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ABSTRACT

The effect of alcohol on some hepatic parameters of albino rats was investigated, after a period of 7 days. The experimental animals were divided into four groups. All the groups received feed and water . In addition to this, group II received 25ml of alcohol/kg body weight once daily, group III received 50ml of alcohol/kg body weight once daily while group IV received 75ml of alcohol/kg body weight once daily also. The alcohol was given by oral compulsion. Blood samples were collected from the rats after the 7th day by cardiac puncture. The blood was allowed to clot, centrifuged and serum collected for analysis. Some hepatic parameters(ALT, AST, ALP, GGT, total bilirubin, conjugated bilirubin and unconjuated bilirubin) were analysed. The result gotten was calculated using statistical package for social sciences(SPSS). From the results, it was observed that there were significant increase in most liver parameters in both group III and IV(P<0.05) when compared to control but no significant different in group II when compared to control(as shown in the tables in chapter 4).  This indicates that the increase in doses of alcohol could be detrimental to the liver particularly in high doses.

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

TABLE OF CONTENTS

Title Page……………………………………………………………………….i

Certification……………………………………………………………………ii

Dedication……………………………………………………………………..iii

Acknowledgement…………………………………………………………….iv

Abstract………………………………………………………………………..v

Table of content……………………………………………………………….vi

List of figures…………………………………………………………………ix

List of tables…………………………………………………………………..x

CHAPTER ONE: INTRODUCTION

1.1 Background of study………………………………………………………1

1.1 Justification………………………………………………………………..3

1.2 Aims and Objectives……………………………………………………….4

CHAPTER TWO: LITERATURE REVIEW

2.1 The Liver……………………………………………..…………………….5

2.1.1 Anatomy of the liver…………………………………………………….5

2.1.2 Physiology of the liver………..…………………………………………6

2.1.3 Liver Functions…………………………………………………………..7

2.1.4 Chemical Findings in Liver Diseases…………………………………….9

2.1.5 Liver Enzymes……………………………………………………………10

2.2. Bilirubin……………….………………………………………………….16

2.2.1 Clinical Implications…………………………………………………….17

2.3    History of Alcohol………………………………………………………18

2.3.1  Alcohol Pharmacology………………………………………………….20

2.3.2 Metabolism of Alcohol……..……………………………………………22

2.3.3  Factors influencing alcohol absorption and metabolism.……………….24

2.3.4 Effects of Alcohol Metabolism…………………………………………..25

2.3.5 Alcoholic Effects on the liver………………..………………………….29

2.3.6 A review on alcohol………………………………………………………33

CHAPTER THREE: MATERIALS AND METHOD

3.0 Materials and Method………………………………………………………37

3.1 Experimental Animals………………………………………………………37

3.2 Experimental Design……………………………………………………….38

3.3 Sample Collection………………………………………………………….39

3.4 Laboratory Procedure………………………………………………………39

3.4.1`Serum Aspartate Amino Transferase Estimation………………………..39

3.4.2 Serum Alanine Amino Transferase Estimation………………………….41

3.4.3 Determination of Alkaline Phosphatase…………………………………43

3.4.4 Determination of Serum Gamma-Glutamyl Transferase………………..44

3.4.5 Determination of Serum Total,Conjugated and Unconjugated Bilirubin.45

3.5 Statistical Analysis………………………………………………………..47

CHAPTER FOUR: RESULTS

4.0 Results…………………………………………………………………….48

CHAPTER FIVE: DISCUSSION

5.0 Discussion…………………………………………………………………54

5.1 Conclusion…………………………………………………………………56

REFERENCE………………………………………………………………….57

APPENDICES………………………………………………………………..66

 

 

 

 

 

 

 

 

 

 

CHAPTER ONE

  • INTRODUCTION       

1.1     Background of study

In chemistry, an alcohol is an organic compound in which the hydroxyl functional group (-OH) is bound to a carbon atom. In particular, this carbon center should be saturated, having single bonds to three other atoms (Nic et al., 2006).

Alcohols are neutral colourless and a water miscible organic solvent and it distributes itself throughout the body. This means that the concentration within tissues will be similar to that in the blood. Alcohol (ethanol) is consumed widely in the form of beer, wines and spirit. Excessive alcohol consumption with its associated consequences is a leading cause of economic, social and medical problems throughout the world. Besides the short term effects most pathophysiological consequences of ethanol abuse are associated with chronic consumption over a long period.

Alcohol is consumed by about 70 % of U.S. adults (Breslow et al.,2008). Consumption of this dietary component has both risks and benefits. Low to moderate doses of alcohol lower the risk of cardiovascular disease and all-cause mortality(USDA, 2010). The Dietary Guidelines for Americans 2010 and American Heart Association’s dietary guidelines suggest that if alcohol is consumed, males consume no more than two alcoholic drinks per/day (28 g/day) and women no more than one per/day (14 g/day) (Lichtenstein et al., 2006).

However, approximately 38 million adults in the United States report binge drinking an average of four times per month and consuming an average of eight drinks per episode (Kanny et al., 2013). Excessive alcohol intake was responsible for approximately 10 % of deaths among working age adults in the United States during 2006–2010 (Stahre et al., 2014) and cost the United States $223.5 billion in 2006. It is estimated to be the fourth leading preventable cause of death in the United States (Mokdad et al., 2000). Heavy drinking, including binge drinking, increases the risk of liver disease, hypertension, stroke, type II diabetes, gastrointestinal cancers, injuries and violence  (USDA, 2010). Alcohol abuse is the leading cause of liver-related morbidity and mortality (USDA, 2010). In alcoholic patients increased levels of several liver-derived biomarkers are associated with excessive ethanol intake and alcoholic liver disease, and a number of studies have reported induction of liver enzyme function due to excessive alcohol consumption (Sharpe, 2001; Niemela, 2006). However, only a few small studies have investigated the effects of moderate alcohol consumption on liver enzymes (Alatalo et al., 2009)

  • During the past decades the total per capita ethanol consumption and associated medical disorders have increased rapidly (Room, 2005). Excessive alcohol consumption and obesity are known to lead to accumulation of fat in hepatic tissue and to induce changes in serum liver-derived enzymes (Ruhl and Everhart, 2005). Clinically, measurements of serum alanineaminotransferase (ALT), aspartateaminotransferase (AST), and γ-glutamyltransferase (GGT) are widely used as markers in evaluating the degree of alcohol liver injury (Conigrave et al., 2003).

1.2 JUSTIFICATION

Alcohol is consumed by about 70 % of U.S. adults (Breslow et al., 2008).Consumption of this dietary component has both risks and benefits. Low to moderate doses of alcohol lower the risk of cardiovascular disease and all-cause mortality (USDA, 2010). Excessive alcohol consumption can cause liver diseases including fatty liver, hepatitis and cirrhosis (Zakhari and Li, 2007; Schwartz and Reinus, 2012). Since alcohol is mainly metabolized by the liver, it is a primary site of alcohol-induced adverse health effects. Changes in liver enzymes activities are biomarkers of liver damage and are routinely assessed for diagnostic purposes and as part of physical examinations (Woreta and Alqahtani, 2013).

Previous studies have suggested the presence of a graded dose–response relationship between alcohol intake and risk of liver disease (Bellentani and Tiribelli, 2001; Day, 1997) and that GGT induction can be initiated at low doses of alcohol intake (Alatalo et al.,2009). But no such research has been done in this part of the world where the intake of alcohol is on the increase. Hence it becomes imperative to carry out this research.

  • 3 AIMS AND OBJECTIVES
  1. A) Aim:
  1. To study the effect of different volumes of alcohol on some hepatic parameters.
  2. Objectives:
  3. To determine the effect of alcohol on total, conjugated and unconjugated bilirubin.
  4. To determine the effect of alcohol on liver enzymes such as (alkaline phosphatase (ALP), alanineaminotransferase (ALT), aspartateaminotransferase (AST), gamma glutamyltransferase (GGT) in albino rats.

 

 

 

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