Effects of ethanol, methanol and n-hexane leaf and fruit extracts of kigelia africana on some oxidative and biochemical parameters in alloxan-induced diabetic rats | Blazingprojects Postgraduate Thesis
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Effects of ethanol, methanol and n-hexane leaf and fruit extracts of kigelia africana on some oxidative and biochemical parameters in alloxan-induced diabetic rats

 

Table Of Contents


Chapter ONE

INTRODUCTION

  • 1.1Introduction
  • 1.2Background of Study
  • 1.3Problem Statement
  • 1.4Objective of Study
  • 1.5Limitation of Study
  • 1.6Scope of Study
  • 1.7Significance of Study
  • 1.8Structure of the Research
  • 1.9Definition of Terms

Chapter TWO

LITERATURE REVIEW

  • 2.1Overview of Diabetes
  • 2.2Oxidative Stress in Diabetes
  • 2.3Biochemical Parameters in Diabetes
  • 2.4Kigelia Africana Plant
  • 2.5Ethanol Extracts of Kigelia Africana
  • 2.6Methanol Extracts of Kigelia Africana
  • 2.7n-Hexane Extracts of Kigelia Africana
  • 2.8Antioxidant Properties of Plant Extracts
  • 2.9Previous Studies on Plant Extracts
  • 2.10Gaps in Current Literature

Chapter THREE

RESEARCH METHODOLOGY

  • 3.1Research Methodology Overview
  • 3.2Study Design
  • 3.3Selection of Plant Material
  • 3.4Preparation of Extracts
  • 3.5Animal Model and Induction of Diabetes
  • 3.6Administration of Plant Extracts
  • 3.7Data Collection Methods
  • 3.8Statistical Analysis Techniques

Chapter FOUR

DATA PRESENTATION AND ANALYSIS

  • 4.1Analysis of Oxidative Parameters
  • 4.2Analysis of Biochemical Parameters
  • 4.3Effects of Ethanol Extracts on Diabetic Rats
  • 4.4Effects of Methanol Extracts on Diabetic Rats
  • 4.5Effects of n-Hexane Extracts on Diabetic Rats
  • 4.6Comparison of Extract Effects
  • 4.7Discussion on Antioxidant Properties
  • 4.8Discussion on Biochemical Effects

Chapter FIVE

SUMMARY, CONCLUSION AND RECOMMENDATIONS

  • 5.1Summary of Findings
  • 5.2Conclusions Drawn
  • 5.3Implications of Study
  • 5.4Recommendations for Future Research
  • 5.5Final Thoughts

Thesis Abstract

Globally, the estimated incidence of diabetes and projection for the year 2030 as given by the International Diabetes Federation (IDF) is 350 million. Kigelia africana is highly used for ethno medicinal purposes although there is paucity of scientific information on its use. This work was therefore, aimed at evaluating the anti-diabetic and antioxidative potential of the plant. Ethanol, methanol and n- hexane extracts of the leaves of Kigelia Africana were used for the study. Alloxan diabetes was induced in a total of 60 adult male albino rats weighing between 90 and 160 g. The alloxan was dissolved in cold normal saline. After 72 hr, diabetes was confirmed and the rats were divided into twelve (12) groups of five (5) rats each. Group 1 served as the normal control, group 2 was the diabetic untreated, group 3 received 2.5 mg /kg b.wt of glibenclamide, groups 4, 6 and 8 received ethanol, methanol and n-hexane leaves extract while group 5, 7 and 9 received ethanol, methanol and n-hexane fruit extract respectively of 500 mg/kg b.wt of the extracts. Groups 10-12 were administered equal combination of the leaves and fruits extracts. The rats were fed orally for 21 days after which some biochemical and oxidative parameters were statistically analysed. Phytochemical screening for different bioactive compounds was done using standard methods and indicated the presence of flavoniods, alkaloids, saponins, soluble carbohydrates, tannin, steroids, glycosides and reducing sugars. Proximate analysis revealed the presence of proteins (13.9%), carbohydrates (63.5%), fats and oil (11.4%) and crude fibre (2.2%). LD50 showed that the extracts were safe.

Thesis Overview

<p> </p><p><strong>INTRODUCTION</strong></p><p>Diabetes mellitus is a metabolic disorder resulting from a defect in insulin secretion, insulin action or both. Insulin deficiency in turn leads to chronic hyperglycemia with disturbances of carbohydrate, fat and protein metabolism (Kumar <em>et al</em>., 2011).</p><p>During diabetes, failure of insulin-stimulated glucose uptake by fat and muscle cause glucose concentration in the blood to remain high, consequently glucose uptake by insulin-independent tissue increases. Increased glucose flux both enhances oxidant production and impairs antioxidant defenses by multiple interacting non-enzymatic, enzymatic and mitochondrial pathways (Klotz 2002; Mehta <em>et al</em>., 2006). These include activation of protein kinase C isoforms (Inoguchi <em>et al.,</em>&nbsp;2000), increased hexosamine pathway (Kaneto <em>et al</em>., 2001), glucose autoxidation (Brownlee, 2001), increased methylglyoxal and advanced glycation end-product (AGEs) formation (Thornalley, 1998) as well as increased polyol pathway flux ( Lee and Chung, 1999). These seemingly different mechanisms are the results of a single process-that is, overproduction of superoxide by the mitochondrial electron transport system (Tushuizen <em>et al.,</em>&nbsp;2005). This hyperglycaemia-induced oxidative stress ultimately results in modification of intracellular proteins resulting in an altered function and DNA damage, activation of the cellular transcription (NFK B), causing abnormal changes in gene expression, decreased production of nitric oxide, and increased expression of cytokines, growth factors and pro-coagulant and pro-inflammatory molecules (Palmer <em>et al</em>., 1988; Evans <em>et al</em>., 2002; Klotz, 2002; Taniyama and Griendling, 2003). Oxidative stress is responsible for molecular and cellular tissue damage in a wide spectrum of human diseases (Halliwell, 1994), amongst which is diabetes mellitus. Diabetes produces disturbances of lipid profiles, especially an increased susceptibility to lipid peroxidation (Lyons, 1991), which is responsible for increased incidence of atherosclerosis (Guigliano <em>et al.,</em>1996), a major complication of diabetes mellitus . An enhanced oxidative stress has been observed in these patients as indicated by increased free radical production, lipid peroxidation and diminished antioxidant status (Baynes, 1991).</p> <br><p></p>

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