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Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications of diuretics

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Page 1: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Diuretics1) the role of different portions

of the nephron in ion exchange;

2) the sites of action and pharmacology of diuretics;

3) the therapeutic applications of diuretics

Page 2: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

A diuretic -

is any drug that elevates the rate of bodily urine excretion (diuresis).

All diuretics increase the excretion of water from the body.

Page 3: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications
Page 4: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Classification /due to location of action/

1. Diuretics which increase glomerular filtration rate

/Xanthines/Caffeine,

Theophyllinum

Euphyllinum

Page 5: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

2. Proximal convoluted tubule diuretics

2.1. Osmotic diuretic Mannitol

2.2. Carbonic anhydrase (CA) inhibitors

Diacarbum (acetazolamide)

Page 6: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

3. Loop (of Henle) diureticsFurosemidum

Bumetanidum

Ethacrynic acid

4. Distal convoluted tubule diuretics/Thiazides and thiazide-like drugs/

Hydrochlorothiazidum

Page 7: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

5. Collecting duct diuretics5.1. Antagonist of aldosterone

Spironolactonum

5.2. Agents inhibit the Na+ channel in the apical membrane

Amiloridum

Triamterenum

Page 8: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Indications:

Hypertension CHF, Nephrotic syndrome Poisonings

Page 9: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Proximal convoluted tubule diuretics

The proximal tubule (PT) determines the rate of Na+ and H2O delivery to the more distal portions of the nephron

A wide variety of transporters couple Na+ movement into the cell to the movement of amino acids, glucose, phosphate, and other solutes

Page 10: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

MannitolMechanism of Action

o Mannitol is a non-metabolizable osmotic diuretic and is filtered into the tubular space where it markedly increases tubular fluid osmolality.

o This results in impared reabsorption of fluid with a resultant increased excretion of water (some Na+ accompanies)

Page 11: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications
Page 12: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Pharmacokinetics of Mannitol:

o Given only i.v. and acts within 10 min; o if given p.o. it causes an osmotic diarrhea

(not well absorbed from gut). o In pts with normal renal function t1/2 is

approx. 1.2 hr.

Page 13: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Indications:

prophylaxis against renal dysfunction, e.g. major surgical procedure

Contraindications: CHF,

chronic renal failure

Page 14: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications
Page 15: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Carbonic anhydrase (CA) inhibitors

Page 16: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications
Page 17: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Carbonic anhydrase (CA) inhibitors Mechanism of Action:

If CA activity is inhibited, HCO3- reabsorption is reduced and exits the proximal tubule in much larger amounts.

In the distal nephron, Na+ is largely reabsorbed (unlike HCO3-) and is exchanged for K+. Therefore acetazolamide primarily causes an increase in urinary HCO3-, K+, and water excretion.

Page 18: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

CA Inhibitors: Adverse Side Effects

hypokalemia metabolic acidosis

Page 19: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Loop Diuretics

Page 20: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Loop Diuretics: Mechanism of Action

block the Na+/K+/Cl- co-transporter in the apical membrane of the thick ascending limb of Henle's loop. Therefore, loop diuretics increase urinary water, ions excretion.

cause dilation of the venous system and renal vasodilation - effects that may be mediated by prostaglandins.

Page 21: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications
Page 22: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Loop diuretics: Pharmacokinetics

- act within 20 min and t1/2 is approx. 1-1.5 hr.

- are rapidly absorbed from the gut and can be given i.v.

- are the most potent available and can cause excretion of up to 20% of the filtered Na+.

Page 23: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Clinical uses of loop diuretics

acute pulmonary oedema chronic heart failure cirrhosis of the liver complicated by

ascites nephrotic syndrome renal failure.

Page 24: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Loop diuretics Adverse Side Effects

hypokalemia metabolic alkalosis hypomagnesemia hyperuricemia dehydration (hypovolemia), leading to

hypotension dose-related hearing loss (ototoxicity)

Page 25: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Thiazides: Mechanism of Action

They inhibit Na+ and Cl- transport in the cortical thick ascending limb and early distal tubule.

They have a milder diuretic action than do the loop diuretics because this nephron site reabsorbs less Na+ than the thick ascending limb.

Page 26: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Thiazides

Page 27: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Thiazides: Pharmacokinetics

All are well absorbed from the gut. Onset of action is within approx. 1 hr;

effects can be long lasting but vary with the drug used (6-48 hr).

Page 28: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Clinical uses of thiazide diuretics

Hypertension. Mild heart failure (loop diuretics are

usually preferred). Severe resistant oedema (together

with loop diuretics).

Page 29: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Thiazides have a week antihypertensive

effect because reduce arterial wall sensitivityto NA (noradrenaline) and AT (Angiotensin).

They potentiate significantly the effectof other antihypertensive drugs.

Page 30: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Thiazide Adverse Side Effects

hypokalemia metabolic alkalosis dehydration (hypovolemia), leading to

hypotension hyponatremia hyperglycemia in diabetics hyperuricemia (at low doses) Erectile dysfunction

Page 31: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Symptoms  of hypokalemia

muscle weaknessparalysisarrhythmia

Page 32: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Potassium sparing diuretics

These agents are often given to avoid the hypokalemia

They should never be given in the setting of hyperkalemia

(diabetes mellitus, multiple myeloma, renal insufficiency)

Page 33: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

SpironolactoneMechanism of Action

It is a competitive antagonist of aldosterone.

Therefore it blocks aldosterone-stimulated Na+ reabsorption and K+ and H+ excretion in the late distal tubule and collecting duct.

Page 34: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Potassium sparing diuretics

Page 35: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications
Page 36: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

SpironolactonePharmacokinetics:

Given orally, spironolactone takes up to 2 days to be effective with a t1/2 approx. 20 hr.

Page 37: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Amiloride and triamtereneMechanism of Action

inhibit the Na+ channel in the apical membrane of the late distal tubule and collecting duct.

Because K+ and H+ secretion in this nephron segment are driven by the electrochemical gradient generated by Na+ reabsorption, K+ and H+ transport into the urine is reduced.

Page 38: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications
Page 39: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Clinical uses of potassium-sparing diuretics (e.g. amiloride, spironolactone) in heart failure, where either of these

improves survival in primary hyperaldosteronism (Conn's

syndrome) in resistant essential hypertension

(especially low-renin hypertension) in secondary hyperaldosteronism caused

by hepatic cirrhosis complicated by ascites.

Page 40: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

K+-sparing diuretics Adverse Side Effects

hyperkalemia metabolic acidosis gynecomastia (aldosterone antagonists) gastric problems including peptic ulcer

Page 41: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications
Page 42: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Arctostaphylos uva-ursi L. (Bearberry)

Page 43: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Stipites Cerasorum(Cherry)

Page 44: Diuretics 1) the role of different portions of the nephron in ion exchange; 2) the sites of action and pharmacology of diuretics; 3) the therapeutic applications

Equisetum arvense(Common horsetail)

Containssilicates with diureticand urolitholytic effects.