Qin Aiping, Tucker Aimee M, Hines Andria, Wood David O
Department of Microbiology and Immunology, University of South Alabama College of Medicine, Mobile, Alabama 36688, USA.
Appl Environ Microbiol. 2004 May;70(5):2816-22. doi: 10.1128/AEM.70.5.2816-2822.2004.
Genetic analysis of Rickettsia prowazekii has been hindered by the lack of selectable markers and efficient mechanisms for generating rickettsial gene knockouts. We have addressed these problems by adapting a gene that codes for rifampin resistance for expression in R. prowazekii and by incorporating this selection into a transposon mutagenesis system suitable for generating rickettsial gene knockouts. The arr-2 gene codes for an enzyme that ADP-ribosylates rifampin, thereby destroying its antibacterial activity. Based on the published sequence, this gene was synthesized by PCR with overlapping primers that contained rickettsial codon usage base changes. This R. prowazekii-adapted arr-2 gene (Rparr-2) was placed downstream of the strong rickettsial rpsL promoter (rpsL(P)), and the entire construct was inserted into the Epicentre EZ::TN transposome system. A purified transposon containing rpsL(P)-Rparr-2 was combined with transposase, and the resulting DNA-protein complex (transposome) was electroporated into competent rickettsiae. Following selection with rifampin, rickettsiae with transposon insertions in the genome were identified by PCR and Southern blotting and the insertion sites were determined by rescue cloning and inverse PCR. Multiple insertions into widely spaced areas of the R. prowazekii genome were identified. Three insertions were identified within gene coding sequences. Transposomes provide a mechanism for generating random insertional mutations in R. prowazekii, thereby identifying nonessential rickettsial genes.
普氏立克次体的遗传分析因缺乏可选择标记和产生立克次体基因敲除的有效机制而受到阻碍。我们通过改造一个编码利福平抗性的基因使其在普氏立克次体中表达,并将这种选择方法整合到一个适合产生立克次体基因敲除的转座子诱变系统中,解决了这些问题。arr-2基因编码一种使利福平进行ADP核糖基化的酶,从而破坏其抗菌活性。根据已发表的序列,该基因通过使用含有立克次体密码子使用碱基变化的重叠引物进行PCR合成。这个适应普氏立克次体的arr-2基因(Rparr-2)被置于强立克次体rpsL启动子(rpsL(P))的下游,整个构建体被插入到Epicentre EZ::TN转座体系统中。将含有rpsL(P)-Rparr-2的纯化转座子与转座酶结合,然后将所得的DNA-蛋白质复合物(转座体)电穿孔导入感受态立克次体中。在用利福平进行选择后,通过PCR和Southern印迹法鉴定基因组中存在转座子插入的立克次体,并通过拯救克隆和反向PCR确定插入位点。在普氏立克次体基因组广泛间隔的区域中鉴定到了多个插入。在基因编码序列内鉴定到了三个插入。转座体为在普氏立克次体中产生随机插入突变提供了一种机制,从而鉴定出非必需的立克次体基因。