Zalcitabine

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Identification

Summary

Zalcitabine is a dideoxynucleoside used to treat HIV.

Generic Name

Zalcitabine

DrugBank Accession Number

DB00943

Background

A dideoxynucleoside compound in which the 3'-hydroxyl group on the sugar moiety has been replaced by a hydrogen. This modification prevents the formation of 5' to 3' phosphodiester linkages, which are needed for the elongation of DNA chains, thus resulting in the termination of viral DNA growth. The compound is a potent inhibitor of HIV replication at low concentrations, acting as a chain-terminator of viral DNA by binding to reverse transcriptase. Its principal toxic side effect is axonal degeneration resulting in peripheral neuropathy.

Type

Small Molecule

Groups

Approved, Investigational

Structure

3D

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MOLSDF3D-SDFPDBSMILESInChI

Similar Structures

Structure for Zalcitabine (DB00943)

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Weight

Average: 211.2178
Monoisotopic: 211.095691297

Chemical Formula

C₉H₁₃N₃O₃

Synonyms

• 2',3'-Dideoxycytidine
• 4-amino-1-[(2R,5S)-5-(hydroxymethyl)tetrahydrofuran-2-yl]pyrimidin-2(1H)-one
• DDC
• DDCYD
• Dideoxycytidine
• Zalcitabine

External IDs

• RO 24-2027/000
• RO-24-2027/000
• RO-24-2027000
• RO-242027000

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Pharmacology

Indication

For the treatment of Human immunovirus (HIV) infections in conjunction with other antivirals.

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Contraindications & Blackbox Warnings

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Pharmacodynamics

Zalcitabine is an analog of 2'-deoxycytidine that is pharmacologically related to but structurally different from other nucleotide reverse transcriptase inhibitors (NRTIs). Zalcitabine inhibits the activity of HIV-1 reverse transcriptase (RT) both by competing with the natural substrate dGTP and by its incorporation into viral DNA.

Mechanism of action

Zalcitabine is a nucleoside reverse transcriptase inhibitor (NRTI) with activity against Human Immunodeficiency Virus Type 1 (HIV-1). Within cells, zalcitabine is converted to its active metabolite, dideoxycytidine 5'-triphosphate (ddCTP), by the sequential action of cellular enzymes. ddCTP interferes with viral RNA-directed DNA polymerase (reverse transcriptase) by competing for utilization of the natural substrate deoxycytidine 5'-triphosphate (dCTP), as well as incorpating into viral DNA. Due to it's lack of a 3'-OH group, the formation of a 5' to 3' phosphodiester linkage that is necessary for DNA chain elongation is inhibited, thus leading to the termination of viral DNA growth.

Target	Actions	Organism
AGag-Pol polyprotein	inhibitor
AReverse transcriptase/RNaseH	inhibitor	Human immunodeficiency virus 1

Absorption

Bioavailability is over 80% following oral administration.

Volume of distribution

• 0.304 to 0.734 L/kg

Protein binding

Less than 4%

Metabolism

Zalcitabine is not reported to undergo significant hepatic metabolism; it is mainly phosphorylated intracellularly to zalcitabine triphosphate, the active substrate for HIV-reverse transcriptase. The concentration of zalcitabine triphosphate remains low for quantitative detection and measurement in the plasma following administration of therapeutic doses ^Label.

Route of elimination

Renal excretion of unchanged drug appears to be the primary route of elimination, accounting for approximately 80% of an intravenous dose and 60% of an orally administered dose within 24 hours after dosing (n=19). Renal clearance exceeds glomerular filtration rate suggesting renal tubular secretion contributes to the elimination of zalcitabine by the kidneys.

Half-life

2 hours

Clearance

• 285 mL/min [HIV-infected patients receiving 1.5 mg IV infusion for 1 hour]

Adverse Effects

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Toxicity

Acute overdose: Inadvertent pediatric overdoses have occurred with doses up to 1.5 mg/kg zalcitabine. Chronic overdose: in an initial dose-finding study in which zalcitabine was administered at doses 25 times (0.25 mg/kg every 8 hours) the currently recommended dose, one patient discontinued zalcitabine after 1½ weeks of treatment subsequent to the development of a rash and fever.

Pathways

Pathway	Category
Zalcitabine Action Pathway	Drug action

Pharmacogenomic Effects/ADRs

Not Available

Interactions

Drug Interactions

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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Acetazolamide	The excretion of Zalcitabine can be decreased when combined with Acetazolamide.
Acetylsalicylic acid	The excretion of Zalcitabine can be decreased when combined with Acetylsalicylic acid.
Acyclovir	The excretion of Zalcitabine can be decreased when combined with Acyclovir.
Adefovir dipivoxil	The excretion of Zalcitabine can be decreased when combined with Adefovir dipivoxil.
Adenovirus type 7 vaccine live	The therapeutic efficacy of Adenovirus type 7 vaccine live can be decreased when used in combination with Zalcitabine.

Food Interactions

• Avoid multivalent ions. Magnesium and aluminum containing products can reduce the absorption of this medication.
• Take on an empty stomach. Take at least 1 hour before or 2 hours after meals.

Products

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Brand Name Prescription Products

Name	Dosage	Strength	Route	Labeller	Marketing Start	Marketing End	Region	Image
Hivid	Tablet, film coated	0.375 mg/1	Oral	Genentech, Inc.	1992-06-19	2009-06-18
Hivid	Tablet, film coated	0.75 mg/1	Oral	Physicians Total Care, Inc.	1992-06-19	2007-08-21
Hivid	Tablet, film coated	0.75 mg/1	Oral	Genentech, Inc.	1992-06-19	2009-06-18
Hivid Tab 0.375mg	Tablet	.375 mg	Oral	Hoffmann La Roche	1992-12-31	2003-07-30
Hivid Tab 0.75 mg	Tablet	.75 mg	Oral	Hoffmann La Roche	1992-12-31	2006-07-25

Categories

ATC Codes

J05AF03 — Zalcitabine

• J05AF — Nucleoside and nucleotide reverse transcriptase inhibitors
• J05A — DIRECT ACTING ANTIVIRALS
• J05 — ANTIVIRALS FOR SYSTEMIC USE
• J — ANTIINFECTIVES FOR SYSTEMIC USE

Drug Categories

• Anti-HIV Agents
• Anti-Infective Agents
• Anti-Retroviral Agents
• Antiinfectives for Systemic Use
• Antimetabolites
• Antiviral Agents
• Antivirals for Systemic Use
• Deoxycytidine
• Deoxyribonucleosides
• Dideoxynucleosides
• Direct Acting Antivirals
• Enzyme Inhibitors
• Noxae
• Nucleic Acid Synthesis Inhibitors
• Nucleic Acids, Nucleotides, and Nucleosides
• Nucleoside and Nucleotide Reverse Transcriptase Inhibitors
• Nucleoside Reverse Transcriptase Inhibitors
• Nucleosides
• OAT1/SLC22A6 Substrates
• Pyrimidine Nucleosides
• Pyrimidines
• Reverse Transcriptase Inhibitors
• Toxic Actions

Chemical TaxonomyProvided by Classyfire

Description

This compound belongs to the class of organic compounds known as pyrimidine 2',3'-dideoxyribonucleosides. These are compounds consisting of a pyrimidine linked to a ribose which lacks a hydroxyl group at positions 2 and 3.

Kingdom

Organic compounds

Super Class

Nucleosides, nucleotides, and analogues

Class

Pyrimidine nucleosides

Sub Class

Pyrimidine 2',3'-dideoxyribonucleosides

Direct Parent

Pyrimidine 2',3'-dideoxyribonucleosides

Alternative Parents

Pyrimidones / Aminopyrimidines and derivatives / Imidolactams / Hydropyrimidines / Tetrahydrofurans / Heteroaromatic compounds / Oxacyclic compounds / Azacyclic compounds / Primary amines / Primary alcohols / Organopnictogen compounds / Organic oxides / Hydrocarbon derivatives

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Substituents

Alcohol / Amine / Aminopyrimidine / Aromatic heteromonocyclic compound / Azacycle / Heteroaromatic compound / Hydrocarbon derivative / Hydropyrimidine / Imidolactam / Organic nitrogen compound / Organic oxide / Organic oxygen compound / Organoheterocyclic compound / Organonitrogen compound / Organooxygen compound / Organopnictogen compound / Oxacycle / Primary alcohol / Primary amine / Pyrimidine / Pyrimidine 2',3'-dideoxyribonucleoside / Pyrimidone / Tetrahydrofuran

show 13 more

Molecular Framework

Aromatic heteromonocyclic compounds

External Descriptors

pyrimidine 2',3'-dideoxyribonucleoside (CHEBI:10101)

Affected organisms

• Human Immunodeficiency Virus

Chemical Identifiers

UNII

6L3XT8CB3I

CAS number

7481-89-2

InChI Key

WREGKURFCTUGRC-POYBYMJQSA-N

InChI

InChI=1S/C9H13N3O3/c10-7-3-4-12(9(14)11-7)8-2-1-6(5-13)15-8/h3-4,6,8,13H,1-2,5H2,(H2,10,11,14)/t6-,8+/m0/s1

IUPAC Name

4-amino-1-[(2R,5S)-5-(hydroxymethyl)oxolan-2-yl]-1,2-dihydropyrimidin-2-one

SMILES

NC1=NC(=O)N(C=C1)[C@H]1CC[C@@H](CO)O1

References

General References

1. Shelton MJ, O'Donnell AM, Morse GD: Zalcitabine. Ann Pharmacother. 1993 Apr;27(4):480-9. [Article]
2. Devineni D, Gallo JM: Zalcitabine. Clinical pharmacokinetics and efficacy. Clin Pharmacokinet. 1995 May;28(5):351-60. [Article]

External Links

Human Metabolome Database

HMDB0015078

KEGG Drug

D00412

KEGG Compound

C07207

PubChem Compound

24066

PubChem Substance

46507879

ChemSpider

22498

BindingDB

50145605

RxNav

3363

ChEBI

10101

ChEMBL

CHEMBL853

ZINC

ZINC000000039906

Therapeutic Targets Database

DNC000527

PharmGKB

PA451950

RxList

RxList Drug Page

Drugs.com

Drugs.com Drug Page

Wikipedia

Zalcitabine

FDA label

Download (244 KB)

MSDS

Download (36 KB)

Clinical Trials

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Phase	Status	Purpose	Conditions	Count	Start Date	Why Stopped	100+ additional columns
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Not Available	Completed	Treatment	Human Immunodeficiency Virus (HIV) Infections	9	somestatus	stop reason	just information to hide
4	Completed	Treatment	Hemophilia A / Human Immunodeficiency Virus (HIV) Infections	1	somestatus	stop reason	just information to hide
3	Completed	Treatment	Human Immunodeficiency Virus (HIV) Infections	7	somestatus	stop reason	just information to hide
2	Completed	Treatment	Human Immunodeficiency Virus (HIV) Infections	15	somestatus	stop reason	just information to hide
2	Completed	Treatment	Human Immunodeficiency Virus (HIV) Infections / Progressive Multifocal Leucoencephalopathy (PML)	1	somestatus	stop reason	just information to hide

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Pharmacoeconomics

Manufacturers

• Hoffmann la roche inc

Packagers

• Murfreesboro Pharmaceutical Nursing Supply
• Pharmaceutical Utilization Management Program VA Inc.
• Physicians Total Care Inc.

Dosage Forms

Form	Route	Strength
Tablet	Oral
Tablet, film coated	Oral	0.375 mg/1
Tablet, film coated	Oral	0.75 mg/1
Tablet	Oral	.375 mg
Tablet	Oral	.75 mg
Tablet	Oral	0.75 mg
Tablet	Oral	0.375 mg
Tablet, film coated	Oral	0.75 mg

Prices

Unit description	Cost	Unit
Hivid 0.75 mg tablet	2.84USD	tablet
Hivid 0.375 mg tablet	2.27USD	tablet

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

Patents

Not Available

Properties

State

Solid

Experimental Properties

Property	Value	Source
melting point (°C)	217-218 °C	PhysProp
water solubility	7.64E+004 mg/L (at 25 °C)	PHYSICIANS DESK REFERENCE (2001)
logP	-1.30	SANGSTER (1993)

Predicted Properties

Property	Value	Source
Water Solubility	7.05 mg/mL	ALOGPS
logP	-1.3	ALOGPS
logP	-1.2	Chemaxon
logS	-1.5	ALOGPS
pKa (Strongest Acidic)	14.67	Chemaxon
pKa (Strongest Basic)	4.48	Chemaxon
Physiological Charge	0	Chemaxon
Hydrogen Acceptor Count	5	Chemaxon
Hydrogen Donor Count	2	Chemaxon
Polar Surface Area	88.15 Å2	Chemaxon
Rotatable Bond Count	2	Chemaxon
Refractivity	52.24 m3·mol-1	Chemaxon
Polarizability	20.92 Å3	Chemaxon
Number of Rings	2	Chemaxon
Bioavailability	1	Chemaxon
Rule of Five	Yes	Chemaxon
Ghose Filter	No	Chemaxon
Veber's Rule	No	Chemaxon
MDDR-like Rule	No	Chemaxon

Predicted ADMET Features

Property	Value	Probability
Human Intestinal Absorption	+	0.9972
Blood Brain Barrier	+	0.9761
Caco-2 permeable	-	0.7931
P-glycoprotein substrate	Non-substrate	0.7746
P-glycoprotein inhibitor I	Non-inhibitor	0.937
P-glycoprotein inhibitor II	Non-inhibitor	0.9171
Renal organic cation transporter	Non-inhibitor	0.8163
CYP450 2C9 substrate	Non-substrate	0.8286
CYP450 2D6 substrate	Non-substrate	0.8493
CYP450 3A4 substrate	Non-substrate	0.5762
CYP450 1A2 substrate	Non-inhibitor	0.9046
CYP450 2C9 inhibitor	Non-inhibitor	0.9071
CYP450 2D6 inhibitor	Non-inhibitor	0.9231
CYP450 2C19 inhibitor	Non-inhibitor	0.9025
CYP450 3A4 inhibitor	Non-inhibitor	0.8893
CYP450 inhibitory promiscuity	Low CYP Inhibitory Promiscuity	0.9213
Ames test	AMES toxic	0.9107
Carcinogenicity	Non-carcinogens	0.8626
Biodegradation	Not ready biodegradable	0.8721
Rat acute toxicity	2.0606 LD50, mol/kg	Not applicable
hERG inhibition (predictor I)	Weak inhibitor	0.925
hERG inhibition (predictor II)	Non-inhibitor	0.875

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	splash10-005c-9600000000-2b4de4867a39d5e3055b
LC-MS/MS Spectrum - LC-ESI-QQ , negative	LC-MS/MS	splash10-03di-0190000000-5d3365f648d5f5675ab9
LC-MS/MS Spectrum - LC-ESI-QQ , negative	LC-MS/MS	splash10-066r-2900000000-843d28df71eab94652c3
LC-MS/MS Spectrum - LC-ESI-QQ , negative	LC-MS/MS	splash10-0a4l-7900000000-628c9e8f6a131581a8d4
LC-MS/MS Spectrum - LC-ESI-QQ , negative	LC-MS/MS	splash10-0006-9200000000-60a00651a71121843a19
LC-MS/MS Spectrum - LC-ESI-QQ , negative	LC-MS/MS	splash10-0006-9000000000-237a0c1094225974a6e8
LC-MS/MS Spectrum - LC-ESI-QQ , positive	LC-MS/MS	splash10-03di-0910000000-95a2a7845a54a61d7c15
LC-MS/MS Spectrum - LC-ESI-QQ , positive	LC-MS/MS	splash10-03di-0900000000-345deba429b644c7b4f5
LC-MS/MS Spectrum - LC-ESI-QQ , positive	LC-MS/MS	splash10-03di-0900000000-6aaba2f2eeb001628ab2
LC-MS/MS Spectrum - LC-ESI-QQ , positive	LC-MS/MS	splash10-03di-5900000000-03b881f85c17ccbe5295
LC-MS/MS Spectrum - LC-ESI-QQ , positive	LC-MS/MS	splash10-01ot-9300000000-2896ce7406bb834c001a
LC-MS/MS Spectrum - LC-ESI-IT , positive	LC-MS/MS	splash10-03di-0900000000-056961b8bc4067346530
Predicted MS/MS Spectrum - 10V, Positive (Annotated)	Predicted LC-MS/MS	splash10-03di-0900000000-9c4b3aee044ce7956a96
Predicted MS/MS Spectrum - 10V, Negative (Annotated)	Predicted LC-MS/MS	splash10-03di-0970000000-54526a661f3d174f6656
Predicted MS/MS Spectrum - 20V, Positive (Annotated)	Predicted LC-MS/MS	splash10-03di-2900000000-891c2cbbddfdec8fdc00
Predicted MS/MS Spectrum - 20V, Negative (Annotated)	Predicted LC-MS/MS	splash10-014i-9200000000-5046c313f3dfd83dc383
Predicted MS/MS Spectrum - 40V, Positive (Annotated)	Predicted LC-MS/MS	splash10-0i01-9200000000-952eba834ff4e8d0ee5d
Predicted MS/MS Spectrum - 40V, Negative (Annotated)	Predicted LC-MS/MS	splash10-014i-9500000000-0aaf211e0a22b65a6a24
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]-	149.4572638	predicted	DarkChem Lite v0.1.0
[M-H]-	149.3093638	predicted	DarkChem Lite v0.1.0
[M-H]-	149.4220638	predicted	DarkChem Lite v0.1.0
[M-H]-	144.52248	predicted	DeepCCS 1.0 (2019)
[M+H]+	150.7527638	predicted	DarkChem Lite v0.1.0
[M+H]+	150.5403638	predicted	DarkChem Lite v0.1.0
[M+H]+	150.5553638	predicted	DarkChem Lite v0.1.0
[M+H]+	146.91806	predicted	DeepCCS 1.0 (2019)
[M+Na]+	149.2785638	predicted	DarkChem Lite v0.1.0
[M+Na]+	149.5527638	predicted	DarkChem Lite v0.1.0
[M+Na]+	149.5601638	predicted	DarkChem Lite v0.1.0
[M+Na]+	152.90862	predicted	DeepCCS 1.0 (2019)

Targets

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Details1. Gag-Pol polyprotein

Kind

Protein

Organism

Not Available

Pharmacological action

Yes

Actions

Inhibitor

General Function

Gag-Pol polyprotein Mediates, with Gag polyprotein, the essential events in virion assembly, including binding the plasma membrane, making the protein-protein interactions necessary to create spherical particles, recruiting the viral Env proteins, and packaging the genomic RNA via direct interactions with the RNA packaging sequence (Psi). Gag-Pol polyprotein may regulate its own translation, by the binding genomic RNA in the 5'-UTR. At low concentration, the polyprotein would promote translation, whereas at high concentration, the polyprotein would encapsidate genomic RNA and then shut off translation.

Specific Function

aspartic-type endopeptidase activity

Gene Name

gag-pol

Uniprot ID

P03366

Uniprot Name

Gag-Pol polyprotein

Molecular Weight

163287.51 Da

References

1. Zhou Y, Zhang Y, Zhao D, Yu X, Shen X, Zhou Y, Wang S, Qiu Y, Chen Y, Zhu F: TTD: Therapeutic Target Database describing target druggability information. Nucleic Acids Res. 2024 Jan 5;52(D1):D1465-D1477. doi: 10.1093/nar/gkad751. [Article]

Details2. Reverse transcriptase/RNaseH

Kind

Protein

Organism

Human immunodeficiency virus 1

Pharmacological action

Yes

Actions

Inhibitor

General Function

Not Available

Specific Function

aspartic-type endopeptidase activity

Gene Name

pol

Uniprot ID

Q72547

Uniprot Name

Reverse transcriptase/RNaseH

Molecular Weight

65223.615 Da

References

1. Devineni D, Gallo JM: Zalcitabine. Clinical pharmacokinetics and efficacy. Clin Pharmacokinet. 1995 May;28(5):351-60. [Article]
2. Adkins JC, Peters DH, Faulds D: Zalcitabine. An update of its pharmacodynamic and pharmacokinetic properties and clinical efficacy in the management of HIV infection. Drugs. 1997 Jun;53(6):1054-80. [Article]
3. De Clercq E: Emerging anti-HIV drugs. Expert Opin Emerg Drugs. 2005 May;10(2):241-73. [Article]

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Drug created at June 13, 2005 13:24 / Updated at August 26, 2024 19:24