Abstract
Lead is a non-essential element that exhibits a high degree of toxicity, especially in children. Most research on lead has focused on its effects on organ systems such as the nervous system, the red blood cells, and the kidneys which are considered to be the primary targets of lead toxicity. However, the molecular mechanisms by which it induces toxicity, and carcinogenesis remain to be elucidated. In this research, we performed the MTT assay to assess the cytotoxicity, and the CAT-Tox assay to assess the transcriptional responses associated with lead exposure to thirteen different recombinant cell lines generated from human liver carcinoma cells (HepG2), by creating stable transfectants of mammalian promoter chloramphenicol (CAT) gene fusions. Study results indicated that lead nitrate is cytotoxic to HepG2 cells, showing LD50 values of 49.0 ± 18.0 mgr;g/mL, 37.5 ± 9.2 μg/mL, and 3.5 ± 0.7 μg/mL for cell mortality upon 24, 48 and 72 h of exposure, respectively; indicating a dose- and time-dependent response with regard to the cytotoxic effect of lead nitrate. A dose-response relationship was also recorded with respect to the induction of stress genes in HepG2 cells exposed to lead nitrate. Overall, six out of the thirteen recombinant cell lines tested showed inductions to statistically significant levels (p < 0.05). At 50 μg/mL of lead nitrate, the average fold inductions were: 2.1 ± 1.0, 5.4 ± 0.4, 12.1 ± 6.2, 5.0 ± 1.7, 2.5 ± 1.3, and 4.8 ± 4.5 for XRE, HSP70, CRE, GADD153, and GRP78, respectively. These results indicate the potential for lead nitrate to undergo biotransformation in the liver (XRE), to cause cell proliferation (c-fos), protein damage (HSP70, GRP78), metabolic perturbation (CRE), and growth arrest and DNA damage (GADD153). Marginal but not significant inductions were also obtained with the GSTYa (1.5 ± 0.8), and GADD45 (5.7 ± 8.1) promoters, and the NF-κB (2.0 ± 1.7) response element, indicating the potential for oxidative stress. No significant inductions (p > 0.05) were recorded for CYP1A1, HMTIIA, p53RE, and RARE.
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References
Agency for Toxic Substances and Disease Registry (ATSDR): Toxicological Profile for Lead. Public Health Service, U.S. Department of Health and Human Services, Atlanta, GA, 1999
Agency for Toxic Substances and Disease Registry (ATSDR): Case Studies in Environmental Medicine — Lead Toxicity. Public Health Science, U.S. Department of Health and Human Services, Atlantic, GA, 1992.
Centers for Disease Control (CDC): Preventing Lead Poisoning in Young Children: A Statement by the Centers for Disease Control, Atlanta, GA, 1991
Pirkle JL, Brady DJ, Gunter EW, Kramer RA, Paschal DC, Flegal KM, Matte TD: The decline in blood lead levels in the United States: The National Health and Nutrition Examination Surveys (NHANES). J Am Med Assoc 272: 284–291, 1994
Pirkle JL, Kaufmann RB, Brody DJ, Hickman T, Gunter EW, Paschal DC: Exposure of the U.S. population to lead, 1991–1994. Environ Health Perspect 106: 745–750, 1998
United States Environmental Protection Agency (U.S. EPA): Lead Compounds. Technology Transfer Network — Air Toxics Website. Online at: http://www.epa.gov/cgi-bin/epaprintonly.cgi,2002
Kaul B, Sandhu RS, Depratt C, Reyes F: Follow-up screening of lead-poisoned children near an auto battery recycling plant, Haina, Dominican Republic. Environ Health Perspect 107: 917–920, 1999
Litvak P, Slavkovich V, Liu X, Popovac D, Preteni E, Capuni-Paracka S, Hadzialjevi S, Lekic V, Lolacono N, Kline J, Graziano J: Hyper-production of erythropoietin in nonanemic lead-exposed children. Environ Health Perspect 106: 361–364, 1998
Amodio-Cocchieri R, Arnese A, Prospero E, Roncioni A, Barulfo L, Ulluci R, Romano V: Lead in human blood form children living in Campania, Italy. J Toxicol Environ Health 47: 311–320, 1996
Wadi SA, Ahmad G: Effects of lead on the male reproductive system in mice. J Toxicol Environ Health 56: 513–521, 1999
Hertz-Picciotto I: The evidence that lead increases the risk for spontaneous abortion. Am J Ind Med 38: 300–309, 2000
Apostoli P, Kiss P, Stefano P, Bonde JP, Vanhoorne M: Male reproduction toxicity of lead in animals and humans. Occup Environ Med 55: 364–374, 1998
Waalkes MP, Hiwan BA, Ward JM, Devor DE, Goyer RA: Renal tubular tumors and a typical hepper plasics in B6C3F, mice exposed to lead acetate during gestation and lactation occur with minimal chronic nephropathy. Cancer Res 55: 5265–5271, 1995
Goyer RA: Lead toxicity: Current concerns. Environ Health Prospect 100: 177–187, 1993
International Agency for Research on Cancer (IARC): Overall Evaluation of Carcinogenicity: An Updating of Monographs, Vols 1–42,suppl 7. In: IARC Monographs on the Evaluation of Carcinogenic Risks to Humans. IARC, Lyons, France, 1987, pp 230–232
Yang JL, Wang LC, Chang CY, Liu TY: Singlet oxygen is the major species participating in the induction of DNA strand breakage and 8-hydroxy-deoxyguanosine aduct by lead acetate. Environ Mol Mutagen 33: 194–201, 1999
Lin RH, Lee CH, Chen WK, Lin-Shiau SY: Studies on cytotoxic and genotoxic effects of cadmium nitrate and lead nitrate in Chinese hamster ovary cells. Environ Mol Mutagen 23: 143–149, 1994
Dipaolo JA, Nelson RH, Casto BC: In vitro neoplastic transformation of Syrian hamster cell by lead acetate and its relevance to environmental carcinogenesis. Br J Cancer 38: 452–455, 1978
Hwua YS, Yang JL: Effect of 3-amonotriazole on anchorage independence and multigenicity in cadmium-treated and lead-treated diploid human fibroblasts. Carcinogenesis 19: 881–888, 1998
Mosmann T: Rapid colorimetric assay for cellular growth and survival: Applications to proliferation and cytotoxicity assays. J Immunol Meth 65: 55–63, 1983
Tchounwou PB, Wilson BA, Ishague AB, Schneider J: Transcriptional activation of stress genes and cytotoxicity in human liver carcinoma cells exposed to 2,4,6-trinitrotoluene, 2,4-dinitrotoluene and 2,6-dinitrotoluene. Environ Toxicol 16: 209–216, 2001
Tchounwou PB, Wilson BA, Ishaque AB, Schneider J: Atrazine potentiation of arsenic trioxide-induced cytotoxicity and gene expression in human liver carcinoma cells (HepG2). Mol Cell Biochem 222: 49–59, 2001
Bradford MM: A rapid and sensitive method for the quantification of microgram quantities of protein utilizing the principle of protein-dye binding. Ann Biochem 72: 248–254, 1976
Todd MD, Lee MJ, Williams JL, Nalenzy JM, Gee P, Benjamin MB, Farr SB: The CAT-Tox assay: A sensitive and specific measure of stress induced transcription in transformed human liver cells. Fund Appl Toxicol 28: 118–128, 1995
Tchounwou PB, Wilson BA, Schneider J, Ishaque A: Cytogenetic assessment of arsenic trioxide toxicity in the Mutatox, Ames II, and CAT-Tox assays. Metal Ions Biol Med 6: 89–91, 2000
Tully DB, Collins BJ, Overstreet JD, Smith CS, Dinse GE, Mumtaz MM, Chapin RE: Effects of arsenic, cadmium, chromium and lead on gene expression regulated by a battery of 13 different promoters in recombinant HepG2 cells. Toxicol Appl Pharmacol 168: 79–90, 2000
Sengupta M, Bishayi B: Effect of lead and arsenic on murine macrophage response. Drug Chem Toxicol 25: 459–472, 2002
Centers for Disease Control (CDC): Epidemiologic notes and reports fatal pediatric poisoning from lead paint — Wisconsin, 1990. Morb Mort Weekly Rep 40: 193–195, 2001
Centers for Disease Control (CDC): Fatal pediatric lead poisoning — New Hampshire, 2000. Morb Mort Weekly Rep 50: 457–459, 2001
Safe S: Polychlorinated biphenyls (BCBs), dibenzo-p-dioxins (PCDDs), dibenzofurants (PCDFs), and related compounds: Environmental and mechanistic considerations, which support the development of toxic equivalency factors (TEFs). Crit Rev Toxicol 21: 51–88, 1990
Poland A, Knutson JC: 2,3,7,8-tetrachlorodibenzo-p-dioxin and related halogenated aromatic hydrocarbons: Examination of the mechanism of toxicity. Annu Rev Pharmacol Toxicol 22: 517–542, 1982
Schmidt JV, Bradfield CA: Ah receptor signaling pathways. Annu Rev Cell Dev Biol 12: 55–89, 1996
Safe S: Comparative toxicology and mechanism of action of polychlorinated dibenzo-p-dioxins and dibenzofurans. Annu Rev Pharmacol Toxicol 26: 371–399, 1986
Sadek CM, Allen-Hoffman BL: Suspension-mediated induction of hepa 1c1c7 YP1a-1 expression is dependent on the Ah receptor signal transduction pathway. J Biol Chem 269: 31505–31509, 1994
Weiss C, Kolluri SK, Kiefer F, Gottlicher M: Complementation of Ah receptor deficiency in hepatoma cells: Negative feedback regulation and cell cycle control by the Ah receptor. Exp Cell Res 226: 154–163, 1996
Ma Q, Whitlock JP Jr: The aromatic hydrocarbon receptor modulates the Hepa 1c1c7 cell cycle and differentiated state independently of dioxin. Mol Cell Biol 16: 2144–2150, 1996
Fujii-Kuriyama Y, Imataka H, Sogawa K, Yasumoto KI, Kikuchi Y: Regulation of CYP1A1 expression. FASEB J 6: 705–710, 1992
Gonzales GJ, Nebert DW: Autoregulation plus upstream positive and negative control regions associated with transcriptional activation of the mouse P1 (450) gene. Nucleic Acids Res 13: 7269–7288, 1985
Hankinson O: The aryl hydrocarbon receptor complex. Annu Rev Pharmacol Toxicol 35: 307–340, 1995
Whitlock JP Jr, Okino S, Dong L, Ko H, Clarke-Ktzenberg R, Ma Q, Li H: Induction of cytochrome P4501A1: A model for analyzing mammalian gene transcription. FASEB J 10: 809–818, 1996
Tchounwou PB, Ishaque AB, Schneider J: Cytotoxicity and transcriptional activation of stress genes in human liver carcinoma cells (HEpG2) exposed to cadmium chloride. Mol Cell Biochem 222: 21–28, 2000
Pande M, Flora SJ: Lead-induced oxidative damage and its response to combined administration of alpha-lipoic acid and succiners in rats. Toxicology 177: 187–196, 2002
Pimental RA, Liang B, Yee GK, Wilhemsson A, Poellinger L, Paulson KE: Dioxin receptor and C/EBP regulate the function of the glutathione-S-transferase Ya gene xenobiotic element. Mol Cell Biol 113: 4265–4373, 1993
Vanden-Heuvel JP: Alterations of cell signaling by xenobiotics. In: J.P. Vanden-Heuvel, G.H. Perdew, W.B. Mattes, W.F. Greenlee (eds). Comprehensive Toxicology, Vol. 14: Cellular and Molecular Toxicology. Elsevier, New York, 2002, pp 311–332
Morimoto RI, Tissieres A, Georgopoulos C (ed).: Stress Proteins in Biology and Medicine. Cold Spring Harbor Laboratory Press, New York, 1990
Mosser DD, Theodorakis NG, Morimoto RI: Coordinate changes in heat shock element-binding activity and HSP70 gene transcription rates in human cells. Mol Cell Biol 8: 4736–4744, 1988
Morimoto RI, Sarge KD, Abravaya K: Transcriptional regulation of heat shock genes: A paradigm for inducible genomic responses. J Biol Chem 267: 2987–21990, 1992
Sarge KD, Murphy SP, Morimoto RI: Activation of heat shock gene transcription by heat shock factor-1 involves oligomerizatin, acquisition of DNA-binding activity, and nuclear localization and can occur in the absence of stress. Mol Cell Biol 13: 1392–1407, 1993
Hatayama T, Asai Y, Wakatsuki T, Kitamura T, Imahara H: Regulation of hsp 70 synthesis induced by cupric sulfate and zinc sulfate in thermotolerant HeLa cells. J Biochem (Tokyo) 114: 592–597, 1993
Wooden SK, Li LJ, Navarro D, Uadri J, Pereira L: Transcription of the grp 78 promoter by malfolded proteins, glycosylation block, and calcium ionophore is mediated through a proximal region containing a CCAAT mortified which interacts with CTF/NF-I. Mol Cell Biol 11: 5612–5623, 1991
Luethy JD, Holbrook NJ: The pathway regulating GADD153 induction in response to DNA damage is independent of protein kinase C and tyrosine kinases. Cancer Res 54: 1902–1906, 1994
Ariza ME, William MV, Mutagenesis of AS52 cells by low concentrations of lead and mercury. Environ Mol Mutagen 27: 30–33, 1996
Borrelli E, Montmayeur JP, Foulkes NS, Sassone-Corsi P: Signal transduction and gene control: The camp pathway. Crit Rev Oncol 3: 321–338, 1992
Lee KAW, Masson N: Transcriptional regulation by CREB and its relatives. Biochim Biophys Acta 1174: 221–233, 1993
Smith DR, Toft DO: Steroid receptors and their associated proteins. Mol Endocrinol 7: 4–11, 1993
Gorski J, Furlow JD, Murdoch FE, Fritsch M, Kanenko K, Ying C, Malayer JR: Perturbations in the model of estrogen receptor regulation of gene expression. Biol Reprod 48: 8–14, 1993
Ignar-Trowbridge DM, Pimentel M, Parker MG, McLachlan JA, Korach KS: Peptide growth factor cross-talk with the estrogen requires the A/B domain and occurs independently of protein kinase C or estradiol. Endocrinol 137: 1735–1744, 1996
Ignar-Trowbridge DM, Nelson KG, Bidwell MC, Curtis SW, Washborn TF, McLachlan JA, Korach KS: Coupling of dual signaling pathways. Epidermal growth factor action involves the estrogen receptor. Proc Natl Acad Sci 89: 4658–4662, 1992
Cho H, Katzenellenbogen BS: Synergistic activation of estrogen receptor-mediated transcription by estradiol and protein kinase activators. Mol Endocrinol 7: 441–452, 1993
Cherian MG, Howell SB, Imura N, Klaassen CD, Koropatnick J, Lazo JS, Waalkes MP: Contemporary issues in toxicology: Role of metallothionein in carcinogenesis. Toxicol Appl Pharmacol 126: 1–5, 1994
Richards RI, Heguy A, Karin M: Structural and functional analysis — the human metallothionein-I gene: Differential induction by metal ions and glucocorticoids. Cell 7: 263–272, 1984
Petering DH, Fowler BA: Roles of metallothionein and related proteins in metal metabolism and toxicity: Problems and perspectives. Environ Health Perspect 65: 217–224, 1986
Cherian MG: Metallothionein and its interaction with metals. In: R.A. Goyer, M.G. Cherian (eds). Handbook of Experimental Pharmacology, Vol. 115. Springer-Verlag, Heidelberg/NY, 1995, pp 121–137
Baeuerle PA: The inducible transcription activator NF-κB: Regulation by distinct protein subunits. Biochem Biophys Acta 1072: 63–80, 1991
Nelsen B, Hellman L, Shen R: The NF-κB binding sites mediates phorbol ester-inducible transcription in non-lymphoid cells. Mol Cell Biol 8: 3526–3531, 1998
de la Fuente H, Portales-Perez D, Baranda L, Dias-Bariga F, Saavedra-Alanis V, Layseca E, Gonzales-Amaro R: Effect of arsenic, cadmium, and lead on the induction of apoptosis of normal human mononuclear cells. Clin Exp Immunol 129: 69–77, 2002
Allenby G, Bosque MT, Saunders M, Kramer S, Speck J: Reginoic acid receptors and retinoic receptors: Interactions with endogenous retinoic acids. Proc Natl Acad Sci 90: 30–34, 1993
Lammer EJ, Chen DT, Hoar RM, Aguish ND, Benke PJ, Brown JT, Curry CJ, Fernhoff PM, Grix AW, Lott IT: Retinoic acid and embryo pathology. New Engl J Med 313: 837–841, 1985
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Tchounwou, P.B., Yedjou, C.G., Foxx, D.N. et al. Lead-induced cytotoxicity and transcriptional activation of stress genes in human liver carcinoma (HepG2) cells. Mol Cell Biochem 255, 161–170 (2004). https://doi.org/10.1023/B:MCBI.0000007272.46923.12
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DOI: https://doi.org/10.1023/B:MCBI.0000007272.46923.12