Laboratoire d'Ingénierie des Systèmes Macromoléculaires (LISM), Institut de Microbiologie, Bioénergies et Biotechnologie (IM2B), Aix-Marseille Université, CNRS, UMR 7255, 13009 Marseille, France.
Mass Spectrometry for Biology Unit, Université Paris Cité, Institut Pasteur, CNRS, UAR 2024, 75015 Paris, France.
Nucleic Acids Res. 2022 Dec 9;50(22):13114-13127. doi: 10.1093/nar/gkac1162.
Rearrangement hot spot (Rhs) proteins are members of the broad family of polymorphic toxins. Polymorphic toxins are modular proteins composed of an N-terminal region that specifies their mode of secretion into the medium or into the target cell, a central delivery module, and a C-terminal domain that has toxic activity. Here, we structurally and functionally characterize the C-terminal toxic domain of the antibacterial Rhsmain protein, TreTu, which is delivered by the type VI secretion system of Salmonella enterica Typhimurium. We show that this domain adopts an ADP-ribosyltransferase fold and inhibits protein synthesis by transferring an ADP-ribose group from NAD+ to the elongation factor Tu (EF-Tu). This modification is specifically placed on the side chain of the conserved D21 residue located on the P-loop of the EF-Tu G-domain. Finally, we demonstrate that the TriTu immunity protein neutralizes TreTu activity by acting like a lid that closes the catalytic site and traps the NAD+.
重排热点(Rhs)蛋白是多态毒素大家族的成员。多态毒素是由模块化蛋白组成的,由指定其分泌到培养基或靶细胞方式的 N 端区域、中央传递模块和具有毒性活性的 C 端结构域组成。在这里,我们对沙门氏菌 Typhimurium 型 VI 分泌系统传递的抗菌 Rhsmain 蛋白 TreTu 的 C 端毒性结构域进行了结构和功能表征。我们表明,该结构域采用 ADP-核糖基转移酶折叠,并通过将 ADP-核糖从 NAD+转移到延伸因子 Tu(EF-Tu)来抑制蛋白质合成。这种修饰特别放在 EF-Tu G 结构域 P 环上保守的 D21 残基的侧链上。最后,我们证明 TriTu 免疫蛋白通过充当封闭催化位点并捕获 NAD+的盖子来中和 TreTu 的活性。
Zotero 插件
