Altretamine

Identification

Summary

Altretamine is an antineoplastic agent used in palliative treatment of persistent or recurrent ovarian cancer.

Generic Name

Altretamine

DrugBank Accession Number

DB00488

Background

An alkylating agent proposed as an antineoplastic. It also acts as a chemosterilant for male houseflies and other insects.

Type

Small Molecule

Groups

Approved

Structure

3D

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MOLSDF3D-SDFPDBSMILESInChI

Similar Structures

Structure for Altretamine (DB00488)

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Weight

Average: 210.2794
Monoisotopic: 210.159294606

Chemical Formula

C₉H₁₈N₆

Synonyms

• 2,4,6-tris(dimethylamino)-1,3,5-triazine
• 2,4,6-tris(dimethylamino)-s-triazine
• Altretamin
• Altretamina
• Altrétamine
• Altretamine
• Altretaminum
• Hexamethylmelamine
• HMM

External IDs

• NSC 13875
• NSC-13875
• RB 1515

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Pharmacology

Indication

For use as a single agent in the palliative treatment of patients with persistent or recurrent ovarian cancer following first-line therapy with a cisplatin and/or alkylating agent-based combination.

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Contraindications & Blackbox Warnings

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Pharmacodynamics

Altretamine is a novel antineoplastic agent. The precise mechanism by which altretamine exerts its cytotoxic effect is unknown, although a number of theoretical possibilities have been studied. Structurally, altretamine resembles the alkylating agent triethylenemelamine, yet in vitro tests for alkylating activity of altretamine and its metabolitics have been negative. Altretamine has been demonstrated to be efficacious for certain ovarian tumors resistant to classical alkylating agents. Metabolism of altretamine is a requirement of cytotoxicity. Synthetic monohydroxymethylmelamines, and products of altretamine metabolism, in vitro and in vivo, can form covalent adducts with tissue macromolecules including DNA, but the relevance of these reactions to antitumor activity is unknown.

Mechanism of action

The precise mechanism by which altretamine exerts its cytotoxic effect is unknown although it is classified as an alkylating anti-neoplastic agent. Through this mechanism, the drug is metabolized into alkylating agents by N-demethylation. These alkylating species consequently damage tumor cells.

Target	Actions	Organism
ADNA	other/unknown	Humans

Absorption

Not Available

Volume of distribution

Not Available

Protein binding

94%

Metabolism

Not Available

Route of elimination

Human urinary metabolites were Ndemethylated homologues of altretamine with <1% unmetabolized altretamine excreted at 24 hours.

Half-life

4.7-10.2 hours

Clearance

Not Available

Adverse Effects

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Toxicity

Not Available

Pathways

Not Available

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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Abatacept	The risk or severity of adverse effects can be increased when Altretamine is combined with Abatacept.
Abciximab	The risk or severity of bleeding can be increased when Abciximab is combined with Altretamine.
Acenocoumarol	The risk or severity of bleeding can be increased when Acenocoumarol is combined with Altretamine.
Acetylsalicylic acid	The risk or severity of bleeding can be increased when Acetylsalicylic acid is combined with Altretamine.
Adalimumab	The risk or severity of adverse effects can be increased when Adalimumab is combined with Altretamine.

Food Interactions

• Take after a meal. Take altretamine after meals and at bedtime.

Products

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International/Other Brands

Hexastat (ProStrakan)

Brand Name Prescription Products

Name	Dosage	Strength	Route	Labeller	Marketing Start	Marketing End	Region	Image
Hexalen	Capsule	50 mg/1	Oral	MGI PHARMA, INC.	1990-12-26	2011-12-31
Hexalen	Capsule	50 mg/1	Oral	Eisai Inc.	1990-12-26	2019-12-31
Hexalen	Capsule	50 mg	Oral	Eisai Limited	1995-12-31	2013-09-09

Categories

ATC Codes

L01XX03 — Altretamine

• L01XX — Other antineoplastic agents
• L01X — OTHER ANTINEOPLASTIC AGENTS
• L01 — ANTINEOPLASTIC AGENTS
• L — ANTINEOPLASTIC AND IMMUNOMODULATING AGENTS

Drug Categories

• Alkylating Activity
• Alkylating Drugs
• Antineoplastic Agents
• Antineoplastic Agents, Alkylating
• Antineoplastic and Immunomodulating Agents
• Immunosuppressive Agents
• Myelosuppressive Agents
• Narrow Therapeutic Index Drugs
• Noxae
• Toxic Actions
• Triazines

Chemical TaxonomyProvided by Classyfire

Description

This compound belongs to the class of organic compounds known as dialkylarylamines. These are aliphatic aromatic amines in which the amino group is linked to two aliphatic chains and one aromatic group.

Kingdom

Organic compounds

Super Class

Organic nitrogen compounds

Class

Organonitrogen compounds

Sub Class

Amines

Direct Parent

Dialkylarylamines

Alternative Parents

N-aliphatic s-triazines / 1,3,5-triazines / Heteroaromatic compounds / Azacyclic compounds / Organopnictogen compounds / Hydrocarbon derivatives

Substituents

1,3,5-triazine / Amino-1,3,5-triazine / Aminotriazine / Aromatic heteromonocyclic compound / Azacycle / Dialkylarylamine / Heteroaromatic compound / Hydrocarbon derivative / N-aliphatic s-triazine / Organoheterocyclic compound

Molecular Framework

Aromatic heteromonocyclic compounds

External Descriptors

triamino-1,3,5-triazine (CHEBI:24564)

Affected organisms

• Humans and other mammals

Chemical Identifiers

UNII

Q8BIH59O7H

CAS number

645-05-6

InChI Key

UUVWYPNAQBNQJQ-UHFFFAOYSA-N

InChI

InChI=1S/C9H18N6/c1-13(2)7-10-8(14(3)4)12-9(11-7)15(5)6/h1-6H3

IUPAC Name

N2,N2,N4,N4,N6,N6-hexamethyl-1,3,5-triazine-2,4,6-triamine

SMILES

CN(C)C1=NC(=NC(=N1)N(C)C)N(C)C

References

General References

1. Keldsen N, Havsteen H, Vergote I, Bertelsen K, Jakobsen A: Altretamine (hexamethylmelamine) in the treatment of platinum-resistant ovarian cancer: a phase II study. Gynecol Oncol. 2003 Feb;88(2):118-22. [Article]
2. Chan JK, Loizzi V, Manetta A, Berman ML: Oral altretamine used as salvage therapy in recurrent ovarian cancer. Gynecol Oncol. 2004 Jan;92(1):368-71. [Article]
3. Malik IA: Altretamine is an effective palliative therapy of patients with recurrent epithelial ovarian cancer. Jpn J Clin Oncol. 2001 Feb;31(2):69-73. [Article]
4. Damia G, D'Incalci M: Clinical pharmacokinetics of altretamine. Clin Pharmacokinet. 1995 Jun;28(6):439-48. [Article]

External Links

Human Metabolome Database

HMDB0014631

PubChem Compound

2123

PubChem Substance

46505760

ChemSpider

2038

BindingDB

37631

RxNav

5296

ChEBI

24564

ChEMBL

CHEMBL1455

ZINC

ZINC000000000905

Therapeutic Targets Database

DAP000989

PharmGKB

PA164743136

RxList

RxList Drug Page

Drugs.com

Drugs.com Drug Page

Wikipedia

Altretamine

Clinical Trials

Clinical Trials

Phase	Status	Purpose	Conditions	Count
1	Completed	Treatment	Lymphoma / Sarcomas	1

Pharmacoeconomics

Manufacturers

• Eisai inc

Packagers

• AAIPharma Inc.
• Eisai Inc.
• Excella GmbH
• MGI Pharma

Dosage Forms

Form	Route	Strength
Capsule	Oral	50 mg
Capsule	Oral	50 mg/1
Capsule	Oral

Prices

Unit description	Cost	Unit
Hexalen 50 mg capsule	12.03USD	capsule

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)	168	von Brachel, H. and Kindler, H.; U.S. Patent 3,424,752; January 28, 1969; assigned to Casella Farbwerke Mainkur AG
water solubility	91 mg/L (at 25 °C)	YALKOWSKY,SH & DANNENFELSER,RM (1992)
logP	2.73	HANSCH,C ET AL. (1995)

Predicted Properties

Property	Value	Source
Water Solubility	3.1 mg/mL	ALOGPS
logP	2.43	ALOGPS
logP	2.22	Chemaxon
logS	-1.8	ALOGPS
pKa (Strongest Basic)	8.75	Chemaxon
Physiological Charge	1	Chemaxon
Hydrogen Acceptor Count	6	Chemaxon
Hydrogen Donor Count	0	Chemaxon
Polar Surface Area	48.39 Å2	Chemaxon
Rotatable Bond Count	3	Chemaxon
Refractivity	65.65 m3·mol-1	Chemaxon
Polarizability	23.7 Å3	Chemaxon
Number of Rings	1	Chemaxon
Bioavailability	1	Chemaxon
Rule of Five	Yes	Chemaxon
Ghose Filter	Yes	Chemaxon
Veber's Rule	No	Chemaxon
MDDR-like Rule	No	Chemaxon

Predicted ADMET Features

Property	Value	Probability
Human Intestinal Absorption	+	0.9817
Blood Brain Barrier	+	0.8794
Caco-2 permeable	+	0.7168
P-glycoprotein substrate	Non-substrate	0.7414
P-glycoprotein inhibitor I	Non-inhibitor	0.9531
P-glycoprotein inhibitor II	Non-inhibitor	0.9797
Renal organic cation transporter	Non-inhibitor	0.7702
CYP450 2C9 substrate	Non-substrate	0.8369
CYP450 2D6 substrate	Non-substrate	0.7122
CYP450 3A4 substrate	Non-substrate	0.5779
CYP450 1A2 substrate	Inhibitor	0.9107
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	0.8821
CYP450 inhibitory promiscuity	Low CYP Inhibitory Promiscuity	0.8293
Ames test	Non AMES toxic	0.9132
Carcinogenicity	Non-carcinogens	0.8823
Biodegradation	Not ready biodegradable	0.9793
Rat acute toxicity	2.7475 LD50, mol/kg	Not applicable
hERG inhibition (predictor I)	Weak inhibitor	0.8907
hERG inhibition (predictor II)	Non-inhibitor	0.8735

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

Spectra

Mass Spec (NIST)

Download (9.6 KB)

Spectra

Spectrum	Spectrum Type	Splash Key
Predicted GC-MS Spectrum - GC-MS	Predicted GC-MS	splash10-01ox-7790000000-e6026ce486911f432231
LC-MS/MS Spectrum - LC-ESI-qTof , Positive	LC-MS/MS	splash10-03dj-9781100000-4553bbbe9a30a0391bb4
MS/MS Spectrum - , positive	LC-MS/MS	splash10-03di-3490000000-4af5631898604d2cec10
MS/MS Spectrum - , positive	LC-MS/MS	splash10-03dj-9781100000-4553bbbe9a30a0391bb4
Predicted MS/MS Spectrum - 10V, Positive (Annotated)	Predicted LC-MS/MS	splash10-03di-0090000000-1d5c67677d081f5d6f78
Predicted MS/MS Spectrum - 10V, Negative (Annotated)	Predicted LC-MS/MS	splash10-0a4i-0090000000-77b93ffadeee9e997f05
Predicted MS/MS Spectrum - 20V, Positive (Annotated)	Predicted LC-MS/MS	splash10-03di-0090000000-c314fdfc0165e3832f82
Predicted MS/MS Spectrum - 20V, Negative (Annotated)	Predicted LC-MS/MS	splash10-0a4i-0290000000-0f544a9826531bb02fb6
Predicted MS/MS Spectrum - 40V, Positive (Annotated)	Predicted LC-MS/MS	splash10-00xr-9200000000-3f73e55dec1811176ec7
Predicted MS/MS Spectrum - 40V, Negative (Annotated)	Predicted LC-MS/MS	splash10-0006-9400000000-20b6aef8fe494bde061c
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]-	159.9917382	predicted	DarkChem Lite v0.1.0
[M-H]-	160.1390382	predicted	DarkChem Lite v0.1.0
[M-H]-	150.45659	predicted	DeepCCS 1.0 (2019)
[M+H]+	160.2959382	predicted	DarkChem Lite v0.1.0
[M+H]+	159.8430382	predicted	DarkChem Lite v0.1.0
[M+H]+	152.85213	predicted	DeepCCS 1.0 (2019)
[M+Na]+	160.1955382	predicted	DarkChem Lite v0.1.0
[M+Na]+	160.1320382	predicted	DarkChem Lite v0.1.0
[M+Na]+	158.884	predicted	DeepCCS 1.0 (2019)

Targets

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Details1. DNA

Kind

Nucleotide

Organism

Humans

Pharmacological action

Yes

Actions

Other/unknown

DNA is the molecule of heredity, as it is responsible for the genetic propagation of most inherited traits. It is a polynucleic acid that carries genetic information on cell growth, division, and function. DNA consists of two long strands of nucleotides twisted into a double helix and held together by hydrogen bonds. The sequence of nucleotides determines hereditary characteristics. Each strand serves as the template for subsequent DNA replication and as a template for mRNA production, leading to protein synthesis via ribosomes.

References

1. Overington JP, Al-Lazikani B, Hopkins AL: How many drug targets are there? Nat Rev Drug Discov. 2006 Dec;5(12):993-6. [Article]
2. Imming P, Sinning C, Meyer A: Drugs, their targets and the nature and number of drug targets. Nat Rev Drug Discov. 2006 Oct;5(10):821-34. [Article]
3. Damia G, D'Incalci M: Clinical pharmacokinetics of altretamine. Clin Pharmacokinet. 1995 Jun;28(6):439-48. [Article]

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Drug created at June 13, 2005 13:24 / Updated at March 03, 2024 02:26