首页> 外文OA文献 >Screening of Streptococcus pneumoniae ABC Transporter Mutants Demonstrates that LivJHMGF, a Branched-Chain Amino Acid ABC Transporter, Is Necessary for Disease Pathogenesis▿
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Screening of Streptococcus pneumoniae ABC Transporter Mutants Demonstrates that LivJHMGF, a Branched-Chain Amino Acid ABC Transporter, Is Necessary for Disease Pathogenesis▿

机译:肺炎链球菌ABC转运蛋白突变体的筛选表明,支链氨基酸ABC转运蛋白LivJHMGF是疾病发病的必要条件▿

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摘要

Bacterial ABC transporters are an important class of transmembrane transporters that have a wide variety of substrates and are important for the virulence of several bacterial pathogens, including Streptococcus pneumoniae. However, many S. pneumoniae ABC transporters have yet to be investigated for their role in virulence. Using insertional duplication mutagenesis mutants, we investigated the effects on virulence and in vitro growth of disruption of 9 S. pneumoniae ABC transporters. Several were partially attenuated in virulence compared to the wild-type parental strain in mouse models of infection. For one ABC transporter, required for full virulence and termed LivJHMGF due to its similarity to branched-chain amino acid (BCAA) transporters, a deletion mutant (ΔlivHMGF) was constructed to investigate its phenotype in more detail. When tested by competitive infection, the ΔlivHMGF strain had reduced virulence in models of both pneumonia and septicemia but was fully virulent when tested using noncompetitive experiments. The ΔlivHMGF strain had no detectable growth defect in defined or complete laboratory media. Recombinant LivJ, the substrate binding component of the LivJHMGF, was shown by both radioactive binding experiments and tryptophan fluorescence spectroscopy to specifically bind to leucine, isoleucine, and valine, confirming that the LivJHMGF substrates are BCAAs. These data demonstrate a previously unsuspected role for BCAA transport during infection for S. pneumoniae and provide more evidence that functioning ABC transporters are required for the full virulence of bacterial pathogens.
机译:细菌ABC转运蛋白是一类重要的跨膜转运蛋白,其底物种类繁多,对几种细菌性病原体(包括肺炎链球菌)的毒力也很重要。但是,许多肺炎链球菌ABC转运蛋白的毒力作用尚待研究。使用插入重复诱变突变体,我们调查了9肺炎链球菌ABC转运蛋白对毒力和体外生长的影响。与野生型亲本菌株相比,在小鼠感染模型中,有几种毒株的毒力部分减弱。对于一个完全毒力所需的ABC转运蛋白,由于其与支链氨基酸(BCAA)转运蛋白的相似性而被称为LivJHMGF,构建了一个缺失突变体(ΔlivHMGF),以更详细地研究其表型。当通过竞争性感染进行测试时,ΔlivHMGF菌株在肺炎和败血病模型中均降低了毒力,但在使用非竞争性实验进行测试时具有完全毒性。 ΔlivHMGF菌株在确定的或完全的实验室培养基中没有可检测到的生长缺陷。放射性结合实验和色氨酸荧光光谱法均显示重组LivJ是LivJHMGF的底物结合成分,可特异性结合亮氨酸,异亮氨酸和缬氨酸,从而证实LivJHMGF底物是BCAAs。这些数据证明了肺炎链球菌感染期间BCAA转运的先前未曾预料到的作用,并提供了更多证据表明功能性ABC转运蛋白对于细菌病原体的完全毒力是必需的。

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