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首页> 外文期刊>Folia histochemica et cytobiologica >Monocyte response receptors in BCG driven delayed type hypersensitivity to tuberculin.
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Monocyte response receptors in BCG driven delayed type hypersensitivity to tuberculin.

机译:BCG中的单核细胞反应受体驱动了对结核菌素的迟发型超敏反应。

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Tuberculosis (TB) still remains the leading cause of mortality due to bacterial pathogen. The only currently available vaccine against TB, Bacille Calmette-Guerin (BCG) is at best credited with a 50% overall protective efficacy. Skin testing with purified protein derivative (PPD) from Mycobacterium tuberculosis is the method of detecting BCG-induced cell mediated immunity, in vivo. In the previous study we found that approximately 60% young volunteers with no history of TB, who had been subjected to neonatal BCG vaccination and revaccination(s) at school age, developed delayed type hypersensitivity (DTH) to tuberculin. The remaining volunteers were persistently tuberculin negative. Moreover, we found a significant association between BCG driven development of DTH to PPD and the polymorphism within the CD14 C/T(-159) gene for macrophage receptor recognising mycobacterial compounds. It has suggested that the CD14 gene variants may play a role in the appearance and persistence of DTH to PPD in BCG vaccinated subjects. In order to extend our study on a possible role of CD14 in BCG driven DTH response to PPD, we measured the expression of mCD14 on macrophages, stimulated or not stimulated with mycobacterial antigens, and the serum levels of sCD14. Considering the importance of CD14 - TLR2/TLR4 interactions in macrophage signalling, we determined the polymorphism of TLR2 and TLR4 genes as well as macrophage expression of TLR2 for the volunteers with and without skin reactivity to PPD. We observed a subtle but significant decrease in CD14 density on adherent monocytes from tuberculin positive versus tuberculin negative volunteers. However, we found no difference in CD14 density on monocytes enriched in CD14+ cells using anti-CD14 mAb coupled to magnetic beads. A significant increase in CD14 density was observed on macrophages stimulated with PPD and LPS but not with live BCG bacilli. However, this increase as well as serum levels of soluble sCD14 were similar in the volunteers with and without skin reactions to PPD. Thus, our suggestion on the role of CD14 in the generation of DTH to tuberculin in BCG vaccinated subjects should be further explored. The most important CD14 co-receptors are Toll-like receptors (TLRs) which activate nuclear factors for the production of inflammatory cytokines. However, we could see no association between the polymorphisms of TLR4 (Asp299Gly and Thr399Ile) and TLR2 genes (Arg753Gln and Arg677Trp) and skin responses to PPD. Also, the TLR2 density was similar on monocytes from tuberculin negative and tuberculin positive volunteers.
机译:由于细菌病原体,结核病(TB)仍然是导致死亡的主要原因。 Bacille Calmette-Guerin(BCG)是目前唯一可用的抗结核疫苗,其最高的整体防护功效被认为是50%。用来自结核分枝杆菌的纯化蛋白衍生物(PPD)进行皮肤测试是体内检测BCG诱导的细胞介导的免疫的方法。在先前的研究中,我们发现大约60%的无结核病史的年轻志愿者在学龄时接受了新生儿BCG疫苗接种和再接种,他们对结核菌素发展为迟发型超敏反应(DTH)。其余志愿者持续结核菌素阴性。此外,我们发现BCG驱动DTH向PPD的发展与巨噬细胞受体识别分枝杆菌化合物的CD14 C / T(-159)基因内的多态性之间存在显着关联。已经表明CD14基因变体可能在接种BCG的受试者中DTH对PPD的出现和持久性中起作用。为了扩展我们对CD14在BCG驱动的DTH对PPD应答中可能作用的研究,我们测量了在分枝杆菌抗原刺激或不刺激的巨噬细胞上mCD14的表达,以及血清sCD14的水平。考虑到CD14-TLR2 / TLR4相互作用在巨噬细胞信号转导中的重要性,我们确定了无论有无皮肤反应性PPD的志愿者,TLR2和TLR4基因的多态性以及TLR2的巨噬细胞表达。我们观察到结核菌素阳性志愿者与结核菌素阴性志愿者的粘附单核细胞CD14密度有细微但显着的降低。但是,我们发现使用抗CD14 mAb偶联磁珠后,富含CD14 +细胞的单核细胞CD14密度没有差异。在用PPD和LPS刺激的巨噬细胞上观察到CD14密度的显着增加,而在活的BCG细菌刺激下却没有。但是,无论是否患有PPD皮肤反应的志愿者,这种增加以及可溶性sCD14的血清水平相似。因此,我们对在接种了BCG的受试者中CD14在结核菌素DTH产生中的作用的建议应该进一步探讨。最重要的CD14协同受体是Toll样受体(TLR),可激活核因子以产生炎性细胞因子。但是,我们看不到TLR4(Asp299Gly和Thr399Ile)和TLR2基因(Arg753Gln和Arg677Trp)的多态性与皮肤对PPD的反应之间没有关联。同样,结核菌素阴性和结核菌素阳性志愿者的单核细胞TLR2密度相似。

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