首页> 美国卫生研究院文献>The American Journal of Pathology >Increased microvascular permeability in vivo in response to intradermal injection of neutrophil-activating protein (NAP-2) in rabbit skin.
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Increased microvascular permeability in vivo in response to intradermal injection of neutrophil-activating protein (NAP-2) in rabbit skin.

机译:皮内注射中性粒细胞活化蛋白(NAP-2)在兔皮肤中响应体内微血管通透性增加。

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摘要

Neutrophil-activating protein-2 (NAP-2), an NH2-terminally processed form of the platelet-release product beta thromboglobulin (beta TG), was purified to homogeneity from stimulated human blood leukocytes. In the presence of a vasodilator substance (PGE2, CGRP) picomolar (pmol/l) amounts of NAP-2 induced neutrophil accumulation and plasma leakage on intradermal injection in rabbit skin, whereas the longer forms, beta TG itself and connective tissue-activating peptide III (CTAP-III), had no such effect. NAP-2-induced increased in microvascular permeability was neutrophil dependent and fast in onset, with a half-life of 65 to 75 minutes, comparable to that previously reported for the structural-related neutrophil-activating protein-1/interleukin-8 (NAP-1/IL-8). However NAP-2 showed a lower potency in that more protein was needed to provoke skin reactivity. Nevertheless the finding that a platelet release product can elicit neutrophil-mediated inflammation further narrows the gap between thrombotic events and inflammatory disorders.
机译:嗜中性粒细胞活化蛋白2(NAP-2)是一种由NH2末端处理的血小板释放产物β血球蛋白(βTG)形式,可从刺激的人血白细胞中纯化至同质。当存在皮下注射血管扩张剂(PGE2,CGRP)皮摩尔(pmol / l)量的NAP-2时,嗜中性白细胞积聚和血浆渗漏,而较长的形式,βTG本身和结缔组织激活肽III(CTAP-III)没有这种效果。 NAP-2诱导的微血管通透性增加是中性粒细胞依赖性的,且起效快,半衰期为65至75分钟,与之前报道的与结构相关的中性粒细胞激活蛋白-1 /白介素8(NAP)相当-1 / IL-8)。然而,NAP-2显示出较低的效力,因为需要更多的蛋白质来激发皮肤反应性。然而,血小板释放产物可引起中性粒细胞介导的炎症的发现进一步缩小了血栓形成事件与炎症性疾病之间的距离。

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