Six different secretory proteins of molecular weights (15, 26, 30, 41, 55 and 70 kDa) were isolated from 8-day-old culture filtrate of Mycobacterium tuberculosis H37Ra using different column chromatography techniques. These proteins were further examined for their ability to induce cell mediated (T-cell proliferation assay) and humoral immune response (ELISA) in mice immunized with total culture filtrate proteins. Out of six proteins, three proteins showed good reactivity. However, the activity was at a maximum with 30 kDa antigen. The immune response induced by 30 kDa antigen emulsified in Freund's incomplete adjuvant (FIA) was investigated and was found to be dose dependent. The T-cell response induced by this protein was skewed towards T-helper (Th1) cells as determined by the pronounced secretion of interleukin-2 (IL-2) and gamma-interferon (IFN-gamma). The protective activity of the 30 kDa protein was also evaluated and compared with reference to Bacillus Calmette Guerin (BCG) vaccine in the mice challenged with virulent M. tuberculosis H37Rv. The degree of protection afforded by the 30 kDa antigen on the basis of mortality and the significant decrease in c.f.u.'s recovered from different organs (lung, liver, spleen) after 30 days of challenge with LD50 of M. tuberculosis H37Rv was significantly higher in comparison to BCG vaccinated animals. However, the degree of immunity induced by this antigen decreased with time (when challenged 8 and 12 weeks post-immunization) but it was still comparable with BCG. These findings suggest that 30 kDa secretory protein of M. tuberculosis is the key immunoprotective antigen and may be a suitable candidate for the development of an alternative subunit vaccine against tuberculosis.

译文

使用不同的柱色谱技术从8天大的结核分枝杆菌H37Ra培养滤液中分离出六种分子量不同的分泌蛋白 (15、26、30、41、55和70 kDa)。进一步检查了这些蛋白质在用总培养滤液蛋白免疫的小鼠中诱导细胞介导的 (T细胞增殖测定) 和体液免疫反应 (ELISA) 的能力。在六种蛋白质中,三种蛋白质显示出良好的反应性。然而,30 kDa抗原的活性最大。研究了在弗氏不完全佐剂 (FIA) 中乳化的30 kDa抗原诱导的免疫反应,并发现其具有剂量依赖性。由该蛋白诱导的T细胞反应向T辅助 (Th1) 细胞倾斜,这是由interleukin-2 (IL-2) 和 γ-干扰素 (IFN-γ) 的明显分泌决定的。还评估了30 kDa蛋白的保护活性,并将其与卡介苗 (BCG) 疫苗进行了比较,该疫苗在用强毒力结核分枝杆菌H37Rv攻击的小鼠中进行了比较。30 kDa抗原在死亡率的基础上提供的保护程度,以及在用结核分枝杆菌H37Rv的LD50攻击30天后从不同器官 (肺,肝,脾) 恢复的c.f.u.的显着降低与BCG接种的动物相比更高。然而,该抗原诱导的免疫程度随时间而降低 (预防接种后8周和12周受到攻击时),但仍与BCG相当。这些发现表明,结核分枝杆菌的30 kDa分泌蛋白是关键的免疫保护性抗原,并且可能是开发针对结核病的替代亚单位疫苗的合适候选者。

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