Adverse Drug Reaction Classification System

Pharmaceutical Information
Drug Name Olmesartan
Drug ID BADD_D01602
Description Olmesartan belongs to the angiotensin II receptor blocker (ARB) family of drugs, which also includes [telmisartan], [candesartan], [losartan], [valsartan], and [irbesartan]. ARBs selectively bind to angiotensin receptor 1 (AT1) and prevent the protein angiotensin II from binding and exerting its hypertensive effects, which include vasoconstriction, stimulation and synthesis of aldosterone and ADH, cardiac stimulation, and renal reabsorption of sodium, among others. Overall, olmesartan's physiologic effects lead to reduced blood pressure, lower aldosterone levels, reduced cardiac activity, and increased excretion of sodium. Olmesartan also affects the renin-angiotensin aldosterone system (RAAS), which plays an important role in hemostasis and regulation of kidney, vascular, and cardiac functions. Pharmacological blockade of RAAS via AT1 receptor blockade inhibits negative regulatory feedback within RAAS, which is a contributing factor to the pathogenesis and progression of cardiovascular disease, heart failure, and renal disease. In particular, heart failure is associated with chronic activation of RAAS, leading to inappropriate fluid retention, vasoconstriction, and ultimately a further decline in left ventricular function. ARBs have been shown to have a protective effect on the heart by improving cardiac function, reducing afterload, increasing cardiac output and preventing ventricular hypertrophy and remodelling.[A174154] By comparison, the angiotensin-converting enzyme inhibitor (ACEi) class of medications (which includes drugs such as [ramipril], [lisinopril], and [perindopril]) inhibit the conversion of angiotensin I to angiotensin II through inhibition of the ACE enzyme. However, this does not prevent the formation of all angiotensin II within the body. The angiotensin II receptor blocker (ARB) family of drugs unique in that it blocks all angiotensin II activity, regardless of where or how it was synthesized. Olmesartan is commonly used for the management of hypertension and Type 2 Diabetes-associated nephropathy, particularly in patients who are unable to tolerate ACE inhibitors. ARBs such as olmesartan have been shown in a number of large-scale clinical outcomes trials to improve cardiovascular outcomes including reducing risk of myocardial infarction, stroke, the progression of heart failure, and hospitalization.[A174124,A178153,A173869,A185324,A185327,A185333,A185342,A185345] Like other ARBs, olmesartan blockade of RAAS slows the progression of diabetic nephropathy due to its renoprotective effects.[A185906,A185909,A185912] Orally available olmesartan is produced as the prodrug olmesartan medoxomil which is rapidly converted _in vivo_ to the pharmacologically active olmesartan.[A175330] It was developed by Daiichi Sankyo Pharmaceuticals and approved in 2002.[A175345, L5560]
Indications and Usage Olmesartan is indicated for the treatment of hypertension either alone or in combination with other antihypertensive agents.[F4709,F4712,A173869] Olmesartan is also used off-label for the management Type 2 Diabetes-associated nephropathy, heart failure, and post-myocardial infarction, particularly in patients who are unable to tolerate ACE inhibitors.[A178153,A185912,A185915] ARBs such as olmesartan have been shown in a number of large-scale clinical outcomes trials to improve cardiovascular outcomes including reducing risk of myocardial infarction, stroke, the progression of heart failure, and hospitalization.[A174124,A178153,A173869,A185324,A185327,A185333,A185342,A185345] Like other ARBs, olmesartan blockade of RAAS slows the progression of diabetic nephropathy due to its renoprotective effects.[A185906,A185909,A185912]
Marketing Status approved; investigational
ATC Code Not Available
DrugBank ID DB00275
KEGG ID D05246
MeSH ID C437965
PubChem ID 158781
TTD Drug ID Not Available
NDC Product Code Not Available
UNII 8W1IQP3U10
Synonyms olmesartan | omesartan | 4-(hydroxy-1-methylethyl)-2-propyl-1-((2'-(1H-tetrazol-5-yl)-1,1'-biphenyl-4-yl)methyl)-1H-imidazole-5-carboxylic acid | RNH 6270 | CS-088
Chemical Information
Molecular Formula C24H26N6O3
CAS Registry Number 144689-24-7
SMILES CCCC1=NC(=C(N1CC2=CC=C(C=C2)C3=CC=CC=C3C4=NNN=N4)C(=O)O)C(C)(C)O
Chemical Structure
ADRs Induced by Drug
*The priority for ADR severity classification is based on FAERS assessment, followed by the most severe level in CTCAE rating. If neither is available, it will be displayed as 'Not available'.
**The 'Not Available' level is hidden by default and can be restored by clicking on the legend twice.
ADR Term ADReCS ID ADR Frequency (FAERS) ADR Severity Grade (FAERS) ADR Severity Grade (CTCAE)
Laryngeal oedema10.01.05.003; 22.04.02.001; 23.04.01.0050.000157%
Laryngeal pain22.12.03.010--
Lethargy08.01.01.008; 17.02.04.003; 19.04.04.004--
Leukopenia01.02.02.001---
Lip swelling07.05.04.005; 10.01.05.005; 23.04.01.007---
Lipoma15.09.01.001; 16.18.01.0010.000105%-
Loss of consciousness17.02.04.004---
Lymphocytosis01.02.01.0030.000524%-
Lymphoma01.12.01.001; 16.20.01.0010.000105%-
Malabsorption07.17.01.001; 14.02.01.0040.011977%
Malaise08.01.01.003--
Melaena07.12.02.004; 24.07.02.0130.000577%-
Metabolic acidosis14.01.01.0030.001731%-
Microalbuminuria05.07.02.002; 14.07.02.002; 20.02.01.026---
Mucosal dryness08.01.06.0010.000157%-
Muscle atrophy15.05.03.003; 17.05.03.0040.000105%-
Muscle spasms15.05.03.004--
Myalgia15.05.02.001--
Myocardial ischaemia02.02.02.008; 24.04.04.0100.000105%-
Myopathy15.05.05.0010.000105%-
Nasal congestion22.04.04.001--
Nasopharyngitis11.01.13.002; 22.07.03.002---
Nausea07.01.07.0010.009166%
Neck pain15.03.04.009--
Nephrolithiasis20.04.01.0020.000388%
Nephropathy20.05.03.0010.000105%-
Nervous system disorder17.02.10.001---
Neutropenia01.02.03.004---
Normochromic normocytic anaemia01.03.02.0050.000210%-
Oedema08.01.07.006; 14.05.06.010---
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