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Enzymes msc

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RAHANAMOIDEENKOYAVK

Enzymes

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ENZYMES Rahana Moideen Koya.V.K MSc,Mphil,Med,MA Assistant Professor,Dept.of Zoology Farook College,Kozhikode.Kerala.
CONTENTS Chemistry Classification Mechanism of EnzymeAction Enzyme Kinetics Inhibition Activation Specificity
Introduction  Enzymes are biological catalysts that speed up the rate of the biochemical reaction.  Most enzymes are three dimensional globular proteins (tertiary and quaternary structure).  Some special RNA species enzymes and are called Ribozymes also act as e.g. hammerhead ribozyme. Hammerhead enzyme
STRUCTURE OF ENZYMES  The active site of an enzyme is the region that binds substrates, co-factors and prosthetic groups and contains residue that helps to hold the substrate.  Active sites generally occupy less than 5% of the total surface area of enzyme.  Active site has a specific shape due to tertiary structure of protein.  A change in the shape of protein affects the shape of active site and function of the enzyme.
ACTIVE SITE It chooses the substrate and binds it to active site. It performs the catalytic action of enzyme. o Active site can be further divided into: Active Site Binding Site Catalytic Site
CO-FACTORS o Co-factor is the non protein molecule which carries out chemical reactions that can not be performed by standard 20 amino acids. o Co-factors are of two types:  Organic co-factors  Inorganic cofactors
INORGANIC CO-FACTORS o These are the inorganic molecules required for the proper activity of enzymes. Examples:  Enzyme carbonic anhydrase requires Zn for it‟sactivity.  Hexokinase has co-factor Mg ORGANIC CO-FACTORS o These are the organic molecules required for the proper activity of enzymes. Example:  Glycogen phosphorylase requires the small organic molecule pyridoxal phosphate. ++ ++
TYPES OF ORGANIC CO-FACTORS Prosthetic Group Coenzyme A prosthetic group is a tightly bound organic co- factor e.g. Flavins, heme groups and biotin. o A coenzyme is loosely bound organic co-factor. factor e.g. heme E.g. NAD+
 An enzyme with it‟ s co-factor removed is designated as apoenzyme.  The complete complex of a protein with all necessary small organic molecules, metal ions and other components is termed as holoenzyme of holoprotein. Types of co-factors Continued…
SUBSTRATE  The reactant in biochemical reaction is termed as substrate.  When a substrate binds to an enzyme it forms an enzyme- substrate complex. Enzyme Joins Substrate
SITES OF ENZYME SYNTHESIS o Enzymes are synthesized by ribosomes which are attached to the rough endoplasmic reticulum. o Information for the synthesis of enzyme is carried by DNA. o Amino acids are bonded together to form specific enzyme according to the DNA‟scodes.
INTRACELLULAR AND EXTRACELLULAR ENZYMES o Intracellular enzymes are synthesized and retained in the cell for the use of cell itself. o They are found in the cytoplasm, nucleus, mitochondria and chloroplast. Example :  Oxydoreductase catalyses biological oxidation.  Enzymes involved in reduction in the mitochondria. in the cell but o Extracellular enzymes are synthesized secreted from the cell to work externally. Example :  Digestive enzyme produced by the pancreas, are not used by the cells in the pancreas but are transported to the duodenum.
CHARACTERISTICS  Enzymes speed up the reaction by lowering the activation energy of the reaction.  Their presence does not effect the nature and properties of end product.  They are highly specific in their action that is each enzyme can catalyze one kind of substrate.  Small amount of enzymes can accelerate chemical reactions.  Enzymes are sensitive to change in pH, temperature and substrate concentration.  Turnover number is defined as the number of substrate molecules transformed per minute by one enzyme molecule. Catalase turnover number = 6 x106/min
NOMENCLATURE OF ENZYMES o An enzyme is named according to the name of the substrate it catalyses. o Some enzymes were named before a systematic way of naming enzyme was formed. Example: pepsin, trypsin and rennin o By adding suffix -ase at the end of the name of the substrate, enzymes are named. o Enzyme for catalyzing the hydrolysis is termed as hydrolase. Example : maltose + water glucose + glucose maltase
EXAMPLES substrate enzymes products lactose lactase glucose + galactose maltose maltase Glucose cellulose cellulase Glucose lipid lipase Glycerol + fatty acid starch amylase Maltose protein protease Peptides + polypeptide
CLASSIFICATION
CLASSIFICATION OF ENZYMES  A systematic classification of enzymes has been developed by International Enzyme Commission.  This classification is based on the type of reactions catalyzed by enzymes.  There are six major classes.  Each class is further divided into sub classes, sub sub-classes and so on, to describe the huge number of different enzyme- catalyzed reactions.
ENZYME CLASS REACTION TYPE EXAMPLES Oxidoreductases Reduction-oxidation (redox) Lactate dehydrogenase Transferases Move chemical group Hexokinase Hydrolases Hydrolysis; bond cleavage with transfer of functional group of water Lysozyme Lyases Non-hydrolytic bond cleavage Fumarase Isomerases Intramolecular group transfer (isomerization) Triose phosphate isomerase Ligases Synthesis of new covalent bond between substrates, using ATPhydrolysis RNA polymerase Continued…….. Classification of enzymes
MECHANISM OF ENZYME ACTION
MECHANISM OF ENZYME ACTION  The catalytic efficiency of enzymes is explained by two perspectives: Thermodynamic changes Processes at the active site
THERMODYNAMIC CHANGES  All chemical reactions have energy barriers between reactants and products.  The difference in transitional state and substrate is called activational barrier.
THERMODYNAMIC CHANGES  Only a few substances cross the activation barrier and change into products.  That is why rate of uncatalyzed reactions is much slow.  Enzymes provide an alternate pathway for conversion of substrate into products.  Enzymes accelerate reaction rates by forming transitional state having low activational energy.  Hence, the reaction rate is increased many folds in the presence of enzymes.  The total energy of the system remains the same and equilibrium state is not disturbed.
THERMO-DYNAMIC CHANGES OVERVIEW
PROCESSES AT THE ACTIVE SITE Covalent catalysis Acid base catalysis Catalysis by strain Catalysis by proximity
COVALENT CATALYSIS o Enzymes form covalent linkages with substrate forming transient enzyme-substrate complex with very low activation energy. o Enzyme is released unaltered after completion of reaction.
ACID-BASE CATALYSIS  Mostly undertaken by oxido- reductases enzyme.  Mostly at the active site, histdine is present which act as both proton donor and proton acceptor.
CATALYSIS BY PROXIMITY forming  In this catalysis molecules must come in bond distance.  When enzyme binds:  A region of high substrate concentration is produced at active site.  This will orient substrate molecules especially in a position ideal for them.
CATALYSIS BY BOND STRAIN  Mostly undertaken by lyases.  The enzyme-substrate binding causes reorientation of the structure of site due to in a strain condition.  Thus transitional state is required and here bond is unstable and eventually broken.  In this way bond between substrate is broken and converted into products.
LOCK AND KEY MODEL  Proposed by EMIL FISCHER in 1894.  Lock and key hypothesis assumes the active site of an enzymes are rigid in its shape.  There is no change in the active site before and after a chemical reaction.
INDUCED FIT MODEL  More recent studies have revealed that the process is much more likely to involve an induced fit model(proposed by DANIAL KOSH LAND in 1958).  According to this exposure of an enzyme to substrate cause a change in enzyme, which causes the active site to change i t ‟ s shape to allow enzyme and substrate to bind.
32 INDUCED FIT MODEL
ENZYMES KINETICS
INTRODUCTION “It is a branch of biochemistry in which we study the rate of enzyme catalyzed reactions.”  Kinetic analysis reveals the number and order of the individual steps by which enzymes transform substrate into products  Studying an enzyme's kinetics in this way can reveal the catalytic mechanism of that enzyme, its role in metabolism, how its activity is controlled, and how a drug or an agonist might inhibit the enzyme
RATES OF REACTION AND THEIR DEPENDENCE ON ACTIVATION ENERGY  Activation Energy (Ea): “The least amount of energy needed for a chemical reaction to take place.”  Enzyme (as a catalyst) acts on substrate in such a way that they lower the activation energy by changing the route of the reaction.  The reduction of activation energy (Ea) increases the amount of reactant molecules that achieve a sufficient level of energy, so that they reach the activation energy and form the product. Example:  Carbonic anhydrase catalyses the hydration of 10⁶ CO₂ molecules per second which is 10⁷x faster than spontaneous hydration.
ENZYMES LOWER THE ACTIVATION ENERGY OF A REACTION Final energy state of products Initial energy state of substrates Activation energy of uncatalysed reactions Activation energy of enzyme catalysed reaction Progress of reaction (time) Energy levels of molecules
KINETICS OF ENZYMES CATALYSIS  Enzymes catalysis: “ It is an increase in the rate of reaction with the help of enzyme(as catalyst).”  Catalysis by enzymes that proceed mechanism, typically occurs when via unique reaction the transition state intermediate forms a covalent bond with the enzyme(covalent catalysis).  During the process of catalysis enzymes always emerge unchanged at the completion of the reaction.
FACTORS AFFECTING RATE OF ENZYME CATALYZED REACTIONS  Temperature  Hydrogen ion concentration(pH)  Substrate concentration
EFFECT OF TEMPERATURE  Raising the temperature increases the rate of enzyme catalyzed reaction by increasing kinetic energy of reacting molecules.  Enzymes work maximum over a particular temperature known as optimum temperature. Enzymes for humans generally exhibit stability temperature up to 35-45 ᵒ C.  The temperature coefficient is a factor Q₁₀ by which the rate of biological processes increases for a 10 ᵒ C increase in temperature.  For most biological processes Q₁₀ =2.  However some times heat energy can also increase kinetic energy to a point that exceed the energy barrier which results in denaturing of enzymes.
Rate of Reaction Temperature 40oC - denatures 5- 40oC Increase inActivity 0 10 20 30 40 50 60 <5oC - inactive
EFFECT OF PH  Rate of almost all enzymes catalyzed reactions depends on pH  Most enzymes exhibit optimal activity at pH value between 5 and 9  High or low pH value than optimum value will cause ionization of enzyme which result in denaturation of enzyme
PH AFFECTS THE FORMATION OF HYDROGEN BONDS AND SULPHUR BRIDGES IN PROTEINS AND SO AFFECTS SHAPE. pepsin trypsin arginase 2 4 8 10 6 pH Rate of Reaction (M) Acidic Basic
MICHAELIS-MENTEN MODEL & EFFECTS OF SUBSTRATE CONCENTRATION  Michaelis-Menten Model: “According to this model the enzyme reversibly combines with substrate to form an ES complex that subsequently yields product, regenerating the free enzyme.”      where: S is the substrate E is the enzyme ES-is the enzyme substrate complex P is the product K1,K-1 and K2 are rate constants E + S ES E + P k₁ k₋₁ k₂
MICHAELIS-MENTEN EQUATION  Michaelis-Menten Equation: “It is an equation which describes how reaction velocity varies with substrate concentration.” Vmax [S] Vo= Km+[S]  Where  Vo is the initial reaction velocity.  Vmax is the maximum velocity.  Km is the Michaelis constant =(k₋₁+k₂)/k₁.  [S] is the substrate concentration.
ASSUMPTIONS FOR MICHAELIS-MENTEN EQUATION  Following assumptions are made in deriving the Michaelis- Menten equation:  Relative concentrations of E and S.  Steady-State assumptions  Initial Velocity
SUBSTRATE CONCENTRATION
SUBSTRATE CONCENTRATION
PHARMACEUTICAL IMPORTANCE  Enzymes are virtually involved in all physiological processes which makes them the targets of choice for drugs that cure or ameliorate human disease.  Applied enzyme kinetics represents the principal tool by which scientist identify and characterize therapeutic agents that selectively inhibit the rates of specific enzymes catalyzed processes.  Enzymes kinetics thus play a critical role in drug discovery as well as elaborating the mode of action of drugs.
INHIBITION
INHIBITION o The prevention of an enzyme process as a result of interaction of inhibitors with the enzyme.  INHIBITORS: Any substance that can diminish the velocity of an enzyme catalyzed reaction is called an inhibitor.
TYPES OF INHIBITION Inhibition Reversible Competitive Uncompetitive Mixed Non- competitive Irreversible
REVERSIBLE INHIBITION o It is an inhibition of enzyme activity in which the inhibiting molecular entity can associate and dissociate from the protein„s binding site. TYPES OF REVERSIBLE INHIBITION o There are four types:  Competitive inhibition.  Uncompetitive inhibition.  Mixed inhibition.  Non-competitive inhibition.
COMPETITIVE INHIBITION  In this type of inhibition, the inhibitors compete with the substrate for the active site. Formation of E.S complex is reduced while a new E.I complex is formed.
EXAMPLES OF COMPETITIVE INHIBITION  Statin Drug As Example Of Competitive Inhibition:  Statin drugs such as lipitor compete with HMG-CoA(substrate) and inhibit the active site of HMG CoA-REDUCTASE (that bring about the catalysis of cholesterol synthesis).  (3-hydroxy-3-methyl-glutaryl-coenzyme A reductase,
UNCOMPETITIVE INHIBITION  In this type of inhibition, inhibitor does not compete with the substrate for the active site of enzyme instead it binds to another site known as allosteric site.
EXAMPLES OF UNCOMPETITIVE INHIBITION  Drugs to treat cases of poisoning by methanol or ethylene glycol act as uncompetitive inhibitors.  T etramethylene sulfoxide and 3- butylthiolene 1-oxide are uncompetitive inhibitors of liver alcohaldehydrogenase.
MIXED INHIBITION o In this type of inhibition both E.I and E.S.I complexes are formed. o Both complexes are catalytically inactive. NON COMPETITIVE INHIBITION o It is a special case of inhibition. o In this inhibitor has the same affinity for either enzyme E or the E.S complex.
IRREVERSIBLE INHIBITION  This type of inhibition involves the covalent attachment of the inhibitor to the enzyme.  The catalytic activity of enzyme is completely lost.  It can only be restored only by synthesizing molecules.
EXAMPLES OF IRREVERSIBLE INHIBITION  Aspirin which targets and covalently modifies a key enzyme involved in inflammation is an irreversible inhibitor.  SUICIDE INHIBITION :  It is an unusual type of irreversible inhibition where the enzyme converts the inhibitor into a reactive form in its active site.
ACTIVATION
ACTIVATION  Activation is defined as the conversion of an inactive form of an enzyme to active form which processes the metabolic activity. TYPES OF ACTIVATION  Activation by co-factors.  Conversion of an enzyme precursor.
ACTIVATION BY CO FACTORS  Many enzymes are activated by co-factors. Examples:  DNA polymerase is a holoenzyme that catalyzes the polymerization of de -oxyribonucleotide into a DNA strand. It uses Mg- ion for catalytic activity.  Horse liver dehydrogenase uses Zn- ion for it‟sactivation.
CONVERSION OF AN ENZYME PRECURSOR  Specific proteolysis is a common method of activating enzymes and other proteins in biological system. Example:  The generation of trypsin from trypsinogen leads to the activation of other zymogens.
ZYMOGEN ACTIVATION BY PROTEOLYTIC CLEAVAGE
ENZYME SPECIFICITY
ENZYME SPECIFICITY  Enzymes are highly specific in nature, interacting with one or few substrates and catalyzing only one type of chemical reaction.  Substrate specificity is due to complete fitting of active site and substrate . Example:  Oxydoreductase do not catalyze hydrolase reactions and hydrolase do not catalyze reaction involving oxidation and reduction.
TYPES OF ENZYME SPECIFICITY  Enzymes show different degrees of specificity:  Bond specificity.  Group specificity.  Absolute specificity.  Optical or stereo-specificity.  Dual specificity.
BOND SPECIFICITY  In this type, enzyme acts on substrates that are similar in structure and contain the same type of bond. Example :  Amylase which acts on α-1-4 glycosidic ,bond in starch dextrin and glycogen, shows bond specificity.
GROUP SPECIFICITY  In this type of specificity, the enzyme is specific not only to the type of bond but also to the structure surrounding it. Example:  Pepsin is an endopeptidase enzyme, that hydrolyzes central peptide bonds in which the amino group belongs to aromatic amino acids e. g phenyl alanine, tyrosine and tryptophan.
SUBSTRATE SPECIFICITY  In this type of specificity ,the enzymes acts only on one substrate Example :  Uricase ,which acts only on uric acid, shows substrate specificity.  Maltase , which acts only on maltose, shows substrate specificity.
OPTICAL / STEREO-SPECIFICITY  In this type of specificity , the enzyme is not specific to substrate but also to its optical configuration Example:  D amino acid oxidase acts only on D amino acids.  L amino acid oxidase acts only on L aminoacids.
DUAL SPECIFICITY  There are two types of dual specificity. may act on one substrate by two different  The enzyme reaction types. Example:  Isocitrate dehydrogenase enzyme acts on isocitrate (one substrate) by oxidation followed by decarboxylation(two different reaction types) .
 The enzyme may act on two substrates by one reaction type Example: • Xanthine oxidase enzyme acts on xanthine and hypoxanthine(two substrates) by oxidation (one reaction type) DUAL SPECIFICITY
REFERENCES  Woodbury.: Biochemistry for the Pharmaceutical Sciences  Lehninger.: Principles of biochemistry  Lippincott.: Biochemistry  Harper's Illustrated Biochemistry  Mushtaq Ahmed.: Essentials of Medical Biochemistry  Pfeiffer, J.: Enzymes, the Physics and Chemistry of Life  Martinek, R.: Practical Clinical Enzymology
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Enzymes msc

  • 1. ENZYMES Rahana Moideen Koya.V.K MSc,Mphil,Med,MA Assistant Professor,Dept.of Zoology Farook College,Kozhikode.Kerala.
  • 2. CONTENTS Chemistry Classification Mechanism of EnzymeAction Enzyme Kinetics Inhibition Activation Specificity
  • 3. Introduction  Enzymes are biological catalysts that speed up the rate of the biochemical reaction.  Most enzymes are three dimensional globular proteins (tertiary and quaternary structure).  Some special RNA species enzymes and are called Ribozymes also act as e.g. hammerhead ribozyme. Hammerhead enzyme
  • 4. STRUCTURE OF ENZYMES  The active site of an enzyme is the region that binds substrates, co-factors and prosthetic groups and contains residue that helps to hold the substrate.  Active sites generally occupy less than 5% of the total surface area of enzyme.  Active site has a specific shape due to tertiary structure of protein.  A change in the shape of protein affects the shape of active site and function of the enzyme.
  • 5. ACTIVE SITE It chooses the substrate and binds it to active site. It performs the catalytic action of enzyme. o Active site can be further divided into: Active Site Binding Site Catalytic Site
  • 6. CO-FACTORS o Co-factor is the non protein molecule which carries out chemical reactions that can not be performed by standard 20 amino acids. o Co-factors are of two types:  Organic co-factors  Inorganic cofactors
  • 7. INORGANIC CO-FACTORS o These are the inorganic molecules required for the proper activity of enzymes. Examples:  Enzyme carbonic anhydrase requires Zn for it‟sactivity.  Hexokinase has co-factor Mg ORGANIC CO-FACTORS o These are the organic molecules required for the proper activity of enzymes. Example:  Glycogen phosphorylase requires the small organic molecule pyridoxal phosphate. ++ ++
  • 8.
  • 9. TYPES OF ORGANIC CO-FACTORS Prosthetic Group Coenzyme A prosthetic group is a tightly bound organic co- factor e.g. Flavins, heme groups and biotin. o A coenzyme is loosely bound organic co-factor. factor e.g. heme E.g. NAD+
  • 10.  An enzyme with it‟ s co-factor removed is designated as apoenzyme.  The complete complex of a protein with all necessary small organic molecules, metal ions and other components is termed as holoenzyme of holoprotein. Types of co-factors Continued…
  • 11.
  • 12. SUBSTRATE  The reactant in biochemical reaction is termed as substrate.  When a substrate binds to an enzyme it forms an enzyme- substrate complex. Enzyme Joins Substrate
  • 13. SITES OF ENZYME SYNTHESIS o Enzymes are synthesized by ribosomes which are attached to the rough endoplasmic reticulum. o Information for the synthesis of enzyme is carried by DNA. o Amino acids are bonded together to form specific enzyme according to the DNA‟scodes.
  • 14. INTRACELLULAR AND EXTRACELLULAR ENZYMES o Intracellular enzymes are synthesized and retained in the cell for the use of cell itself. o They are found in the cytoplasm, nucleus, mitochondria and chloroplast. Example :  Oxydoreductase catalyses biological oxidation.  Enzymes involved in reduction in the mitochondria. in the cell but o Extracellular enzymes are synthesized secreted from the cell to work externally. Example :  Digestive enzyme produced by the pancreas, are not used by the cells in the pancreas but are transported to the duodenum.
  • 15. CHARACTERISTICS  Enzymes speed up the reaction by lowering the activation energy of the reaction.  Their presence does not effect the nature and properties of end product.  They are highly specific in their action that is each enzyme can catalyze one kind of substrate.  Small amount of enzymes can accelerate chemical reactions.  Enzymes are sensitive to change in pH, temperature and substrate concentration.  Turnover number is defined as the number of substrate molecules transformed per minute by one enzyme molecule. Catalase turnover number = 6 x106/min
  • 16. NOMENCLATURE OF ENZYMES o An enzyme is named according to the name of the substrate it catalyses. o Some enzymes were named before a systematic way of naming enzyme was formed. Example: pepsin, trypsin and rennin o By adding suffix -ase at the end of the name of the substrate, enzymes are named. o Enzyme for catalyzing the hydrolysis is termed as hydrolase. Example : maltose + water glucose + glucose maltase
  • 17. EXAMPLES substrate enzymes products lactose lactase glucose + galactose maltose maltase Glucose cellulose cellulase Glucose lipid lipase Glycerol + fatty acid starch amylase Maltose protein protease Peptides + polypeptide
  • 19. CLASSIFICATION OF ENZYMES  A systematic classification of enzymes has been developed by International Enzyme Commission.  This classification is based on the type of reactions catalyzed by enzymes.  There are six major classes.  Each class is further divided into sub classes, sub sub-classes and so on, to describe the huge number of different enzyme- catalyzed reactions.
  • 20. ENZYME CLASS REACTION TYPE EXAMPLES Oxidoreductases Reduction-oxidation (redox) Lactate dehydrogenase Transferases Move chemical group Hexokinase Hydrolases Hydrolysis; bond cleavage with transfer of functional group of water Lysozyme Lyases Non-hydrolytic bond cleavage Fumarase Isomerases Intramolecular group transfer (isomerization) Triose phosphate isomerase Ligases Synthesis of new covalent bond between substrates, using ATPhydrolysis RNA polymerase Continued…….. Classification of enzymes
  • 22. MECHANISM OF ENZYME ACTION  The catalytic efficiency of enzymes is explained by two perspectives: Thermodynamic changes Processes at the active site
  • 23. THERMODYNAMIC CHANGES  All chemical reactions have energy barriers between reactants and products.  The difference in transitional state and substrate is called activational barrier.
  • 24. THERMODYNAMIC CHANGES  Only a few substances cross the activation barrier and change into products.  That is why rate of uncatalyzed reactions is much slow.  Enzymes provide an alternate pathway for conversion of substrate into products.  Enzymes accelerate reaction rates by forming transitional state having low activational energy.  Hence, the reaction rate is increased many folds in the presence of enzymes.  The total energy of the system remains the same and equilibrium state is not disturbed.
  • 26. PROCESSES AT THE ACTIVE SITE Covalent catalysis Acid base catalysis Catalysis by strain Catalysis by proximity
  • 27. COVALENT CATALYSIS o Enzymes form covalent linkages with substrate forming transient enzyme-substrate complex with very low activation energy. o Enzyme is released unaltered after completion of reaction.
  • 28. ACID-BASE CATALYSIS  Mostly undertaken by oxido- reductases enzyme.  Mostly at the active site, histdine is present which act as both proton donor and proton acceptor.
  • 29. CATALYSIS BY PROXIMITY forming  In this catalysis molecules must come in bond distance.  When enzyme binds:  A region of high substrate concentration is produced at active site.  This will orient substrate molecules especially in a position ideal for them.
  • 30. CATALYSIS BY BOND STRAIN  Mostly undertaken by lyases.  The enzyme-substrate binding causes reorientation of the structure of site due to in a strain condition.  Thus transitional state is required and here bond is unstable and eventually broken.  In this way bond between substrate is broken and converted into products.
  • 31. LOCK AND KEY MODEL  Proposed by EMIL FISCHER in 1894.  Lock and key hypothesis assumes the active site of an enzymes are rigid in its shape.  There is no change in the active site before and after a chemical reaction.
  • 32. INDUCED FIT MODEL  More recent studies have revealed that the process is much more likely to involve an induced fit model(proposed by DANIAL KOSH LAND in 1958).  According to this exposure of an enzyme to substrate cause a change in enzyme, which causes the active site to change i t ‟ s shape to allow enzyme and substrate to bind.
  • 35. INTRODUCTION “It is a branch of biochemistry in which we study the rate of enzyme catalyzed reactions.”  Kinetic analysis reveals the number and order of the individual steps by which enzymes transform substrate into products  Studying an enzyme's kinetics in this way can reveal the catalytic mechanism of that enzyme, its role in metabolism, how its activity is controlled, and how a drug or an agonist might inhibit the enzyme
  • 36.
  • 37.
  • 38.
  • 39.
  • 40.
  • 41.
  • 42.
  • 43. RATES OF REACTION AND THEIR DEPENDENCE ON ACTIVATION ENERGY  Activation Energy (Ea): “The least amount of energy needed for a chemical reaction to take place.”  Enzyme (as a catalyst) acts on substrate in such a way that they lower the activation energy by changing the route of the reaction.  The reduction of activation energy (Ea) increases the amount of reactant molecules that achieve a sufficient level of energy, so that they reach the activation energy and form the product. Example:  Carbonic anhydrase catalyses the hydration of 10⁶ CO₂ molecules per second which is 10⁷x faster than spontaneous hydration.
  • 44. ENZYMES LOWER THE ACTIVATION ENERGY OF A REACTION Final energy state of products Initial energy state of substrates Activation energy of uncatalysed reactions Activation energy of enzyme catalysed reaction Progress of reaction (time) Energy levels of molecules
  • 45. KINETICS OF ENZYMES CATALYSIS  Enzymes catalysis: “ It is an increase in the rate of reaction with the help of enzyme(as catalyst).”  Catalysis by enzymes that proceed mechanism, typically occurs when via unique reaction the transition state intermediate forms a covalent bond with the enzyme(covalent catalysis).  During the process of catalysis enzymes always emerge unchanged at the completion of the reaction.
  • 46. FACTORS AFFECTING RATE OF ENZYME CATALYZED REACTIONS  Temperature  Hydrogen ion concentration(pH)  Substrate concentration
  • 47. EFFECT OF TEMPERATURE  Raising the temperature increases the rate of enzyme catalyzed reaction by increasing kinetic energy of reacting molecules.  Enzymes work maximum over a particular temperature known as optimum temperature. Enzymes for humans generally exhibit stability temperature up to 35-45 ᵒ C.  The temperature coefficient is a factor Q₁₀ by which the rate of biological processes increases for a 10 ᵒ C increase in temperature.  For most biological processes Q₁₀ =2.  However some times heat energy can also increase kinetic energy to a point that exceed the energy barrier which results in denaturing of enzymes.
  • 48. Rate of Reaction Temperature 40oC - denatures 5- 40oC Increase inActivity 0 10 20 30 40 50 60 <5oC - inactive
  • 49. EFFECT OF PH  Rate of almost all enzymes catalyzed reactions depends on pH  Most enzymes exhibit optimal activity at pH value between 5 and 9  High or low pH value than optimum value will cause ionization of enzyme which result in denaturation of enzyme
  • 50. PH AFFECTS THE FORMATION OF HYDROGEN BONDS AND SULPHUR BRIDGES IN PROTEINS AND SO AFFECTS SHAPE. pepsin trypsin arginase 2 4 8 10 6 pH Rate of Reaction (M) Acidic Basic
  • 51. MICHAELIS-MENTEN MODEL & EFFECTS OF SUBSTRATE CONCENTRATION  Michaelis-Menten Model: “According to this model the enzyme reversibly combines with substrate to form an ES complex that subsequently yields product, regenerating the free enzyme.”      where: S is the substrate E is the enzyme ES-is the enzyme substrate complex P is the product K1,K-1 and K2 are rate constants E + S ES E + P k₁ k₋₁ k₂
  • 52. MICHAELIS-MENTEN EQUATION  Michaelis-Menten Equation: “It is an equation which describes how reaction velocity varies with substrate concentration.” Vmax [S] Vo= Km+[S]  Where  Vo is the initial reaction velocity.  Vmax is the maximum velocity.  Km is the Michaelis constant =(k₋₁+k₂)/k₁.  [S] is the substrate concentration.
  • 53. ASSUMPTIONS FOR MICHAELIS-MENTEN EQUATION  Following assumptions are made in deriving the Michaelis- Menten equation:  Relative concentrations of E and S.  Steady-State assumptions  Initial Velocity
  • 56. PHARMACEUTICAL IMPORTANCE  Enzymes are virtually involved in all physiological processes which makes them the targets of choice for drugs that cure or ameliorate human disease.  Applied enzyme kinetics represents the principal tool by which scientist identify and characterize therapeutic agents that selectively inhibit the rates of specific enzymes catalyzed processes.  Enzymes kinetics thus play a critical role in drug discovery as well as elaborating the mode of action of drugs.
  • 58. INHIBITION o The prevention of an enzyme process as a result of interaction of inhibitors with the enzyme.  INHIBITORS: Any substance that can diminish the velocity of an enzyme catalyzed reaction is called an inhibitor.
  • 59. TYPES OF INHIBITION Inhibition Reversible Competitive Uncompetitive Mixed Non- competitive Irreversible
  • 60.
  • 61. REVERSIBLE INHIBITION o It is an inhibition of enzyme activity in which the inhibiting molecular entity can associate and dissociate from the protein„s binding site. TYPES OF REVERSIBLE INHIBITION o There are four types:  Competitive inhibition.  Uncompetitive inhibition.  Mixed inhibition.  Non-competitive inhibition.
  • 62. COMPETITIVE INHIBITION  In this type of inhibition, the inhibitors compete with the substrate for the active site. Formation of E.S complex is reduced while a new E.I complex is formed.
  • 63.
  • 64.
  • 65. EXAMPLES OF COMPETITIVE INHIBITION  Statin Drug As Example Of Competitive Inhibition:  Statin drugs such as lipitor compete with HMG-CoA(substrate) and inhibit the active site of HMG CoA-REDUCTASE (that bring about the catalysis of cholesterol synthesis).  (3-hydroxy-3-methyl-glutaryl-coenzyme A reductase,
  • 66. UNCOMPETITIVE INHIBITION  In this type of inhibition, inhibitor does not compete with the substrate for the active site of enzyme instead it binds to another site known as allosteric site.
  • 67.
  • 68. EXAMPLES OF UNCOMPETITIVE INHIBITION  Drugs to treat cases of poisoning by methanol or ethylene glycol act as uncompetitive inhibitors.  T etramethylene sulfoxide and 3- butylthiolene 1-oxide are uncompetitive inhibitors of liver alcohaldehydrogenase.
  • 69. MIXED INHIBITION o In this type of inhibition both E.I and E.S.I complexes are formed. o Both complexes are catalytically inactive. NON COMPETITIVE INHIBITION o It is a special case of inhibition. o In this inhibitor has the same affinity for either enzyme E or the E.S complex.
  • 70.
  • 71.
  • 72. IRREVERSIBLE INHIBITION  This type of inhibition involves the covalent attachment of the inhibitor to the enzyme.  The catalytic activity of enzyme is completely lost.  It can only be restored only by synthesizing molecules.
  • 73.
  • 74. EXAMPLES OF IRREVERSIBLE INHIBITION  Aspirin which targets and covalently modifies a key enzyme involved in inflammation is an irreversible inhibitor.  SUICIDE INHIBITION :  It is an unusual type of irreversible inhibition where the enzyme converts the inhibitor into a reactive form in its active site.
  • 76. ACTIVATION  Activation is defined as the conversion of an inactive form of an enzyme to active form which processes the metabolic activity. TYPES OF ACTIVATION  Activation by co-factors.  Conversion of an enzyme precursor.
  • 77. ACTIVATION BY CO FACTORS  Many enzymes are activated by co-factors. Examples:  DNA polymerase is a holoenzyme that catalyzes the polymerization of de -oxyribonucleotide into a DNA strand. It uses Mg- ion for catalytic activity.  Horse liver dehydrogenase uses Zn- ion for it‟sactivation.
  • 78. CONVERSION OF AN ENZYME PRECURSOR  Specific proteolysis is a common method of activating enzymes and other proteins in biological system. Example:  The generation of trypsin from trypsinogen leads to the activation of other zymogens.
  • 81. ENZYME SPECIFICITY  Enzymes are highly specific in nature, interacting with one or few substrates and catalyzing only one type of chemical reaction.  Substrate specificity is due to complete fitting of active site and substrate . Example:  Oxydoreductase do not catalyze hydrolase reactions and hydrolase do not catalyze reaction involving oxidation and reduction.
  • 82. TYPES OF ENZYME SPECIFICITY  Enzymes show different degrees of specificity:  Bond specificity.  Group specificity.  Absolute specificity.  Optical or stereo-specificity.  Dual specificity.
  • 83. BOND SPECIFICITY  In this type, enzyme acts on substrates that are similar in structure and contain the same type of bond. Example :  Amylase which acts on α-1-4 glycosidic ,bond in starch dextrin and glycogen, shows bond specificity.
  • 84. GROUP SPECIFICITY  In this type of specificity, the enzyme is specific not only to the type of bond but also to the structure surrounding it. Example:  Pepsin is an endopeptidase enzyme, that hydrolyzes central peptide bonds in which the amino group belongs to aromatic amino acids e. g phenyl alanine, tyrosine and tryptophan.
  • 85. SUBSTRATE SPECIFICITY  In this type of specificity ,the enzymes acts only on one substrate Example :  Uricase ,which acts only on uric acid, shows substrate specificity.  Maltase , which acts only on maltose, shows substrate specificity.
  • 86. OPTICAL / STEREO-SPECIFICITY  In this type of specificity , the enzyme is not specific to substrate but also to its optical configuration Example:  D amino acid oxidase acts only on D amino acids.  L amino acid oxidase acts only on L aminoacids.
  • 87. DUAL SPECIFICITY  There are two types of dual specificity. may act on one substrate by two different  The enzyme reaction types. Example:  Isocitrate dehydrogenase enzyme acts on isocitrate (one substrate) by oxidation followed by decarboxylation(two different reaction types) .
  • 88.  The enzyme may act on two substrates by one reaction type Example: • Xanthine oxidase enzyme acts on xanthine and hypoxanthine(two substrates) by oxidation (one reaction type) DUAL SPECIFICITY
  • 89. REFERENCES  Woodbury.: Biochemistry for the Pharmaceutical Sciences  Lehninger.: Principles of biochemistry  Lippincott.: Biochemistry  Harper's Illustrated Biochemistry  Mushtaq Ahmed.: Essentials of Medical Biochemistry  Pfeiffer, J.: Enzymes, the Physics and Chemistry of Life  Martinek, R.: Practical Clinical Enzymology