Coinfecting phages impede each other's entry into the cell

Thu Vu Phuc Nguyen; Yuchen Wu; Tianyou Yao; Jimmy T. Trinh; Lanying Zeng; Yann R. Chemla; Ido Golding

doi:10.1016/j.cub.2024.05.032

Coinfecting phages impede each other's entry into the cell

Thu Vu Phuc Nguyen, Yuchen Wu, Tianyou Yao, Jimmy T. Trinh, Lanying Zeng, Yann R. Chemla, Ido Golding

Research output: Contribution to journal › Article › peer-review

Abstract

The developmental choice made by temperate phages, between cell death (lysis) and viral dormancy (lysogeny), is influenced by the relative abundance of viruses and hosts in the environment. The paradigm for this abundance-driven decision is phage lambda of E. coli, whose propensity to lysogenize increases with the number of viruses coinfecting the same bacterium. It is believed that lambda uses this number to infer whether phages or bacteria outnumber each other. However, this interpretation is premised on an accurate mapping between the extracellular phage-to-bacteria ratio and the intracellular multiplicity of infection (MOI). Here, we show this premise to be faulty. By simultaneously labeling phage capsids and genomes, we find that, while the number of phages landing on each cell reliably samples the population ratio, the number of phages entering the cell does not. Single-cell infections, performed in a microfluidic device and interpreted using a stochastic model, reveal that the probability and rate of phage entry decrease with the number of adsorbed phages. This decrease reflects an MOI-dependent perturbation to host physiology caused by phage attachment, as evidenced by compromised membrane integrity and loss of membrane potential. The dependence of entry dynamics on the surrounding medium results in a strong impact on the infection outcome, while the protracted entry of coinfecting phages increases the heterogeneity in infection outcome at a given MOI. Our findings in lambda, and similar results we obtained for phages T5 and P1, demonstrate the previously unappreciated role played by entry dynamics in determining the outcome of bacteriophage infection.

Original language	English (US)
Pages (from-to)	2841-2853.e18
Journal	Current Biology
Volume	34
Issue number	13
DOIs	https://doi.org/10.1016/j.cub.2024.05.032
State	Published - Jul 8 2024

Keywords

Escherichia coli
bacteriophage
biophysics
genome ejection
lambda
lysogeny
mathematical modeling
membrane potential
microbiology
microscopy

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology
General Agricultural and Biological Sciences

Online availability

10.1016/j.cub.2024.05.032

Library availability

Discover UIUC Full Text

Cite this

@article{b409e04141f841c5a7e4edab8559d197,

title = "Coinfecting phages impede each other's entry into the cell",

abstract = "The developmental choice made by temperate phages, between cell death (lysis) and viral dormancy (lysogeny), is influenced by the relative abundance of viruses and hosts in the environment. The paradigm for this abundance-driven decision is phage lambda of E. coli, whose propensity to lysogenize increases with the number of viruses coinfecting the same bacterium. It is believed that lambda uses this number to infer whether phages or bacteria outnumber each other. However, this interpretation is premised on an accurate mapping between the extracellular phage-to-bacteria ratio and the intracellular multiplicity of infection (MOI). Here, we show this premise to be faulty. By simultaneously labeling phage capsids and genomes, we find that, while the number of phages landing on each cell reliably samples the population ratio, the number of phages entering the cell does not. Single-cell infections, performed in a microfluidic device and interpreted using a stochastic model, reveal that the probability and rate of phage entry decrease with the number of adsorbed phages. This decrease reflects an MOI-dependent perturbation to host physiology caused by phage attachment, as evidenced by compromised membrane integrity and loss of membrane potential. The dependence of entry dynamics on the surrounding medium results in a strong impact on the infection outcome, while the protracted entry of coinfecting phages increases the heterogeneity in infection outcome at a given MOI. Our findings in lambda, and similar results we obtained for phages T5 and P1, demonstrate the previously unappreciated role played by entry dynamics in determining the outcome of bacteriophage infection.",

keywords = "Escherichia coli, bacteriophage, biophysics, genome ejection, lambda, lysogeny, mathematical modeling, membrane potential, microbiology, microscopy",

author = "Nguyen, {Thu Vu Phuc} and Yuchen Wu and Tianyou Yao and Trinh, {Jimmy T.} and Lanying Zeng and Chemla, {Yann R.} and Ido Golding",

note = "We are grateful to the following people for their generous advice: M. Gruebele, M. Goulian, C. Herman, K. Maxwell, I. Molineux, T. Pilizota, A. Sokac, K. Venken, T. Wensel, Z. Yu, C. Zong, and all members of the Golding lab. Work in the Golding lab is supported by the National Institutes of Health grant R35 GM140709, the National Science Foundation grant 2243257 (NSF Science and Technology Center for Quantitative Cell Biology), and the Alfred P. Sloan Foundation under grant G-2023-19649. Work in the Chemla lab is supported by the National Science Foundation Physics Frontiers Center (PFC) \u201CCenter for the Physics of Living Cells\u201D (CPLC) grant PHY 1430124 and the National Institutes of Health grant R35 GM144125. Work in the Zeng lab is supported by the National Science Foundation grant MCB 2013762. We gratefully acknowledge the computing resources provided by the Computational and Integrative Biomedical Research Center of Baylor College of Medicine. Conceptualization, T.V.P.N. and I.G.; methodology, T.V.P.N. Y.W. T.Y. J.T.T. L.Z. Y.R.C. and I.G.; investigation and formal analysis, T.V.P.N. Y.W. Y.R.C. and I.G.; visualization, T.V.P.N.; writing \u2013 original draft, T.V.P.N. and I.G.; writing \u2013 review & editing, T.V.P.N. L.Z. Y.R.C. and I.G.; funding acquisition and supervision, L.Z. Y.R.C. and I.G.; project administration, I.G. The authors declare no competing interests. We are grateful to the following people for their generous advice: M. Gruebele, M. Goulian, C. Herman, K. Maxwell, I. Molineux, T. Pilizota, A. Sokac, K. Venken, T. Wensel, Z. Yu, C. Zong, and all members of the Golding lab. Work in the Golding lab is supported by the National Institutes of Health grant R35 GM140709 , the National Science Foundation grant 2243257 (NSF Science and Technology Center for Quantitative Cell Biology), and the Alfred P. Sloan Foundation under grant G-2023-19649 . Work in the Chemla lab is supported by the National Science Foundation Physics Frontiers Center (PFC) \u201CCenter for the Physics of Living Cells\u201D (CPLC) grant PHY 1430124 and the National Institutes of Health grant R35 GM144125 . Work in the Zeng lab is supported by the National Science Foundation grant MCB 2013762 . We gratefully acknowledge the computing resources provided by the Computational and Integrative Biomedical Research Center of Baylor College of Medicine.",

year = "2024",

month = jul,

day = "8",

doi = "10.1016/j.cub.2024.05.032",

language = "English (US)",

volume = "34",

pages = "2841--2853.e18",

journal = "Current Biology",

issn = "0960-9822",

publisher = "Cell Press",

number = "13",

}

TY - JOUR

T1 - Coinfecting phages impede each other's entry into the cell

AU - Nguyen, Thu Vu Phuc

AU - Wu, Yuchen

AU - Yao, Tianyou

AU - Trinh, Jimmy T.

AU - Zeng, Lanying

AU - Chemla, Yann R.

AU - Golding, Ido

N1 - We are grateful to the following people for their generous advice: M. Gruebele, M. Goulian, C. Herman, K. Maxwell, I. Molineux, T. Pilizota, A. Sokac, K. Venken, T. Wensel, Z. Yu, C. Zong, and all members of the Golding lab. Work in the Golding lab is supported by the National Institutes of Health grant R35 GM140709, the National Science Foundation grant 2243257 (NSF Science and Technology Center for Quantitative Cell Biology), and the Alfred P. Sloan Foundation under grant G-2023-19649. Work in the Chemla lab is supported by the National Science Foundation Physics Frontiers Center (PFC) \u201CCenter for the Physics of Living Cells\u201D (CPLC) grant PHY 1430124 and the National Institutes of Health grant R35 GM144125. Work in the Zeng lab is supported by the National Science Foundation grant MCB 2013762. We gratefully acknowledge the computing resources provided by the Computational and Integrative Biomedical Research Center of Baylor College of Medicine. Conceptualization, T.V.P.N. and I.G.; methodology, T.V.P.N. Y.W. T.Y. J.T.T. L.Z. Y.R.C. and I.G.; investigation and formal analysis, T.V.P.N. Y.W. Y.R.C. and I.G.; visualization, T.V.P.N.; writing \u2013 original draft, T.V.P.N. and I.G.; writing \u2013 review & editing, T.V.P.N. L.Z. Y.R.C. and I.G.; funding acquisition and supervision, L.Z. Y.R.C. and I.G.; project administration, I.G. The authors declare no competing interests. We are grateful to the following people for their generous advice: M. Gruebele, M. Goulian, C. Herman, K. Maxwell, I. Molineux, T. Pilizota, A. Sokac, K. Venken, T. Wensel, Z. Yu, C. Zong, and all members of the Golding lab. Work in the Golding lab is supported by the National Institutes of Health grant R35 GM140709 , the National Science Foundation grant 2243257 (NSF Science and Technology Center for Quantitative Cell Biology), and the Alfred P. Sloan Foundation under grant G-2023-19649 . Work in the Chemla lab is supported by the National Science Foundation Physics Frontiers Center (PFC) \u201CCenter for the Physics of Living Cells\u201D (CPLC) grant PHY 1430124 and the National Institutes of Health grant R35 GM144125 . Work in the Zeng lab is supported by the National Science Foundation grant MCB 2013762 . We gratefully acknowledge the computing resources provided by the Computational and Integrative Biomedical Research Center of Baylor College of Medicine.

PY - 2024/7/8

Y1 - 2024/7/8

N2 - The developmental choice made by temperate phages, between cell death (lysis) and viral dormancy (lysogeny), is influenced by the relative abundance of viruses and hosts in the environment. The paradigm for this abundance-driven decision is phage lambda of E. coli, whose propensity to lysogenize increases with the number of viruses coinfecting the same bacterium. It is believed that lambda uses this number to infer whether phages or bacteria outnumber each other. However, this interpretation is premised on an accurate mapping between the extracellular phage-to-bacteria ratio and the intracellular multiplicity of infection (MOI). Here, we show this premise to be faulty. By simultaneously labeling phage capsids and genomes, we find that, while the number of phages landing on each cell reliably samples the population ratio, the number of phages entering the cell does not. Single-cell infections, performed in a microfluidic device and interpreted using a stochastic model, reveal that the probability and rate of phage entry decrease with the number of adsorbed phages. This decrease reflects an MOI-dependent perturbation to host physiology caused by phage attachment, as evidenced by compromised membrane integrity and loss of membrane potential. The dependence of entry dynamics on the surrounding medium results in a strong impact on the infection outcome, while the protracted entry of coinfecting phages increases the heterogeneity in infection outcome at a given MOI. Our findings in lambda, and similar results we obtained for phages T5 and P1, demonstrate the previously unappreciated role played by entry dynamics in determining the outcome of bacteriophage infection.

AB - The developmental choice made by temperate phages, between cell death (lysis) and viral dormancy (lysogeny), is influenced by the relative abundance of viruses and hosts in the environment. The paradigm for this abundance-driven decision is phage lambda of E. coli, whose propensity to lysogenize increases with the number of viruses coinfecting the same bacterium. It is believed that lambda uses this number to infer whether phages or bacteria outnumber each other. However, this interpretation is premised on an accurate mapping between the extracellular phage-to-bacteria ratio and the intracellular multiplicity of infection (MOI). Here, we show this premise to be faulty. By simultaneously labeling phage capsids and genomes, we find that, while the number of phages landing on each cell reliably samples the population ratio, the number of phages entering the cell does not. Single-cell infections, performed in a microfluidic device and interpreted using a stochastic model, reveal that the probability and rate of phage entry decrease with the number of adsorbed phages. This decrease reflects an MOI-dependent perturbation to host physiology caused by phage attachment, as evidenced by compromised membrane integrity and loss of membrane potential. The dependence of entry dynamics on the surrounding medium results in a strong impact on the infection outcome, while the protracted entry of coinfecting phages increases the heterogeneity in infection outcome at a given MOI. Our findings in lambda, and similar results we obtained for phages T5 and P1, demonstrate the previously unappreciated role played by entry dynamics in determining the outcome of bacteriophage infection.

KW - Escherichia coli

KW - bacteriophage

KW - biophysics

KW - genome ejection

KW - lambda

KW - lysogeny

KW - mathematical modeling

KW - membrane potential

KW - microbiology

KW - microscopy

UR - http://www.scopus.com/inward/record.url?scp=85196985077&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85196985077&partnerID=8YFLogxK

U2 - 10.1016/j.cub.2024.05.032

DO - 10.1016/j.cub.2024.05.032

M3 - Article

C2 - 38878771

AN - SCOPUS:85196985077

SN - 0960-9822

VL - 34

SP - 2841-2853.e18

JO - Current Biology

JF - Current Biology

IS - 13

ER -

Coinfecting phages impede each other's entry into the cell

Abstract

Keywords

ASJC Scopus subject areas

Online availability

Library availability

Related links

Fingerprint

Cite this