The proline-rich antimicrobial peptide Onc112 inhibits translation by blocking and destabilizing the initiation complex

被引:139
作者
Seefeldt, A. Carolin [1 ,2 ]
Fabian Nguyen [3 ]
Antunes, Stephanie [1 ,4 ]
Perebaskine, Natacha [1 ,2 ]
Graf, Michael [3 ]
Arenz, Stefan [3 ]
Inampudi, K. Kishore [1 ,2 ]
Douat, Celine [1 ,4 ]
Guichard, Gilles [1 ,4 ]
Wilson, Daniel N. [3 ,5 ]
Innis, C. Axel [1 ,2 ]
机构
[1] Inst Europeen Chim & Biol, Pessac, France
[2] INSERM, U869, Bordeaux, France
[3] Univ Munich, Dept Biochem, Gene Ctr, Munich, Germany
[4] Univ Bordeaux, CNRS, Inst Chim & Biol Membranes & Nano Objets CBMN, Inst Polytech Bordeaux,UMR 5248, Pessac, France
[5] Univ Munich, Ctr Integrated Prot Sci Munich CiPSM, Munich, Germany
关键词
CELL-PENETRATING PEPTIDE; BOND FORMATION; SECONDARY STRUCTURE; MOLECULAR-BASIS; RIBOSOME; RNA; MECHANISM; BACTERIA; SBMA;
D O I
10.1038/nsmb.3034
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The increasing prevalence of multidrug-resistant pathogenic bacteria is making current antibiotics obsolete. Proline-rich antimicrobial peptides (PrAMPs) display potent activity against Gram-negative bacteria and thus represent an avenue for antibiotic development. PrAMPs from the oncocin family interact with the ribosome to inhibit translation, but their mode of action has remained unclear. Here we have determined a structure of the Onc112 peptide in complex with the Thermus thermophilus 70S ribosome at a resolution of 3.1 angstrom by X-ray crystallography. The Onc112 peptide binds within the ribosomal exit tunnel and extends toward the peptidyl transferase center, where it overlaps with the binding site for an aminoacyl-tRNA. We show biochemically that the binding of Onc112 blocks and destabilizes the initiation complex, thus preventing entry into the elongation phase. Our findings provide a basis for the future development of this class of potent antimicrobial agents.
引用
收藏
页码:470 / U59
页数:8
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