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High-throughput mapping of the phage resistance landscape in E. coli

High-throughput mapping of the phage resistance landscape in E. coli

来源:bioRxiv_logobioRxiv
英文摘要

Abstract Bacteriophages (phages) are critical players in the dynamics and function of microbial communities and drive processes as diverse as global biogeochemical cycles and human health. Phages tend to be predators finely tuned to attack specific hosts, even down to the strain level, which in turn defend themselves using an array of mechanisms. However, to date, efforts to rapidly and comprehensively identify bacterial host factors important in phage infection and resistance have yet to be fully realized. Here, we globally map the host genetic determinants involved in resistance to 14 phylogenetically diverse double-stranded DNA phages using two model Escherichia coli strains (K-12 and BL21) with known sequence divergence to demonstrate strain-specific differences. Using genome-wide loss-of-function and gain-of-function genetic technologies, we are able to confirm previously described phage receptors as well as uncover a number of previously unknown host factors that confer resistance to one or more of these phages. We uncover differences in resistance factors that strongly align with the susceptibility of K-12 and BL21 to specific phage. We also identify both phage specific mechanisms, such as the unexpected role of cyclic-di-GMP in host sensitivity to phage N4, and more generic defenses, such as the overproduction of colanic acid capsular polysaccharide that defends against a wide array of phages. Our results indicate that host responses to phages can occur via diverse cellular mechanisms. Our systematic and high-throughput genetic workflow to characterize phage-host interaction determinants can be extended to diverse bacteria to generate datasets that allow predictive models of how phage-mediated selection will shape bacterial phenotype and evolution. The results of this study and future efforts to map the phage resistance landscape will lead to new insights into the coevolution of hosts and their phage, which can ultimately be used to design better phage therapeutic treatments and tools for precision microbiome engineering.

Zhong Crystal、Mutalik Vivek K.、Adler Benjamin A.、Rishi Harneet S.、Novichkov Pavel、Deutschbauer Adam M.、Piya Denish、Koskella Britt、Price Morgan N.、Arkin Adam P.、Calendar Richard

Environmental Genomics and Systems Biology Division, Lawrence Berkeley National LaboratoryEnvironmental Genomics and Systems Biology Division, Lawrence Berkeley National Laboratory||Innovative Genomics InstituteInnovative Genomics Institute||Department of Bioengineering, University of California - BerkeleyBiophysics Graduate Group, University of California - Berkeley||Designated Emphasis Program in Computational and Genomic Biology, University of California - BerkeleyEnvironmental Genomics and Systems Biology Division, Lawrence Berkeley National LaboratoryEnvironmental Genomics and Systems Biology Division, Lawrence Berkeley National Laboratory||Innovative Genomics Institute||Department of Plant and Microbial Biology, University of California - BerkeleyInnovative Genomics Institute||Department of Bioengineering, University of California - BerkeleyDepartment of Integrative Biology, University of California - BerkeleyEnvironmental Genomics and Systems Biology Division, Lawrence Berkeley National LaboratoryEnvironmental Genomics and Systems Biology Division, Lawrence Berkeley National Laboratory||Innovative Genomics Institute||Department of Bioengineering, University of California - BerkeleyDepartment of Molecular and Cell Biology, University of California - Berkeley

10.1101/2020.02.15.951020

微生物学遗传学分子生物学

Zhong Crystal,Mutalik Vivek K.,Adler Benjamin A.,Rishi Harneet S.,Novichkov Pavel,Deutschbauer Adam M.,Piya Denish,Koskella Britt,Price Morgan N.,Arkin Adam P.,Calendar Richard.High-throughput mapping of the phage resistance landscape in E. coli[EB/OL].(2025-03-28)[2025-05-23].https://www.biorxiv.org/content/10.1101/2020.02.15.951020.点此复制

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