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采用差异蛋白质组学方法鉴定巨噬细胞感染早期呈现的结核分枝杆菌假定保护性抗原,并将其评估为DNA疫苗。

Differential proteomics approach to identify putative protective antigens of Mycobacterium tuberculosis presented during early stages of macrophage infection and their evaluation as DNA vaccines.

作者信息

Sharma Shingar, Rajmani R S, Kumar Arun, Bhaskar Ashima, Singh Amit, Manivel Venkatasamy, Tyagi Anil K, Rao Kanury V S

出版信息

Indian J Exp Biol. 2015 Jul;53(7):429-39.

Abstract

Unsatisfactory performance of the existing BCG vaccines, especially against the adult pulmonary disease, has urged the need for an effective vaccine against tuberculosis (TB). In this study, we employed differential proteomics to obtain a list of antigens as potential vaccine candidates. Bacterial epitopes being presented at early stages on MHC class I and class II molecules of macrophages infected with Mycobacterium tuberculosis (M. tb) were identified using iTRAQ labelling and reverse phase LC-MS/MS. The putative vaccine candidates, thus identified, were tested as plasmid DNA vaccines in mice to ascertain their protective efficacy against the aerosolized M. tb challenge, based on their ability to reduce the bacterial load in the lungs of infected mice. Here, we observed that 4 out of the 17 selected antigens imparted significant protection against the challenge of M. tb. The four shortlisted antigens were further assessed in a more stringent guinea pig model, where too, they demonstrated.significant protection. It concludes that combining a proteomics approach with the in vivo assessment of vaccine candidates in animal models can be valuable in identifying new potential candidates to expand the antigenic repertoire for novel vaccines against TB.

摘要

现有卡介苗(BCG)疫苗的效果不尽人意,尤其是在预防成人肺结核方面,这促使人们需要一种有效的抗结核疫苗。在本研究中,我们采用差异蛋白质组学来获取一系列作为潜在疫苗候选物的抗原。利用iTRAQ标记和反相液相色谱-串联质谱法(LC-MS/MS),鉴定了在感染结核分枝杆菌(M. tb)的巨噬细胞的MHC I类和II类分子上早期呈现的细菌表位。如此鉴定出的假定疫苗候选物,作为质粒DNA疫苗在小鼠中进行测试,以根据它们降低感染小鼠肺部细菌载量的能力,确定其对雾化M. tb攻击的保护效力。在此,我们观察到,17种选定的抗原中有4种对M. tb攻击具有显著的保护作用。这4种入围抗原在更严格的豚鼠模型中进一步评估,在该模型中它们也表现出显著的保护作用。研究得出结论,将蛋白质组学方法与在动物模型中对疫苗候选物进行体内评估相结合,对于识别新的潜在候选物以扩大新型抗结核疫苗的抗原库可能具有重要价值。

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