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Roles of B739_1343 in iron acquisition and pathogenesis in Riemerella anatipestifer CH-1 and evaluation of the RA-CH-1ΔB739_1343 mutant as an attenuated vaccine

机译:B739_1343在厌食耶氏杆菌CH-1中铁的获取和发病中的作用以及作为减毒疫苗的RA-CH-1ΔB739_1343突变体的评估

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摘要

Iron is one of the most important elements for bacterial survival and pathogenicity. The iron uptake mechanism of Riemerella anatipestifer (R. anatipestifer, RA), a major pathogen that causes septicemia and polyserositis in ducks, is largely unknown. Here, the functions of the putative TonB-dependent iron transporter of RA-CH-1, B739_1343, in iron utilization and pathogenicity were investigated. Under iron-starved conditions, the mutant strain RA-CH-1ΔB739_1343 exhibited more seriously impaired growth than the wild-type strain RA-CH-1, and the expression of B739_1343 in the mutant strain restored growth. qRT-PCR results showed that the transcription of B739_1343 was not regulated by iron conditions. In an animal model, the median lethal dose (LD50) of the mutant strain RA-CH-1ΔB739_1343 increased more than 104-fold (1.6×1012 CFU) compared to that of the wild-type strain RA-CH-1 (1.43×108 CFU). In a duck co-infection model, the mutant strain RA-CH-1ΔB739_1343 was outcompeted by the wild-type RA-CH-1 in the blood, liver and brain of infected ducks, indicating that B739_1343 is a virulence factor of RA-CH-1. Finally, immunization with live bacteria of the mutant strain RA-CH-1ΔB739_1343 protected 83.33% of ducks against a high-dose (100-fold LD50) challenge with the wild-type strain RA-CH-1, suggesting that the mutant strain RA-CH-1ΔB739_1343 could be further developed as a potential live attenuated vaccine candidate for the duck industry.
机译:铁是细菌存活和致病性的最重要元素之一。引起鸭鸭败血症和多发性浆膜炎的主要病原体-厌食里氏杆菌(R. anatipestifer,RA)的铁吸收机制在很大程度上尚不清楚。在此,研究了RA-CH-1的TonB依赖性铁转运蛋白B739_1343在铁利用和致病性方面的功能。在铁饥饿的条件下,突变菌株RA-CH-1ΔB739_1343的生长比野生型菌株RA-CH-1严重受损,并且突变菌株中B739_1343的表达恢复了生长。 qRT-PCR结果表明,B739_1343的转录不受铁条件的调节。在动物模型中,突变株RA-CH-1ΔB739_1343的平均致死剂量(LD50)增加了10 4 倍(1.6×10 12 CFU)与野生型RA-CH-1菌株(1.43×10 8 CFU)相似。在鸭共感染模型中,突变株RA-CH-1ΔB739_1343在感染的鸭的血液,肝和脑中被野生型RA-CH-1竞争,表明B739_1343是RA-CH的毒力因子-1。最后,用突变菌株RA-CH-1ΔB739_1343的活细菌进行免疫可以保护83.33%的鸭子免受野生型菌株RA-CH-1的高剂量(100倍LD50)攻击,这表明突变菌株RA -CH-1ΔB739_1343可以进一步发展为鸭业的潜在减毒活疫苗。

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