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Genomic Expression Analysis Reveals Strategies of Burkholderia cenocepacia to Adapt to Cystic Fibrosis Patients' Airways and Antimicrobial Therapy

机译:基因组表达分析揭示了伯克霍尔德氏菌的策略,以适应囊性纤维化患者的气道和抗菌疗法

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摘要

Pulmonary colonization of cystic fibrosis (CF) patients with Burkholderia cenocepacia or other bacteria of the Burkholderia cepacia complex (Bcc) is associated with worse prognosis and increased risk of death. During colonization, the bacteria may evolve under the stressing selection pressures exerted in the CF lung, in particular, those resulting from challenges of the host immune defenses, antimicrobial therapy, nutrient availability and oxygen limitation. Understanding the adaptive mechanisms that promote successful colonization and long-term survival of B. cenocepacia in the CF lung is essential for an improved therapeutic outcome of chronic infections. To get mechanistic insights into these adaptive strategies a transcriptomic analysis, based on DNA microarrays, was explored in this study. The genomic expression levels in two clonal variants isolated during long-term colonization of a CF patient who died from the cepacia syndrome were compared. One of the isolates examined, IST439, is the first B. cenocepacia isolate retrieved from the patient and the other isolate, IST4113, was obtained three years later and is more resistant to different classes of antimicrobials. Approximately 1000 genes were found to be differently expressed in the two clonal variants reflecting a marked reprogramming of genomic expression. The up-regulated genes in IST4113 include those involved in translation, iron uptake (in particular, in ornibactin biosynthesis), efflux of drugs and in adhesion to epithelial lung tissue and to mucin. Alterations related with adaptation to the nutritional environment of the CF lung and to an oxygen-limited environment are also suggested to be a key feature of transcriptional reprogramming occurring during long-term colonization, antibiotic therapy and the progression of the disease.
机译:合并伯克霍尔德菌和其他伯克霍尔德菌复合体(Bcc)细菌的囊性纤维化(CF)患者的肺部定植与预后不良和死亡风险增加相关。在定殖过程中,细菌可能会在施加于CF肺的压力下(特别是宿主免疫防御,抗微生物治疗,养分利用率和氧气限制等挑战所产生的选择压力)下进化。了解促进CF肺中新细菌双歧杆菌成功定植和长期存活的适应性机制对于改善慢性感染的治疗效果至关重要。为了获得对这些适应性策略的机械学见解,本研究探索了基于DNA微阵列的转录组分析。比较了由cepacia综合征死亡的CF患者长期定居期间分离出的两个克隆变异体中的基因组表达水平。被检查的一种分离株IST439是从患者体内回收的首个葡萄球菌,另一种分离株IST4113则是在三年后获得的,并且对不同种类的抗菌药更具抵抗力。发现在两个克隆变体中大约有1000个基因表达不同,这反映了基因组表达的明显重编程。 IST4113中的上调基因包括那些参与翻译,铁摄取(特别是在鸟氨酸生物合成中),药物外流以及与上皮肺组织和粘蛋白的黏附的基因。与适应CF肺的营养环境和氧气受限环境有关的改变也被认为是在长期定居,抗生素治疗和疾病进展过程中发生的转录重编程的关键特征。

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