Mechanisms That Regulate the Function of the Selectins and Their Ligands

Overview

Journal Physiol Rev

Publisher American Physiological Society

Specialty Physiology

Date 1999 Jan 29

PMID 9922371

Citations 229

Authors

D Vestweber

J E Blanks

Affiliations

Soon will be listed here.

Abstract

Selectins are a family of three cell adhesion molecules (L-, E-, and P-selectin) specialized in capturing leukocytes from the bloodstream to the blood vessel wall. This initial cell contact is followed by the selectin-mediated rolling of leukocytes on the endothelial cell surface. This represents the first step in a cascade of molecular interactions that lead to leukocyte extravasation, enabling the processes of lymphocyte recirculation and leukocyte migration into inflamed tissue. The central importance of the selectins in these processes has been well documented in vivo by the use of adhesion-blocking antibodies as well as by studies on selectin gene-deficient mice. This review focuses on the molecular mechanisms that regulate expression and function(s) of the selectins and their ligands. Cell-surface expression of the selectins is regulated by a variety of different mechanisms. The selectins bind to carbohydrate structures on glycoproteins, glycolipids, and proteoglycans. Glycoproteins are the most likely candidates for physiologically relevant ligands. Only a few glycoproteins are appropriately glycosylated to allow strong binding to the selectins. Recently, more knowledge about the structure and the regulated expression of some of the carbohydrates on these ligands necessary for selectin binding has been accumulated. For at least one of these ligands, the physiological function is now well established. A novel and exciting aspect is the signaling function of the selectins and their ligands. Especially in the last two years, convincing data have been published supporting the idea that selectins and glycoprotein ligands of the selectins participate in the activation of leukocyte integrins.

Citing Articles

Two-in-one nanoparticle platform induces a strong therapeutic effect of targeted therapies in P-selectin-expressing cancers.

Koshrovski-Michael S, Ajamil D, Dey P, Kleiner R, Tevet S, Epshtein Y Sci Adv. 2024; 10(50):eadr4762.

PMID: 39671487 PMC: 11641104. DOI: 10.1126/sciadv.adr4762.

Leukocyte rolling on engineered nanodot surfaces.

Lin-Schmidt X, Ham A, Reed M, Lawrence M, Helmke B Micro Nano Lett. 2024; 6(5):301-305.

PMID: 39512362 PMC: 11542712. DOI: 10.1049/mnl.2011.0184.

The Anti-Inflammatory Effect of -Ling-Zhi 8 on Ameliorating Atherosclerosis and Nonalcoholic Fatty Liver in High-Fat Diet Rabbits.

Lee M, Wang N, Chu Y, Wu C, Lin W Int J Mol Sci. 2024; 25(20).

PMID: 39457059 PMC: 11508337. DOI: 10.3390/ijms252011278.

Identification of a Novel Activated NK-Associated Gene Score Associated with Diagnosis and Biological Therapy Response in Ulcerative Colitis.

Dong S, Zhang Y, Ye L, Cao Q Digestion. 2024; 106(1):1-22.

PMID: 39182484 PMC: 11825133. DOI: 10.1159/000540939.

Glycosylation: mechanisms, biological functions and clinical implications.

He M, Zhou X, Wang X Signal Transduct Target Ther. 2024; 9(1):194.

PMID: 39098853 PMC: 11298558. DOI: 10.1038/s41392-024-01886-1.