α-Amino diphenyl phosphonates as novel inhibitors of Escherichia coli ClpP protease

Carlos Moreno-Cinos; Elisa Sassetti; Irene G. Salado; Gesa Witt; Siham Benramdane; Laura Reinhardt; Cristina D. Cruz; Jurgen Joossens; Pieter Van der Veken; Heike Brötz-Oesterhelt; Päivi Sirpa Marjaana Tammela; Mathias Winterhalter; Philip Gribbon; Björn Windshügel; Koen Augustyns

doi:10.1021/acs.jmedchem.8b01466

α-Amino diphenyl phosphonates as novel inhibitors of Escherichia coli ClpP protease

Carlos Moreno-Cinos, Elisa Sassetti, Irene G. Salado, Gesa Witt, Siham Benramdane, Laura Reinhardt, Cristina D. Cruz, Jurgen Joossens, Pieter Van der Veken, Heike Brötz-Oesterhelt, Päivi Sirpa Marjaana Tammela, Mathias Winterhalter, Philip Gribbon, Björn Windshügel, Koen Augustyns

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

Abstract

Increased Gram-negative bacteria resistance to antibiotics is becoming a global problem, and new classes of antibiotics with novel mechanisms of action are required. The caseinolytic protease subunit P (ClpP) is a serine protease conserved among bacteria that is considered as an interesting drug target. ClpP function is involved in protein turnover and homeostasis, stress response, and virulence among other processes. The focus of this study was to identify new inhibitors of Escherichia coli ClpP and to understand their mode of action. A focused library of serine protease inhibitors based on diaryl phosphonate warheads was tested for ClpP inhibition, and a chemical exploration around the hit compounds was conducted. Altogether, 14 new potent inhibitors of E. coli ClpP were identified. Compounds 85 and 92 emerged as most interesting compounds from this study due to their potency and, respectively, to its moderate but consistent antibacterial properties as well as the favorable cytotoxicity profile.

Original language	English
Journal	Journal of Medicinal Chemistry
Volume	62
Issue number	2
Pages (from-to)	774-797
Number of pages	24
ISSN	0022-2623
DOIs	https://doi.org/10.1021/acs.jmedchem.8b01466
Publication status	Published - 24 Jan 2019
MoE publication type	A1 Journal article-refereed

Fields of Science

317 Pharmacy
116 Chemical sciences
BETA-LACTONES
LISTERIA-MONOCYTOGENES
PLASMINOGEN-ACTIVATOR
STAPHYLOCOCCUS-AUREUS
POTENT INHIBITORS
SERINE-PROTEASE
VIRULENCE
CHYMOTRYPSIN
ANALOGS
ACID

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10.1021/acs.jmedchem.8b01466

Moreno-Sassetti_Manuscript_181220Accepted author manuscript, 2.75 MB

New antimicrobials against Gram-positive bacteria
Tammela, P. & Durante Cruz, C.
01/10/2016 → 30/09/2018
Project: Research project
INTEGRATE: Interdisciplinary Training Network for Validation of Gram-negative Antibacterial Targets (H2020-MCSA-ITN-2014)
Tammela, P., Peltonen, K. & Gatta, V.
European Commission / Horizon 2020
01/01/2015 → 31/12/2018
Project: Research project
Phenotypic biosensor-based HTS and mode of action analysis by metabolomics and transcriptomics for enhancing antimicrobial drug discovery against Gram-negative bacteria
Tammela, P.
01/09/2014 → 31/08/2019
Project: Research project

Cite this

Moreno-Cinos, C., Sassetti, E., Salado, I. G., Witt, G., Benramdane, S., Reinhardt, L., Cruz, C. D., Joossens, J., Van der Veken, P., Brötz-Oesterhelt, H., Tammela, P. S. M., Winterhalter, M., Gribbon, P., Windshügel, B., & Augustyns, K. (2019). α-Amino diphenyl phosphonates as novel inhibitors of Escherichia coli ClpP protease. Journal of Medicinal Chemistry, 62(2), 774-797. https://doi.org/10.1021/acs.jmedchem.8b01466

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title = "α-Amino diphenyl phosphonates as novel inhibitors of Escherichia coli ClpP protease",

abstract = "Increased Gram-negative bacteria resistance to antibiotics is becoming a global problem, and new classes of antibiotics with novel mechanisms of action are required. The caseinolytic protease subunit P (ClpP) is a serine protease conserved among bacteria that is considered as an interesting drug target. ClpP function is involved in protein turnover and homeostasis, stress response, and virulence among other processes. The focus of this study was to identify new inhibitors of Escherichia coli ClpP and to understand their mode of action. A focused library of serine protease inhibitors based on diaryl phosphonate warheads was tested for ClpP inhibition, and a chemical exploration around the hit compounds was conducted. Altogether, 14 new potent inhibitors of E. coli ClpP were identified. Compounds 85 and 92 emerged as most interesting compounds from this study due to their potency and, respectively, to its moderate but consistent antibacterial properties as well as the favorable cytotoxicity profile.",

keywords = "317 Pharmacy, 116 Chemical sciences, BETA-LACTONES, LISTERIA-MONOCYTOGENES, PLASMINOGEN-ACTIVATOR, STAPHYLOCOCCUS-AUREUS, POTENT INHIBITORS, SERINE-PROTEASE, VIRULENCE, CHYMOTRYPSIN, ANALOGS, ACID",

author = "Carlos Moreno-Cinos and Elisa Sassetti and Salado, {Irene G.} and Gesa Witt and Siham Benramdane and Laura Reinhardt and Cruz, {Cristina D.} and Jurgen Joossens and {Van der Veken}, Pieter and Heike Br{\"o}tz-Oesterhelt and Tammela, {P{\"a}ivi Sirpa Marjaana} and Mathias Winterhalter and Philip Gribbon and Bj{\"o}rn Windsh{\"u}gel and Koen Augustyns",

year = "2019",

month = jan,

day = "24",

doi = "10.1021/acs.jmedchem.8b01466",

language = "English",

volume = "62",

pages = "774--797",

journal = "Journal of Medicinal Chemistry",

issn = "0022-2623",

publisher = "American Chemical Society",

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Moreno-Cinos, C, Sassetti, E, Salado, IG, Witt, G, Benramdane, S, Reinhardt, L, Cruz, CD, Joossens, J, Van der Veken, P, Brötz-Oesterhelt, H, Tammela, PSM, Winterhalter, M, Gribbon, P, Windshügel, B & Augustyns, K 2019, 'α-Amino diphenyl phosphonates as novel inhibitors of Escherichia coli ClpP protease', Journal of Medicinal Chemistry, vol. 62, no. 2, pp. 774-797. https://doi.org/10.1021/acs.jmedchem.8b01466

TY - JOUR

T1 - α-Amino diphenyl phosphonates as novel inhibitors of Escherichia coli ClpP protease

AU - Moreno-Cinos, Carlos

AU - Sassetti, Elisa

AU - Salado, Irene G.

AU - Witt, Gesa

AU - Benramdane, Siham

AU - Reinhardt, Laura

AU - Cruz, Cristina D.

AU - Joossens, Jurgen

AU - Van der Veken, Pieter

AU - Brötz-Oesterhelt, Heike

AU - Tammela, Päivi Sirpa Marjaana

AU - Winterhalter, Mathias

AU - Gribbon, Philip

AU - Windshügel, Björn

AU - Augustyns, Koen

PY - 2019/1/24

Y1 - 2019/1/24

N2 - Increased Gram-negative bacteria resistance to antibiotics is becoming a global problem, and new classes of antibiotics with novel mechanisms of action are required. The caseinolytic protease subunit P (ClpP) is a serine protease conserved among bacteria that is considered as an interesting drug target. ClpP function is involved in protein turnover and homeostasis, stress response, and virulence among other processes. The focus of this study was to identify new inhibitors of Escherichia coli ClpP and to understand their mode of action. A focused library of serine protease inhibitors based on diaryl phosphonate warheads was tested for ClpP inhibition, and a chemical exploration around the hit compounds was conducted. Altogether, 14 new potent inhibitors of E. coli ClpP were identified. Compounds 85 and 92 emerged as most interesting compounds from this study due to their potency and, respectively, to its moderate but consistent antibacterial properties as well as the favorable cytotoxicity profile.

AB - Increased Gram-negative bacteria resistance to antibiotics is becoming a global problem, and new classes of antibiotics with novel mechanisms of action are required. The caseinolytic protease subunit P (ClpP) is a serine protease conserved among bacteria that is considered as an interesting drug target. ClpP function is involved in protein turnover and homeostasis, stress response, and virulence among other processes. The focus of this study was to identify new inhibitors of Escherichia coli ClpP and to understand their mode of action. A focused library of serine protease inhibitors based on diaryl phosphonate warheads was tested for ClpP inhibition, and a chemical exploration around the hit compounds was conducted. Altogether, 14 new potent inhibitors of E. coli ClpP were identified. Compounds 85 and 92 emerged as most interesting compounds from this study due to their potency and, respectively, to its moderate but consistent antibacterial properties as well as the favorable cytotoxicity profile.

KW - 317 Pharmacy

KW - 116 Chemical sciences

KW - BETA-LACTONES

KW - LISTERIA-MONOCYTOGENES

KW - PLASMINOGEN-ACTIVATOR

KW - STAPHYLOCOCCUS-AUREUS

KW - POTENT INHIBITORS

KW - SERINE-PROTEASE

KW - VIRULENCE

KW - CHYMOTRYPSIN

KW - ANALOGS

KW - ACID

U2 - 10.1021/acs.jmedchem.8b01466

DO - 10.1021/acs.jmedchem.8b01466

M3 - Article

VL - 62

SP - 774

EP - 797

JO - Journal of Medicinal Chemistry

JF - Journal of Medicinal Chemistry

SN - 0022-2623

IS - 2

ER -

α-Amino diphenyl phosphonates as novel inhibitors of Escherichia coli ClpP protease

Abstract

Fields of Science

Access to Document

Projects

New antimicrobials against Gram-positive bacteria

INTEGRATE: Interdisciplinary Training Network for Validation of Gram-negative Antibacterial Targets (H2020-MCSA-ITN-2014)

Phenotypic biosensor-based HTS and mode of action analysis by metabolomics and transcriptomics for enhancing antimicrobial drug discovery against Gram-negative bacteria

Cite this