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白三烯B4和白三烯D4对白细胞向豚鼠结膜迁移的协同作用。

Synergistic effects of LTB4 and LTD4 on leukocyte emigration into the guinea pig conjunctiva.

作者信息

Spada C S, Woodward D F, Hawley S B, Nieves A L, Williams L S, Feldmann B J

机构信息

Pharmacology Department, Allergan Eye and Skin Care Group, Irvine, CA 92715.

出版信息

Am J Pathol. 1988 Feb;130(2):354-68.

Abstract

Leukotrienes (LT) B4 and D4, alone and in combination, were topically applied to the eyes of guinea pigs, and their effects on conjunctival leukocyte infiltration studied. LTD4 potentiated the neutrophil response to LTB4, even though no neutrophil emigration was evoked by LTD4 itself over a dose range of 10-1000 ng. LTB4 alone at the 1-ng and 10-ng doses failed to evoke any leukocyte emigration, but significant numbers of neutrophils were observed at these concentrations when LTD4 (1-1000 ng) was present. Although a dose-dependent increase in neutrophil infiltration was observed for the 100-ng and 1000-ng doses of LTB4, cell counts were substantially higher with these doses in the presence of LTD4. Eosinophil numbers increased in a dose-related manner in response to LTB4 and LTD4 alone, with a greater response to LTD4. The addition of either 10 ng or 100 ng of LTB4 to graded doses of LTD4 (10-1000 ng) caused increased eosinophil numbers, the lower dose of LTB4 potentiating the response to LTD4 and the higher LTB4 dose showing no significant effect. The effects on leukocyte infiltration that were evoked by the LT combinations could not be explained simply on the basis of an increase in vascular permeability. Bradykinin (BK), a potent conjunctival microvascular permeability factor that does not elicit any leukocyte infiltration, did not significantly potentiate LTB4-induced eosinophil or neutrophil emigration. The synergistic effects of LTs on leukocyte emigration are also difficult to ascribe to hyperemia (ie, increased blood volume in the conjunctiva), because both LTB4 and LTD4 caused only very modest increases in conjunctival blood content, and BK, which did not potentiate the leukocytic responses to LTB4, caused marked increases in tissue blood content. High-dose LT combinations caused eosinophils, but not neutrophils, to migrate into the conjunctival epithelium and fragment, resulting in overt tissue damage. These results further suggest a synergistic interaction between LTB4 and LTD4 that directly alters leukocyte function. The relevance of these observations to a number of disease and trauma states is discussed.

摘要

将白三烯(LT)B4和D4单独及联合局部应用于豚鼠眼部,并研究它们对结膜白细胞浸润的影响。尽管在10 - 1000 ng剂量范围内,LTD4本身未引起中性粒细胞迁移,但LTD4增强了中性粒细胞对LTB4的反应。单独使用1 ng和10 ng剂量的LTB4未能引起任何白细胞迁移,但当存在LTD4(1 - 1000 ng)时,在这些浓度下观察到大量中性粒细胞。尽管对于100 ng和1000 ng剂量的LTB4观察到中性粒细胞浸润呈剂量依赖性增加,但在存在LTD4的情况下,这些剂量的细胞计数显著更高。单独使用LTB4和LTD4时,嗜酸性粒细胞数量呈剂量相关增加,对LTD4的反应更大。向不同剂量的LTD4(10 - 1000 ng)中添加10 ng或100 ng的LTB4会导致嗜酸性粒细胞数量增加,较低剂量的LTB4增强了对LTD4的反应,而较高剂量的LTB4未显示出显著影响。LT组合引起的对白细胞浸润的影响不能简单地基于血管通透性增加来解释。缓激肽(BK)是一种强效的结膜微血管通透性因子,不会引起任何白细胞浸润,它并未显著增强LTB4诱导的嗜酸性粒细胞或中性粒细胞迁移。LT对白细胞迁移的协同作用也难以归因于充血(即结膜血容量增加),因为LTB4和LTD4仅引起结膜血容量非常适度的增加,而未增强对LTB4的白细胞反应的BK却引起组织血容量显著增加。高剂量的LT组合导致嗜酸性粒细胞而非中性粒细胞迁移到结膜上皮并破碎,导致明显的组织损伤。这些结果进一步表明LTB4和LTD4之间存在直接改变白细胞功能的协同相互作用。讨论了这些观察结果与多种疾病和创伤状态的相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9fb9/1880531/864f5d5cb4cb/amjpathol00137-0147-a.jpg

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