Browse > Article

Cytotoxicity of paraquat and compensatory effects of 3-methylcholanthrene in rat lung  

Rim, Yo-Sup (Division of Environment and Agricultural Science, College of Agriculture and Life Sciences, Sunchon National University)
Kim, Doc-Soo (Division of Environment and Agricultural Science, College of Agriculture and Life Sciences, Sunchon National University)
Han, Du-Seok (Department of Oral Anatomy, School of Dentistry, Wonkwang University)
Hwang, In-Taek (Korea Research Institute of Chemical Technology)
Publication Information
The Korean Journal of Pesticide Science / v.6, no.2, 2002 , pp. 96-104 More about this Journal
Abstract
This study was carried out to investigate cytotoxicity of paraquat on NIH 3T3 fibroblasts, toxicity of paraquat and compensatory effects of 3-methylcholanthrene (3-MC) on the rat lung. In order to conduct MIT [3-(4,5-Dimethylthiazol-2-yl) -2,5-diphenyl -2H-tetrazolium-bromide] and NR (Neutral red) assay, the $5.0{\times}10^4cell/ml$ of NIH 3T3 fibroblast in each well of 24 multi-dish were cultured. After 24 hours, the cells were treated with solution of paraquat (1, 25, 50 and $100{\mu}M$ respectively). After the NIH 3T3 fibroblast of all groups were cultured in same condition for 48 hours. MIT and NR assay were performed to evaluate the cytotoxicity of cell organelles. $MTT_{50}\;and\;NR_{50}$ of paraquat were $1668.97{\mu}M\;and\;1030.85{\mu}M$, respectively. These $IC_{50}$ of Paraquat were decided as a low cytotoxicity by Borenfreund and Puemer (1984). In order to observe the toxicity and compensatory effects of paraquat on the rat lung, Spraque Dawley male rats were used as experimental animals and were divided into paraquat only treated group and simultaneous application group of paraquat and 3-MC, at 30 min and 1, 3, 6, 12, 24, 48 and 96 hrs interval after each treatment. The animals were sacrificed by decapitation and their or the lungs were immediately removed, immersed in fixatives, and were processed with routine method for light microscopic study. Paraffin sections were stained with H&E and iron hematoxylin of Verhoeff. Under the light microscopy, erythrocytes were full in alveolar capillaries at 3 hrs and congested at 24 hrs after paraquat administration. The great alveolar cells (Type II cell) were increased and mitosis of great alveolar were observed in interalveolar septa. Many lymphocytes, macrophages and polymorphonuclear (PMN) cells were observed in connective tissue surrounding lung tissue and germinal center in lymph follicles of terminal bronchiole. Alveolar macrophages were increased in interalveolar septa and alveoli at 48 hrs. And observed many alveolar macrophages at 96 hrs. In iron hematoxylin stain of Verhoeff, Collagen fiber were increased in respiratory bronchiole, interalveolar septa and alveoli and breath of alveoli, and alveolar pore were broaden. But, in paraquat plus 3-MC treated group, morphological changes were mild in lung tissue. These results indicate that 3-MC has a compensatory effects against toxicity of paraquat by conjugation with oxygen.
Keywords
NIH 3T3 fibroblast; paraquat; 3-methylcholanthrene (3-MC); NR assay; iron hematoxylin stain of Verhoeff;
Citations & Related Records
연도 인용수 순위
  • Reference
1 Borenfreund, E. and Puemer, JA. (1984) A simple quantitative procedure using monolayer cultures for cytotoxicity assays(HTD/Nr-90). Tissue Culture Meth. 9:7-9
2 Hemmati AA and Hicks R. (1999) Increased myofibroblast contractile sensitivity in paraquat pretreated rat lung tissue. Life Sci. 65(22):2325-32
3 Silva MF and Saldiva PH. (1998) Paraquat poisoning: an experimental model of dose-dependent acute lung injury due to surfactant dysfunction. Braz. J. Med. Biol. Res., 31(3):445-50
4 Takahashi T, Takahashi Y and Nio M (1994) Remodeling of the alveolar structure in the paraquat lung of humans : a morphometric study. Human Pathology, 257):702-708
5 The Toronto Lung Transplant Group (1985) Sequential bilateral lung transplantation for paraquat poisoning : a case report. J. Thorac. Cardiovasc. Surg., 89:734
6 Vale JA, Meredith TJ and Buckley BM (1987) Paraquat poisoning : clinical features and immediate general management. Hum. Toxieol. 6:41
7 채영암, 구자옥, 서학수, 이영만 (1991) 기초생물통계학 제9장 직선회귀, 향문사 pp.176-198
8 Ilizarov AM, Koo HC, Kazzaz JA, Mantell LL, Li Y, Bhapat R, Pollack S, Horowitz S and Davis JM. (2001) Overexpression of manganese superoxide dismutase protects lung epithelial cells against oxidant injury. Am. J. Respir. Cell Mol. Biol 24(4):436-41
9 박경아, 이원택, 박미경, 이종은 (1992) 조직학. 고려의학 pp.465-473
10 Situnayake RD, Crump BJ, Thurnham DI and Davies M (1987) Evidence for lipid peroxidation in man following paraquat ingestion. Hum Toxicol., 6:94
11 Mosmann, T. (1983) Rapid colorimetric assays for cellular growth and survival: Application to proliferation and cytotoxicity assays. J. Immunol. Methods., 65:55-63
12 Cappelletti G, Maggioni MG and Mad R.(1998) Apoptosis in human lung epithelial cells: triggering by paraquat and modulation by antioxidants. Cell. Biol. Int. 22(9-10):671-8
13 Franek WR, Horowitz S, Stansberry L, Kazzaz JA, Koo HC, Li Y, Arita Y, Davis JM, Mantell AS, Scott Wand Mantell LL. (2001) Hyperoxia inhibits oxidant-induced apoptosis in lung epithelial cells. J. Biol. Chem. 276(1):569-75
14 Meredith TJ and Vale JA (1987) Treaternnt of paraquat poisoning in man: methods to prevent absorption. Hum Toxicol. 6:49
15 Statham CN, Elcombe CR, Szyjka SP and Lech JJ (1978) Effect of polycyclic hydrocarbons on hepatic microsomal enzymes and disposition of methylnaphtalene in rainbow trout. in vitro Xenbiotica, 8:65-71
16 Tomita M, Okuyama T, Ishikawa T, Hidaka K and Nohno T. (2001) The role of nitric oxide in paraquat-induced cytotoxicity in the human A549 lung carcinoma cell line. Free Radic Res. 34(2)193-202
17 Eisenman A, Armali Z, Raikhlin-Eisenkraft B, Bentur L, Bentur Y, Guralnik L and Enat R. (1998) Nitric oxide inhalation for paraquat-induced lung injury. J Toxicol Clin Toxicol. 36(6):585-6
18 Leeson TS, Leeson CR and Paparo AA (1988) Text/atlas of histology. W.B. Saunders. pp.513-534
19 Day BJ and Crapo JD. (1996) A metalloporphyrin superoxide dismutase mimetic protects against paraquat-induced lung injury in vivo. Toxicol. Appl. Pharmacol. 140(1):94-100
20 Smith LL (1987) Mechanism of paraquat toxicity in lung and its relevance to treatment. Hum. Toxicol., 6(1):31-36
21 Nebert DW, Atlas SA, Guenthner TM and Kouri RE (1978) the ah locus: Genetic regulation of the enzymes which metabolize polycyclic hydrocarbons and the risk for cancer, In polycyclic hygrocarbons and cancer(P.O.P. Ts’o and H.B. Gelboin, eds.), Academic Press, New York, 2:345-390. (1978)