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Details

Stereochemistry ACHIRAL
Molecular Formula C25H19N4O5.C5H14NO
Molecular Weight 559.6129
Optical Activity NONE
Defined Stereocenters 0 / 0
E/Z Centers 0
Charge 0

SHOW SMILES / InChI
Structure of AZILSARTAN TRIMETHYLETHANOLAMINE

SMILES

C[N+](C)(C)CCO.CCOC1=NC2=C(N1CC3=CC=C(C=C3)C4=CC=CC=C4C5=NOC(=O)N5)C(=CC=C2)C([O-])=O

InChI

InChIKey=RGPFEJSMFMFCIT-UHFFFAOYSA-M
InChI=1S/C25H20N4O5.C5H14NO/c1-2-33-24-26-20-9-5-8-19(23(30)31)21(20)29(24)14-15-10-12-16(13-11-15)17-6-3-4-7-18(17)22-27-25(32)34-28-22;1-6(2,3)4-5-7/h3-13H,2,14H2,1H3,(H,30,31)(H,27,28,32);7H,4-5H2,1-3H3/q;+1/p-1

HIDE SMILES / InChI
Molecular Formula C25H20N4O5
Molecular Weight 456.4501
Charge 0
Count
Stereochemistry ACHIRAL
Additional Stereochemistry No
Defined Stereocenters 0 / 0
E/Z Centers 0
Optical Activity NONE
Molecular Formula C5H13NO
Molecular Weight 103.1628
Charge 0
Count
Stereochemistry RACEMIC
Additional Stereochemistry No
Defined Stereocenters 0 / 0
E/Z Centers 0
Optical Activity NONE

Description
Curator's Comment: description was created based on several sources, including https://www.ncbi.nlm.nih.gov/pubmed/23487168

TAK-536 (generic name: azilsartan) is an angiotensin II type 1 receptor blocker, discovered by Takeda and its mechanism of action is to lower blood pressure by inhibiting action of a vasopressor hormone Angiotensin II. Angiotensin II type 1 receptor antagonists have become an important drug class in the treatment of hypertension and heart failure. TAK-536 is in phase III clinical trial for treatment hypertension. This drug also known as active metabolite of the prodrug azilsartan medoxomil (also known as azilsartan kamedoxomil), but in some countries azilsartan rather than its prodrug is used for oral treatment.

CNS Activity

CNS Penetrant
2554
Curator's Comment: In rats, minimal azilsartan-associated radioactivity crossed the blood-brain barrier.

Originator

Approval Year

2011
587
Targets

Targets

Primary TargetPharmacologyConditionPotency
Type-1 angiotensin II receptor
40
Target ID: P30556
Gene ID: 185.0
Gene Symbol: AGTR1
Target Organism: Homo sapiens (Human)
Antagonist
2778
 0.62 nM [IC50]
Antagonist
2778
Conditions

Conditions

ConditionModalityTargetsHighest PhaseProduct
Primary
Approved
8429
EDARBI

Approved Use

Indicated for the treatment of hypertension to lower blood pressure. Lowering blood pressure reduces the risk of fatal and nonfatal cardiovascular events, primarily strokes and myocardial infarctions. Edarbi may be used either alone or in combination with other antihypertensive agents.

Launch Date

2011
Primary
Phase III
656
Unknown

Approved Use

Unknown
Cmax

Cmax

ValueDoseCo-administeredAnalytePopulation
5355.71 ng/mL
EXPERIMENT
https://pubmed.ncbi.nlm.nih.gov/27514506/
80 mg single, oral
dose: 80 mg
route of administration: Oral
experiment type: SINGLE
co-administered: Chlorthalidone
Chlorthalidone
 AZILSARTAN plasma
Homo sapiens
population: HEALTHY
age: ADULT
sex: FEMALE / MALE
food status: FASTED
141.3 ng/mL
Clinical Trial
https://clinicaltrials.gov/ct2/show/NCT02451150
10 mg single, oral
dose: 10 mg
route of administration: oral
experiment type: single
co-administered:
AZILSARTAN METABOLITE M-I plasma
Homo sapiens
population: unhealthy
age: Children
sex:
food status: Fed
191.3 ng/mL
Clinical Trial
https://clinicaltrials.gov/ct2/show/NCT02451150
5 mg single, oral
dose: 5 mg
route of administration: oral
experiment type: single
co-administered:
AZILSARTAN METABOLITE M-I plasma
Homo sapiens
population: unhealthy
age: Children
sex:
food status: Fed
227.7 ng/mL
Clinical Trial
https://clinicaltrials.gov/ct2/show/NCT02451150
5 mg single, oral
dose: 5 mg
route of administration: oral
experiment type: single
co-administered:
AZILSARTAN METABOLITE M-II plasma
Homo sapiens
population: unhealthy
age: Children
sex:
food status: Fed
179.3 ng/mL
Clinical Trial
https://clinicaltrials.gov/ct2/show/NCT02451150
10 mg single, oral
dose: 10 mg
route of administration: oral
experiment type: single
co-administered:
AZILSARTAN METABOLITE M-II plasma
Homo sapiens
population: unhealthy
age: Children
sex:
food status: Fed
888.3 ng/mL
Clinical Trial
https://clinicaltrials.gov/ct2/show/NCT02451150
5 mg single, oral
dose: 5 mg
route of administration: oral
experiment type: single
co-administered:
AZILSARTAN plasma
Homo sapiens
population: unhealthy
age: Children
sex:
food status: Fed
831.3 ng/mL
Clinical Trial
https://clinicaltrials.gov/ct2/show/NCT02451150
10 mg single, oral
dose: 10 mg
route of administration: oral
experiment type: single
co-administered:
AZILSARTAN plasma
Homo sapiens
population: unhealthy
age: Children
sex:
food status: Fed
AUC

AUC

ValueDoseCo-administeredAnalytePopulation
46688.2 ng × h/mL
EXPERIMENT
https://pubmed.ncbi.nlm.nih.gov/27514506/
80 mg single, oral
dose: 80 mg
route of administration: Oral
experiment type: SINGLE
co-administered: Chlorthalidone
Chlorthalidone
 AZILSARTAN plasma
Homo sapiens
population: HEALTHY
age: ADULT
sex: FEMALE / MALE
food status: FASTED
1420.5 ng*h/mL
Clinical Trial
https://clinicaltrials.gov/ct2/show/NCT02451150
10 mg single, oral
dose: 10 mg
route of administration: oral
experiment type: single
co-administered:
AZILSARTAN METABOLITE M-I plasma
Homo sapiens
population: unhealthy
age: Children
sex:
food status: Fed
1592.7 ng*h/mL
Clinical Trial
https://clinicaltrials.gov/ct2/show/NCT02451150
5 mg single, oral
dose: 5 mg
route of administration: oral
experiment type: single
co-administered:
AZILSARTAN METABOLITE M-I plasma
Homo sapiens
population: unhealthy
age: Children
sex:
food status: Fed
1986.5 ng*h/mL
Clinical Trial
https://clinicaltrials.gov/ct2/show/NCT02451150
5 mg single, oral
dose: 5 mg
route of administration: oral
experiment type: single
co-administered:
AZILSARTAN METABOLITE M-II plasma
Homo sapiens
population: unhealthy
age: Children
sex:
food status: Fed
3526 ng*h/mL
Clinical Trial
https://clinicaltrials.gov/ct2/show/NCT02451150
10 mg single, oral
dose: 10 mg
route of administration: oral
experiment type: single
co-administered:
AZILSARTAN METABOLITE M-II plasma
Homo sapiens
population: unhealthy
age: Children
sex:
food status: Fed
6350.3 ng*h/mL
Clinical Trial
https://clinicaltrials.gov/ct2/show/NCT02451150
5 mg single, oral
dose: 5 mg
route of administration: oral
experiment type: single
co-administered:
AZILSARTAN plasma
Homo sapiens
population: unhealthy
age: Children
sex:
food status: Fed
6871.7 ng*h/mL
Clinical Trial
https://clinicaltrials.gov/ct2/show/NCT02451150
10 mg single, oral
dose: 10 mg
route of administration: oral
experiment type: single
co-administered:
AZILSARTAN plasma
Homo sapiens
population: unhealthy
age: Children
sex:
food status: Fed
T1/2

T1/2

ValueDoseCo-administeredAnalytePopulation
12.1 h
EXPERIMENT
https://pubmed.ncbi.nlm.nih.gov/27514506/
80 mg single, oral
dose: 80 mg
route of administration: Oral
experiment type: SINGLE
co-administered: Chlorthalidone
Chlorthalidone
 AZILSARTAN plasma
Homo sapiens
population: HEALTHY
age: ADULT
sex: FEMALE / MALE
food status: FASTED
Funbound

Funbound

ValueDoseCo-administeredAnalytePopulation
1%
DRUG LABEL
https://www.accessdata.fda.gov/drugsatfda_docs/label/2020/200796s012lbl.pdf
80 mg 1 times / day unknown, oral
dose: 80 mg
route of administration: Oral
experiment type: UNKNOWN
co-administered:
AZILSARTAN plasma
Homo sapiens
population: UNKNOWN
age: UNKNOWN
sex: UNKNOWN
food status: UNKNOWN
Doses

Doses

DosePopulationAdverse events​
80 mg 1 times / day multiple, oral (max)
Recommended
Dose: 80 mg, 1 times / day
Route: oral
Route: multiple
Dose: 80 mg, 1 times / day
Sources:
https://pubmed.ncbi.nlm.nih.gov/25619410
Page: p.187
unhealthy, 50.4+/-10.2
n = 179
Health Status: unhealthy
Condition: Hypertension
Age Group: 50.4+/-10.2
Sex: M+F
Population Size: 179
Sources:
https://pubmed.ncbi.nlm.nih.gov/25619410
Page: p.187
Disc. AE: Dizziness, Fatigue...
AEs leading to
discontinuation/dose reduction:
Dizziness (3.35%)
Fatigue (2.79%)
Sources:
https://pubmed.ncbi.nlm.nih.gov/25619410
Page: p.187
320 mg 1 times / day multiple, oral
Overdose
Dose: 320 mg, 1 times / day
Route: oral
Route: multiple
Dose: 320 mg, 1 times / day
Sources:
https://www.accessdata.fda.gov/drugsatfda_docs/label/2011/200796s000lbl.pdf
Page: p.6
healthy
Health Status: healthy
Sources:
https://www.accessdata.fda.gov/drugsatfda_docs/label/2011/200796s000lbl.pdf
Page: p.6
Sources:
https://www.accessdata.fda.gov/drugsatfda_docs/label/2011/200796s000lbl.pdf
Page: p.6
80 mg 1 times / day multiple, oral (max)
Recommended
Dose: 80 mg, 1 times / day
Route: oral
Route: multiple
Dose: 80 mg, 1 times / day
Sources:
https://www.accessdata.fda.gov/drugsatfda_docs/label/2011/200796s000lbl.pdf
Page: p.4
unhealthy
n = 2146
Health Status: unhealthy
Condition: Hypertension
Population Size: 2146
Sources:
https://www.accessdata.fda.gov/drugsatfda_docs/label/2011/200796s000lbl.pdf
Page: p.4
Disc. AE: Hypotension orthostatic...
AEs leading to
discontinuation/dose reduction:
Hypotension orthostatic (0.4%)
Sources:
https://www.accessdata.fda.gov/drugsatfda_docs/label/2011/200796s000lbl.pdf
Page: p.4
AEs

AEs

AESignificanceDosePopulation
Fatigue 2.79%
Disc. AE
80 mg 1 times / day multiple, oral (max)
Recommended
Dose: 80 mg, 1 times / day
Route: oral
Route: multiple
Dose: 80 mg, 1 times / day
Sources:
https://pubmed.ncbi.nlm.nih.gov/25619410
Page: p.187
unhealthy, 50.4+/-10.2
n = 179
Health Status: unhealthy
Condition: Hypertension
Age Group: 50.4+/-10.2
Sex: M+F
Population Size: 179
Sources:
https://pubmed.ncbi.nlm.nih.gov/25619410
Page: p.187
Dizziness 3.35%
Disc. AE
80 mg 1 times / day multiple, oral (max)
Recommended
Dose: 80 mg, 1 times / day
Route: oral
Route: multiple
Dose: 80 mg, 1 times / day
Sources:
https://pubmed.ncbi.nlm.nih.gov/25619410
Page: p.187
unhealthy, 50.4+/-10.2
n = 179
Health Status: unhealthy
Condition: Hypertension
Age Group: 50.4+/-10.2
Sex: M+F
Population Size: 179
Sources:
https://pubmed.ncbi.nlm.nih.gov/25619410
Page: p.187
Hypotension orthostatic 0.4%
Disc. AE
80 mg 1 times / day multiple, oral (max)
Recommended
Dose: 80 mg, 1 times / day
Route: oral
Route: multiple
Dose: 80 mg, 1 times / day
Sources:
https://www.accessdata.fda.gov/drugsatfda_docs/label/2011/200796s000lbl.pdf
Page: p.4
unhealthy
n = 2146
Health Status: unhealthy
Condition: Hypertension
Population Size: 2146
Sources:
https://www.accessdata.fda.gov/drugsatfda_docs/label/2011/200796s000lbl.pdf
Page: p.4
Overview

Overview

CYP3A4CYP2C9CYP2D6hERG
inhibitor
1587

substrate
1737

inducer
781
inhibitor
1767

substrate
1037
inhibitor
1852

substrate
1217
inhibitor
1612

OverviewOther

Other InhibitorOther SubstrateOther Inducer
CYP1A2
1524

CYP2B6
810

CYP2C8
911

CYP2C19
1478

CYP2E1
882

CYP1A1
110

CYP2A6
707

P-gp
1461
CYP2C8
693

CYP1A1
349

CYP1A2
1054

CYP2A6
543

CYP2B6
664

CYP2C19
991

CYP2E1
667

CYP4A11
119

P-gp
1537
Drug as perpetrator​

Drug as perpetrator​

TargetModalityActivityMetaboliteClinical evidence
CYP1A1
218
 no [IC50 >100 uM]
CYP2A6
739
 no [IC50 >100 uM]
CYP2B6
1001
 no [IC50 >100 uM]
CYP2C19
1553
 no [IC50 >100 uM]
CYP2E1
970
 no [IC50 >100 uM]
CYP1A2
1692
 no [IC50 >100 uM]
no (co-administration study)
Comment: Human liver microsomes (Phenacetin O-deethylation), Maximum inhibition = 5.1%; Coadministration of Azilsartan medoxomil (80 mg QD for 6 days) did not significantly affect Caffeine (200 mg QD on Day 6, CYP1A2 substrate) AUC and Cmax.
Page: 9, 46-47, (ClinPharm) 15, 17-18, 58-59
CYP2C8
965
 no [IC50 >100 uM]
no (co-administration study)
Comment: Human liver microsomes (Paclitaxel 6a-hydroxylation), Maximum inhibition = 10.1%; Pioglitazone does not affect systemic exposure to Azilzartan, and systemic exposure to pioglitazone is not affected by Azilzartan.
Page: 9, 46-47, (ClinPharm) 15, 17-18, 77-78
CYP2C9
1819
 no [IC50 >100 uM]
no (co-administration study)
Comment: Human liver microsomes (Diclofenac 4'-hydroxylation), Inhibited CYP2C9 activities at 30 (14.4%) and 100 mcM (37.9%); Human CYP expressing microsomes derived from B-lymphoblastoid cells (tolbutamide hydroxylation); Coadministration of Azilsartan medoxomil (80 mg QD for 6 days) did not significantly affect Tolbutamide (500 mg QD on Day 6, CYP2C9 substrate) AUC and Cmax.; Azilzartan dose not affect the pharmacokinetics and pharmacodynamics of warfarin and is not expected to significantly affect systemic exposure to other CYP 2C9 substartes.
Page: 9, 46-47, (ClinPharm) 15, 17-18, 58-59, 66-68
CYP2D6
1891
 no [IC50 >100 uM]
no (co-administration study)
Comment: Human liver microsomes (Bufuralol 1'-hydroxylation), Maximum inhibition = 5.1%; Coadministration of Azilsartan medoxomil (80 mg QD for 6 days) did not significantly affect Dextromethorphan (30 mg QD on Day 6, CYP2D6 substrate) AUC and Cmax.
Page: 9, 46-47, (ClinPharm) 15, 17-18, 58-59
CYP3A4
1925
 no [IC50 >100 uM]
no (co-administration study)
Comment: Human liver microsomes (Midazolam 17-hydroxylation, Testosterone 6b-hydroxylation), Maximum inhibition = /<0%; Coadministration of Azilsartan medoxomil(80 mg QD for 6 days) did not significantly affect Midazolam (4 mg QD on Day 6, CYP3A4 substrate) AUC and Cmax.; Amlodipine does not affect systemic exposure to Azilzartan, and systemic exposure to amlodipine is not affected by Azilzartan.
Page: 9, 46-47, (ClinPharm) 15, 17-18, 58-59, 73-74
CYP3A4
1925
 unlikely
P-gp
1650
 unlikely
weak (co-administration study)
Comment: Caco-2 cells (After incubation at 37°C for 2 hours with Azilzartan (at 0, 20, 100, and 500 μmol/L), efflux ratios of digoxin were 6.4, 7.0, 6.6, and 7.23. These results show that Azilsartan had no inhibitory effect on P-gp-mediated efflux activity.; Coadministration of Azilsartan medoxomil (80 mg QD for 6 days) did not significantly affect Fexofenadine (60 mg QD on Day 6, P-gp substrate) AUC and Cmax.; Coadminitration of Azilzartan (80 mg QD for 10 days) increased Digoxin (200 mcg QD for 10 days) AUC0-tau by 2.87% and decreased Cmax by 5.71%.
Page: 35, (ClinPharm) 22-23, 58-59, 62-63
Drug as victim

Drug as victim

TargetModalityActivityMetaboliteClinical evidence
P-gp
1537
 inconclusive
CYP2C9
1037
 major
yes (co-administration study)
Comment: O-dealkylation to form Azilsartan M-II primarily by CYP2C9, Incubation of 14C-AZILSARTAN with microsomes from baculovirus-infected insect cellsexpressuing human CYP isoforms (elimination and formation (M-1 & M-II) rate); Human liver microsomes (16 donors); Clearance of Azilzartan (40 mg QD on Days 1 & 10) is reduced when co-administered with fluconazole (200 mg QD on Days 4-10), a CYP 2C9 inhibitor. This is evident from the ~ 40% increase in AUC, but only ~ 14% increase in Cmax. However, this is not of clinical significance given the flat D-R relationship for Azilzartan and the absence of serious adverse events.; Systemic exposure to glyburide (5 mg QD on DAy 8) is not affected by Azilzartan (40 mg QD for 8 days).
Page: 9, 45, (ClinPharm) 14, 64-65, 69-70
CYP1A1
349
 yes
CYP1A2
1054
 yes
CYP2A6
543
 yes
CYP2B6
664
 yes
CYP2C19
991
 yes
CYP2C8
693
 yes
CYP2D6
1217
 yes
CYP2E1
667
 yes
CYP4A11
119
 yes
CYP3A4
1737
 yes
yes (co-administration study)
Comment: Incubation of 14C-AZILSARTAN with microsomes from baculovirus-infected insect cellsexpressuing human CYP isoforms (elimination and formation (M-1 & M-II) rate); Human liver microsomes (16 donors); When co-administered with ketoconazole (400 mg QD on Days 4-10), Cmax of Azilzartan (40 mg QD on Day 1 & 10) decreased by ~ 30% and AUC by ~ 20%. However, the reason for this is not apparent.
Page: 9, 45, (ClinPharm) 14, 64-65
Tox targets

Tox targets

TargetModalityActivityMetaboliteClinical evidence
hERG
1647
Sourcing

Sourcing

Vendor/AggregatorIDURL
ChEBI
CHEBI:68850
https://www.ebi.ac.uk/chebi/searchId.do?chebiId=CHEBI:68850
ChemicalBook
CB21090899
https://www.chemicalbook.com/ChemicalProductProperty_EN_CB21090899
MolPort
MolPort-023-219-167
https://www.molport.com/shop/molecule-link/MolPort-023-219-167
MolPort
MolPort-023-220-072
https://www.molport.com/shop/molecule-link/MolPort-023-220-072
Selleck Chemicals
azilsartan-tak-536
http://www.selleckchem.com/products/azilsartan-tak-536.html
ZINC
ZINC000000598390
http://zinc15.docking.org/substances/ZINC000000598390
eMolecules
36762351
https://www.emolecules.com/cgi-bin/more?vid=36762351
eMolecules
36905408
https://www.emolecules.com/cgi-bin/more?vid=36905408
PubMed

PubMed

TitleDatePubMed
Azilsartan Medoxomil (Edarbi): The Eighth Angiotensin II Receptor Blocker.
2011 Oct
Differential pharmacology and benefit/risk of azilsartan compared to other sartans.
2012
A systematic comparison of the properties of clinically used angiotensin II type 1 receptor antagonists.
2013 Apr
Azilsartan, aliskiren, and combination antihypertensives utilizing renin-angiotensin-aldosterone system antagonists.
2014 Sep-Oct
Patents

Patents

07157584
9
07572920
9
07875637
9
20050187269
8
20060281795
8
20090270464
8

Sample Use Guides

In Vivo Use Guide
The recommended dose in adults is 80 mg taken orally once daily. Consider a starting dose of 40 mg for patients who are treated with high doses of diuretics.
Route of Administration: Oral
In Vitro Use Guide
Unknown
Substance Class Chemical
Created
by admin
on Sat Dec 16 08:31:48 GMT 2023
Edited
by admin
on Sat Dec 16 08:31:48 GMT 2023
Record UNII
6RDT9MR9SQ
Record Status Validated (UNII)
Record Version
  • Download
Name Type Language
AZILSARTAN TRIMETHYLETHANOLAMINE
Common Name English
ETHANAMINIUM, 2-HYDROXY-N,N,N-TRIMETHYL-, 1-((2'-(2,5-DIHYDRO-5-OXO-1,2,4-OXADIAZOL-3-YL)(1,1'-BIPHENYL)-4-YL)METHYL)-2-ETHOXY-1H-BENZIMIDAZOLE-7-CARBOXYLATE (1:1)
Systematic Name English
Code System Code Type Description
CAS
1309776-70-2
Created by admin on Sat Dec 16 08:31:48 GMT 2023 , Edited by admin on Sat Dec 16 08:31:48 GMT 2023
PRIMARY
PUBCHEM
135565150
Created by admin on Sat Dec 16 08:31:48 GMT 2023 , Edited by admin on Sat Dec 16 08:31:48 GMT 2023
PRIMARY
FDA UNII
6RDT9MR9SQ
Created by admin on Sat Dec 16 08:31:48 GMT 2023 , Edited by admin on Sat Dec 16 08:31:48 GMT 2023
PRIMARY
Related Record Type Details
Structure of AZILSARTAN
PARENT -> SALT/SOLVATE
Related Record Type Details
Structure of AZILSARTAN
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