Abstract

SummaryIdentifying how microbes are able to manipulate, survive, and thrive in complex multispecies communities has expanded our understanding of how microbial ecosystems impact human health and the environment. The ability of bacteria to negatively affect neighbors, through explicit toxin delivery systems, provides them with an opportunity to manipulate the composition of growing microbial communities. Contact-dependent inhibition (CDI) systems (a Type Vb secretion system) are a distinct subset of competition systems whose contribution to shaping the development of spatially structured bacterial communities are yet to be fully understood. Here, we compare the impact of different CDI systems, at both the single-cell and population level, to determine the key drivers of CDI-mediated competition within spatially structured bacterial populations. Through an iterative approach using both an Escherichia coli experimental system and computational modeling, we show that CDI systems have subtle and system-specific effects at the single-cell level, generating single-cell-wide boundaries between CDI-expressing inhibitor cells and their neighboring targets. Despite the subtle effects of CDI at a single-cell level, CDI systems greatly diminished the ability of susceptible targets to expand their range during colony growth. The inoculum density of the population, together with the CDI system-specific variables of the speed of inhibition after contact and biological cost of CDI, strongly affects CDI-mediated competition. In contrast, the magnitude of the toxin-induced growth retardation of target cells only weakly impacts the composition of the population. Our work reveals how distinct CDI systems can differentially affect the composition and spatial arrangement of bacterial populations.

Highlights

  • Each inhibitor strain was competed with an isogenic E. coli MG1655 strain lacking the Contact-dependent inhibition (CDI) system

  • Cell lysis of target cells was very rarely observed when in contact with either of the CDI systems, and membrane integrity was maintained in the vast majority of target cells (Figures S1 and S2). These results show that the CDI systems tested cause a subtle growth retardation of target cells along the contact interface rather than immediate growth arrest or cell lysis and that the extent of growth retardation is dependent on the type of CDI system expressed

  • We aimed to determine the extent to which different CDI systems of E. coli were capable of influencing the growth of mixed spatially structured populations consisting of targets and inhibitor cells and

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Summary

Objectives

We aimed to determine the extent to which different CDI systems of E. coli were capable of influencing the growth of mixed spatially structured populations consisting of targets and inhibitor cells and

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