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新生儿中性粒细胞上凝集素、表皮生长因子、补体结合域细胞黏附分子-1减少是其体外CD18非依赖性黏附于内皮细胞受损的基础。

Diminished lectin-, epidermal growth factor-, complement binding domain-cell adhesion molecule-1 on neonatal neutrophils underlies their impaired CD18-independent adhesion to endothelial cells in vitro.

作者信息

Anderson D C, Abbassi O, Kishimoto T K, Koenig J M, McIntire L V, Smith C W

机构信息

Department of Pediatrics, Baylor College of Medicine, Houston, TX 77030.

出版信息

J Immunol. 1991 May 15;146(10):3372-9.

PMID:1709192
Abstract

To define further the molecular basis for abnormal interactions of cord blood or neonatal neutrophils with endothelial cells in vitro, we studied neutrophil adhesion and migration under experimental conditions specifically designed to evaluate CD18-independent mechanisms. Unstimulated cord blood neutrophils of healthy term neonates demonstrated significantly diminished adhesion to IL-1-stimulated endothelial cell monolayers under conditions of shear stress (congruent to 1.85 dynes/cm2); overall levels of migration by neonatal cells were also significantly diminished, although the adherent subpopulation of these cells migrated relatively normally. A mAb (DREG-56) against the human homologue of the murine MEL-14 antigen (termed lectin-, epidermal growth factor-, complement binding domain-cell adhesion molecule-1 (LECAM-1), a member of the LEC-CAM family of adhesion molecules) markedly inhibited adhesion of healthy adult but not cord blood neutrophils. In additional assessments of endothelial cell adhesion or migration in the absence of shear forces, cord blood neutrophils demonstrated significantly diminished values compared to adult controls. Moreover, mAb DREG-56 significantly diminished adhesion of healthy adult but not cord blood suspensions in the presence or absence of the anti-CD18 mAb R15.7. Immunofluorescence assessments of unstimulated cord blood neutrophils or neutrophils of neonates 12 to 48 h of age showed dramatically diminished levels of surface LECAM-1 compared to adult neutrophils. Chemotactic stimuli (FMLP, 10 nM, 15 min) consistently "down-regulated" surface LECAM-1 on adult neutrophils to levels approximately 10% of unstimulated suspensions and comparable to those of most unstimulated neonatal suspensions. Moreover, FMLP stimuli elicited little or no down-regulation of LECAM-1 on neonatal cells. In comparative studies, endothelial cell adhesion of unstimulated cord blood or adult control neutrophils (assessed under conditions of flow) was directly related to levels of neutrophil surface LECAM-1. Although FMLP stimulation significantly diminished both adhesion and LECAM-1 surface levels of adult control cells, the adhesion and LECAM-1 expression observed with cord blood cells were not significantly influenced by this stimulus. The mechanisms underlying diminished LECAM-1 expression and LECAM-1-dependent adhesion of neonatal neutrophils and the physiologic significance of these abnormalities deserve investigation.

摘要

为了进一步明确脐血或新生儿中性粒细胞在体外与内皮细胞异常相互作用的分子基础,我们在专门设计用于评估不依赖CD18机制的实验条件下研究了中性粒细胞的黏附和迁移。健康足月儿的未刺激脐血中性粒细胞在剪切应力条件下(约1.85达因/平方厘米)对IL-1刺激的内皮细胞单层的黏附显著减少;新生儿细胞的总体迁移水平也显著降低,尽管这些细胞的黏附亚群迁移相对正常。一种针对小鼠MEL-14抗原的人同源物的单克隆抗体(DREG-56)(称为凝集素、表皮生长因子、补体结合域细胞黏附分子-1(LECAM-1),是LEC-CAM黏附分子家族的成员)显著抑制健康成人中性粒细胞的黏附,但不抑制脐血中性粒细胞的黏附。在无剪切力情况下对内皮细胞黏附或迁移的额外评估中,脐血中性粒细胞与成人对照相比,其值显著降低。此外,无论有无抗CD18单克隆抗体R15.7,单克隆抗体DREG-56都显著降低健康成人但不降低脐血悬浮液的黏附。对未刺激的脐血中性粒细胞或12至48小时龄新生儿的中性粒细胞进行免疫荧光评估显示,与成人中性粒细胞相比,表面LECAM-1水平显著降低。趋化刺激(FMLP,10 nM,15分钟)持续将成人中性粒细胞表面的LECAM-1“下调”至未刺激悬浮液水平的约10%,与大多数未刺激的新生儿悬浮液水平相当。此外,FMLP刺激对新生儿细胞上的LECAM-1几乎没有下调作用。在比较研究中,未刺激的脐血或成人对照中性粒细胞的内皮细胞黏附(在流动条件下评估)与中性粒细胞表面LECAM-1水平直接相关。尽管FMLP刺激显著降低了成人对照细胞的黏附和LECAM-1表面水平,但脐血细胞观察到的黏附和LECAM-1表达不受该刺激的显著影响。新生儿中性粒细胞LECAM-1表达减少和LECAM-1依赖性黏附的潜在机制以及这些异常的生理意义值得研究。

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