InvG secretin domain beta-barrel from Salmonella SPI-1 injectisome NC-base
マップデータ
InvG secretin domain beta-barrel from Salmonella SPI-1 injectisome NC-base
試料
複合体: InvG secretin domain beta-barrel from Salmonella SPI-1 injectisome NC-base
機能・相同性
機能・相同性情報
type III protein secretion system complex / type II protein secretion system complex / protein secretion by the type III secretion system / protein secretion / cell outer membrane / identical protein binding 類似検索 - 分子機能
: / SPI-1 type 3 secretion system secretin, N0 domain / Type III secretion system outer membrane pore YscC/HrcC / Bacterial type II secretion system protein D signature. / Type II secretion system protein GspD, conserved site / : / NolW-like / NolW-like superfamily / Bacterial type II/III secretion system short domain / Type II/III secretion system / Bacterial type II and III secretion system protein 類似検索 - ドメイン・相同性
SPI-1 type 3 secretion system secretin 類似検索 - 構成要素
生物種
Salmonella enterica subsp. enterica serovar Typhimurium str. SL1344 (サルモネラ菌)
ジャーナル: Nat Microbiol / 年: 2019 タイトル: T3S injectisome needle complex structures in four distinct states reveal the basis of membrane coupling and assembly. 著者: Jinhong Hu / Liam J Worrall / Marija Vuckovic / Chuan Hong / Wanyin Deng / Claire E Atkinson / B Brett Finlay / Zhiheng Yu / Natalie C J Strynadka / 要旨: The bacterial injectisome is a syringe-shaped macromolecular nanomachine utilized by many pathogenic Gram-negative bacteria, including the causative agents of plague, typhoid fever, whooping cough, ...The bacterial injectisome is a syringe-shaped macromolecular nanomachine utilized by many pathogenic Gram-negative bacteria, including the causative agents of plague, typhoid fever, whooping cough, sexually transmitted infections and major nosocomial infections. Bacterial proteins destined for self-assembly and host-cell targeting are translocated by the injectisome in a process known as type III secretion (T3S). The core structure is the ~4 MDa needle complex (NC), built on a foundation of three highly oligomerized ring-forming proteins that create a hollow scaffold spanning the bacterial inner membrane (IM) (24-mer ring-forming proteins PrgH and PrgK in the Salmonella enterica serovar Typhimurium Salmonella pathogenicity island 1 (SPI-1) type III secretion system (T3SS)) and outer membrane (OM) (15-mer InvG, a member of the broadly conserved secretin pore family). An internalized helical needle projects from the NC and bacterium, ultimately forming a continuous passage to the host, for delivery of virulence effectors. Here, we have captured snapshots of the entire prototypical SPI-1 NC in four distinct needle assembly states, including near-atomic resolution, and local reconstructions in the absence and presence of the needle. These structures reveal the precise localization and molecular interactions of the internalized SpaPQR 'export apparatus' complex, which is intimately encapsulated and stabilized within the IM rings in the manner of a nanodisc, and to which the PrgJ rod directly binds and functions as an initiator and anchor of needle polymerization. We also describe the molecular details of the extensive and continuous coupling interface between the OM secretin and IM rings, which is remarkably facilitated by a localized 16-mer stoichiometry in the periplasmic-most coupling domain of the otherwise 15-mer InvG oligomer.
ムービー
コントローラー
データを開く
基本情報
マップデータ
試料
機能・相同性情報
Salmonella enterica subsp. enterica serovar Typhimurium str. SL1344 (サルモネラ菌)
データ登録者
カナダ, 1件 
引用
構造の表示
ダウンロードとリンク
emd_20315.png
http://ftp.pdbj.org/pub/emdb/structures/EMD-20315
Z (Sec.)
Y (Row.)
X (Col.)
試料の構成要素
解析
電子顕微鏡法
FIELD EMISSION GUN