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Abstract

Metaizil yellow and Orange II are extertsively used in various industries and have not been included in the list of permitted food colours because of inadequate safety evaluation data. In this investigation the effect of Metanil yellow and Orange II on the lipid peroxidation in different subcellular fractions of liver was studied in order to understand the site of hepato-toxic potential and whether its blend has an additive, synergistic or antagonistic effect. Parenteral administration of Metanil yellow (80 mg/kg body weight) to rats for 3 days produced a highly significant (p < 0.001) increase in NADPH-dependent enzymatic lipid peroxidation in nuclear (62%), mitochondrial (104%) and microsomal (54%) fractions. The same dose of Orange II to rats showed a relatively less but significant effect in nuclear (62%), mitochondrial (59%) and microsomal (38%) membranes. The blend of Metanil yellow and Orange 11 (40 mg + 40 mg/kg body weight) given intraperitoneally for 3 days resulted in either synergistic or additive effect in nuclear (122%), mitochondrial (130%), and microsomal (62%) membranes. The pro-oxidant free or FeSO ₄/ ADP (1 mM/5 mM) or ascorbate (1 mM) dependent non-enzymatic lipid peroxidation in nuclear, mitochondrial and microsomal fractions was found to be enhanced by Metanil yellow to a greater extent as compared to Orange II, while the blend showed a synergistic or additive response. These results suggest that Metanil yellow and Orange II causes hepatic nuclear, mitochondrial and microsomal membrane damage and that the effect may be more severe with the use of blend.

Keywords

Lipid peroxidation metanil yellow orange II. blend subcellular membranes.

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References

Baird, M.B. , Birnbaum, L.S. and Sfeir, G.T. (1980). NADPH driven lipid peroxidation in rat liver nuclei and nuclear membranes. Arch. Biochem. Biophys. 200:108-115.

Benedetti, A. , Barbieri, L. , Ferrali, M. , Casini, A.P. , Fulceri, R. and Comporti, M. (1981). Inhibition of protein synthesis by carbonyl compounds (4-hydroxyl-alkenals) originating from the peroxidation of liver microsomal lipids. Chem. Biol. Interact. 35:331-340.

Bus, J.S. and Gibson, J.E. (1979). Lipid peroxidation and its role in toxicology . In: Rev. Biochem. Toxicol. Vol. I (eds. Hodgson, E., Bend, J.R. and Philpot, R.M.) Elsevier North Holland Inc., pp. 125-149.

Cook, J.W. , Hewett, C.L. , Kennaway, E.L. and Kennaway, N.M. (1940). Effects produced in the livers of mice by azonaphthalenes and related compounds. Am. J. Cancer 40:62-77.

Das, M. , Seth, P.K. and Mukhtar, H. (1981). Characterization of microsomal aryl hydrocarbon hydroxylase of rat brain. J. Pharmacol. Exptl. Ther. 216:156-161.

Ellman, G.L. (1959). Tissue sulphydryl groups. Arch. Biochem. Biophys. 82:70-77.

Gurr, E. (1971). Synthetic dyes in biology, medicine and chemistry . Academic Press, Inc., London .

Hansen, W.H. , Wilson, D.C. and Fitzhugh, O.G. (1960). Subacute oral toxicity of ten D&C coal-tar colors. Fed. Proc. 19:390.

Hochstein, P. , Nordenbrand, K. and Ernster, L. (1964). Evidence for the involvement of iron in the ADP-activated peroxidation of lipids in microsomes and mitochondria. Biochem. Biophys. Res. Commun. 14:323-329.

10.

Horton, A.A. and Fairhurst, S. (1987). Lipid peroxidation and mechanisms of toxicity . CRC Critical Reviews in Toxicology Vol. 18, 27-79.

11.

Hruszkewyez, A.M. and Bergtold, D.S. (1989). Oxygen radicals, lipid peroxidation and DNA damage in mitochondria. In: Oxygen radicals in Biology and Medicine (ed. M.G. Simic , K.A. Taylor , J.E. Ward and C.V. Sonntag ) Plenum Publishing Corp., pp. 449-456.

12.

Hunter, JR , F.E., Scott, A. , Weinstein, J. , Schneider, A. (1964). Effect of phosphate, arsenate and other substances on swelling and lipid peroxide when mitochondria are treated with oxidized and reduced glutathione. J. Biol. Chem. 239:622-630.

13.

Joint Fao/Who Expert Committee On Food Additives (1965). 8th Report technical report series, No.: 309 (World Health Organization, Geneva).

14.

Khanna, S.K. , Singh, G.B. and Singh, S.B. (1973). Non-permitted colours in food and their toxocity . J. Food Sci. Technol. 10:33-36.

15.

Khanna, S.K. , Singh, G.B. and Dixit, A.K. (1985). Use of synthetic dyes in eatable of rural area . J. Food Sci. Technol. 22:269-273.

16.

Khanna, S.K. , Srivastava, L.P. and Singh, G.B. (1986). Comparative usage pattern of synthetic dyes in yellow to orange coloured eatables among city and rural markets. Ind. Food Pack. 40:33-37.

17.

Lowry, O.H. , Rosebrough, N.J. , Farr, A.L. and Randall, R.J. (1951). Protein measurement with Folin phenol reagent . J. Biol. Chem., 193:265-275.

18.

Ottolenghi, A. (1959). Interaction of ascorbic acid and mitochondrial lipids. Arch. Biochem. Biophys. 79:355-363.

19.

Pederson, T.C. and Aust, S.D. (1972). NADPH-dependent lipid peroxidation catalyzed by purified NADPH cytochrome c reductase from rat liver microsomes. Biochem. Biophys. Res. Commun. 48:789-795.

20.

Plaa, G.L. and Witschi, H. (1976). Chemicals, drugs and lipid peroxidation. Ann. Rev. Pharmacol. Toxicol. 16:125-141.

21.

Player, T.J. , Mills, D.J. and Horton, A.A. (1977). Age dependent change in rat liver microsomal and mitochondrial NADPH dependent lipid peroxidation. Biochem. Biophys. Res. Commun. 78:1397-1402.

22.

Ramachandani, S. , Das, M. , Joshi, A. and Khanna, S.K. (1989). Induction of hepatic xenobiotic metabolizing enzymes by Metanil yellow. Presented in the 58th Annual Meeting of Society of Biological Chemists, India at IVRI, Izatnagar, Oct. 16-18.

23.

Richardson, T. , Tappel, A.L. and Gruger, JR , E.H. (1961). Essential fatty acids in mitochondria. Arch. Biochem. Biophys. 94:1-6.

24.

Singh, R.L. , Khanna, S.K. and Singh, G.B. (1987a). Safety evaluation studies on pure Metanil yellow. I. Acute and sub-chronic exposure responses. Beverage and Food World April/June, 9-13.

25.

Singh, R.L. , Khanna, S.K. and Singh, G.B. (1987b). Acute and short-term toxicity studies on Orange II. Vet. & Human Toxicol., 29:300-304.

26.

Singh, R.L. , Khanna, S.K. and Singh, G.B. (1988). Acute and shortterm toxicity of a popular blend of.Metanil yellow and Orange II in albino rats. Indian J. Expt. Biol. 26:105-111.

27.

Takeshige, K. , Takayanagi, R. and Minakami; S. (1980). Lipid peroxidation and the reduction of ADP-Fe+++ chelate by NADH ubiquinone reductase preparation from bovine heart mitochondria . Biochem. J. 192:861-866.

28.

Tangeras, A. , Flatmark, T. , Backstrom, D. and Ehrenberg, A. (1980). Mitochondrial iron not bound in heme and iron-sulphur centres: Estimation, compartmentation and redox state. Biochim. Biophys. Acta. 589:162-175.

29.

Tappel, A.L. (1973). Lipid peroxidation damage to cell components. Fed. Proc. 32:1870-1874.

30.

Tien, M. , Svingen, B.A. and Aust, S.D. (1982). An investigation into the role of hydroxyl radical in xanthine oxidase dependent lipid peroxidation. Arch. Biochem. Biophys. 216:142-151.

31.

Utley, H.G. , Bernheim, E. and Hochstein, P. (1967). Effect of sulphydryl reagents on peroxidation in microsomes. Arch. Biochem. Biophys. 118:29-32.

Lipid Peroxidation of Ultrastructural Components of Rat Liver Induced By Metanil Yellow and Orange II: Comparison With Blend

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