Division of Infectious Diseases and International Health, Carter Harrison Bldg, Charlottesville, VA 22908, USA.
BMC Infect Dis. 2012 Dec 10;12:342. doi: 10.1186/1471-2334-12-342.
Activation of the A2A adenosine receptor (A2AAR) decreases production of inflammatory cytokines, prevents C. difficile toxin A-induced enteritis and, in combination with antibiotics, increases survival from sepsis in mice. We investigated whether A2AAR activation improves and A2AAR deletion worsens outcomes in a murine model of C. difficile (strain VPI10463) infection (CDI).
C57BL/6 mice were pretreated with an antibiotic cocktail prior to infection and then treated with vancomycin with or without an A2AAR agonist. A2AAR-/- and littermate wild-type (WT) mice were similarly infected, and IFNγ and TNFα were measured at peak of and recovery from infection.
Infected, untreated mice rapidly lost weight, developed diarrhea, and had mortality rates of 50-60%. Infected mice treated with vancomycin had less weight loss and diarrhea during antibiotic treatment but mortality increased to near 100% after discontinuation of antibiotics. Infected mice treated with both vancomycin and an A2AAR agonist, either ATL370 or ATL1222, had minimal weight loss and better long-term survival than mice treated with vancomycin alone. A2AAR KO mice were more susceptible than WT mice to death from CDI. Increases in cecal IFNγ and blood TNFα were pronounced in the absence of A2AARs.
In a murine model of CDI, vancomycin treatment resulted in reduced weight loss and diarrhea during acute infection, but high recurrence and late-onset death, with overall mortality being worse than untreated infected controls. The administration of vancomycin plus an A2AAR agonist reduced inflammation and improved survival rates, suggesting a possible benefit of A2AAR agonists in the management of CDI to prevent recurrent disease.
激活 A2A 腺苷受体 (A2AAR) 可减少炎症细胞因子的产生,防止艰难梭菌毒素 A 诱导的肠炎,并与抗生素联合使用,可提高小鼠脓毒症的存活率。我们研究了在艰难梭菌(VPI10463 株)感染(CDI)的小鼠模型中,A2AAR 激活是否改善了结果,A2AAR 缺失是否恶化了结果。
在感染前,C57BL/6 小鼠用抗生素鸡尾酒进行预处理,然后用万古霉素治疗,并用或不用 A2AAR 激动剂。A2AAR-/-和同窝野生型(WT)小鼠也进行了类似的感染,在感染高峰期和恢复期测量 IFNγ 和 TNFα。
未治疗的感染小鼠体重迅速下降,出现腹泻,死亡率为 50-60%。用万古霉素治疗的感染小鼠在抗生素治疗期间体重减轻和腹泻减少,但停药后死亡率增加到近 100%。用万古霉素和 A2AAR 激动剂(ATL370 或 ATL1222)治疗的感染小鼠体重减轻最小,长期存活率优于单用万古霉素治疗的小鼠。A2AAR KO 小鼠比 WT 小鼠更容易死于 CDI。在缺乏 A2AAR 时,盲肠 IFNγ 和血液 TNFα 的增加更为明显。
在 CDI 的小鼠模型中,万古霉素治疗可减少急性感染期间的体重减轻和腹泻,但复发率高,晚期死亡率高,总死亡率比未治疗的感染对照组更差。万古霉素加 A2AAR 激动剂的给药减少了炎症并提高了存活率,表明 A2AAR 激动剂在预防复发性疾病方面可能对 CDI 的治疗有益。
