Holley Concerta L, Dhulipala Vijaya, Van Adriana Le, Balthazar Jacqueline T, Oliver Vincent J, Jerse Ann E, Shafer William M
bioRxiv. 2025 Jun 11:2025.06.11.659166. doi: 10.1101/2025.06.11.659166.
The continued emergence of (Ng) isolates resistant to first-line antibiotics has focused efforts on understanding how alternative therapies such as expanded use of gentamicin (Gen) might counteract this global public health problem. Focusing on Gen as a viable alternative antibiotic for treatment of gonorrheal infections, we used RNA-Seq to determine if sub-lethal levels of Gen might impact gonococci on a transcriptional level. We found that sub-lethal Gen levels altered expression of 23 genes in Ng strain FA19. Many of the differentially regulated genes were associated with known stress responses elaborated by Ng under different harmful conditions. We found that the transcripts of the operon, which encodes a putative HicA-HicB toxin-antitoxin system that is encoded by tandem genes with the prophage Ngo φ3, were increased in response to Gen. While loss of did not impact gonococcal susceptibility to a variety of antimicrobial agents or harmful environmental conditions it did reduce biofilm formation in Ng strains F62, FA1090, WHO X and CDC200 but not that of strain FA19. Further, in strain F62, but not FA19, loss of reduced the fitness of Ng during experimental lower genital tract infection of female mice. Further, we found that expression of can influence levels of the transcript, which encodes the nitrate reductase shown previously to be upregulated in gonococcal biofilms. We propose that sub-lethal Gen has the capacity to influence gonococcal pathogenesis through the action of the HicAB toxin-antitoxin system.
During antibiotic treatment bacteria can be exposed to sub-lethal levels that could serve as a stress signal resulting in changes in gene expression. The continued emergence of multi-drug resistant strains of Ng has rekindled interest in expanded use of gentamicin (Gen) for treatment of gonorrheal infections. We report that sub-lethal levels of Gen can influence levels of Ng transcripts including that of the gonococcal -encoded toxin-antitoxin (TA) locus, which is embedded within an integrated prophage, While loss of this TA locus did not impact Ng susceptibility to Gen it reduced the biofilm forming ability of 4/5 Ng strains. Further, in an examined strain in this group we found that Ng fitness during experimental infection was negatively impacted. We propose that that levels of the transcripts can be increased by sub-lethal levels of an antibiotic used in treatment of gonorrhea and that this could influence pathogenicity.
对一线抗生素耐药的淋病奈瑟菌(Ng)菌株不断出现,这促使人们致力于了解诸如扩大庆大霉素(Gen)的使用等替代疗法如何应对这一全球公共卫生问题。以Gen作为治疗淋病感染的一种可行替代抗生素为重点,我们使用RNA测序来确定亚致死水平的Gen是否会在转录水平上影响淋病奈瑟菌。我们发现,亚致死水平的Gen改变了Ng菌株FA19中23个基因的表达。许多差异调节基因与Ng在不同有害条件下阐述的已知应激反应相关。我们发现,编码假定的HicA-HicB毒素-抗毒素系统的操纵子转录本在对Gen的反应中增加,该系统由与噬菌体Ngo φ3串联的基因编码。虽然缺失该操纵子对淋病奈瑟菌对多种抗菌剂或有害环境条件的敏感性没有影响,但它确实降低了Ng菌株F62、FA1090、WHO X和CDC200的生物膜形成能力,而对菌株FA19没有影响。此外,在菌株F62中,而不是FA19中,缺失该操纵子降低了雌性小鼠实验性下生殖道感染期间Ng的适应性。此外,我们发现该操纵子的表达可以影响编码硝酸盐还原酶的转录本水平,该硝酸盐还原酶先前已证明在淋病奈瑟菌生物膜中上调。我们提出,亚致死水平的Gen有能力通过HicAB毒素-抗毒素系统的作用影响淋病奈瑟菌的致病性。
在抗生素治疗期间,细菌可能会暴露于亚致死水平,这可能作为一种应激信号导致基因表达发生变化。Ng多药耐药菌株的不断出现重新激发了人们对扩大使用庆大霉素(Gen)治疗淋病感染的兴趣。我们报告说,亚致死水平的Gen可以影响Ng转录本水平,包括淋病奈瑟菌编码的毒素-抗毒素(TA)位点的转录本水平,该位点嵌入整合噬菌体中。虽然缺失这个TA位点对Ng对Gen的敏感性没有影响,但它降低了5个Ng菌株中4个的生物膜形成能力。此外,在该组中检测的一个菌株中,我们发现实验感染期间Ng的适应性受到负面影响。我们提出,淋病治疗中使用的抗生素亚致死水平可以增加该操纵子的转录本水平,这可能会影响致病性。
