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Steven D. Rosen

Researcher at City of Hope National Medical Center

Publications -  156
Citations -  15576

Steven D. Rosen is an academic researcher from City of Hope National Medical Center. The author has contributed to research in topics: L-selectin & High endothelial venules. The author has an hindex of 67, co-authored 156 publications receiving 14957 citations. Previous affiliations of Steven D. Rosen include Beckman Research Institute & University of California, San Francisco.

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A chemokine expressed in lymphoid high endothelial venules promotes the adhesion and chemotaxis of naive T lymphocytes

TL;DR: SLC is the first chemokine demonstrated to have the characteristics required to mediate homing of lymphocytes to secondary lymphoid organs and the expression of SLC in lymphatic endothelium suggests that the migration of lymphocyte from tissues into efferent lymphatics may be an active process mediated by this molecule.
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Ligands for L-selectin: homing, inflammation, and beyond.

TL;DR: This review focuses on the ligands for L-selectin that are found on vascular endothelium, leukocytes, carcinoma cells, and at various extravascular sites.
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Binding of L-selectin to the vascular sialomucin CD34

TL;DR: An HEV glycoform of CD34 can function as a ligand for L-selectin, and a polyclonal antiserum to recombinant murine CD34 stains peripheral lymph node endothelium and recognizes Sgp90 that is functionally bound by L- selectin.
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Cloning of a lymphocyte homing receptor reveals a lectin domain

TL;DR: Cl cloning of a murine cDNA that encodes the antigen recognized by the MEL-14 antibody shows that it contains a lectin domain that appears to be involved in the binding of lymphocytes to peripheral lymph node endothelium, thus defining a new type of cellular adhesion molecule.
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The selectins and their ligands

TL;DR: The selectins are a family of carbohydrate-binding proteins, or lectins, that have stimulated tremendous interest because of their involvement in a wide array of interactions between leukocytes and endothelial cells.