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Expression of recombinant HBD3 protein that reduces Mycobacterial infection capacity

机译:降低分枝杆菌感染能力的重组HBD3蛋白的表达

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摘要

Bovine tuberculosis is a disease caused by Mycobacterium bovis ( M. bovis ) that leads to great economic losses in cattle production. The discovery of a reasonable bioagent to reduce M. bovis infection risk and environment contamination becomes significant and urgent. Previous study reported that human β-defensin-3 (HBD3) participated in Mycobacterial immunity and was recognized as a suitable candidate reagent. However, its minimal inhibitory concentration to M. bovis is not yet reported. In this study, we first purified HBD3 protein by recombinant-DNA technology and prokaryotic expression system. Subsequently, anti-bacterial tests were used to evaluate the basic bioactivity of the protein. Results revealed that recombinant HBD3 (rHBD3) protein inhibits Staphylococcus multiplication but not the host Escherichia coli . The growth curve of M. bovis showed that rHBD3 protein controls the proliferation of M. bovis in 20?μg/ml concentration. In addition, rHBD3 protein-incubated M. bovis exhibited reduced infectivity to alveolar epithelial cells and macrophages. In conclusion, the expression of rHBD3 protein is a potential ideal bio-regent for reducing M. bovis infection.
机译:牛结核病是由牛分枝杆菌(牛分枝杆菌)引起的疾病,导致牛生产中的巨大经济损失。寻找降低牛分枝杆菌感染风险和环境污染的合理生物制剂变得重要而紧迫。先前的研究报道,人β-防御素3(HBD3)参与了分枝杆菌免疫,被认为是合适的候选试剂。然而,尚未报道其对牛分枝杆菌的最小抑制浓度。在这项研究中,我们首先通过重组DNA技术和原核表达系统纯化了HBD3蛋白。随后,使用抗菌测试评估该蛋白的基本生物活性。结果显示重组HBD3(rHBD3)蛋白抑制葡萄球菌繁殖,但不能抑制宿主大肠杆菌。牛分枝杆菌的生长曲线表明,rHBD3蛋白以20?μg/ ml的浓度控制牛分枝杆菌的增殖。此外,rHBD3蛋白孵育的牛分枝杆菌对肺泡上皮细胞和巨噬细胞的感染力降低。总之,rHBD3蛋白的表达是减少牛分枝杆菌感染的潜在理想生物试剂。

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