[www.rhodium.ws] [] [Chemistry Archive]
 
 

Para-Selective Oxychlorination of Aromatic Compounds Using Potassium Chloride and Oxone

N. Narender, P. Srinivasu, S. J. Kulkarni, K. V. Raghavan
Synth. Commun. 32(2), 279-286 (2002)

HTML by Rhodium

Abstract

A highly efficient, regioselective method for oxychlorination of aromatic compounds is possible through electrophilic substitution of chlorine generated in situ from KCl as a chlorine source and Oxone as an oxidant for the first time.

Chlorinated aromatic compounds have a wide diversity of uses. They can serve as precursors for numerous functionalities, such as phenols aromatic ethers and thioethers, amines, arylhydrazines, benzonitriles, fluoroaromatic, silylated aromatics and aromatic hydrocarbons.1 The chlorination of aromatic compounds has been extensively described using many reagents,2 such as molecular chlorine,3 sulfuryl chloride,4 alkyl and acyl hypochlorites,5 inorganic chlorides,6 KCl/m-CPBA/18-crown-6,7 KCl/NaBO3/Na2WO4,8 KCl/H2O2/NH4VO3,9 N-chloro-succinimide,10 benzyltrimethyl ammonium tetrachloroiodate (BTMAICl4),11 dichlorinemonoxide (Cl2O),12 PhICl2 in trifluoroacetic acid13 and N-chloroamines,14 N-chloroamides and N-chlorosulfonamides.15 The methods reported have some limitations such as use of strong and non-selective chlorinating agents, toxic and expensive reagents, low yields and long reaction times.

Industrial synthesis of chloroarenes are commonly performed with molecular chlorine in the presence of Lewis or mineral acids at 20–80°C.16 Catalysts such as aluminium(III), iron(III), tin(IV) or zinc(II) chlorides, to name just a few, have been used widely.17 The major disadvantages are poor regioselectivities, corrosion caused by the highly reactive species and hydrogen chloride side product and disposal problems. Thus, a great deal of efforts are being directed toward carrying out the chlorination of arenes in the gas and liquid phases using alumino-silicate catalysts, especially zeolites, in order to achieve better selectivities under milder conditions.18 Irreversible damage caused to the zeolites by hydrogen chloride is, however, a stumbling block, so that industrial applications are still rare. To overcome these difficulties some researchers have utilized a combination of hydrochloric acid and suitable oxidant19 such as tert-butyl hydroperoxide, hydrogen peroxide or m-chloroperbenzoic acid, which in situ generates positive chlorine species for the chlorination of aromatic substrates.

In this communication we report a new method for the para selective (regioselective) oxychlorination of aromatic compounds using commercially available Oxone as an oxidant and KCl as a chlorine source. We observed smooth chlorinations in acetonitrile without any additional catalyst.

Scheme 1

A number of different aromatic substrates were subjected to the chlorination reaction to test the generality of this method and the results are summarized in Table 1. These reactions proceeded efficiently under mild conditions in acetonitrile with high yields and regioselectivity with KCl and Oxone. Potassium peroxymonosulfate is an inexpensive and readily accessible oxidizing agent. It is commonly used as Oxone (2KHSO5·KHSO4·K2SO4) and is a versatile oxidant for the transformation of a wide range of functional groups.20 The results shown in Table 1 indicate that the reaction is successful for a variety of aromatic compounds.

Table 1.
Regioselective Oxychlorination of Aromatic Compounds with KCl and Oxone in Acetonitrile1a

[Table missing. If found, please email it to me]

  1. Substrate (2 mmol), KCl (2.2 mmol), Oxone (2.2 mmol), CH3CN (10 ml), r.t.
  2. The products were characterised by NMR, Mass, GC analysis.

Introduction of an electron-withdrawing group on the aromatic ring substantially decreases the rate of ring chlorination (Table 1, Entries 7 and 10) while on electron donating group increases it. As is evident from the Table 1 aromatic substrates of greater, moderate reactivity ex. methoxy, hydroxy and alkyl benzenes react readily with KCl/Oxone to give essentially quantitative yields of the monochloro derivatives with high para selectivity with little or no tendency to polychlorination. Less reactive substrates such as nitrobenzene, chlorobenzene, benzoic acid could not be chlorinated even at elevated temperature (80°C). In the case of 2-nitrophenol the corresponding monochloro phenol (4-chloro-2-nitrophenol) was obtained in moderate yields.

Table 2.
Aromatic Oxychlorination with 2.2 eq. KCl/Oxone in MeCN3a

Entry
Substrate
Time
Conv.
Yield4b
Para
Ortho
Di
Other
1
Anisole
15 h
100%
12%
81%
7%
2
Phenol
15 h
100%
20%
2%
78%
3
Acetanilide
15 h
100%
12%
61%
27%
4
Toluene
24 h
100%
68%
29%
3%
  1. Substrate (2 mmol), KCl (4.4 mmol),
    Oxone (4.4 mmol), CH3CN (10 ml), r.t.
  2. The products were characterised by NMR, MS, GC.

The results show that chlorination of toluene (Table 2, Entry 4) with two fold excess of KCl and Oxone afforded (mono) 2- and 4-chlorotoluene in 97% yield and a small amount (3%) of 2,4-dichlorotoluene, whereas anisole, phenol and acetanilide (Table 2, Entries 1–3) furnished dichlorinated compounds as a major products along with a small amount of monochlorinated compounds. The interesting difference between highly activated aromatics gives the dichlorinated compounds whereas moderately activated aromatics gives the monochlorinated compounds. Then, we can selectively prepare the desired chloro-substituted compound by using calculated amount of KCl and Oxone in case of highly activated aromatics. A wide range of solvents has been employed in these reactions (Table 3), including carbon tetrachloride, hexane, dichloromethane, methanol and acetonitrile. However, the yields, rates of reaction and degree of paraselectivity generally appeared to be optimum in acetonitrile.

Table 3.
The Effect of Solvent on the Oxychlorination
of Anisole Using KCl-Oxone System5a

Entry
Solvent
Time
Conv.
Yield6b
Para
Ortho
Di
1
Acetonitrile
15 h
98%
90%
8%
2
Methanol
15 h
97%
72%
24%
1%
3
Dichloro-
methane
15 h
5%
5%
4
Carbon
Tetrachloride
15 h
5
Hexane
15 h
  1. Anisole (2 mmol), KCl (2.2 mmol),
    Oxone (2.2 mmol), Solvent (10 ml), r.t.
  2. The products were characterised
    by NMR, Mass and GC analysis.

Two experimental parameters deserve emphasis. First, the nature of the solvent has a dramatic influence on the regioselectivity. Switching from the non-polar carbon tetrachloride (polarity = 0.0D) to the strongly polar acetonitrile (polarity = 3.92D) results in a change of yields from 0 to 98% for anisole chlorination. Even greater paraselectivity (para/ortho up to 90/8) was obtained by using acetonitrile as a solvent compared to methanol. Secondly, the nature of oxidant used has a dramatic influence on the yields and selectivity. We surveyed the oxychlorination with various oxidants. Reactions were conducted with anisole as a probe-substrate at room temperature in acetonitrile. However, Oxone is far superior to the other oxidants for example, H2O2 give little of the product and TBHP and molecular O2 showed no sign of reaction after 15 h. The best oxidant is Oxone from the standpoint of highest yield and selectivity.

The reaction proceeds efficiently in high yields at ambient temperature and pressure. The role of Oxone was confirmed by conducting a blank experiment, where the formation of chloro compound was not observed.

A typical oxychlorination of an aromatic compound in the presence of Oxone proceeds according to the stoichiometry of Equation 1. It is believed that the chlorination proceeds via the formation of hypochlorous acid. The hypochlorous acid has higher instability due to pronounced ionic nature and thus more reactivity towards the aromatic nucleus. The absence of chlorination of the ring methyl group (Table 1, Entries 9–13) is indicative of the electrophilic mechanism of the reaction rather than a radical pathway. Furthermore, chlorination of alkylbenzenes gives large amounts of benzyl chlorides as side products,21 such drawbacks could be avoided using this system.

Equations
  1. ArH + KCl + 2 KHSO5·KHSO4·K2SO4 ArCl + KOH + K2S2O8·KHSO4·K2SO4 + H2O
  2. 2 KHSO5·KHSO4·K2SO4 + KCl KOH + HOCl + K2S2O8·KHSO4·K2SO4
  3. 2 HOOSO3K 2 HO· + 2 ·OSO3K
  4. KCl + HO· + 2 ·OSO3K KOH + HOCl + K2S2O8
  5. ArH + HOCl ArCl + H2O

In conclusion, we have developed a novel system for the regioselective oxychlorination of aromatic compounds by using KCl and Oxone in acetonitrile under ambient conditions. The results reported here demonstrate that reagent system possess considerable practical advantages over traditional reagents for electrophilic chlorination reactions. The commercial availability of the reagents and reactions are clean, high yielding and work-up is simple. The absence of side chain chlorination products in reaction conducted in acetonitrile suggests a substantial increase in the rate of the ionic process. We are currently extending this methodology to other halogenation reactions.

Experimental

General Procedure for the Chlorination of Aromatic Compounds

Oxone (2.2 mmol) was added to a well stirred solution of KCl (2.2 mmol) and substrate (2 mmol) in acetonitrile (10 ml) and the reaction mixture was allowed to stir at room temperature. The reaction was monitered by thin layer chromatography (TLC). After the completion of the reaction, the mixture was filtered and solvent evaporated under reduced pressure. The products were purified by column chromatography over silica gel and confirmed by 1H NMR and Mass spectra.

References

  1. Krumenacker L., Ratton S., L'actualite Chemique., 6 (1986) 29.
  2.  
    1. Happer D.A.R., Vaughan J. The Chemistry of the Hydroxyl Group, Patai S. Part 1, Interscience Publishers, New York, 1971, p. pp. 418.
    2. Stroh R. Methoden der Organischen Chemie, (Houben-Weyl), Muller E. Bd. V/3.S., George Thieme Verlag Stuttgart, Stuttgart, 1962, p. pp. 679.
  3.  
    1. Huston R.H., Neeley A.H., J. Am. Chem. Soc., 57 (1935) 2176.
    2. Harvey D.R., Norman R.O.C., J. Chem. Soc., (1961) 3604.
  4.  
    1. Hojo M., Masuda R., Synth. Commun., 5 (1975) 169.
    2. Delaude L., Laszlo P., J. Org. Chem., 55 (1990) 5260.
    3. Bolton R., De la Mare P.B.D., J. Chem. Soc. B., (1967) 1044.
  5.  
    1. Anbar M., Ginsburg D., Chem. Rev., 54 (1954) 925.
    2. Ginsburg D., J. Am. Chem. Soc., 73 (1951) 2723.
    3. Smith K., Butters M., Paget W.E., J. Chem. Soc., Chem. Commun., (1985) 1155.
    4. Lengyel I., Cesare V., Stephani R., Synth. Commun., 28 (10) , (1998) 1891.
    5. Smith K., Butters M., J. Chem. Soc., Chem. Commun., (1985) 1157.
  6.  
    1. Masilamani D., Rogic M.M., J. Org. Chem., 46 (1981) 4486.
    2. Stebnik M., Mechoulam R., Yoha I., J. Chem. Soc., Perkin Trans, I (1987) 1423.
    3. Kosower E.M., Cole W.J., Wu G.-S., Cardy D.E., Meisters G., J. Org. Chem., 28 (1963) 630.
    4. Lubbecke H., Bolt P., Tetrahedron, 34 (1978) 1577.
  7. Usami N., Kobana K., Yoshida H., Kimura T., Watanabe K., Yoshimura H., Yamamoto I., Chem. Pharm. Bull., 46 (1998) 1462–1467.
  8. Bandgar B.P., Nigal N.J., Synth. Commun., 28 (1998) 3225–3229.
  9. Hegde V.R., Pais G.C.G., Kumar R., Kumar P., Pandey B., J. Chem. Res(S), (1996) 62–63.
  10.  
    1. Goldberg Y., Alper H., J. Mol. Catal., 88 (1994) 377.
    2. Lambert F.L., Elllis W.D., Parry R.J., J. Org. Chem., 30 (1965) 304.
  11. Kajigaeshi S., Shinmasu Y., Fujisaki S., Kakinami T., Bull. Chem. Soc., Jpn., 63 (1990) 941.
  12. Marsh F.D., Farnham W.B., Sam D.J., Smart B.E., J. Am. Chem. Soc., 104 (1982) 4680.
  13. Andrews L.J., Keefer R.M., J. Am. Chem. Soc., 82 (1960) 5823.
  14. Lindsay Smith J.R., McKeer L.C., Taylor J.M., J. Chem. Soc., Perkins Trans., 2, 1533 (1987);
    Ibid. 385 (1988); Ibid. 1529 (1989); Ibid. 1537 (1989)
  15. Boronsombat P., McNelis E., Synthesis, (1993) 237.
  16.  
    1. De la Mare P.B.D. Electrophilic Halogenation, Cambridge University Press, Cambridge, 1976.
    2. Taylor R. Electrophilic Aromatic Substitution, p. 362 (1990) Wiley, Chichester.
  17. Wiegandt H.F., Lantos P.R., Ind. Eng. Chem., 43 (1951) 2167.
  18. Holderlich W., Hesse M., Naumann F., Angew. Chem., Int. Ed. Engl., 27 (1988) 226.
  19.  
    1. Barhate N.B., Gajare A.S., Wakharkar R.D., Bedekar A.V., Tetrahedron Lett., 39 (1998) 6349.
    2. Chung K.H., Kim K.M., Kim J.N., Ryu E.K., Synth. Commun., 21 (1991) 1917.
    3. Chung K.H., Kim H.J., Kim H.R., Ryu E.K., Synth. Commun., 20 (1990) 2991.
  20. Webb K.S., Levy D., Tetrahedron Lett., 36 (1995) 5117 and references cited therein.
  21. Van Dijk J., Van Daalen J.J., Paerels G.B., Recl. Trav. Chim. Pays-Bas., 93 (1974) 72.