112-99-2

Basic information

• Product Name: DIOCTADECYLAMINE
• Synonyms: AURORA KA-7662;DODA;DISTEARYLAMINE;DIOCTADECYLAMINE;n-octadecyl-1-octadecanamin;N-octadecyl-1-Octadecanamine;1-Octadecanamine, N-octadecyl-;N-octadecyloctadecan-1-amine
• CAS NO: 112-99-2
• Molecular Formula: C₃₆H₇₅N
• Molecular Weight: 521.99
• EINECS: 204-020-2
• Mol File: 112-99-2.mol
• Article Data: 21

Chemical Properties

• Melting Point: 71-73 °C
• Boiling Point: 524.75°C (estimate)
• Flash Point: 197.249 °C
• Appearance: /
• Density: 0.9086 (estimate)
• Vapor Pressure: 1.43E-13mmHg at 25°C
• Refractive Index: 1.4841 (estimate)
• Solubility: water: soluble(lit.)
• PKA: 10.84±0.19(Predicted)
• BRN: 1801688
• CAS DataBase Reference: DIOCTADECYLAMINE(CAS DataBase Reference)
• NIST Chemistry Reference: DIOCTADECYLAMINE(112-99-2)
• EPA Substance Registry System: DIOCTADECYLAMINE(112-99-2)

Safety Data

• Hazard Codes: Xi
• Statements: 36/37/38
• Safety Statements: 26-36
• WGK Germany: 3
• F: 10-34
• Hazardous Substances Data: 112-99-2(Hazardous Substances Data)

Usage

Uses

Dioctadecylamine (DODA) is suitable reagent used in the synthesis of the following:Dioctadecylamine-BCN (bicyclo[6.1.0]nonyne) conjugate.Lipid derivatives of bisethylnorspermine (BSP).Functional VP (N-vinylpyrrolidone ) polymers.It may be used in the following studies:As a reactant in the synthesis of 4,4′-azobis(4-cyano-N,N-dioctadecyl)pentanamide (DODA-501) by reacting with disuccinimidyl 4,4′-azobis(4-cyanovalerate).As a reagent in the synthesis of dioctadecyl heptapeptides.As a phase transfer and stabilizer agent for gold nanoparticles (AuNPs) in non-polar solvent.

General Description

Dioctadecylamine (DODA), a secondary amine, is a fatty amine derivative. Its biodegradation potential has been assessed. It has been observed that in aqueous medium DODA self organizes into plate like structures. Its partial charge distribution as a function of its conformation has been analyzed. The phase diagram of dioctadecylamine Langmuir monolayers has been determined and investigations show it does not form a monolayer above pH 3.9. DODA has been utilized in forming liposomes, cationic lipids or lipid chelating agents.

InChI:InChI=1/C36H75N/c1-3-5-7-9-11-13-15-17-19-21-23-25-27-29-31-33-35-37-36-34-32-30-28-26-24-22-20-18-16-14-12-10-8-6-4-2/h37H,3-36H2,1-2H3

Upstream product

• 3386-33-2 1-chlorooctadecane 
• 112-61-8 Methyl stearate 
• 638-65-3 stearonitrile 
• 17248-34-9 N-Stearylioden-stearylamin 
• 555-43-1 glycerol tristearate 
• 124-30-1 1-aminooctadecane 
• 112-76-5 Stearoyl chloride 
• 57-11-4 stearic acid 
• 112-92-5 1-octadecanol 
• 638-66-4 n-Octadecanal 
• 112-89-0 1-Bromooctadecane 
• 7664-41-7 ammonia 
• 13276-08-9 N-(octadecanoyl)octadecylamide 
• 124-26-5 stearamide 

Downstream Products

• 94135-17-8 N,N-dioctadecyl-adipamic acid 
• 102-88-5 trioctadecylamine 
• 131362-15-7 N,N-dioctadecyl-benzamide 
• 124-30-1 1-aminooctadecane 
• 173278-40-5 N,N-dioctadecylterephthalamic acid 
• 407629-44-1 [2-(2-{[1-(2-{2-[2-(2-dioctadecylcarbamoylmethoxyacetylamino)acetylamino]acetylamino}acetyl)pyrrolidine-2-carbonyl]amino}acetylamino)acetylamino]acetic acid benzyl ester 
• 68800-69-1 3-[4-bis-(octadecyl)-aminomethylbenzylidene]-camphor 

Relevant articles and documents

Design, synthesis, and transfection biology of novel cationic glycolipids for use in liposomal gene delivery

The molecular structure of the cationic lipids used in gene transfection strongly influences their transfection efficiency. High transfection efficiencies of non-glycerol-based simple monocationic transfection lipids with hydroxyethyl headgroups recently reported by us (Banerjee et al. J. Med. Chem. 1999, 42, 4292-4299) are consistent with the earlier observations that the presence of hydroxyl functionalities in the headgroup region of a cationic lipid contributes favorably in liposomal gene delivery. Using simple sugar molecules as the source of multiple hydroxyl functionalities in the headgroup region of the transfection lipids, we have synthesized four novel simple monocationic transfection lipids, namely, 1-deoxy-1-[dihexadecyl(methyl)-ammonio]-D-xylitol (1), 1-deoxy-1-[methyl(ditetradecyl)ammonio]-D-arabinitol (2), 1-deoxy-1-[dihexadecyl(methyl)ammonio]-D-arabinitol (3) and 1-deoxy-1-[methyl(dioctadecyl)ammonio]-D-arabinitol (4), containing hydrophobic aliphatic tails and the hydrophilic arabinosyl or xylose sugar groups linked directly to the positively charged nitrogen atom. Syntheses, chemical characterizations, and the transfection biology of these novel transfection lipids 1-4 are described in this paper. Lipid 1, the xylosyl derivative, showed maximum transfection on COS-1 cells. All the lipids showed transfection with cholesterol as colipid and not with dioleoylphosphatidylethanolamine (DOPE). Radioactive quantitation of free and complexed DNA combined with ethidium bromide exclusion measurements suggest that though nearly 70% of the DNA exists as complexed DNA, the DNA may not have condensed as was observed with other cationic lipids. Presence of additional (more than two) hydroxyl functionalities in the headgroup of the cationic lipids appears to have improved the transfection efficiency and made these lipids less cytotoxic compared to two-hydroxyl derivatives.

Oppi briefs: Convenient synthesis of di(n-octadecyl)amine and di(n-hexadecyl)amine

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Conversion of Primary Amines to Symmetrical Secondary and Tertiary Amines using a Co-Rh Heterobimetallic Nanocatalyst

Symmetrical tertiary amines have been efficiently realized from amine and secondary amines via deaminated homocoupling with heterogeneous bimetallic Co2Rh2/C as catalyst (molar ratio Co:Rh=2:2). Unsymmetric secondary anilines were produced from the reaction of anilines with symmetric tertiary amines. The Co2Rh2/C catalyst exhibited very high catalytic activity towards a wide range of amines and could be conveniently recycled ten times without considerable leaching. (Figure presented.).

RADIOACTIVE FLUORINE LABELING PRECURSOR COMPOUND AND METHOD FOR MANUFACTURING RADIOACTIVE FLUORINE LABELED COMPOUND USING THE SAME

There is provided a labeling precursor compound represented by the following general formula (2): wherein R1 represents an alkynyl group, an alkynyloxy group, an azide group, an azidoalkyl group, an arylazide group, a monocyclic or condensed polycyclic aryl group or a nitrogen-containing heterocycle; R2 and R3 each independently represent an alkyl group or a hydroxyalkyl group which hydroxy group may be protected with a protecting group, and n is an integer of 1 or 2; R6 represents an alkyl group or —CONR11R12 wherein R11 and R12 each independently represent an alkyl group or a monocyclic or condensed polycyclic aryl group; and R4, R5, R7 and R8 each independently represent a hydrogen atom, an alkyl group or an alkoxy group.