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James S. Bus

Researcher at Research Triangle Park

Publications -  43
Citations -  2292

James S. Bus is an academic researcher from Research Triangle Park. The author has contributed to research in topics: Glutathione & Toxicity. The author has an hindex of 23, co-authored 42 publications receiving 2243 citations.

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Paraquat: model for oxidant-initiated toxicity.

TL;DR: Paraquat-induced pulmonary toxicity is a potentially useful model for evaluation of oxidant mechanisms of toxicity and characterization of the consequences of intracellular redox cycling of xenobiotics will no doubt provide basic information regarding the role of this phenomena in the development of chemical toxicity.
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Benzene disposition in the rat after exposure by inhalation.

TL;DR: It is indicated that free catechol and hydroquinone persist in bone marrow longer than benzene or free phenol.
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Paraquat toxicity: proposed mechanism of action involving lipid peroxidation.

TL;DR: Oxygen-tolerant rats, which increased activities of pulmonary enzymes which combat lipid peroxidation, were also tolerant to lethal doses of paraquat as indicated by an increased paraquats LT50, and rats chronically exposed to 100 ppm paraqu at in the water had elevated pulmonary activities of glucose-6-phosphate dehydrogenase and GSH reductase.
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The morphogenesis of testicular degeneration induced in rats by orally administered 2,5-hexanedione.

TL;DR: These studies indicate that the Sertoli cell is probably an initial target for 2,5-HD action in the testis, and it is likely that this cell is derived from fused spermatocytes or sPermatids.
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A proposed mechanism of benzene toxicity: Formation of reactive intermediates from polyphenol metabolites

TL;DR: A mechanism for benzene toxicity in which the formation of potentially cytotoxic metabolites, semiquin one, and quinone oxidation products and superoxide radicals, result from autoxidation of at least two polyphenol metabolites of benzene, hydroquinone, and 1,2,4-benzenetriol is supported.