Center for Pharmaceutical Biotechnology, Department of Medicinal Chemistry and Pharmacognosy, College of Pharmacy, University of Illinois at Chicago, Chicago, Illinois, USA.
mBio. 2013 Jul 23;4(4):e00382-13. doi: 10.1128/mBio.00382-13.
Quorum sensing (QS) regulates diverse and coordinated behaviors in bacteria, including the production of virulence factors, biofilm formation, sporulation, and competence development. It is now established that some streptococci utilize Rgg-type proteins in concert with short hydrophobic peptides (SHPs) to mediate QS, and sequence analysis reveals that several streptococcal species contain highly homologous Rgg/SHP pairs. In group A streptococcus (GAS), two SHPs (SHP2 and SHP3 [SHP2/3]) were previously identified to be important in GAS biofilm formation. SHP2/3 are detected by two antagonistic regulators, Rgg2 and Rgg3, which control expression of the shp genes. In group B streptococcus (GBS), RovS is a known virulence gene regulator and ortholog of Rgg2, whereas no apparent Rgg3 homolog exists. Adjacent to rovS is a gene (shp1520) encoding a peptide nearly identical to SHP2. Using isogenic mutant strains and transcriptional reporters, we confirmed that RovS/SHP1520 comprise a QS circuit in GBS. More important, we performed experiments demonstrating that production and secretion of SHP1520 by GBS can modulate Rgg2/3-regulated gene expression in GAS in trans; likewise, SHP2/3 production by GAS can stimulate RovS-mediated gene regulation in GBS. An isolate of Streptococcus dysgalactiae subsp. equisimilis also produced a secreted factor capable of simulating the QS circuits of both GAS and GBS, and sequencing confirms the presence of an orthologous Rgg2/SHP2 pair in this species as well. To our knowledge, this is the first documented case of bidirectional signaling between streptococcal species in coculture and suggests a role for orthologous Rgg/SHP systems in interspecies communication between important human pathogens.
Pathogenic streptococci, such as group A (GAS) and group B (GBS) streptococcus, are able to persist in the human body without causing disease but become pathogenic under certain conditions that are not fully characterized. Environmental cues and interspecies signaling between members of the human flora likely play an important role in the transition to a disease state. Since quorum-sensing (QS) peptides have been consistently shown to regulate virulence factor production in pathogenic species, the ability of bacteria to signal via these peptides may prove to be an important link between the carrier and pathogenic states. Here we provide evidence of a bidirectional QS system between GAS, GBS, and Streptococcus dysgalactiae subsp. equisimilis, demonstrating the possibility of evolved communication systems between human pathogens.
群体感应 (QS) 调节细菌的多种协调行为,包括毒力因子的产生、生物膜形成、孢子形成和感受态发育。现已确定,一些链球菌利用 Rgg 型蛋白与短疏水性肽 (SHP) 协同作用来介导 QS,序列分析表明,几种链球菌种含有高度同源的 Rgg/SHP 对。在 A 组链球菌 (GAS) 中,先前已鉴定出两种 SHP (SHP2 和 SHP3 [SHP2/3]) 对 GAS 生物膜形成很重要。SHP2/3 由两个拮抗调节因子 Rgg2 和 Rgg3 检测,它们控制 shp 基因的表达。在 B 组链球菌 (GBS) 中,RovS 是一种已知的毒力基因调节剂,是 Rgg2 的同源物,而没有明显的 Rgg3 同源物。RovS 旁边是一个编码与 SHP2 几乎相同肽的基因 (shp1520)。使用基因相同的突变株和转录报告基因,我们证实 RovS/SHP1520 构成了 GBS 中的 QS 回路。更重要的是,我们进行的实验表明,GBS 产生和分泌 SHP1520 可以在转导中调节 GAS 中由 Rgg2/3 调节的基因表达;同样,GAS 产生的 SHP2/3 可以刺激 GBS 中 RovS 介导的基因调节。缓症链球菌亚种 equisimilis 的分离株也产生了一种可模拟 GAS 和 GBS 的 QS 回路的分泌因子,测序证实该物种中也存在同源 Rgg2/SHP2 对。据我们所知,这是首次记录到在共培养物中链球菌种之间的双向信号传递,并且表明同源 Rgg/SHP 系统在重要人类病原体之间的种间通信中起作用。
致病性链球菌,如 A 组 (GAS) 和 B 组 (GBS) 链球菌,能够在不引起疾病的情况下在人体内持续存在,但在某些尚未完全确定的条件下会变得致病。环境线索和人类菌群成员之间的种间信号传递可能在向疾病状态的转变中发挥重要作用。由于群体感应 (QS) 肽已被一致证明可调节致病性物种中毒力因子的产生,因此细菌通过这些肽进行信号传递的能力可能是携带者和致病性状态之间的重要联系。在这里,我们提供了 GAS、GBS 和缓症链球菌亚种 equisimilis 之间双向 QS 系统的证据,证明了人类病原体之间可能存在进化的通信系统。
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