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猪链球菌2型LuxS肽抑制剂的生物学活性及鉴定

Biological activity and identification of a peptide inhibitor of LuxS from Streptococcus suis serotype 2.

作者信息

Han Xiangan, Lu Chengping

机构信息

Key Laboratory of Animal Disease Diagnostics and Immunology, Ministry of Agriculture, Nanjing Agricultural University, Nanjing, China.

出版信息

FEMS Microbiol Lett. 2009 May;294(1):16-23. doi: 10.1111/j.1574-6968.2009.01534.x. Epub 2008 Mar 18.

Abstract

The virulence of bacterial communities may be regulated by mechanisms involving the synthesis of the quorum-sensing signal autoinducer 2 (AI-2), which allows both intra- and interspecies communication. AI-2 is produced in bacteria that express the gene luxS. In the present study, expressed and purified LuxS from Streptococcus suis serotype 2 (SS2) was used to catalyze the substrate S-ribosylhomocysteine in a reaction that leads to the production of AI-2. The biological activity of the in vitro synthesized AI-2 was demonstrated in a Vibrio harveyi strain BB170 bioassay; real-time PCR results showed that biosynthesis of AI-2 can increase the virulence of SS2. Phage-encoded peptides that specifically interact with the LuxS enzyme were selected following three rounds of phage display. One such peptide inhibitor (TNRHNPHHLHHV) of LuxS was shown to partially inhibit the activity of the enzyme. Furthermore, 14 peptides containing the consensus sequence HSIR showed high affinity with LuxS. The selected and characterized specific inhibitor as well as the high-affinity ligands may facilitate the identification of new vaccination targets, opening up new approaches to the development of therapeutic drugs.

摘要

细菌群落的毒力可能受群体感应信号自诱导物2(AI-2)合成相关机制的调控,AI-2可实现种内和种间通讯。AI-2由表达luxS基因的细菌产生。在本研究中,利用从猪链球菌2型(SS2)中表达并纯化的LuxS催化底物S-核糖基高半胱氨酸,该反应可生成AI-2。体外合成的AI-2的生物活性在哈维氏弧菌BB170菌株生物测定中得到证实;实时PCR结果表明,AI-2的生物合成可增加SS2的毒力。经过三轮噬菌体展示,筛选出了与LuxS酶特异性相互作用的噬菌体编码肽。其中一种LuxS肽抑制剂(TNRHNPHHLHHV)被证明可部分抑制该酶的活性。此外,14个含有共有序列HSIR的肽与LuxS具有高亲和力。所筛选和鉴定的特异性抑制剂以及高亲和力配体可能有助于确定新的疫苗靶点,为治疗药物的开发开辟新途径。

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