Inxight Drugs

Search results for "WHO ESSENTIAL MEDICINES LIST|Cardiovascular medicines" in comments (approximate match)

Showing 1 - 10 of 19 results

BISOPROLOL

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Y41JS2NL6U

Status:

US Approved Rx (2024)

First approved in 1992

Class (Stereo):

CHEMICAL (RACEMIC)

Targets:

Conditions:

Bisoprolol is a cardioselective beta1-adrenergic blocking agent. It lower the heart rate and blood pressure and may be used to reduce workload on the heart and hence oxygen demands. This results in a reduction of heart rate, cardiac output, systolic ...

AMLODIPINE

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1J444QC288

Status:

US Approved Rx (2015)

First approved in 1987

Class (Stereo):

CHEMICAL (RACEMIC)

Targets:

Conditions:

Amlodipine is a dihydropyridine calcium antagonist (calcium ion antagonist or slow-channel blocker) that inhibits the transmembrane influx of calcium ions into vascular smooth muscle and cardiac muscle. Experimental data suggest that amlodipine binds...

AMIODARONE

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N3RQ532IUT

Status:

US Approved Rx (2008)

First approved in 1985

Class (Stereo):

CHEMICAL (ACHIRAL)

Targets:

Conditions:

Amiodarone is an antiarrhythmic with mainly class III properties, but it possesses electrophysiologic characteristics of all four Vaughan Williams classes. Like class I drugs, amiodarone blocks sodium channels at rapid pacing frequencies, and like cl...

VERAPAMIL

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CJ0O37KU29

Status:

US Approved Rx (1987)

First approved in 1978

Class (Stereo):

CHEMICAL (RACEMIC)

Targets:

Conditions:

Verapamil is a FDA approved drug used to treat high blood pressure and to control chest pain. Verapamil is an L-type calcium channel blocker that also has antiarrythmic activity. The R-enantiomer is more effective at reducing blood pressure compared ...

DOPAMINE

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VTD58H1Z2X

Status:

US Approved Rx (2018)

First approved in 1974

Class (Stereo):

CHEMICAL (ACHIRAL)

Targets:

Conditions:

Dopamine, a sympathomimetic amine vasopressor, is the naturally occurring immediate precursor of norepinephrine. G protein-coupled dopamine receptors (D1, D2, D3, D4, and D5) mediate all of the physiological functions of the catecholaminergic neurotr...

FUROSEMIDE

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7LXU5N7ZO5

Status:

US Approved Rx (2014)

First approved in 1966

Class (Stereo):

CHEMICAL (ACHIRAL)

Targets:

Conditions:

Furosemide, a sulfonamide-type loop diuretic structurally related to bumetanide, is used to manage hypertension and edema associated with congestive heart failure, cirrhosis, and renal disease, including the nephrotic syndrome. Furosemide inhibits wa...

HYDROCHLOROTHIAZIDE

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0J48LPH2TH

Status:

US Approved Rx (2013)

First approved in 1959

Class (Stereo):

CHEMICAL (ACHIRAL)

Targets:

Conditions:

CAPOZIDE (captopril and hydrochlorothiazide tablets, USP) for oral administration combines two antihypertensive agents: captopril and hydrochlorothiazide. The mechanism of action of captopril has not yet been fully elucidated. Captopril prevents the ...

Digoxin

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73K4184T59

Status:

US Approved Rx (2004)

First approved in 1954

Class (Stereo):

CHEMICAL (ABSOLUTE)

Targets:

Conditions:

Digoxin, a cardiac glycoside similar to digitoxin, is used to treat congestive heart failure and supraventricular arrhythmias due to reentry mechanisms, and to control ventricular rate in the treatment of chronic atrial fibrillation. Digoxin inhibits...

HYDRALAZINE

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26NAK24LS8

Status:

US Approved Rx (2001)

First approved in 1953

Class (Stereo):

CHEMICAL (ACHIRAL)

Targets:

Conditions:

Hydralazine is a direct-acting vasodilator that is used as an antihypertensive agent. Hydralazine works by relaxing blood vessels (arterioles more than venules) and increasing the supply of blood and oxygen to the heart while reducing its workload. I...

LIDOCAINE

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98PI200987

Status:

US Approved OTC

First approved in 1948

Class (Stereo):

CHEMICAL (ACHIRAL)

Targets:

Conditions:

Lidocaine is a local anesthetic and cardiac depressant used to numb tissue in a specific area and for management of cardiac arrhythmias, particularly those of ventricular origins, such as occur with acute myocardial infarction. Lidocaine alters signa...

l conduction in neurons by blocking the fast voltage-gated Na+ channels in the neuronal cell membrane responsible for signal propagation. With sufficient blockage, the membrane of the postsynaptic neuron will not depolarize and will thus fail to transmit an action potential. This creates the anesthetic effect by not merely preventing pain signals from propagating to the brain, but by stopping them before they begin. Careful titration allows for a high degree of selectivity in the blockage of sensory neurons, whereas higher concentrations also affect other modalities of neuron signaling. Lidocaine exerts an antiarrhythmic effect by increasing the electrical stimulation threshold of the ventricle during diastole. In usual therapeutic doses, lidocaine hydrochloride produces no change in myocardial contractility, in systemic arterial pressure, or an absolute refractory period. The efficacy profile of lidocaine as a local anesthetic is characterized by a rapid onset of action and intermediate duration of efficacy. Therefore, lidocaine is suitable for infiltration, block, and surface anesthesia. Longer-acting substances such as bupivacaine are sometimes given preference for spinal and epidural anesthesias; lidocaine, though, has the advantage of a rapid onset of action. Lidocaine is also the most important class-1b antiarrhythmic drug; it is used intravenously for the treatment of ventricular arrhythmias (for acute myocardial infarction, digoxin poisoning, cardioversion, or cardiac catheterization) if amiodarone is not available or contraindicated. Lidocaine should be given for this indication after defibrillation, CPR, and vasopressors have been initiated. A routine preventative dose is no longer recommended after a myocardial infarction as the overall benefit is not convincing. Inhaled lidocaine can be used as a cough suppressor acting peripherally to reduce the cough reflex. This application can be implemented as a safety and comfort measure for patients who have to be intubated, as it reduces the incidence of coughing and any tracheal damage it might cause when emerging from anesthesia. Adverse drug reactions (ADRs) are rare when lidocaine is used as a local anesthetic and is administered correctly. Most ADRs associated with lidocaine for anesthesia relate to administration technique (resulting in systemic exposure) or pharmacological effects of anesthesia, and allergic reactions only rarely occur. Systemic exposure to excessive quantities of lidocaine mainly result in a central nervous system (CNS) and cardiovascular effects – CNS effects usually occur at lower blood plasma concentrations and additional cardiovascular effects present at higher concentrations, though cardiovascular collapse may also occur with low concentrations.

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Highest Phase

Approval Year

Condition

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ATC Level 1

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Substance Form

Search results for "WHO ESSENTIAL MEDICINES LIST|Cardiovascular medicines" in comments (approximate match)

BISOPROLOL

Y41JS2NL6U

AMLODIPINE

1J444QC288

AMIODARONE

N3RQ532IUT

VERAPAMIL

CJ0O37KU29

DOPAMINE

VTD58H1Z2X

FUROSEMIDE

7LXU5N7ZO5

HYDROCHLOROTHIAZIDE

0J48LPH2TH

Digoxin

73K4184T59

HYDRALAZINE

26NAK24LS8

LIDOCAINE

98PI200987