Abstract

The type VI secretion system (T6SS) is a secretion pathway widespread in Gram-negative bacteria that targets toxins in both prokaryotic and eukaryotic cells. Although most T6SSs identified so far are involved in inter-bacterial competition, a few are directly required for full virulence of pathogens. The T6SS comprises 13 core proteins that assemble a large complex structurally and functionally similar to a phage contractile tail structure anchored to the cell envelope by a trans-membrane spanning stator. The central part of this stator, TssM, is a 1129-amino-acid protein anchored in the inner membrane that binds to the TssJ outer membrane lipoprotein. In this study, we have raised camelid antibodies against the purified TssM periplasmic domain. We report the crystal structure of two specific nanobodies that bind to TssM in the nanomolar range. Interestingly, the most potent nanobody, nb25, competes with the TssJ lipoprotein for TssM binding in vitro suggesting that TssJ and the nb25 CDR3 loop share the same TssM binding site or causes a steric hindrance preventing TssM-TssJ complex formation. Indeed, periplasmic production of the nanobodies displacing the TssM-TssJ interaction inhibits the T6SS function in vivo. This study illustrates the power of nanobodies to specifically target and inhibit bacterial secretion systems.

Highlights

  • The type VI secretion system (T6SS) is a machinery widespread in Gram-negative bacteria and dedicated to the delivery of toxins in bacterial and eukaryotic host cells

  • Nanobodies were raised by immunization of llamas with the purified periplasmic domain of the enteroaggregative Escherichia coli (EAEC) TssM protein (TssMp)

  • We raised and selected two camelid variable fragments of heavy-chain antibodies specific to the EAEC T6SS TssM periplasmic domain

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Summary

Introduction

The type VI secretion system (T6SS) is a machinery widespread in Gram-negative bacteria and dedicated to the delivery of toxins in bacterial and eukaryotic host cells. By its anti-bacterial antagonistic action, the T6SS is one of the main players in the bacterial warfare for the access to nutrients and for colonization of the ecological niche [1, 2]. Nanobody-Mediated T6SS Inhibition no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript

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