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Localization of leucocytes in sites of delayed-type hypersensitivity and in lymph nodes: dependence on vasoactive amines.

机译:白细胞在迟发型超敏反应部位和淋巴结中的定位:依赖于血管活性胺。

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摘要

Murine delayed-type hypersensitivity (DTH) reactions and the localization of 51chromium-labelled leucocytes into DTH sites, as well as into lymph nodes, can be markedly inhibited by drugs that deplete vasoactive amines (VAA; reserpine); antagonize VAA action (methysergide, cyproheptadine), or block the release of VAA from mast cells (Proxicromil). These drug treatments have much less of an effect on the cells that localize in tissues that are not separated from the blood by venule endothelium such as spleen, liver and the bone marrow. These results suggest that localization of many blood borne leucocytes in tissues that are separated from the blood by venule endothelium requires VAA to induce the formation of 'gaps' between the endothelial cells in order for the leucocytes to make an exit from the blood. Thus DTH may be considered, at least in part, as a tissue equivalent of a lymph node 'trap', with the difference being the type of recruited or 'trapped' cell type; inflammatory leucocytes in DTH responses and lymphocytes in lymph nodes.
机译:耗尽血管活性胺的药物(VAA;利血平)可显着抑制鼠类迟发型超敏反应(DTH)以及将51铬标记的白细胞定位于DTH部位以及淋巴结。拮抗VAA的作用(甲基麦角酰胺,赛庚啶),或阻止VAA从肥大细胞中释放(Proxicromil)。这些药物处理对局部细胞的作用要小得多,这些细胞未通过小静脉内皮与血液分离开来的组织,例如脾脏,肝脏和骨髓。这些结果表明,在通过小静脉内皮与血液分离的组织中许多血源性白细胞的定位需要VAA诱导内皮细胞之间形成“缺口”,以便白细胞从血液中排出。因此,DTH可以至少部分地视为与淋巴结“陷阱”等效的组织,区别在于募集或“陷阱”细胞的类型。 DTH反应中的炎症性白细胞和淋巴结中的淋巴细胞。

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