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Nimra Nimi
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PROTEIN BINDING presented by : Nimra Zulfiqar Faiza Aslam Zeenat Fatima Fakhra Bukhari Zubaira Afzal Biopharmaceutics The University of Faisalabad
"Many drugs interact with plasma or tissue proteins or with other macromolecules, such as melanin and DNA ,to form a drug- macromolecule complex. The formation of a drug protein complex is named as drug protein binding."
Binding of drug to proteins may: Facilitate the distribution of drugs Inactivate the drug by not enabling a sufficient concentration of free drug to develop at a receptor site be a reversible or an irreversible process.
Binding of drug:
Two Important Plasma Proteins ALBUMINALBUMIN Is the most important protein that binds to drug molecule due to its high concentration compared with other proteins It binds both acidic and basic Constitute 5% of the total plasma
Two Important Plasma Protein ∂∂1-ACIDGLYCOPROTEIN1-ACIDGLYCOPROTEIN Also known as orosomucoid (∂1-globulin) Binds to numerous drugs Have greater affinity for basic than acidic drugs molecules Binds only basic and highly lipophilic drugs
Drugs may bind to protein through: Hydrophobic Interaction Proposed by Kauzmann tendency to develop of hydrophobic molecules or parts of molecules to avoid water because they are not readily accommodated in the H-bond structure of water
Drugs may bind to protein through: Self-Association Some drug may self dissociate to form dimers, trimers or aggregates of larger size Dimers or trimers - is a reaction product of two or three identical molecules May affect solubility, diffusion, transport, therapeutic action of drugs
Amino Acids A. Basic Group Arginine Histidine Lysine bind Acidic Drugs Amino Acids B. Acidic Group Aspartic Acid Glutamic Acid bin d Basic Drugs
Protein binding is determined by: Dialysis Ultracentrifugation Ultrafiltration Sephadex-gel filtration Molecular filtration Electrophoresis Agar plate test
Factors affecting protein-Binding 1. Factors relating to the drug 2. The Protein 3. Factors relating to the protein and other binding component 4. Drug interactions 5. Patient related factors
1. DRUG RELATED FACTORS Physicochemical Characteristics of the DrugPhysicochemical Characteristics of the Drug  E.g. Cloxacillin 95% bound, Ampicillin 20% bound; hence Cloxacillan is released slowly after i.m. injection.  Increase in lipophilicity increases the extend of binding.  Acidic/anionic drugs bind to HSA; basic/cationic drugs to AAG; neutral/unionized drugs to lipoproteins.
Concentration of Drug in the Body At low concentrations, most drugs may be bound to proteins At high concentrations, more free drugs may be present owing to saturation of binding sites on protein
Drug-Protein/Tissue Affinity Lidocaine has greater affinity for AAG than for HSA. Digoxin has more affinity for proteins of cardiac muscles than those of skeletal muscles or plasma. Iophenoxic acid has half life of 2 ½ yrs due to its high affinity to plasma proteins.
2. PROTEIN RELATED FACTORS Physicochemical Properties of Protein/Binding Component o Lipophilicitylipoproteins bind with lipophilic drugs. o Albumindepend on physiological pH. Concentration of Protein/Binding Components o Disease states affect the concentration of proteins in blood.
Number of Binding Sites on the Protein o Albumin has a large number of binding sites as compared to other proteins. o Indomethacin binds to 3 sites on albumin. o AAG is a protein with limited binding capacity due to low concentration & molecular size. o Lidocaine binds to 2 sites on AAG in presence of HSA.
3. DRUG INTERACTIONS  Displacement Interactions Competition between Drugs for the Binding Sites. e.g. warfarin and phenyl butazone
Interactions will result when: The displaced drug (E.g. warfarin)— a) is more than 95% bound b) has a small volume of distribution c) shows a rapid onset of therapeutic or adverse effects d) has a narrow therapeutic index
The displacer drug (E.g. phenyl butazone)— a) competes for the same binding sites b) the drug/protein concentration ratio is high c) shows a rapid and large increase in plasma drug concentration d) has a high degree of affinity as the drug to be displaced
Competition between Drugs and Normal Body Constituents: a) Interaction with free fatty acids. b) Free fatty acid levels are increased during fasting, diabetes, MI, etc. c) Eg.: Interaction of sod. salicylate with bilirubin in neonates.
Allosteric Changes in Protein Molecule: involves alteration of the protein structure by the drug/metabolite modify binding capacity. Eg.: Aspirin acetylation of albumin; modify the binding capacity of NSAIDs (increased affinity).
4. PATIENT RELATED FACTORS Age: Neonates Change in albumin content affects the drugs binding to it. Infants Elderly Intersubject Variations: Disease States: Hypoalbuminemia severely impair protein-drug binding.
Influence of Disease States on Protein-Drug Binding
Clinical Example Macfie et al (1992) studied the disposition of intravenous dosing of alfentanil in six patients who suffered 10% to 30% surface area burns compared with a control group of six patients matched for age, sex, and wieght. Alfentanil binding to plasma proteins was meisured by equilibrium dialysis. The burn patients had significantly greater concentration of AAG and smaller concentration of albumin.
The mean alfentanil binding was 94.2%± 0.05 (SEM) in the burn group and 90.7% ± 0.4 in the control group (p=0.004). A good correlation was found between AAG concentration and protein binding. The greater AAG concentration in the burn group corresponded with significantly reduced volume of distribution and total clearance of alfentanil. The clearance of unbound drug and half life of alfentanil were not decreased.
The Pharmacokinetic Importance of Protein Binding Drug-protein binding influences the distribution equilibrium of the drug Plasma proteins exert a buffer and transport function in the distribution process Only free and unbound drug acts can leave the circulatory system and diffuse into the tissue
Disease and Protein Binding The reduced albumin concentration and binding capacity is due to: Change in albumin molecule  presence of endogenous binding inhibitors such as free fatty acids, and metabolic acidosis. Hypoalbuminemia may result in patients with cancer, burms, cardiac failure, cystic fibrosis, enteropathy, inflammations, liver impairment, malabsorption, nephrotic syndrome, renal failure, sepsis and trauma.
Binding of Drugs to RBC Lipophilic molecules dissolved in the lipid material of the RBC membrane Anions can be attracted to and enter the positively charged pores of RBC.  Drugs absorbed in the RBC membrane inhibits the deformity of RBC thus becoming lodged in the capillaries
Kinetics of protein binding:- The kinetics of reversible drug-protein binding for a protein with one simple binding site can be described by law of mass action, as follows :- Protein + drug drug protein-complex or, [P] + [D] [PD ] ……………. 1 From eq. 1 and law of mass action , an association constant, Ka, can be expressed as the ratio of molar concentration of product and the molar concentration of the reactants. The assumes only one binding site per protein molecule. Ka = [PD] [P] [D] ………………..2
 The extent of drug-protein complex formed is dependent on the association binding constant Ka.  The magnitude of Ka yields information on the degree of drug protein binding. Drug strongly bound to protein have a very large Ka and exist mostly as the drug-protein complex. With such drugs , a large dose may be needed to obtain a reasonable concentration of free drug.
 Most kinetic studies in vitro use purified albumin as a standard protein source, b’coz these protein is responsible for the major portion of plasma drug-protein binding.  Experimentally, both the free drug [D] and the protein bound drug [PD], as well as the total protein concentration [P] + [PD], may be determined. To study the binding behavior of drugs, a determinable ratio ( r ) is defined, as follows; r = Moles of drug bound Total moles of protein
B’coz moles of drug bound is PD and the total moles of protein is P + PD, this eq. becomes According to eq.2 , [PD] = Ka [P][D]; by substitution into eq.3, the following eq. is obtain,
This equation describes the simplest situation, in which 1 mole of drug binds to 1 mole of protein in a 1:1 complex. This case assumes only one independent binding site for each molecule of drug. If there are n identical independent binding sites per protein molecule, then the following is used: In terms of Kd, which is 1/ Ka, eq. 5 reduces to:-
 protein molecule are quit large than drug molecules and contain more than one type of binding site for the drug. If there is more than one type of the binding site with its own association constants, eq. 6 expands where the subscripts represents different types of binding sites, the K’s represents binding constants, and the n’s represents the number of binding sites per molecule of albumin.
These eq. assumes that each drug molecule binds to the protein at an independent binding site, and the affinity of a drug at one binding site does not influence binding to other sites. In reality Drug- protein binding sometimes exhibits a phenomenon of co-operativiy. For these drugs the binding of the first drug molecule at one site on protein molecule influences the successive binding of other drug molecule. E.g. binding of oxygen to hemoglobin. Each method for the investigation of drug-protein binding in vitro has advantages and disadvantages like; cost, ease of measurement, time, instrumentation and other considerations. Drug-protein binding kinetics yields valuable information concerning proper therapeutic use of the drug and prediction of possible drug interactions.
Determination of Binding Constants and Binding Sites by Graphic Methods 1. in vitro methods ( known protein concentration) 2.in vivo methods ( unknown protein concentration)
In vitro methods 1.Direct plot : A plot of the ratio of r ( moles of drug bound per mole of protein) versus free drug concentration increases, number of moles of drug bound per mole of protein becomes saturated and plateaus. Thus drug protein binding resembles a Langmuir adsorption isotherm, which is also similar to adsorption of a drug to an adsorbent becoming saturated as the drug concentration increases. B’coz of nonlinearity in drug-protein binding, eq. 6 is rearrange for the estimation of n and Ka, using various graphic methods.
Scatchard plot : It is a rearrangement of eq. 6. The scatcherd plot spreads the data give a better line for the estimation of the binding constants and binding sites. From eq. 6 , we obtain, The graph constructed by plotting r / [D] verses r yields a straight line with the intercept and
References:-  ‘‘APPLIED BIOPHARMACEUTICS AND PHARMACOKINETICS’’  By Leon Shargel, Susanna Wu – Pong, Andrew B. C. Fifth edition, Mc Graw Hill. Page no.251 – 282  ‘‘ Biopharmaceutics and Pharmacokinetics’’By D. M. Brahmnkar , Sunil B. Jaiswal Vallabh prakashan. Page no. 86-90, 106-110  Principles and Applications of ‘‘ Biopharmaceutics and Pharmacokinetics’ By H. P. Tipnis, Amrita Bajaj, Carrer Publications. Page no. 61-72  Expression of Epidermal Growth Factor Receptor Detected by Cetuximab Indicates Its Efficacy to Inhibit In Vitro and In Vivo Proliferation of Colorectal Cancer Cells Kohei Shigeta,Tetsu Hayashida mail,Yoshinori Hoshino,Koji Okabayashi,Takashi Endo,Yoshiyuki Ishii, Hirotoshi Hasegawa,Yuko Kitagawa,Published: June 18, 2013, international researh journal of pharmacy.  Journal of the Hong Kong Geriatrics Society • Vol. 9 No.1 Mar. 1999, Jean Woo Dept. of Medicine, Prince of Wales Hospital, The Chinese University of Hong Kong, Hong Kong. J HK Geriatr Soc 1999;9:14 - 17

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  • 1. PROTEIN BINDING presented by : Nimra Zulfiqar Faiza Aslam Zeenat Fatima Fakhra Bukhari Zubaira Afzal Biopharmaceutics The University of Faisalabad
  • 2. "Many drugs interact with plasma or tissue proteins or with other macromolecules, such as melanin and DNA ,to form a drug- macromolecule complex. The formation of a drug protein complex is named as drug protein binding."
  • 3. Binding of drug to proteins may: Facilitate the distribution of drugs Inactivate the drug by not enabling a sufficient concentration of free drug to develop at a receptor site be a reversible or an irreversible process.
  • 5. Two Important Plasma Proteins ALBUMINALBUMIN Is the most important protein that binds to drug molecule due to its high concentration compared with other proteins It binds both acidic and basic Constitute 5% of the total plasma
  • 6. Two Important Plasma Protein ∂∂1-ACIDGLYCOPROTEIN1-ACIDGLYCOPROTEIN Also known as orosomucoid (∂1-globulin) Binds to numerous drugs Have greater affinity for basic than acidic drugs molecules Binds only basic and highly lipophilic drugs
  • 7. Drugs may bind to protein through: Hydrophobic Interaction Proposed by Kauzmann tendency to develop of hydrophobic molecules or parts of molecules to avoid water because they are not readily accommodated in the H-bond structure of water
  • 8. Drugs may bind to protein through: Self-Association Some drug may self dissociate to form dimers, trimers or aggregates of larger size Dimers or trimers - is a reaction product of two or three identical molecules May affect solubility, diffusion, transport, therapeutic action of drugs
  • 9. Amino Acids A. Basic Group Arginine Histidine Lysine bind Acidic Drugs Amino Acids B. Acidic Group Aspartic Acid Glutamic Acid bin d Basic Drugs
  • 10. Protein binding is determined by: Dialysis Ultracentrifugation Ultrafiltration Sephadex-gel filtration Molecular filtration Electrophoresis Agar plate test
  • 11. Factors affecting protein-Binding 1. Factors relating to the drug 2. The Protein 3. Factors relating to the protein and other binding component 4. Drug interactions 5. Patient related factors
  • 12. 1. DRUG RELATED FACTORS Physicochemical Characteristics of the DrugPhysicochemical Characteristics of the Drug  E.g. Cloxacillin 95% bound, Ampicillin 20% bound; hence Cloxacillan is released slowly after i.m. injection.  Increase in lipophilicity increases the extend of binding.  Acidic/anionic drugs bind to HSA; basic/cationic drugs to AAG; neutral/unionized drugs to lipoproteins.
  • 13. Concentration of Drug in the Body At low concentrations, most drugs may be bound to proteins At high concentrations, more free drugs may be present owing to saturation of binding sites on protein
  • 14. Drug-Protein/Tissue Affinity Lidocaine has greater affinity for AAG than for HSA. Digoxin has more affinity for proteins of cardiac muscles than those of skeletal muscles or plasma. Iophenoxic acid has half life of 2 ½ yrs due to its high affinity to plasma proteins.
  • 15. 2. PROTEIN RELATED FACTORS Physicochemical Properties of Protein/Binding Component o Lipophilicitylipoproteins bind with lipophilic drugs. o Albumindepend on physiological pH. Concentration of Protein/Binding Components o Disease states affect the concentration of proteins in blood.
  • 16. Number of Binding Sites on the Protein o Albumin has a large number of binding sites as compared to other proteins. o Indomethacin binds to 3 sites on albumin. o AAG is a protein with limited binding capacity due to low concentration & molecular size. o Lidocaine binds to 2 sites on AAG in presence of HSA.
  • 17. 3. DRUG INTERACTIONS  Displacement Interactions Competition between Drugs for the Binding Sites. e.g. warfarin and phenyl butazone
  • 18. Interactions will result when: The displaced drug (E.g. warfarin)— a) is more than 95% bound b) has a small volume of distribution c) shows a rapid onset of therapeutic or adverse effects d) has a narrow therapeutic index
  • 19. The displacer drug (E.g. phenyl butazone)— a) competes for the same binding sites b) the drug/protein concentration ratio is high c) shows a rapid and large increase in plasma drug concentration d) has a high degree of affinity as the drug to be displaced
  • 20. Competition between Drugs and Normal Body Constituents: a) Interaction with free fatty acids. b) Free fatty acid levels are increased during fasting, diabetes, MI, etc. c) Eg.: Interaction of sod. salicylate with bilirubin in neonates.
  • 21. Allosteric Changes in Protein Molecule: involves alteration of the protein structure by the drug/metabolite modify binding capacity. Eg.: Aspirin acetylation of albumin; modify the binding capacity of NSAIDs (increased affinity).
  • 22. 4. PATIENT RELATED FACTORS Age: Neonates Change in albumin content affects the drugs binding to it. Infants Elderly Intersubject Variations: Disease States: Hypoalbuminemia severely impair protein-drug binding.
  • 23.
  • 24. Influence of Disease States on Protein-Drug Binding
  • 25. Clinical Example Macfie et al (1992) studied the disposition of intravenous dosing of alfentanil in six patients who suffered 10% to 30% surface area burns compared with a control group of six patients matched for age, sex, and wieght. Alfentanil binding to plasma proteins was meisured by equilibrium dialysis. The burn patients had significantly greater concentration of AAG and smaller concentration of albumin.
  • 26. The mean alfentanil binding was 94.2%± 0.05 (SEM) in the burn group and 90.7% ± 0.4 in the control group (p=0.004). A good correlation was found between AAG concentration and protein binding. The greater AAG concentration in the burn group corresponded with significantly reduced volume of distribution and total clearance of alfentanil. The clearance of unbound drug and half life of alfentanil were not decreased.
  • 27. The Pharmacokinetic Importance of Protein Binding Drug-protein binding influences the distribution equilibrium of the drug Plasma proteins exert a buffer and transport function in the distribution process Only free and unbound drug acts can leave the circulatory system and diffuse into the tissue
  • 28. Disease and Protein Binding The reduced albumin concentration and binding capacity is due to: Change in albumin molecule  presence of endogenous binding inhibitors such as free fatty acids, and metabolic acidosis. Hypoalbuminemia may result in patients with cancer, burms, cardiac failure, cystic fibrosis, enteropathy, inflammations, liver impairment, malabsorption, nephrotic syndrome, renal failure, sepsis and trauma.
  • 29. Binding of Drugs to RBC Lipophilic molecules dissolved in the lipid material of the RBC membrane Anions can be attracted to and enter the positively charged pores of RBC.  Drugs absorbed in the RBC membrane inhibits the deformity of RBC thus becoming lodged in the capillaries
  • 30. Kinetics of protein binding:- The kinetics of reversible drug-protein binding for a protein with one simple binding site can be described by law of mass action, as follows :- Protein + drug drug protein-complex or, [P] + [D] [PD ] ……………. 1 From eq. 1 and law of mass action , an association constant, Ka, can be expressed as the ratio of molar concentration of product and the molar concentration of the reactants. The assumes only one binding site per protein molecule. Ka = [PD] [P] [D] ………………..2
  • 31.  The extent of drug-protein complex formed is dependent on the association binding constant Ka.  The magnitude of Ka yields information on the degree of drug protein binding. Drug strongly bound to protein have a very large Ka and exist mostly as the drug-protein complex. With such drugs , a large dose may be needed to obtain a reasonable concentration of free drug.
  • 32.  Most kinetic studies in vitro use purified albumin as a standard protein source, b’coz these protein is responsible for the major portion of plasma drug-protein binding.  Experimentally, both the free drug [D] and the protein bound drug [PD], as well as the total protein concentration [P] + [PD], may be determined. To study the binding behavior of drugs, a determinable ratio ( r ) is defined, as follows; r = Moles of drug bound Total moles of protein
  • 33. B’coz moles of drug bound is PD and the total moles of protein is P + PD, this eq. becomes According to eq.2 , [PD] = Ka [P][D]; by substitution into eq.3, the following eq. is obtain,
  • 34. This equation describes the simplest situation, in which 1 mole of drug binds to 1 mole of protein in a 1:1 complex. This case assumes only one independent binding site for each molecule of drug. If there are n identical independent binding sites per protein molecule, then the following is used: In terms of Kd, which is 1/ Ka, eq. 5 reduces to:-
  • 35.  protein molecule are quit large than drug molecules and contain more than one type of binding site for the drug. If there is more than one type of the binding site with its own association constants, eq. 6 expands where the subscripts represents different types of binding sites, the K’s represents binding constants, and the n’s represents the number of binding sites per molecule of albumin.
  • 36. These eq. assumes that each drug molecule binds to the protein at an independent binding site, and the affinity of a drug at one binding site does not influence binding to other sites. In reality Drug- protein binding sometimes exhibits a phenomenon of co-operativiy. For these drugs the binding of the first drug molecule at one site on protein molecule influences the successive binding of other drug molecule. E.g. binding of oxygen to hemoglobin. Each method for the investigation of drug-protein binding in vitro has advantages and disadvantages like; cost, ease of measurement, time, instrumentation and other considerations. Drug-protein binding kinetics yields valuable information concerning proper therapeutic use of the drug and prediction of possible drug interactions.
  • 37. Determination of Binding Constants and Binding Sites by Graphic Methods 1. in vitro methods ( known protein concentration) 2.in vivo methods ( unknown protein concentration)
  • 38. In vitro methods 1.Direct plot : A plot of the ratio of r ( moles of drug bound per mole of protein) versus free drug concentration increases, number of moles of drug bound per mole of protein becomes saturated and plateaus. Thus drug protein binding resembles a Langmuir adsorption isotherm, which is also similar to adsorption of a drug to an adsorbent becoming saturated as the drug concentration increases. B’coz of nonlinearity in drug-protein binding, eq. 6 is rearrange for the estimation of n and Ka, using various graphic methods.
  • 39.
  • 40. Scatchard plot : It is a rearrangement of eq. 6. The scatcherd plot spreads the data give a better line for the estimation of the binding constants and binding sites. From eq. 6 , we obtain, The graph constructed by plotting r / [D] verses r yields a straight line with the intercept and
  • 41. References:-  ‘‘APPLIED BIOPHARMACEUTICS AND PHARMACOKINETICS’’  By Leon Shargel, Susanna Wu – Pong, Andrew B. C. Fifth edition, Mc Graw Hill. Page no.251 – 282  ‘‘ Biopharmaceutics and Pharmacokinetics’’By D. M. Brahmnkar , Sunil B. Jaiswal Vallabh prakashan. Page no. 86-90, 106-110  Principles and Applications of ‘‘ Biopharmaceutics and Pharmacokinetics’ By H. P. Tipnis, Amrita Bajaj, Carrer Publications. Page no. 61-72  Expression of Epidermal Growth Factor Receptor Detected by Cetuximab Indicates Its Efficacy to Inhibit In Vitro and In Vivo Proliferation of Colorectal Cancer Cells Kohei Shigeta,Tetsu Hayashida mail,Yoshinori Hoshino,Koji Okabayashi,Takashi Endo,Yoshiyuki Ishii, Hirotoshi Hasegawa,Yuko Kitagawa,Published: June 18, 2013, international researh journal of pharmacy.  Journal of the Hong Kong Geriatrics Society • Vol. 9 No.1 Mar. 1999, Jean Woo Dept. of Medicine, Prince of Wales Hospital, The Chinese University of Hong Kong, Hong Kong. J HK Geriatr Soc 1999;9:14 - 17