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Robert C. Fahey

Researcher at University of California, San Diego

Publications -  109
Citations -  9016

Robert C. Fahey is an academic researcher from University of California, San Diego. The author has contributed to research in topics: Mycothiol & Glutathione. The author has an hindex of 53, co-authored 109 publications receiving 8663 citations. Previous affiliations of Robert C. Fahey include University of California & University of British Columbia.

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Journal ArticleDOI

Distribution of thiols in microorganisms: mycothiol is a major thiol in most actinomycetes.

TL;DR: The results, which indicate that MSH production is restricted to the actinomycetes, could have significant implications for the detection and treatment of infections with actinomers, especially those caused by mycobacteria.
Journal ArticleDOI

Occurrence of glutathione in bacteria.

TL;DR: Glutathione and soluble thiol content were examined in a broad spectrum of bacteria and the glutathione content of Escherichia coli increased significantly during transition from exponential to stationary phase.
Journal ArticleDOI

Analysis of biological thiols: Derivatization with monobromobimane and separation by reverse-phase high-performance liquid chromatography

TL;DR: Since monobromobimane has little fluorescence and reacts very selectively with thiols to produce fluorescent derivatives, crude extracts can be derivatized and analyzed without prepurification of the thiolS, the entire process requiring only 1 to 2 h.
Book ChapterDOI

Determination of low-molecular-weight thiols using monobromobimane fluorescent labeling and high-performance liquid chromatography.

TL;DR: This chapter describes methods for the preparation and high-performance liquid chromatography (HPLC) analysis of monobromobimane derivatives of low molecular weight thiols in extracts of biological samples and discusses typical problems encountered in the development and application of these methods.
Journal ArticleDOI

Biosynthesis and Functions of Mycothiol, the Unique Protective Thiol of Actinobacteria

TL;DR: Evidence suggests that several MSH biosynthetic and metabolic enzymes are potential targets for drugs against tuberculosis, and the functions of MSH in antibiotic-producing streptomycetes and in bioremediation are areas for future study.