4.8 Article

Mechanism of effector capture and delivery by the type IV secretion system from Legionella pneumophila

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NATURE COMMUNICATIONS
卷 11, 期 1, 页码 -

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NATURE PUBLISHING GROUP
DOI: 10.1038/s41467-020-16681-z

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资金

  1. ERC [321630]
  2. Wellcome grant [098302]
  3. NIAID [R21AI130671, R37AI041699]
  4. Wellcome [202679/Z/16/Z, 206166/Z/17/Z]
  5. Wellcome Trust
  6. Medical Research Council UK
  7. Biotechnology and Biological Sciences Research Council
  8. Wellcome Trust [206166/Z/17/Z, 202679/Z/16/Z] Funding Source: Wellcome Trust
  9. European Research Council (ERC) [321630] Funding Source: European Research Council (ERC)

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Legionella pneumophila is a bacterial pathogen that utilises a Type IV secretion (T4S) system to inject effector proteins into human macrophages. Essential to the recruitment and delivery of effectors to the T4S machinery is the membrane-embedded T4 coupling complex (T4CC). Here, we purify an intact T4CC from the Legionella membrane. It contains the DotL ATPase, the DotM and DotN proteins, the chaperone module IcmSW, and two previously uncharacterised proteins, DotY and DotZ. The atomic resolution structure reveals a DotLMNYZ hetero-pentameric core from which the flexible IcmSW module protrudes. Six of these hetero-pentameric complexes may assemble into a 1.6-MDa hexameric nanomachine, forming an inner membrane channel for effectors to pass through. Analysis of multiple cryo EM maps, further modelling and mutagenesis provide working models for the mechanism for binding and delivery of two essential classes of Legionella effectors, depending on IcmSW or DotM, respectively. A membrane-embedded complex (called T4CC) is essential for injection of Legionella pneumophila effector proteins into human macrophages via a Type IV secretion system. Here, the authors purify and study the T4CC using functional and cryo-EM structural analyses, providing insights into the secretion mechanisms.

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