Abstract
The effect of cadmium (Cd2+), mercury (Hg2+) and copper (Cu2+) was studied with partially purified flavokinase (ATP:riboflavin 5′-phosphotransferase EC 2.7.1.26) from rat liver. All the divalent heavy metal cations inhibited flavokinase activity in a concentration-dependent manner. The inhibitory effect of cadmium on the enzyme was completely reversed by increasing concentration, of Zinc (Zn2+) indicating a competition between Zn2+ and Cd2+ for binding with the enzyme. A competition between riboflavin and Cd2+ is also evident from the present investigation. These observations hint at the possibility that Zn2+ and Cd2+ probably compete for the same site on the enzyme where riboflavin binds. However, inhibition of flavokinase by Hg2+ could not be reversed by Zn2+. Our studies further reveal that hepatic flavokinase appears to contain an essential, accessible and functional thiol group(s) which is evident from a concentration dependent inhibition of activity by sulfhydryl reagent s like parachloromercuribenzoate (PCMB), 5,5′-dithiobis (2-nitrobenzoic acid)(DTNB), and N-ethylmaleimide (NEM). Inhibition of flavokinase by sulfhydryl reagents were protected, except in case of NEM inhibition, when the enzyme was incubated with thiol protectors like glutathione (GSH) and dithiothreitol (DTT). Furthermore, the enzyme could also be protected from the inhibitory effect of Cd2+ and Hg2+ by GSH and DTT suggesting that Cd2+ probably interacts with a reactive thiol group at or near the active site of enzyme in bringing about its inhibitory effect. (Mol Cell Biochem 167: 73-80, 1997)
This is a preview of subscription content, log in via an institution to check access.
Similar content being viewed by others
References
Cerletti P, Ipata P: Determination of riboflavin and its coenzymes in tissues. Biochem J 75: 119–124, 1960
McCormick DB: Flavokinase activity of rat tissues and masking effect of phosphatases. Proc Soc Exp Biol Med 107: 784–786, 1961
McCormick DB: The intracellular localization, partial purification, and properties of flavokinase from rat liver. J Biol Chem 237: 959–962, 1962
Rivlin RS, Langdon RG: Regulation of hepatic FAD levels by thyroid hormone. Advances Enz Regulation 4: 45–88, 1966
Rivlin RS: Regulation of flavoprotein enzymes in hypothyroidism and in riboflavin deficiency. Advances Enz Regulation 8: 239–250, 1970
Bandyopadhyay D, Chatterjee AK, Datta AG: Effect of cadmium treatment on hepatic flavin metabolism. J Nutr Biochem 4: 510–514, 1993
Kearney EB, Englard S: The enzymatic phosphorylation of riboflavin. J Biol Chem 193: 821–834, 1951
Mayhew SG, Wassink JH: A continuous fluorometric assay for flavokinase. Properties of flavokinase from Peptostreptococcus elsdeni. Biochim Biophys Acta 482: 341–347, 1976
Spencer R, Fisher J, Walsh C: Preparation, characterization, and chemical properties of the flavin co-enzyme analogues 5-Deazariboflavin, 5-Deazariboflavin ′-phosphate and 5-Deazariboflavin ′-diphosphate, 5-′—′-Adenosine ester. Biochemistry 15: 1043–1053, 1976
Kashchenko VE, Shaviovskii GM: Purification and properties of ribo-flavin kinase of Pichia guilliermondii. Biokhimiya 41: 376–383 (313– 319 in English translation), 1976
Mitsuda H, Tomozawa Y, Kawai F: Studies on plant flavokinase II. The purification and some properties of bean flavokinase. J Vitaminol 9: 142–148, 1963
Sadasivam S, Shanmugasundaram ERB: Studies on the flavokinase of Solanum nigrum L. Enzymologia 31: 203–208, 1966
Arsenis C, McCormick DB: Purification of liver flavokinase by column chromatography on flavin cellulose compounds. J Biol Chem 239: 3093–3097, 1964
Merrill AH Jr, McCormick DB: Affinity chromatographic purification and properties of flavokinase (ATP: riboflavin ′-phosphotransferase) from rat liver. J Biol Chem 255: 1335–1338, 1980
McCormick DB: Flavokinase from rat liver. In: DB McCormick and LD Wright (eds). Methods in Enzymology, XVIII Part B: 1971, pp 544–548
Lowry OH, Rosebrough NJ, Parr AR, Randall RJ: Protein measurement with folin phenol reagent. J Biol Chem 193: 265–275, 1951
Burch HB, Bessey OA, Lowry OH: Fluorometric measurement of ribo-flavin and its natural derivatives in small quantities of blood, serum and cells. J Biol Chem 175: 457–470, 1948
Huennekens FM, Felton SP: Preparation and enzymatic assay of FAD and FMN. In: SP Colowick and NO Kaplan (eds). Methods in Enzymology, Vol III: 1957, pp 950–959
McCormick DB, Russel M: Hydrolysis of flavin mononucleotide by acid phosphatases from animal tissues. Comp Biochem Physiol 5: 113–121, 1962
Lucis O, Link ME, Rucis R: Turnover of cadmium 109 in rats. Arch Environ Health 18: 307–310, 1969
Dudley RE, Svoboda DJ, Klaassen CD: Acute exposure to cadmium causes severe liver injury in rats. Toxicol Appl Pharmacol 65: 302–313, 1982
Morita S: Defense mechanisms against cadmium toxicity. I. A biochemical and histological study of the effects of pretreatment with cadmium on the acute oral toxicity of cadmium in mice. Japan J Pharmacol 39: 129–141, 1984
Sato M, Nagai Y: Mode of existence of cadmium in rat liver and kidney after prolonged subcutaneous administration. Toxicol Appl Pharmacol 54: 90–99, 1980
Shimizu M, Morita S: Effects of fasting on cadmium toxicity, glutathione metabolism, and metallothionein synthesis in rats. Toxicol Appl Pharmacol 103: 28–39, 1990
Stoll RE, White JF, Miya TS, Bonsquet WF: Effects of cadmium on nucleic acid and protein synthesis in rat liver. Toxicol Appl Pharmacol 37: 61–74, 1976
Vallee BL, Ulmer DD: Biochemical effects of mercury, cadmium and lead. Ann Rev Biochem 41: 91–128, 1972
Braestrup C, Andersen PH: Effects of heavy metal cations and other sulfhydryl reagents on brain dopamine D1 receptors: Evidence for involvement of a thiol group in the conformation of the active site. J Neurochem 48: 1667–1672, 1987
Habeeb AFSA: Reaction of protein sulfhydryl groups with Ellman's reagent. Meth Enzymol 25: 457–464, 1972
Leonard JL, Visser TJ: Selective modification of the active center of renal iodothyronine ′-deiodinase by iodoacetate. Biochim Biophys Acta 787: 122–130, 1984
Nakano H, McCormick DB: Modification of arginyl and lysyl residues of flavokinase from rat small intestine. Biochemistry International 28: 441–450, 1992
Fridman M: The chemistry and biochemistry of the sulfhydryl group in amino acids, peptides and proteins Pergamon Press, Oxford: 311-374, 1973
Mizuta K, Tokushige M: Studies on aspartase. II. Role of sulfhydryl groups in aspartase from Escherichia coli. Biochim Biophys Acta 403: 221–231, 1975
Miller NR, Simons SS Jr: Steroid binding to hepatoma tissue culture cell glucocorticoid receptors involves at least two sulfhydryl groups. J Biol Chem 263: 15217–15225, 1988
Author information
Authors and Affiliations
Rights and permissions
About this article
Cite this article
Bandyopadhyay, D., Chatterjee, A.K. & Datta, A.G. Effect of cadmium, mercury and copper on partially purified hepatic flavokinase of rat. Mol Cell Biochem 167, 73–80 (1997). https://doi.org/10.1023/A:1006815504302
Issue Date:
DOI: https://doi.org/10.1023/A:1006815504302