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缺乏E-选择素的小鼠滚动白细胞数量正常,但细胞因子激活的微血管内皮上白细胞的稳定黏附减少。

Mice lacking E-selectin show normal numbers of rolling leukocytes but reduced leukocyte stable arrest on cytokine-activated microvascular endothelium.

作者信息

Milstone D S, Fukumura D, Padgett R C, O'Donnell P E, Davis V M, Benavidez O J, Monsky W L, Melder R J, Jain R K, Gimbrone M A

机构信息

Department of Pathology, Brigham and Women's Hospital, Boston, MA, USA.

出版信息

Microcirculation. 1998;5(2-3):153-71.

PMID:9789256
Abstract

OBJECTIVE

Previous work indicated that E-selectin mediates transient interactions between leukocytes and cytokine-activated endothelium in vitro. Here we examine the role of E-selectin in blood leukocyte interactions with microvascular endothelium in vivo.

METHODS

E-selectin-deficient (E-/-) mice were produced by gene targeting. The effect of this null mutation on leukocyte-endothelial interactions was determined by intravital microscopy before and 4 to 5 hours after local administration of the proinflammatory cytokine tumor necrosis factor alpha (TNF alpha) in dermal microvessels with low blood flow (dorsal skin-fold chambers, intact ear skin), and after endotoxin activation in exteriorized mesenteric microvessels with higher blood flow.

RESULTS

E-/- mice were viable, fertile with normal circulating leukocyte and platelet profiles. Approximately 60% of circulating leukocytes rolled in dermal microvessels of both normal (E+/+) and E-/- mice without inflammatory stimulation. After local administration of TNF alpha, rolling increased modestly and equivalently in both genotypes. The main effect of TNF alpha was a dramatic increase in leukocyte stable adhesion and, unlike rolling, this manifestation of endothelial activation was significantly reduced in E-/- animals. This reflected fewer dermal microvessels supporting higher adhesion densities in E-/- mice, and a similar trend was observed in mesenteric microvessels.

CONCLUSIONS

E-selectin plays a previously unappreciated role in facilitating and/or mediating stable adhesion of leukocytes to inflamed microvascular endothelium.

摘要

目的

先前的研究表明,E-选择素在体外介导白细胞与细胞因子激活的内皮细胞之间的短暂相互作用。在此,我们研究E-选择素在体内血液白细胞与微血管内皮细胞相互作用中的作用。

方法

通过基因靶向产生E-选择素缺陷(E-/-)小鼠。通过活体显微镜检查,在低血流的真皮微血管(背部皮肤褶皱腔室、完整耳部皮肤)局部给予促炎细胞因子肿瘤坏死因子α(TNFα)之前和之后4至5小时,以及在高血流的肠系膜微血管内毒素激活后,确定这种无效突变对白细胞-内皮细胞相互作用的影响。

结果

E-/-小鼠存活、可育,循环白细胞和血小板谱正常。在无炎症刺激的情况下,正常(E+/+)和E-/-小鼠的真皮微血管中约60%的循环白细胞发生滚动。局部给予TNFα后,两种基因型的滚动均适度且同等增加。TNFα的主要作用是白细胞稳定黏附显著增加,与滚动不同,内皮细胞激活的这种表现在E-/-动物中显著降低。这反映出E-/-小鼠中支持更高黏附密度的真皮微血管较少,在肠系膜微血管中也观察到类似趋势。

结论

E-选择素在促进和/或介导白细胞与炎症微血管内皮细胞的稳定黏附中发挥了先前未被认识到的作用。

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