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Comparative Evolutionary Patterns of Burkholderia cenocepacia and B. multivorans During Chronic Co-infection of a Cystic Fibrosis Patient Lung

机译:Burkholderia Cenocepacia和B.多转移症期间的比较进化模式在慢性纤维化患者肺部慢性相关过程中

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摘要

During chronic respiratory infections of cystic fibrosis (CF) patients, bacteria adaptively evolve in response to the nutritional and immune environment as well as influence other infecting microbes. The present study was designed to gain insights into the genetic mechanisms underlying adaptation and diversification by the two most prevalent pathogenic species of the Burkholderia cepacia complex (Bcc), B. cenocepacia and B. multivorans. Herein, we study the evolution of both of these species during coinfection of a CF patient for 4.4 years using genome sequences of 9 B. multivorans and 11 B. cenocepacia. This co-infection spanned at least 3 years following initial infection by B. multivorans and ultimately ended in the patient’s death by cepacia syndrome. Both species acquired several mutations with accumulation rates of 2.08 (B. cenocepacia) and 2.27 (B. multivorans) SNPs/year. Many of the mutated genes are associated with oxidative stress response, transition metal metabolism, defense mechanisms against antibiotics, and other metabolic alterations consistent with the idea that positive selection might be driven by the action of the host immune system, antibiotic therapy and low oxygen and iron concentrations. Two orthologous genes shared by B. cenocepacia and B. multivorans were found to be under strong selection and accumulated mutations associated with lineage diversification. One gene encodes a nucleotide sugar dehydratase involved in lipopolysaccharide O-antigen (OAg) biosynthesis (wbiI). The other gene encodes a putative two-component regulatory sensor kinase protein required to sense and adapt to oxidative- and heavy metal- inducing stresses. This study contributes to understanding of shared and species-specific evolutionary patterns of B. cenocepacia and B. multivorans evolving in the same CF lung environment.
机译:在患囊性纤维化(CF)患者的慢性呼吸道感染期间,细菌以响应营养和免疫环境而自适应地发展,以及影响其他感染微生物。本研究旨在深入了解缅因力术(BCC),B. Cenocepacia和B. Multivorans的两种最普遍的致病性物种潜在的适应和多样化的遗传机制。在此,我们在CF患者的辛凝聚期间使用9 b.多转移率和11b.Cenocepacia的基因组序列进行44年的CF患者在CF患者的患者中进行44岁的进化。这种共同感染在B. Multivorans初始感染后至少3年,最终在患者通过Cepacia综合征死亡。两种物种在累积率为2.08(B. cenocepacia)和2.27(B. Multivorans)SNP /年的几种突变。许多突变基因与氧化应激反应,过渡金属代谢,对抗抗生素的防御机制以及与阳性选择的思想符合的其他代谢改变,抗生素治疗和低氧气和低氧气的作用一致铁浓度。 B. Cenocepacia和B.共用的两种正交基因被发现是与谱系多样化相关的强烈选择和积累的突变。一种基因编码参与脂多糖O-抗原(OAG)生物合成(WBII)的核苷酸糖脱水酶。另一个基因编码了一种推定的双组分调节传感器激酶蛋白,需要感测和适应氧化和重金属诱导的应力。该研究有助于了解B. cenocepacia和B.的特异性进化模式和在同一CF肺环境中发展的多转韦尔斯的特异性进化模式。

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