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Antihypertensive drugs

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Sushmitha Sushma

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UNDER THE GUIDENCE OF: Ms. G. USHA SREE Asst.Prof Dept. Of Pharmaceutical Analysis. SEMINAR BY: SUSHMITHA.K 11T21R0070. CMR COLLEGE OF PHARMACY
Contents  Introduction  Classification of hypertension  Types  Signs and symptoms  Causes  Classification  Treatment  Conclusion  References
Introduction Hypertension Systolic Blood Pressure (SBP) Diastolic Blood Pressure (DBP) > 140 mmHg > 90 mmHg
Classification of hypertension: Systolic B.P. Diastolic B.P. Normal < 120 <80 Pre Hypertension 120-139 80-89 Stage I 140-159 90-99 Stage II ≥160 ≥100
sphygmomanometer
Types Types of Hypertension Essential Secondary disorder of unknown origin affecting the Blood Pressure regulating mechanisms Secondary to other disease processes
Signs and symptoms  Severe headache  Fatigue or confusion  Vision problems  Chest pain  Difficulty in breathing  Irregular heartbeat  Blood in urine  Pounding in your chest, neck or ears  Hypertensive crisis may lead to heart attack or stroke
Causes
A.Primary Hypertension  It is present in 95%of the population No defective cause Build of fatty deposits inside arteries (atherosclerosis) Thickening of artery walls Excessive contraction of small arteries (arterioles)
B. Secondary hypertension  It occurs in about 5-10% of the population  It develops through manifestation of other medical problems like  Renal problems  Harmonal disorders  Heart problems  Sleep apnea  Over the counter drugs  Obsety  Alcohol  Genitics  stress
Mechanisms for controlling blood pressure  1. Baroreceptors and the sympathetic nervous system  2. The Humoral Renin Angiotensin Aldosterone System
Baroreceptors and the sympathetic nervous system
Classification: ANTI-HYPERTENSIVE DRUGS Diuretics ACE Inhibitor Angiotensin receptor Blocker Direct Renin Inhibitor Calcium channel Blocker Alpha Adrenergic Blockers Beta Adrenergic Blockers α + β Adrenergic Blockers Central Sympatholytic Vasodil- ators Thiazide, High- ceiling, K+ sparing Losartan, Valsartan Aliskiren Verapamil, Diltiazem, Nifedipine Prazosin, Terazosin, Doxazosin Propronolo Metaprolol Atenolol Labetalol, Carvedilol Clonidine Methyldopa Hydralazine, Minoxidil Sodium nitroprusside Captopril Enalapril lisnopril
DIURETICS  Diuretics can be used as first-line drug therapy for hypertension.  Prevent stroke, myocardial infraction and congestive heart failure.  Diuretics are superior to β-blockers for treating hypertension in older patients.  Diuretics are classified in to: Thiazide diuretics High ceiling diuretics and K + sparing diuretics
Thiazide diuretics  The diuretic of choice for uncomplicated hypertension. Mechanism of action:
Pharmacokinetics:  Orally active.  Absorption and elimination rates may vary.  All thiazides are ligands and compete with uric acid for elimination. Therapeutic uses: • Particularly useful in treatment of black and elderly patients.  They decreases blood pressure in both supine and standing position.  They do not cause reflex tachycardia or reduce the cardic output.
Adverse effects:  Thiazides diuretics induce hypokalemia and hypouricemia in 70% of patients and hypoglycemia in 10% of patients.  Acute gout disorders may be triggered.  Hypomagnesaemia may also occur.  Serum potassium levels should be monitored closely in patients who are predisposed to cardiac arrhythmias.
High ceiling diuretics  Furosimide, the prototype of this class, is a strong diuretic.  They cause decreased renal vascular resistance and increased renal blood flow.  They are more liable to cause fluid and electrolyte imbalance, weakness and other side effects.  Indicated in hypertension only when it is complicated by : Chronic renal failure. Coexisting refractory congestive heart failure.
Potassium sparing diuretics  Spironolactone, amiloride, eplerenone lower blood pressure slightly.  They are used only in conjunction with a thiazide diuretic to prevent K+ loss and to aggument the anti-hypertensive action.  Hyperkalemia should be watched when K+ sparing diuretics are used with ACE inhibitors/ARBs.
Angiotensin converting enzyme (ACE) inhibitors Mechanism of action: Angiotensin-I Angiotensin-II Angiotensin-II Na+ and water level Angiotensin converting enzyme Cardiac work and blood pressure
Pharmacokinetics:  Orally well absorbed.  Prescence of food in stomach reduces its bioavailability.  Penetration in brain is poor.  It is partly metabolized and excreted unchanged in urine.  The plasma t1/2 is 2 hours. Therapeutic uses:  Hypertension  Chronic congestive heart failure  Diabetic nephropathy
Adverse effects:  Dry persistent cough  Skin rashes, fever, altered taste, hypotension and hyperkalemia.  Potassium levels must be monitored.  They can induce fetal malformation.  Contraindications: Severe renal artery stenosis. Aortic stenosis Coarctation of the aorta. pregnancy.
Direct Renin Inhibitor o Aliskiren is a selective renin inhibitor. Mechanism of action:
Pharmacokinetics:  It is administered orally, but bioavailability is very low.  It is mainly eliminated in faeces, small amount in urine.  The plasma t1/2 is >24 hours. Therapeutic uses:  It lowers blood pressure as effective as ARBs, ACE inhibitors and thiazides.  Combined with diuretics, calcium-channel blockers, ACE inhibitors, and with ARBs. Adverse effects:  Dyspepsia, abdominal pain, loose motions, headache, and dizziness.  Acute hypotension, hyperkalaemia, cough, angioedema  It is contraindicated during pregnancy.
Calcium Channel Blockers  Calcium channel blockers are recommended when the preferred first-line agents are ineffective or contraindicated.  They are effective in treating hypertension in patients with angina or diabetics. Three important classes of Calcium channel blockers are:  Diphenylalkylamines: Verapamil (a hydrophilic papaverine congener)  Benzothiazepine: Dilthiazem (hydrophilic)  Dihydropiridines: Nifedipine (lipophilic)
Mechanism of action:
Verapamil:  It dilates arterioles and has some α-adrenergic blocking activity.  It has significant effect in both cardiac and vascular smooth muscle cells.  It is used to treat angina, supra ventricular tachyarrthymias and migraine and cluster headache.  Adverse effects are nausea, constipation and bradycardia.  Interactions- i. It should not be given with β-blockers ii. It increases plasma digoxin level iii. It should not be used along with other cardiac depressants like quinidine.
Pharmacokinetics:  Most of calcium-channel blockers have short half-lives (3- 8hours) following an oral dose.  Amlodipine has a very long half life. Therapeutic uses:  Used as one of the first line monotherapy.  They are preferred in elderly and black hypertensive patients.  Useful in treatment of asthma, angina. Adverse effects:  Constipation occurs in 10% 0f patients with verapamil.  Dizziness, fatigue are more frequent with verapamil.  Verapamil should be avoided in patients with congestive heart failure due to its negative ionotropic and dromotropic effects.  Nifedipine cause gingival enlargement.
TREATMENT OF HYPERTENSION  Hypertension is treated by: Combination therapy Oral therapy Parentral therapy.
ANTI-HYPERTENSIVE COMBINATIONS  Amlodipine 5mg + Lisnopril 5mg - AMLOPRES-L, LISTRIL-AM  Amlodipine 5mg + Atenolol 50mg – AMCARD-AT, AMLOPIN-AT, AMLOPRES-AT  Amlodipine 5mg + Enalopril 5mg – AMACE, AMTAS-E  Atenolol 25mg or 50mg + Chlorthalidone 12.5mg – TENOCLOR, TENORIC  Enalapril 10mg + Hydrochlorothiazide 25mg – ENACE-D, VASONORM-H  Rampril 2.5mg + Hydrochlorothiazide 12.5mg – CARDACE-H  Losartan 50mg + Hydrochlorothiazide 12.5mg – LOSAR-H, TOZAARH-H, LOSACAR-H
ANTI-HYPERTENSIVES TO BE AVOIDED DURING PREGNANCY: SL.NO DRUGS RISK 1. ACE Inhibitors, ARBs Foetal damage 2. Diuretics Reduce blood volume, placental infraction 3. Nonselective β-blockers neonatal bradycardia, hypoglycaemia. 4. Sodium nitroprusside Contraindicated in eclampsia. SL.NO. DRUGS 1. Methyldopa 2. Dihydropyridine 3. Cardio selective beta-blocker 4. Prazosin, clonidine ANTI-HYPERTENSIVES FOUND SAFER DURING PREGNANCY:
HYPERTENSIVE EMERGENCIES AND URGENCIES:  Cerebrovascular accident or head injury with high blood pressure  Hypertensive encephalopathy  Hypertensive acute left ventricular failure and pulmonary edema  Unstable angina or myocardial infraction with raised blood pressure  Dissecting aortic aneurysm  Acute renal failure with raised blood pressure  Eclampsia  Hypertensive episodes in pheochromocytoma.
 ORAL THERAPY: NIFEDIPINE:  10 mg soft geletine capsules  Oral or sub-lingual administration for every 30 mins  Causes fall in blood pressure, myocardial infraction or stroke CAPTOPRIL:  25 mg orally for every 1-2 hours  Response is variable  Carries risk of excessive hypotension CLONIDINE:  100 µg orally for every 1-2 hours  Produces sedation  Rebound rise in blood pressure on stopping the drug.
PARENTRAL THERAPY: SL.NO. DRUG Route of administration and dose 1. Sodium nitroprusside Intravenous, 20-30µg/min 2. Glyceryl trinitrate Intravenous, 5-20 µg/min 3. Esmolol Intravenous,50-10µg/kg/min 4. Phentolamine Intravenous, 5-10 mg 5. Furosemide Oral/Intravenous,20-80 mg
Preparations available:  Captopril (generic, capotus) Oral-12.5, 25,100 mg tablets. Parenteral (Enalaprilat)-12.5 mg/ml for injection  Losartan (lozaar) Oral- 25, 50,100 mg tablet  Verapamil (generic, calan, Isoptin) Oral- 40, 80, 120 mg tablet  Diltiazem (generic, cardizem) Oral- 30, 60, 90, 120 mg tablet Parenteral- 5 mg/ml for injection  Nitroprusside (generic, Nitropress) Parenteral- 50 mg/vial.
Conclusion:  Hypertension is a common disorder in adults.  Now a days it was common problem seen in youngsters mainly due to changes in life style modifications, obesity and hereditary.  Maintenance of a healthy life style and proper follow up of non-pharmacological treatment like food habits, regular exercise can overcome the usage of anti hypertensive drugs.  Normalize blood pressure and prevent complications.
References:  Barar F.S.K, Anti-Hypertensive drugs. Essentials of Pharmcotherapeutics, 2007.4th edition. Pg. 239-249.  Lippincott Williams and Wilkins, Anti-Hypertensive drugs. Pharmacology, 2012.5th. Pg. 227-242.  Rang and Dale, Anti-Hypertensive drugs. Pharmacology, 2007.6th edition. Pg. 311-312.  Satoskar R.S, Bhandarkar S.D, Nirmala N.Rege, Anti- Hypertensive drugs. Pharmacology and Pharmcotherapeutics, 2009.21th edition. Pg. 404-433.  Tripathi KD, Anti-Hypertensive drugs. Essentials of Medicinal Pharmacology, 2013.7th edition. Pg. 558-574.  www.coursewareobjects.com  www.pitt.edu.com
Thank you….

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Antihypertensive drugs

  • 1. UNDER THE GUIDENCE OF: Ms. G. USHA SREE Asst.Prof Dept. Of Pharmaceutical Analysis. SEMINAR BY: SUSHMITHA.K 11T21R0070. CMR COLLEGE OF PHARMACY
  • 2. Contents  Introduction  Classification of hypertension  Types  Signs and symptoms  Causes  Classification  Treatment  Conclusion  References
  • 3. Introduction Hypertension Systolic Blood Pressure (SBP) Diastolic Blood Pressure (DBP) > 140 mmHg > 90 mmHg
  • 4. Classification of hypertension: Systolic B.P. Diastolic B.P. Normal < 120 <80 Pre Hypertension 120-139 80-89 Stage I 140-159 90-99 Stage II ≥160 ≥100
  • 6. Types Types of Hypertension Essential Secondary disorder of unknown origin affecting the Blood Pressure regulating mechanisms Secondary to other disease processes
  • 7. Signs and symptoms  Severe headache  Fatigue or confusion  Vision problems  Chest pain  Difficulty in breathing  Irregular heartbeat  Blood in urine  Pounding in your chest, neck or ears  Hypertensive crisis may lead to heart attack or stroke
  • 9. A.Primary Hypertension  It is present in 95%of the population No defective cause Build of fatty deposits inside arteries (atherosclerosis) Thickening of artery walls Excessive contraction of small arteries (arterioles)
  • 10. B. Secondary hypertension  It occurs in about 5-10% of the population  It develops through manifestation of other medical problems like  Renal problems  Harmonal disorders  Heart problems  Sleep apnea  Over the counter drugs  Obsety  Alcohol  Genitics  stress
  • 11. Mechanisms for controlling blood pressure  1. Baroreceptors and the sympathetic nervous system  2. The Humoral Renin Angiotensin Aldosterone System
  • 12. Baroreceptors and the sympathetic nervous system
  • 13.
  • 14. Classification: ANTI-HYPERTENSIVE DRUGS Diuretics ACE Inhibitor Angiotensin receptor Blocker Direct Renin Inhibitor Calcium channel Blocker Alpha Adrenergic Blockers Beta Adrenergic Blockers α + β Adrenergic Blockers Central Sympatholytic Vasodil- ators Thiazide, High- ceiling, K+ sparing Losartan, Valsartan Aliskiren Verapamil, Diltiazem, Nifedipine Prazosin, Terazosin, Doxazosin Propronolo Metaprolol Atenolol Labetalol, Carvedilol Clonidine Methyldopa Hydralazine, Minoxidil Sodium nitroprusside Captopril Enalapril lisnopril
  • 15. DIURETICS  Diuretics can be used as first-line drug therapy for hypertension.  Prevent stroke, myocardial infraction and congestive heart failure.  Diuretics are superior to β-blockers for treating hypertension in older patients.  Diuretics are classified in to: Thiazide diuretics High ceiling diuretics and K + sparing diuretics
  • 16. Thiazide diuretics  The diuretic of choice for uncomplicated hypertension. Mechanism of action:
  • 17. Pharmacokinetics:  Orally active.  Absorption and elimination rates may vary.  All thiazides are ligands and compete with uric acid for elimination. Therapeutic uses: • Particularly useful in treatment of black and elderly patients.  They decreases blood pressure in both supine and standing position.  They do not cause reflex tachycardia or reduce the cardic output.
  • 18. Adverse effects:  Thiazides diuretics induce hypokalemia and hypouricemia in 70% of patients and hypoglycemia in 10% of patients.  Acute gout disorders may be triggered.  Hypomagnesaemia may also occur.  Serum potassium levels should be monitored closely in patients who are predisposed to cardiac arrhythmias.
  • 19. High ceiling diuretics  Furosimide, the prototype of this class, is a strong diuretic.  They cause decreased renal vascular resistance and increased renal blood flow.  They are more liable to cause fluid and electrolyte imbalance, weakness and other side effects.  Indicated in hypertension only when it is complicated by : Chronic renal failure. Coexisting refractory congestive heart failure.
  • 20. Potassium sparing diuretics  Spironolactone, amiloride, eplerenone lower blood pressure slightly.  They are used only in conjunction with a thiazide diuretic to prevent K+ loss and to aggument the anti-hypertensive action.  Hyperkalemia should be watched when K+ sparing diuretics are used with ACE inhibitors/ARBs.
  • 21. Angiotensin converting enzyme (ACE) inhibitors Mechanism of action: Angiotensin-I Angiotensin-II Angiotensin-II Na+ and water level Angiotensin converting enzyme Cardiac work and blood pressure
  • 22. Pharmacokinetics:  Orally well absorbed.  Prescence of food in stomach reduces its bioavailability.  Penetration in brain is poor.  It is partly metabolized and excreted unchanged in urine.  The plasma t1/2 is 2 hours. Therapeutic uses:  Hypertension  Chronic congestive heart failure  Diabetic nephropathy
  • 23. Adverse effects:  Dry persistent cough  Skin rashes, fever, altered taste, hypotension and hyperkalemia.  Potassium levels must be monitored.  They can induce fetal malformation.  Contraindications: Severe renal artery stenosis. Aortic stenosis Coarctation of the aorta. pregnancy.
  • 24. Direct Renin Inhibitor o Aliskiren is a selective renin inhibitor. Mechanism of action:
  • 25. Pharmacokinetics:  It is administered orally, but bioavailability is very low.  It is mainly eliminated in faeces, small amount in urine.  The plasma t1/2 is >24 hours. Therapeutic uses:  It lowers blood pressure as effective as ARBs, ACE inhibitors and thiazides.  Combined with diuretics, calcium-channel blockers, ACE inhibitors, and with ARBs. Adverse effects:  Dyspepsia, abdominal pain, loose motions, headache, and dizziness.  Acute hypotension, hyperkalaemia, cough, angioedema  It is contraindicated during pregnancy.
  • 26. Calcium Channel Blockers  Calcium channel blockers are recommended when the preferred first-line agents are ineffective or contraindicated.  They are effective in treating hypertension in patients with angina or diabetics. Three important classes of Calcium channel blockers are:  Diphenylalkylamines: Verapamil (a hydrophilic papaverine congener)  Benzothiazepine: Dilthiazem (hydrophilic)  Dihydropiridines: Nifedipine (lipophilic)
  • 28. Verapamil:  It dilates arterioles and has some α-adrenergic blocking activity.  It has significant effect in both cardiac and vascular smooth muscle cells.  It is used to treat angina, supra ventricular tachyarrthymias and migraine and cluster headache.  Adverse effects are nausea, constipation and bradycardia.  Interactions- i. It should not be given with β-blockers ii. It increases plasma digoxin level iii. It should not be used along with other cardiac depressants like quinidine.
  • 29. Pharmacokinetics:  Most of calcium-channel blockers have short half-lives (3- 8hours) following an oral dose.  Amlodipine has a very long half life. Therapeutic uses:  Used as one of the first line monotherapy.  They are preferred in elderly and black hypertensive patients.  Useful in treatment of asthma, angina. Adverse effects:  Constipation occurs in 10% 0f patients with verapamil.  Dizziness, fatigue are more frequent with verapamil.  Verapamil should be avoided in patients with congestive heart failure due to its negative ionotropic and dromotropic effects.  Nifedipine cause gingival enlargement.
  • 30. TREATMENT OF HYPERTENSION  Hypertension is treated by: Combination therapy Oral therapy Parentral therapy.
  • 31. ANTI-HYPERTENSIVE COMBINATIONS  Amlodipine 5mg + Lisnopril 5mg - AMLOPRES-L, LISTRIL-AM  Amlodipine 5mg + Atenolol 50mg – AMCARD-AT, AMLOPIN-AT, AMLOPRES-AT  Amlodipine 5mg + Enalopril 5mg – AMACE, AMTAS-E  Atenolol 25mg or 50mg + Chlorthalidone 12.5mg – TENOCLOR, TENORIC  Enalapril 10mg + Hydrochlorothiazide 25mg – ENACE-D, VASONORM-H  Rampril 2.5mg + Hydrochlorothiazide 12.5mg – CARDACE-H  Losartan 50mg + Hydrochlorothiazide 12.5mg – LOSAR-H, TOZAARH-H, LOSACAR-H
  • 32. ANTI-HYPERTENSIVES TO BE AVOIDED DURING PREGNANCY: SL.NO DRUGS RISK 1. ACE Inhibitors, ARBs Foetal damage 2. Diuretics Reduce blood volume, placental infraction 3. Nonselective β-blockers neonatal bradycardia, hypoglycaemia. 4. Sodium nitroprusside Contraindicated in eclampsia. SL.NO. DRUGS 1. Methyldopa 2. Dihydropyridine 3. Cardio selective beta-blocker 4. Prazosin, clonidine ANTI-HYPERTENSIVES FOUND SAFER DURING PREGNANCY:
  • 33. HYPERTENSIVE EMERGENCIES AND URGENCIES:  Cerebrovascular accident or head injury with high blood pressure  Hypertensive encephalopathy  Hypertensive acute left ventricular failure and pulmonary edema  Unstable angina or myocardial infraction with raised blood pressure  Dissecting aortic aneurysm  Acute renal failure with raised blood pressure  Eclampsia  Hypertensive episodes in pheochromocytoma.
  • 34.  ORAL THERAPY: NIFEDIPINE:  10 mg soft geletine capsules  Oral or sub-lingual administration for every 30 mins  Causes fall in blood pressure, myocardial infraction or stroke CAPTOPRIL:  25 mg orally for every 1-2 hours  Response is variable  Carries risk of excessive hypotension CLONIDINE:  100 µg orally for every 1-2 hours  Produces sedation  Rebound rise in blood pressure on stopping the drug.
  • 35. PARENTRAL THERAPY: SL.NO. DRUG Route of administration and dose 1. Sodium nitroprusside Intravenous, 20-30µg/min 2. Glyceryl trinitrate Intravenous, 5-20 µg/min 3. Esmolol Intravenous,50-10µg/kg/min 4. Phentolamine Intravenous, 5-10 mg 5. Furosemide Oral/Intravenous,20-80 mg
  • 36. Preparations available:  Captopril (generic, capotus) Oral-12.5, 25,100 mg tablets. Parenteral (Enalaprilat)-12.5 mg/ml for injection  Losartan (lozaar) Oral- 25, 50,100 mg tablet  Verapamil (generic, calan, Isoptin) Oral- 40, 80, 120 mg tablet  Diltiazem (generic, cardizem) Oral- 30, 60, 90, 120 mg tablet Parenteral- 5 mg/ml for injection  Nitroprusside (generic, Nitropress) Parenteral- 50 mg/vial.
  • 37. Conclusion:  Hypertension is a common disorder in adults.  Now a days it was common problem seen in youngsters mainly due to changes in life style modifications, obesity and hereditary.  Maintenance of a healthy life style and proper follow up of non-pharmacological treatment like food habits, regular exercise can overcome the usage of anti hypertensive drugs.  Normalize blood pressure and prevent complications.
  • 38. References:  Barar F.S.K, Anti-Hypertensive drugs. Essentials of Pharmcotherapeutics, 2007.4th edition. Pg. 239-249.  Lippincott Williams and Wilkins, Anti-Hypertensive drugs. Pharmacology, 2012.5th. Pg. 227-242.  Rang and Dale, Anti-Hypertensive drugs. Pharmacology, 2007.6th edition. Pg. 311-312.  Satoskar R.S, Bhandarkar S.D, Nirmala N.Rege, Anti- Hypertensive drugs. Pharmacology and Pharmcotherapeutics, 2009.21th edition. Pg. 404-433.  Tripathi KD, Anti-Hypertensive drugs. Essentials of Medicinal Pharmacology, 2013.7th edition. Pg. 558-574.  www.coursewareobjects.com  www.pitt.edu.com