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Diuretics

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Diuretics Why do we want to know about diuretics? What do kidneys do? What can go wrong? Interventions that can be used how do they work? Effects, side effects ... – PowerPoint PPT presentation

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Title: Diuretics


1
Diuretics
2
Why do we want to know about diuretics?
  • What do kidneys do?
  • What can go wrong?
  • Interventions that can be used
  • how do they work?
  • Effects, side effects

3
Functions of the kidney?
  • Excretion of waste products
  • regulation of salt and electrolyte content
  • and volume of extra -cellular fluid
  • acid -base balance

4
How?
  • Several hundred litres of plasma filtered/day
  • filtrate - very little protein/protein bound
    substances
  • 99 of sodium is reabsorbed, some substances
    secreted
  • 1.5 litres voided as urine
  • Diuretics increase salt and water excretion

5
Why diuretics?
  • important group of drugs employed for their
    effects on the kidney to enhance salt and water
    excretion (only when needed)
  • when used heart failure, other causes of salt
    and water retention (renal failure, liver
    failure), hypertension

6
Variety of compounds with diuretic activity
  • Xanthines - theophylline, caffeine
  • osmotic diuretics - urea
  • carbonic-anhydrase inhibitors
  • thiazides
  • loop diuretics
  • aldosterone antagonists
  • potassium sparing diuretics

7
How do they work?
  • Direct effect on cells of the nephron..
  • where most of the active and selective solute
    reabsorption occurs
  • ascending loop of Henle
  • early distal tubule
  • collecting tubules and ducts
  • OR
  • modifying the content of the filtrate by their
    presence

8
Loop diuretics (Rang and Dale p361-363)
  • Frusemide, bumetanide, piretanide
  • act on thick segment of ascending loop
  • inhibit NaCl transport OUT of tubule by
    inhibiting Na/K/2Cl- carrier (co-transporter)
    in luminal membrane ( acting on chloride binding
    site)
  • Reduces the hypertonic interstitial area in the
    medull, so reducing water re-absorption
  • increases Na solute concentration in the distal
    tubule which is exchanged for K and H
    (hypokalemia and alkalosis)
  • Can increase the excreted sodium from 1 to 15
    of filtrate
  • Also reduce peripheral vascular resistance

9
Loop diuretics
  • Kinetics
  • oral and IV preparations
  • bound to plasma protein, secreted into tubule
  • metabolised by the liver ( P450)
  • act within 1 hour
  • half life about 90 minutes longer in renal
    failure
  • duration - 3-6 hours (Lasts Six Hours Lasix)

10
Loop diuretics
  • Effects
  • pass urine in large amounts!
  • Side effects
  • electrolyte depletion
  • Hypovolemia
  • other reactions rare
  • Main Use
  • Heart failure particularly acute left
    ventricular failure
  • Hepatic cirrhosis
  • Nephrotic syndrome
  • Renal failure

11
thiazide diuretics
  • bendrofluazide, hydrochlorothiazide, indapamide
  • act on distal convoluted tubule
  • bind to chloride site of Na/Cl cotransport
    system and inhibit action
  • decrease active Na resorption
  • decrease water resorption
  • changes in Ca, magnesium and uric acid

12
thiazide diuretcis
  • kinetics
  • rapidly absorbed orally
  • secreted into the tubule
  • maximal effect 4- 6 hours, duration 8-12 hours

13
thiazide diuretics
  • effects
  • increase urine output
  • side effects
  • electrolyte disturbances
  • increased cholesterol
  • impotence
  • hypersensitivity reactions (rare)
  • Main uses
  • hypertension
  • mild heart failure

14
aldosterone antagonists
  • spirololactone
  • inhibits action of aldosterone (intracellular
    receptor binding anatagonism), increases sodium
    and decreases potassium secretion
  • kinetics
  • well absorbed orally, active metabolite half life
    of 16 hours
  • effects
  • limited diuresis
  • Main uses heart failure and cirrhosis
  • side effects
  • Hyperkalemia, estrogen like effects

15
other potassium sparing diuretics
  • Triamterene, amiloride
  • act on collecting ducts
  • inhibit Na resorption, decrease potassium
    excretion
  • effects
  • limited diuresis
  • side effects
  • electrolyte disturbances

16
clinical choices
  • Uses
  • cardiac failure
  • hypertension
  • fluid overload
  • NOT for everyone with oedema (eg from venous
    insufficiency)
  • acute versus chronic
  • evidence of benefit

17
references
  • Rang Dale, 5th edition
  • Cardiovascular Therapeutic Guidelines
  • Australian Medicines Handbook
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