John D. Turnbull scite author profile

Toxicity testing in AS52 cells (24-hr exposures) gave LC50 values of 2 to 130 pg Ni/ml for particulate nickel compounds and 45 to 60 pg Ni/ml for water-soluble salts (NiCI2, NiSO4, Ni(CH3COO)2). The Ni(OH)2, NiCO3, and sulfides (Ni3S2, Ni7S6, "amorphous NiS") exhibited similar toxicities (LC50's of 2 to 8 pg Ni/ml), while three nickel oxides were more variable and less toxic (LC50's of 18 to 130 pg Ni/ml). Most compounds displayed nuclear to cytoplasmic nickel ratios of -1:1.5 to 1:5 (except -1:20 for nickel salts). At the LC50's, a 75-fold range in exposure levels occurred compared to a 1 0-fold range in cytoplasmic and nuclear nickel concentrations, [Nil. Cellular nickel distribution indicated three groupings: inert compounds (green NiO, lithium nickel oxide, relatively low nuclear and cytosolic [Nil); water-soluble salts (very low nuclear [Nil; high cytosolic [Nil), and slightly soluble compounds (relatively high cytosolic and nuclear [Nil). Nickel compounds are considered to be only weak or equivocal mutagens. In this study, a low but significant increase in mutation rate at the gpt locus was shown. Although the results would not be sufficient to deem nickel compounds mutagenic by traditional criteria, characterization by PCR analysis indicated that the spontaneous and nickel-induced mutants exhibited different and compound-specific mutational spectra (thus confirming nickel compound involvement). The results reported illustrate some of the methodologic problems involved in testing "weak" mutagens and indicate that alternative approaches may be necessary in classifying the mutagenicity of nickel and other compounds. -Environ Health Perspect 1 02(Suppl 3): 69-79 (1994).

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Polymerase gamma mutator mice rely on increased glycolytic flux for energy production

Saleem

Safdar

Kitaoka

et al. 2015

Mitochondrion

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Characterization of nickel-induced mutations

Rossetto

Turnbull

Nieboer

1994

Science of The Total Environment

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Effect of ascorbic acid on heme metabolism in hepatic microsomes

Omaye¹,

Turnbull²

1980

Life Sciences

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John D. Turnbull

[1] Selected methods for the determination of ascorbic acid in animal cells, tissues, and fluids

Toxicity, uptake, and mutagenicity of particulate and soluble nickel compounds.

Polymerase gamma mutator mice rely on increased glycolytic flux for energy production

Characterization of nickel-induced mutations

Effect of ascorbic acid on heme metabolism in hepatic microsomes

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