Презентация на тему Antihypertensive and lipid-lowering drugs

and 0.1 g
Furosemide (Lasix) – Tab. 0.04 g ;

amp 1%-2 ml
Bumetanide (Burinexe) –
Tab. 0.001 g; amp 0.025% - 2 ml
Indapamide – Tab. 2.5 mg (0.0025 g)
Verospirone (Spironolactone) – Tab. 25 mg
Amiloride – Tab. 2.5 and 5 mg
Triamteren – Caps. 50 mg (0.05 g)

and Water Excretion =>
=> ? Extracellular Volume =>

?Cardiac Output and Renal Blood Flower
Electrolyte disturbance: ?K+ , ?Mg2+, ?Ca2+
Thiazide diuretics counteract the Na+ and water retention observed with other agents used
in the treatment of hypertension.
Thiazide diuretics are useful in combination therapy with
a variety of other antihypertensive drugs including
β-blockers and ACE inhibitors.
Adverse effects:
Hypokalemia and Hyperuricemia – in 70% of patients,
Hyperglycemia - in 10% of patients

be the diuretic of choice
in ⇓ Extracellular Volume

If the thiazide fails - a Loop diuretic
3. Hypercalciuria:
Thiazides inhibit urinary Ca2+ excretion
4. Diabetes Insipidus.

and Glucosuria.
3. Hyperuricemia - ? Plasma Urate Levels =>

Gout
4. Hyperlipidemia

/ K+ /2Cl- cotransport inhibition of
the Luminal

Membrane in the Proximal Part of
the Ascending Loop of Henle =>
=> increase the excretion Na+, H2O, Cl-, and K+

Clopheline (Clonidine) -
Tab. 0.000 075 and 0.00015

g amp. 0.01% - 1 ml
Methyldopa Tab. 0.25 g
Guanfacine Tab. 0.0005, 0.001 and 0.002 g
Moxonidine Tab. 0.0002 and 0.0004 g

mild to moderate hypertension that has not responded adequately

to the treatment with diuretics alone.
After IV injection, Clopheline → a brief ?BP followed by more prolonged hypotension.
The pressor response is due to direct stimulation of presynaptic α2 adrenoreceptors in arterioles.

– tab. 0.1 mg and 0.25 mg
Octadine (Guanethidine) –

tab. 0.025 g (25 mg)
b) Ganglioblockers:
Benzohexonium – tab. 0.1 and 0.25 g, amp. 2.5% - 1 ml
Pentamine – amp. 5% - 1 ml
c) β-Blockers:
Propranolol (Anaprilin) – tab. 10 and 40 mg; amp. 0.1%-1 ml
Atenolol –tab. 50 and 100 mg
Metoprolol – Tab. 50 and 100 mg
d) α – Blockers:
Phentolamine – tab. 0.025 (25 mg)
Tropaphen – (amp. 20 mg)

dependent transport of amines - Noradrenaline , Dopamine and

Serotonin
from the cytoplasm into storage vesicles
in the adrenergic nerves of all body tissues
=> depletion of Noradrenaline levels in the adrenergic neuron,
since MAO degrades the Noradrenaline (NA)
=> Sympathetic function is impaired because of ?NA release

Reserpine ? Blood Pressure by a combination of :
? Cardiac Output and
? Peripheral Vascular Resistance
Adverse effect:
Sedation, Lassitude, Nightmares, Mental Depression,
Extrapyramidal Effects resembling Parkinson's disease
as a result of dopamine depletion in the corpus striatum
GIT abnormalities - diarrhea, gastrointestinal cramps,
increase of gastric acid secretion, ulcer

in mild

to moderate hypertension
In Severe Hypertension, it is especially useful in preventing the reflex tachycardia that results from treatment with direct vasodilators
Propranolol ?BP by:
? Cardiac Output
? Sympathetic outflow from the CNS
? Renin Release and Renin-Angiotensin-Aldosteron system
Adverse effect: Bradycardia, Bronchospasm, CHF, Vasoconstriction, Cold Extremities,
Intermittent Claudication, Fatigue, Lethargy,
Mental Depression, Memory Loss, Hallucination, Impotence,
Dislipidemia: ↑ Cholesterol, ↑ Triglycerides ,
?HDL-cholesterol

Apressine (Hydralasine) – Tab. 0.01 and 0.025

g
MgSO4 – amp. 25% – 10 ml IM
Dibazole (Bendazole) –
amp. 1% - 1 and 5 ml, Tab. 2 and 4 mg
No-spa - (Drotaverine) – amp. 2%-2 ml, Tab. 0.04 g
Papaverine hydrochloride – amp. 2%-2 ml, Tab. 0.04 g
Nanipruss (Na+ Nitroprusside) –
amp. 25 and 50 mg
Euphylline (Aminophylline) –
tab. 0.15 g, amp. 2.4% - 10 ml, 24% - 1 ml

g)
●Direct Vasodilation, acting primarily on arteries and arterioles.

● ⇩Central Sympathetic Tonus
● Hydrazine Group inhibits NO inactivation.
=> Decreased Peripheral Resistance,
=> a reflex ⇧HR and cardiac output.
Clinical uses: moderately severe hypertension.
It is almost always administered in combination with
a β-blocker such as propranolol (to balance the reflex tachycardia) and a diuretic (to decrease Na+ retention).
Together, the three drugs decrease cardiac output, plasma volume, and peripheral vascular resistance.
Adverse effects: headache, nausea, sweating, arrhythmia,
lupus-like syndrome.

It was regarded as a poison because

of its
cyanide group CN.
Given in small, the drug has a specific, vascular-smooth-muscle relaxant action.
It dilates both arterial and venous vessels, resulting in reduced peripheral vascular resistance and venous return.
The drug dilates the Arterial Vessels => ⇩ the Cardiac Afterload;
dilates the Veins Vessels => ⇩ the Cardiac Preload .
=> ⇩ myocardial O2 consumption and
=> improves myocardial function in low output states.
The fall in AP is accompanied by reflex tachycardia.
Nitroprusside ?plasma renin activity.

channels of L-type
A. Diphenylalkylamines:
Verapamil (Isoptin) – Tab.

40, 80 mg
B. Dihydropyridines:
1st Generation:
Nifedipine (Phenigidin) – Tab. 10 mg
2nd Generation:
Amlodipine (Norvasc) – Tab. 2.5, 5, and 10 mg
Isradipine – Caps. 2.5 and 5 mg
Nicardipine
C. Benzothiazepines:
Diltiazem – Tab. 30, 60, 120 mg

1, 3, 5 mg
Doxazosin – Tab. 2 and 4

mg
Terazosin – Tab. 2 and 5 mg

4. K+ Channel Activator:
Diazoxide – amp. 1.5% - 20 ml IV infusion
Minoxidil – Tab. 5 mg
Vial - 2%-10 ml IV infusion

Treatment of Patients with:
▼ Asthma
▼

Diabetes
▼ Peripheral Vascular Diseases

antihypertensive and antiarrhythmic action.
It manages unstable and chronic stable

angina by:
? Afterload => ? O2 Consumption.
It also ? myocardial O2 demand and cardiac work by:
Exerting Negative Inotropic Effect - ? Heart Rate:
the drug slows Cardiac Conduction directly .

In patients with Prinzmetal’s Variant Angina:
Relieving coronary artery spasm => myocardial ?O2 Delivery

Adverse Effects:
Myocardial Depression, including Cardiac Arrest,
Bradycardia, AV block, Hypotension, Heart Failure, Constipation, Peripheral Edema.

It dilates systemic arteries, resulting in:
?Total Peripheral Resistance
? Systemic

AP with slightly Increased Heart Rate,
? Afterload, and increased cardiac index.

The vasodilation effect of Nifidipine is useful in the treatment of Variant Angina caused by spontaneous coronary spasm.
In Prinzmetal’s angina, Nifedipine inhibits coronary artery spasm, increasing myocardial Oxygen Delivery.

Adverse effects: Flushing, Headache, Tachycardia, Hypotension , Dizziness, Nausea,
Constipation, and Peripheral Edema
as side effects of its vasodilation activity.

Generation long-acting Ca2+ antagonist.
It blocks the inward movement

of Ca2+ by binding to L-type Ca2+ channels in the Heart and in Smooth Muscle of
the Coronary and Peripheral Vasculature =>
=> vascular smooth muscle relaxation dilating mainly arterioles.
The drug has an Intrinsic Natriuretic Effect.
It has Antianginal, Hypotensive, Vasodilative and Spasmolytic Action
Clinical Uses:
Arterial Hypertension,
Stable and Unstable angina,
Prinzmetal’s or Variant Angina Pectoris.
Peak effects occur within 1-2 hours and persist for 24 hours.
Adverse effects: headache, peripheral edema.
Ca2+ channel blockers are useful in the treatment of patients who also have asthma, hypertension, diabetes, and/or peripheral vascular disease.

ml –
K+ Channel Activator.
The effect results from the

opening of K+ channels
in smooth muscle membranes.
This action Stabilizes the Membrane at its Resting Potential and makes contraction less likely.
Like Hydralazine, Minoxidil dilates Arterioles but not Veins.
Minoxidil is well absorbed from the GIT and is metabolized, primarily by conjugation, in the liver.
Clinical use: treatment of severe to malignant hypertension that is refractory to other drugs.
Reflex tachycardia may be severe and may require the concomitant use of a β-blocker.
Adverse effects: serious Na+ and water retention, leading to volume overload, edema, and CHF.
Hypertrichosis – the Growth of Body Hair
Minoxidil is used topically to treat Male Pattern Baldness

– Tab. 25 and 50 mg
Enalapril – Tab. 5;

10 and 20 mg
Lisinopril – Tab. 10; 20 and 40 mg
2) Angiotensine II Antagonists:
Losartan (Cozaar) – Tab. 50 mg
Valsartan – Tab. 80 mg

the ACE that cleaves Angiotensin I to form
Angiotensin

II – a potent vasoconstrictor.
They also ? the rate of Bradykinin inactivation.
Vasodilation occurs as a result of the combined effects of diminished levels of Angiotensin II and
the potent vasodilating effect of increased Bradykinin.
By reducing circulating angiotensin II levels, ACEIs:
? Aldesterone Secretion, resulting in decreased Na+ and water retention.
Unlike β-blockers, ACEIs are effective in the management of patients with chronic CHF.
ACE inhibitors are now a standard in the care of a patient following a Myocardial Infarction.

– tab. 20 and 40 mg
Pravastatin –

tab. 10 and 20 mg
Simvastatin – tab. 20 and 40 mg
Fluvastatin - tab. 20 and 40 mg
Atorvastatin
2. Fibrates:
Сlofibrate – caps. 0.25 g
Fenofibrate
Gemfibrozil – caps. 0.3 g, tab. 0.6 g

Tab. 0.05 g; 0.1 g and 0.5 g; amp.

10% - 1 ml
Nicotinamid Tab. 50 mg, amp 1% - 1 ml
Xantinol nicotinate (Complamin)
4). Bile Acid Binding Resinse:
Cholestyramine – pulv. 16.0-18.0 g PO
Colestipol – pulv. 5.0-10.0 g PO
5). Antioxidants:
Probucol – Tab. 0.5 g
6). The others: Lipostabil, Pentoxiphylline

Fluvastatin, and Atorvastatin –

inhibit the 1st enzymatic step of Sterol Synthesis -
as structural analogs of the natural substrate,
3-hydroxy-3-methylglutaric acid (HMG),
they compete to block hydroxymethylglutaryl-CoA reductase (HMG-CoA reductase).
Adverse effects: Liver Failure, Myopathy,
Rhabdomyolysis (disintegration and
purulent melting of skeletal muscles).

acid and
are similar to Endogenous Fatty Acids.
Mechanism of

Action:
? the activity of Lipoprotein Lipase,
hydrolyzing triglycerides in chylomicrons and VLDL =>
=> ?the removal of these particles from the plasma.
In contrast, HDL levels ?moderately.
Adverse Effects:
● Lithiasis: because ?Biliary Cholesterol Excretion,
a predisposition to the formation of Gallstones
● Malignancy: Treatment with Clofibrate has resulted in
a significant number of malignancy-related deaths
● Myositis

tissue –
the producer of circulating Free Fatty Acids
=>

Eliminates the building blocks needed by the liver
to produce triglycerides and VLDL .
Adverse effects:
Pruritus, gastric irritation, hyperglycaemia, hyperuriacemia, elevated hepatic aminotransferase enzymes, and hepatitis.

Food sources of nicotinic acid,
such as avocadoes and bananas,
pose no health dangers.

that bind
Negatively Charged Bile Acid and Bile Salts

in the small intestine =>
=> the Bile Acids are excreted in faeces and
are not recirculated to the liver.
Adverse effects:
Abdominal Fullness
Flatulence
Constipation