Structure and Function of the Dot/Icm T4SS

Author:

Dutka PrzemysławORCID,Liu Yuxi,Maggi Stefano,Ghosal Debnath,Wang Jue,Carter Stephen D.,Zhao Wei,Vijayrajratnam Sukhithasri,Vogel Joseph P.,Jensen Grant J.ORCID

Abstract

AbstractTheLegionella pneumophilaDot/Icm type IV secretion system (T4SS) delivers effector proteins into host cells during infection. Despite its significance as a potential drug target, our current understanding of its atomic structure is limited to isolated subcomplexes. In this study, we used subtomogram averaging and integrative modeling to construct a nearly-complete model of the Dot/Icm T4SS accounting for seventeen protein components. We locate and provide insights into the structure and function of six new components including DotI, DotJ, DotU, IcmF, IcmT, and IcmX. We find that the cytosolic N-terminal domain of IcmF, a key protein forming a central hollow cylinder, interacts with DotU, providing insight into previously uncharacterized density. Furthermore, our model, in combination with analyses of compositional heterogeneity, explains how the cytoplasmic ATPase DotO is connected to the periplasmic complex via interactions with membrane-bound DotI/DotJ proteins. Coupled within situinfection data, our model offers new insights into the T4SS-mediated secretion mechanism.

Publisher

Cold Spring Harbor Laboratory

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