The short cytoplasmic region of phage T4 holin is essential for the transition from impermeable membrane protein complexes to permeable pores

Jan Michel Frederik Schwarzkopf; Ruth Paola Viveros; Ali Nazmi Burdur; Denise Mehner-Breitfeld; Natalia Tschowri; Thomas Brüser

doi:10.3389/fmicb.2025.1579756

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Originalsprache	Englisch
Aufsatznummer	1579756
Fachzeitschrift	Frontiers in Microbiology
Jahrgang	16
Publikationsstatus	Veröffentlicht - 30 Mai 2025

Abstract

Virulent as well as temperate phages usually require lysis of bacteria to release their progeny into the surrounding. Double-stranded DNA phages achieve lysis by phage-encoded endolysins that degrade the bacterial cell wall. Endolysins cross the cytoplasmic membrane by the aid of phage-encoded hole-forming membrane proteins, the holins. Canonical holins have been shown to multimerize and form very large holes in membranes, and it is believed that these holes enable a non-specific release of endolysins from cytoplasm. We studied these aspects with Escherichia coli and the phage T4 model lysis system, consisting of the holin T and the endolysin E. By following the endolysin function in a microfluidic chamber with mEGFP-fused holin, we found that large multimerizations were not required for endolysin release. Moreover, while we found in further analyses of this construct that the periplasmic globular domain was not required for hole formation and thus likely serves only regulatory functions, the short cytoplasmic domain was essential for hole formation. A truncation as well as single point mutations abolished hole formation without affecting holin interactions. In agreement with this, AlphaFold 3 indicates that rings of holin T dimers can form aqueous holes that require a conformational switch of the N-terminal cytoplasmic amphipathic helix to a trans-membrane orientation inside the rings. Our data indicate that already small holin assemblies enable endolysin-mediated cell lysis, although large multimers may be formed in the absence of endolysins due to the clustering of such assemblies. Further, we provide a convincing structural model of a ring-shaped holin T complex that can form an aqueous pore of sufficient diameter to permit endolysin release.

ASJC Scopus Sachgebiete

Immunologie und Mikrobiologie (insg.)
Mikrobiologie
Medizin (insg.)
Mikrobiologie (medizinisch)

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The short cytoplasmic region of phage T4 holin is essential for the transition from impermeable membrane protein complexes to permeable pores. / Schwarzkopf, Jan Michel Frederik; Viveros, Ruth Paola; Burdur, Ali Nazmi et al.
in: Frontiers in Microbiology, Jahrgang 16, 1579756, 30.05.2025.

Publikation: Beitrag in Fachzeitschrift › Artikel › Forschung › Peer-Review

Schwarzkopf, JMF, Viveros, RP, Burdur, AN, Mehner-Breitfeld, D, Tschowri, N & Brüser, T 2025, 'The short cytoplasmic region of phage T4 holin is essential for the transition from impermeable membrane protein complexes to permeable pores', Frontiers in Microbiology, Jg. 16, 1579756. https://doi.org/10.3389/fmicb.2025.1579756

Schwarzkopf, J. M. F., Viveros, R. P., Burdur, A. N., Mehner-Breitfeld, D., Tschowri, N., & Brüser, T. (2025). The short cytoplasmic region of phage T4 holin is essential for the transition from impermeable membrane protein complexes to permeable pores. Frontiers in Microbiology, 16, Artikel 1579756. https://doi.org/10.3389/fmicb.2025.1579756

Schwarzkopf JMF, Viveros RP, Burdur AN, Mehner-Breitfeld D, Tschowri N , Brüser T. The short cytoplasmic region of phage T4 holin is essential for the transition from impermeable membrane protein complexes to permeable pores. Frontiers in Microbiology. 2025 Mai 30;16:1579756. doi: 10.3389/fmicb.2025.1579756

Schwarzkopf, Jan Michel Frederik ; Viveros, Ruth Paola ; Burdur, Ali Nazmi et al. / The short cytoplasmic region of phage T4 holin is essential for the transition from impermeable membrane protein complexes to permeable pores. in: Frontiers in Microbiology. 2025 ; Jahrgang 16.

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title = "The short cytoplasmic region of phage T4 holin is essential for the transition from impermeable membrane protein complexes to permeable pores",

abstract = "Virulent as well as temperate phages usually require lysis of bacteria to release their progeny into the surrounding. Double-stranded DNA phages achieve lysis by phage-encoded endolysins that degrade the bacterial cell wall. Endolysins cross the cytoplasmic membrane by the aid of phage-encoded hole-forming membrane proteins, the holins. Canonical holins have been shown to multimerize and form very large holes in membranes, and it is believed that these holes enable a non-specific release of endolysins from cytoplasm. We studied these aspects with Escherichia coli and the phage T4 model lysis system, consisting of the holin T and the endolysin E. By following the endolysin function in a microfluidic chamber with mEGFP-fused holin, we found that large multimerizations were not required for endolysin release. Moreover, while we found in further analyses of this construct that the periplasmic globular domain was not required for hole formation and thus likely serves only regulatory functions, the short cytoplasmic domain was essential for hole formation. A truncation as well as single point mutations abolished hole formation without affecting holin interactions. In agreement with this, AlphaFold 3 indicates that rings of holin T dimers can form aqueous holes that require a conformational switch of the N-terminal cytoplasmic amphipathic helix to a trans-membrane orientation inside the rings. Our data indicate that already small holin assemblies enable endolysin-mediated cell lysis, although large multimers may be formed in the absence of endolysins due to the clustering of such assemblies. Further, we provide a convincing structural model of a ring-shaped holin T complex that can form an aqueous pore of sufficient diameter to permit endolysin release.",

keywords = "endolysins, Escherichia coli, holins, membrane proteins, phage lysis, phages",

author = "Schwarzkopf, {Jan Michel Frederik} and Viveros, {Ruth Paola} and Burdur, {Ali Nazmi} and Denise Mehner-Breitfeld and Natalia Tschowri and Thomas Br{\"u}ser",

note = "Publisher Copyright: Copyright {\textcopyright} 2025 Schwarzkopf, Viveros, Burdur, Mehner-Breitfeld, Tschowri and Br{\"u}ser.",

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doi = "10.3389/fmicb.2025.1579756",

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T1 - The short cytoplasmic region of phage T4 holin is essential for the transition from impermeable membrane protein complexes to permeable pores

AU - Schwarzkopf, Jan Michel Frederik

AU - Viveros, Ruth Paola

AU - Burdur, Ali Nazmi

AU - Mehner-Breitfeld, Denise

AU - Tschowri, Natalia

AU - Brüser, Thomas

PY - 2025/5/30

Y1 - 2025/5/30

N2 - Virulent as well as temperate phages usually require lysis of bacteria to release their progeny into the surrounding. Double-stranded DNA phages achieve lysis by phage-encoded endolysins that degrade the bacterial cell wall. Endolysins cross the cytoplasmic membrane by the aid of phage-encoded hole-forming membrane proteins, the holins. Canonical holins have been shown to multimerize and form very large holes in membranes, and it is believed that these holes enable a non-specific release of endolysins from cytoplasm. We studied these aspects with Escherichia coli and the phage T4 model lysis system, consisting of the holin T and the endolysin E. By following the endolysin function in a microfluidic chamber with mEGFP-fused holin, we found that large multimerizations were not required for endolysin release. Moreover, while we found in further analyses of this construct that the periplasmic globular domain was not required for hole formation and thus likely serves only regulatory functions, the short cytoplasmic domain was essential for hole formation. A truncation as well as single point mutations abolished hole formation without affecting holin interactions. In agreement with this, AlphaFold 3 indicates that rings of holin T dimers can form aqueous holes that require a conformational switch of the N-terminal cytoplasmic amphipathic helix to a trans-membrane orientation inside the rings. Our data indicate that already small holin assemblies enable endolysin-mediated cell lysis, although large multimers may be formed in the absence of endolysins due to the clustering of such assemblies. Further, we provide a convincing structural model of a ring-shaped holin T complex that can form an aqueous pore of sufficient diameter to permit endolysin release.

AB - Virulent as well as temperate phages usually require lysis of bacteria to release their progeny into the surrounding. Double-stranded DNA phages achieve lysis by phage-encoded endolysins that degrade the bacterial cell wall. Endolysins cross the cytoplasmic membrane by the aid of phage-encoded hole-forming membrane proteins, the holins. Canonical holins have been shown to multimerize and form very large holes in membranes, and it is believed that these holes enable a non-specific release of endolysins from cytoplasm. We studied these aspects with Escherichia coli and the phage T4 model lysis system, consisting of the holin T and the endolysin E. By following the endolysin function in a microfluidic chamber with mEGFP-fused holin, we found that large multimerizations were not required for endolysin release. Moreover, while we found in further analyses of this construct that the periplasmic globular domain was not required for hole formation and thus likely serves only regulatory functions, the short cytoplasmic domain was essential for hole formation. A truncation as well as single point mutations abolished hole formation without affecting holin interactions. In agreement with this, AlphaFold 3 indicates that rings of holin T dimers can form aqueous holes that require a conformational switch of the N-terminal cytoplasmic amphipathic helix to a trans-membrane orientation inside the rings. Our data indicate that already small holin assemblies enable endolysin-mediated cell lysis, although large multimers may be formed in the absence of endolysins due to the clustering of such assemblies. Further, we provide a convincing structural model of a ring-shaped holin T complex that can form an aqueous pore of sufficient diameter to permit endolysin release.

KW - endolysins

KW - Escherichia coli

KW - holins

KW - membrane proteins

KW - phage lysis

KW - phages

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DO - 10.3389/fmicb.2025.1579756

M3 - Article

AN - SCOPUS:105007974474

VL - 16

JO - Frontiers in Microbiology

JF - Frontiers in Microbiology

SN - 1664-302X

M1 - 1579756

ER -

Research@Leibniz University

The short cytoplasmic region of phage T4 holin is essential for the transition from impermeable membrane protein complexes to permeable pores

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