Kunkel E J, Ley K
Department of Biomedical Engineering, University of Virginia School of Medicine, Charlottesville 22908, USA.
Circ Res. 1996 Dec;79(6):1196-204. doi: 10.1161/01.res.79.6.1196.
Leukocyte capture and rolling are mediated by calcium-dependent lectins expressed on most leukocytes (L-selectin) and the vascular endothelium (P- and E-selectin). To study the role of the selectins during inflammation, we have investigated leukocyte rolling in venules of tumor necrosis factor-alpha (TNF-alpha)-treated mouse cremaster muscles in wild-type mice and gene-targeted mice with homozygous deficiency for L-, P-, or E-selectin (L-/-, P-/-, or E-/-, respectively). TNF-alpha treatment induces expression of E-selectin and increases expression of P-selectin on endothelial cells. Consistent with previous reports of redundant P- and E-selectin function, a combination of monoclonal antibodies (mAbs) against P- and E-selectin (RB40.34 and 9A9, respectively) was necessary to block rolling in wild-type mice. The rolling leukocyte flux fraction (percent rolling cells) in L-/- mice was similar to that in wild-type mice, but rolling in these mice was blocked by a P-selectin mAb. The velocity of rolling leukocytes in TNF-alpha-treated wild-type, P-/-, or L-/- mice was 5 to 10 times slower (3 to 7 microns/s) than during trauma-induced rolling (20 to 50 microns/s). In contrast, leukocytes in venules of TNF-alpha-treated E-/- mice rolled significantly faster (12 to 20 microns/s): the rolling leukocyte flux fraction was more than doubled compared with wild-type, L-/-, or P-/- mice; and the number of adherent leukocytes was reduced. Addition of an E-selectin mAb, but not a P-selectin mAb, increased rolling flux fraction and rolling velocity in wild-type mice. Histological analysis revealed that 90% to 95% of all leukocytes interacting (rolling and adherent) with the venular endothelium in TNF-alpha-treated wild-type, L-/-, P-/-, and E-/- mice were granulocytes. These results identify a previously unrecognized phenotype of E-/- mice by establishing that at the site densities prevailing in vivo, E-selectin in responsible for slow (approximately 5 microns/s) granulocyte rolling. E-selectin-dependent slow rolling drastically increases the transit time of leukocytes rolling through an inflamed tissue and thus aids in targeting leukocytes activated by chemoattractants to the inflammatory microenvironment.
白细胞的捕获和滚动由大多数白细胞(L-选择素)和血管内皮细胞(P-选择素和E-选择素)上表达的钙依赖性凝集素介导。为了研究选择素在炎症过程中的作用,我们研究了野生型小鼠以及L-、P-或E-选择素纯合缺失的基因靶向小鼠(分别为L-/-、P-/-或E-/-)肿瘤坏死因子-α(TNF-α)处理的小鼠提睾肌小静脉中的白细胞滚动情况。TNF-α处理可诱导E-选择素表达,并增加内皮细胞上P-选择素的表达。与先前关于P-选择素和E-选择素功能冗余的报道一致,针对P-选择素和E-选择素的单克隆抗体(分别为RB40.34和9A9)组合对于阻断野生型小鼠中的滚动是必需的。L-/-小鼠中的滚动白细胞通量分数(滚动细胞百分比)与野生型小鼠相似,但这些小鼠中的滚动被一种P-选择素单克隆抗体阻断。在TNF-α处理的野生型、P-/-或L-/-小鼠中,滚动白细胞的速度比创伤诱导的滚动(20至50微米/秒)慢5至10倍(3至7微米/秒)。相比之下,TNF-α处理的E-/-小鼠小静脉中的白细胞滚动速度明显更快(12至20微米/秒):滚动白细胞通量分数比野生型、L-/-或P-/-小鼠增加了一倍多;并且黏附白细胞的数量减少。添加E-选择素单克隆抗体而非P-选择素单克隆抗体可增加野生型小鼠中的滚动通量分数和滚动速度。组织学分析显示,在TNF-α处理的野生型、L-/-、P-/-和E-/-小鼠中,与小静脉内皮相互作用(滚动和黏附)的所有白细胞中有90%至95%是粒细胞。这些结果通过证实体内普遍存在的位点密度下,E-选择素负责缓慢(约5微米/秒)的粒细胞滚动,确定了E-/-小鼠以前未被认识的表型。E-选择素依赖性的缓慢滚动极大地增加了白细胞在炎症组织中滚动的通过时间,从而有助于将由趋化因子激活的白细胞靶向炎症微环境。
