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通过L-选择素的细胞质结构域对白细胞向高内皮微静脉滚动和黏附的调节。

Regulation of leukocyte rolling and adhesion to high endothelial venules through the cytoplasmic domain of L-selectin.

作者信息

Kansas G S, Ley K, Munro J M, Tedder T F

机构信息

Division of Tumor Immunology, Dana Farber Cancer Institute, Boston, Massachusetts.

出版信息

J Exp Med. 1993 Mar 1;177(3):833-8. doi: 10.1084/jem.177.3.833.

Abstract

L-selectin (leukocyte adhesion molecule 1/MEL-14), a member of the selectin family of cell adhesion molecules, mediates leukocyte rolling and leukocyte adhesion to endothelium at sites of inflammation. In addition, L-selectin mediates the binding of lymphocytes to high endothelial venules (HEV) of peripheral lymph nodes. The strong amino acid sequence conservation of the cytoplasmic domain of L-selectin between humans and mice suggests an important role for this region. Deletion of the COOH-terminal 11 amino acids from the approximately 17 amino acid cytoplasmic domain of L-selectin eliminated binding of lymphocytes to HEV in the in vitro frozen section assay, and also abolished leukocyte rolling in vivo in exteriorized rat mesenteric venules, but did not alter the lectin activity of L-selectin. Pretreatment of cells with cytochalasin B, which disrupts actin microfilaments, also abolished adhesion without affecting carbohydrate recognition. Therefore, the cytoplasmic domain of L-selectin regulates leukocyte adhesion to endothelium independent of ligand recognition, by controlling cytoskeletal interactions and/or receptor avidity.

摘要

L-选择素(白细胞黏附分子1/MEL-14)是细胞黏附分子选择素家族的一员,在炎症部位介导白细胞滚动及白细胞与内皮细胞的黏附。此外,L-选择素介导淋巴细胞与外周淋巴结高内皮微静脉(HEV)的结合。人与小鼠L-选择素胞质结构域的氨基酸序列高度保守,提示该区域具有重要作用。在体外冰冻切片试验中,从L-选择素约17个氨基酸的胞质结构域中缺失羧基末端的11个氨基酸,消除了淋巴细胞与HEV的结合,并且在体外大鼠肠系膜小静脉中也消除了白细胞滚动,但未改变L-选择素的凝集素活性。用破坏肌动蛋白微丝的细胞松弛素B预处理细胞,同样消除了黏附,而不影响碳水化合物识别。因此,L-选择素的胞质结构域通过控制细胞骨架相互作用和/或受体亲和力,独立于配体识别来调节白细胞与内皮细胞的黏附。

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