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Class 4- LOOP DIURETICS High ceiling Diuretics

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1 Class 4- LOOP DIURETICS High ceiling Diuretics
Lec-4 Class 4- LOOP DIURETICS High ceiling Diuretics

2 The diuretics that belong to this class are of extremely diverse chemical structure, such as:
The organomercurial diuretics, The 5-Sulfamoyl-2- and -3-aminobenzoic acid derivatives. Examples, furosemide and bumetanide Phenoxyacetic acid derivatives as ethacrynic acid

3 Loop diuretics Act by inhibition of Na+, K+, and Cl- reabsorption from the ascending limb of the loop of Henle in the renal tubule. They also tend to reduce renal Ca+ reabsorption, thus they are used in treatment of hypercalcemia. High efficiency diuretics. High ceiling diuretics.( what is mean? )

4

5 Mechanism of Action: Adverse Effects:
They inhibit the 1Na+/1K+/2Cl- cotransport system located on the luminal membrane of cells of the thick ascending limb of Henle’s loop Adverse Effects: 1. Hypokalemic alkalosis. 2. Fluid and electrolyte losses 3. Reduction in plasma volume may result from long-term use of these diuretics. 4.Hypersensitivity reactions such as urticaria, fever, and interstitial nephritis.

6 High-ceiling or loop diuretics
Results from structure-activity relationship studies that led to the development of furosemide.

7 Loop Diuretics active in “loop” of Henle Furosemide (prototype)
Bumetanide Torsemide Ethacrynic acid

8 Furosemide Name: 5-(Aminosulfonyl)-4-chloro-2-[(2-furanylmethyl)amino] benzoic acid

9 Synthesis of Furosemide

10 SAR of 5-Sulfamoyl-2- and -3-aminobenzoic acid derivatives
1)  The substituent at the 1-position must be acidic, The carboxyl group provides optimal diuretic activity, but other groups, as tetrazole, may have respectable diuretic activity. 2) A sulfamoyl group in the 5-position is essential for optimal high-ceiling diuretic activity. 3)  The activating group (x-) in the 4-position can be Cl- or CF3-, a phenoxy-, alkoxy-, anilino-, benzyl-, or benzoyl- group. 4)  Substitutents that can be tolerated on the 2-amino group series: only furfuryl-, > benzyl-, > thienylmethyl. 5) Substituent, on the 3-amino group series: can very widely without affecting optimal diuretic activity.

11 Phenoxyacetic acids, Ethacrynic Acid, (Edecrin®).
2,3-Dichloro-4-(2-methylene-1-oxobutyl) phenoxyacetic acid Uses: Ethacrynic acid is prescribed for individual who has a known hypersensitivity to Sulfamoyl containing drugs.

12 Phenoxyacetic acids, Ethacrynic Acid, (Edecrin®).
SARs: Optimal diuretic activity is achieved when: 1. An oxyacetic acid moiety is placed in the 1-position on the benzene ring, 2. A sulfhydryl-reactive acryloyl moiety is located para to the oxyacetic acid group, 3. Activating groups (Cl- or CH3-) occupy either the 3-position or the 2- and 3-positions. 4. Alkyl substituent of two- to four-carbon atoms in length occupy the position α to the carbonyl on the acryloyl moiety.

13 Synthesis of Ethacrynic acid

14 Class 5:Potassium sparing diuretics

15 three groups 1- steroid aldosterone antagonists as spironolactone,
2- triamterene 3- Pyrazinoylguanidines amiloride

16 Potassium-sparing diuretics
Competitive aldosterone antagonists: Spironolactone Blockers of the amiloride-sensitive Na+ channels: Amiloride Triamterene

17

18 Spirolactones

19 Mechanism of Action Keep K+
Aldosterone-stimulated sodium reabsorption in exchange for potassium and hydrogen ion, in the distal, collecting tubules and ducts K+ sparing diuretics function in CCD decrease Na+ transport in collecting tubule all previous-discussed diuretics is that they increase the renal excretion rate of K+ and thus can induce hypokalemia

20 5. Potassium- sparing diuretics Amiloride Triamterene Spironolactone
3% Often they are used in combination with diuretics, causing hypokalemia. They have weak diuretic action and save K+.

21 Other potassium-sparing diuretics: triamterene and amiIoride:
Mechanism and site of action: Triamterene and amiloride (organic bases) inhibit sodium transport in nephron segments beyond the distal convoluted tubule. They do not interact with aldosterone receptors.

22 Triamterene & amiloride
Interferes with cationic exchange by blocking luminal Na+ channels in the late distal convoluted tubule and collecting duct. amiloride Triamterene

23 Activity Brain Storming

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