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Diuretics

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Thus a diuretic is an agent which inhibits tubular Na reabsorption ... This alleviates the hypernatremia that accompanies DI. 22. Potassium-Sparing Diuretics ... – PowerPoint PPT presentation

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Title: Diuretics


1
  • Diuretics
  • Diuresis increased urine flow
  • Diuretics substances which elicit diuresis
  • In the kidney, water reabsorption dependent
    primarily on Na reabsorption
  • Thus a diuretic is an agent which inhibits
    tubular Na reabsorption (along with Cl-, HCO3-)
    resulting in increased excretion of these ions.

2
  • Natriuretic effect (enhance secretion of sodium
    and thus
  • water)
  • Mainly act by decreasing tubular reabsorption at
    one or more sites in nephron
  • Diuretics can have effects on
  • - Sodium reabsorption
  • - Potassium loss
  • - Body fluids

3
  • Effect on sodium reabsorption
  • Na reabsorption could be reduced by
  • 1. Inhibition of uptake into tubular cells
  • 2. Inhibition of reabsorption through the tight
    junctions
  • 3. Inhibition of extrusion across the
    basolateral membrane
  • Most diuretics in common use act on sodium
    transporters in luminal membranes of cells in
    distal and/or collecting ducts

4
  • Mechanism for salt reabsorption
  • 1 Na, 2 Cl- and possibly one K enter cell
    together across luminal membrane by co-transport
    process.
  • If K required, it leaks back into lumen
  • Overall process causes lumen to become positive
  • Positive lumen drives out more Na through tight
    junctions (cation permeable)
  • Na entering nephron cells pumped out of cells
    across basolateral membrane by sodium pump

5
Sodium reabsorption in the early PCT
Lumen (urine)
Peritubular (Blood)
Na
Na
H
K
Na
Glucose, Phosphate, Amino acids,
6
Sodium reabsorption in the late PCT
Lumen (urine)
Peritubular (Blood)

Cl-

Na

H

H-Anion
H-Anion


Anion

Cl-
Na


7
Sodium reabsorption in the thick ascending limb
of loop of Henle
Lumen (urine)
Peritubular (Blood)
Na
Cl-
2Cl-
K
Na
Na
K
H
8
Sodium reabsorption in the DCT
Lumen (urine)
Peritubular (Blood)
Na
Na
K
Cl-
H2O
Cl-
9
Sodium transport in the Collecting Duct
Lumen (urine)
Peritubular (Blood)
Na
Na
K
K
10
  • Except for K-sparing diuretics, all diuretics
    not only increase Na excretion, but also cause
    increased K secretion (unwanted side-effect)
  • Diuretics (except osmotic diuretics) are organic
    acids
  • Secreted by the PCT secretory mechanism
  • Higher concentration within tubule than blood
  • Exert their effects from within tubule
  • There are several chemical types and several
    possible sites of action for diuretcis within the
    nephron.

11
  • Diuretics are substances that increase the rate
    of urine output.
  • Therefore typically larger volumes of dilute
    urine might be expected to be produced.
  • Many diuretics act to block the reabsorption of
    sodium chloride from the tubule.
  • Sodium chloride is a solute and as such exerts an
    osmotic effect which reduces the rate of water
    reabsorption from the tubule.
  • Consequently if the rate of reabsorption of
    sodium chloride is reduced the volume of urine
    produced increases.
  • Diuretics maybe used to aid in the correction of
    fluid accumulation or the effects of fluid
    accumulation such as hypertension.

12
  • Types Of Diuretics.
  • There are a number of different types of
    diuretics.
  • Types of diuretics are generally classified
    according to their mode of action.
  • Some example of types of diuretics are shown
    below.
  • Osmotic diuretics.
  • Loop diuretics.
  • Thiazide diuretics.
  • Carbonic anhydrase diuretics.
  • Competitive inhibitors of aldosterone.
  • Sodium channel blockers.

13
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14
  • Osmotic Diuretics.
  • Osmotic diuretics generally consist of molecules
    which are small enough to pass through the
    ultrafiltration barrier and enter the nephron.
  • However, the molecules that form osmotic
    diuretics either block the reabsorption of
    solutes from the nephron (especially sodium) or
    are not easily absorbed from the nephron
    themselves (mannitol).
  • Consequently solutes remain within the filtrate
    and exert an osmotic effect that inhibits the
    reabsorption of water.
  • This effect can also be seen if blood plasma
    levels of glucose become very high (e.g. in
    hyperglycaemic episodes experienced by
    individuals with diabetes mellitus). The glucose
    that remains unabsorbed inhibits the reabsorption
    of water and larger volumes of urine are
    typically produced, initially.

15
  • Loop diuretics
  • Loop diuretics include furosemide (Lasix),
    bumetanide
  • (Bumex), and torsemide (Demadex).
  • They are often described as "high ceiling"
    diuretics
  • Due to their high diuretic potential they can
    cause up to
  • 20 of the filtered load of NaCl H2O to be
    excreted in
  • the urine.
  • Act by inhibiting the Na- K-2Cl- cotransporter
    in the
  • thick ascending limb of the loop of Henle. They
    also
  • interfere with the reabsorption of K , Ca, and
    Mg
  • in the loop.

16
  • Sodium chloride transport inhibited by loop
    diuretics
  • - frusomide, bumetanide, ethacrynic acid
  • These block sodium-chloride cotransporter from
    luminal side
  • Act on thick ascending limb specifically since
  • - Na transport exclusively due to
    co-transporters in this region whist Na
    transport can be by other methods in other parts
    of nephron
  • - These diuretics more effective since they are
    secreted into proximal tubule so concentrations
    much higher than in plasma

17
  • Loop diuretics are indicated in the treatment of
  • following conditions
  • Fluid overload / oedema Congestive heart
    failure, acute pulmonary oedema, hepatic ascites,
    nephrotic syndrome, renal failure, etc
  • Hypertension, especially when accompanied by
    renal impairment
  • Acute treatment of hypercalcemia.

18
  • Thiazide Thiazide-like Diuretics
  • Include chlorothiazide, hydrochlorothiazide
    (HCTZ),
  • benzthiazide, cyclothiazide, indapamide,
  • chlorthalidone, bendroflumethizide, metolazone,
    etc
  • Exert their diuretic effect by inhibiting the Na
    - Cl-
  • cotransport in the early distal convoluted
    tubules.
  • They elicit a weaker diuretic response compared
    to the
  • loop diuretics as illustrated by the
    dose-response
  • curve.
  • Increase the loss of K and Mg2, but reduce Ca2
  • excretion (may cause hypercalcemia).

19
of filtered Na load excreted
20
  • They are indicated for
  • Hypertension (1st line therapy for mild to
    moderate HTN). They also exert a vasodilatory
    effect. In fact, on chronic use, their diuretic
    effect may become insignificant due to a
    compensatory increase in fractional Na
    reabsorption in the proximal tubules. However,
    their vasodilatory action persists and may
    account for most of their beneficial effect in
    the management of chronic hypertension.
  • Mild heart failure
  • In combination with loop diuretics, for severe,
    resistant oedema (especially metolazone)

21
  • 4. Idiopathic hypercalciuria
  • 5. Nephrogenic diabetes insipidus (DI). They
    prevent the urine from being diluted further in
    the distal convoluted tubules. This alleviates
    the hypernatremia that accompanies DI.

22
  • Potassium-Sparing Diuretics
  • They include amiloride, triamterene, and
  • spironolactone.
  • They are weak diuretics that exert their action
    mainly
  • on the collecting ducts.
  • Amiloride and triamterene act by blocking the Na
  • channels in the luminal membrane of the principal
    cells
  • of the cortical collecting ducts. This reduces
    the Na
  • entry through the luminal membrane and hence the
    net
  • reabsorption of NaCl.
  • Spironolactone (Aldactone) is a competitive
  • aldosterone antagonist at the cytosolic receptor
    level.

23
  • Potassium-sparing diuretics are used in the
    following
  • To prevent hypokalemia induced by loop or
    thiazide diuretics
  • 2dary hyperaldosteronism due to hepatic cirrhosis
    ascites.
  • Primary hyperaldosteronism (Conn's syndrome)

24
  • Potassium-sparing diuretics
  • Spironolactone
  • Act as antagonists to aldosterone, competes with
    aldosterone for receptor sites in DCT (see fig)
  • Results in decreased Na reabsorption in DCT
  • Promotes Na and water loss
  • Decreased Na reabsorption balanced by K
    retention at this site (and H).
  • Used in combination with diuretic e.g.. frusomide

25
CH2OH
Aldosterone
CO
HCO
HO
Spironolactone
CH3
O
O
CH3
CH3
O
SCOCH3
26
  • Triamterene and Amiloride
  • Similar effect to spironolactone by reducing Na
    absorption and H/K secretion in DCT
  • Independent of aldosterone
  • Have little diuretic effect
  • Used in conjunction with diuretics
  • In low doses blocks entry of Na into tubule
    cells across luminal membrane
  • Decrease availability of Na to Na-K-ATPase at
    basal cell membrane
  • Called Na channel blockers

27
  • Carbonic Anhydrase Inhibitors
  • Weak diuretics
  • Used clinically to correct acid-base disturbances
    (alkalosis) rather than for diuretic action
  • Acetazolamide (Diamox)
  • In PCT HCO3- absorbed form tubule
  • Carbonic Anhydrase (enzyme) present in proximal
    tubule cells
  • Inhibition of CA inhibits HCO3- absorption from
    tubule
  • Presence in lumen of HCO3- reduces Na
    reabsorption
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