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鉴定 CovS 失活对无荚膜 A 组链球菌转录组的不同影响。

Identification of distinct impacts of CovS inactivation on the transcriptome of acapsular group A streptococci.

机构信息

Department of Infectious Diseases Infection Control and Employee Health, University of Texas MD Anderson Cancer Center , Houston, Texas, USA.

Division of Infectious Diseases and Department of Pediatrics, McGovern Medical School at UTHealth Houston and Children's Memorial Hermann Hospital , Houston, Texas, USA.

出版信息

mSystems. 2023 Aug 31;8(4):e0022723. doi: 10.1128/msystems.00227-23. Epub 2023 Jun 26.

Abstract

Group A streptococcal (GAS) strains causing severe, invasive infections often have mutations in the control of virulence two-component regulatory system (CovRS) which represses capsule production, and high-level capsule production is considered critical to the GAS hypervirulent phenotype. Additionally, based on studies in GAS, hyperencapsulation is thought to limit transmission of CovRS-mutated strains by reducing GAS adherence to mucosal surfaces. It has recently been identified that about 30% of invasive GAS strains lacks capsule, but there are limited data regarding the impact of CovS inactivation in such acapsular strains. Using publicly available complete genomes ( = 2,455) of invasive GAS strains, we identified similar rates of CovRS inactivation and limited evidence for transmission of CovRS-mutated isolates for both encapsulated and acapsular types. Relative to encapsulated GAS, CovS transcriptomes of the prevalent acapsular types , , and revealed unique impacts such as increased transcript levels of genes in the /mga region along with decreased transcript levels of pilus operon-encoding genes and the streptokinase-encoding gene . CovS inactivation in and strains, but not , increased GAS survival in human blood. Moreover, CovS inactivation in acapsular GAS reduced adherence to host epithelial cells. These data suggest that the hypervirulence induced by CovS inactivation in acapsular GAS follows distinct pathways from the better studied encapsulated strains and that factors other than hyperencapsulation may account for the lack of transmission of CovRS-mutated strains. IMPORTANCE Devastating infections due to group A streptococci (GAS) tend to occur sporadically and are often caused by strains that contain mutations in the control of virulence regulatory system (CovRS). In well-studied GAS, the increased production of capsule induced by CovRS mutation is considered key to both hypervirulence and limited transmissibility by interfering with proteins that mediate attachment to eukaryotic cells. Herein, we show that the rates of covRS mutations and genetic clustering of CovRS-mutated isolates are independent of capsule status. Moreover, we found that CovS inactivation in multiple acapsular GAS types results in dramatically altered transcript levels of a diverse array of cell-surface protein-encoding genes and a unique transcriptome relative to encapsulated GAS. These data provide new insights into how a major human pathogen achieves hypervirulence and indicate that factors other than hyperencapsulation likely account for the sporadic nature of the severe GAS disease.

摘要

A 组链球菌(GAS)菌株引起的严重侵袭性感染通常在控制毒力的双组分调节系统(CovRS)中发生突变,该系统抑制荚膜产生,高水平的荚膜产生被认为是 GAS 超强毒力表型的关键。此外,基于 GAS 的研究,超荚膜化被认为通过减少 GAS 对粘膜表面的粘附来限制 CovRS 突变株的传播。最近已经确定,大约 30%的侵袭性 GAS 菌株缺乏荚膜,但关于这种无荚膜菌株中 CovS 失活的影响的数据有限。使用公开的侵袭性 GAS 菌株完整基因组(=2455),我们发现,对于有荚膜和无荚膜的两种类型,CovRS 失活的相似率以及 CovRS 突变株的有限传播证据。与有荚膜的 GAS 相比,流行的无荚膜 、 和 型 CovS 转录组显示出独特的影响,例如 /mga 区域中基因的转录水平增加,而菌毛操纵子编码基因和链激酶编码基因的转录水平降低。CovS 在 和 株中的失活,但不在 株中,增加了 GAS 在人血中的存活能力。此外,无荚膜 GAS 中的 CovS 失活减少了对宿主上皮细胞的粘附。这些数据表明,CovS 在无荚膜 GAS 中失活引起的超强毒力遵循与研究较好的有荚膜菌株不同的途径,并且除了超荚膜化之外,其他因素可能解释了 CovRS 突变株缺乏传播的原因。

重要性

由 A 组链球菌(GAS)引起的破坏性感染往往是零星发生的,通常是由含有毒力调节系统(CovRS)控制突变的菌株引起的。在研究较好的 GAS 中,CovRS 突变引起的荚膜产量增加被认为是超强毒力和通过干扰介导与真核细胞附着的蛋白质来限制可传播性的关键。在此,我们表明 covRS 突变的比率和 CovRS 突变株的遗传聚类与荚膜状态无关。此外,我们发现,与有荚膜的 GAS 相比,多个无荚膜 GAS 型中的 CovS 失活导致一系列细胞表面蛋白编码基因的转录水平发生显著改变,并具有独特的转录组。这些数据为主要人类病原体如何实现超强毒力提供了新的见解,并表明除了超荚膜化之外,其他因素可能解释了严重 GAS 疾病的偶发性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b4bf/10470059/1e4ac2b94f26/msystems.00227-23.f001.jpg

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