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Grading Average = 91. Errata Michaelis-Menten Derivation KmKm k cat Formation of ES complex is rapid (k cat <<k off ), therefore Rate Limiting.

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Presentation on theme: "Grading Average = 91. Errata Michaelis-Menten Derivation KmKm k cat Formation of ES complex is rapid (k cat <<k off ), therefore Rate Limiting."— Presentation transcript:

1 Grading Average = 91

2 Errata

3 Michaelis-Menten Derivation KmKm k cat Formation of ES complex is rapid (k cat <<k off ), therefore Rate Limiting

4 Michaelis-Menten Derivation KmKm k cat Formation of ES complex is rapid (k cat <<k off ), therefore Rate Limiting

5 Clarifications

6 Michaelis-Menten Assumptions Quasi-steady-state approximation – [ES] remains constant at saturating [S] – d[ES]/dt=0 (i.e. forward rate = reverse rate) [E]<<K m and [S] Rapid Equilibrium for the ES complex k cat << k off Product formation is irreversible KmKm k cat k on k off

7 20% Decrease in Dose (250 mg/day  200 mg/day) 50% decrease anti-seizure (a.k.a. Dilantin) Capacity-Limited Metabolism Excitatory Synapse

8 NON-LINEARITIES CONTINUED Lecture #35

9 Review Constant Rate Input IV Bolus Constant Rate Input

10 Review: Reasons Individualization – Pain – Low Therapeutic Index – Anesthesia Drug Solubility Rapid Degradation/Elimination  High Enough [Drug] plasma Maintain/Control Response Drug Toxicity  Control plasma levels

11 Review: Time to Reach Plateau 90% of the plateau value

12 Constant Rate Infusion t 90

13 Constant Rate Infusion: Plateau R o = constant rate input (mg/hr) KmKm VmVm Cu SS Higher K m (weaker)ConstantHigher Lower K m (tighter)ConstantLower ConstantHigher V m (inducing)Lower ConstantLower V m (inhibiting)Higher What does the extraction ratio have to be?

14 Constant Rate Infusion: Time to Plateau R o = constant rate input (mg/hr) Km’Km’ VmVm t 90 Higher K m (weaker)Constantlonger Lower K m (tighter)Constantshorter ConstantHigher V m (inducing)shorter ConstantLower V m (inhibiting)longer Basically, it has this correlation.

15 Concentration-Dependent Renal Excretion

16 penicillin antibiotic

17 Concentration-Dependent Renal Excretion A = GFR Only B = GFR and Active Secretion C = GFR and Active Reabsorption

18 GFR and Active Reabsorption

19 Saturable Binding to Plasma Proteins n = number of binding sites P t = protein concentration n*P t = concentration of drug binding sites KDKD Cu + Assumptions?

20 Non-linear binding to  1 -acid glycoprotein  1 -acid glycoprotein Na + channel inhibitor

21 Saturable Albumin Binding NSAID

22 Saturable Albumin Binding Binding to Albumin Cephalosporin Antibiotic

23 Saturable Plasma Protein Binding ACE Inhibitor Prodrug Trandolaprilat Active

24 Saturable Transport T m = maximum transport rate active or passive transport? Cu in Cu out KTKT

25

26 Saturable Tissue Binding endothelin receptor antagonist (ERA) Endothelin-1 ECE = Endothelin Converting Enzyme

27 Time-Dependent PK (Chronopharmacokinetics) Enzyme Induction Circadian variations – Renal Function, Urine pH,  1 -acid glycoprotein GI Physiology (Food and Drink) – Gastric emptying slowed/delayed by food Autoinduction Mechanism-based Autoinhibition

28 Chronopharmacokinetics: Renal Function aminoglycoside

29 Saturable Tissue Binding imirestat aldose reductase inhibitor glaucoma

30 Saturable Tissue Binding nucleoside transporter inhibitor

31 Chronopharmacokinetics: Food VDCC =Voltage-dependent Calcium Channel Verapamil Taken At Different Times of the Day

32 Chronopharmacokinetics: Mechanism- Based Autoinhibition

33 Chronopharmacokinetics: Autoinduction Excitatory Synapse anticonvulsant

34 Recognition of Non-linearities Compare with Linear Kinetics Identify altered Kinetic parameters Determine Primary PK parameters (e.g. k, V) Consistent with Mechanism

35 Assessment of Non-linearities Urine Recovery Concentration-Time Profile Protein Binding

36 Assessment of Non-linearities Salicylic Acid For Skin

37 Urine Recovery If Linear If Non-Linear 33333333 83 17

38 Concentration-Time Profile If Linear If Non-linear

39 Protein Binding If linear If Non-linear

40 Constant Rate Infusion

41 PK of a Drug Overdose CL T and V often changed t 1/2 increased – e.g. Ethchlorvynol 25 hrs  100 hrs Plasma rebound after dialysis – redistribution in fat (poorly perfused) hypnotic, euphoria insomnia

42 PK of a Drug Overdose Sedative/Hypnotic If Linear If Non-Linear * Plasma rebound due to redistribution. * schedule IV (USA) controlled cerebral depression mechanism of action is not known.

43 Therapeutic Consequences of Non- linearities Dose Dependence – Capacity-Limited Metabolism (Major) low E – Dissolution-Limited  Bioavailability – GI physiology  Bioavailability Chronopharmacokinetics – Autoinduction – Mechanism-based Inhibition

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