Antimicrobial drug discovery against persisters

Wooseong Kim; Iliana Escobar; Beth Burgwyn Fuchs; Eleftherios Mylonakis

doi:10.1007/978-3-030-25241-0_12

Antimicrobial drug discovery against persisters

Wooseong Kim, Iliana Escobar, Beth Burgwyn Fuchs, Eleftherios Mylonakis

Houston Methodist

Research output: Chapter in Book/Report/Conference proceeding › Chapter

2 Scopus citations

Abstract

The efficacy of most currently prescribed antibiotics that target biosynthetic processes during cell growth or cellular uptake is energy dependent. However, because persisters are non-growing, dormant cell population with low-energy metabolic states (Conlon et al., Nature Microbiology, 1, 2016; Lewis, Annual Review of Microbiology, 64, 357, 2010; Shan et al., MBio, 8, 2017), conventional antibiotics fail to effectively eliminate bacterial persisters, which may lead to chronic and reoccurring infection (Lewis, Annual Review of Microbiology, 64, 357, 2010). The lack of antibiotics to treat infections caused by persisters entreats the urgency for developing new therapeutics effective against bacterial persisters. In response to this dire need, several strategies and anti-persister antimicrobials have been developed. Anti-persister strategies can be grouped into two approaches (1) direct killing of persisters through growth-independent targets and (2) converting persisters to antibiotic susceptible states by antibiotic adjuvants. In this chapter, we review growth-independent targets, such as bacterial proteases (Conlon, Nature, 503, 365–370, 2013), membrane lipid bilayers (Hurdle et al., Nature Reviews Microbiology, 9, 62–75, 2011), and bacterial DNA (Kwan et al., Environmental Microbiology, 2015). We also discuss a Caenorhabditis elegans-based screening strategy to identify membrane-active antimicrobials with relatively low cytotoxicity, which overcomes the membrane selectivity issue (Kim et al., ACS Infectious Diseases, 4, 1540–1545, 2018b, Nature, 556, 103–107, 2018c). Lastly, we review antibiotic adjuvants that resuscitate persisters to conventional antibiotic susceptible conditions (Allison et al., Nature, 473, 216–220, 2011). Included among these strategies, we explore the engineering of conventional antibiotics conjugated with drug carriers such as a peptide and an antibody that facilitate uptake or accessibility of antibiotics (Brezden et al., Journal of the American Chemical Society, 138, 10945–10949, 2016; Lehar et al., Nature, 527, 323–328, 2015; Schmidt et al., ACS Nano, 8, 8786–8793, 2014).

Original language	English (US)
Title of host publication	Persister Cells and Infectious Disease
Publisher	Springer International Publishing
Pages	273-295
Number of pages	23
ISBN (Electronic)	9783030252410
ISBN (Print)	9783030252403
DOIs	https://doi.org/10.1007/978-3-030-25241-0_12
State	Published - Jan 1 2019

Keywords

Anti-persister agents
Antibiotic adjuvants
Engineered antibiotics
Growth-independent targets
High-throughput screen
Membrane-active agents

ASJC Scopus subject areas

Medicine(all)
Immunology and Microbiology(all)

Access to Document

10.1007/978-3-030-25241-0_12

Cite this

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title = "Antimicrobial drug discovery against persisters",

abstract = "The efficacy of most currently prescribed antibiotics that target biosynthetic processes during cell growth or cellular uptake is energy dependent. However, because persisters are non-growing, dormant cell population with low-energy metabolic states (Conlon et al., Nature Microbiology, 1, 2016; Lewis, Annual Review of Microbiology, 64, 357, 2010; Shan et al., MBio, 8, 2017), conventional antibiotics fail to effectively eliminate bacterial persisters, which may lead to chronic and reoccurring infection (Lewis, Annual Review of Microbiology, 64, 357, 2010). The lack of antibiotics to treat infections caused by persisters entreats the urgency for developing new therapeutics effective against bacterial persisters. In response to this dire need, several strategies and anti-persister antimicrobials have been developed. Anti-persister strategies can be grouped into two approaches (1) direct killing of persisters through growth-independent targets and (2) converting persisters to antibiotic susceptible states by antibiotic adjuvants. In this chapter, we review growth-independent targets, such as bacterial proteases (Conlon, Nature, 503, 365–370, 2013), membrane lipid bilayers (Hurdle et al., Nature Reviews Microbiology, 9, 62–75, 2011), and bacterial DNA (Kwan et al., Environmental Microbiology, 2015). We also discuss a Caenorhabditis elegans-based screening strategy to identify membrane-active antimicrobials with relatively low cytotoxicity, which overcomes the membrane selectivity issue (Kim et al., ACS Infectious Diseases, 4, 1540–1545, 2018b, Nature, 556, 103–107, 2018c). Lastly, we review antibiotic adjuvants that resuscitate persisters to conventional antibiotic susceptible conditions (Allison et al., Nature, 473, 216–220, 2011). Included among these strategies, we explore the engineering of conventional antibiotics conjugated with drug carriers such as a peptide and an antibody that facilitate uptake or accessibility of antibiotics (Brezden et al., Journal of the American Chemical Society, 138, 10945–10949, 2016; Lehar et al., Nature, 527, 323–328, 2015; Schmidt et al., ACS Nano, 8, 8786–8793, 2014).",

keywords = "Anti-persister agents, Antibiotic adjuvants, Engineered antibiotics, Growth-independent targets, High-throughput screen, Membrane-active agents",

author = "Wooseong Kim and Iliana Escobar and Fuchs, {Beth Burgwyn} and Eleftherios Mylonakis",

note = "Publisher Copyright: {\textcopyright} Springer Nature Switzerland AG 2019.",

year = "2019",

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doi = "10.1007/978-3-030-25241-0_12",

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AU - Kim, Wooseong

AU - Escobar, Iliana

AU - Fuchs, Beth Burgwyn

AU - Mylonakis, Eleftherios

N1 - Publisher Copyright: © Springer Nature Switzerland AG 2019.

PY - 2019/1/1

Y1 - 2019/1/1

N2 - The efficacy of most currently prescribed antibiotics that target biosynthetic processes during cell growth or cellular uptake is energy dependent. However, because persisters are non-growing, dormant cell population with low-energy metabolic states (Conlon et al., Nature Microbiology, 1, 2016; Lewis, Annual Review of Microbiology, 64, 357, 2010; Shan et al., MBio, 8, 2017), conventional antibiotics fail to effectively eliminate bacterial persisters, which may lead to chronic and reoccurring infection (Lewis, Annual Review of Microbiology, 64, 357, 2010). The lack of antibiotics to treat infections caused by persisters entreats the urgency for developing new therapeutics effective against bacterial persisters. In response to this dire need, several strategies and anti-persister antimicrobials have been developed. Anti-persister strategies can be grouped into two approaches (1) direct killing of persisters through growth-independent targets and (2) converting persisters to antibiotic susceptible states by antibiotic adjuvants. In this chapter, we review growth-independent targets, such as bacterial proteases (Conlon, Nature, 503, 365–370, 2013), membrane lipid bilayers (Hurdle et al., Nature Reviews Microbiology, 9, 62–75, 2011), and bacterial DNA (Kwan et al., Environmental Microbiology, 2015). We also discuss a Caenorhabditis elegans-based screening strategy to identify membrane-active antimicrobials with relatively low cytotoxicity, which overcomes the membrane selectivity issue (Kim et al., ACS Infectious Diseases, 4, 1540–1545, 2018b, Nature, 556, 103–107, 2018c). Lastly, we review antibiotic adjuvants that resuscitate persisters to conventional antibiotic susceptible conditions (Allison et al., Nature, 473, 216–220, 2011). Included among these strategies, we explore the engineering of conventional antibiotics conjugated with drug carriers such as a peptide and an antibody that facilitate uptake or accessibility of antibiotics (Brezden et al., Journal of the American Chemical Society, 138, 10945–10949, 2016; Lehar et al., Nature, 527, 323–328, 2015; Schmidt et al., ACS Nano, 8, 8786–8793, 2014).

AB - The efficacy of most currently prescribed antibiotics that target biosynthetic processes during cell growth or cellular uptake is energy dependent. However, because persisters are non-growing, dormant cell population with low-energy metabolic states (Conlon et al., Nature Microbiology, 1, 2016; Lewis, Annual Review of Microbiology, 64, 357, 2010; Shan et al., MBio, 8, 2017), conventional antibiotics fail to effectively eliminate bacterial persisters, which may lead to chronic and reoccurring infection (Lewis, Annual Review of Microbiology, 64, 357, 2010). The lack of antibiotics to treat infections caused by persisters entreats the urgency for developing new therapeutics effective against bacterial persisters. In response to this dire need, several strategies and anti-persister antimicrobials have been developed. Anti-persister strategies can be grouped into two approaches (1) direct killing of persisters through growth-independent targets and (2) converting persisters to antibiotic susceptible states by antibiotic adjuvants. In this chapter, we review growth-independent targets, such as bacterial proteases (Conlon, Nature, 503, 365–370, 2013), membrane lipid bilayers (Hurdle et al., Nature Reviews Microbiology, 9, 62–75, 2011), and bacterial DNA (Kwan et al., Environmental Microbiology, 2015). We also discuss a Caenorhabditis elegans-based screening strategy to identify membrane-active antimicrobials with relatively low cytotoxicity, which overcomes the membrane selectivity issue (Kim et al., ACS Infectious Diseases, 4, 1540–1545, 2018b, Nature, 556, 103–107, 2018c). Lastly, we review antibiotic adjuvants that resuscitate persisters to conventional antibiotic susceptible conditions (Allison et al., Nature, 473, 216–220, 2011). Included among these strategies, we explore the engineering of conventional antibiotics conjugated with drug carriers such as a peptide and an antibody that facilitate uptake or accessibility of antibiotics (Brezden et al., Journal of the American Chemical Society, 138, 10945–10949, 2016; Lehar et al., Nature, 527, 323–328, 2015; Schmidt et al., ACS Nano, 8, 8786–8793, 2014).

KW - Anti-persister agents

KW - Antibiotic adjuvants

KW - Engineered antibiotics

KW - Growth-independent targets

KW - High-throughput screen

KW - Membrane-active agents

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ER -

Antimicrobial drug discovery against persisters

Abstract

Keywords

ASJC Scopus subject areas

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