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      Mechanisms That Regulate the Function of the Selectins and Their Ligands

      1 , 1
      Physiological Reviews
      American Physiological Society

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          Lymphocyte homing and leukocyte rolling and migration are impaired in L-selectin-deficient mice.

          L-selectin, a cell adhesion molecule expressed by leukocytes, mediates the attachment of lymphocytes to high endothelial venules (HEV) of peripheral lymph nodes and mediates the earliest interactions between leukocytes and activated vascular endothelium. Mice possessing a mutant L-selectin gene that results in the complete loss of cell surface receptor expression were generated by gene targeting. Lymphocytes from these mice did not bind to peripheral lymph node HEV and these mice had a severe reduction in the number of lymphocytes localized to peripheral lymph nodes. Short-term homing experiments demonstrated that L-selectin was also involved in lymphocyte migration to mucosal lymph nodes, Peyer's patches, and spleen. Furthermore, significant defects in leukocyte rolling and neutrophil migration into the peritoneum in response to an inflammatory stimulus were observed. Thus, L-selectin plays an essential role in leukocyte homing to lymphoid tissues and sites of inflammation.
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            α4β7 integrin mediates lymphocyte binding to the mucosal vascular addressin MAdCAM-1

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              Leukocyte rolling and extravasation are severely compromised in P selectin-deficient mice.

              P selectin, expressed on surfaces of activated endothelial cells and platelets, is an adhesion receptor for leukocytes. We report that P selectin-deficient mice, generated by gene targeting in embryonic stem cells, exhibit a number of defects in leukocyte behavior, including elevated numbers of circulating neutrophils, virtually total absence of leukocyte rolling in mesenteric venules, and delayed recruitment of neutrophils to the peritoneal cavity upon experimentally induced inflammation. These results clearly demonstrate a role for P selectin in leukocyte interactions with the vessel wall and in the early steps of leukocyte recruitment at sites of inflammation. These mutant mice should prove useful in deciphering the contributions of P selectin in various inflammatory responses as well as in platelet functions.

                Author and article information

                Journal
                Physiological Reviews
                Physiological Reviews
                American Physiological Society
                0031-9333
                1522-1210
                January 1999
                January 1999
                : 79
                : 1
                : 181-213
                Affiliations
                [1 ]Institute of Cell Biology, Center of Molecular Biology of Inflammation, University of Münster, Münster, Germany
                Article
                10.1152/physrev.1999.79.1.181
                9922371
                28f73b37-a043-411d-97af-cc0c0ae7d943
                © 1999
                History

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