Diaza-anthracene Antibiotics from a Freshwater-Derived Actinomycete with Selective Antibacterial Activity toward Mycobacterium tuberculosis

Michael W. Mullowney; Chang Hwa Hwang; Andrew G. Newsome; Xiaomei Wei; Urszula Tanouye; Baojie Wan; Skylar Carlson; Nanthida Joy Barranis; Eoghainín Ó Hainmhire; Wei Lun Chen; Kalyanaraman Krishnamoorthy; John White; Rachel Blair; Hyunwoo Lee; Joanna E. Burdette; Pradipsinh K. Rathod; Tanya Parish; Sanghyun Cho; Scott G. Franzblau; Brian T. Murphy

doi:10.1021/acsinfecdis.5b00005

Diaza-anthracene Antibiotics from a Freshwater-Derived Actinomycete with Selective Antibacterial Activity toward Mycobacterium tuberculosis

Michael W. Mullowney
, Chang Hwa Hwang
, Andrew G. Newsome
, Xiaomei Wei
, Urszula Tanouye
, Baojie Wan
, Skylar Carlson
, Nanthida Joy Barranis
, Eoghainín Ó Hainmhire
, Wei Lun Chen
, Kalyanaraman Krishnamoorthy
, John White
, Rachel Blair
, Hyunwoo Lee
, Joanna E. Burdette
, Pradipsinh K. Rathod
, Tanya Parish
, Sanghyun Cho
, Scott G. Franzblau
, Brian T. Murphy

University of Illinois at Chicago
University of Washington
Infectious Disease Research Institute
TB Discovery Research

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

36 Citations (Scopus)

Abstract

Multidrug- and extensively drug-resistant strains of Mycobacterium tuberculosis are resistant to first- and second-line drug regimens and resulted in 210,000 fatalities in 2013. In the current study, we screened a library of aquatic bacterial natural product fractions for their ability to inhibit this pathogen. A fraction from a Lake Michigan bacterium exhibited significant inhibitory activity, from which we characterized novel diazaquinomycins H and J. This antibiotic class displayed an in vitro activity profile similar or superior to clinically used anti-tuberculosis agents and maintained this potency against a panel of drug-resistant M. tuberculosis strains. Importantly, these are among the only freshwater-derived actinomycete bacterial metabolites described to date. Further in vitro profiling against a broad panel of bacteria indicated that this antibiotic class selectively targets M. tuberculosis. Additionally, in the case of this pathogen we present evidence counter to previous reports that claim the diazaquinomycins target thymidylate synthase in Gram-positive bacteria. Thus, we establish freshwater environments as potential sources for novel antibiotic leads and present the diazaquinomycins as potent and selective inhibitors of M. tuberculosis.

Original language	English
Pages (from-to)	168-174
Number of pages	7
Journal	ACS Infectious Diseases
Volume	1
Issue number	4
DOIs	https://doi.org/10.1021/acsinfecdis.5b00005
Publication status	Published - 8 Mar 2015
Externally published	Yes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

actinobacteria
antibiotic
diazaquinomycin
drug discovery
Great Lakes
natural products

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10.1021/acsinfecdis.5b00005

Cite this

Mullowney, M. W., Hwang, C. H., Newsome, A. G., Wei, X., Tanouye, U., Wan, B., Carlson, S., Barranis, N. J., Ó Hainmhire, E., Chen, W. L., Krishnamoorthy, K., White, J., Blair, R., Lee, H., Burdette, J. E., Rathod, P. K., Parish, T., Cho, S., Franzblau, S. G., & Murphy, B. T. (2015). Diaza-anthracene Antibiotics from a Freshwater-Derived Actinomycete with Selective Antibacterial Activity toward Mycobacterium tuberculosis. ACS Infectious Diseases, 1(4), 168-174. https://doi.org/10.1021/acsinfecdis.5b00005

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title = "Diaza-anthracene Antibiotics from a Freshwater-Derived Actinomycete with Selective Antibacterial Activity toward Mycobacterium tuberculosis",

abstract = "Multidrug- and extensively drug-resistant strains of Mycobacterium tuberculosis are resistant to first- and second-line drug regimens and resulted in 210,000 fatalities in 2013. In the current study, we screened a library of aquatic bacterial natural product fractions for their ability to inhibit this pathogen. A fraction from a Lake Michigan bacterium exhibited significant inhibitory activity, from which we characterized novel diazaquinomycins H and J. This antibiotic class displayed an in vitro activity profile similar or superior to clinically used anti-tuberculosis agents and maintained this potency against a panel of drug-resistant M. tuberculosis strains. Importantly, these are among the only freshwater-derived actinomycete bacterial metabolites described to date. Further in vitro profiling against a broad panel of bacteria indicated that this antibiotic class selectively targets M. tuberculosis. Additionally, in the case of this pathogen we present evidence counter to previous reports that claim the diazaquinomycins target thymidylate synthase in Gram-positive bacteria. Thus, we establish freshwater environments as potential sources for novel antibiotic leads and present the diazaquinomycins as potent and selective inhibitors of M. tuberculosis.",

keywords = "actinobacteria, antibiotic, diazaquinomycin, drug discovery, Great Lakes, natural products",

author = "Mullowney, \{Michael W.\} and Hwang, \{Chang Hwa\} and Newsome, \{Andrew G.\} and Xiaomei Wei and Urszula Tanouye and Baojie Wan and Skylar Carlson and Barranis, \{Nanthida Joy\} and \{{\'O} Hainmhire\}, Eoghain{\'i}n and Chen, \{Wei Lun\} and Kalyanaraman Krishnamoorthy and John White and Rachel Blair and Hyunwoo Lee and Burdette, \{Joanna E.\} and Rathod, \{Pradipsinh K.\} and Tanya Parish and Sanghyun Cho and Franzblau, \{Scott G.\} and Murphy, \{Brian T.\}",

year = "2015",

month = mar,

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doi = "10.1021/acsinfecdis.5b00005",

language = "English",

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Mullowney, MW, Hwang, CH, Newsome, AG, Wei, X, Tanouye, U, Wan, B, Carlson, S, Barranis, NJ, Ó Hainmhire, E, Chen, WL, Krishnamoorthy, K, White, J, Blair, R, Lee, H, Burdette, JE, Rathod, PK, Parish, T, Cho, S, Franzblau, SG & Murphy, BT 2015, 'Diaza-anthracene Antibiotics from a Freshwater-Derived Actinomycete with Selective Antibacterial Activity toward Mycobacterium tuberculosis', ACS Infectious Diseases, vol. 1, no. 4, pp. 168-174. https://doi.org/10.1021/acsinfecdis.5b00005

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T1 - Diaza-anthracene Antibiotics from a Freshwater-Derived Actinomycete with Selective Antibacterial Activity toward Mycobacterium tuberculosis

AU - Mullowney, Michael W.

AU - Hwang, Chang Hwa

AU - Newsome, Andrew G.

AU - Wei, Xiaomei

AU - Tanouye, Urszula

AU - Wan, Baojie

AU - Carlson, Skylar

AU - Barranis, Nanthida Joy

AU - Ó Hainmhire, Eoghainín

AU - Chen, Wei Lun

AU - Krishnamoorthy, Kalyanaraman

AU - White, John

AU - Blair, Rachel

AU - Lee, Hyunwoo

AU - Burdette, Joanna E.

AU - Rathod, Pradipsinh K.

AU - Parish, Tanya

AU - Cho, Sanghyun

AU - Franzblau, Scott G.

AU - Murphy, Brian T.

PY - 2015/3/8

Y1 - 2015/3/8

N2 - Multidrug- and extensively drug-resistant strains of Mycobacterium tuberculosis are resistant to first- and second-line drug regimens and resulted in 210,000 fatalities in 2013. In the current study, we screened a library of aquatic bacterial natural product fractions for their ability to inhibit this pathogen. A fraction from a Lake Michigan bacterium exhibited significant inhibitory activity, from which we characterized novel diazaquinomycins H and J. This antibiotic class displayed an in vitro activity profile similar or superior to clinically used anti-tuberculosis agents and maintained this potency against a panel of drug-resistant M. tuberculosis strains. Importantly, these are among the only freshwater-derived actinomycete bacterial metabolites described to date. Further in vitro profiling against a broad panel of bacteria indicated that this antibiotic class selectively targets M. tuberculosis. Additionally, in the case of this pathogen we present evidence counter to previous reports that claim the diazaquinomycins target thymidylate synthase in Gram-positive bacteria. Thus, we establish freshwater environments as potential sources for novel antibiotic leads and present the diazaquinomycins as potent and selective inhibitors of M. tuberculosis.

AB - Multidrug- and extensively drug-resistant strains of Mycobacterium tuberculosis are resistant to first- and second-line drug regimens and resulted in 210,000 fatalities in 2013. In the current study, we screened a library of aquatic bacterial natural product fractions for their ability to inhibit this pathogen. A fraction from a Lake Michigan bacterium exhibited significant inhibitory activity, from which we characterized novel diazaquinomycins H and J. This antibiotic class displayed an in vitro activity profile similar or superior to clinically used anti-tuberculosis agents and maintained this potency against a panel of drug-resistant M. tuberculosis strains. Importantly, these are among the only freshwater-derived actinomycete bacterial metabolites described to date. Further in vitro profiling against a broad panel of bacteria indicated that this antibiotic class selectively targets M. tuberculosis. Additionally, in the case of this pathogen we present evidence counter to previous reports that claim the diazaquinomycins target thymidylate synthase in Gram-positive bacteria. Thus, we establish freshwater environments as potential sources for novel antibiotic leads and present the diazaquinomycins as potent and selective inhibitors of M. tuberculosis.

KW - actinobacteria

KW - antibiotic

KW - diazaquinomycin

KW - drug discovery

KW - Great Lakes

KW - natural products

U2 - 10.1021/acsinfecdis.5b00005

DO - 10.1021/acsinfecdis.5b00005

M3 - Article

AN - SCOPUS:84969185783

SN - 2373-8227

VL - 1

SP - 168

EP - 174

JO - ACS Infectious Diseases

JF - ACS Infectious Diseases

IS - 4

ER -

Diaza-anthracene Antibiotics from a Freshwater-Derived Actinomycete with Selective Antibacterial Activity toward Mycobacterium tuberculosis

Abstract

UN SDGs

Keywords

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