Checked by Harvey W. Taylor and Henry E. Baumgarten.
1. Procedure
A.
N,N'-Diethylsulfamide. A
dry, 2-l., three-necked, round-bottomed flask fitted with a mechanical stirrer, a reflux condenser, a thermometer, and a dropping funnel, and protected from atmospheric moisture with calcium chloride drying tubes is charged with
500 ml. of petroleum ether,
100 g. (2.20 moles) of ethylamine, and
140 g. (1.76 moles) of pyridine (Note
1). The stirred mixture is cooled in an
acetone–dry ice bath to −30° to −15°; a solution of
120 g. (0.889 mole) of sulfuryl chloride in
220 ml. of petroleum ether is added, dropwise and with stirring, to the reaction flask at such a rate that the temperature remains below −15°. After addition is complete, the reaction mixture is stirred at room temperature for one hour. The
petroleum ether layer is separated and discarded. The dark semisolid residue is made acidic by addition of
6 M hydrochloric acid, and the acidic mixture is heated under reflux for 2 hours (Note
2). The resulting solution is extracted with
diethyl ether in a
continuous extractor (Note
3) until all of the
diethylsulfamide has dissolved. The
ether is evaporated using a
rotary evaporator, yielding
58–61 g.. (
44–45%) of crude
N,N'-diethylsulfamide, m.p.
65–67°, (Note
4) which is of sufficient purity for use in the next step.
B.
Azoethane. A
3-l., three-necked, round-bottomed flask fitted with a mechanical stirrer, a reflux condenser, a thermometer, and a dropping funnel is charged with
500 ml. of an aqueous 2 M solution of sodium hydroxide and
152 g. (1.00 mole) of N,N'-diethylsulfamide, which is brought into solution by warming the reaction flask. The reaction flask is cooled in a
cold water bath before
715 ml. (1.0 mole) of aqueous 1.4 M sodium hypochlorite (Note
5) is added dropwise with stirring. After addition is complete, the reaction mixture is stirred for 15 minutes at room temperature. The mixture is brought to pH 1 by addition of 6
M hydrochloric acid and stirred for an additional 30 minutes at 60° (Note
6). The mixture is cooled to room temperature, then is brought to pH 14 by addition of aqueous 2
M sodium hydroxide (Note
7). Addition of
715 ml. (1.0 mole) of aqueous 1.4 M sodium hypochlorite solution causes the separation of
azoethane as an oil, having a fruitlike odor. The mixture is extracted with three
100-ml. portions of toluene (Note
8). The combined extracts are dried over
anhydrous sodium sulfate and distilled through a
50-cm. packed column, yielding
44–46 g. (
51–54%) of
azoethane, b.p.
58–59°,
n20D 1.3861 (Note
9).
2. Notes
1. The submitters dried the
ethylamine and
pyridine by distillation over
potassium hydroxide pellets and used
600 ml. of petroleum ether,
113 g. (2.50 moles) of ethylamine, and
158 g. (2.00 moles) of pyridine to which was added
135 g. (1.00 mole) of sulfuryl chloride in
250 ml. of petroleum ether. In the United States
ethylamine is sold in 100-g. quantities in sealed-glass vials (Eastman Organic Chemicals) or as the compressed gas in cylinders (Matheson Gas Products). The checkers used the contents of a freshly opened vial (without distillation) for each run, as a matter of convenience, and used either
pentane or
petroleum ether (b.p.
38–51°). Note that step B requires the product from at least two [submitters' scale
and yield (Note
4)] or three (checkers' scale) step A runs. Step B can be run at half scale with the same percentage yield.
2. The purpose of this step is to hydrolyze any alkyl imido compound that may have formed from the further reaction of the sulfamide.
4
3. A convenient continuous extractor has been described earlier in this series.
5
4. After purification by dissolving the crude product in
ether and precipitating with
petroleum ether,
N,N'-diethylsulfamide is obtained as shiny, white leaflets, m.p.
67°. The submitters reported a
54% yield of the purified product.
For sulfamides with larger alkyl groups (C
3 to C
6) the following procedure is preferred. A solution of
316 g. (4.00 moles) of pyridine in 400 ml. of chloroform is added dropwise, with cooling to −10° to −5°, to a stirred mixture of
135 g. (1.00 mole) of sulfuryl chloride and
500 ml. of chloroform. Maintaining a temperature of −5° to 0°, a solution of 2.5 moles of alkylamine in
600 ml. of chloroform is added to the reaction. After addition is complete the mixture is stirred for 30 minutes at room temperature, evaporated under reduced pressure to a thick brown liquid, and treated with 2
M hydrochloric acid until the
pyridine dissolves. Cooling the acidic solution, the crystalline sulfamide precipitates and is filtered. Any dissolved sulfamide may be recovered by extraction of the filtrate with ether. The crude product may be purified by recrystallization from
50% ethanol.
The
pyridine used in the submitters' procedures apparently reacts with the
sulfuryl chloride to form an intermediate, quaternary pyridinium complex which undergoes aminolysis, yielding the sulfamide.
6 However, in many instances the
pyridine may be replaced by an equivalent quantity of the primary alkylamine being used.
4,7 Using this variation the checkers obtained a
78% yield of
N,N'-dicyclohexylsulfamide (compare with Table I). Moreover, in the reaction of
4-aminospiro(cyclohexane-1,9'-fluorene) with
sulfuryl chloride no sulfamide could be isolated from reactions run in the presence of
pyridine (or
triethylamine); however, a
54% (purified) yield of
N,N'-dispiro(cyclohexane-1,9'-fluorene)-4-ylsulfamide was obtained when 2.7
equivalents of the amine (relative to
sulfuryl chloride) were used. Probably the failure of the mixed pyridine-alkylamine technique was the result of combined bulk of the pyridinium complex and the amine.
TABLE I
PREPARATION OF AZOALKANES
|
R |
RNHSO2NHR |
R-N=N-R |
|
m.p. |
Yield, % |
b.p. |
Yield, % |
|
n-C3H7 |
118° |
69 |
113–115° |
54 |
n-C4H9 |
126° |
66 |
59–60° (18 mm.) |
54 |
tert-C4H9 |
140–142° |
68 |
109–110° |
84 |
cyclo-C6H11 |
154° |
59 |
m.p. 33–34° |
80 |
4-NO2-C6H4 |
197° |
58 |
m.p. 216° |
31 |
|
In some small-scale preparations of this type the checkers used commercial household bleach (Chlorox®, 5.25% NaOCl) and followed the course of the reaction by TLC. The yields appear to be somewhat lower than those obtained with
sodium hypochlorite prepared as described above. The obvious attractive alternative, preparation of
potassium hypochlorite as described elsewhere in this series,
8 apparently has not been tried.
7. In the preparation of
azomethane a
gas-inlet tube is used to pass
nitrogen slowly through the reaction mixture, during the second oxidation stage while the temperature is raised to 60°. The reflux condenser is fitted with a
drying tube filled with potassium hydroxide pellets connected via rubber hose to two dry ice-cooled cold traps connected in series and terminated with a second drying tube filled with potassium hydroxide pellets. The
azomethane collects in the cold traps. Redistillation gives a
39% yield of
azomethane, b.p.
1°.
8. For the homologous azoalkanes
ether,
pentane, or
petroleum ether may be used for extraction. The extraction solvent may be added before the addition of hypochlorite.
6
9. The checkers used a
60-cm. Vigreux column. Their product gave the following
1H NMR spectrum (CDCl
3): δ 1.17 (q,
J = 7 Hz., 2H, C
H2), 3.77 (t,
J = 7Hz., 3H, C
H3).
3. Discussion
The present procedure may be used for the preparation of azoalkanes with alkyl, cycloalkyl, or aromatic substituents (Table I). Azoalkanes have been used as radical sources for inducing of radical reactions (
e.g., polymerization). The present procedure may also be used for the preparation of
N,N'-dialkylhydrazines.
6 For this purpose only one equivalent of
sodium hypochlorite solution is employed and the reaction mixture is worked up after its addition (yields:
60–95%).
Appendix
Compounds Referenced (Chemical Abstracts Registry Number)
petroleum ether
Diazene, diethyl
ethanol (64-17-5)
hydrochloric acid (7647-01-0)
Benzene (71-43-2)
ether,
diethyl ether (60-29-7)
sodium hydroxide (1310-73-2)
chloroform (67-66-3)
sodium sulfate (7757-82-6)
nitrogen (7727-37-9)
mercury(II) oxide (21908-53-2)
platinum (7440-06-4)
sulfuryl chloride (7791-25-5)
pyridine (110-86-1)
chlorine (7782-50-5)
potassium hydroxide (1310-58-3)
toluene (108-88-3)
copper(II) chloride (7758-89-6)
Pentane (109-66-0)
sodium hypochlorite (7681-52-9)
methylamine (74-89-5)
potassium hypochlorite
lithium aluminum hydride (16853-85-3)
triethylamine (121-44-8)
ethylamine (75-04-7)
Azoethane (38534-43-9)
diethylsulfamide
azocyclohexane
azomethane
N,N'-diformylhydrazine
N,N'-Diethylsulfamide (6104-21-8)
N,N'-dimethylsulfamide
N,N'-dicyclohexylsulfamide
4-aminospiro(cyclohexane-1,9'-fluorene)
N,N'-dispiro(cyclohexane-1,9'-fluorene)-4-ylsulfamide
2,2'-azoisobutane
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