Details
Stereochemistry | ABSOLUTE |
Molecular Formula | C19H24N2O3 |
Molecular Weight | 328.4055 |
Optical Activity | UNSPECIFIED |
Defined Stereocenters | 2 / 2 |
E/Z Centers | 0 |
Charge | 0 |
SHOW SMILES / InChI
SMILES
C[C@H](CCC1=CC=CC=C1)NC[C@H](O)C2=CC=C(O)C(=C2)C(N)=O
InChI
InChIKey=SGUAFYQXFOLMHL-ACJLOTCBSA-N
InChI=1S/C19H24N2O3/c1-13(7-8-14-5-3-2-4-6-14)21-12-18(23)15-9-10-17(22)16(11-15)19(20)24/h2-6,9-11,13,18,21-23H,7-8,12H2,1H3,(H2,20,24)/t13-,18+/m1/s1
Dilevalol, the RR-stereoisomer of labetalol, is a non-cardioselective β-adrenoceptor antagonist with substantial partial β2-agonist and negligible α1-blocking activity. Reduction in blood pressure during dilevalol administration is associated with peripheral vasodilatation, and heart rate remains essentially unchanged. Following oral administration, dilevalol is completely absorbed. Once-daily administration is possible, due to a long elimination half-life. In vitro and in vivo animal studies and results obtained in humans reveal that dilevalol is a nonselective blocker of β1- and β2-adrenoceptors, with a similar potency to propranolol, but has negligible antagonistic activity at α1-receptors. Dilevalol, the R,R′ stereoisomer, makes up 25% of racemic labetalol, the drug, approved by FDA for the treatment of hypertension. The relaxing potency of dilevalol was approximately 4.7 times more potent than that of labetalol. Dilevalol markedly reduced the diastolic blood pressure with only a slight increase of heart rate In pithed rats, while isoproterenol and pindolol caused moderate to marked positive chronotropic effects in proportion to their hypotensive effects. These results suggest that dilevalol has more potent ISA than labetalol. In contrast to labetalol, dilevalol possesses little, if any, alpha-adrenergic blocking activity. The compound is 3 to 10 times less potent than labetalol at α1-adrenergic receptors under a variety of experimental conditions. Moreover, it is 300- to 1000-fold less potent at alpha1-adrenergic receptors compared with β1-adrenergic receptors. The pA2 values for dilevalol as an α antagonist range from 5.9 to 6.4. Because maximal plasma concentrations of the drug after administration of a 400-mg dose are approximately 0.5 pmol, it is doubtful that alpha blockade is involved in the antihypertensive response to dilevalol in humans.
Approval Year
Targets
Primary Target | Pharmacology | Condition | Potency |
---|---|---|---|
8.2 null [pKi] | |||
3.77 nM [Ki] |
Conditions
Condition | Modality | Targets | Highest Phase | Product |
---|---|---|---|---|
Primary | Trandate Approved UseTrandate Tablets are indicated in the management of hypertension. Trandate Tablets may be used alone
or in combination with other antihypertensive agents, especially thiazide and loop diuretics. Launch Date1984 |
Sample Use Guides
In Vivo Use Guide
Sources: https://www.ncbi.nlm.nih.gov/pubmed/2184002
Once-daily oral administration of 200 to 400mg, titrated up to 800mg if necessary, is the recommended dosage of dilevalol in adult patients with mild to moderate essential hypertension.
Route of Administration:
Oral
In Vitro Use Guide
Sources: https://www.ncbi.nlm.nih.gov/pubmed/8968966
Curator's Comment: Incubation of L6 cells for 24 hours in the presence of isoproterenol and B antagonists with ISA resulted in a concentration-dependent down-regulation of Beta2ARs. EC50 values characterized drug-induced receptor loss.
Dilevalol caused a concentration-dependent increase in cAMP
accumulation which maximally was 2.1-fold over mean basal (6.75 pmol/10(6) cells). Dilevalol down-regulated (EC50 35.9 nM) β2-adrenoceptor in rat muscle L6 cells.
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NCI_THESAURUS |
C29707
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C72900
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P6629XE33T
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DTXSID2043828
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5180
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CHEMBL27193
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m6647
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SUB07145MIG
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C65390
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134044
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100000082609
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ACTIVE MOIETY
SALT/SOLVATE (PARENT)