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Active and passive immunization protects against lethal, extreme drug resistant-Acinetobacter baumannii infection

机译:主动和被动免疫可防止致命,极端耐药的鲍曼不动杆菌感染

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摘要

Extreme-drug-resistant (XDR) Acinetobacter baumannii is a rapidly emerging pathogen causing infections with unacceptably high mortality rates due to inadequate available treatment. New methods to prevent and treat such infections are a critical unmet medical need. To conduct a rational vaccine discovery program, OmpA was identified as the primary target of humoral immune response after intravenous infection by A. baumannii in mice. OmpA was > 99% conserved at the amino acid level across clinical isolates harvested between 1951 and 2009 from cerebrospinal fluid, blood, lung, and wound infections, including carbapenem-resistant isolates, and was ≥89% conserved among other sequenced strains, but had minimal homology to the human proteome. Vaccination of diabetic mice with recombinant OmpA (rOmpA) with aluminum hydroxide adjuvant markedly improved survival and reduced tissue bacterial burden in mice infected intravenously. Vaccination induced high titers of anti-OmpA antibodies, the levels of which correlated with survival in mice. Passive transfer with immune sera recapitulated protection. Immune sera did not enhance complement-mediated killing but did enhance opsonophagocytic killing of A. baumannii. These results define active and passive immunization strategies to prevent and treat highly lethal, XDR A. baumannii infections. © 2012 Luo et al.
机译:极度耐药(XDR)鲍曼不动杆菌是一种迅速出现的病原体,由于可用的治疗不足而导致感染,死亡率高得令人无法接受。预防和治疗此类感染的新方法是医疗需求的关键。为了进行合理的疫苗发现程序,在小鼠中鲍曼不动杆菌静脉感染后,OmpA被确定为体液免疫应答的主要靶标。 OmpA在1951年至2009年间从脑脊液,血液,肺和伤口感染(包括对碳青霉烯类耐药的分离株)中收获的临床分离株中,氨基酸水平上> 99%保守,在其他测序菌株中均≥89%保守,但与人类蛋白质组的最小同源性。用氢氧化铝佐剂对重组OmpA(rOmpA)的糖尿病小鼠进行疫苗接种可显着提高静脉内感染小鼠的存活率并减少组织细菌负担。疫苗接种可产生高滴度的抗OmpA抗体,其水平与小鼠的存活率相关。带有免疫血清的被动转移概括了保护作用。免疫血清不能增强补体介导的杀伤作用,但可以增强鲍曼不动杆菌的调理吞噬作用。这些结果确定了预防和治疗高度致死的鲍德曼不动杆菌感染的主动和被动免疫策略。 ©2012罗等人。

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