
Sandro Keller,
Christian Rupp,
Alexander Stoeck,
Steffen Runz,
Mina Fogel,
Sebastian Lugert,
H. D. Hager,
Mohamed S. AbdelBakky,
Paul Gutwein,
Peter Altevogt
Publication year - 2007
Publication title -
kidney international
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.499
H-Index - 276
eISSN - 1523-1755
pISSN - 0085-2538
DOI - 10.1038/sj.ki.5002486
Subject(s) - microvesicles , exosome , amniotic fluid , vesicle , secretion , microbiology and biotechnology , transplacental , cd24 , chemistry , biology , fetus , endocrinology , stem cell , biochemistry , placenta , pregnancy , membrane , microrna , genetics , gene , cancer stem cell
Exosomes are small membrane vesicles that are secreted from a variety of cell types into various body fluids including the blood and urine. These vesicles are thought to play a role in cell-cell interactions. CD24 is a small but extensively glycosylated protein linked to the cell surface by means of a glycosyl-phosphatidylinositol anchor. In this study we found that CD24 is present in membrane vesicles characterized as exosomes that were isolated from the urine of normal individuals. CD24 was expressed by both tubule cells and podocytes and treatment of the latter with a cholesterol-extracting agent, but not with a calcium ionophore, caused the release of CD24-containing exosomes. Using CD24 as a marker, we found exosomes in the urine of newborn infants and in the amniotic fluid of pregnant women with similar findings made in mice. Interestingly, studies with CD24 knockout mice showed that the exosomes are released from the fetus but not from the mother; however, exosome release was similar from both the knockout and the wild-type mice. This indicates that CD24 is not essential for exosome formation or release but may be a convenient exosome marker. Our studies suggest that exosomal secretion from the embryonic kidney could play a biological role at the fetal-maternal interphase.

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