Paraquat and nitrofurantoin inhibit growth of<i>escherichia coli</i>by inducing stringency

Seither, Richard L.; Brown, Olen R.

doi:10.1080/15287398409530625

Cited by 12 publications

(6 citation statements)

References 18 publications

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“…Seither and Brown (46) reported that growth inhibition of E. coli by paraquat, a herbicide, and nitrofurantoin, an antibiotic, was induced by the stringent response. Both compounds are believed to block biosynthetic pathways of specific amino acids and cause amino acid starvation in the cells.…”

Section: Resultsmentioning

confidence: 99%

Growth inhibition of putrefactive anaerobe 3679 caused by stringent-type response induced by protonophoric activity of sorbic acid

RONNING¹,

Frank²

1987

Appl Environ Microbiol

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The inhibitory effects of potassium sorbate on the bioenergetics, phenylalanine uptake, protein synthesis, and certain aspects of cell regulation were examined in putrefactive anaerobe 3679. Undissociated sorbic acid appeared to act as a protonophore by lowering the intracellular pH and dissipating the proton motive force of the membrane. Sorbate inhibited the uptake of phenylalanine, decreased the rate of protein synthesis, and altered patterns of phosphorylated nucleotide accumulation, resulting in increased intracellular concentrations of GTP, ppGpp, and an unidentified compound (possibly pppGpp). The addition of a noninhibitory amount of tetracycline released the inhibition of growth by sorbate. Based on these results, we concluded that the inhibition of putrefactive anaerobe 3679 by sorbate resulted from a stringent-type regulatory response induced by the protonophoric activity of sorbic acid.

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Section: Resultsmentioning

confidence: 99%

Growth inhibition of putrefactive anaerobe 3679 caused by stringent-type response induced by protonophoric activity of sorbic acid

RONNING¹,

Frank²

1987

Appl Environ Microbiol

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“…The stringency response is defined as intracellular accumulation of guanosine 5'-diphosphate 3'-diphosphate, which is a regulatory inhibitor of biosynthetic processes in bacteria (25). Nitrofurantoin blocks synthesis of branchedchain amino acids such as valine and leucine (26). The observed decrease in the MIC of nitrofurantoin for a clinical bacterial isolate (E. coli serotype 018) during hyperoxic exposure may be due to a combination of these mechanisms.…”

Section: Discussionmentioning

confidence: 97%

“…This oxygen-derived free radical may undergo further reduction to form H202, which is toxic for bacteria. Hydrogen peroxide may take part in the Fenton reaction, where it is converted to the highly reactive hydroxyl radical (16 (25,26). The stringency response is defined as intracellular accumulation of guanosine 5'-diphosphate 3'-diphosphate, which is a regulatory inhibitor of biosynthetic processes in bacteria (25).…”

Section: Discussionmentioning

confidence: 99%

Hyperoxia and the antimicrobial susceptibility of Escherichia coli and Pseudomonas aeruginosa

Muhvich

Park

Myers

et al. 1989

Antimicrob Agents Chemother

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We have tested the ability of hyperoxia (98% 02-2% CO2 at 2.8 atmospheres absolute [ca. 284.6 kPa]) to enhance killing of Escherichia coli (serotype 018 or ATCC 25922) by nitrofurantoin, sulfamethoxazole, trimethoprim, gentamicin, and tobramycin. We have also looked for interactions between hyperoxia and the aminoglycosides against Pseudomonas aeruginosa ATCC 27853. Hyperoxia significantly enhanced bacteriostatic activity of nitrofurantoin and trimethoprim as measured by MIC testing. The possibility exists that these effects might be due to the method required to test MICs under hyperoxic conditions rather than to the effect of hyperoxia itself. In addition, hyperoxia enhanced killing of bacteria by trimethoprim as measured by MBC testing. Hyperoxia decreased numbers of E. coli by 1.3 loglo and P. aeruginosa by 2.7 log1o in cationsupplemented Mueller-Hinton broth medium. The bacteriostatic effects of hyperoxia did not affect MICs of gentamicin or tobramycin. The lack of interaction between hyperoxia and gentamicin or tobramycin was confirmed by determining the number of viable bacteria remaining after 24 h of exposure to hyperoxia by using a pour plate method. We conclude that hyperoxia potentiates the antimicrobial activity of the reductionoxidation-cycling antibiotic tested (nitrofurantoin) and of one of the antimetabolites tested (trimethoprim). Hyperoxia does not enhance the bactericidal effects of gentamicin and tobramycin, which require oxidative metabolism for transport into bacterial cells.

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“…SB 205952 therefore appears to have a second mechanism of action which induces stringency but which is independent of IRS inhibition. Nitrofurantoin and related compounds (27,38) are among the agents known to invoke ppGpp accumulation and stringency, and oxidative inactivation of dihydroxyacid dehydratase has been implicated (38). This enzyme is a key component of the isoleucine biosynthetic pathway in which it functions to convert ␣,␤-dihydroxy-␤-methylvalerate to ␣-keto-␤-methylvalerate (41).…”

Section: Discussionmentioning

confidence: 99%

SB 205952, a novel semisynthetic monic acid analog with at least two modes of action

Wilson

Oliva

Cassels

et al. 1995

Antimicrob Agents Chemother

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The biological properties of SB 205952, a nitrofuryl oxazole derivative of monic acid, differ from those of the closely related antibacterial agent mupirocin. Compared with mupirocin, SB 205952 has increased antimicrobial potency, an extended spectrum including mupirocin-resistant staphylococci, and rapid bactericidal activity. SB 205952, like mupirocin, is a potent inhibitor of bacterial isoleucyl-tRNA synthetase (IRS) in mupirocinsusceptible organisms but does not inhibit IRS from mupirocin-resistant staphylococci, indicating that SB 205952 has more than one mechanism of action. SB 205952 rapidly inhibits protein, RNA, and DNA syntheses in mupirocin-susceptible and mupirocin-resistant staphylococci. In each case, the effect on RNA synthesis is relaxed by treatment with chloramphenicol, indicating that inhibition of RNA synthesis is probably a secondary consequence of stringent control. It is proposed that SB 205952 possesses one or more mechanisms of action in addition to IRS inhibition, probably mediated by its nitrofuryl component.

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Paraquat and nitrofurantoin inhibit growth ofescherichia coliby inducing stringency

Cited by 12 publications

References 18 publications

Growth inhibition of putrefactive anaerobe 3679 caused by stringent-type response induced by protonophoric activity of sorbic acid

Growth inhibition of putrefactive anaerobe 3679 caused by stringent-type response induced by protonophoric activity of sorbic acid

Hyperoxia and the antimicrobial susceptibility of Escherichia coli and Pseudomonas aeruginosa

SB 205952, a novel semisynthetic monic acid analog with at least two modes of action

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