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Diuretics

Diuretics are drugs that increase the excretion of sodium, potassium, and water from the body through the kidneys. There are several classes of diuretics including loop diuretics, thiazide diuretics, potassium-sparing diuretics, and osmotic diuretics. Loop diuretics such as furosemide work by inhibiting sodium reabsorption in the loop of Henle, thiazide diuretics inhibit sodium reabsorption in the distal convoluted tubule, and potassium-sparing diuretics block sodium transport channels to reduce sodium reabsorption and potassium loss. Diuretics are used to treat conditions involving fluid retention such as heart failure, liver disease,

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1K views4 pages

Diuretics

Diuretics are drugs that increase the excretion of sodium, potassium, and water from the body through the kidneys. There are several classes of diuretics including loop diuretics, thiazide diuretics, potassium-sparing diuretics, and osmotic diuretics. Loop diuretics such as furosemide work by inhibiting sodium reabsorption in the loop of Henle, thiazide diuretics inhibit sodium reabsorption in the distal convoluted tubule, and potassium-sparing diuretics block sodium transport channels to reduce sodium reabsorption and potassium loss. Diuretics are used to treat conditions involving fluid retention such as heart failure, liver disease,

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dhainey
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  • Diuretics Overview: Provides an overview of diuretics including their action on the body to increase renal secretion of sodium and water.
  • Classification of Diuretics: Describes the classification of diuretics including loop and high-ceiling diuretics.
  • Thiazide Diuretics: Explains the pharmacokinetics, ADR, and summary of thiazide diuretics and their effect on metabolic alkalosis.
  • Osmotic Diuretics: Covers the agents and administration of osmotic diuretics as well as potential interactions with other drugs.
  • Potassium-Sparing Diuretics: Discusses the agents, mechanisms of action, and structural features of potassium-sparing diuretics.
  • Carbonic Anhydrase Inhibitors & Vasopressin: Details carbonic anhydrase inhibitors, their indications, and effects, along with a focus on vasopressin hormone functions.

DIURETICS  DOA: 3-5 hours.

 Drugs that increase the renal excretion of  t1/2: 90 minutes.


solutes and water.
 Plasma CHON binding:Strong.
 Drugs that increase the excretion of sodium
and water from the body by an action on the  MOA: Inhibits the NA/K/Cl transport system
kidneys. in the luminal membrane of the thick
ascending limb of the loop of
Henle.

CLASSIFICATION LOOP OR HIGH-CEILING DIURETICS

 Drugs acting directly on the nephron  ADR


 Loop diuretics  Hypokalemic metabolic alkalosis
 Thiazide diuretics  Ototoxicity
 Potassium-sparing diuretics  Hyperuricemia
 Drugs acting indirectly by modifying the  Hypomagnesemia, hypocalcemia
content of the filtrate  Allergic reactions, nausea, deafness
 Osmotic diuretics  Hypovolemia, hypotension
 Carbonic anhydrase inhibitors  CLINICAL USES
THERAPEUTIC INDICATIONS  Acute pulmonary edema and other
edematous conditions
 Edematous states  Acute hypercalcemia, hyperkalemia
 Congestive heart failure  Acute renal failure
 Hepatic cirrhosis  Anion overdose: Bromide,
 Renal disease fluoride, and iodide
 Idiopathic edema
 Non-edematous states THIAZIDE DIURETICS
 HPN
 Nephrolithiasis  Short-acting (up to 12 hours)
 Hypercalcemia  Chlorothiazide, hydrochlorothiazide
 Diabetes insipidus
 Intermediate-acting (12-24 hours)
LOOP OR HIGH-CEILING DIURETICS  Bendroflumethazide, benzthiazide,
cyclothiazide, hydroflumethiazide,
 Anthranilic derivatives with sulfonamide metolazone, quinethazone,
substituent (furosemide, bumetanide) or trichlormethiazide
aryloxyacetic acid without a sulfonamide  Long-acting (> 24 hours)
component (ethacrynic acid).  Chlorthalidone, indapamide,
 AGENTS: Ethacrynic acid, furosemide, methyclothiazide, polythiazide
bumetanide, Chlorthalidone, Indapamide, and Metolazone:
muzolimine, piretanide, Thiazide-like diuretics à with sulfonamide residue
torsemide. and same MOA.
 PHARMACOKINETICS
 Administered by: Oral or Structural Features
parenteral route.
 Peak effect: 30-60 minutes.
 Benzene ring with a sulfonamide group at  Nephrogenic diabetes insipidus
position 7 and halogen at position 6.
 Saturation of 3,4 double bonds à increased POTASSIUM-SPARING DIURETICS
potency (hydrochlorothiazide).  AGENTS: Spironolactone (steroid analogue
 Lipophilic substituents at position 3 or antagonist of aldosterone), eplerenone,
methyl groups at position 2 à enhanced triamterene, amiloride (pteridine orpyrazine
potency and prolonged activity derivative).
(cyclothiazide).  PHARMACOKINETICS
 Replacement of sulfonyl group in position 1  Spironolactone: Oral, t1/2 of 10
by carbonyl group à prolonged activity minutes, canrenone (active
(quinethazone). metabolite) à t1/2 of 16 hours.
 Thiazides without the sulfonamide group  Triamterene: Oral, DOA of 12-16
(diazoxide) à anti-HPN activity without hours, metabolized in liver, excreted
diuretic activity. through the urine (unchanged).
 Amiloride: Oral, DOA of 24 hours,
THIAZIDE DIURETICS excreted through the urine
(unchanged).
 PHARMACOKINETICS
 Administration: Oral. POTASSIUM-SPARING DIURETICS
 Onset of action: Within 12
hours.  MOA
 Peak effects: 4-6 hours.  Spironolactone: Competes with
 Duration of action: 8-12 hours. aldosterone for receptor sites à
 Excretion: Tubular inhibition of sodium-retaining action
secretion. of aldosterone (distal tubule).
 MOA: Inhibits NaCl cotransporter in the  Triamterene/Amiloride: Blocks
luminal side of the distal convoluted tubule. sodium transport channels à
decreased sodium reabsorption and
potassium excretion.
 SOA: Collecting tubule
 ADR:
 Hyperkalemia, hyperchloremic
metabolic acidosis
 Gynecomastia, menstrual disorders,
testicular atrophy
 Peptic ulcer, acute renal failure,
kidney stones, increased uric acid

THIAZIDE DIURETICS

 ADR
 Hypokalemic metabolic alkalosis
 Hyperuricemia, impaired
carbohydrate tolerance
 Hypercholesterolemia, hyponatremia
 Sulfonamide-type allergic reactions
 Weakness, fatigue, paresthesia,
headache, restlessness POTASSIUM-SPARING DIURETICS
 Male impotence, encephalopathy
 NAV, bloating, constipation  CLINICAL USES
 CLINICAL USES  Primary hyperaldosteronism
 HPN  Secondary hyperaldosteronism due
 CHF to hepatic cirrhosis complicated by
 Nephrolithiasis due to idiopathic ascites
hypercalciuria
To prevent potassium loss in
combination with potassium-losing
diuretics
 As adjunct with thiazides and loop
diuretics to treat HPN
 CONTRAINDICATIONS
 Oral potassium administration à
fatal hyperkalemia
 Liver disease
 ACE inhibitor or b-blocker

OSMOTIC DIURETICS

 AGENTS: Mannitol, urea, glycerin, sorbitol.


 ADMINISTRATION: Intravenous.
 Duration of Action: 1-2 hours. POTENTIAL DRUG INTERACTIONS
 MOA: Prevents the normal absorption of
water by interposing a counteracting  b-blocker + thiazide à Increased blood
osmotic force. glucose,
 SOA: Proximal tubule, descending limb of urates, and lipids
Henle’s loop, collecting tubule.  Digitalis glycosides + thiazide/loop diuretic
 ADR: Extracellular volume expansion à
manifested Hypokalemia
by headache, NAV; dehydration,
hyponatremia.  ACE inhibitor + K-sparing diuretic à
Hyperkalemia,
 CLINICAL USES: Short-term treatment of
cardiac effects
glaucoma; cerebral edema associated with
tumors and neurosurgical procedures  Aminoglycosides + loop diuretic à
(decreases ICP); to prevent development of Ototoxicity,
renal failure associated with severe nephrotoxicity
traumatic injury, CV and other complicated  Adrenal steroids + thiazide/loop diuretic à
procedures; renal extraction of bromide, Enhanced hyperkalemia
barbiturates, salicylates, etc. in overdosage.  Chlorpropamide + thiazide à Hyponatremia
 Loop diuretic/thiazides + NSAID à
decreased effects of diuretic
CARBONIC ANHYDRASE INHIBITORS
SUMMARY
 AGENTS: Acetazolamide,
dichlorphenamide, dorzolamide,  LOOP DIURETICS
methazolamide.  Used for conditions associated with
 Given orally except for dorzolamide which is moderated or severe HPN or fluid
used topically for glaucoma. retention (HF, cirrhosis, nephrotic
 MOA: Inhibits the enzyme that catalyzes syndrome).
the dehydration of carbonic acid à reduced  They are sulfonamides except
sodium bicarbonate absorption. ethacrynic acid.
 SOA: Proximal tubule.  THIAZIDES
 Duration of action: 8-12 hours.  Used to treat mild to moderate HPN,
mild heart failure, chronic calcium
 ADR: Metabolic acidosis, potassium
stone formation, and nephrogenic
depletion, renal stones, drowsiness and
diabetes insipidus.
paresthesia, sulfonamide allergy, GI upset,
BM depression.  Most important toxicity is potassium
wasting.
 CLINICAL USES: Glaucoma, urinary
alkalinization,  They are sulfonamides.
metabolic alkalosis, acute mountain  POTASSIUM-SPARING DIURETICS
sickness, epilepsy (adjuvant).  Used for prevention of potassium
 CONTRAINDICATION: Hepatic cirrhosis à wasting by other diuretics.
decreased  Spironolactone and eplerenone are
ammonia excretion. particularly effective in treating heart
failure and other high-aldosterone
conditions.
 The major toxicity is hyperkalemia.
 Eplerenone has no anti-androgen
effects.
 They are not sulfonamides.

 CARBONIC ANHYDASE INHIBITORS


 Used as therapy for galucoma and
altitude sickness and to reduce
metabolic alkalosis.
 May cause hepatic encephalopathy.
 They are sulfonamides and are cross-
allergenic with other sulfonamides.
 OSMOTIC DIURETICS
 Used to treat acute glaucoma and to
protect the kidney from solute
overload caused by crush injury or
chemotherapy.
 Mannitol is the major osmotic
diuretic.

VASOPRESSIN
(ADH, anti-diuretic hormone)

 A peptide hormone released by the posterior


pituitary in response to rising plasma tonicity
or falling BP.
 Possesses antidiuretic and vasopressor
properties.
 A deficiency of the hormone results in
diabetes insipidus.
 MOA: Activates 2 subtypes of G-protein-
coupled receptors: 1. V1 receptors – on
vascular smooth muscle cells; mediate
vasoconstriction.
2. V2 receptors – on renal tubule
cells; reduce diuresis through increased water
permeability and water resorption in the
collecting tubules.
 Administered IV or IM.
 t ½ of circulating vasopressin: 15
minutes.
 ADR: Headache, nausea, abdominal
cramps, agitation, and allergic reactions;
hyponatremia, seizures, vasoconstriction.
 ADH agonist: Desmopressin
 ADH antagonists: Conivaptan, Tolvaptan

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