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布鲁氏菌L型菌的神话以及布鲁氏菌青霉素结合蛋白(PBPs)在致病过程中的可能作用。

The myth of Brucella L-forms and possible involvement of Brucella penicillin binding proteins (PBPs) in pathogenicity.

作者信息

Banai M, Adams L G, Frey M, Pugh R, Ficht T A

机构信息

Department of Bacteriology, Kimron Veterinary Institute, PO Box 12, Bet Dagan 50250, Israel.

出版信息

Vet Microbiol. 2002 Dec 20;90(1-4):263-79. doi: 10.1016/s0378-1135(02)00213-4.

Abstract

Brucella spp. L-forms have been proposed to be stationary phase organisms in the evolution of new variants and enduring entities in the host in complicated cases of brucellosis and during latent brucellosis. In vitro formation of Brucella L-forms has been achieved by treating the cells with sub-lethal doses of penicillin. Interestingly, Brucella spp. have classified during the evolution into two groups, penicillin susceptible or penicillin resistant, yet both types grow on 20 microg/ml of methicillin. Strains proven susceptible to penicillin grew in the presence of methicillin as L-forms as demonstrated by light and electron microscopy. In addition, the B. melitensis vaccine strain Rev.1, a penicillin susceptible organism, responded to sheep serum by development of L-form-like structures unlike wild type, strain 16M. The two strains grew normally in sheep macrophages. We propose, for the first time, a model that associates Brucella pathogenicity with the structure and activity of two of their penicillin binding proteins (PBPs). According to the model, PBP1 has evolved as the major cell wall synthesizing enzyme of the genus, capable of responding to host serum growth factor(s) necessary for Brucella survival in the host. This property is associated with high avidity to beta-lactam antibiotics. PBP2 complements the activity of PBP1. New beta-lactam antibiotics and improved vaccines might be developed based on this property.

摘要

布鲁氏菌属L型被认为是布鲁氏菌病复杂病例和潜伏性布鲁氏菌病中宿主新变种和持久实体进化过程中的稳定期生物体。通过用亚致死剂量的青霉素处理细胞,已在体外实现了布鲁氏菌L型的形成。有趣的是,布鲁氏菌属在进化过程中已分为两组,即对青霉素敏感或耐药,但两种类型都能在20微克/毫升的甲氧西林上生长。经证实对青霉素敏感的菌株在甲氧西林存在下以L型生长,光学显微镜和电子显微镜均证实了这一点。此外,布鲁氏菌羊种疫苗株Rev.1是一种对青霉素敏感的生物体,与野生型菌株16M不同,它对绵羊血清的反应是形成类似L型的结构。这两种菌株在绵羊巨噬细胞中正常生长。我们首次提出了一个模型,将布鲁氏菌的致病性与其两种青霉素结合蛋白(PBPs)的结构和活性联系起来。根据该模型,PBP1已进化为该属的主要细胞壁合成酶,能够对布鲁氏菌在宿主体内存活所需的宿主血清生长因子作出反应。这一特性与对β-内酰胺抗生素的高亲和力有关。PBP2补充PBP1的活性。基于这一特性,可能会开发出新的β-内酰胺抗生素和改良疫苗。

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