Department of Biology, Georgia State University, Atlanta, Georgia, USA.
Antimicrob Agents Chemother. 2012 Oct;56(10):5309-14. doi: 10.1128/AAC.01158-12. Epub 2012 Aug 6.
Polyamines are absolute requirements for cell growth. When in excess, Pseudomonas aeruginosa possesses six γ-glutamylpolyamine synthetases (GPSs) encoded by the pauA1-pauA7 genes to initiate polyamine catabolism. Recently, the pauA2 mutant was reported to lose the capability to grow on spermine (Spm) and spermidine (Spd) as sole carbon and nitrogen sources. Although this mutant grew normally in defined minimal medium and LB broth, growth was completely abolished by the addition of Spm or Spd. These two compounds exert a bactericidal effect (Spm > Spd) on the mutants as demonstrated by MIC measurements (over 500-fold reduction) and time-killing curves. Spm toxicity in the pauA2 mutant was attenuated when the major uptake system was further deleted from the strain, suggesting cytoplasmic targets of toxicity. In addition, the synergistic effect of Spm and carbenicillin in the wild-type strain PAO1 was diminished in mutants without functional PauA2. Furthermore, Spm MIC was reduced by 8-fold when the Spm uptake system was deleted from the wild-type strain, suggesting a second target of Spm toxicity in the periplasm. Experiments were also conducted to test the hypothesis that native Spm and Spd in human serum may be sufficient to kill the pauA2 mutant. Growth of the mutant was completely inhibited by 40% (vol/vol) human serum, whereas the parental strain required 80%. Colony counts indicated that the mutant but not the parent was in fact killed by human plasma. In addition, carbenicillin MIC against the mutant was reduced by 16-fold in the presence of 20% human serum while that of the parental strain remained unchanged. Taking PauA2 as the template, sequence comparison indicates that putative PauA2 homologues are widespread in a variety of Gram-negative bacteria. In summary, this study reveals the importance of GPS in alleviation of polyamine toxicity when in excess, and it provides strong support to the feasibility of GPS as a molecular target for new antibiotic development.
多胺是细胞生长的绝对需求。当过量时,铜绿假单胞菌拥有六个由 pauA1-pauA7 基因编码的 γ-谷氨酰多胺合成酶 (GPS) 来启动多胺分解代谢。最近,报道 pauA2 突变体失去了以腐胺 (Spm) 和亚精胺 (Spd) 作为唯一碳源和氮源生长的能力。尽管该突变体在定义明确的最低培养基和 LB 肉汤中正常生长,但添加 Spm 或 Spd 会完全抑制其生长。MIC 测量(超过 500 倍减少)和时间杀伤曲线表明,这两种化合物对突变体具有杀菌作用(Spm > Spd)。当从菌株中进一步删除主要摄取系统时,pauA2 突变体中的 Spm 毒性减弱,表明毒性的细胞质靶标。此外,野生型菌株 PAO1 中 Spm 和羧苄青霉素的协同作用在没有功能 PauA2 的突变体中减弱。此外,当从野生型菌株中删除 Spm 摄取系统时,Spm MIC 减少了 8 倍,这表明 Spm 毒性的第二个靶标在周质中。还进行了实验以测试假设,即人血清中的天然 Spm 和 Spd 可能足以杀死 pauA2 突变体。突变体的生长完全被 40%(体积/体积)人血清抑制,而亲本菌株需要 80%。菌落计数表明突变体而不是亲本实际上被人血浆杀死。此外,在存在 20%人血清的情况下,突变体对羧苄青霉素的 MIC 减少了 16 倍,而亲本菌株的 MIC 保持不变。以 PauA2 为模板,序列比较表明,假定的 PauA2 同源物在多种革兰氏阴性菌中广泛存在。总之,这项研究揭示了 GPS 在缓解多胺毒性方面的重要性,当多胺过量时,它为 GPS 作为新抗生素开发的分子靶标提供了强有力的支持。
