Garcinia kolaheckel stem bark ethanolic extract and its triterpenoid fraction protected against sodium arsenite-induced hepatotoxicity and nephrotoxicity in rat models | Blazingprojects Postgraduate Thesis
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Garcinia kolaheckel stem bark ethanolic extract and its triterpenoid fraction protected against sodium arsenite-induced hepatotoxicity and nephrotoxicity in rat models

 

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 Garcinia kolaheckel
  • 2.2Pharmacological Properties of Garcinia kolaheckel
  • 2.3Hepatoprotective Effects
  • 2.4Nephroprotective Effects
  • 2.5Mechanisms of Action
  • 2.6Previous Studies on Garcinia kolaheckel
  • 2.7Studies on Triterpenoids
  • 2.8Studies on Sodium Arsenite-induced Toxicity
  • 2.9Combined Effects of Garcinia kolaheckel and Sodium Arsenite
  • 2.10Summary of Literature Review

Chapter THREE

RESEARCH METHODOLOGY

  • 3.1Research Design
  • 3.2Participants and Sampling
  • 3.3Data Collection Methods
  • 3.4Data Analysis Techniques
  • 3.5Ethical Considerations
  • 3.6Validity and Reliability
  • 3.7Limitations of Methodology
  • 3.8Timeframe and Budget

Chapter FOUR

DATA PRESENTATION AND ANALYSIS

  • 4.1Characteristics of Study Participants
  • 4.2Effects on Hepatotoxicity
  • 4.3Effects on Nephrotoxicity
  • 4.4Comparison with Control Group
  • 4.5Triterpenoid Fraction Analysis
  • 4.6Discussion on Mechanisms of Protection
  • 4.7Implications of Findings
  • 4.8Recommendations for Future Research

Chapter FIVE

SUMMARY, CONCLUSION AND RECOMMENDATIONS

  • 5.1Summary of Findings
  • 5.2Conclusion
  • 5.3Contributions to the Field
  • 5.4Practical Implications
  • 5.5Recommendations for Practice
  • 5.6Recommendations for Policy
  • 5.7Areas for Future Research
  • 5.8Final Thoughts

Thesis Abstract

Arsenite is an environmental toxicant known to elicit adverse effects on liver and kidney organs. This study was designed to investigate the protective effects of Garcinia kola Heckel stem bark ethanolic extract (EEGK) and triterpenoid fraction (TFGK) against sodium arsenite-induced hepatotoxicity and nephrotoxicity in rats.

Sodium arsenite was used to induce hepatotoxicity and nephrotoxicity in Wistar strain albino rats for 14 days.EEGK and TFGK were used as test samples while silymarin served as a standard drug for comparison. Biomarkers measured were plasma alanine aminotransferase (ALT), aspartate aminotransferase (AST), alkaline phosphatase (ALP), urea, and creatinine. Ferric reducing antioxidant potential (FRAP), 1-1- diphenyl 2-picryl hydrazyl (DPPH), hydroxyl radical scavenging activity (HRSA), and total antioxidant capacity (TAC) assays were used to determine the antioxidant activity in vitro and In vivo antioxidant assays on the liver, kidney, and plasma superoxide dismutase (SOD), glutathione peroxidase (GPx) and reduced glutathione (GSH) were carried out. In vitro mitochondrial membrane permeability transition (MMPT) was carried out. Histopathological examination of liver and kidney sections were performed and GC-MS analytical method was used to identify the bioactive compounds present in TFGK and EEGK.

Data showed that TFGK reduced ALT, AST, ALP activity and total bilirubin while EEGK reduced plasma creatinine and urea. Furthermore, EEGK elevated DPPH and hydroxyl radical scavenging activity, FRAP, and TAC when compared with TFGKin vitro. In addition, EEGK elevated plasma, liver and kidney SOD, GPx, GSH while TFGK modulated hematological markers. Further study showed thatTFGK inhibited the formation of liver and kidney MMPT.Histopathological examination showed that TFGK and EEGK reversed sodium arsenite-induced hepatotoxicity and nephrotoxicity respectively. GC/MS analysis detected 14 bioactive compounds in EEGK and 15 bioactive compounds in TFGK.

The study concluded that TFGK substantially protected against sodium arsenite-induced hepatotoxicity than EEGK while EEGK substantially protected against sodium arsenite-induced nephrotoxicity than TFGK. In addition, this study provided scientific insight to account for the traditional use of G. kola stem bark extract in ethnomedical practice.


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