Hepato-Protective Effect of Karisalai Karpa Chooranam against Paracetamol Induced Hepato Toxicity in Zebra fish (Daniorerio) Model

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IOSR Journal of Dental and Medical Sciences (IOSR-JDMS) e-issn: 2279-0853, p-issn: 2279-0861.Volume 17, Issue 6 Ver. 12 (June. 2018), PP 51-55 www.iosrjournals.org Hepato-Protective Effect of Karisalai Karpa Chooranam against Paracetamol Induced Hepato Toxicity in Zebra fish (Daniorerio) Model Juliet. L 1 * Sivakkumar. S, 2 1 Research Officer (Siddha), Siddha Central Research Institute, Chennai- 600106. 2 Lecturer, Department of Gunapadam, National Institute of Siddha, Chennai- 600047. Corresponding Author: Juliet. L Abstract: Background: The liver may be considered as the most important organ in drug toxicity because it is functionally interposed between the site of absorption and the systemic circulation and is a major site of metabolism and elimination of foreign substances; these features render it a preferred target for drug toxicity. Drug-induced liver injury (DILI) therefore possess a major clinical problem. DILI is initiated by direct hepatotoxic effects of a drug. Paracetamol, a widely used analgesic and antipyretic drug, which causes acute liver damage in higher doses in both animals and in humans. Paracetamol administration causes necrosis of the centrilobular hepatocytes characterized by nuclear pyknosis and eosinophilic cytoplasm followed by large excessive hepatic lesion. Exposure of Paracetamol in Zebrafish causes 75% reduction in liver antioxidant enzyme level within 24 hours post exposure. Aim: The present study is aimed to evaluate the hepato protective effect of Siddha preparation Karisalai Karpa Chooranam (KKC) in Zebrafish model. Materials and methods: In this study, the liver injury was induced by Paracetamol and the test drug KKC has been administered at the dose of 250 and 500 mg/liter for seven days. After one-week exposure period, the liver of Zebrafish was dissected and histopathological studies were performed. Result: The result of this present investigation indicates that Paracetamol treated groups show severe liver degeneration whereas treatment with test drug KKC at both the dose levels significantly attenuated the Paracetamol induced damages. Conclusion: This study concluded that the drug KKC possesses promising hepato protective activity in dose dependent manners and restores the basic liver architecture by means of its rejuvenating potential against Paracetamol induced toxicity in Zebra fish model. Key Words: Siddha medicine; Karisalai Karpa Chooranam; Hepato Protective activity. ----------------------------------------------------------------------------------------------------------------------------- ---------- Date of Submission: 12-06-2018 Date Of Acceptance: 27-06-2018 ----------------------------------------------------------------------------------------------------------------------------- ---------- I. Introduction Liver is the most important organ of living system and performs vital functions in regulations of physiological processes in the body. It is involved in metabolism, secretion and storage. Liver diseases are mainly caused due to excess consumption of alcohol, toxic chemicals, infectious diseases and autoimmune disorders may also be the major cause. Diseases like jaundice, liver cirrhosis, and fatty liver disease are commonly occurring worldwide. 1 Liver diseases have become one of the major causes of morbidity and mortality all over the world. From among, drug induced liver injury (DILI) is one of the most common causative factor that possess a major clinical and regulatory challenge 2. The manifestations of drug-induced hepatotoxicity are highly variable, ranging from asymptomatic elevation of liver enzymes to fulminant hepatic failure 3. In recent years there has been tremendous advancement in the field of science and hematology; however liver problems are on high rise, the two major liver diseases which has caused high death rate annually account for jaundice and hepatitis 4. Hepatotoxic chemicals damage liver cells by inducing lipid peroxidation and other oxidative damages 5. More than 900 drugs have been found to cause liver diseases and have been stopped from implications 6. Drug induced liver injury has become a major challenge. Various models have been identified for predicting the toxicity, Paracetamol, a widely used analgesic and antipyretic drug, which causes acute liver damage in high doses in both animals and in humans. Paracetamol administration causes necrosis of the centrilobular hepatocytes characterized by nuclear pyknosis and eosinophilic cytoplasm followed by large excessive hepatic lesion. A hepatotoxic metabolite, NAPQI (N-acetyl-p-benzoquinone imine) that is produced by cytochrome P450 of liver enzymes, remain inactivated at therapeutic doses by Liver GSH 7, 8.at higher doses, DOI: 10.9790/0853-1706125155 www.iosrjournals.org 51 Page

these metabolite gets activated due to decrease in level of GSH, which accounts for the dysfunction of liver, causing mitochondrial DNA damage, oxidative stress and apoptosis of immune cells 9-11. In spite of advancement in the recent trends in drug development, presently only a few hepatoprotective drugs are available for the treatment of liver disorders 12. Various natural remedies from traditional medicinal plants, ie in Siddha have been found to be effective against liver damages and has been recommended for the treatment of liver diseases in the Indian system of medicines 13. The relative accessibility, low prices, local availability and acceptance by the local communities have made heavy reliability on plant medicine. Since the ancient time, plant medicine is an important part of healthcare system. In Siddha system, there are many herbal formulations available which helps in preventing liver damage 14. In the present study an attempt has been made to screen the hepatoprotective effect of Karisalai Karpa Chooranam on paracetomol induced liver injury in Zeebra Fish. II. Materials and Methods 2.1 Karisalai Karpa Chooranam 15 : The test drug Karisalai Karpa Chooranam has been purchased from SKM Siddha and Ayurvedha Pharmacy, Erode, Tamilnadu. It is a poly herbal Siddha preparation prepared from seven herbs ( Table: 1) which is indicated for Paandu (Anaemia), Kaamalai (Jaundice), Kalleral veekkam ( Hepatomegaly), Sobai ( Generalized oedema), Skin diseases and helps to enhance the immune system. It is a powerful rejuvenating medicine in Siddha system and used as a Kaayakalpam. 2.2 Experimental Animals : Adult Zeebra Fish (Daniorerio) were purchased from the local supplier and were maintained in a laboratory condition 28 C + 1 C and a period of 14:10 h light/dark cycle photo period. All fishes were acclimatized to lab condition four weeks prior to the start of experimentation. Animals were divided in to four groups of 10 fish each. Grouping Group I : Control Group II : Paracetamol 5mM (755.8mg) per liter concentration Group III : Paracetamol 5mM + Karisalai Karpa Chooranam 250 mg/liter Group IV : Paracetamol 5mM + Karisalai Karpa Chooranam 500 mg/liter 2.2 Treatment Animal belongs to Group I treated as Control and Group II treated with Paracetamol at the concentration of 5mM (755.8mg) per liter concentration for the period of seven days. Animal belongs to Group III treated with test drug Karisalai Karpam Chooranam (KKC) at the concentration of 250 mg/liter and Group IV treated with test drug Karisalai Karpam Chooranam (KKC) at the concentration of 500 mg/liter along with Paracetamol 5mM for the period of seven days. 2.4 Histopathology : After one-week exposure period, the livers of Zebrafish were dissected and fixed in 10% formalin for 24h. Subsequently, the fixed liver tissues were dehydrated in gradient ethanol, hyalinized in xylene, and embedded in paraffin wax at 56 C. Then, the paraffin blocks were sectioned at 5-μm thickness. The sections were collected on glass slides and stained with hematoxylin and eosin (H&E) using an H&E Staining Kit. Histologic lesions were observed using an optical microscope equipped with a digital camera. III. Results and Discussion The results obtained from the present investigation indicates that Paracetamol treated groups shows severe liver degeneration whereas treatment with test drug Karisalai Karpa Chooranam at both the dose levels significantly attenuated the Paracetamol induced damage in group III and IV. Hence from the study it was concluded that the drug Karisalai Karpa Chooranam possesses promising hepato protective activity in dose dependent manners and restores the basic liver architecture by means of its rejuvenating potential against Paracetamol induced toxicity in Zebra fish model. In the present study, the histopathological studies were carried out to check the hepatoprotective effect of Karisalai Karpa Chooranam on Paracetamol induced liver damage. The H&E staining of the liver tissue of Paracetamol and post treated group as shown in Figure: 1. shows the control group with normal liver morphology with nomal liver cells, Figure: 2. Paracetamol treated group which shows the degeneration of vacuoles in the cell, and necrotic aggregation of cells, Figure: 3&4. shows the post treatment with Karisalai Karpa Chooranam indicating the regeneration of vacuoles, with no necrotic zone, and normal hepatocytes. DOI: 10.9790/0853-1706125155 www.iosrjournals.org 52 Page

The Paracetamol liver injury resulting in degeneration of cells may be due to the accumulation of nonadipose tissue which results in cell necrosis and cell death and Treatment with Karisalai Karpa Chooranam resulted in regeneration of vacuoles and liver cells indicating that the Karisalai Karpa Chooranam decreases the oxidative hepatic injuries such as necrotic aggregations due to Paracetamol. IV. Conclusion This study concluded that the test drug Karisalai Karpa Chooranam possess hepatoprotective effect against Paracetamol induced liver damage in Zebra fish. This effect may due to the presence of natural phytochemicals and anti oxidants in the test formulation. Further clinical studies to be conducted to confirm its therapeutic effect on Liver diseases. Table: 1. Ingredients of Karisalai Karpa Chooranam S.No Siddha Name Botanical Name Quantity 1 Vellai Karisalai Eclipta prostrata 10 gm 2 Manjal Karisalai Wedelia chinensis 10 gm 3 Kuppaimeni Acalypha indica 10 gm 4 Seruppadai Coldenia Procumbens 10 gm 5 Vallarai Centella asiatica 10 gm 6 Neeli Indigofera tinctoria 10 gm 7 Kottai Karanthai Sphaeranthus indicus 10 gm Figure: 1. Control Group: Regular sinusoidal space with perfectly aligned hepatocytes Figure: 2. Paracetamol treated Group: Centrilobular necrosis with changes pertains to Karryohexis (nuclear fragmentation) and Extremely Widened sinusoidal space. DOI: 10.9790/0853-1706125155 www.iosrjournals.org 53 Page

Fig: 3. KKC (250 mgm) treated Group: Widened sinusoidal space with Moderate necrotic changes. Fig: 3. KKC (500 mgm) treated Group: Normal Hepatocytes with Mild degenerative changes. References [1]. Jyotsna, Swarnalatha Y. ; Effect of Flavonoids in Acetaminophen Induced Liver Injury in Danio Rerio; International Journal of Health Sciences & Research; Vol.6; Issue: 2; February 2016. [2]. Russmann, S., Gerd, A., and Grattagliano, I.: Curr Med Chem., 16: 3041-3053 (2009). [3]. Vermeulen, N.P.E., Bessems, J.G.M. and Vandestreat, R.: Drug Metab Rev., 24: 367-407 (1992). [4]. Pang S, Xin X, Stpierre MV. Determinants of Metabolic Disposition. Rev. Pharmacol. Toxicol., 1992; 32: 625-626. [5]. IlangoK and ChitraV. Hepatproteactive and Antioxidant activities of Fruit Pulp of Limoniaacidissima Linn. International Journal of Health Research. 2009;2(4):361 367. [6]. Friedman, Scott E.; Grendell, James H, McQuaid, Kenneth R. Current diagnosis & treatment in gastroenterology. New York: Lang Medical Books/McGraw-Hill.2003; 664-679. [7]. Lee SS, Buters JT, Pineau T, Fernandez-Salguero P, Gonzalez FJ. Role of CYP2E1in the hepatotoxicity of acetaminophen. J Biol Chem.1996; 271:12063 12067. [8]. Mitchell JR, Jollow DJ, Potter WZ, Gillette JR, Brodie BB.Acetaminophen-induced hepatic necrosis. IV. Protective role of glutathione. J Pharmacol Exp Ther. 1973; 187:211 217. [9]. Kon K, Kim JS, Jaeschke H, Lemasters JJ. Mitochondrial permeability transition in acetaminophen-induced necrosis and apoptosis of cultured mouse hepatocytes. Hepatology. 2004; 40:1170 1179. [10]. Ruepp SU, Tonge RP, Shaw J, Wallis N, Pognan F. Genomics and proteomics analysis of acetaminophen toxicity in mouse liver. Toxicol Sci. 2002; 65:135 150. DOI: 10.9790/0853-1706125155 www.iosrjournals.org 54 Page

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