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Protein and Peptides .ppt

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Girdhar Sahu

PROTEINS: Proteins are the organic compounds made of amino acids and joined together by peptide bonds. PEPTIDES: These are short polymers formed from the linking in a defined order of amino acids. Protein and peptides are the most abundant material which act as hormones, transport protein, structural protein, receptor, immunoglobulin’s in living system and biological cell. Protein and peptides are important part in several metabolic process, immunogenic defense and many other biological activities. Protein and peptide use in the treatment of various diseases including Endocrine dysfunction, Infection diseases, Cancer, and CNS disorders. According to their biological roles Enzymes- Catalyses virtually all chemical reaction Transport proteins i.e. Haemoglobin of erythrocytes Defense proteins i.e. Immuno globulins Antibodies Structural proteins i.e. Collagen in bones Regulatory proteins i.e. insulin Nutrient and storage proteins i.e. ovalbumin According to their solubility Globular proteins: Soluble in Water Fibrous proteins: Insoluble in water WHY PROTEN AND PEPTIDE DRUGS? The protein and peptide are very important in biological cells. Lack of proteins and peptides causes diseases like Diabetes mellitus. Diabetes mellitus is cause due to the lack of protein called INSULIN. Now a day R-DNA technology and hybridoma also use in protein and peptide based pharmaceuticals. FUNCTIONS Transport and storage of small molecules. Coordinated motion via muscle contraction. Mechanical support from fibrous protein. Generation and transmission of nerve impulses. Enzymatic catalysis. Immune protection through antibodies. Control of growth and differentiation via hormones. Problems with proteins Elimination by B and T cells. Proteolysis by endo/exo peptidases. Small proteins filtered out by the kidneys very quickly. Unwanted allergic reactions may develop (even toxicity). Loss due to insolubility/adsorption.

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PROTEN AND PEPTIDE DRUG DELIVERY SYSTEM UNDER THE GUIDENCE, OF Dr. Lalit Kumar Tyagi M. Pharm, Ph.D. Presented By Girdhar kumar Sahu M. Pharm 1st Yr Department of pharmaceutics Lloyd Institute of Management and Technology [PHARM.]
CONTENTS  Protein and peptides  Classification of protein  Properties of proteins and peptides  Stability problems  Barriers to protein drug delivery  Drug delivery system  Stability testing  References
INTRODUCTION PROTEINS: Proteins are the organic compounds made of amino acids and joined together by peptide bonds. PEPTIDES: These are short polymers formed from the linking in a defined order of amino acids.  Protein and peptides are the most abundant material which act as hormones, transport protein, structural protein, receptor, immunoglobulin’s in living system and biological cell.
Cont.. Protein and peptides are important part in several metabolic process, immunogenic defense and many other biological activities. Protein and peptide use in the treatment of various diseases including Endocrine dysfunction, Infection diseases, Cancer, and CNS disorders.
CLASSIFICATION OF PROTEINS According to their biological roles Enzymes- Catalyses virtually all chemical reaction Transport proteins i.e. Haemoglobin of erythrocytes Defense proteins i.e. Immuno globulins Antibodies Structural proteins i.e. Collagen in bones Regulatory proteins i.e. insulin Nutrient and storage proteins i.e. ovalbumin According to their solubility Globular proteins: Soluble in Water Fibrous proteins: Insoluble in water
WHY PROTEN AND PEPTIDE DRUGS? The protein and peptide are very important in biological cells. Lack of proteins and peptides causes diseases like Diabetes mellitus. Diabetes mellitus is cause due to the lack of protein called INSULIN. Now a day R-DNA technology and hybridoma also use in protein and peptide based pharmaceuticals.
FUNCTIONS Transport and storage of small molecules. Coordinated motion via muscle contraction. Mechanical support from fibrous protein. Generation and transmission of nerve impulses. Enzymatic catalysis. Immune protection through antibodies. Control of growth and differentiation via hormones.
ADVANTAGES Erythroprotein used for production of RBC. Tissue plasminogen activitor is used for heart attack, stroke. Oxytocin maintain labor pain. Somatostatin decrease bleeding in gastric ulcer. Gonadotropin induce ovulation. Insulin maintain blood sugar lever.
DISADVANTGES Very large and unstable molecules. Easily destroyed by relatively mild storage condition and gastric juices. Hard to obtain in large quantities.
PROPERTIES OF PROTEEINNS AND PEPTIDES  Molecular size weight of protein: The large molecular weight have low diffusivity and small molecule (75-100 dalton) cross barrier.  Stereo-specificity, Conformation: Affects the permeability.  Solubility and partition coefficient: Peptides are very hydrophilic, so to improve the absorption of peptides by passive diffusion, their lipophilicity should be increased.
PROBLEMS WITH PROTEINS Elimination by B and T cells. Proteolysis by endo/exo peptidases. Small proteins filtered out by the kidneys very quickly. Unwanted allergic reactions may develop (even toxicity). Loss due to insolubility/adsorption.
 Enzymatic Barrier  Intestinal Epithelial Barrier  Capillary Epithelial Barrier  Blood Brain Barrier BARRIERS TO PROTEIN DRUG DELIVERY
ENZYMATIC BARRIERS  • The enzymatic degradation is brought about mainly via two ways:  1. Hydrolytic cleavage of peptide bonds by processes, such as insulin-degrading enzyme, angiotensin- converting enzymes and renin. Proteolysis is an irreversible reaction and hence potentially causes the of damage of the peptide and protein drug.  2.Chemical modification of protein such as phosphorylation by kinases, oxidation by xanthine- oxidase or glucos oxidase.  It limits absorption of protein drugs from G.I tract
INTESTINAL EPITHELIAL BARRIER  Intestinal epithelial barrier Serves as a barrier for transport of protein drugs across the intestinal epithelium.  Several mechanisms that are involved in the transport of peptide /protein drugs across the intestinal epithelium are  A. Passive & carrier mediated transport  B. Endocytosis & Transcytosis  C. Paracellular Movement
A. Passive and carrier mediated transport:  Active transport appears to be the predominant mechanism. Accounts for the extensive absorption of di-and tripeptides from small intestine. B. Endocytosis and transcytosis  Cellular internalization of peptides/proteins may occur by Endocytosis whereby peptide /proteins, which are too large to be absorbed by carrier mediated transport, are taken up.  The Different pathways of Endocytosis involve Phagocytosis Pinocytosis (cell drinking). C. Paracellular movement:  The transport of drugs through the junction between the GI epithelial cells.  Two mechanism involved in drug absorption are-1.Permeation through tight junction of epithelial cells (insulin) 2.Persorption  The small intestine epithelial mucosa serves as a barrier to the permeation of macromolecules
CAPILLARY ENDOTHELIAL BARRIER  To cross the capillary endothelium the peptides/proteins must pass between the cells or alternatively transverse across the endothelial cells themselves.  Solutes that transverse the endothelial cell membrane may get modified or metabolized by cytoplasmic enzymes.  Thus, the endothelial passage poses metabolic or enzymatic barrier to the solution passage
BLOOD BRAIN BARRIER (BBB)  The blood-brain barrier (BBB) represents a major obstacle to the delivery of proteins to the brain compartment. It consists of several barriers with the two that are best described being the vascular BBB, and the blood- cerebrospinal fluid (blood-CSF) barrier.  At both sites, the BBB is formed by a monolayer of cells that are cementedtogether by tight junctions and have other mechanisms that control or retardleakage of plasma into the CNS.  Allows passage of small, lipophilic, uncharged molecules and gases. Large molecules like proteins do not pass the BBB easily
PHARMACEUTICALAPPROACHES OF PROTEIN AND PEPTIDES  CHEMICAL MODIFICATION  ENZYME INHIBITORS  PENETRATION ENHANCERS  FORMULATION VEHICLE  MUCOADHESIVE POLYMERIC SYSTEM
1. CHEMICAL MODIFICATION (PRODRUG APPROACH)  The Chemical Modification of Protein and Peptide Drug Delivery System of Drugs is Important to Improve the Enzymatic Stability as well as Membrane Permeations.  It is Applicable for the reducing the Immunogenicity.  The Chemical Modification is Includes in Two Types of Modifications 1. Amino acid Modification: The Modification of amino acid is one of the important approach in which the Substitution of the D- amino acid and L- amino acid is important to alter the Physiological Properties of Protein and Peptide Drug Delivery Systems 2. Hydrophobization: It is having an important approach for the Lipophilic Moieties
2. ENZYME INHIBITORS (PROTEASE): The enzyme (protease) inhibitors are the enzymatic approach of the Protein a 3 . PENETRATION ENHANCERS: Penetration enhancers are the one of the most important Component of Protein and Peptides formulation is responsible for the Disruption of the Mucosal Barriers and applicable to improve the Membrane Permeations of Large Macromolecular substances lie Proteins and Peptides. 4 . FORMULATION VEHICLES: The Protein and Peptide Drug Delivery system is important for the Oral Delivery of Protein and Peptides can be successfully achieved by using various carrier systems are like 1. Dry Emulsion 2. Microspheres 3. Liposomes 4. Nanoparticles
 1. Dry Emulsion is prepared by the Spray drying, Lyophollization and evaporation Techniques. In dry emulsion preparation application of the PH responsive polymers like HPMCP, is important for the emulsions are the enteric coated and site specific achieved.  2. Microspheres: The uniform distribution of drug in oral drug delivery in Protein peptides drug are known as Microspheres. The PH responsive microspheres are the mainly used in oral delivery for the protection of the stomach from proteolytic degradations and Protection upper portion of small intestine from proteolytic degradations.
 3. Liposomes: Liposomes are the small microscopic vesicles in which aqueous volume is entirely enclosed by the membrane composed lipid molecules. Liposomes in drug delivery system, the encapsulation of the insulin with sugar chain portion of mucin and PEG completely suppressed the degradation of the insulin molecules in intestinal fluid. The uncoated from of liposomes are suppressed it on partially surface coating of the liposomes molecules in PEG or mucin gained resistances against dagestion by salts and increased the stability of GI tract.  4. Nanoparticles: Nanoparticles are Nano sized colloidal structure having size is 10-1000nm. The particles in nanometric sized range of the particles are absorbed intact by the intestinal epithelium and they are the less prone towards the enzymatic degradations. The particle size surface charges are the influencing the uptake of nanoparticle system in GI tract.
5. MUCOADHESIVE POLYMERIC SYSTEMS The mucoadhesive polymeric system is important to prevent the problem associated in Presystemic Metabolism or first pass metabolism and maintain its therapeutic efficacy. The residence time of this drug delivery systems at the site of action and the increasing or decreasing the drug clearance rate.
STABILITY ASPECTS In stability of protein and peptide is determined by the Protein degradations PathwaysIn This drug delivery system under two Pathways of degradation of Protein and Peptide Molecules 1.Physical Degradation Pathways (Instability Aspects) 2.Chemical Degradation Pathways (Instability Aspects) 1. Physical Instabilities: The Physical Degradation Pathways the Native or original structure of Protein is Changes or Modified to from Higher order Structure of Proteins (secondary, tertiary or quaternary structure). 2. Chemical Instabilities: Chemical degradation Pathways the Native or original structure of protein is changes by the modification of their Primary Structure of Protein Molecules.The chemical instability of the protein and Peptide can causes following four types of reactions. 3. Oxidation 4. 2. Deamination 5. 3. Peptide bond hydrolysis 6. 4. Disulphide exchange
APPLICATION  1. CVS acing drugs Protein and Peptides  CNS active Protein and Peptides  GI-active Protein and Peptides  Immunomodulation of the Protein and Peptides  Metabolism modulating Protein and Peptides
REFERENCE  Sagar Kishor Savale, Protein and peptide drug delivery system, world journal of pharmacy and pharmaceutical sciences, Vol 5, Issue 4, 2016  A text book of drug delivery system, Prafull P.Patil pg. 189-216.  P. keerthi, Protein and peptide drug delivery system, 201 4.
Thankyou!

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Protein and Peptides .ppt

  • 1. PROTEN AND PEPTIDE DRUG DELIVERY SYSTEM UNDER THE GUIDENCE, OF Dr. Lalit Kumar Tyagi M. Pharm, Ph.D. Presented By Girdhar kumar Sahu M. Pharm 1st Yr Department of pharmaceutics Lloyd Institute of Management and Technology [PHARM.]
  • 2. CONTENTS  Protein and peptides  Classification of protein  Properties of proteins and peptides  Stability problems  Barriers to protein drug delivery  Drug delivery system  Stability testing  References
  • 3. INTRODUCTION PROTEINS: Proteins are the organic compounds made of amino acids and joined together by peptide bonds. PEPTIDES: These are short polymers formed from the linking in a defined order of amino acids.  Protein and peptides are the most abundant material which act as hormones, transport protein, structural protein, receptor, immunoglobulin’s in living system and biological cell.
  • 4. Cont.. Protein and peptides are important part in several metabolic process, immunogenic defense and many other biological activities. Protein and peptide use in the treatment of various diseases including Endocrine dysfunction, Infection diseases, Cancer, and CNS disorders.
  • 5. CLASSIFICATION OF PROTEINS According to their biological roles Enzymes- Catalyses virtually all chemical reaction Transport proteins i.e. Haemoglobin of erythrocytes Defense proteins i.e. Immuno globulins Antibodies Structural proteins i.e. Collagen in bones Regulatory proteins i.e. insulin Nutrient and storage proteins i.e. ovalbumin According to their solubility Globular proteins: Soluble in Water Fibrous proteins: Insoluble in water
  • 6. WHY PROTEN AND PEPTIDE DRUGS? The protein and peptide are very important in biological cells. Lack of proteins and peptides causes diseases like Diabetes mellitus. Diabetes mellitus is cause due to the lack of protein called INSULIN. Now a day R-DNA technology and hybridoma also use in protein and peptide based pharmaceuticals.
  • 7. FUNCTIONS Transport and storage of small molecules. Coordinated motion via muscle contraction. Mechanical support from fibrous protein. Generation and transmission of nerve impulses. Enzymatic catalysis. Immune protection through antibodies. Control of growth and differentiation via hormones.
  • 8. ADVANTAGES Erythroprotein used for production of RBC. Tissue plasminogen activitor is used for heart attack, stroke. Oxytocin maintain labor pain. Somatostatin decrease bleeding in gastric ulcer. Gonadotropin induce ovulation. Insulin maintain blood sugar lever.
  • 9. DISADVANTGES Very large and unstable molecules. Easily destroyed by relatively mild storage condition and gastric juices. Hard to obtain in large quantities.
  • 10. PROPERTIES OF PROTEEINNS AND PEPTIDES  Molecular size weight of protein: The large molecular weight have low diffusivity and small molecule (75-100 dalton) cross barrier.  Stereo-specificity, Conformation: Affects the permeability.  Solubility and partition coefficient: Peptides are very hydrophilic, so to improve the absorption of peptides by passive diffusion, their lipophilicity should be increased.
  • 11. PROBLEMS WITH PROTEINS Elimination by B and T cells. Proteolysis by endo/exo peptidases. Small proteins filtered out by the kidneys very quickly. Unwanted allergic reactions may develop (even toxicity). Loss due to insolubility/adsorption.
  • 12.  Enzymatic Barrier  Intestinal Epithelial Barrier  Capillary Epithelial Barrier  Blood Brain Barrier BARRIERS TO PROTEIN DRUG DELIVERY
  • 13. ENZYMATIC BARRIERS  • The enzymatic degradation is brought about mainly via two ways:  1. Hydrolytic cleavage of peptide bonds by processes, such as insulin-degrading enzyme, angiotensin- converting enzymes and renin. Proteolysis is an irreversible reaction and hence potentially causes the of damage of the peptide and protein drug.  2.Chemical modification of protein such as phosphorylation by kinases, oxidation by xanthine- oxidase or glucos oxidase.  It limits absorption of protein drugs from G.I tract
  • 14. INTESTINAL EPITHELIAL BARRIER  Intestinal epithelial barrier Serves as a barrier for transport of protein drugs across the intestinal epithelium.  Several mechanisms that are involved in the transport of peptide /protein drugs across the intestinal epithelium are  A. Passive & carrier mediated transport  B. Endocytosis & Transcytosis  C. Paracellular Movement
  • 15. A. Passive and carrier mediated transport:  Active transport appears to be the predominant mechanism. Accounts for the extensive absorption of di-and tripeptides from small intestine. B. Endocytosis and transcytosis  Cellular internalization of peptides/proteins may occur by Endocytosis whereby peptide /proteins, which are too large to be absorbed by carrier mediated transport, are taken up.  The Different pathways of Endocytosis involve Phagocytosis Pinocytosis (cell drinking). C. Paracellular movement:  The transport of drugs through the junction between the GI epithelial cells.  Two mechanism involved in drug absorption are-1.Permeation through tight junction of epithelial cells (insulin) 2.Persorption  The small intestine epithelial mucosa serves as a barrier to the permeation of macromolecules
  • 16. CAPILLARY ENDOTHELIAL BARRIER  To cross the capillary endothelium the peptides/proteins must pass between the cells or alternatively transverse across the endothelial cells themselves.  Solutes that transverse the endothelial cell membrane may get modified or metabolized by cytoplasmic enzymes.  Thus, the endothelial passage poses metabolic or enzymatic barrier to the solution passage
  • 17. BLOOD BRAIN BARRIER (BBB)  The blood-brain barrier (BBB) represents a major obstacle to the delivery of proteins to the brain compartment. It consists of several barriers with the two that are best described being the vascular BBB, and the blood- cerebrospinal fluid (blood-CSF) barrier.  At both sites, the BBB is formed by a monolayer of cells that are cementedtogether by tight junctions and have other mechanisms that control or retardleakage of plasma into the CNS.  Allows passage of small, lipophilic, uncharged molecules and gases. Large molecules like proteins do not pass the BBB easily
  • 18. PHARMACEUTICALAPPROACHES OF PROTEIN AND PEPTIDES  CHEMICAL MODIFICATION  ENZYME INHIBITORS  PENETRATION ENHANCERS  FORMULATION VEHICLE  MUCOADHESIVE POLYMERIC SYSTEM
  • 19. 1. CHEMICAL MODIFICATION (PRODRUG APPROACH)  The Chemical Modification of Protein and Peptide Drug Delivery System of Drugs is Important to Improve the Enzymatic Stability as well as Membrane Permeations.  It is Applicable for the reducing the Immunogenicity.  The Chemical Modification is Includes in Two Types of Modifications 1. Amino acid Modification: The Modification of amino acid is one of the important approach in which the Substitution of the D- amino acid and L- amino acid is important to alter the Physiological Properties of Protein and Peptide Drug Delivery Systems 2. Hydrophobization: It is having an important approach for the Lipophilic Moieties
  • 20. 2. ENZYME INHIBITORS (PROTEASE): The enzyme (protease) inhibitors are the enzymatic approach of the Protein a 3 . PENETRATION ENHANCERS: Penetration enhancers are the one of the most important Component of Protein and Peptides formulation is responsible for the Disruption of the Mucosal Barriers and applicable to improve the Membrane Permeations of Large Macromolecular substances lie Proteins and Peptides. 4 . FORMULATION VEHICLES: The Protein and Peptide Drug Delivery system is important for the Oral Delivery of Protein and Peptides can be successfully achieved by using various carrier systems are like 1. Dry Emulsion 2. Microspheres 3. Liposomes 4. Nanoparticles
  • 21.  1. Dry Emulsion is prepared by the Spray drying, Lyophollization and evaporation Techniques. In dry emulsion preparation application of the PH responsive polymers like HPMCP, is important for the emulsions are the enteric coated and site specific achieved.  2. Microspheres: The uniform distribution of drug in oral drug delivery in Protein peptides drug are known as Microspheres. The PH responsive microspheres are the mainly used in oral delivery for the protection of the stomach from proteolytic degradations and Protection upper portion of small intestine from proteolytic degradations.
  • 22.  3. Liposomes: Liposomes are the small microscopic vesicles in which aqueous volume is entirely enclosed by the membrane composed lipid molecules. Liposomes in drug delivery system, the encapsulation of the insulin with sugar chain portion of mucin and PEG completely suppressed the degradation of the insulin molecules in intestinal fluid. The uncoated from of liposomes are suppressed it on partially surface coating of the liposomes molecules in PEG or mucin gained resistances against dagestion by salts and increased the stability of GI tract.  4. Nanoparticles: Nanoparticles are Nano sized colloidal structure having size is 10-1000nm. The particles in nanometric sized range of the particles are absorbed intact by the intestinal epithelium and they are the less prone towards the enzymatic degradations. The particle size surface charges are the influencing the uptake of nanoparticle system in GI tract.
  • 23. 5. MUCOADHESIVE POLYMERIC SYSTEMS The mucoadhesive polymeric system is important to prevent the problem associated in Presystemic Metabolism or first pass metabolism and maintain its therapeutic efficacy. The residence time of this drug delivery systems at the site of action and the increasing or decreasing the drug clearance rate.
  • 24. STABILITY ASPECTS In stability of protein and peptide is determined by the Protein degradations PathwaysIn This drug delivery system under two Pathways of degradation of Protein and Peptide Molecules 1.Physical Degradation Pathways (Instability Aspects) 2.Chemical Degradation Pathways (Instability Aspects) 1. Physical Instabilities: The Physical Degradation Pathways the Native or original structure of Protein is Changes or Modified to from Higher order Structure of Proteins (secondary, tertiary or quaternary structure). 2. Chemical Instabilities: Chemical degradation Pathways the Native or original structure of protein is changes by the modification of their Primary Structure of Protein Molecules.The chemical instability of the protein and Peptide can causes following four types of reactions. 3. Oxidation 4. 2. Deamination 5. 3. Peptide bond hydrolysis 6. 4. Disulphide exchange
  • 25. APPLICATION  1. CVS acing drugs Protein and Peptides  CNS active Protein and Peptides  GI-active Protein and Peptides  Immunomodulation of the Protein and Peptides  Metabolism modulating Protein and Peptides
  • 26. REFERENCE  Sagar Kishor Savale, Protein and peptide drug delivery system, world journal of pharmacy and pharmaceutical sciences, Vol 5, Issue 4, 2016  A text book of drug delivery system, Prafull P.Patil pg. 189-216.  P. keerthi, Protein and peptide drug delivery system, 201 4.