The Journal of Experimental Medicine
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© The Rockefeller University Press, 0022-1007/1998/10/1385/ $5.00
The Journal of Experimental Medicine, Volume 188, Number 7, October 5, 1998 1385-1390

Brief Definitive Reports

Regulation of L-Selectin–mediated Rolling through Receptor Dimerization

Xuan Li*, Douglas A. Steeber*, Mimi L.K. Tang*, Michael A. Farrar{ddagger}, Roger M. Perlmutter{ddagger}, and Thomas F. Tedder*

From the * Department of Immunology, Duke University Medical Center, Durham, North Carolina 27710; and {ddagger} Merck Co., Inc., Rahway, New Jersey 07065

L-selectin binding activity for its ligand expressed by vascular endothelium is rapidly and transiently increased after leukocyte activation. To identify mechanisms for upregulation and assess how this influences leukocyte/endothelial cell interactions, cell-surface dimers of L-selectin were induced using the coumermycin–GyrB dimerization strategy for cross-linking L-selectin cytoplasmic domains in L-selectin cDNA-transfected lymphoblastoid cells. Coumermycin- induced L-selectin dimerization resulted in an approximately fourfold increase in binding of phosphomanan monoester core complex (PPME), a natural mimic of an L-selectin ligand, comparable to that observed after leukocyte activation. Moreover, L-selectin dimerization significantly increased (by ~700%) the number of lymphocytes rolling on vascular endothelium under a broad range of physiological shear stresses, and significantly slowed their rolling velocities. Therefore, L-selectin dimerization may explain the rapid increase in ligand binding activity that occurs after leukocyte activation and may directly influence leukocyte migration to peripheral lymphoid tissues or to sites of inflammation. Inducible oligomerization may also be a common mechanism for rapidly upregulating the adhesive or ligand-binding function of other cell-surface receptors.

Key Words: L-selectin • dimerization • leukocyte/endothelial interaction • rolling • regulation

Address correspondence to Thomas Tedder, Box 3010, Department of Immunology, Rm. 353 Jones Bldg., Research Dr., Duke University Medical Center, Durham, NC 27710. Phone: 919-684-3578; Fax: 919-684-8982; E-mail: tedde003{at}mc.duke.edu


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