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  • TITLE
  • DECLARATION
  • SUPERVISORS NOTE
  • ACKNOWLEDGEMENT
  • CONTENTS
  • ABBREVIATIONS
  • 1. INTRODUCTION
  • 2. REVIEW OF LITERATURE
  • 2.1 REVIEW OF REACTIVE OXYGEN SPECIES
  • 2.2 ANTIOXIDANT DEFENCE SYSTEM
  • 2.2.1 Superoxide dismutase (SOD)
  • 2.2.2 Catalase (CAT)
  • 2.2.3 Glutathione peroxidase (GPx)
  • 2.2.4 Reduced glutathione
  • 2.3 WHY IS BRAIN PRONE TO FREE RADICAL DAMAGE?
  • 2.4 WHAT IS HYPOXIA AND WHY IS HYPOXIA OF THE BRAIN IMPORTANT?
  • 2.5 HYPOXIA AND FREE RADICAL GENERATION
  • 2.6 RESPONSE OF ANTIOXIDANT DEFENCE SYSTEM TO HYPOXIC CONDITIONS IN TISSUES
  • 2.7 PATHOPHYSIOLOGICAL ALTERATIONS IN BRAIN IN RESPONSE TO HYPOXIA
  • 2. 7.1 Cellular acidosis
  • 2.7.2 Energy depletion
  • 2.7.3 Intracellular calcium overload
  • 2.7.4 Accumulation of free fatty acids
  • 2.7.5 Lipid peroxidation
  • 2.7.6 Changes in lysosomal enzyme levels
  • 2.7.7 Impairment of protein synthesis
  • 2.7.8 Changes in blood brain barrier permeability
  • 2.8 ULTRASTRUCTURAL CHANGES OBSERVED IN BRAIN UNDER HYPOXIC CONDITIONS
  • 2.9 SELECTIVE VULNERABILITY OF HIPPOCAMPAL NEURONS TO HYPOXIA
  • 2.10 ANTIOXIDANT THERAPY
  • 2.10.1 Liposomes
  • Table 1 Methods of liposome preparation
  • 2.10.2 Liposomes as a multifunctional carrier system
  • 3. MATERIAL AND METHODS
  • 3.1 MATERIALS
  • 3.1. I Experimental design
  • Table: 2 Experimental Design Animal pool
  • 3.2.1.1 Estimation of protein
  • Fig: 2 Standard curve- Protein
  • 3.2.1.2 Determination of superoxide dismutase activity
  • 3.2.1.3 Biochemical assay for catalase
  • 3.2.1.4 Biochemical assay for glutathione peroxidase
  • 3.2.1.5 Estimation of reduced glutathione
  • 3.2.1.6 Biochemical assay for acid phosphatase
  • 3.2.1.7 Estimation of malondialdehyde
  • 3.2.2 Liposome preparation and entrapment of SOD
  • 3.2.3 Confirmation of liposome formation by electron microscopy
  • 3.2.4 Estimation of protein entrapment in liposomes
  • 3.2.5 SOD entrapped liposome administration
  • Fig: 5 Superoxide dismutase administration through jugular vein
  • 3.2.6 Electron microscopic studies
  • 3.2.7 Statistical analysis
  • 4. OBSERVATIONS
  • 4.1 PROTEIN CONTENT IN THE CONTROL RAT BRAIN
  • Table: 3 Protein content in the control rat brain regions
  • Table: 4 Result of one-way ANOVA used to compare the regional variation in the protein content in the young rat brain
  • Table: 5 Result of one-way ANOVA used to compare the regional variation in the protein content in the adult rat brain
  • Fig: 6 Protein content in the young and adult rat brain regions
  • 4.2 SUPEROXIDE DISMUTASE ACTIVITY IN THE CONTROL RAT BRAIN
  • Fig.SOD activity in the young and the adult rat brain regions
  • Table 6 Superoxide dismutase activity in the control rat brain regions
  • Table 7 Result of one-way ANOVA used to compare thr regional variation in the SOD activity in the young rat brain
  • Table 8 Result of one-way ANOVA used to compare regional variation in the SOD activity in the adult rat brain
  • 4.3 CATALASE ACTIVITY IN THE CONTROL RAT BRAIN
  • Table: 9 Catalase activity in the control rat brain regions
  • Table: 10 Result of one-way ANOVA used to compare the regional variation in the CAT activity in the young rat brain
  • Table: 11 Result of one-way ANOVA used to compare the regional variation in the CAT activity in the adult rat brain
  • 4.4 GLUTATHIONE PEROXIDASE ACTIVITY IN THE CONTROL RAT BRAIN
  • Table: 12 Glutathione peroxidase activity in the control rat brain regions
  • Table: 13 Result of one-way ANOVA used to compare the regional variation in the GPx activity in the young rat brain
  • Table: 14 Result of one-way ANOVA used to compare the regional variation in the GPx activity in the adult rat brain
  • 4.5 REDUCED GLUTEIHIONE CONTENT IN THE CONTROL RAT BRAIN
  • Table: 15 Reduced glutathione content in the control rat brain regions
  • Table: 16 Result of one-way ANOVA used to compare the regional variation in the GSH content in the young rat brain
  • Table: 17 Result of one way ANOVA used to compare the regional variation in the GSH content i the adult rat brain
  • 4.6 MALONDIALDEHYDE CONTENT IN THE CONTROL RAT BRAIN
  • Table: 18 Malondialdehyde content in the control rat brain regions
  • Table: 19 Result of one-way ANOVA used to compare the regional variation in the MDA content in the young rat brain
  • Table: 20 Result of one-way ANOVA used to compare the regional variation in the MDA content in the adult rat brain
  • 4.7 ACID PHOSPHATASE ACTIVITY IN THE CONTROL RAT BRAIN
  • Table: 21 Acid phosphatase activity in the control rat brain regions
  • Table: 22 Result of one-way ANOVA used to compare the regional variation in the ACP activity in the young rat brain
  • Table: 23 Result of one-way ANOVA used to compare the regional variation in the ACP activity in the adult rat brain
  • 4.8 EFFECT OF ISOBARIC HYPOXIA ON THE RAT BRAIN
  • 4.8.1. Effect of isobaric hypoxia on protein content in the rat brain
  • Table: 24 Changes in the protein content in the rat brain after hypoxia for 1 hour
  • Table: 25 Changes the protein content in the rat brain after hypoxia for 3 hours
  • 4.8..2 Effect of isobaric hypoxia on superoxide dismutase activity in the rat brain
  • Table: 26 Changes in the SOD activity in the rat brain after hypoxia for 1 hour
  • Table: 27 Changes in the SOD activity in the rat brain after hypoxia for 3 hours
  • 4.8.3 Effect of isobaric hypoxia on catalase activity in the rat brain
  • Table: 28 Changes in the CAT activity in the rat brain after hypoxia for 1 hour
  • Table: 29 Changes in the CAT activity in the rat brain after hypoxia for 3 hours
  • 4.8.4 Effect of isobaric hypoxia on glutathione peroxidase activity in the rat brain
  • Fig: 21 (GPx activity in the rat brain after hypoxia for 3 hours
  • Table: 30 Changes in the GPx activity in the rat brain after hypoxia of 1 hour
  • Table: 31Changes in the GPx activity in the rat brain after hypoxia for 3 hours
  • 4.8.5 Effect of isobaric hypoxia on reduced glutathione content in the rat brain
  • 4.8.6 Effect of isobaric hypoxia on malondialdehyde content in the rat brain
  • Table: 32 Changes in the GSH content in the rat brain after hypoxia for 1 hour
  • Table: 33 Changes in the GSH content in the rat brain after hypoxia for 3 hours
  • Fig.27 Percentage increase in MDA content in young and adult rat brain after hypoxia for 3 hours
  • Table: 34 Changes in the MDA content in the rat brain after hypoxia for 1 hour
  • Table: 35 Changes in the MDA content in the rat brain after hypoxia for 3 hours
  • 4.8.7 Effect of isobaric hypoxia on acid phosphatase activity in the rat brain
  • Table: 36 Changes in the ACP activity in the rat brain after hypoxia for 1 hour
  • Table: 37 Changes in the ACP activity in the rat brain after hypoxia for 3 hours
  • 4.9 ULTRASTRUCTLRAL CHANGES IN RAT BRAIN AFTER SUBJECTING TO HYPOXIA
  • 4.9.1 Changes in the ultrastructure of mitochondria
  • 4.9.2 Vacuolization
  • 4.9.3 Accumulation of lipid granules
  • 4.9.4 Damage to the ultrastructure of protein synthesizing apparatus
  • 4.9.5 Changes in brain cell processes
  • 4.9.6 Changes in neuroglial cells
  • 4.9.7 Changes in capillary morphology
  • 4.10 SUPEROXIDE DISMUTASE ADMINISTRATION
  • 4.10.1 Detection of liposome in rat brain by electron microscopy
  • 4. 10.2 Biochemical changes in the young rat brain after the administration of SOD entrapped in liposomes under hypoxic conditions
  • Table: 38 Changes in the protein content in the young rat brain regions after the administration of liposome entrapped SOD under hypoxic conditions 3 hours)
  • Table: 39 Changes in the SOD activity in the young rat brain regions after the administration of liposome entrapped SOD under hypoxic conditions (3 hours)
  • Table: 40 Changes in the CAT activity in the young rat brain regions after the administration of liposome entrapped SOD under hypoxic conditions (3 hours)
  • Table: 41Changes in the Gpx activity in the young rat brain regions after the administration of liposome entrapped SOD under hypoxic conditions (3 hours)
  • Table: 42 Changes in the GSH content in the young rat brain regions after the administration of liposome entrapped SOD under hypoxic conditions (3 hours)
  • Table: 43 Changes in the MDA content in the young rat brain regions after the administration of liposome entrapped SOD under hypoxic conditions (3 hours)
  • 4 10.3 Structural modifications in the young rat brain after administration of SOD entrapped in liposomes under hypoxic conditions
  • Fig.57 ACP activity in the rat brain after SOD administration
  • 4.10.3.1 Control
  • 4.10.3.2 Experimental
  • 5. DISCUSSION
  • 5.1 ANTIOXIDANT DEFENCE ENZYMES IN RAT BRAIN -THE REGIONAL VARIATION
  • 5.2 INFLUENCE OF AGE ON ANTIOXIDANT ENZYME ACTIVITIES IN THE RAT BRAIN
  • 5.3 EFFECT OF HYPOXIA ON ANTIOXIDANT DEFENCE SYSTEM IN THE RAT BRAIN
  • 5.4 DOES A DECREASE IN THE PROTEIN CONTENT IN THE BRAIN FOLLOWING HYPOXIA EXPLAIN THE DECREASE IN ANTIOXIDANT ENZYME ACTIVITIES?
  • 5.5 CASH DEPLETION IN THE RAT BRAIN AFTER HYPOXIA
  • 5.6 LIPID PEROXIDATION - AN INDICATOR OF FREE RADICAL DAMAGE IN THE RAT BRAIN
  • 5.7 ACID PHOSPHATASE - AN INDICATOR OF PATHOLOGICAL CONDITION IN TISSUES
  • 5.8 HIPPOCAMPUS AS THE REGION MOST VULNERABLE TO HYPOXIA
  • 5.9 IS ADULT RAT BRAIN LESS SUSCEPTABLE TO HYPOXIA THAN THE YOUNG?
  • 5.10 VACUOLIZATION AND DAMAGED MITOCHONDRIA - A COMMON FEATURE IN ULTRATHIN SECTIONS OF THE RAT BRAIN ALTER HYPOXIA
  • 5.11 CHANGES IN THE CAPILLARY ULTRASTRUCTURE [N THE HIPPOCAMPAL SLICES OF THE YOUNG RAT BRAIN AFTER HYPOXIA
  • 5.12 SOD THERAPY
  • 5.13 SOD ADMINISTRATION PREVENTED/ REDUCED OXIDATIVE INJURY IN RAT BRAIN FOLLOWING HYPOX IA-REOXYGENATION
  • 6. SUMMARY AND CONCLUSION
  • 6.1 COMPONENTS OF ANTIOXIDANT DEFENCE SYSTEM SHOWED REGIONAL VARIATIONS IN RAT BRAIN
  • 6.2 ADULT RAT BRAIN SHOWED A DECREASE IN THE DEFENCE ENZYME ACTIVITIES IN COMPARISON WITH THE YOUNG
  • 6.3 HYPOXlA [MPARTED BIOCHEMICAL AND ULTRASTRUCTURAL ALTERATIONS IN RAT BRAIN LEADING TO OXIDATIVE INJURY
  • 6.4 SOD ADMINISTRATION LEAD TO A DECREASE IN OXIDATIVE INJURY IMPARTED BY HYPOXIA
  • 7. REFERENCES
  • 8. LIST OF PUBLICATIONS