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The Effects of Modeled Microgravity on Growth Kinetics Antibiotic Susceptibility Cold Growth and the Virulence Potential of a Yersinia pestis ymoA-Deficient Mutant and Its Isogenic Parental Strain

机译:模拟微重力对鼠疫耶尔森氏菌ymoA缺陷型突变体及其同基因亲本菌株生长动力学抗生素敏感性冷生长和毒力的影响

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摘要

Previously, we reported that there was no enhancement in the virulence potential (as measured by cell culture infections) of the bacterial pathogen Yersinia pestis (YP) following modeled microgravity/clinorotation growth. We have now further characterized the effects of clinorotation (CR) on YP growth kinetics, antibiotic sensitivity, cold growth, and YP's virulence potential in a murine model of infection. Surprisingly, none of the aforementioned phenotypes were altered. To better understand why CR did not enhance YP's virulence potential as it did for other bacterial pathogens, a YP ΔymoA isogenic mutant in the KIM/D27 background strain that is unable to produce the histone-like YmoA protein and influences DNA topography was used in both cell culture and murine models of infection. YmoA represses type three secretion system (T3SS) virulence gene expression in the yersiniae. Similar to our CR-grown parental YP strain data, the CR-grown ΔymoA mutant induced reduced HeLa cell cytotoxicity with concomitantly decreased Yersinia outer protein E (YopE) and low calcium response V (LcrV) antigen production and secretion. Important, however, were our findings that, although no significant differences were observed in survival of mice infected intraperitoneally with either normal gravity (NG)- or CR-grown parental YP, the ΔymoA mutant induced significantly more mortality in infected mice than did the parental strain following CR growth. Taken together, our data demonstrate that CR did enhance the virulence potential of the YP ΔymoA mutant in a murine infection model (relative to the CR-grown parental strain), despite inducing less HeLa cell rounding in our cell culture infection assay due to reduced T3SS activity. Therefore, CR, which induces a unique type of bacterial stress, might be enhancing YP's virulence potential in vivo through a T3SS-independent mechanism when the histone-like YmoA protein is absent. Key Words: Type three secretion system (T3SS)—Low-shear modeled microgravity—High-aspect ratio vessel—Cell culture infection models—Mouse infection model. Astrobiology 13, 821–832.
机译:以前,我们报道了在模拟微重力/倾斜旋转生长之后,细菌病原体鼠疫耶尔森菌(YP)的致病力(通过细胞培养感染来衡量)没有增强。现在,我们进一步表征了在小鼠感染模型中,旋转旋转(CR)对YP生长动力学,抗生素敏感性,寒冷生长和YP毒力潜能的影响。令人惊讶的是,上述表型均未改变。为了更好地理解为什么CR不能像其他细菌病原体那样增强YP的毒力潜力,在这两种方法中都使用了KIM / D27背景菌株中的YPΔymoA等基因突变体,该突变体无法产生组蛋白样YmoA蛋白并影响DNA形貌。细胞培养和小鼠感染模型。 YmoA抑制耶尔森氏菌中的三型分泌系统(T3SS)毒力基因表达。与我们的CR生长的父母YP菌株数据相似,CR生长的ΔymoA突变体诱导的HeLa细胞杀伤力降低,同时耶尔森氏菌外蛋白E(YopE)和钙反应低(LcrV)抗原产生和分泌降低。然而,重要的是我们的发现,尽管在正常重力(NG)或CR生长的亲本YP腹膜内感染的小鼠的存活率中未观察到显着差异,但ΔymoA突变体在感染小鼠中的致死率明显高于亲本CR生长后的菌株。两者合计,我们的数据表明,尽管由于T3SS降低,在我们的细胞培养感染试验中诱导的HeLa细胞变圆较少,但CR确实增强了小鼠感染模型(相对于CR生长的亲本菌株)中YPΔymoA突变体的毒力潜能。活动。因此,当缺乏组蛋白样的YmoA蛋白时,诱导细菌压力的独特类型的CR可能通过T3SS独立机制增强体内YP的毒力潜力。关键词:三型分泌系统(T3SS)-低剪切微重力-高纵横比血管-细胞培养感染模型-小鼠感染模型。天体生物学13,821–832。

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