Vardenafil

Identification

Summary

Vardenafil is a phosphodiesterase 5 inhibitor used to treat erectile dysfunction.

Brand Names

Levitra, Staxyn

Generic Name

Vardenafil

DrugBank Accession Number

DB00862

Background

Vardenafil is a selective inhibitor of cyclic guanosine monophosphate (cGMP)-specific phosphodiesterase type 5 (PDE5) and an oral therapy for the treatment of erectile dysfunction.^5,6 During sexual stimulation, nitric oxide (NO) is released from nerve endings and endothelial cells in the corpus cavernosum, activating the enzyme guanylate cyclase and increasing the synthesis of cGMP in the smooth muscle cells of the corpus cavernosum. PDE5 inhibitors, such as vardenafil, inhibit the degradation of cGMP and allow increased blood flow into the penis, resulting in an erection.^1,5,6. Compared to sildenafil and tadalafil, vardenafil is a more potent inhibitor of PDE5; however, its selectivity for other PDE isoforms is lower than the one detected for tadalafil.⁴

The FDA approved the use of vardenafil for the treatment of erectile dysfunction in 2003. Although other PDE5 inhibitors such as sildenafil and tadalafil have been associated with rare cases of acute liver injury, the use of vardenafil has not been linked to hepatotoxic effects.³ The use of vardenafil as a monotherapy for the treatment of pulmonary arterial hypertension has also been evaluated.²

Type

Small Molecule

Groups

Approved

Structure

3D

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MOLSDF3D-SDFPDBSMILESInChI

Similar Structures

Structure for Vardenafil (DB00862)

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Weight

Average: 488.603
Monoisotopic: 488.220574232

Chemical Formula

C₂₃H₃₂N₆O₄S

Synonyms

• Vardénafil
• Vardenafil
• Vardenafilo
• Vardenafilum

External IDs

• BAY 389456
• BAY-389456
• BAY38-9456
• DE 19750085 1997
• WO 99/24433 1999

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Pharmacology

Indication

Vardenafil is indicated for the treatment of erectile dysfunction.^5,6,7

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Associated Conditions

Indication Type	Indication	Combined Product Details	Approval Level	Age Group	Patient Characteristics	Dose Form
Management of	Erectile dysfunction		••••••••••••			••••••• ••••••• •••••• ••••••••••••••

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Contraindications & Blackbox Warnings

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Pharmacodynamics

Vardenafil is a potent and selective inhibitor of cyclic guanosine monophosphate (cGMP)-specific phosphodiesterase type 5 (PDE5), an enzyme responsible for the degradation of cGMP in the corpus cavernosum. The presence of cGMP in the corpus cavernosum leads to smooth muscle relaxation, an increased inflow of blood and an erection. Therefore, in patients with erectile dysfunction given vardenafil, normal sexual stimulation will increase cGMP levels in the corpus cavernosum. Without sexual stimulation and no cGMP production, vardenafil should not cause an erection.^5,6

Vardenafil should not be used in men for whom sexual activity is not recommended due to their underlying cardiovascular status. There is also a risk of developing prolonged erections that last longer than 4 hours, as well as priapism. In the event of a sudden loss of vision in one or both eyes, patients should stop using vardenafil. Patients taking PDE5 inhibitors, such as vardenafil, may also develop sudden hearing loss and experience a prolonged QT interval.^5,6

Mechanism of action

Vardenafil inhibits cyclic guanosine monophosphate (GMP) specific phosphodiesterase type 5 (PDE5), which is responsible for the degradation of cyclic GMP in the corpus cavernosum located around the penis. Penile erection during sexual stimulation is caused by increased penile blood flow resulting from the relaxation of penile arteries and corpus cavernosal smooth muscle. This response is mediated by the release of nitric oxide (NO) from nerve terminals and endothelial cells, which stimulates the synthesis of cyclic GMP in smooth muscle cells. Cyclic GMP causes smooth muscle relaxation and increased blood flow into the corpus cavernosum. The tissue concentration of cyclic GMP is regulated by both the rates of synthesis and degradation via phosphodiesterases (PDEs), and the most abundant PDE in the human corpus cavernosum is PDE5. Therefore, the inhibition of PDE5 by vardenafil enhances erectile function by increasing the amount of cyclic GMP.⁵

Target	Actions	Organism
AcGMP-specific 3',5'-cyclic phosphodiesterase	inhibitor	Humans
URetinal rod rhodopsin-sensitive cGMP 3',5'-cyclic phosphodiesterase subunit gamma	inhibitor allosteric modulator	Humans
URetinal cone rhodopsin-sensitive cGMP 3',5'-cyclic phosphodiesterase subunit gamma	inhibitor allosteric modulator	Humans

Absorption

Over the recommended dose range, vardenafil has a dose-proportional pharmacokinetics profile. In healthy male volunteers given a single oral dose of 20 mg of vardenafil, maximum plasma concentrations were reached between 30 minutes and 2 hours (median 60 minutes) after oral dosing in the fasted state, and 0.00018% of the dose was detected in semen 1.5 hours after dosing. Vardenafil has a bioavailability of approximately 15%.⁵ High-fat meals cause a C_max reduction of 18%-50%; however, no changes were detected in AUC or T_max.^5,6

Volume of distribution

Vardenafil has a steady-state volume of distribution of 208 L.⁵

Protein binding

Approximately 95% of vardenafil and its major circulating metabolite is bound to plasma proteins. Their protein binding is reversible and independent of total drug concentrations.⁵

Metabolism

Vardenafil is mainly metabolized by CYP3A4 in the liver, although CYP3A5 and CYP2C isoforms also contribute to its metabolism. The major circulating metabolite, M1 (N-desethylvardenafil), results from desethylation at the piperazine moiety of vardenafil, and has a plasma concentration of approximately 26% of that of the parent compound. M1 has a phosphodiesterase selectivity profile similar to that of vardenafil and an in vitro inhibitory potency for PDE5 28% of that of vardenafil.⁵

Hover over products below to view reaction partners

• Vardenafil
  • N-desethylvardenafil

Route of elimination

Vardenafil is excreted as metabolites mainly through feces and urine. Approximately 91-95% of administered oral dose is found in feces, while 2-6% of administered oral dose is found in urine.⁵

Half-life

Vardenafil and its primary metabolite (M1) have a terminal half-life of 4-5 hours.⁵

Clearance

Vardenafil has a total body clearance of 56 L/h.⁵

Adverse Effects

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Toxicity

Healthy male volunteers given a single dose of 120 mg of vardenafil experienced reversible back pain, myalgia and abnormal vision. Patients given vardenafil once daily over 4 weeks in single doses up to 80 mg and multiple doses up to 40 mg did not present serious adverse side effects. Cases of severe back pain were observed when 40 mg of vardenafil was administered twice daily; however patients did not present muscle or neurological toxicity. In cases of overdose, standard supportive measures should be taken as required. Renal dialysis is not expected to accelerate clearance as vardenafil is highly bound to plasma proteins and not significantly eliminated in the urine.^5,6

No carcinogenic effects were detected in rats and mice given vardenafil daily for 24 months. Vardenafil was not mutagenic or clastogenic, and did not have an effect in fertility in male and female rats given up to 100 mg/kg/day for 28 days prior to mating in males, and for 14 days prior to mating and through day 7 of gestation in females.^5,6

Pathways

Not Available

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Interactions

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This information should not be interpreted without the help of a healthcare provider. If you believe you are experiencing an interaction, contact a healthcare provider immediately. The absence of an interaction does not necessarily mean no interactions exist.

• Approved
• Vet approved
• Nutraceutical
• Illicit
• Withdrawn
• Investigational
• Experimental
• All Drugs

Drug	Interaction
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Abaloparatide	The risk or severity of hypotension can be increased when Vardenafil is combined with Abaloparatide.
Abametapir	The serum concentration of Vardenafil can be increased when it is combined with Abametapir.
Abatacept	The metabolism of Vardenafil can be increased when combined with Abatacept.
Abemaciclib	The serum concentration of Abemaciclib can be increased when it is combined with Vardenafil.
Abrocitinib	The serum concentration of Vardenafil can be increased when it is combined with Abrocitinib.

Food Interactions

• Avoid grapefruit products. Vardenafil is metabolized by CYP3A4, and grapefruit products are CYP3A4 inhibitors; therefore, coadministration may increase serum levels of vardenafil and result in increased hypotension. .
• Take with or without food. High-fat meals reduce the Cmax of vardenafil; however, there are no changes in AUC or Tmax.

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Product Ingredients

Ingredient	UNII	CAS	InChI Key
Vardenafil hydrochloride	5M8S2CU0TS	330808-88-3	FBCDRHDULQYRTB-UHFFFAOYSA-N

Product Images

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International/Other Brands

Levitra (Bayer) / Staxyn (GlaxoSmithKline)

Brand Name Prescription Products

Name	Dosage	Strength	Route	Labeller	Marketing Start	Marketing End	Region	Image
Levitra	Tablet, orally disintegrating	10 mg	Oral	Bayer Ag	2016-09-08	Not applicable
Levitra	Tablet	5 mg	Oral	Bayer	2004-03-17	2020-11-16
Levitra	Tablet, film coated	20 mg/1	Oral	Schering Plough	2008-05-15	2013-07-01
Levitra	Tablet, film coated	20 mg	Oral	Bayer Ag	2016-09-08	Not applicable
Levitra	Tablet, film coated	20 mg/1	Oral	GlaxoSmithKline LLC	2003-08-25	2021-10-31

Generic Prescription Products

Name	Dosage	Strength	Route	Labeller	Marketing Start	Marketing End	Region	Image
Ag-vardenafil	Tablet	20 mg	Oral	Angita Pharma Inc.	Not applicable	Not applicable
Ag-vardenafil	Tablet	10 mg	Oral	Angita Pharma Inc.	Not applicable	Not applicable
Ag-vardenafil	Tablet	5 mg	Oral	Angita Pharma Inc.	Not applicable	Not applicable
Apo-vardenafil	Tablet	5 mg	Oral	Apotex Corporation	2018-12-21	Not applicable
Apo-vardenafil	Tablet	20 mg	Oral	Apotex Corporation	2018-12-21	Not applicable

Categories

ATC Codes

G04BE09 — Vardenafil

• G04BE — Drugs used in erectile dysfunction
• G04B — UROLOGICALS
• G04 — UROLOGICALS
• G — GENITO URINARY SYSTEM AND SEX HORMONES

Drug Categories

• Cardiovascular Agents
• Cytochrome P-450 CYP2C19 Inhibitors
• Cytochrome P-450 CYP2C19 Inhibitors (weak)
• Cytochrome P-450 CYP2C8 Inhibitors
• Cytochrome P-450 CYP2C8 Inhibitors (weak)
• Cytochrome P-450 CYP2C9 Inhibitors
• Cytochrome P-450 CYP2C9 Inhibitors (weak)
• Cytochrome P-450 CYP2C9 Substrates
• Cytochrome P-450 CYP2D6 Inhibitors
• Cytochrome P-450 CYP2D6 Inhibitors (weak)
• Cytochrome P-450 CYP3A Inhibitors
• Cytochrome P-450 CYP3A Substrates
• Cytochrome P-450 CYP3A4 Inhibitors
• Cytochrome P-450 CYP3A4 Inhibitors (weak)
• Cytochrome P-450 CYP3A4 Substrates
• Cytochrome P-450 CYP3A5 Substrates
• Cytochrome P-450 Enzyme Inhibitors
• Cytochrome P-450 Substrates
• Drugs Used in Erectile Dysfunction
• Enzyme Inhibitors
• Genito Urinary System and Sex Hormones
• Genitourinary Agents
• Imidazoles
• P-glycoprotein inhibitors
• P-glycoprotein substrates
• Phosphodiesterase 5 Inhibitors
• Phosphodiesterase Inhibitors
• Piperazines
• Potential QTc-Prolonging Agents
• QTc Prolonging Agents
• Urological Agents
• Urologicals
• Vasodilating Agents

Chemical TaxonomyProvided by Classyfire

Description

This compound belongs to the class of organic compounds known as benzenesulfonamides. These are organic compounds containing a sulfonamide group that is S-linked to a benzene ring.

Kingdom

Organic compounds

Super Class

Benzenoids

Class

Benzene and substituted derivatives

Sub Class

Benzenesulfonamides

Direct Parent

Benzenesulfonamides

Alternative Parents

Benzenesulfonyl compounds / Phenoxy compounds / Phenol ethers / N-alkylpiperazines / Alkyl aryl ethers / Organosulfonamides / N-substituted imidazoles / 1,2,4-triazines / Sulfonyls / Heteroaromatic compounds / Trialkylamines / Azacyclic compounds / Organopnictogen compounds / Organic oxides / Hydrocarbon derivatives

show 5 more

Substituents

1,2,4-triazine / 1,4-diazinane / Alkyl aryl ether / Amine / Aromatic heteropolycyclic compound / Azacycle / Azole / Benzenesulfonamide / Benzenesulfonyl group / Ether / Heteroaromatic compound / Hydrocarbon derivative / Imidazole / N-alkylpiperazine / N-substituted imidazole / Organic nitrogen compound / Organic oxide / Organic oxygen compound / Organic sulfonic acid or derivatives / Organoheterocyclic compound / Organonitrogen compound / Organooxygen compound / Organopnictogen compound / Organosulfonic acid amide / Organosulfonic acid or derivatives / Organosulfur compound / Phenol ether / Phenoxy compound / Piperazine / Sulfonyl / Tertiary aliphatic amine / Tertiary amine / Triazine

show 23 more

Molecular Framework

Aromatic heteropolycyclic compounds

External Descriptors

N-alkylpiperazine, imidazotriazine, N-sulfonylpiperazine (CHEBI:46295)

Affected organisms

• Humans and other mammals

Chemical Identifiers

UNII

UCE6F4125H

CAS number

224785-90-4

InChI Key

SECKRCOLJRRGGV-UHFFFAOYSA-N

InChI

InChI=1S/C23H32N6O4S/c1-5-8-20-24-16(4)21-23(30)25-22(26-29(20)21)18-15-17(9-10-19(18)33-7-3)34(31,32)28-13-11-27(6-2)12-14-28/h9-10,15H,5-8,11-14H2,1-4H3,(H,25,26,30)

IUPAC Name

2-{2-ethoxy-5-[(4-ethylpiperazin-1-yl)sulfonyl]phenyl}-5-methyl-7-propyl-1H,4H-imidazo[4,3-f][1,2,4]triazin-4-one

SMILES

CCCC1=NC(C)=C2N1NC(=NC2=O)C1=C(OCC)C=CC(=C1)S(=O)(=O)N1CCN(CC)CC1

References

Synthesis Reference

Yogesh S. Deshpande, Sandra Brueck, Julia Schulze Nahrup, Birgit Schnitter, Ganesh Gat, Javed Hussain, "PROCESS FOR THE PREPARATION OF A MEDICAMENT COMPRISING VARDENAFIL HYDROCHLORIDE TRIHYDRATE." U.S. Patent US20100159003, issued June 24, 2010.

US20100159003

General References

1. Forstermann U, Sessa WC: Nitric oxide synthases: regulation and function. Eur Heart J. 2012 Apr;33(7):829-37, 837a-837d. doi: 10.1093/eurheartj/ehr304. Epub 2011 Sep 1. [Article]
2. Jing ZC, Yu ZX, Shen JY, Wu BX, Xu KF, Zhu XY, Pan L, Zhang ZL, Liu XQ, Zhang YS, Jiang X, Galie N: Vardenafil in pulmonary arterial hypertension: a randomized, double-blind, placebo-controlled study. Am J Respir Crit Care Med. 2011 Jun 15;183(12):1723-9. doi: 10.1164/rccm.201101-0093OC. Epub 2011 Mar 11. [Article]
3. Authors unspecified: Vardenafil. . [Article]
4. Rosen RC, Kostis JB: Overview of phosphodiesterase 5 inhibition in erectile dysfunction. Am J Cardiol. 2003 Nov 6;92(9A):9M-18M. doi: 10.1016/s0002-9149(03)00824-5. [Article]
5. FDA Approved Drug Products: LEVITRA (vardenafil hydrochloride) tablets for oral use (March 2023) [Link]
6. FDA Approved Drug Products: STAXYN (vardenafil hydrochloride) orally disintegrating tablets (March 2023) [Link]
7. Health Canada Approved Drug Products: STAXYN (vardenafil) orally disintegrating tablets (February 2020) [Link]

External Links

Human Metabolome Database

HMDB0015000

KEGG Drug

D08668

PubChem Compound

110634

PubChem Substance

46506777

ChemSpider

99300

BindingDB

14776

RxNav

306674

ChEBI

46295

ChEMBL

CHEMBL1520

ZINC

ZINC000018324776

Therapeutic Targets Database

DAP000414

PharmGKB

PA10229

PDBe Ligand

VDN

RxList

RxList Drug Page

Drugs.com

Drugs.com Drug Page

PDRhealth

PDRhealth Drug Page

Wikipedia

Vardenafil

PDB Entries

1uho / 1xot / 1xp0 / 3b2r / 7jsn

Clinical Trials

Clinical Trials Learn More" title="About Clinical Trials" id="clinical-trials-info" class="drug-info-popup" href="javascript:void(0);">

Phase	Status	Purpose	Conditions	Count
4	Completed	Treatment	Acquired Immune Deficiency Syndrome (AIDS)	1
4	Completed	Treatment	Endothelial Dysfunction / Erectile Dysfunction / Hypertension Arterial	1
4	Completed	Treatment	Erectile Dysfunction	15
4	Completed	Treatment	Erectile Dysfunction / Sexual Dysfunctions	1
4	Completed	Treatment	Erectile Dysfunction / Spinal Cord Injuries	1

Pharmacoeconomics

Manufacturers

• Bayer healthcare pharmaceuticals inc

Packagers

• A-S Medication Solutions LLC
• Bayer Healthcare
• Bryant Ranch Prepack
• Kaiser Foundation Hospital
• Lake Erie Medical and Surgical Supply
• Murfreesboro Pharmaceutical Nursing Supply
• Physicians Total Care Inc.
• Prepak Systems Inc.
• Redpharm Drug
• Schering Corp.
• Va Cmop Dallas

Dosage Forms

Form	Route	Strength
Tablet, film coated	Oral	20 MG
Tablet	Oral	20 mg
Tablet	Oral	5 mg
Tablet, coated	Oral
Tablet, film coated	Oral	10 mg/1
Tablet, film coated	Oral	2.5 mg/1
Tablet, film coated	Oral	20 mg/1
Tablet, film coated	Oral	5 mg/1
Tablet, soluble	Oral
Tablet, orally disintegrating	Oral	10.0 mg
Tablet, film coated	Oral	11.852 mg
Tablet, film coated	Oral	23.705 mg
Tablet, film coated	Oral	5.926 mg
Tablet, orally disintegrating	Oral	10 mg/1
Tablet, orally disintegrating	Oral	11.85 mg/1
Tablet	Oral	11.85 mg/1
Tablet, film coated	Oral
Tablet, orally disintegrating	Oral	10 MG
Tablet	Oral	10 mg/1
Tablet	Oral	2.5 mg/1
Tablet	Oral	20 mg/1
Tablet	Oral	5 mg/1
Tablet, film coated	Oral	10 MG
Tablet, film coated	Oral	5 MG
Tablet, orally disintegrating	Oral
Tablet, coated	Oral	10 MG
Tablet	Oral	10 mg
Tablet, coated	Oral	20 mg
Tablet, coated	Oral	5 mg

Prices

Unit description	Cost	Unit
Levitra 10 mg tablet	19.04USD	tablet
Levitra 20 mg tablet	19.04USD	tablet
Levitra 5 mg tablet	19.04USD	tablet
Levitra 2.5 mg tablet	18.66USD	tablet

DrugBank does not sell nor buy drugs. Pricing information is supplied for informational purposes only.

Patents

Patent Number	Pediatric Extension	Approved	Expires (estimated)	Region
CA2309332	No	2002-12-03	2018-10-31
US6362178	No	2002-03-26	2018-10-31
US7696206	No	2010-04-13	2018-10-31
US8273876	No	2012-09-25	2027-07-23
US8841446	No	2014-09-23	2023-07-03
US8613950	No	2013-12-24	2028-12-23

Properties

State

Solid

Experimental Properties

Property	Value	Source
melting point (°C)	192 °C	Patent US 9,845,328 B2
water solubility	0.11 mg/mL (HCl salt)	FDA label
logP	1.4	Not Available

Predicted Properties

Property	Value	Source
Water Solubility	0.325 mg/mL	ALOGPS
logP	2.18	ALOGPS
logP	1.43	Chemaxon
logS	-3.2	ALOGPS
pKa (Strongest Acidic)	11.75	Chemaxon
pKa (Strongest Basic)	6.21	Chemaxon
Physiological Charge	0	Chemaxon
Hydrogen Acceptor Count	8	Chemaxon
Hydrogen Donor Count	1	Chemaxon
Polar Surface Area	109.13 Å2	Chemaxon
Rotatable Bond Count	7	Chemaxon
Refractivity	142.71 m3·mol-1	Chemaxon
Polarizability	53.22 Å3	Chemaxon
Number of Rings	4	Chemaxon
Bioavailability	1	Chemaxon
Rule of Five	Yes	Chemaxon
Ghose Filter	No	Chemaxon
Veber's Rule	No	Chemaxon
MDDR-like Rule	Yes	Chemaxon

Predicted ADMET Features

Property	Value	Probability
Human Intestinal Absorption	+	1.0
Blood Brain Barrier	+	0.6682
Caco-2 permeable	+	0.5502
P-glycoprotein substrate	Substrate	0.7415
P-glycoprotein inhibitor I	Inhibitor	0.6976
P-glycoprotein inhibitor II	Inhibitor	0.8552
Renal organic cation transporter	Non-inhibitor	0.6975
CYP450 2C9 substrate	Non-substrate	0.6386
CYP450 2D6 substrate	Substrate	0.7909
CYP450 3A4 substrate	Substrate	0.697
CYP450 1A2 substrate	Non-inhibitor	0.8215
CYP450 2C9 inhibitor	Inhibitor	0.7426
CYP450 2D6 inhibitor	Non-inhibitor	0.8464
CYP450 2C19 inhibitor	Non-inhibitor	0.7472
CYP450 3A4 inhibitor	Inhibitor	0.8857
CYP450 inhibitory promiscuity	High CYP Inhibitory Promiscuity	0.7205
Ames test	Non AMES toxic	0.5748
Carcinogenicity	Non-carcinogens	0.6141
Biodegradation	Not ready biodegradable	0.8875
Rat acute toxicity	2.6208 LD50, mol/kg	Not applicable
hERG inhibition (predictor I)	Weak inhibitor	0.8367
hERG inhibition (predictor II)	Inhibitor	0.7696

ADMET data is predicted using admetSAR, a free tool for evaluating chemical ADMET properties. (23092397)

Spectra

Mass Spec (NIST)

Not Available

Spectra

Spectrum	Spectrum Type	Splash Key
Predicted GC-MS Spectrum - GC-MS	Predicted GC-MS	splash10-03di-9304600000-78a6e2bde8e38b367f38
LC-MS/MS Spectrum - LC-ESI-QFT , negative	LC-MS/MS	splash10-000i-0040900000-a78a646244f2fb1f6276
MS/MS Spectrum - , positive	LC-MS/MS	splash10-000f-0011900000-88f62b9a8f7aec917a41
MS/MS Spectrum - , positive	LC-MS/MS	splash10-0002-0092000000-cf98ecae287c01370dbc
Predicted MS/MS Spectrum - 10V, Positive (Annotated)	Predicted LC-MS/MS	splash10-000i-0002900000-0b3a3d3b8a696b6c1c84
Predicted MS/MS Spectrum - 10V, Negative (Annotated)	Predicted LC-MS/MS	splash10-052r-0000900000-e57c1c9091e26873edc4
Predicted MS/MS Spectrum - 20V, Positive (Annotated)	Predicted LC-MS/MS	splash10-000i-0001900000-9f332b16d2a563673357
Predicted MS/MS Spectrum - 20V, Negative (Annotated)	Predicted LC-MS/MS	splash10-05fr-0901600000-4231ac001d7a0b4e7bc1
Predicted MS/MS Spectrum - 40V, Positive (Annotated)	Predicted LC-MS/MS	splash10-02mi-2501900000-2c2edea1cbb4c1a058e2
Predicted MS/MS Spectrum - 40V, Negative (Annotated)	Predicted LC-MS/MS	splash10-014i-0101900000-94265f5da0fe5589caf3
Predicted 1H NMR Spectrum	1D NMR	Not Applicable
Predicted 13C NMR Spectrum	1D NMR	Not Applicable

Chromatographic Properties

Collision Cross Sections (CCS)

Adduct	CCS Value (Å2)	Source type	Source
[M-H]-	240.2311048	predicted	DarkChem Lite v0.1.0
[M-H]-	213.71483	predicted	DeepCCS 1.0 (2019)
[M+H]+	240.7878048	predicted	DarkChem Lite v0.1.0
[M+H]+	216.1104	predicted	DeepCCS 1.0 (2019)
[M+Na]+	239.8316048	predicted	DarkChem Lite v0.1.0
[M+Na]+	222.02293	predicted	DeepCCS 1.0 (2019)

Targets

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insights and accelerate drug research.

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Details1. cGMP-specific 3',5'-cyclic phosphodiesterase

Kind

Protein

Organism

Humans

Pharmacological action

Yes

Actions

Inhibitor

General Function

Metal ion binding

Specific Function

Plays a role in signal transduction by regulating the intracellular concentration of cyclic nucleotides. This phosphodiesterase catalyzes the specific hydrolysis of cGMP to 5'-GMP (PubMed:9714779, ...

Gene Name

PDE5A

Uniprot ID

O76074

Uniprot Name

cGMP-specific 3',5'-cyclic phosphodiesterase

Molecular Weight

99984.14 Da

References

1. Blount MA, Zoraghi R, Ke H, Bessay EP, Corbin JD, Francis SH: A 46-amino acid segment in phosphodiesterase-5 GAF-B domain provides for high vardenafil potency over sildenafil and tadalafil and is involved in phosphodiesterase-5 dimerization. Mol Pharmacol. 2006 Nov;70(5):1822-31. Epub 2006 Aug 22. [Article]
2. Carrier S: Pharmacology of phosphodiesterase 5 inhibitors. Can J Urol. 2003 Feb;10 Suppl 1:12-6. [Article]
3. Kim NN, Huang YH, Goldstein I, Bischoff E, Traish AM: Inhibition of cyclic GMP hydrolysis in human corpus cavernosum smooth muscle cells by vardenafil, a novel, selective phosphodiesterase type 5 inhibitor. Life Sci. 2001 Sep 28;69(19):2249-56. [Article]
4. Saenz de Tejada I, Angulo J, Cuevas P, Fernandez A, Moncada I, Allona A, Lledo E, Korschen HG, Niewohner U, Haning H, Pages E, Bischoff E: The phosphodiesterase inhibitory selectivity and the in vitro and in vivo potency of the new PDE5 inhibitor vardenafil. Int J Impot Res. 2001 Oct;13(5):282-90. [Article]
5. Scheen AJ: [Medication of the month. Vardenafil (Levitra)]. Rev Med Liege. 2003 Sep;58(9):576-9. [Article]
6. Sung BJ, Hwang KY, Jeon YH, Lee JI, Heo YS, Kim JH, Moon J, Yoon JM, Hyun YL, Kim E, Eum SJ, Park SY, Lee JO, Lee TG, Ro S, Cho JM: Structure of the catalytic domain of human phosphodiesterase 5 with bound drug molecules. Nature. 2003 Sep 4;425(6953):98-102. [Article]
7. Wang H, Ye M, Robinson H, Francis SH, Ke H: Conformational variations of both phosphodiesterase-5 and inhibitors provide the structural basis for the physiological effects of vardenafil and sildenafil. Mol Pharmacol. 2008 Jan;73(1):104-10. Epub 2007 Oct 24. [Article]
8. Zoraghi R, Francis SH, Corbin JD: Critical amino acids in phosphodiesterase-5 catalytic site that provide for high-affinity interaction with cyclic guanosine monophosphate and inhibitors. Biochemistry. 2007 Nov 27;46(47):13554-63. Epub 2007 Nov 3. [Article]
9. FDA Approved Drug Products: LEVITRA (vardenafil hydrochloride) tablets for oral use (March 2023) [Link]
10. FDA Approved Drug Products: STAXYN (vardenafil hydrochloride) orally disintegrating tablets (March 2023) [Link]

Details2. Retinal rod rhodopsin-sensitive cGMP 3',5'-cyclic phosphodiesterase subunit gamma

Kind

Protein

Organism

Humans

Pharmacological action

Unknown

Actions

Inhibitor

Allosteric modulator

General Function

Enzyme inhibitor activity

Specific Function

Participates in processes of transmission and amplification of the visual signal. cGMP-PDEs are the effector molecules in G-protein-mediated phototransduction in vertebrate rods and cones.

Gene Name

PDE6G

Uniprot ID

P18545

Uniprot Name

Retinal rod rhodopsin-sensitive cGMP 3',5'-cyclic phosphodiesterase subunit gamma

Molecular Weight

9643.09 Da

References

1. Zhang XJ, Cahill KB, Elfenbein A, Arshavsky VY, Cote RH: Direct allosteric regulation between the GAF domain and catalytic domain of photoreceptor phosphodiesterase PDE6. J Biol Chem. 2008 Oct 31;283(44):29699-705. doi: 10.1074/jbc.M803948200. Epub 2008 Sep 8. [Article]
2. FDA Approved Drug Products: LEVITRA (vardenafil hydrochloride) tablets for oral use (March 2023) [Link]
3. FDA Approved Drug Products: STAXYN (vardenafil hydrochloride) orally disintegrating tablets (March 2023) [Link]

Details3. Retinal cone rhodopsin-sensitive cGMP 3',5'-cyclic phosphodiesterase subunit gamma

Kind

Protein

Organism

Humans

Pharmacological action

Unknown

Actions

Inhibitor

Allosteric modulator

General Function

Enzyme inhibitor activity

Specific Function

Participates in processes of transmission and amplification of the visual signal. cGMP-PDEs are the effector molecules in G-protein-mediated phototransduction in vertebrate rods and cones.

Gene Name

PDE6H

Uniprot ID

Q13956

Uniprot Name

Retinal cone rhodopsin-sensitive cGMP 3',5'-cyclic phosphodiesterase subunit gamma

Molecular Weight

9074.36 Da

References

1. Zhang XJ, Cahill KB, Elfenbein A, Arshavsky VY, Cote RH: Direct allosteric regulation between the GAF domain and catalytic domain of photoreceptor phosphodiesterase PDE6. J Biol Chem. 2008 Oct 31;283(44):29699-705. doi: 10.1074/jbc.M803948200. Epub 2008 Sep 8. [Article]
2. FDA Approved Drug Products: LEVITRA (vardenafil hydrochloride) tablets for oral use (March 2023) [Link]
3. FDA Approved Drug Products: STAXYN (vardenafil hydrochloride) orally disintegrating tablets (March 2023) [Link]

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Drug created at June 13, 2005 13:24 / Updated at February 20, 2024 23:55