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肺炎链球菌在严重侵袭性疾病表现中的生长特征差异。

Differential Pneumococcal Growth Features in Severe Invasive Disease Manifestations.

机构信息

Laboratory of Medical Immunology, Radboud Institute of Molecular Life Sciences, Radboudumc Center for Infectious Diseases, Radboudumc, Nijmegen, The Netherlands.

TenWise BV, Leiden, The Netherlands.

出版信息

Microbiol Spectr. 2022 Jun 29;10(3):e0005022. doi: 10.1128/spectrum.00050-22. Epub 2022 Jun 9.

Abstract

The nasopharyngeal commensal Streptococcus pneumoniae can become invasive and cause metastatic infection. This requires the pneumococcus to have the ability to adapt, grow, and reside in diverse host environments. Therefore, we studied whether the likelihood of severe disease manifestations was related to pneumococcal growth kinetics. For 383 S. pneumoniae blood isolates and 25 experimental mutants, we observed highly reproducible growth curves in nutrient-rich medium. The derived growth features were lag time, maximum growth rate, maximum density, and stationary-phase time before lysis. First, the pathogenicity of each growth feature was probed by comparing isolates from patients with and without marked preexisting comorbidity. Then, growth features were related to the propensity of causing severe manifestations of invasive pneumococcal disease (IPD). A high maximum bacterial density was the most pronounced pathogenic growth feature, which was also an independent predictor of 30-day mortality ( = 0.03). Serotypes with an epidemiologically higher propensity for causing meningitis displayed a relatively high maximum density ( < 0.005) and a short stationary phase ( < 0.005). Correspondingly, isolates from patients diagnosed with meningitis showed an especially high maximum density and short stationary phase compared to isolates from the same serotype that had caused uncomplicated bacteremic pneumonia. In contrast, empyema-associated strains were characterized by a relatively long lag phase ( < 0.0005), and slower growth ( < 0.005). The course and dissemination of IPD may partly be attributable to the pneumococcal growth features involved. If confirmed, we should tailor the prevention and treatment strategies for the different infection sites that can complicate IPD. Streptococcus pneumoniae is a leading infectious cause of deaths worldwide. To understand the course and outcome of pneumococcal infection, most research has focused on the host and its response to contain bacterial growth. However, bacterial epidemiology suggest that certain pneumococcal serotypes are particularly prone to causing complicated infections. Therefore, we took the bacterial point of view, simply examining growth features for hundreds of pneumococcal blood isolates. Their growth curves were very reproducible. Certain poles of pneumococcal growth features were indeed associated with specific clinical manifestations like meningitis or pleural empyema. This indicates that bacterial growth style potentially affects the progression of infection. Further research on bacterial growth and adaptation to different host environments may therefore provide key insight into pathogenesis of complicated invasive disease. Such knowledge could lead to more tailored vaccine targets or therapeutic approaches to reduce the million deaths that are caused by pneumococcal disease every year.

摘要

鼻咽共生肺炎链球菌可侵袭并引起转移性感染。这要求肺炎链球菌具有适应、生长和驻留在不同宿主环境中的能力。因此,我们研究了严重疾病表现的可能性是否与肺炎链球菌的生长动力学有关。对于 383 株肺炎链球菌血培养分离株和 25 株实验突变株,我们在富含营养的培养基中观察到高度可重复的生长曲线。衍生的生长特征包括潜伏期、最大生长速率、最大密度和裂解前的静止期时间。首先,通过比较来自有和没有明显预先存在合并症的患者的分离株,探究每种生长特征的致病性。然后,将生长特征与侵袭性肺炎链球菌病(IPD)引起严重表现的倾向相关联。高最大细菌密度是最显著的致病性生长特征,也是 30 天死亡率的独立预测因子(=0.03)。在流行病学上更容易引起脑膜炎的血清型显示出相对较高的最大密度(<0.005)和较短的静止期(<0.005)。相应地,与同一血清型引起单纯菌血症性肺炎的分离株相比,从诊断为脑膜炎的患者中分离出的分离株显示出特别高的最大密度和较短的静止期。相比之下,与 empyema 相关的菌株的特点是潜伏期相对较长(<0.0005),生长速度较慢(<0.005)。IPD 的病程和传播部分可能归因于所涉及的肺炎链球菌生长特征。如果得到证实,我们应该针对可能使 IPD 复杂化的不同感染部位调整预防和治疗策略。

肺炎链球菌是全球死亡的主要感染原因。为了了解肺炎链球菌感染的过程和结果,大多数研究都集中在宿主及其对控制细菌生长的反应上。然而,细菌流行病学表明,某些肺炎链球菌血清型特别容易引起复杂感染。因此,我们从细菌的角度出发,简单地检查了数百株肺炎链球菌血培养分离株的生长特征。它们的生长曲线非常可重复。肺炎链球菌生长特征的某些极点确实与特定的临床表现(如脑膜炎或胸腔积脓)有关。这表明细菌生长方式可能会影响感染的进展。因此,进一步研究细菌生长及其对不同宿主环境的适应能力,可能会为复杂侵袭性疾病的发病机制提供关键的见解。这种知识可以导致更有针对性的疫苗靶点或治疗方法,以减少每年由肺炎球菌病引起的百万人死亡。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a0d5/9241771/62364541faf9/spectrum.00050-22-f001.jpg

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