Novel compounds that specifically bind and modulate MscL: insights into channel gating mechanisms

Robin Wray; Irene R Iscla; Zoltan Kovacs; Junmei Wang; Paul Blount

doi:10.1096/fj.201801628R

Novel compounds that specifically bind and modulate MscL: insights into channel gating mechanisms

Robin Wray, Irene R Iscla, Zoltan Kovacs, Junmei Wang, Paul Blount

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16 Scopus citations

Abstract

The bacterial mechanosensitive channel of large conductance (MscL) normally functions as an emergency release valve discharging cytoplasmic solutes upon osmotic stress. Opening the large pore of MscL inappropriately is detrimental to the cell, and thus it has been speculated to be a potential antibiotic target. Although MscL is one of the best studied mechanosensitive channels, no chemical that influenced bacterial growth by modulating MscL is known. We therefore used a high-throughput screen to identify compounds that slowed growth in an MscL-dependent manner. We characterized 2 novel sulfonamide compounds identified in the screen. We demonstrated that, although both increase MscL gating, one of these compounds does not work through the folate pathway, as other antimicrobial sulfonamides; indeed, the sulfonamide portion of the compound is not needed for activity. The only mode of action appears to be MscL activation. The binding pocket is where an α-helix runs along the cytoplasmic membrane and interacts with a neighboring subunit; analogous motifs have been observed in several prokaryotic and eukaryotic channels. The data not only demonstrate that MscL is a viable antibiotic target, but also give insight into the gating mechanisms of MscL, and they may have implications for developing agonists for other channels.—Wray, R., Iscla, I., Kovacs, Z., Wang, J., Blount, P. Novel compounds that specifically bind and modulate MscL: insights into channel gating mechanisms. FASEB J. 33, 3180–3189 (2019). www.fasebj.org.

Original language	English (US)
Pages (from-to)	3180-3189
Number of pages	10
Journal	FASEB Journal
Volume	33
Issue number	3
DOIs	https://doi.org/10.1096/fj.201801628R
State	Published - Mar 1 2019

Keywords

antibiotic
mechanosensitive
osmoregulation

ASJC Scopus subject areas

Biotechnology
Biochemistry
Molecular Biology
Genetics

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10.1096/fj.201801628R

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title = "Novel compounds that specifically bind and modulate MscL: insights into channel gating mechanisms",

abstract = "The bacterial mechanosensitive channel of large conductance (MscL) normally functions as an emergency release valve discharging cytoplasmic solutes upon osmotic stress. Opening the large pore of MscL inappropriately is detrimental to the cell, and thus it has been speculated to be a potential antibiotic target. Although MscL is one of the best studied mechanosensitive channels, no chemical that influenced bacterial growth by modulating MscL is known. We therefore used a high-throughput screen to identify compounds that slowed growth in an MscL-dependent manner. We characterized 2 novel sulfonamide compounds identified in the screen. We demonstrated that, although both increase MscL gating, one of these compounds does not work through the folate pathway, as other antimicrobial sulfonamides; indeed, the sulfonamide portion of the compound is not needed for activity. The only mode of action appears to be MscL activation. The binding pocket is where an α-helix runs along the cytoplasmic membrane and interacts with a neighboring subunit; analogous motifs have been observed in several prokaryotic and eukaryotic channels. The data not only demonstrate that MscL is a viable antibiotic target, but also give insight into the gating mechanisms of MscL, and they may have implications for developing agonists for other channels.—Wray, R., Iscla, I., Kovacs, Z., Wang, J., Blount, P. Novel compounds that specifically bind and modulate MscL: insights into channel gating mechanisms. FASEB J. 33, 3180–3189 (2019). www.fasebj.org.",

keywords = "antibiotic, mechanosensitive, osmoregulation",

author = "Robin Wray and Iscla, {Irene R} and Zoltan Kovacs and Junmei Wang and Paul Blount",

note = "Funding Information: The authors thank Drs. Limin Yang (University of Texas, Southwestern Medical Center) and Andriy Anishkin (University of Maryland, College Park, MD, USA) for helpful suggestions and critical reading of the manuscript. This work was supported by U.S. National Institutes of Health (NIH) National Institute of General Medical Sciences (NIGMS) Grants R01 GM061028 and GM121780, and NIH National Institute of Biomedical Imaging and Bioengineering Grant P41-EB015908 (to Z.K.); Welch Foundation Grant 1–1420 (to P.B.). The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. The content is solely the responsibility of the authors and does not necessarily represent the official views of the NIH or other funding organizations. The authors declare no conflicts of interest. Publisher Copyright: {\textcopyright} FASEB",

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doi = "10.1096/fj.201801628R",

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AU - Wray, Robin

AU - Iscla, Irene R

AU - Kovacs, Zoltan

AU - Wang, Junmei

AU - Blount, Paul

N1 - Funding Information: The authors thank Drs. Limin Yang (University of Texas, Southwestern Medical Center) and Andriy Anishkin (University of Maryland, College Park, MD, USA) for helpful suggestions and critical reading of the manuscript. This work was supported by U.S. National Institutes of Health (NIH) National Institute of General Medical Sciences (NIGMS) Grants R01 GM061028 and GM121780, and NIH National Institute of Biomedical Imaging and Bioengineering Grant P41-EB015908 (to Z.K.); Welch Foundation Grant 1–1420 (to P.B.). The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. The content is solely the responsibility of the authors and does not necessarily represent the official views of the NIH or other funding organizations. The authors declare no conflicts of interest. Publisher Copyright: © FASEB

PY - 2019/3/1

Y1 - 2019/3/1

N2 - The bacterial mechanosensitive channel of large conductance (MscL) normally functions as an emergency release valve discharging cytoplasmic solutes upon osmotic stress. Opening the large pore of MscL inappropriately is detrimental to the cell, and thus it has been speculated to be a potential antibiotic target. Although MscL is one of the best studied mechanosensitive channels, no chemical that influenced bacterial growth by modulating MscL is known. We therefore used a high-throughput screen to identify compounds that slowed growth in an MscL-dependent manner. We characterized 2 novel sulfonamide compounds identified in the screen. We demonstrated that, although both increase MscL gating, one of these compounds does not work through the folate pathway, as other antimicrobial sulfonamides; indeed, the sulfonamide portion of the compound is not needed for activity. The only mode of action appears to be MscL activation. The binding pocket is where an α-helix runs along the cytoplasmic membrane and interacts with a neighboring subunit; analogous motifs have been observed in several prokaryotic and eukaryotic channels. The data not only demonstrate that MscL is a viable antibiotic target, but also give insight into the gating mechanisms of MscL, and they may have implications for developing agonists for other channels.—Wray, R., Iscla, I., Kovacs, Z., Wang, J., Blount, P. Novel compounds that specifically bind and modulate MscL: insights into channel gating mechanisms. FASEB J. 33, 3180–3189 (2019). www.fasebj.org.

AB - The bacterial mechanosensitive channel of large conductance (MscL) normally functions as an emergency release valve discharging cytoplasmic solutes upon osmotic stress. Opening the large pore of MscL inappropriately is detrimental to the cell, and thus it has been speculated to be a potential antibiotic target. Although MscL is one of the best studied mechanosensitive channels, no chemical that influenced bacterial growth by modulating MscL is known. We therefore used a high-throughput screen to identify compounds that slowed growth in an MscL-dependent manner. We characterized 2 novel sulfonamide compounds identified in the screen. We demonstrated that, although both increase MscL gating, one of these compounds does not work through the folate pathway, as other antimicrobial sulfonamides; indeed, the sulfonamide portion of the compound is not needed for activity. The only mode of action appears to be MscL activation. The binding pocket is where an α-helix runs along the cytoplasmic membrane and interacts with a neighboring subunit; analogous motifs have been observed in several prokaryotic and eukaryotic channels. The data not only demonstrate that MscL is a viable antibiotic target, but also give insight into the gating mechanisms of MscL, and they may have implications for developing agonists for other channels.—Wray, R., Iscla, I., Kovacs, Z., Wang, J., Blount, P. Novel compounds that specifically bind and modulate MscL: insights into channel gating mechanisms. FASEB J. 33, 3180–3189 (2019). www.fasebj.org.

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KW - osmoregulation

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Novel compounds that specifically bind and modulate MscL: insights into channel gating mechanisms

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Keywords

ASJC Scopus subject areas

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