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A model for the investigation of factors influencing haemorrhagic necrosis mediated by tumour necrosis factor in tissue sites primed with mycobacterial antigen preparations.

机译:在分枝杆菌抗原制剂引发的组织部位中由肿瘤坏死因子介导的影响出血坏死的因素研究模型。

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摘要

Mycobacterial lesions and skin sites challenged with soluble mycobacterial antigen are very sensitive to the necrotizing effect of tumour necrosis factor (TNF). We have used a model that permits separate quantitative assessment of swelling and haemorrhage to show that when these reactions are elicited in mice that have not been deliberately immunized, pretreatment of the mice with lipopolysaccharide (LPS), or with a MoAb to CR3 which blocks emigration of myeloid cells into the tissues, will block both the swelling and the haemorrhage. On the other hand, treatment with an inhibitor of platelet-activating factor (PAF), or with misoprostol (a synthetic prostaglandin E1 analogue), or with cobra venom factor (CVF) which depletes complement, preferentially blocks the haemorrhagic component, while leaving the swelling relatively unaltered. As swelling occurs before the haemorrhage is seen, it is possible that these factors act at a late stage in the cascade of events leading to the tissue damage. However, LPS and CVF were able to inhibit swelling and haemorrhage in the massive reactions elicited in pre-immunized animals, whereas the PAF inhibitor had no detectable effect.
机译:用可溶性分枝杆菌抗原攻击的分枝杆菌病变和皮肤部位对肿瘤坏死因子(TNF)的坏死作用非常敏感。我们使用的模型允许对肿胀和出血进行单独的定量评估,以表明当在未刻意免疫的小鼠中引发这些反应时,可以用脂多糖(LPS)或用MoAb预处理小鼠来阻止CR3迁移髓样细胞进入组织,将阻止肿胀和出血。另一方面,用血小板活化因子(PAF)抑制剂,米索前列醇(合成的前列腺素E1类似物)或补充补体的眼镜蛇毒因子(CVF)治疗,优先阻断出血成分,同时保留肿胀相对不变。由于在看到出血之前会发生肿胀,因此这些因素有可能在导致组织损伤的一系列事件的后期起作用。但是,LPS和CVF能够抑制免疫前动物引起的大规模反应中的肿胀和出血,而PAF抑制剂则没有可检测的作用。

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