CALIXARENE COMPOUNDS

BACKGROUND OF THE INVENTION

1. Field of the Invention

The present invention is related to calixarenes and their preparation. More specifically, it is directed to a new and useful method for the preparation of known as well as of new calixarenes. The invention further aims at the new calixarenes obtained and at an installation for synthesiz- ing calixarenes.

Calixarenes are cyclic phenolic oligomers wherein two suc¬ ceeding phenol rings are linked together by an ortho-ortho C__ ₂ bridge or an analogous homo CH bridge. Some calixare¬ nes have already been known, in particular the tetramers, hexamers and octamers as well as several calixarenes having an odd number of rings in their molecule.

The calixarenes have found several applications in indus¬ try; ^_ they are for example used as starting materials for solid foams, as capturing agents for other, small mole- cules, as reactants for confining waste or dangerous sol¬ ids, etc.

2. Description of the Prior Art

As it has already been mentioned above, some calixarenes are already known, see, e.g., the work of Gutsche et al. in Org.Syn. 1989, 68, 234; Niederl and Vogel in J.Am.Chem.Soc. 1990, 62, 2512, and Hogberg in J.Am.Chem.Soc. 1980, 102, 6046. p-Methylcalix[4] arene has already been synthesized

in 1956 by a ten-step synthesis method using brominated in¬ termediates. This methods has been taken over and devel¬ oped in order to prepare linear phenolic oligomers which are then cyclized for yielding calixarenes having an even or odd number of phenolic rings, sometimes differently sub¬ stituted, or asymmetric calixarenes (see, e.g., V. Bδhmer et al., Makromol.Chem. 180, 2503-06 (1979) , who however only discloses cyclic tetramers) . In all cases, the syn¬ theses are long-lasting and give very low yields only.

In 1981, a critical review of the two most common methods for synthesizing calixarenes has been published by CD. Gutsche and co-workers in J.Am.Chem.Soc. 1981, 103, 3782- 92. These two methods are a one-step method, called Munch method, and a three-step method, called Zinke method.

In the Munch method, a mixture containing p- tert- butylphenol, paraformaldehyde, and potassium hydroxide in an approximate ratio of 45:75:1 is heated during 4 hours in a xylene solution that is approximately 1.3 M in phenol, using a Dean and Stark trap to remove water. Typically, a colorless, xylene insoluble product is obtained in about

75% yield. This product contains linear phenolic oligomers and p-tert-butylcalix [8] arene (45%) whereas the 6- and 4- calixarene homologues can be isolated in small amounts

(i.e. 9.5% and 9%, respectively) from the mother liquor.

The Zinke method comprises warming a mixture of the above mentioned starting materials during about 45 hours to 50-55 °C and then for about 2 hours to 110-120 °C. Then, the re¬ action mixture is acidified, the separated solids are re¬ moved, and the washed and dried solids are heated for about 2 hours in a high-boiling liquid to about 210-220 °C. This methods principally yields cyclic tetramer and small amounts of hexamer and octamer. It has also been proposed

by Gutsche, see the document cited in the preceding para¬ graph, to combine the first two steps of this method.

European patent application No. 0,447,977 discloses a one- step method for the preparation of cyclic phenolic tetra- mers by heating a precondensate of p-alkylphenols and form¬ aldehyde or an alkylcalix [8] arene together with an aqueous alkali metal hydroxide during about 1 to 10 hours at 217 to 257 °C in a hydrocarbon solvent. This variant of the Zinke method only yields cyclic tetramer in a yield of 50 to 60% only.

Finally, attempts have been made to synthesize calixarenes comprising an odd number of rings in their molecule. Thus, A.Ninagawa suggests in Makromol . Chem. , Rapid Commun. 3, 65- 67 (1982) the isolation of the cyclic pentamer from the re- action product of the first two steps of a modified Zinke method. According to Y.Nakamoto [Makromol .Chem. , Rapid Commun. 3, 705-07 (1982)] , the heptamer was obtained in low yield from the solid reaction product of p-tert- butylphenol, paraformaldehyde and potassium hydroxide after refluxing this mixture for 30 hours in dioxane.

SUMMARY OF THE INVENTION

The methods of the prior art discussed above suffer from several severe drawbacks . No one of these methods can be used to prepare a desired calixarene in high yields on an industrial scale since on one hand, these known methods are either too time consuming and require a great number of separating, washing, drying and isolating operations, or they only give calixarenes in an industrially unsatisfac¬ torily low yield, on the other hand, or both.

The first and major object of the present invention is to provide a universal method which allows the manufacture of any desired calixarene on an industrial scale. Another ob¬ ject is to provide such a method which is simple, comprises relatively few process steps, and gives satisfactory yields of calixarene. Further, still another object of the inven¬ tion is to provide a method which permits the preparation of any desired calixarene by appropriately selecting the respective starting materials without undue changes in re- action conditions and parameters.

Still a further object of the invention is to provide a useful installation for the preparation of a great variety of calixarenes on a laboratory or an industrial scale. And still another object of the invention is to provide novel compounds of the calixarene family.

These objects are attained by the process of the invention which is a two-step process although both steps need not be performed in separate reaction vessels. The first step of the process comprises the synthesis of linear phenolic oli- go ers in a basic reaction medium, starting from a phenol source and a formaldehyde source, and the second step com¬ prises the cyclization of these linear oligomers in a sub¬ stantially water-free, neutral or acidic medium, the linear oligomers obtained in the first step not being isolated.

Basically, it will not be required to use another reaction medium when passing from the first to the second step; it will be sufficient to adapt the reaction medium used in the first step to the conditions required in the second step. For example, when the first step is conducted in an aque- ous, a base containing medium without completely removing the water from it, the second step can be started after neutralization or, if desired, acidification and adding a

desired solvent, typically an organic, higher boiling one that is preferably not miscible with water, and remaining water as well as reaction water will be removed during the operation by means of a well known Dean-Stark water trap. Neutralization or acidification may be effected before or after starting the second step of the process.

The linear phenolic oligomers obtained in the first step are generally not isolated from the reaction mixture for cyclization in the second step. However, it may sometimes be desirable to precipitate them from the reaction medium for purification or analysis purposes.

Typically, the first step is conducted at temperatures in the range of from 40 to 150 °C, in most cases and when an aqueous medium is used, between 50 and 90 °C or at the boiling point of the medium. The second step is typically operated at temperatures well above 100 °C. It is pre¬ ferred to carry out the cyclization in using an organic liquid as a reaction medium such as toluene, xylenes, tetraline, petrol fractions of appropriate boiling range, diphenyl ether, etc. The liquid may be a solvent or not; its nature is not at all critical as far as it does not im¬ pair the cyclization. Sometimes, it is advantageous to use polar liquids such as dimethylsulfoxide, diethylformamide, etc.

Starting materials for the process of this invention are the already known ones for the calixarene synthesis, namely a para substituted phenol. This para substituent is pref¬ erably an alkyl or aralkyl group such as methyl, ethyl, propyl, isopropyl, the butyls, tert-octyl, benzyl, etc. Specially preferred is tert-butyl. This substituent is be¬ fore all, if it is not desired as such to be present in the final calixarene, a para protecting group in order to force

oligomerization and cyclization reactions to occur in the ortho positio (s) to the phenolic OH group. The second starting material is formaldehyde. Since the first step of the present process is often carried out in an aqueous me- dium, formalin or for ol (an aqueous solution of formalde¬ hyde at normally 37%) can be used. If it is desired to have a higher formaldehyde concentration in the reaction medium, paraformaldehyde may be used alone or together with formol. It will also possible to introduce gaseous formal- dehyde into the reaction medium.

The first step of the process requires a basic medium. Thus, a base should be added. Suitable bases are NaOH and KOH. In some cases, other bases, alone or mixed with oth¬ ers, will be used, such as LiOH, CsOH, RbOH, (CH ₃ ) ₃ COK, [CH ₃ (CH ₂ ) ₃ ] ₄ NOH or still others. The proper choice of the base depend on the optimization of the reaction in terms of yield and selectivity.

During the first step of the present process, linear pheno¬ lic oligomers are formed. Generally, a mixture is obtained containing oligomers comprising between 2 and 6 monomeric phenolic units and still momoraeric phenol. The number of phenolic units in the oligomer is generally influenced by reaction conditions such as temperature, duration, relative concentration of the reactants, the nature and sometimes the amount of the base used. Typically, the chain of the oligomers will become longer when the reaction time is in¬ creased and also the formaldehyde-phenol ratio. The yield and the nature of the oligomers can be influenced when the reaction temperature is increased, in particular above 100 °C.

The reactions that occur during the second step of the pre¬ sent process are also already known per se. However, it

has quite surprisingly been found that, when monomeric phe¬ nol or another oligomer than that contained in the reaction mixture and, optionally, formaldehyde is added to the starting mixture for the second step, a calixarene having an odd number of phenolic units m the cycle, a calixarene having more than 8 units m the cycle, and/or even an asym¬ metric calixarene can be obtained. All these compounds have only been, at most, minor by-products of the known cy¬ clization reactions, or were completely unknown.

The attached drawing shows reaction diagrams being at the base of the present process, and further schematically the different synthesis possibilities. An installation for carrying out the process of the invention is also shown.

BRIEF DESCRIPTION OF THE DRAWING

In the drawing,

FIG. 1A and IB is a reaction diagram showing the formation mechanism of p-tert-butylcalix [6]arene starting from linear oligomers;

FIG. 2A and 2B is a reaction diagram showing the formation mechanism of p-tert-butylcalix[8]arene starting from linear oligomers;

FIG. 3 is an overview showing some possibilities of the syntheses when using the process of the invention;

FIG. 4 shows, as an Example, some structural formulae of the calixarenes to be prepared; and

FIG. 5 schematically shows an installation for carrying out the process of the present invention.

DETAILED DESCRIPTION OF THE INVENTION

According to the experimental conditions which are used, different combinations, organizations and reactions between linear oligomers are possible in the process of this inven¬ tion. Thus, certain calixarenes are formed during the cy¬ clization of a sole linear oligomer (pseudocalixarene route) whereas others result from the combination of two identical or different linear oligomers (hemicalixarene route), as shown in the following diagrams.

A) p-tert-Butylcalix[6]arene, pseudocalixarene route:

B) p-tert-Butylcalix [ 8 _ areι_e, hemicalixarene route :

hemicalix[8]arene p-tert-butylcalix(8]arene

The diagrams shown in FIG. 1 and 2 do not need any detailed explanation; it can easily be seen how a linear oligomer is first be formed which is then cyclized, see the last line

of the diagrams. In FIG. 1, this cyclization runs the pseudocalixarene route whereas in FIG. 2, the cyclization follows the hemicalixarene route.

FIG. 3 shows some examples of the possibilities of the syn- theses and preparations disclosed herein; this diagram is by no way exhaustive. Starting from a para substituted phenol and a formaldehyde source, different linear oli¬ gomers can be prepared. Following the two routes described above, a great variety of calixarenes can be synthesized by cyclization from identical or different linear oligomers, with optional addition of monomeric phenolic compounds.

FIG. 4 shows as an example the structural formula of three calixarene compounds that can be prepared according to the process of the present invention, together with their sys- temic nomenclature.

The abbreviations that are used in FIG. 3 and FIG. 4 and in the following description are the following:

1 p-tert-butylphenol ("monomer") , optional substituted in meta position to the OH group

1 ^A o-hydroxymethyl-p-tert-butylphenol ("hydroxymethyl monomer") ^Λ 1 ^Λ "o,o-dihydroxymethyl monomer"

2 o,o' -methylene-p,p' -di- ert-butyldiphenol ("dimer") 2 ^Λ o,o' -methylene-o-hydroxymethyl-p,p' -di- tert- butyldiphenol ("hydroxymethyl dimer")

^A 2 ^A o,o' -methylene-0,0 ¹ -dihydroxyτnethyl-p,p' -di-tert- butyldiphenol ("dihydroxymethyl dimer") , etc. 4+ p-tert-butylcalix[4] arene

40+ p-tert-butyldihomooxacalix [4] arene

4θΛ p-isopropyldihomooxacalix[4] arene nH calix [n] arene, unsubstituted in para position

Generally: digit = number of phenolic units; H = para un- substituted; ^A = hydroxymethyl; + = p-ter -butyl; Λ = p- isopropyl; O = dihomooxa

The diagram of FIG. 3 is not limitative nor exhaustive since, for example, the p-tert-butyl substituent shown may be replaced by any other one, e.g. isopropyl, and the dia- gram does not contain all possible reactions or products which can be prepared. The diagram rather shows that the present invention provides a process for the controlled and basically selective synthesis of any desired particular calixarene compound.

As it has already been stated above in part, the present invention provides also novel compounds. All oligomers and calixarenes that are para substituted by an isopropyl group have not yet been described. Most asymmetric calixarenes are also new compounds. Furthermore, all calixarenes com- prising more than 8 phenolic units in their molecule are new compounds, be they even or odd calixarenes.

FIG. 5 schematically shows an installation allowing the re¬ alization of the process of this invention. Of course, the dimensions of the individual parts of the installation may vary in order to adapt it to a preparation on a laboratory scale, an intermediate scale, or an industrial process.

The installation comprises two substantially identical re¬ action units 10 and 20. In unit 20, the parts bearing a reference numeral where an "A" has been added, are similar or identical to the corresponding parts of unit 10 and are described together.

Each reaction unit 10; 20 comprises a reactor 32; 32A, re¬ spectively, having a double shell for heating and cooling by circulating an appropriate heat transfer fluid. The re¬ actors 32, 32A are equipped with a temperature measuring and recording device 33; 33A, a storage tank 12; 12A for the phenol (s) and/or the precursors, a formol storage ves¬ sel 14; 14A, a catalyst storage vessel 16; 16A, a storage tank with preheating means 22; 22A for solvents, and a res¬ ervoir 18; 18A for inert gas. Further, reactors 32; 32A are equipped with a motor driven stirring device 28; 28A and a Dean-Stark system for water removal; this system com¬ prises a condenser 24; 24A connected by a pipe 26; 26A to the reactor 32; 32A, and by another conduit to a receptacle for condensed water 30; 30A.

The reactors 32; 32A can be emptied into a collecting basin 36; 36A. A pump 38; 38A is provided for sending the prod¬ uct from the collecting basin 36A to a purification equip¬ ment (not shown) or to other post-treatment stages. Fi¬ nally, the first collecting basin 36 has a conduit 37 that leads to the second reactor 32A.

The functioning of the installation is quite evident and will further be explained in the following Examples which illustrate and explain the invention in more detail but which are not to be understood to limit the invention in any way.

Example 1

A. Synthesis of the linear dihydroxymethylated ( ^Λ 4 ^Λ ) and monohydroxy ethylated ( ^A 4) tetramer

The reactor 32 of part 10 of the installation (see FIG. 1) , is charged with 20 g (0.133 mole) of p-tert-butylphenol,

12.4 ml (0.166 mole) of 37% formol, and 0.24 g (0.006 mole)

of solid 98% NaOH. The reaction mixture is heated to 110 °C under stirring for 2 hours, finally yielding a viscous mass containing about 40% of linear phenolic tetramers, namely the compounds 4 ^Λ and ^Λ 4 ^A , the remainder being dimers and the monomer.

B. Synthesis of p-tert-butylcalix[4]arene (4+)

The reaction mixture obtained in Example 1A above is trans¬ ferred into reactor 32A of installation part 20. Dry HC1 gas is pearled through the mixture until neutrality. Then, 200 ml of hot diphenyl ether are added under stirring. The reaction mixture is heated to reflux for about 2 hours. After cooling, allowing a precipitate to form, addition of ethyl acetate, filtering, washing, dissolution in toluene and concentration, virtually pure p-tert-butylcalix[4]arene is obtained in a 49% yield.

Example

A. Synthesis of the linear dihydroxymethylated hexamer ( ^A 6 ^Λ )

The reactor 32 of part 10 of the installation (see FIG. 1) , is charged with 20 g (0.133 mole) of p- ert-butylphenol, 27 ml (0.36 mole) of 37% formol, and 3 g (0.045 mole) of 84% KOH pastilles. This mixture is heated under stirring until the formation of a dry mass.

A sample thereof is dissolved in cold CHCI ₃ , and the solu- tion is neutralized with concentrated hydrochloric acid. After evaporation to dryness and analysis, it is found that the above reaction has given the ^A 6 ^Λ compound with a yield of 80 to 90%.

B. Synthesis of p-tert-butylcalix[6] arene (6+)

The yellow dry residue in reactor 32, obtained in Example 2A, is treated with or tho-xylene, and the suspension ob¬ tained is transferred after neutralization into reactor 32A. The reaction mixture is refluxed for 3 hours while stirring and is filtered after cooling. The solid obtained on the filter is dissolved in chloroform, then treated by hydrochloric acid, and the organic layer is concentrated to 200 ml. 200 ml of hot acetone are added. After cooling and filtration, p-tert-butylcalix[6]arene is recovered in a 80 to 90% yield.

Example 3

Synthesis of p-tert-butylcalix[7] arene (7+)

In this Example, the cyclization is effected as a second stage immediately after the oligomerization in the same re¬ actor.

First, the dihydroxymethylated linear oligomer ^Λ 6 ^A is pre¬ pared in reactor 32. This reactor is charged with 10 g (66.5 mmole) of p- ert-butylphenol, 18.83 ml (250.6 mmole) of 37% formol, and 0.63 g (15 mmole) of LiOH.H ₂ 0 under stirring. This mixture is heated, the water is removed in the Dean-Stark trap 24 and 30, and a solid yellow dry crust is obtained comprising linear oligomer.

The subsequent cyclization step is carried out in the same reactor 32 in the presence of an additional monomer. A so¬ lution of 1.792 g (11.95 mmole) of p- ert-butylphenol in 25 ml xylene is added to the crust in the reactor 32; then, 75 ml of more xylene, saturated with dry gaseous HC1, are added. This reaction mixture is refluxed for 3 hours. Af-

ter purification, p- ert-butylcali [7] arene is recovered in an 11% yield .

Example

Synthesis of calix[6]arene (6H)

This Example illustrates the preparation of an unsubsti- tuted calixarene by dealkylation.

1.46 g (1.5 mmole) of p-tert-butylcalix[6] arene, obtained e.g. according Example 2, 0.84 g (8.93 mmole) of phenol, 1.68 g (12.53 mmole) of AICI ₃ , and 22 ml of toluene are mixed in reactor 32 in a nitrogen atmosphere. The mixture is stirred at room temperature for 4 hours, and 32 ml of 3N HCl are the added to the reaction mixture which is then transferred into reactor 32A. After another 2 hours of stirring, the mixture is filtered and the residue is washed and dried. After recrystallization, calix[6]arene is ob¬ tained in an 80% yield.

Example 5

Preparation of p-isopropyldihomooxacalix[4] arene (4θA)

This Example describes the synthesis of a compound of the p-isopropyl family and of a new calixarene.

In reactor 32, 29.92 g (0.22 mole) of p-isopropylphenol, 19.8 g (0.66 mole) of p-formaldehyde, and 150 ml of tetra- line are mixed together. 0.2 ml (0.026 mole) of 13N KOH are added. The mixture is a suspension which is vigorously stirred and heated to 150 °C. After 15 minutes at this temperature, the mixture becomes homogenous. Gaseous, dry HCl is introduced until neutrality, and the mixture is held for 2 hours at 150 °C under stirring. The mixture is then

transferred into reactor 32A. After cooling down and fil¬ tering, the mother liquors are concentrated. The addition of methanol provokes a white precipitate which allows, af¬ ter filtration, the recovery of p-isopropyldihomooxacalix- [4]arene, .p. 324-325 °C, in a 16% yield.

Example 6

Preparation of p- ert-butyldihomooxacalix [4] arene (40+)

This Example illustrates the preparation of a homooxacalix- arene, useful as intermediate for the preparation of odd or higher calixarenes.

The following materials are blended in reactor 32: 33.33 g (0.22 mole) of p- ert-butylphenol, 11.67 g (0.389 mole) of p-formaldehyde, and 200 ml of xylene. After 20 minutes of stirring, 0.667 ml (0.0667 mole) of ION NaOH is added. The reaction mixture is refluxed for 45 minutes under stirring, then transferred into reactor 32A, cooled and filtered. The filtered mixture is left standing at 10 °C for 2 to 3 days. After filtration and recrystallization, the p- ert- butyldihomooxacalix [4] arene is recovered in a 24% yield.

Example 7

Preparation of p-tert-butylcalix[5] arene (5+)

In this Example, a linear oligomer (4) is combined with a monomer, and the combination is cyclized. The linear (4) is obtained in opening the ring of compound 40+ obtained by the method of Example 6. All reactions take place in the same reaction medium.

1.6 g (2.35 mmole) of p-tert-butyldihomooxacalix[4]arene, 0.354 g (2.35 mmole) of p- ert-butylphenol, and 30 ml of tetraline are mixed under stirring in reactor 32. The re¬ action mixture is heated to 180-190 °C and, when it have become transparent, 100 μl (0.4 mmol) of KOH are added. The reaction mixture is refluxed at 200 °C during 1 hour. It is then rapidly transferred into reactor 32A, the mix¬ ture is neutralized with HCl gas, and then refluxed for an¬ other 4 hours. After evaporation to dryness in vacuo and recrystallization of the residue, p-tert-butylcalix[5]arene is obtained in a 20% yield.

Example 8

Preparation of an asymmetric calixarene

The process of this invention allows for the first time a simple preparation, without exchanging side chain substitu¬ ents as described by Boehmer et al. (see above), of asym¬ metric calixarenes, i.e. calixarenes wherein the ring mem¬ bers are not identical, in fairly good yields.

Example 7 is repeated with the exception that, for making an asymmetric calix[5]arene, the 2.35 mmole of p- ert- butylphenol added to the linear-4 oligomer, are replaced by equivalent amounts of other monomers unsubstituted in para position or substituted by another group than tert-butyl.

After evaporation of the solvent, neutralization and re- crystallization from the reaction mixture, the respective asymmetric calix[5]arene is recovered in a 5 to 15% yield.

Example 9

Preparation of p- ert-butylcalix [9] arene (9+)

This Example illustrates the preparation of another odd calixarene by combining the dihydroxymethylated linear hex- amer with the linear trimer.

A. Preparation of the linear trimer

100 g (0.66 mole) of p- ert-butylphenol and 33.33 ml (0.333 mole) of ION NaOH are charged into reactor 32. The mixture is warmed for 1 hour to 50 °C. Then, 148.5 ml (1.98 mole) of 37% formol are portionwise added. The mixture is heated for 90 minutes to 90 °C. Xylene and more p- ert- butylphenol (399 g, 2.66 mole) are added, and the mixture is refluxed for 3 hours. The mixture is acidified by add¬ ing 3.33 ml (0.0266 mole) of concentrated HCl. A sample, recrystallized from a mixture of benzene and acetone, shows that the mixture contains the linear trimer in a 65% yield.

B. Preparation of p-tert-butylcalix[9] arene (9+)

In reactor 32A, 0.025 mole of the dihydroxymethylated lin¬ ear hexamer ( ^Λ 6 ^A ) are prepared according to the method of Example 2A as a suspension in xylene. Then, a portion of the mixture in reactor 32, obtained according to part A of this Example and corresponding to 0.025 mole of the trimer, is transferred into reactor 32A. The reaction mixture, containing 200 ml of xylene, is refluxed during 3 hours for cyclization. After purification, 5% of p- ert-butylcalix- [9] arene are obtained, m.p. 297-300 °C, molecular mass 1460, ε _max = 24420 in the UV spectrum, giving the following elemental analysis:

By using the techniques of the preceding Examples, p-tert- butylcalix[10] arene has been prepared. This compound is obtained by a cyclization of corresponding linear oli- gomers, e.g. starting from a mixture of the oligomers ^Λ 6 ^A and ^Λ 4 ^A , or passing through the intermediate which forms when the linear oligomer ^A 4 ^A is reacted with formaldehyde and phenol.

The compound which has been obtained has a m.p. of 300-305 °C, a molecular mass of 1621, and an ε,-^-- of 44570 in the UV spectrum. The elemental analysis is C, 80.98; H, 8.77; and 0, 10.00.

Example 11

Using the techniques described in the preceding Examples, each comprising the preparation of oligomers in a basic, aqueous medium and their cyclization in a neutral or acidic, water-free medium, the p-tert-butylcalix[11, 12, 13 and 14]arenes have been prepared. A mixture of these calixarenes is obtained starting from the oligomers ^A 6 ^Λ and 3 which, by disruption and recombination, yield cyclic structures comprising 11, 12, 13 and 14 phenolic units. The reaction mixture is treated on a silica column with chloroform/hexane. The fractions are recrystallized from a chloroform/acetonitrile mixture, and each of the 11, 12, 13 and 14 calixarenes is obtained in crystallized form. The physical properties are the following:

M.P.,°C Elemental analysis molecular mass

C H O (negative electrospray)

11+ 383-384 81.02 8.83 9.94 1784

12+ > 400 80.92 9.02 9.90 1947

13+ > 400 80.94 9.07 9.93 2109

14+ 350 81.17 8.81 9.76 2271

Example 12

Several p-isopropylcalixarenes have been prepared by re¬ peating the previous Examples, in particular Examples 1 and 2, with the exception that the starting p- ert-butylphenol has been replaced by the corresponding molar amount of p- isopropylphenol .

The following results have been obtained after the isola¬ tion of different isopropylcalixarenes from the reaction mixture by chromatography:

A) p-Isopropylcalix[4] arene (4A]

This compound has been recovered in a 19% yield as a pure, crystalline powder, m.p. 291-293 °C, molecular mass 592 (FAB+) ; Rf = 0.60 eluted by chloroform/hexane 1:1. Elemen¬ tal analysis:

B) p-Isopropylcalix[6] arene (6λ)

This compound has been recovered in a 55% yield as a pure, crystalline powder, m.p. 348-351 °C, molecular mass 888 (FAB+) ; Rf = 0.67 eluted by chloroform/hexane 1:1. Elemen- tal analysis :

C) p-Isopropylcalix [8] arene (8λ)

This compound has been recovered in a 32% yield as a pure, crystalline powder, m.p. 368-371 °C, molecular mass 1184.6 (FAB+) ; Rf = 0.84 eluted by chloroform/hexane 1:1. Elemen- tal analysis: