法国专利FR3022246A1 MONOANHYDRO-HEXITOL MONO-ALKYL ETHERS COMPOSITIONS, METHODS OF PREPARATION AND USE THEREOF

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专利摘要:
The present invention relates to a monoanhydro-hexitol monoalkyl ether isomer composition having a C-3, C-5 or C-6 alkyl ether (OR) radical of monoanhydrohexitol, wherein the alkyl group (R) is a cyclic or non-cyclic hydrocarbon group, linear or branched, comprising between 4 to 18 carbon atoms. The invention also relates to the process for obtaining such a composition and its use as a nonionic surfactant, emulsifier, lubricant, antimicrobial agent or dispersing agent.
公开号:FR3022246A1
申请号:FR1401346
申请日:2014-06-13
公开日:2015-12-18
发明作者:Charlotte Gozlan；Nicolas Duguet；Marc Lemaire；Andreas Redl
申请人:Syral Belgium NV；Universite Claude Bernard Lyon 1 UCBL；
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[0001] The present invention relates to mono-alkyl ether compositions based on sugars, and a process for obtaining such ethers. In the scientific and technical literature, surfactant molecules based on sugar are well known. Among them, sucrose fatty acid esters, sorbitan esters and long chain polyglucoside alkyls have been widely used in food, personal care, cosmetic or pharmaceutical applications. Some of these surfactants have also been widely used as household or industrial cleaners or as lubricants. Despite their widespread use and acceptance, it is well known that ester-based surfactants are stable only over a limited pH range, whereas alkyl glucosides are stable under alkaline and neutral conditions, but not under strongly acidic conditions.
[0002] Other disadvantages are related to the processes used to obtain these derivatives. Indeed, in the case of higher chain length alkyl glucosides, a trans-acetalization is necessary. The use of rather complicated and expensive facilities is necessary in order to obtain a sufficiently pure product. In the case of sugar-based esters, especially sorbitan esters, expensive but toxic solvents are required, or high reaction temperatures are required to obtain the products in sufficiently high yield. In order to improve the acidic stability of sugar-based surfactant compounds, a sugar alcohol ether has been recently proposed in WO 2012/148530. This application describes a process for preparing polyol ethers in which a mass of molten polyols is reacted with a long-chain aldehyde under reducing alkylation conditions. According to this disclosure, difficult and extreme reaction conditions are required, this in combination with high pressure equipment in order to carry out the reductive alkylation reaction. In order to obtain the desired products, an excess of sugar alcohol is considered necessary in relation to the aldehyde. This induces energy consumption per mole of high sugar alcohol ether. Furthermore, the prior art describes methods for obtaining monoanhydro-sorbitol. Thus, a method in which sorbitol is dissolved in water in the presence of an acid catalyst and heated under atmospheric conditions for a time sufficient to obtain the maximum 1,4-sorbitan content is described in Acta Chemical Scandinavica B ( 1981) p.441-449. Also similar processes have been disclosed in which the reaction is carried out under reduced pressure (US 2,390,395 and US 2007/173651) or under moderate hydrogen pressure (US2007 / 173654). In US2007 / 173654, a noble metal cocatalyst is used, however, measured isosorbide concentrations are quite high compared to 1,4-sorbitan. Thus, the methods of the prior art do not allow to observe a high production yield of monoanhydro-sorbitol under mild reaction conditions. Thus, it is clear that there is a need to provide sugar alcohol ethers with surfactant properties that can be obtained by high efficiency processes that are both environmentally acceptable. , advantageous in the energy consumption and easy to implement industrially.
[0003] This need has been solved by establishing a monoanhydro-hexitol monoalkyl ether isomer composition having a C-3, C-5 or C-6 alkyl ether (OR) radical of monoanhydrohexitol, in wherein the alkyl group (R) is a linear or branched hydrocarbon group comprising between 4 to 18 carbon atoms preferably between 8 and 12 carbon atoms.
[0004] By "C-3, C-5 or C-6 alkyl ether radical (OR)" is meant an alkoxy radical substituting the carbon atom at the 3, 5 or 6 position of the monoanhydrohexitol. By "isomers of monoalkyl monoanhydro-hexitol ethers having a C-3, C-5 or C-6 alkyl (OR) alkyl ether radical of monoanhydro-hexitol" or "C-3, C-5 or C-isomers" Monoalkyl monoanhydrohexitol ethers are understood to mean 3-alkyl monoanhydrohexitol, 5-alkyl monoanhydrohexitol and 6-alkyl monoanhydrohexitol. As examples of an alkyl group, mention may be made of butyl, pentyl, hexyl, heptyl, octyl, nonyl, decyl, undecyl or dodecyl groups. Typically, the alkyl group is selected from octyl, decyl or dodecyl groups. More particularly, the composition according to the invention comprises at least 15% (w / w) of any monoanhydro-hexitol monoalkyl ether isomer. Advantageously, the majority isomer is 6-alkyl monoanhydrohexitol. Preferably, the ratio [(3-alkyl monoanhydro-hexitol + 5-alkyl monoanhydro-hexitol) / 6-alkyl monoanhydro-hexitol] is between 0.5 and 2, preferentially between 0.7 and 1.8, more preferentially between 0 and 1.8. , 8 and 1.7. Typically, the ratio of monoanhydro-hexitol monoalkyl ether isomers having a C-3, C-5 and C-6 (3-alkyl monoanhydro-hexitol / 5-alkyl monoanhydro) alkyl ether (OR) radical is hexitol / 6-alkyl monoanhydro-hexitol) is between 15/15/100 and 95/95/100, preferably between 20/20/100 and 90/90/100, more preferably 25/25/100 and 85/85. / 100. Typically, the ratio of monoanhydro-hexitol monoalkyl ether isomers is between 30/30/100 and 83/83/100. Preferably, the composition according to the invention comprises at least 90% (w / w), preferably at least 95% (w / w) isomers of monoalkyl monoanhydro-hexitol ethers. Advantageously, the mono-anhydro hexitol is chosen from mono-anhydro-sorbitol, mono-anhydro-mannitol, mono-anhydro-iditol and mono-anhydro-galactitol. Typically, mono-anhydro hexitol is mono-anhydro sorbitol or mono-anhydro-mannitol.
[0005] Typically, the isomers of monoalkyl monoanhydro-sorbitol ethers may be of formula I wherein R 1, R 2 and R 3 are an alkyl group and two hydrogen atoms. For example, a C-3 isomer of a monoanhydro-sorbitol alkyl ether (or 3-alkyl monoanhydro-sorbitol) is of formula II wherein R 1 is an alkyl group. Preferably, the C-5 isomer of a monoanhydrosorbitol alkyl ether (or 5-alkyl monoanhydro-sorbitol) is of formula III wherein R 2 is an alkyl group.
[0006] Preferably, the C-6 isomer of a monoanhydrosorbitol alkyl ether (or 6-alkyl monoanhydro-sorbitol) is of formula IV wherein R 3 is an alkyl group. R3 (IV) The present invention also relates to a process for obtaining a monoanhydro-hexitol monoalkyl ether isomer composition having a C-3, C-5 or C-6 alkyl ether (OR) monoanhydrohexitol, wherein the alkyl group (R) comprises between 4 to 18 carbon atoms according to the invention, said method comprising the steps of: dehydrating a hexitol to obtain a monoanhydro-hexitol substrate; obtaining a hexitan alkyl acetal by acetalization or transacetalization of the obtained monoanhydro-hexitol substrate, with an aliphatic aldehyde reagent containing from 4 to 18 carbon atoms, by acetalization, preferably in a ratio of substrate / reagent between 5: 1 and 1: 1, or o a derivative of an aliphatic aldehyde reagent containing from 4 to 18 carbon atoms, by trans-acetalization, preferably, in a ratio of substrate / reagent between 1: 1 and 1: 3, catalytic hydrogenolysis of the hexitan acetal alkyl, and recovery of a monoanhydro-hexitol monoalkylether ether isomer composition having a C-3, C-5 or C-6 alkyl ether (OR) monoanhydro-hexitol, wherein the alkyl group (R) comprises from 4 to 18 carbon atoms.
[0007] Typically, the method according to the invention further comprises, at least one neutralization step, and / or filtration and / or purification after any of steps a), b) and / or d). Preferably, step a) of dehydration is carried out by treatment of hexitol, for example in the form of a hexitol melt, with an acid catalyst. Typically, step a) is carried out under a hydrogen atmosphere preferentially at a pressure of 20 to 50 bar. Advantageously, step a) is carried out at a temperature between 120 and 170 ° C, preferably between 130 and 140 ° C.
[0008] Step b) of acetalization or transacetalization may be preceded by a purification step of monoanhydro hexitol. The purification may be for example a chromatography or crystallization step. Preferentially, step b) of acetalization or transacetalization comprises bi) optionally, a first step of preheating the monoanhydro-hexitol substrate, preferably at a temperature between 70 and 130 ° C., typically between 90 and 110 ° C. bii) a step of adding the aliphatic aldehyde reagent or the aliphatic aldehyde derivative and biii) a third step of adding a catalyst, preferably an acid catalyst. Typically, the acetalization or trans-acetalization reaction is carried out at temperatures between 70 and 130 ° C, typically between 90 and 110 ° C. The reaction mixtures are heated at varying temperatures depending on the reagents and solvents used. The reaction time is determined by the degree of conversion achieved. The acid catalysts used in steps a) and b) may be independently selected from solid or liquid acids, organic or inorganic, with solid acids being preferred. In particular, the preferred acids are chosen from para-toluenesulphonic acid, methanesulfonic acid and camphorsulphonic acid (CSA or camphor sulfonic acid) and sulphonic resins. When carrying out the acetalization or transacetalization reaction with an aliphatic aldehyde reagent or an aliphatic aldehyde derivative, the reaction can be carried out with or without a solvent. When the reaction is carried out in the presence of a solvent, the solvent is preferably a polar solvent, typically a non-aqueous polar solvent. When using a solvent, it may be chosen from polar solvents such as dimethylformamide (DMF), dimethylsulfoxide (DMSO), dimethylacetamide (DMA), acetonitrile (CH3CN), tetrahydrofuran ( THF), 2-methyltetrahydrofuran (2Me-THF), cyclopentyl methyl ether (CPME) or isopropanol. The acetalization step b) can be carried out with an aliphatic aldehyde reagent, wherein the aldehyde reagent contains from 4 to 18 carbon atoms. These aldehydes can be chosen from linear or branched aliphatic aldehydes. In a preferred embodiment, the aliphatic aldehydes contain from 4 to 18 carbon atoms, preferably 5 to 12 carbon atoms. Some typical representatives of aldehydes are: pentanal, hexanal, heptanal, octanal, nonanal, decanal, undecanal and dodecanal.
[0009] Extensive experimental work has made it possible to select conditions which ensure optimum conversion rates and yields of the acetalization step b). The best results have been obtained when the molar ratio of the substrate to the reagent is between 5: 1 and 1: 1, preferably between 4: 1 and 1: 1, and more preferably between 3: 1 and 2: 1. The trans-acetalization step b) can be carried out in the presence or absence of a solvent in order to obtain alkyl long-chain cyclic acetals based on sugar. Typically, when step b) of transacetalization is carried out in the presence of a solvent, the preferred solvent is the alcohol corresponding to the acetal reagent used.
[0010] During step b) of transacetalization, the derivatives of an aliphatic aldehyde reagent may be the di-alkyl acetals of the corresponding aldehydes. Di-methyl acetals and diethyl acetals are preferred. Extensive experimental work has made it possible to select conditions ensuring that during trans-acetalization reactions, optimal yields and conversion rates were obtained when the molar ratio of substrate to reagent is between 1: 1 and 1: 3. and preferably between 2: 3 and 2: 5. The catalysts used are the same as during the acetalization reactions. Typically, step c) of hydrogenolysis of the hexitan acetal alkyl may be preceded by a filtration and / or purification step.
[0011] The purification may be for example a chromatography or crystallization step. Preferably, the purification by chromatography is carried out using a non-aqueous polar solvent. For example, the nonaqueous polar solvent is identical to that used in the hydrogenolysis step c). Advantageously, the hydrogenolysis step c) is carried out at a temperature of between 80 ° C. and 140 ° C., preferably at a pressure between 15 and 40 bar. The hydrogenolysis step c) is advantageously carried out in the presence of a polar solvent that is preferentially aprotic or non-aqueous. Examples of aprotic solvents include but are not limited to trimethoxypropane (TMP), methylterbutyl ether (MTBE), THF, MeTHF, dibutyl ether and CPME. Preferably, the aprotic solvent is CPME. The hydrogenolysis step c) is preferably carried out in an aprotic polar solvent, at a temperature of between 80 ° C. and 140 ° C. and a pressure of between 5 and 40 bar, in the presence of a catalyst suitable for hydrogenolysis reactions. Preferably, the hydrogenolysis step c) is carried out in a non-aqueous polar solvent, at a temperature ranging between 100 ° C. and 130 ° C. and / or at a pressure between 25 and 35 bar. Typically, step c) is carried out in the presence of a suitable catalyst such as a precious metal or metal-based catalyst belonging to the group of ferrous metals. As an indication, a catalyst based on metals belonging to the group of ferrous metals may be nickel, cobalt or iron. Preferably, the hydrogenolysis is carried out using a catalyst based on precious metals, such as palladium, rhodium, ruthenium, platinum or iridium. Typically, the catalyst used in step c) can be attached to a support such as charcoal, alumina or silica. Such a support is for example in the form of 20 balls. A palladium catalyst attached to coal (Pd / C) beads is preferred. According to the invention, the hexitol such as that used in step a) is a hydrogenated monosaccharide preferentially chosen from sorbitol, mannitol, iditol, galactitol and their mixture. Sorbitol and / or mannitol are preferred.
[0012] When the hexitol is sorbitol, the monoanhydrohexitol obtained is the 1,4 sorbitan of formula (V). (V) The inventors have demonstrated that the 1,4-sorbitan intermediate product can be obtained in good yield by treating a sorbitol melt with a solid acid catalyst in a hydrogen atmosphere at a pressure of 20 to 50 bar, this at a reaction temperature which can vary between 120 and 170 ° C for a period of time sufficient to obtain an optimal sorbitan yield. Preferred reaction temperatures are from 130 to 140 ° C. The reaction mixture thus obtained consists of 1,4-sorbitan, unreacted sorbitol, isosorbide and minor amounts of by-products, as illustrated in the chromatogram shown in the figure. 1. One of the advantages observed thus is the lowering of the level of coloration, this in contrast with the previous conventional methods. The dehydration step a) may optionally be followed by a step of purifying the 1,4 sorbitan. Thus, the 1,4-sorbitan is purified from the reaction mixture and the remainder is recycled to the dehydration step. In a particular embodiment, the 1,4-sorbitan is recovered and purified by crystallization. In another preferred embodiment, the 1,4-sorbitan is recovered and purified by chromatography. This purified 1,4-sorbitan is preferably used as a substrate for the acetalization reaction. When the acetalization step b) is carried out without solvent, the 1,4-sorbitan is first heated to 90 ° to 110 ° C., then the aldehyde reagent is added slowly, followed by the addition of the catalyst.
[0013] The sorbitan acetal compositions obtained by the processes described above are composed of 4 isomers. This is illustrated in Figure 2. Two of these isomers correspond to a diastereomeric mixture of 5-membered 5-membered sorbitan acetal at the 5,6-position and the other two isomers correspond to a diastereomeric mixture of a 6-membered sorbitan acetal in position 3.5.
[0014] The 5,6-sorbitan acetals are of formula VI wherein the R 'group is an alkyl group. Typically, R 'is a linear or branched aliphatic chain of C3 to C17. (VI) The 3,5-sorbitan acetals are of formula VII in which the R group is an alkyl group. Typically, R 'is a linear or branched aliphatic chain of C3 to C17.
[0015] The hexitan alkyl acetals obtained above are then subjected to a hydrogenolysis reaction and this mixture of acetals can be used after recovery from the reaction mixture. This hydrogenolysis reaction is carried out in an aprotic polar solvent, at a temperature of between 80 ° C. and 140 ° C. and a pressure of between 15 and 40 bar, in the presence of at least one reaction medium. A catalyst suitable for carrying out hydrogenolysis reactions Preferably, the hydrogenolysis is carried out in a non-aqueous polar solvent, at a temperature between 100 ° C and 130 ° C and a pressure between 25 and 35 bar.
[0016] The non-aqueous polar solvent CPME (cyclopentyl methyl ether) has been proved to be particularly advantageous in the hydrogenolysis reaction of the cyclic acetals 5.6 and 3.5 of sorbitan. The invention also relates to the product obtained by carrying out the process. The invention further relates to the use of the composition according to the invention as a nonionic surfactant, emulsifier, lubricant, antimicrobial agent or dispersing agent. Typically, the composition according to the invention can be used in a food or non-food product or in a pharmaceutical or cosmetic product. When the composition according to the invention is used as a nonionic, dispersing or emulsifying surfactant, the food product may be selected from aerated products such as foams, ice cream, or non-aerated products such as materials. fat spreads or salad dressings. The food product may be in the form of a liquid product selected from the group consisting of sauces, soups and beverages. Preferentially, C1-C12 alkyl groups are preferred for their use as antimicrobial agents or nonionic surfactants.
[0017] Preferentially, the C5-C8 alkyl groups are preferred in use as emulsifying, lubricating or dispersing agents. Without limiting the scope of the invention, the invention will now be further illustrated by means of a number of modifications. examples describing the methods of preparation of these derivatives.
[0018] FIGURES FIG. 1 represents a chromatogram of the reaction mixture obtained during the dehydration reaction; FIG. 2: represents a chromatogram of the reaction mixture obtained by transacetalization without solvent according to example 8. FIG. 3: represents a chromatogram of the reaction mixture obtained by hydrogenolysis according to example 10. EXAMPLES Example 1: Dehydration sorbitol: D-sorbitol (20 g, 110 mmol) and 0.1 mol% of camphorsulfonic acid are added to a 150 ml autoclave of stainless steel. The reactor is hermetically sealed, purged three times with hydrogen and then the hydrogen is introduced to a pressure of 50 bar. The system is then heated to 140 ° C and stirred with a mechanical stirrer for 15 hours. After cooling to room temperature, the hydrogen pressure was released and the white foam was diluted in ethanol (200 mL) to obtain a yellow homogeneous mixture. The solvent is evaporated under reduced pressure and the residue is then crystallized from cold methanol and filtered under vacuum. The crystalline material was washed with cold methanol to give 1,4-sorbitan (5.88 g, 35% theoretical) as a white solid. The purity is> 98%, as determined by HPLC, while the crystals showed a melting point of 113-114 ° C. The degree of conversion of the reaction was determined to be 73%, whereby a mixture of sorbitol, 1,4-sorbitan, isosorbide and some by-products in a very limited amount was obtained, so that the ratio of 1,4-sorbitan: isosorbide was determined to be 80:20. EXAMPLE 2: Sorbitan Acetalisation in DMF: In a sealed tube, the 1.4 sorbitan (X) (0.5 g, 3 mmol) dissolved in DMF (1.4 mL). Valeraldehyde (Y) (107 μL, 1 mmol) was added dropwise under argon followed by the addition of camphorsulfonic acid (10 mg, 10% w / w) before closing the tube. The mixture is heated to 95 ° C with magnetic stirring. After 15 hours, the dark reaction mixture was cooled and the solvent evaporated under reduced pressure. A degree of conversion of 95% has been achieved. The residue was diluted in ethyl acetate and the excess of 1.4 sorbitan was filtered and washed with ethyl acetate. The filtrate was concentrated under reduced pressure. The residue was purified by flash chromatography (80:20 to 100: 0 cyclohexane) to give the sorbitan acetal (0.22 g, 89% isolated yield) as a colorless oil. HPLC revealed a mixture of 4 isomers. Example 3: In this example, different ratios of sorbitan against the aldehyde reagent were tested. The same reaction conditions as in Example 2 were used, but the sorbitan: aldehyde ratio was varied between 1: 1 and 3: 1. The results are shown in Table 1, below. X / Y ratio Conversion Isolated yield (% by weight 1: 1 96% 62% 2: 1 81% 83% 3: 1 95% 89% Table 1: Effect of sorbitan: aldehyde ratio on degree of conversion and isolated yield Example 4: With a sorbitan: aldehyde ratio of 3: 1 different aldehyde reactants were used to provide sorbitan acetal reaction products The same reaction conditions and purification steps as in Example 2 were used .
[0019] The results are shown in Table 2. Aldehyde Conversion Yield Isolated Hexanal 100% 98% Octanal 89% 95% Decanal 69% 85% Dodecanal 61% 80% Table 2: Example 5: In addition to the use of DMF as a solvent, also d Other solvents were used to prepare the sorbitan acetal compositions. Again, the same reagents were used and the same procedure was followed as in Example 2 except that the reaction temperatures were around 80 ° C. The results are shown in Table 3.
[0020] Solvent Conversion Isolated yield Acetonitrile 100% 75% i-PrOH 97% 66% DMF 92% 92% Table 3: Example 6: Sorbitan Acetalisation Without Solvent: In a sealed tube, the 1.4 sorbitan (X) (0.5) g, 3 mmol) was heated to 95 ° C. Valeraldehyde (Y) (107pt, 1mmol) was added dropwise under argon followed by camphorsulfonic acid (10mg, 10% w / w) before closing the tube. The mixture is heated to 95 ° C with magnetic stirring. After 15 hours, the dark reaction mixture was cooled and diluted with ethyl acetate (2 mL) and the solvent was then evaporated under reduced pressure. A degree of conversion of 80% was obtained. The residue was further diluted in ethyl acetate and the excess of 1.4 sorbitan was filtered and washed with ethyl acetate. The filtrate was concentrated under reduced pressure. The residue was purified by flash chromatography (EtOAc: 80:20 cyclohexane to 100: 0) to give the sorbitan acetal (0.13 g, 54% isolated yield) as a colorless oil. HPLC revealed a mixture of 4 isomers. Example 7: Trans-aetalisation of sorbitan in ethanol: In a round bottom flask of 1,4-sorbitan (0.5 g, 3 mmol) was dissolved in ethanol (7.5 mL) and the 1,1-diethoxypentane (1.15 mL, 6 mmol) was added under a stream of argon followed by camphorsulfonic acid (50 mg, 10% w / w). The mixture is heated to 80 ° C and with magnetic stirring. After 3 hours, the mixture was neutralized and concentrated under reduced pressure. The residue was purified by flash chromatography (80:20 to 100: 0 ethyl acetate / cyclohexane) to give the sorbitan acetal (0.43 g, 66% isolated yield) as a colorless oil. HPLC revealed a mixture of 4 isomers. Example 8 Transacetalization of sorbitan without solvent: In a round-bottomed flask, 1,4-sorbitan (0.5 g, 3 mmol) and 1,1-diethoxypentane (1,1-DEP) (1, 15 mL, 6 mmol) (1: 2 molar ratio) was added under argon flow, followed by camphorsulfonic acid (50 mg, 10 w / w%). The mixture is heated to 80 ° C with magnetic stirring. After 3 hours, the mixture was directly purified by flash chromatography (80:20 to 100: 0 ethyl acetate / cyclohexane) to give the sorbitan acetal (0.517 g, 73% isolated yield) as a colorless oil. HPLC revealed a mixture of 4 isomers. (FIG 2) EXAMPLE 9 The solventless transacetalization reactions were carried out using different molar ratios, different reagents (1,1-dimethoxypentane), different reaction temperatures and different reaction times, the catalyst being the same . The purification of the reaction mixtures was carried out by flash chromatography, as in Example 8.
[0021] The results are given in Table 4. Reagent Sorbitan / Reaction Rate Time (h) Temperature Conversion Isolated Yield 1,1-DMP 1: 1 70 ° C 99% 66% 1,1-DEP 1: 1 15 70 ° C 81% 66% 1,1-DEP 1: 1 80 ° C - 49% 1,1-DEP 1: 2 3 80 ° C 80% 73% Table 4: Example 10: Hydrogenolysis of sorbitan acetals: Du Pentylidene- (1,4) -sorbitane (51:49 mixture of regioisomers, 0.98g, 4.22 mmol) was diluted in dry CPME (30 mL) and placed in a stainless steel autoclave, with a catalyst. 5% Pd / C (0.45 g). The reactor is well closed, purged three times with hydrogen, before hydrogen is introduced under pressure (30 bar). The system is heated to 120 ° C and stirred for 15 hours. After cooling to room temperature, pressurized hydrogen is released, the reaction mixture is dissolved in absolute ethanol (100 mL) and filtered (Millipore Durapore Filter 0.01 micron). The filtrate is evaporated under reduced pressure and the residue is purified by flash chromatography (EtOAc / cyclohexane 90:10 to 100: 0, then EtOH / EtOAc 10:90). Thus, a mixture of pentyl (1,4) -sorbitane ethers (0.686 g, 69%) was obtained as a colorless oil. HPLC analysis (column C18, eluent water / 80/20 CH3CN + 0.1% v / v H3PO4) showed a 27:33:40 mixture of penty1 (1,4) -sorbitan regioisomers at position 3, 5 and 6. The retention times Rt are 7.20 min (27%), 9.25 min (33%) and 10.79 min (40%) (the peaks have not been assigned and the isomers are described in order digital) (Fig.3) Spectroscopic data: 1H NMR (400MHz, d6-DMS0) SH 0.85 (3H, t, J = 7), 1.20-1.37 (4H, m), 1.38-1.58 (2H) , m), 3'20-3.98 (10H, m, sorbitan protons + OCH2 ethers), 4.02-5.15 (3H, 7m, OH protons); 13C NMR (100 MHz, d6-DMSO) Sc for major isomer: 13.99 (CH3), 22.01 (CH2), 27.88 (CH2), 28.99 (CH2), 67.50 (CH), 70.59 (CH2), 73.36 (CH2), 73.49 (CH2), 75.66 (CH), 76.37 (CH), 80.34 (CH). Sc for minor isomers: 14.02 (2 CH3), 22.03 (2 CH2), 27.86 and 27.91 (2 CH2), 29.21 and 29.55 (2 CH2), 62.02 (CH2) ), 64.20 (CH2), 68.71 (CH), 69.51 (CH2), 69.79 (CH2), 73.15 (CH2), 73.23 (CH), 73.60 (CH2) , 75.53 (CH), 76.45 (CH), 77.37 (CH), 79.28 (CH), 80.10 (CH), 83.95 (CH) ,. HRMS (ESI +) calcd for C11H22NaO5: 257.1363 [M + Na]; found: 257.1359 (-1.4 ppm) Example 11: One-pot synthesis of sorbitan ethers from 1,4-sorbitan: In a 100 mL round-bottomed flask, 1,4- Sorbitan (10 g, 62 mmol) was dissolved in dry CPME (30 mL) in the presence of Na 2 SO 4 (6.5 g, 50 mmol) under an argon atmosphere. Valdeldehyde (3.3 mL, 31 mmol) was added dropwise followed by Amberlyst 15 (530 mg, 20 w / w% valeraldehyde). The mixture is heated to 80 ° C with magnetic stirring. After 3 hours, the hot mixture is filtered, washed with CPME (2 x 25 mL) and the filtrate is concentrated under reduced pressure. Without further purification, the mixture is diluted in CPME (300 mL), dried over MgSO4 and filtered. The filtrate is introduced into a 500 ml stainless steel autoclave, and 5% -Pd / C (3.3 mg) is added. The reactor is well closed, purged three times with hydrogen, before hydrogen is introduced under pressure (30 bar). The system is heated to 120 ° C and stirred for 15 hours. After cooling to room temperature, pressurized hydrogen is released, the reaction mixture is dissolved in absolute ethanol (250 mL) and filtered (Millipore Durapore Filter 0.01 micron). The filtrate is evaporated under reduced pressure and the residue (5.8 g) is purified by flash chromatography (EtOAc / cyclohexane 90:10 to 100: 0, then EtOH / EtOAc 10:90). Thus a mixture of pentyl (1,4) sorbitan ethers (3.97 g, 56%) was obtained as a colorless oil (purity> 98% by 1 H NMR).
[0022] Example 12: Octyl-1,4-sorbitan is prepared according to the procedure described in Example 10 from octylidene-1,4-sorbitan (39:61 mixture of 5,6- and 3,5-regioisomers) (5.61 g, 20.4 mmol). The residue is purified by flash chromatography (EtOAc / cyclohexane 80:20 to 100: 0 then EtOH / EtOAc 10:90) to obtain a mixture of isomers of octyl-1,4-sorbitan as a white solid product. HPLC analysis (Column C18, eluent water / 80/20 CH3CN + 0.1% v / v H3PO4) showed a 33:22:45 mixture of octy (1,4) -sorbitan regioisomers at the 3-position. , 5 and 6 (the peaks have not been assigned and the isomers are described in numerical order).
[0023] Spectroscopic data: 1H NMR (300 MHz, d6-DMSO) HS 0.86 (3H, t, J = 7), 1.08-1.39 (10H, m), 1.39-1.58 (2H, m), 3.28-3.95 (10H, m, sorbitan protons + OCH2 ethers), 4.02-5.10 (3H, 7m, OH protons); 13C NMR (75 MHz, d6-DMSO): 5c for major isomer: 13.98 (CH3), 22.12 (CH2), 25.69 (CH2), 28.73 (CH2), 28.92 (CH2) , 29.31 (CH2), 31.29 (CH2), 67.48 (CH), 70.60 (CH2), 73.35 (CH2), 73.48 (CH2), 75.64 (CH), 76.36 (CH), 80.33 (CH) Sc for minor isomers: 13.98 (2 CH3), 22.12 (2 CH2), 25.69 (2 CH2), 28.88 (2 CH2), 28.92 (2 CH 2), 28.98 (CH 2), 29.52 (CH 2), 29.88 (CH 2), 31.32 (CH 2), 62.00 (CH 2), 64.17 (CH 2), 68.69 (CH), 69.51 (CH2), 69.82 (CH2), 73.14 (CH2), 73.22 (CH), 73.59 (CH2), 75.53 (CH), 76 , 44 (CH), 77.37 (CH), 79.27 (CH), 80.07 (CH), 83.94 (CH) HRMS (ESI +) calculated for C14H28NaO5: 299.1829 [M + N1; Found: 299.1832 (-1.2 ppm) Example 13: Decy1-1,4-sorbitan is prepared according to the procedure described in Example 10 from decylidene-1,4-sorbitan (36:64 mixture of 5,6- and 3.5-regioisomers) (6.12 g, 20.2 mmol). The residue is purified by flash chromatography (EtOAc / cyclohexane 70:30 to 100: 0 then EtOH / EtOAc 10:90) to obtain a mixture of isomers of decyl-1,4-sorbitan as a white solid product. HPLC analysis (Column C18, eluent water / 50/50 CH3CN + 0.1% v / v H3PO4) showed a 32: 16: 52 mixture of decyl (1,4) -sorbitan regioisomers at the 3-position. , 5 and 6 (the peaks have not been assigned and the isomers are described in numerical order). Spectroscopic data: Ifi NMR (300 MHz, d6-DMSO) .3110.86 (3H, t, J = 7), 1.09-1.38 (14H, m), 1.38-1.58 (2H, m), 3.25-4.01 (10H, m, sorbitan protons + OCH2 ethers), 4.02-5.08 (3H, 7m, OH protons); 13C NMR (75 MHz, d6-DMSO) Sc for major isomer: 13.98 (CH3), 22.16 (CH2), 25.76 (CH2), 28.79 (CH2), 29.04 (CH2), 29.07 (CH 2), 29.14 (CH 2), 29.17 (CH 2), 29.35 (CH 2), 67.53 (CH), 70.63 (CH 2), 73.38 (CH 2), 73 , 50 (CH2), 75.69 (CH), 76.40 (CH), 80.35 (CH). 3c for minor isomers: 13.98 (2 CH 3), 22.16 (2 CH 2), 28.98 (2 CH 2), 29.01 (2 CH 2), 29.14 (2 CH 2), 29.17 (2 CH 2), 29.35 (2 CH 2), 29.57 (2 CH 2), 29.92 (2 CH 2), 62.01 (CH 2), 64.18 (CH 2), 68.72 (CH), 69, 56 (CH2), 69.84 (CH2), 73.16 (CH2), 73.27 (CH), 73.60 (CH2), 75.56 (CH), 76.48 (CH), 77.41 (CH), 79.30 (CH), 80.08 (CH), 83.96 (CH) HRMS (ESr) calcd for CI6H32NaO5: 327.2142 [M + N1; found: 327.2135 (+ 2.1 ppm).

权利要求:
Claims (2)
[0001]
REVENDICATIONS1. An isomer composition of monoalkyl monoanhydro-hexitol ethers having a C-3, C-5 or C-6 alkyl (OR) alkyl ether radical of monoanhydrohexitol, wherein the alkyl group (R) is a linear hydrocarbon group or branched comprising between 4 to 18 carbon atoms, preferably 8 to 12 carbon atoms. 3. 4. 5. 6. Composition according to claim 1, characterized in that the mono-anhydro hexitol is chosen from mono-anhydro sorbitol, mono-anhydro-mannitol, mono-anhydro-iditol and mono-anhydro galactitol and their mixture, preferably mono-anhydro sorbitol or mono-anhydro-mannitol. Composition according to either of Claims 1 and 2, characterized in that it comprises at least 15% (w / w) of any of the isomers of monoanhydro-hexitol monoalkyl ethers. Composition according to any one of Claims 1 to 3, characterized in that it comprises at least 90% (w / w), preferably 95% of monoanhydro-hexitol monoalkyl ether isomers. Composition according to any one of Claims 1 to 4, characterized in that the ratio of [(3-alkyl monoanhydro-hexitol + 5-alkyl monoanhydrohexitol) / 6-alkyl monoanhydro-hexitol] is between 0.5 and
[0002]
2. A process for obtaining a monoanhydro-hexitol monoalkyl ether isomer composition having a monoanhydro-hexitol C-3, C-5 or C-6 alkyl ether (OR) radical, wherein the alkyl group (R) comprises from 4 to 18 carbon atoms, comprising the steps of: a) dehydrating a hexitol to obtain a monoanhydrohexitol substrate; b) obtaining a hexitan alkyl acetal by acetalization or transacetalization of the obtained monoanhydro-hexitol substrate, with i. an aliphatic aldehyde reagent containing from 4 to 18 carbon atoms, by acetalization preferably in a ratio of substrate / reagent between 5: 1 and 1: 1, or ii. a derivative of an aliphatic aldehyde reagent containing from 4 to 18 carbon atoms, by transacetalization preferentially in a ratio of substrate / reagent between 1: 1 and 1: 3; c) catalytic hydrogenolysis of the hexitan acetal alkyl, and d) recovering a monoanhydro-hexitol monoalkyl ether isomer composition having a C-3, C-5 or C-alkyl (OR) alkyl ether radical. 6 of the monoanhydro-hexitol in which the alkyl group (R) comprises between 4 to 18 carbon atoms. 7. Process according to claim 6, characterized in that step b) of acetalization or transacetalization is carried out in the presence of an acid catalyst, preferably in an environment which is solvent-free or which consists of a solvent. . 8. Method according to either of claims 6 and 7, characterized in that the hydrogenolysis is carried out in a solvent, preferably at a temperature between 80 and 140 ° C and / or a pressure between 15 and 40 bar, in the presence of a catalyst, preferably a catalyst based on precious metals. 9. Method according to either of claims 7 and 8, characterized in that the solvent is a polar solvent preferentially, non-aqueous or aprotic such as cyclopentyl methyl ether (CPME) .10. Process according to any one of Claims 6 to 9, characterized in that it comprises at least one filtration and / or purification step after any of the steps a), b) and / or d). 11. Process according to claim 10, characterized in that the purification step is carried out by chromatography or crystallization. 12. Process according to claims 6 to 11, characterized in that the hexitol used is chosen from sorbitol and mannitol. 13. Use of a composition according to any one of claims 1 to 5 as nonionic surfactant, emulsifier, lubricant, antimicrobial agent or dispersing agent. 14. Use of a composition according to any one of claims 1 to 5 in a food or non-food product such as a pharmaceutical or cosmetic product. 15. Product obtained by carrying out the method according to any one of claims 1 to 12.

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DE19749202C1|1997-11-07|1999-05-27|Degussa|Process for the preparation of five- or six-membered cyclic ethers and anhydrohexite mixtures|

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优先权:

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FR1401346|2014-06-13|

FR1401346A|FR3022246B1|2014-06-13|2014-06-13|MONOANHYDRO-HEXITOL MONO-ALKYL ETHERS COMPOSITIONS, METHODS OF PREPARATION AND USE THEREOF|FR1401346A| FR3022246B1|2014-06-13|2014-06-13|MONOANHYDRO-HEXITOL MONO-ALKYL ETHERS COMPOSITIONS, METHODS OF PREPARATION AND USE THEREOF|

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CN201580031768.8A| CN106687206B|2014-06-13|2015-06-11|The composition of the monoalky lether of single dewatering hexitol, its manufacturing method and application thereof|

CA2947523A| CA2947523C|2014-06-13|2015-06-11|Compositions of mono-alkyl ethers of monoanhydro-hexitols, production methods thereof and use of same|

JP2016572619A| JP6549162B2|2014-06-13|2015-06-11|Composition of monoalkyl ether of monoanhydro-hexitol, process for its preparation and its use|

EP15732440.1A| EP3154669B1|2014-06-13|2015-06-11|Compositions of mono-alkyl ethers of monoanhydro-hexitols, production methods thereof and use of same|

PCT/IB2015/054418| WO2015189796A1|2014-06-13|2015-06-11|Compositions of mono-alkyl ethers of monoanhydro-hexitols, production methods thereof and use of same|

US16/259,553| US10653664B2|2014-06-13|2019-01-28|Antibacterial compositions of mono-alkyl ethers of monoanhydro-hexitols and antibacterial methods using of the same|

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