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Connecting Pharmacology with Therapeutics Clive Roberts.

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Connecting Pharmacology with Therapeutics Clive Roberts
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Page 1: Connecting Pharmacology with Therapeutics Clive Roberts.

Connecting Pharmacology with Therapeutics

Clive Roberts

Page 2: Connecting Pharmacology with Therapeutics Clive Roberts.

Become wise!

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What can be predicted from a drug’s pharmacological profile

• Pharmacological actions

• Some adverse effects

• Some contraindications

• Some drug interactions

• Acute toxicity risk

• Mode of administration possibilities

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What can NOT be predicted?

• Therapeutic effect

• Appropriate usage in comparison with other drugs

• Some adverse effects

• Some drug interactions

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What does the pharmacological profile consist of

• Pharmacodynamic data• Pharmacokinetic data• Physicochemical properties• Potential to induce or inhibit hepatic enzymes• Acute toxicity information• “The therapeutic ratio”• Usage history• Cost

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Pharmacodynamic information

• What receptors does it block or stimulate

• Or what ionic channels or enzymes etc does it affect

• What is the hypersensitivity risk

• What unrelated toxicity occurs, how serious and how often

• What happens in acute overdose

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Pharmacokinetic information

• How is it cleared from the blood – liver/kidney/lung etc

• First order / zero order process

• If liver, how high is the clearance rate

• What is the bioavailability

• If low is it due to pre-systemic hepatic clearance or poor absorption

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Pharmacokinetic info. continued

• How is the drug distributed in the body

• What is the volume of distribution

• What is the extent of plasma protein binding

• What is the plasma half life

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Patient groups at risk

• Liver disease

• Renal disease

• Heart disease

• Lung disease

• Elderly

• Those taking other drugs

• Pregnancy

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So let’s take the example of

Phenytoin

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?? Digoxin

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Mrs Y.Y. Born 1912

• Admitted late Feb with general deterioration in health, nausea, anorexia, constipation

• At her EPH there had been an outbreak of D+V 4 weeks previous. She had never really got better.

• Dehydrated, hypotensive, pale, slow reg pulse

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• Drugs – perindopril, digoxin, frusemide, aspirin, Isosorbide mononitrate

• Urea 31, creatinine 223

• ECG ……………

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• Digoxin level 3.5

• What went wrong?

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What is it about the patient with hepatic failure that puts them at

risk• Pharmacokinetic disturbance -

– Decreased clearance of some drugs– Increased bioavailability of some drugs– Altered distribution volume– Decreased protein binding

• CNS sensitivity

• Electrolyte abnormality

Page 36: Connecting Pharmacology with Therapeutics Clive Roberts.

What is it about the patient with hepatic failure that puts them at

risk - continued

• Fluid retention

• Risk of bleeding – generally and specifically in gut

• Metabolic disturbance

• Encephalopathy risk

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And the renal patient ?

• Pharmacokinetic disturbance – Mainly affecting drug clearance– Also protein binding

• Increased sensitivity

• Poor tolerance of adverse effects

• Decreased effectiveness of some drugs

Page 38: Connecting Pharmacology with Therapeutics Clive Roberts.

Drugs in the elderly

• Multiple indications leads to polypharmacy

• Pharmacokinetic disturbance of metabolism, excretion, protein binding and drug distribution

• Increased sensitivity to the actions of drugs on CVS, CNS, GIT

• Poor tolerance of adverse effect

Page 39: Connecting Pharmacology with Therapeutics Clive Roberts.

Drug interaction

• Pharmacodynamic mechanisms usually easy to predict

• Pharmacokinetic mechanisms – need to know / look up.

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Le Fin

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Profile of new drug for reflux oesophagitis

• Phenothiazine drug with powerful antigastric secretory action at low doses.

• Acts on both h2 receptors and the proton pump• Also blocks muscarinic receptors throughout the

body• Inhibits some hepatic enzymes• Causes a rise in transaminases in some patients• Limited experience in overdose

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Profile of new drug for reflux oesophagitis

• High hepatic clearance with extraction ratio of 65%

• Widely distributed in tissues

• Plasma half life of 48 h

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What might you predict about the adverse effects?

Who might be at greatest risk?What drug interactions might

occur?What about self harm doses?

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