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首页> 外文期刊>Journal of Leukocyte Biology: An Official Publication of the Reticuloendothelial Society >Nonspecific and immune-specific up-regulation of cytokines in rabbit dermal tuberculous (BCG) lesions.
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Nonspecific and immune-specific up-regulation of cytokines in rabbit dermal tuberculous (BCG) lesions.

机译:兔皮肤结核(BCG)病变中细胞因子的非特异性和免疫特异性上调。

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To our knowledge, this is the first sequential study of cytokines in tissue sections of developing and healing tuberculous (BCG) lesions. In situ hybridization, immunohistochemical, and RT-PCR techniques were used. Cytokine mRNAs showed a biphasic pattern. The percentage of mononuclear cells (MN) containing IL-1beta, TNF-alpha, MCP-1, and IL-8 mRNAs was highest in 1- to 3-day lesions, apparently because of the nonspecific inflammatory response caused by the tubercle bacilli in the BCG vaccine. At 5 days, this percentage was significantly reduced. With IFN-gamma, the peak and trough were delayed by 2 days. By 9 days, the percentage of MN containing the mRNAs of all five cytokines had again increased and the rabbits had become tuberculin-positive. In general, MCP-1 and TNF-alpha proteins and the vascular adhesion molecules, ICAM, VCAM, and perhaps ELAM, peaked at about 3 days. Many mononuclear cells surrounding the central areas of solid and liquefied caseous necrosis contained chemokine IL-8 mRNA. IL-8 is known to attract PMN, and PMN were present nearby. In contrast, MN containing chemokine MCP-1 mRNA were present more peripherally in areas rich in macrophages and lymphocytes. The early nonspecific cytokine response seems to be an adjuvant effect of the mycobacteria in BCG vaccine in that it causes a rapid entry of macrophages, lymphocytes, granulocytes, and probably dendritic cells into local sites of antigen deposition. This effect should be considered in developing improved vaccines for the prevention of tuberculosis, because BCG vaccines producing a strong early cytokine response should be more immunogenic than BCG vaccines with similar antigens producing a weak response.
机译:据我们所知,这是对发展中的和愈合的结核病(BCG)病变组织切片中的细胞因子进行的第一个顺序研究。使用原位杂交,免疫组化和RT-PCR技术。细胞因子mRNA显示出双相模式。含有IL-1β,TNF-α,MCP-1和IL-8 mRNA的单核细胞(MN)的百分比在1至3天的病变中最高,这显然是由于结核杆菌引起的非特异性炎症反应所致。卡介苗疫苗。在第5天,该百分比显着降低。使用IFN-γ时,峰谷降低了2天。到9天时,含有所有五种细胞因子mRNA的MN的百分比再次增加,兔的结核菌素阳性。通常,MCP-1和TNF-α蛋白以及血管黏附分子ICAM,VCAM甚至ELAM在约3天达到峰值。固态和液化干酪坏死中心区域周围的许多单核细胞均含有趋化因子IL-8 mRNA。已知IL-8会吸引PMN,而PMN则在附近。相比之下,含有趋化因子MCP-1 mRNA的MN在富含巨噬细胞和淋巴细胞的区域中更外围存在。早期的非特异性细胞因子应答似乎是BCG疫苗中分枝杆菌的辅助作用,因为它会导致巨噬细胞,淋巴细胞,粒细胞以及可能的树突状细胞迅速进入抗原沉积的局部位点。在开发用于预防结核病的改良疫苗时应考虑这种效果,因为产生强的早期细胞因子应答的BCG疫苗应比具有类似抗原而产生弱应答的BCG疫苗更具免疫原性。

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