Checked by David Oare and Clayton Heathcock.
1. Procedure
A.
Diethyl 2-chloro-2-cyclopropylethene-1,1-dicarboxylate. A
1-L, two-necked flask equipped with
magnetic stirrer,
reflux condenser, and
dropping funnel is charged with
166 g (0.73 mol) of diethyl cyclopropylcarbonylmalonate (Note
1) and
0.5 kg of phosphorus oxychloride (Note
2). The flask is cooled with a
water bath, stirring is started and
135 g (0.73 mol) of tributylamine (Note
3) is added from the dropping funnel. The reaction is exothermic. When the addition is complete, the dropping funnel is replaced by a
glass stopper and the water bath is replaced by an
oil bath. The mixture is heated at 110°C with stirring for 5–6 hr.
Excess
phosphorus oxychloride is removed as well as possible with a
rotary evaporator under reduced pressure. The residue is cooled to room temperature and
300 mL of diethyl ether is added. The mixture is poured into a
separatory funnel.
Hexane is added until the two phases separate cleanly and the funnel is shaken vigorously. The phases are separated and the lower layer is extracted with three
250-mL portions of ether (Note
4). The combined organic layers are washed with
300 mL of cold aqueous 10% hydrochloric acid and
200 mL of aqueous 5% sodium hydroxide (Note
5) and then concentrated carefully with a rotary evaporator to give
136–156 g (
70–87%) of crude
diethyl 2-chloro-2-cyclopropylethene-1,1-dicarboxylate.
2
B. The crude chloromalonate is dissolved in
100 mL of 95% ethanol and transferred to a
1-L, round-bottomed flask equipped with a
magnetic stirring bar. Stirring is begun and a solution of
potassium hydroxide in 350 mL of 95% ethanol (0.0035 mol of potassium hydroxide per gram of chloromalonate) (Note
6) is added dropwise from an
additional funnel. A slightly exothermic reaction is noted. After the addition is complete, the mixture is stirred for 3 hr (or until the mixture is neutral to litmus; (Note
7)). Excess
ethanol is removed with a rotary evaporator under reduced pressure and the residue is dissolved in 300 mL of water and extracted with
350 mL of ether (Note
8). The phases are separated and some ice is added to the aqueous phase. The cooled aqueous phase is acidified with concentrated
hydrochloric acid and extracted with three
300-mL portions of ether. The
ether phase is dried with anhydrous
sodium sulfate, filtered, and concentrated under reduced pressure with a rotary evaporator to give 72–94 g (70–80%) of crude monoester.
C.
Ethyl cyclopropylpropiolate. The crude product is transferred to a
500-mL, round-bottomed flask equipped with a magnetic stirring bar and a reflux condenser. A solution of
0.70 mL of triethylamine (Note
9) per gram of crude monoester from Part B in about
200 mL of toluene is added. The mixture is heated using an oil bath at 90°C with stirring until the evolution of
carbon dioxide has subsided, and is then heated for another hour (Note
10). The mixture is cooled to room temperature, and washed with
300 mL of aqueous 10% hydrochloric acid (Note
11) and finally with
300 mL of aqueous 5% sodium carbonate. The organic layer is dried with anhydrous
sodium sulfate, filtered, and concentrated under reduced pressure with a rotary evaporator. Fractional distillation of the residue gives the product, 87–95°C at 10 mm. The yield of the final step is
30–46 g (
66–78%); the overall yield is
33–54% (Note
12).
2. Notes
1.
Diethyl cyclopropylcarbonylmalonate is prepared by the procedure of Price and Tarbell
3 or Reynolds and Hauser.
4 On scale-up the checkers found that a slight modification is necessary. The procedure of Price and Tarbell was used:
3 45 g (1.9 mol) of magnesium turnings,
1 mL of carbon tetrachloride, and approximately
20 mL of a solution of 281 mL (269 g, 1.9 mol) of diethyl malonate in
148 mL of absolute ethanol were combined. After the reaction begins, the addition of
diethyl malonate solution is completed so that the reaction is maintained at a fairly vigorous rate. If the reaction subsides prior to the completion of the addition of the
diethyl malonate solution, the addition is interrupted and a portion
(300–400 mL) of the specified 550 mL of dry ether is added cautiously until the reaction resumes, whereupon the addition of the
diethyl malonate solution is resumed. After the remainder of the
diethyl malonate solution has been added and the reaction mixture cooled, the remaining dry ether is added cautiously and the mixture is worked up as described
3 using
350 mL of dry benzene. The residue is dissolved in
550 mL of dry ether and treated as described by Reynolds and Hauser
4 with
168 mL (194 g, 1.9 mol) of cyclopropanecarboxylic acid chloride in
230 mL of dry ether. After the addition is completed, an additional
40 mL of dry ether is added and the mixture is cooled and worked up as described
4 using
2 L of aqueous 25% sulfuric acid,
800 mL of ether,
600 mL of saturated aqueous sodium bicarbonate, 200 mL of water, and
100 mL of brine. The crude product is distilled (85–95°C; 0.05 mm) and
362 g (1.6 mol,
86%) of a clear liquid is obtained.
1H NMR δ: 1.01 (m, 2 H), 1.20 (m, 2 H), 1.31 (t, 6 H,
J = 7.1), 2.12 (tt, 1 H,
J = 4.5, 7.8), 4.28 (q, 4 H,
J = 7.1), 4.58 (s, 1 H).
4. Extraction with a mixture of
ether and
hexane is repeated until
ether and the lower layer readily separate.
7. Dilution of 1 mL of the mixture in 5 mL of water gave pH 7–8.
8. The
ether phase is dried with anhydrous
sodium sulfate, filtered, and concentrated with a rotary evaporator to give 32–46 g of recovered starting material.
10. The checkers found that this process requires approximately 24 hr.
12. Cyclopropylpropiolic acid ethyl ester has the following spectra:
1H NMR (CCl
4) δ: 0.84 and 0.93 (4 H, ring CH
2), 1.25 (t, 3 H, CH
3 ester), the ring–CH is hidden under the ester CH
3-triplet, 4.05 (q, 2 H, CH
2 ester); IR (CCl
4) cm
−1: 2220 (C

C), m, 1710 (C=O), s, 1255 (C-O-C), s, 1030–1040 two bands (cyclopropyl), m, and 860–880 two bands (cyclopropyl), w; MS: M (calculated for C
8H
10O
2) 138.068, M
+ is not readily detected, 94 (20%), 93 (100%), 66 (65%), 65 (53%), 63 (10%), 53 (15%), 40 (10%).
3. Discussion
Substituted cyclopropyl rings conjugated with a triple-bond system have recently received attention as C
5 building blocks.
5 The procedure described here is a modification of the decarboxylation–elimination reaction for the preparation of α,β acetylenic acids from enol sulfonates of acyl malonates.
6,7,8 Addition of aqueous alkali to the enol sulfonate of
diethyl cyclopropylcarbonylmalonate gives
cyclopropylpropiolic acid, but the yield is low.
The major advantages of this procedure over the enol sulfonate procedure lie in the availability of
diethyl 2-chloro-2-cyclopropylethene-1,1-dicarboxylate from the corresponding acylmalonate and
phosphorus oxychloride, and the fast, homogeneous, decarboxylative elimination reaction of the triethylamine salt of the half-ester in dry organic solvents. The conditions described here, with slight modifications (overnight treatment), have been used for a variety of β-chloro alkylidene/arylidene malonates as shown in Table I.
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