血清淀粉样蛋白P抑制粒细胞粘附。

Anu S Maharjan, David Roife, Derrick Brazill, Richard H Gomer
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引用次数: 33

摘要

背景:粒细胞(如中性粒细胞)在炎症部位的外渗是先天免疫系统的一个关键方面。来自炎症部位的信号上调了粒细胞对内皮的粘附,从而引发外渗,同时也增强了粒细胞对细胞外基质蛋白的粘附,促进了粒细胞在炎症组织中的运动。在炎症消退过程中,其他信号抑制粒细胞粘附,减缓并最终阻止粒细胞流入组织。在各种炎症性疾病中,如急性呼吸窘迫综合征,粒细胞过度浸润到组织中会引起不希望的附带损害,能够减少粒细胞的粘附和内流可以减少这种损害。结果:我们发现血清淀粉样蛋白P (SAP),血液的组成蛋白成分,抑制粒细胞扩散和粒细胞粘附到细胞外基质成分。这表明,除了在炎症消退过程中分泌的粒细胞粘附抑制剂外,血液中还存在一种粒细胞粘附抑制剂。虽然SAP影响粘附,但它不影响粒细胞粘附分子CD11b、CD62L、CD18或CD44。SAP对静止或刺激的粒细胞或n -甲酰蛋氨酸-赖氨酸-苯丙氨酸(fMLP)诱导的粒细胞迁移产生过氧化氢也没有影响。在气管内注射博来霉素诱导肺中粒细胞积聚的小鼠中,SAP注射减少了肺中粒细胞的数量。结论:我们发现血的组成成分SAP是一种粒细胞粘附抑制剂。我们假设SAP允许粒细胞感知它们是在血液中还是在组织中。
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Serum amyloid P inhibits granulocyte adhesion.

Background: The extravasation of granulocytes (such as neutrophils) at a site of inflammation is a key aspect of the innate immune system. Signals from the site of inflammation upregulate granulocyte adhesion to the endothelium to initiate extravasation, and also enhance granulocyte adhesion to extracellular matrix proteins to facilitate granulocyte movement through the inflamed tissue. During the resolution of inflammation, other signals inhibit granulocyte adhesion to slow and ultimately stop granulocyte influx into the tissue. In a variety of inflammatory diseases such as acute respiratory distress syndrome, an excess infiltration of granulocytes into a tissue causes undesired collateral damage, and being able to reduce granulocyte adhesion and influx could reduce this damage.

Results: We found that serum amyloid P (SAP), a constitutive protein component of the blood, inhibits granulocyte spreading and granulocyte adhesion to extracellular matrix components. This indicates that in addition to granulocyte adhesion inhibitors that are secreted during the resolution of inflammation, a granulocyte adhesion inhibitor is present at all times in the blood. Although SAP affects adhesion, it does not affect the granulocyte adhesion molecules CD11b, CD62L, CD18, or CD44. SAP also has no effect on the production of hydrogen peroxide by resting or stimulated granulocytes, or N-formyl-methionine-leucine-phenylalanine (fMLP)-induced granulocyte migration. In mice treated with intratracheal bleomycin to induce granulocyte accumulation in the lungs, SAP injections reduced the number of granulocytes in the lungs.

Conclusions: We found that SAP, a constitutive component of blood, is a granulocyte adhesion inhibitor. We hypothesize that SAP allows granulocytes to sense whether they are in the blood or in a tissue.

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