WO2006048166A1

WO2006048166A1 - Microcapsule dispersions

Info

Publication number: WO2006048166A1
Application number: PCT/EP2005/011485
Authority: WO
Inventors: Petra SCHÖCKER; Ralf Widmaier; Bettina MÜLLER; Dirk Wulff; Peter Gernert; Hardy Korb
Original assignee: Basf Aktiengesellschaft
Priority date: 2004-11-05
Filing date: 2005-10-27
Publication date: 2006-05-11
Also published as: US20080103265A1; JP2008518764A; BRPI0517066A; EP1809414A1; CN101056700A

Abstract

The present invention relates to microcapsule dispersions comprising microcapsules in a hydrophobic solvent, wherein the microcapsules have a capsule core, comprising a water-soluble organic substance, and a capsule shell which is composed essentially of reaction products of polyisocyanates with polyfunctional amines, and also to a process for preparing them and additionally to microcapsules obtainable from the corresponding microcapsule dispersions.

Description

Microcapsule dispersions

Description

Microcapsules are particles which comprise a capsule core and surrounding said cap¬ sule core a capsule shell, also referred to as capsule wall. The various uses depend on the nature of the capsule core. Critical to the properties is also the wall material and the encapsulation process, in the case for example of capsules with controlled release for active ingredients.

Microcapsules find broad application in the case of carbonless copying papers. Thus microcapsules with core oils comprising color formers have been known for a long time. The capsule walls, based on melamine-formaldehyde resin (EP-A-O 026 914) or on polyurea (EP-A-O 535 384), are formed by polycondensation or polyaddition, re¬ spectively, at the interfaces of an oil-in-water emulsion.

Conversely to the oil-in-water emulsions, where the oil is the disperse, i.e. discontinu- ous, phase and the water is the continuous phase, there also known encapsulation processes in which the two phases are reversed. Inverse microencapsulation is a term also used for these processes.

DE-A 101 20 480 describes one such inverse encapsulation. It teaches microcapsules having a capsule core comprising water-soluble substances and a capsule wall made of melamine/formaldehyde resins.

Further, US 5,859,075 teaches microcapsules with diols and polyols as capsule core and with a polyurethane wall, these microcapsules being prepared in paraffins as the continuous phase. The microcapsules thus obtained are suitable as a powder coating component. According to this teaching it is also possible to encapsulate water-sensitive substances by this process.

EP-A-O 148 169 describes microcapsules having a water-soluble core and a polyure- thane wall, which are prepared in a vegetable oil. Besides herbicides, water-soluble dyes are among the capsule core materials mentioned. WO 03/042274 discloses a process for preparing polyurea-based microcapsules hav¬ ing a liquid, suspension-containing or solid capsule core. The capsule walls are formed by an isocyanate/amine system and are further stabilized by the addition of crosslinking components such as, for example, mono- or dialdehydes.

WO 02/09862 describes processes for preparing active ingredient polymer capsules, beads or droplets with in situ encapsulation of the respective active ingredient by means of non-radical miniemulsion polymerization. Microemulsions having particle sizes of up to 500 nm are obtained.

In decorative cosmetology it is usual to use organic or inorganic pigments as coloring ingredients. Because of their insolubility the pigments are substantially inert to the other ingredients of the cosmetic product, unlike soluble dyes. The insolubility of the pig¬ ments has the advantage, moreover, that permanent discoloration of areas of the body treated with the cosmetic product can be avoided.

WO 03/015910 relates to microcapsule dispersions comprising microcapsules having a capsule core that comprises water-soluble organic substances, particularly dyes, and a capsule shell which is composed essentially of polyurethane and/or polyurea in a hy- drophobic solvent composed of from 50 to 100% by weight of glycerol ester oils and from 0 to 50% by weight of solvents miscible with glycerol ester oils, and to the incorpo¬ ration thereof into cosmetic compositions.

A disadvantage associated with the use of pigments in comparison to dyes, however, is their lower color brightness. A problem associated with the use of microcapsules is the often high and thus unsatisfactory permeability of the capsule walls for the enclosed core materials.

It was an object of the present invention to provide organic, water-soluble substances such as dyes for cosmetic compositions in the form of microcapsule dispersions that do not have the disadvantages of the prior art microcapsule dispersions and are distin¬ guished by a high degree of imperviousness in respect of the encapsulated contents.

Accordingly microcapsule dispersions have been found comprising microcapsules in a hydrophobic solvent, wherein the microcapsules have a capsule core, comprising at least one water-soluble organic substance, and a capsule shell, and wherein the cap¬ sule shell comprises reaction products of

a) at least one di-, oligo- and/or polyisocyanate and b) at least one polyfunctional amine selected from the group consisting of polyvinyl- amines, polyethylenimines and polyoxyalkylenamines having a number-average molecular weight of from 600 to 380 000 g/mol and c) if appropriate, one or more different alkyldiamines having 2 to 10 carbon atoms.

The capsules comprise a capsule shell and capsule core. The capsule core comprises at least one water-soluble organic substance in solid form and/or, as a result of prepa- ration, in the form of a solution in the hydrophilic solvent. Preferred capsule cores com¬ prise solutions of the water-soluble organic substance.

By reactants for the purposes of this specification are meant the at least one polyfunc- tional amine having an average molecular weight of from 600 to 380 000 g/mol and the alkyldiamine having 2 to 10 carbon atoms, to be used if desired, as compounds which react with di-, oligo- and/or polyisocyanate groups.

The basic principle of microencapsulation is based on what is called interfacial addition polymerization or interfacial polyaddition. With interfacial polyaddition, in a first process step, the materials for encapsulation and the reactants, as they are known, are dis¬ solved in a hydrophilic solvent, after which a hydrophobic solvent is added and the sys¬ tem is processed to an emulsion. The continuous phase of the emulsion normally in¬ cludes surface-active substances, preventing coalescence of the droplets. Within this emulsion the hydrophilic solvent is the discontinuous, disperse phase and the hydro- phobic solvent is the continuous phase. Where the hydrophilic solvent is water, the term water-in-oil emulsion is also illustrative. The emulsified droplets possess a size that corresponds approximately to the size of the subsequent microcapsules. To form the capsule wall in a second process step the emulsion is mixed with the isocyanate capable of wall forming. The reactants are capable of reacting with the isocyanate in solution in the continuous phase, at the interface between the discontinuous and con¬ tinuous phases, to form the polymeric capsule wall.

The third step of the process, which may optionally be carried out, comprises what is called the aftertreatment of the freshly prepared capsule dispersion. In this step, under temperature and residence time control and, if desired, using further auxiliaries, the reaction between isocyanate and reactant is carried out to completion.

By a hydrophilic solvent is meant not only water but also aqueous mixtures which in addition to water contain up to 20% by weight of a water-miscible organic solvent such as C₁ to C₄ alkanols, especially methanol, ethanol or isopropanol, or a cyclic ether such as tetrahydrofuran. A preferred hydrophilic solvent is water.

Suitable hydrophilic solvents are additionally ethylene glycol, glycerol, polyethylene glycols and butylene glycol and also mixtures thereof and also mixtures thereof with water or with the aqueous mixtures listed above. Preferred hydrophilic solvents are mixtures of these solvents with water. Examples of suitable hydrophobic solvents include mineral oils, mineral waxes, branched and/or unbranched hydrocarbons and triglycerides of saturated and/or un¬ saturated, branched and/or unbranched C₈-C₂₄ alkanecarboxylic acids. Further sub¬ stances suitable as hydrophobic solvents include the synthetic, semisynthetic or natural oils such as olive oil, palm oil, almond oil or mixtures; oils, fats or waxes, esters of satu¬ rated and/or unsaturated, branched and/or unbranched C₃-C₃₀ alkanecarboxylic acids and saturated and/or unsaturated, branched and/or unbranched C₃-C₃₀ alcohols of aromatic carboxylic acids and saturated and/or unsaturated, branched and/or un¬ branched C₃-C₃₀ alcohols, by way of example isopropyl myristate, isopropyl stearate, hexyldecyl stearate, oleyl oleate; and also synthetic, semisynthetic and natural mix¬ tures of such esters, such as jojoba oil, alkylbenzoate or silicone oils such as cyclome- thicone, dimethylpolysiloxane, diethylpolysiloxane, octamethylcyclotetrasiloxane, for example, and also mixtures thereof, or dialkyl ethers, such as linear or branched, symmetric or unsymmetric dialkyl ethers having 6 to 22 carbon atoms per alkyl group, for example.

Ring opening products of epoxidized fatty acid esters with polyols and/or aliphatic and/or naphthenic hydrocarbons may also be suitable.

Preferred hydrophobic solvents are esters, particularly esters of polyols, more prefera¬ bly pure glycerol ester oils. Particularly preferred glycerol ester oils in this context are C₆-C₁₂ fatty acid triglycerides or mixtures thereof, especially octanoic and decanoic triglycerides and mixtures thereof. One preferred octanoyl glyceride/decanoyl glyceride mixture is, for example, Miglyol^® 812 from Sasol.

In one preferred embodiment the hydrophobic solvents used in accordance with the invention are pure glycerol ester oils or glycerol ester oil mixtures with a concentration of from about 50 to about 100% by weight. By glycerol ester oils are meant esters of saturated or unsaturated fatty acids with glycerol. Mono-, di- and triglycerides and also their mixtures are suitable. Fatty acid triglycerides are preferred.

The hydrophobic solvent is composed, for example, of from 50 to 100% by weight, preferably from 70 to 100% by weight, more preferably from 90 to 100% by weight of glycerol ester oils and from 0 to 50% by weight, preferably from 0 to 30% by weight, more preferably from 0 to 10% by weight of solvents miscible with glycerol ester oils. Particular preference as hydrophobic solvent is given to glycerol ester oils, which are used individually or in their mixtures.

Examples of oils miscible with glycerol ester oils include the following:

hydrocarbon oils, such as liquid paraffin, purcellin oil, perhydrosqualene and so¬ lutions of microcrystalline waxes in these oils, animal or vegetable oils, such as sweet almond oil, avocado oil, calophyllum oil, lanolin and derivatives thereof, castor oil, horse oil, pig oil, sesame oil, olive oil, jojoba oil, karite oil and hoplostethus oil, mineral oils with an atmospheric pressure distillation start point at about 250⁰C and a distillation end point at 410⁰C, such as vaseline oil, for example, and esters of saturated or unsaturated fatty acids, such as alkyl myristates, e.g., iso- propyl, butyl or cetyl myristate, hexadecyl stearate, ethyl or isopropyl palmitate and cetyl ricinoleate.

Further suitable compounds which are miscible with glycerol ester oils are silicone oils, such as dimethylpolysiloxane, methylphenylpolysiloxane and the silicone glycol co¬ polymer, fatty acids and fatty alcohols or waxes such as carnauba wax, candellila wax, beeswax, microcrystalline wax, ozokerite wax and Ca, Mg and Al oleates, myristates, linoleates and stearates.

The compounds specified as hydrophobic solvents can each be used individually or as mixtures with one another.

The addition of perfume oils to mask the odor of the polymers is generally unneces- sary. If desired, however, the cosmetic formulations may nevertheless include perfume oils. Examples that may be mentioned of perfume oils include mixtures of natural and synthetic fragrances. Natural fragrances are, for example, extracts of blossoms (e.g., lily, lavender, rose, jasmine, neroli, ylang-ylang), stems and leaves (e.g., geranium, patchouli, petit grain), fruit (e.g., aniseed, coriander, caraway, juniper), fruit rinds (e.g., bergamot, lemon, orange), roots (e.g., mace, angelica, celeriac, cardamom, costus, iris, calmus), woods (e.g., pinewood, sandalwood, guajak wood, cedarwood, rose¬ wood), herbs and grasses (e.g., tarragon, lemon grass, sage, thyme), needles and twigs (e.g., spruce, fir, pine, mountain pine), resins and balsams (e.g., galbanum, el- emi, benzoine, myrrh, olibanum, opoponax). Also suitable are animal raw materials, such as amber grease, zibet and castoreum.

Typical synthetic fragrance compounds which can be used if desired are, furthermore, compounds of the type of the esters, ethers, aldehydes, ketones, alcohols and hydro¬ carbons. Fragrance compounds of the ester type are, for example, benzyl acetate, phenoxyethyl isobutyrate, 4-tert-butylcyclohexyl acetate, linalyl acetate, dimethylben- zylcarbinyl acetate, phenylethyl acetate, linalyl benzoate, benzyl formate, ethyl methyl- phenylglycinate, allyl cyclohexylpropionate, styrallyl propionate and benzyl salicylate. The ethers include, for example, benzyl ethyl ether; the aldehydes include, for exam¬ ple, the linear alkanals having 8 to 18 carbon atoms, citral, citronellal, citronellyloxya- cetaldehyde, cyclamenaldehyde, hydroxycitronellal, lilial and bourgeoal; the ketones include, for example, the ionones, α-isomethyl ionone and methyl cedryl ketone; the alcohols including anethole, citronellol, eugenol, isoeugenol, geraniol, linalool, phenylethyl alcohol and terpineol; and the hydrocarbons include, for example, the ter- penes and balsams. Preference is given, however, to using mixtures of different fra¬ grances which in unison produce an appealing fragrance note. Essential oils of low volatility as well, usually used as aroma components, are suitable as perfume oils, ex- amples being sage oil, chamomile oil, oil of clove, balm oil, mint oil, cinnamon leaf oil, lime blossom oil, juniper berry oil, vertiver oil, olibanum oil, galbanum oil, labdanum oil and lavandin oil. Preference is given to using bergamot oil, dihydromyrcenol, lilial, lyral, citronellol, phenylethyl alcohol, α-hexylcinnamaldehyde, geraniol, benzylacetone, cy- clamenaldehyde, linalool, boisambrene forte, ambroxane, indol, hedione, sandelice, lemon oil, mandarin oil, orange oil, allyl amyl glycolate, cyclovertal, lavandin oil, clary sage oil, β-damascone, geranium oil bourbon, cyclohexyl salicylate, Vertofix Coeur, Iso-E-Super, Fixolide NP, Evernyl, iraldein gamma, phenylacetic acid, geranyl acetate, benzyl acetate, rose oxide, Romillat, lrotyl and Floramat, alone or in the form of mix¬ tures.

The capsule core of the microcapsules of the invention comprises at least one, i.e., one or a mixture of two or more, generally from about 2 to 5 different water-soluble organic substance(s). Preferably the capsule core comprises one water-soluble organic sub¬ stance. By a water-soluble organic substance is meant a carbon-based compound which is at least partly soluble in water. The organic substance must have a greater affinity to the hydrophilic phase than to the hydrophobic phase. This is generally en¬ sured when the substance has a solubility in the hydrophilic solvent at room tempera¬ ture of at least 1 g/l. Preferably the organic substances have a solubility of at least 20 g/l in the hydrophilic solvent.

The water-soluble organic substances are, for example, water-soluble dyes, water- soluble vitamins like for example Vitamin B6 agrochemicals, flavors, pharmaceutical actives, fertilizers or cosmetic actives. The dyes are preferred water-soluble organic substances according to the invention.

The term "dye" here and below embraces organic compounds and salts of organic compounds and also charge transfer complexes of organic compounds with a chromo- phore which has an absorption maximum in the wavelength range from 400 to 850 nm and therefore evokes to the human eye an impression of color (conventional dyes) and which may also itself emit light in the visible range (florescent dyes). Dyes for the pur¬ poses of this invention also include compounds having an absorption maximum in the range from 250 to 400 nm which on irradiation with UV light emit fluorescence radiation in the visible range (optical brighteners). Dyes in the sense of this invention further include organic compounds which absorb light of wavelength < 400 nm and deactivate it without radiation (UV stabilizers). In general the water-soluble dyes contain ionic functional groups which improve the solubility in the aqueous solvent. The modification carried out may be cationic or ani¬ onic. Suitable substituents are, for example, sulfonic, carboxylic and phosphoric acid radicals and also ammonium and alkylammonium radicals.

Dyes suitable in accordance with the invention embrace different classes of dye with different chromophores, examples being monoazo and bisazo dyes, triarylmethane dyes, metal complex dyes, such as phthalocyanine dyes, quinophthalones and methine and azamethine dyes. Preferred dyes among these are the monoazo and bisazo dyes, quinophthalones, methine and azamethine dyes and metal complex dyes, such as phthalocyanine dyes.

Mention may be made by way of example of the following numbers from the Colour Index:

Direct Yellow 4, 5, 10, 11 , 50, 127, 137, 147, 153; Acid Orange 7, 8; Direct Orange 15, 34, 102; Direct Red 81 , 239, 252-255; Direct Violet 9, 51 ; Acid Blue 9, 86; Direct Blue 199, 218, 267, 273, 279, 281 ; Acid Black 194, 208, 210, 221 ; Direct Black 19, 161 , 170 and 171;

Basic Red 1 , Basic Red 14, Basic Blue 7, Basic Blue 11 , Basic Blue 26, Basic Violet 1 , Basic Violet 4, Basic Violet 10 etc.; reactive dyes such as Reactive Red 120, Reactive Red 2, etc.

The dyes further include complexes of basic and acidic dyes and complexes of anionic and cationic dyes, an example being the complex of chrysoidine base and metanil yel¬ low acid.

In accordance with the invention the dyes also include optical brighteners which are at least partly soluble in water.

The organic dyes also include, by definition, UV-absorbing compounds (UV stabilizers) which deactivate the absorbed radiation nonradiatively. Compounds of this kind are frequently used as UV absorbers in sun protection products. They include derivatives of p-aminobenzoic acid, in particular its esters; 2-phenylbenzimidazole-5-sulfonic acid and salts thereof, salicylates, cinnamates, benzophenones, 2-phenylbenzimidazole-4- sulfonic acid and salts thereof, urocanic acid, salts thereof and esters thereof, ben- zoxazoles, benzotriazoles, benzylidenecamphor and its derivatives, 3,3'-(1 ,4- phenylendimethine)-bis(7,7-dimethyl-2-oxobicyclo[2.2.1]heptane-1-sulfonic acid) and salts thereof, 2-hydroxy-4-methoxy-benzophenon-5-sulfonic acid and salts thereof, dimethoxyphenylglyoxalic acid and salts thereof, 3-(4'sulfobenzyliden)- bornan-2-one and salts thereof, 2,2'-(1.4-phenylen)-bis-1 H-benzimidazole-4,6- disulfonic acid and salts therof.

Likewise highly suitable are Colour Index dyes used in cosmetology, such as 42045, 42051 , 42080, 42090, 42735, 44045, 61585, 62045, 73015, 74180, bromothymol blue, caramel, 10316, 13015, 18690, 18820, 18965, 19140, 45350, 47005, 75100, lactofla- vin, 10020, 42053, 42100, 42170, 44090, 59040, 61570, 75810, bromocresol green, 14270, 15510, 15980, 15985, 16230, 20170, 40215, 14700, 14720, 14815, 15620, 16035, 16185, 16255, 16290, 17200, 18050, 18130, 18736, 24790, 27290, 45100, 45220, 45380, 45405, 45410, 45425, 45430, 75470, beetroot red, anthocyans, Acid Red 195, Black 20470, 27755, 28440, 50420, 42510, 42520, 45190, 60725 and 60730.

As preferred dyes mention may be made by way of example of the dyes having the Colour Indices 15510, 15985, 16255, 17200, 19140, 20170, 42053, 42090, 45350, 45380, 45410, 47005, 60725, 61570 and 75470.

Depending on the color intensity and solubility of the dye the microcapsule generally contains 0.1% by weight, based on the hydrophilic solvent, preferably from 1 to 50% by weight, more preferably from 5 to 40% by weight and in particular from 5 to 30% by weight of at least one dye.

The water-soluble organic substances to be encapsulated in accordance with the in¬ vention may be used individually or in the form of mixtures of two or more different wa¬ ter-soluble organic substances. By this means it is possible if desired to obtain, in ac- cordance with the invention, microcapsule dispersions which contain either a single water-soluble organic substance or a mixture thereof, such as a mixture of different dyes, for example.

The capsule wall of the invention comprises one or different polyureas, which consti- tute(s) the reaction product of the at least one polyfunctional amine having a number- average molecular weight of from 600 to 380 000 g/mol, for use in accordance with the invention, and/or of the at least one alkyl diamine having 2 to 10, preferably 2 to 6, car¬ bon atoms with di- and/or polyisocyanates. In one preferred embodiment the capsule wall is composed of the stated reaction products.

Suitable are di- and polyisocyanates, such as aliphatic, cycloaliphatic, araliphatic, aro¬ matic and heterocyclic di- and polyisocyanates, as are described by W. Siefken in Justus Liebigs Annalen der Chemie, 562, pages 75 to 136, for example ethylene diiso- cyanate, 1 ,4-tetramethylene diisocyanate, 1 ,6-hexamethylene diisocyanate, 1 ,12- dodecane diisocyanate, cyclobutane 1 ,3-diisocyanate, cyclohexane 1 ,3- and 1 ,4- diisocyanate and any mixtures of these isomers, 1-isocyanato-3,3,5-trimethyl-5- isocyanatomethylcyclohexane, as described, for example, in DE-B 1 202 785 and US patent 3 401 190, 2,4- and 2,6-hexahydrotolylene diisocyanate, and any mixtures of these isomers, hexahydro-1 ,3- and -1 ,4-phenylene diisocyanate, perhydro-1 ,4'- and - 4,4'-diphenylmethane diisocyanate, 1 ,3- and 1 ,4-phenylene diisocyanate, 2,4- and 2,6- tolylene diisocyanate, and any mixtures of these isomers, diphenylmethane 2,4'- and 4,4'-diisocyanate, naphthylene 1 ,5-diisocyanate, thphenylmethane 4,4',4"-triisocyanate, polyphenylpolymethylene polyisocyanates, as obtained by aniline-formaldehyde con¬ densation and subsequent phosgenation and described, for example, in GB patents 874 430 and 848 671 , m- and p-isocyanatophenylsulfonyl isocyanates according to US patent 3 454 606, perchlorinated aryl polyisocyanates, as are described, for example, in DE-B 1 157 601 , polyisocyanates containing carbodiimide groups, as are described in DE patent 1 092 007 (= US patent 3 152 162), diisocyanates as described in US patent 3 492 330, polyisocyanates containing allophanate groups, as are described in GB patent 761 626 and the published NL patent application 7 102 524, polyisocyanates containing isocyanurate groups, as described, for example, in US patent 3 001 973, in the German patents 1 022 789, 1 222 067 and 1 027 394, and in German laid-open patents 1 929 034 and 2 004 048, polyisocyanates containing urethane groups, as de¬ scribed, for example, in BE patent 752 261 or in US patent 3 394 164, polyisocyanates containing acylated urea groups according to German patent 1 230 778, polyisocy¬ anates containing biuret groups, as described, for example, in German patent 1 101 394 and in GB patent 889 050, polyisocyanates prepared by telomerization reac¬ tions, as are described, for example, in US patent 3 654 106, polyisocyanates contain¬ ing ether groups, as are mentioned, for example, in GB patents 965 474 and 1 072 956, in US patent 3 567 763 and in German patent 1 231 688, reaction products of the abovementioned isocyanates with acetals according to German patent 1 072 385, and polyisocyanates containing polymeric fatty acid radicals in accordance with US patent 3 455 883.

It is also possible to use the distillation residues containing isocyanate groups which form during the industrial preparation of isocyanate, optionally dissolved in one or more of the abovementioned polyisocyanates. It is further possible to use any mixtures of the abovementioned polyisocyanates.

Suitable modified, aliphatic isocyanates are, for example, those based on hexamethyl- ene 1 ,6-diisocyanate, m-xylylene diisocyanate, 4,4'-diisocyanatodicyclohexylmethane and isophorone diisocyanate, which contain at least two isocyanate groups per mole¬ cule.

Also suitable are, for example, polyisocyanates based on derivatives of hexamethylene 1 ,6-diisocyanate with a biuret structure as described in DE-B 1 101 394, DE-B 1 453 543, DE-A 1 568 017 and DE-A 1 931 055. It is also possible to use polyisocyanate-polyuretonimines, as arise as a result of the carbodiimidization of hexamethylene 1 ,6-diisocyanate, containing biuret groups, with organophosphorus catalysts, where carbodiimide groups formed primarily react with further isocyanate groups to give uretonimine groups.

It is also possible to use isocyanurate-modified polyisocyanates containing more than two terminal isocyanate groups, e.g., those whose preparation on the basis of hexame¬ thylene diisocyanate is described in DE-A 2 839 133. Other isocyanurate-modified polyisocyanates can be obtained analogously thereto.

It is also possible to use mixtures of said isocyanates, e.g., mixtures of aliphatic isocy- anates, mixtures of aromatic isocyanates, mixtures of aliphatic and aromatic isocy¬ anates, in particular mixtures which optionally comprise modified diphenylmethane diisocyanates.

The di- and/or polyisocyanates described here can also be used as mixtures with di- and polycarbonyl chlorides, such as sebacoyl chloride, terephthaloyl chloride, adipoyl dichloride, oxaloyl dichloride, tricarballyloyl trichloride and 1 ,2,4,5-benzene- carbonyl tetrachloride, with di- and polysulfonyl chlorides, such as 1 ,3-benzenesulfonyl dichloride and 1 ,3,5-benzenesulfonyl trichloride, phosgene and with dichloro- and poly- chloroformic esters, such as 1 ,3,5-benzenetrichloroformate and ethylenebischlorofor- mate.

Preferred isocyanates are biuretic hexamethylene diisocyanate, optionally in a mixture with 4,4'-diphenylmethane isocyanate and optionally 2,4-diphenylmethane isocyanate, trimerized hexamethylene diisocyanate optionally in a mixture with 4,4'-diphenyl- methane diisocyanate and optionally 2,4-diphenylmethane diisocyanate.

Further suitable diisocyanates are the alkylbenzene diisocyanates and alkoxybenzene diisocyanates specified in DE-A 3 105 776 and 3 521 126, including those in the form of their biuret isocyanate uretdione oligomers.

Preferred di- or polyisocyanates are 4,4'-diphenylmethane diisocyanate, the mixtures of monomeric diphenylmethane diisocyanates and oligomeric diphenylmethane diisocy¬ anates (polymer MDI), tetramethylene diisocyanate, tetramethylene diisocyanate trimers, hexamethylene diisocyanate, hexamethylene diisocyanate trimers, isophorone diisocyanate trimer, 4,4'-methylenebis(cyclohexyl) diisocyanate, xylylene diisocyanate, tetramethylxylylene diisocyanate, dodecyl diisocyanate, lysine alkyl ester diisocyanate, where alkyl is C₁ to C₁₀, 2,2,4- or 2,4,4-trimethyl-1 ,6-hexamethylene diisocyanate, 2- butyl-2-ethylpentamethylene diisocyanate, 1 ,4-diisocyanato cyclohexane or 4- isocyanatomethyl-1 ,8-octamethylene diisocyanate. Further preference is given to di- or polyisocyanates having NCO groups of different reactivity, such as 2,4-tolylene diisocyanate (2,4-TDI), 2,4'-diphenylmethane diisocy- anate (2,4'-MDI), triisocyanatotoluene, isophorone diisocyanate (IPDI), 2-butyl-2- ethylpentamethylene diisocyanate, 2-isocyanatopropyl-cyclohexyl isocyanate, 3(4)- isocyanatomethyl-i-methylcyclohexyl isocyanate, 1 ,4-diisocyanato-4-methylpentane, 2,4'-methylene-bis(cyclohexyl) diisocyanate and 4-methylcyclohexane 1 ,3-diisocyanate (H-TDI). Particular preference is also given to isocyanates whose NCO groups are ini¬ tially equally reactive, but in which a reactivity decrease in the case of the second NCO group can be induced as a result of a first addition of an alcohol or amine onto an NCO group. Examples thereof are isocyanates whose NCO groups are coupled via a delo- calized electron system, e.g., 1 ,3- and 1 ,4-phenylene diisocyanate, 1 ,5-naphthylene diisocyanate, diphenyl diisocyanate, tolidine diisocyanate or 2,6-tolylene diisocyanate.

A group of isocyanates which is additionally preferred according to the invention is rep- resented by the following compounds: tetramethylene diisocyanate, hexamethylene diisocyanate, dodecamethylene diisocyanate, 1 ,4-diisocyanatocyclohexane, 4,4'- di(isocyanatocyclohexyl)methane, trimethylhexane diisocyanate, tetramethylhexane diisocyanate, 1-isocyanato-3,3,5-trimethyl-5-(isocyanatomethyl)cyclohexane (IPDI), 2,4-tolylene diisocyanate and 2,6-tolylene diisocyanate, tetramethylxylylene diisocy- anate, 2,4'-diisocyanatodiphenylmethane and 4,4'-diisocyanatodiphenylmethane.

Particular preference is given to oligo- or polyisocyanates which can be prepared from the stated di- or polyisocyanates or mixtures thereof by linking by means of urethane, allophanate, urea, biuret, uretdione, amide, isocyanurate, carbodiimide, uretonimine, oxadiazinetrione or iminooxadiazinedione structures. Preference in turn among these is given to oligo- or polyisocyanates which can be prepared from the stated di- or polyiso¬ cyanates or mixtures thereof by linking by means of urethane, isocyanurate, allophan¬ ate, urea or biuret structures.

Reactants that can be reacted with the di- and/or poyisocyanates mentioned in a man¬ ner according to the invention are polyfunctional amines having an average molecular weight of from about 600 to about 380 000 g/rnol, preferably from about 600 to about 300 000 g/mol, more preferably from about 600 to about 100 000 g/mol and very pref¬ erably from about 800 to about 70 000 g/mol. These compounds can each be used singly or as mixtures with one another. The term "polyfunctional amine" embraces, for the purposes of the present invention, polyvinylamines of the general formula (I),

(I)

NH.

polyethylenimines (polyethylenamines) of the general formula (II) or (III) respectively,

-[(CH₂)₂-NH]_X-[(CH₂)₂-N]_y-

(NI)

[(CH₂)₂-NH]₂-(CH₂)₂-NH₂

and/or polyoxyalkylenamines of the general formula (IV) to (VI)

NH₂CH(CH₃)CH₂-[OCH₂CH(CH₃)]_X-NH₂

(IV)

CH₂[OCH₂CH(CH₃)_X-NH₂

CH₃CH₂CCH₂[OCH₂CH(CH₃)_y-NH₂ (^V)

CH₂[OCH₂CH(CH₃)_Z-NH₂

CH₂[OCH₂CHCH(CH₃)]_X-NH₂

CH₂[OCH₂CHCH(CH₃)]_y-NH₂ ^

I CH₂[OCH₂CHCH(CH₃)J₂-NH₂

where the indices x, y and z in the formulae (I) to (IV) are integers each selected inde¬ pendently of one another such that the respective polyfunctional amines have molecu¬ lar weights situated within the ranges indicated above. Examples that may be men- tioned of the class of compound of the polyoxyalkylenamines are the JEFFAMINE^® products such as JEFFAMINE^® D-230, JEFFAMINE^® D-400, JEFFAMINE^® D-2000, JEFFAMINE^® T-403, XTJ-510 (D-4000), XTJ-500 (ED-600), XTJ 501 (ED-900), XTJ- 502 (ED-2003), XTJ 509 (T-3000) and JEFFAMINE^® T-5000.

Polyfunctional amines preferred in the context of the present invention are the polyvi- nylamines of the formula (I) and the branched polyethylenimines of the formula (III), especially the polyvinylamines of the formula (I). Polyvinylamines of this kind are ob¬ tainable, for example, by hydrolyzing the corresponding polyvinylformamides of the formula (VII)

Where the polyvinylamine used in accordance with the invention is the product of the hydrolysis of a polyvinylformamide it may still contain polyvinylformamide of the formula (IV), depending on the extent or completeness of the hydrolysis that has occurred. For the purposes of the present invention it is preferred to use hydrolysis products having a degree of hydrolysis of from about 60 to about 100% (mol/mol) which therefore contain about 40 to about 0% (mol/mol) of the polyvinylformamide used originally. Preference is given to using hydrolysis products which have a degree of hydrolysis of from about 80 to about 100%, more preferably from about 90 to about 100% and with particular preference from about 95 to about 100%.

The polyethylenimines likewise preferred as polyfunctional amines in accordance with the invention are obtainable by methods known per se to the skilled worker, as are de- scribed, for example, in Rompp Chemie Lexikon, 9th edition, 1992.

The stated polyfunctional amines may each be used individually or in the form of mix¬ tures of about 2 to about 5 different amines from among those stated, for preparing the microcapsule dispersions of the invention.

In one preferred embodiment they are used together with alkyldiamines having 2 to 10, preferably 2 to 6 carbon atoms. Suitable alkyldiamines are for example aliphatic al¬ kyldiamines having 2 to 10, preferably 2 to 6, carbon atoms, such as, for example, ethylenediamine, propylenediamine, butylenediamine and/or hexamethylenediamine, preferably ethylenediamine and/or hexamethylenediamine. Likewise suitable are the cyclic alkyldiamines such as, for example, piperazine, 2,5-dimethylpiperazine, amino-3- aminomethyl-3,5,5-trimethylcyclohexane (isophoronediamine, IPDA), 4,4'-diamino- dicyclohexylmethane and/or 1 ,4-diaminocyclohexane. The stated alkyldiamines may also each be used individually or in the form of mixtures of the compounds stated.

In one preferred embodiment of the preparation of the microcapsule dispersions of the invention the selected polyfunctional amine, in particular the selected polyvinylamine, is used in the form of mixtures with one of the stated alkyldiamines or with a mixture of the stated alkyldiamines. In that case the mixing ratio is advantageously selected such that about 20 to about 65%, preferably about 30 to about 60%, in particular about 40 to about 55% of the amino groups in the mixture originate from the selected alkyldiamine or mixture of selected alkyldiamines. The amount of isocyanates to be used according to the invention varies within the scope customary for interracial polyaddition processes. Thus generally 20 to 150% by weight, preferably 40 to 150% by weight, of isocyanate are used based on the discon¬ tinuous phase provided for the encapsulation (hydrophilic solvent + water-soluble sub- stance). Good shear stabilities of the capsules are observed from amounts as low as 40% by weight. Amounts above 150% by weight are possible, but do not generally lead to more stable capsule walls.

The theoretical amount of the isocyanate necessary for wall forming is calculated from the amount of reactive amino groups of the reactant component(s) used. These quanti¬ tative ratios are usually expressed by equivalent weights.

42 equivalent weight X 100

NCO content ^*)

^*) = e.g., to be determined titrimetrically (DIN 53 185)

equivalent weight reactant = molar Weight reactant number of reactive groups in the molecule

Reaction of all of the NCO groups present in the oil phase requires at least theoretically equal numbers of NH₂ and/or -NH groups. It is therefore advantageous to use the iso¬ cyanate and the polyfunctional amine and optionally selected alkyldiamine in the ratio of their equivalent weights. It is, however, likewise possible to deviate from the stoichiometrically calculated amount of crosslinker either downward, since, during inter- facial polyaddition processes, a side reaction of the isocyanate with the water present in excess cannot be ruled out, or to use an excess of the reactant component, because such an excess is uncritical, and because, in the case of the polyfunctional amines used, steric reasons mean that generally not all of the amino funtionalities are reacted.

In particular, therefore, the reactants are used in an amount between about 50 and 250% by weight of the theoretically calculated amount. This amount is preferably be¬ tween about 90 and 200% by weight, in particular between about 105 and 170% by weight, based on the theoretically calculated amount.

The present invention further provides a process for the preparation of the microcap¬ sule dispersion according to the invention, in which an emulsion of the hydrophilic sol¬ vent in the hydrophobic solvent is prepared with the aid of a surface-active substance, where the hydrophilic phase comprises the water-soluble organic substance and the NH or NH₂ group-carrying reactants which react with di- and/or polyisocyanate groups, and di- and/or polyisocya nates are added to the emulsion.

In order to obtain a stable emulsion, surface-active substances such as protective col- loids and/or emulsifiers are required. Usually, surface-active substances which mix with the hydrophobic phase are used.

Preferred protective colloids are linear block copolymers with a hydrophobic structural unit of length > 50 A, alone or in mixtures with other surface-active substances. The linear block copolymers are given by the formula

C_w ( B-A-B_y ) _XD_Z

in which w is 0 or 1 , x is a part of 1 or more, y is 0 or 1 and A is a hydrophilic structural unit, having a solubility in water at 25°C of > 1 % by weight and a number-average mo¬ lecular weight of from 200 to 50 000 g/mol, which is bonded covalently to the B blocks, and B is a hydrophobic structural unit having a number-average molecular weight of from 300 to 60 000 g/mol and a solubility in water at 25°C of < 1 % by weight and can form covalent bonds to A; and in which C and D are end groups which, dependently on one another, may be A or B. The end groups may be identical or different and are de¬ pendent on the preparation process.

Examples of hydrophilic groups are polyethylene oxides, poly(1 ,3-dioxolane), copoly¬ mers of polyethylene oxide or poly(1 ,3-dioxolane), poly(2-methyl-2-oxazoline), poly(glycidyltrimethylammonium chloride) and polymethylene oxide.

Examples of hydrophobic groups are polyesters in which the hydrophobic moiety is a steric barrier > 50 A, preferably > 75 A, in particular > 100 A. The polyesters are de¬ rived from components such as 2-hydroxybutanoic acid, 3-hydroxybutanoic acid, 4-hydroxybutanoic acid, 2-hydroxycaproic acid, 10-hydrodecanoic acid, 12-hydroxy- dodecanoic acid, 16-hydroxyhexadecanoic acid, 2-hydroxyisobutanoic acid, 2-(4- hydroxyphenoxy)propionic acid, 4-hydroxyphenylpyruvic acid, 12- hydroxys tea he acid, 2-hydroxyvaleric acid, polylactones of caprolactone and butyrolactone, polylactams of caprolactam, polyurethanes and polyisobutylenes.

The linear block copolymers contain both hydrophilic units and hydrophobic units. The block polymers have a molecular weight above 1000 g/mol and a length of the hydro¬ phobic moiety of > 50 A calculated according to the law of cosines. These sizes are calculated for the extended configuration, taking into consideration the bond lengths and angles given in the literature. The preparation of these units is general knowledge. Preparation processes are, for example, condensation reaction of hydroxy acid, con¬ densations of polyols, such as diols, with polycarboxylic acids, such as dicarboxylic acids. Also suitable is the polymerization of lactones and lactams, and the reaction of polyols with polyisocyanates. Hydrophobic polymer units are reacted with the hydro- philic units, as generally known, for example by condensation reaction and coupling reaction. The preparation of such block copolymers is described, for example, in US 4 203 877, to which reference is expressly made. The proportion of linear block copolymer is preferably 20 - 100% by weight of the total amount of surface-active sub¬ stance used.

Suitable surface-active substances are also the emulsifiers customarily used for water- in-oil emulsions, for example

C₁₂-Ci₈ sorbitan fatty acid esters, esters of hydroxystearic acid and C₁₂-C₃₀ fatty alcohols, mono- and diesters of C₁₂-C₁₈ fatty acids and glycerol or polyglycerol, - condensates of ethylene oxide and propylene glycols, oxypropylenated/oxyethylenated C₁₂-C₂₀ fatty alcohols, polycyclic alcohols, such as sterols, aliphatic alcohols with a high molecular weight, such as lanolin, mixtures of oxypropylenated/polyglycerylated alcohols and magnesium isostearate, succinic esters of polyoxyethylated or polyoxypropylenated fatty alcohols, the lanolates and stearates of magnesium, calcium, lithium, zinc and aluminum, optionally as a mixture with hydrogenated lanolin, lanolin alcohol, or stearic acid or stearyl alcohol.

Emulsifiers of the Span® series have proven particularly advantageous. These are cyclized sorbitol, sometimes polyesterified with a fatty acid, where the base structure can also be substituted by further radicals known from surface-active compounds, for example by polyethylene oxide. Examples which may be mentioned are the sorbitan esters with lauric, palmitic, stearic and oleic acid, such as Span® 80 (sorbitan monoo- leate), Span® 60 (sorbitan monostearate) and Span® 85 (sorbitan trioleate).

In one preferred embodiment oxypropylenated/oxyethylenated C₁₂-C₂₀ fatty alcohols are used as mixing component with further surface-active substances. These fatty al- cohols usually have 3 to 12 ethylene oxide and/or propylene oxide units.

Preference is given to using C₁₂-C₁₈ sorbitan fatty acid esters as emulsifier. These can be used individually, in their mixtures and/or as mixtures with other abovementioned types of emulsifier. The proportion of sorbitan fatty acid esters is preferably 20 - 100% by weight of the total amount of surface-active substance used. In one preferred embodiment a mixture of surface-active substances comprising the above-defined linear block copolymers and C₁₂-C₁₈ sorbitan fatty acid esters is chosen.

With particular preference a mixture of surface-active substances comprising the linear block copolymers, C₁₂-C₁₈ sorbitan fatty acid esters and oxypropylenated/oxy- ethylenated C₁₂-C₂₀ fatty alcohols are chosen.

Preference is given to those mixtures containing 20 to 95% by weight, in particular 30 to 75% by weight, of linear block copolymer and 5 to 80% by weight, in particular 25 to 70% by weight, of C₁₂-C₁₈ sorbitan fatty acid esters, based on the total amount of sur¬ face-active substance. The proportion of oxypropylenated/oxyethylenated Ci₂-C₂₀ fatty alcohol is preferably 0 to 20% by weight.

Particular preference is given to mixtures of surface-active substances containing es- sentially 30 to 50% by weight of linear block copolymer, 40 to 60% by weight of C₁₂-C₁₈ sorbitan fatty acid esters and 2 to 10% by weight of oxypropylenated/oxy-ethylenated C₁₂-C₂₀ fatty alcohols, based on the total amount of surface-active substance.

The optimum amount of surface-active substance is influenced firstly by the surface- active substance itself and secondly by the reaction temperature, the desired micro¬ capsule size and the wall materials. The optimally required amount can be readily de¬ termined by simple serial experiments. For preparing the emulsion the surface-active substance is generally used in an amount of 0.01 to 10% by weight, preferably 0.05 to 5% by weight and in particular 0.1 to 2% by weight, based on the hydrophobic phase.

To prepare the microcapsules according to the invention, according to one preferred embodiment, a solution of water-soluble organic substance, a dye for example, and at least one polyfunctinal amine as described above and, if appropriate, one or more dif¬ ferent alkyldiamines in the hydrophilic solvent can be added to the hydrophobic solvent. With the help of the surface-active substance, a stable emulsion is prepared with stir¬ ring. According to a likewise preferred variant, the water-soluble organic substances and the reactant(s) are added only to the stable emulsion or during the emulsifying step. The isocyanate can then be metered into such an emulsion. Generally, this starts the interfacial polyaddition or polycondensation and thus the formation of the wall.

The selected isocyanate component can be added continuously or discontinuously. The isocyanate component is successfully added continuously, in which case the rate of addition can be held constant or varied during the reaction. In one particularly pre¬ ferred embodiment of the preparation of the microcapsule dispersions of the invention a procedure is followed in which the di- and/or polyisocyanates are added to the emul¬ sion continuously and at a rate which decreases as reaction progresses, i.e., in gradi¬ ent mode. This preferred preparation process makes it possible in particular to provide the microcapsule dispersions of the invention with high encapsulation efficiencies in terms of the water-soluble organic substance to be encapsulated. This means that by this preparation process, advantageously, dispersions are obtained of microcapsules whose walls are distinguished by particularly low permeability to the encapsulated wa- ter-soluble organic substance.

The interface reaction can proceed, for example, at temperatures in the range from -3 to +70⁰C₁ preference being given to working at 15 to 65⁰C.

Depending on the size of the capsules to be prepared, the core material is dispersed in a known manner. For the preparation of large capsules, dispersion using effective stir¬ rers, in particular propeller or impeller stirrers, suffices. Small capsules, particularly if the size is to be less than 50 μrπ, require homogenizing or dispersing machines, it be¬ ing possible for these devices to be provided with or without forced-flow means.

The homogenization can also be carried out using ultrasound (e.g., Branson Sonifier Il 450). For homogenization by means of ultrasound, suitable equipment is, for exam¬ ple, that described in GB 2250930 and US 5,108,654.

The capsule size can be controlled via the rotational speed of the dispersion de- vice/homogenization apparatus and/or using suitable thickeners such as polyisobuty- lenes (Glissopal®, BASF Aktiengesellschaft) in dependence of their concentration mo¬ lecular weight thereof, i.e., via the viscosity of the continuous oil phase, within certain limits. In this connection, as the rotational speed increases up to a limiting speed, the size of the dispersed particles decreases. Further thickeners that can be used include weathered aluminas such as, for example Bentone® 38.

In this connection it is important that the dispersion devices are used at the start of capsule formation. In the case of continuously operating devices with forced flow, it is advantageous to pass the emulsion through the shear field a number of times.

As mentioned in the beginning, the microcapsules that can be prepared according to the invention may be subjected to an aftertreatment. Suitable reagents for such after- treatment are compounds of low molecular weight that are capable of completing the reaction between the isocyanate component used and the amine component used, i.e., the chosen polyfunctional amines and/or the chosen alkyldiamines, or of reacting with unreacted isocyanate functions. Examples that may be mentioned thereof include the following reagents for instance: 2-aminomethylpropanol, propylamine, butylamine, pen- tylamine, hexylamine, 2-aminocyclohexanol and octylamine. A preferred aftertreatment reagent is 2-aminomethylpropanol. Using the process according to the invention it is possible to prepare microcapsule dis¬ persions with a microcapsules content of from 5 to 50% by weight. The microcapsules are individual capsules. If suitable conditions are chosen during the dispersion it is possible to produce capsules with an average particle size in the range from about 0.1 to 200 μm and above. Preference is given to capsules with an average particle size of from about 0.1 to 50 μm, in particular from about 0.1 to about 30 μm most preferred from about 0.1 to about 10 μm. The average particle diameter is the z-average particle diameter, determined by Fraunhofer diffraction with Mie correction for counting individ¬ ual particles. It is usually determined using a Malvern Mastersizer S. The very narrow size distribution of the capsules is a particular advantage.

The microcapsule dispersions according to the invention can be incorporated into cos¬ metic compositions in a known manner. Incorporation into the cosmetic composition takes place by the procedures customary for this purpose, usually by stirring and ho- mogenizing into the other constituents of the cosmetic composition.

Examples of cosmetic compositions which are formulated as decorative cosmetic com¬ positions are compositions for the treatment of facial skin, in particular in the eye area, such as kohl pencils, eyeliner pencils, eyebrow pencils, eyeshadows, cream blusher, powder blusher, foundation, make-up, e.g. stage make-up, lipsticks.

Further cosmetic compositions that may be mentioned include compositions compris¬ ing UV-absorbing compounds, such as, for example, sun protection products such as sun protection creams or sun protective sticks, for example.

In the case of cosmetic compositions which consist exclusively of oils or fats, in particu¬ lar those which have a solid form, e.g. pencils, such as kohl pencils, eyeliner pencils, eyebrow pencils, stick stage make-up, lipsticks and the like, and in the case of coarse or fine powder cosmetic compositions, such as eyeshadows and cream blusher or loose powder blusher, preference is given to using microcapsule dispersions.

The amount of microcapsules in the cosmetic composition is guided primarily by the desired color impression which the decorative cosmetic composition is to have. De¬ pending on the nature of the cosmetic composition and the desired color impression, the microcapsules content of the cosmetic composition is in the range from 0.1 to 50% by weight, based on the total weight of the cosmetic composition.

The present invention further provides microcapsules obtainable by removing the hy¬ drophobic solvent from the microcapsule dispersions of the invention. This can be done by any methods which are known to the skilled worker and appear suitable: for exam¬ ple, by filtration or extraction of the microcapsule dispersions of the invention with a suitable solvent such as heptane, for example, with subsequent drying of the micro¬ capsules.

The microcapsules obtainable in this way are also suitable for all of the uses referred to above for the microcapsule dispersions of the invention - for example, for incorporation into cosmetic compositions.

The examples below serve to illustrate the invention without restricting it in any way whatsoever:

General details:

The viscosities were measured in accordance with ISO 3219 (DIN 53019) with the Par Physika viscometer (MC20) in the Z3DIN at a shear rate of 100 s^'1 and a tempera¬ ture of 23°C. The capsule diameter was determined visually at 500-times magnification using a microscope from Olympus (BX 51 ).

Instructions for determining the encapsulation efficiency:

0.2 g of a uniformly mixed sample of the microcapsule dispersion obtained was weighed into a 50 ml centrifuge tube (polyethylene). 10 ml of an extraction solution (1 :1 mixture of fully deionized water and 2-propanol) were added to the sample. The solu¬ tion was mixed thoroughly and then centrifuged for 20 minutes. Thereafter the super¬ natant solution was transferred to a glass beaker. The wash extraction process was repeated until the supernatant liquid was colorless. The collected wash solutions were made up to 100 ml with the extraction solution. One portion of the collected solution was filtered through a 0.2 μm filter and the amount of water-soluble organic substance for encapsulation was determined by UV spectroscopy using a UV-VIS spectrometer from HP (HP 8453).

The encapsulation efficiency is calculated by the following formula:

A - B Encapsulation efficiency = ^* 100

where A is the total amount of organic material for encapsulation present in the ana¬ lyzed sample and B is the product of the UV-spectroscopically determined concentra- tion and the volume of the analyzed sample.

Example 1 :

A 4 I stirred vessel was charged with a solution of 5.8 g of Span® 80 (sorbitan monoo- leate, Roth), 1.2 g of Cremophor® A6 [75% by weight of cetareth-6 (ethoxylated cetyl alcohol) 25% by weight of stearyl alcohol, BASF] and 8.2 g of Arlacel® P135 (PEG-30 dipolyhydroxystearate, Atlas Chemie) in 1306.9 g of Miglyol® 812 (decanoyl/ octanoyl glyceride; Sasol). Following addition of a solution of 8.8 g of ethylenediamine (Merck, 99%) and 46.9 g of C.I. 42090 (BASF Aktiengesellschaft), 23 g of polyvinyl- amine (Lupamin® 5095SF, dialyzed, degree of hydrolysis > 90%, molecular weight about 45 000 g/mol, BASF Aktiengesellschaft), 6.9 g of polyvinylamine (Lupamin® 1595SF, dialyzed, degree of hydrolysis > 90%, molecular weight < 10 000 g/mol, BASF Aktiengesellschaft) in 312.6 g of water, a water-in-oil emulsion was produced with a rotational speed of 2000 rpm (RZR 2102, Heidolph). At a stirring speed of 2000 rpm a solution of 195.9 g of Basonat® TU 75E (polyfunctional tolylene diisocyanate (TDI) adduct of TDI and polyol, 75% strength by weight in ethyl acetate, BASF Aktiengesell- schaft) in 1 151.9 g of Miglyol was added over the course of 90 minutes. After the end of the addition the dispersion was heated to 60⁰C over the course of 15 minutes and stirred for a further 60 minutes. Thereafter the reaction mixture was cooled to room temperature over the course of 15 minutes. 5.1 g of 2-aminomethylpropanol (Merck, 95%) were added and stirring was continued at room temperature for 40 minutes. The dispersion obtained was milky blue and according to microscopic evaluation contained individual capsules predominantly 1-5 μm in diameter. The viscosity was 1370 mPas (100 s^"1) and the solids content was 20 percent by weight. UV-Vis spectroscopy indi¬ cated an encapsulation efficiency of 76%.

Example 2:

A cylindrical 4 I stirred vessel was charged with a solution of 4.7 g of Span® 80 (sorbi- tan monooleate, Roth), 1.2 g of Span® 85 (sorbitan trioleate, Roth), 1.2 g of Cremo- phor® A6 [75% by weight Cetareth-6 (ethoxylated cetyl alcohol) 25% by weight stearyl alcohol, BASF] and 4.7 g of Arlacel® P135 (PEG-30 dipolyhydroxystearate, Atlas Chemie) in 1295.6 g of Miglyol® 812 (decanoyl/octanoyl glyceride; Sasol). A solution of 8.8 g of ethylenediamine (Merck, 99%), 23.0 g of polyvinylamine (Lupamin® 5095SF, dialyzed, degree of hydrolysis > 90%, molecular weight about 45 000 g/mol, BASF Ak¬ tiengesellschaft), 6.9 g of polyvinylamine (Lupamin® 1595SF, dialyzed, degree of hy¬ drolysis > 90%, molecular weight < 10 000 g/mol, BASF Aktiengesellschaft) and 47 g of C.I. 42090 (BASF) in 313.3 g of water was added and dispersion was carried out for four minutes using a disperser (Pendraulik stirrer model LD-50) at a rotational speed of 4000 rpm (RZR 2102, Heidolph). The water-in-oil emulsion obtained in this way was admixed at a stirring speed of 2000 rpm with a solution of 195.8 g of Basonat® TU 75E (polyfunctional tolylene diisocyanate adduct of TDI and polyol, 75% strength by weight in ethyl acetate, BASF Aktiengesellschaft) in 1080.8 g of Miglyol over the course of 90 minutes in a linearly descending gradient. After the end of the addition the disper¬ sion was heated to 60⁰C over the course of 15 minutes and stirred for a further 60 min¬ utes. Thereafter the reaction mixture was cooled to room temperature over the course of 15 minutes. 5.1 g of 2-aminomethylpropanol (Merck, 95%) were added and the mix- ture was stirred at room temperature for 40 minutes more. The dispersion obtained was milky blue and according to microscopic evaluation contained individual capsules pre¬ dominantly 1-5 μm in diameter. The viscosity was 510 mPas (100 s^'1) and the solids content 20 percent by weight. UV-Vis spectroscopy indicated an encapsulation effi¬ ciency of 98%.

Example 3: By the method of example 1 a microcapsule dispersion was prepared, using 46.9 g of Sicovit® Cochineal Red 8OE 124 (BASF Aktiengesellschaft) instead of C.I. 42090 (BASF Aktiengesellschaft). The dispersion obtained was milky red and according to microscopic evaluation contained individual capsules predominantly 1-5 μm in diame¬ ter. The viscosity was 1180 mPas (100 s^'1) and the solids content 20 percent by weight. UV-Vis spectroscopy indicated an encapsulation efficiency of 81 %.

Example 4:

By the method of example 2 a microcapsule dispersion was prepared, using 46.9 g of Sicovit® Cochineal Red 8OE 124 (BASF Aktiengesellschaft) instead of C.I. 42090 (BASF Aktiengesellschaft). The dispersion obtained was milky red and according to microscopic evaluation contained individual capsules predominantly 1-5 μm in diame¬ ter. The viscosity was 21 10 mPas (100 s^~1) and the solids content 20 percent by weight. UV-Vis spectroscopy indicated an encapsulation efficiency of 91%.

Example 5:

Using the method of example 4 a microcapsule dispersion was prepared, using as amine component 68.5 g of polyvinylamine (Lupamin® 5095SF, dialyzed, degree of hydrolysis > 95%, molecular weight about 45 000 g/mol, BASF Aktiengesellschaft) and as isocyanate component 166.9 g of Basonat® TU 75E (polyfunctional tolylene diiso- cyanate adduct of TDI and polyol, 75% strength by weight in ethyl acetate, BASF Akti¬ engesellschaft). The dispersion obtained was milky blue and contained microcapsules predominantly 1-30 μm in diameter. The solids content was 20 percent by weight. UV- VIS spectroscopy indicated an encapsulation efficiency of 83%.

Comparative example 1 :

A 4 I stirred vessel was charged with a solution of 5.5 g of Span® 80 (sorbitan monoo- leate, Roth), 1.1 g of Cremophor® A6 [75% by weight Cetareth-6 (ethoxylated cetyl alcohol) 25% by weight stearyl alcohol, BASF] and 7.7 g of Arlacel® P135 (PEG-30 dipolyhydroxystearate, Atlas Chemie) in 1226.1 g of Miglyol® 812 (decanoyl/ octanoyl glyceride; Sasol). Following addition of a solution of 24.5 g of ethylenediamine (Merck, 99%) and 44 g of C.I. 42090 (BASF Aktiengesellschaft) in 293.3 g of water a water-in-oil emulsion was produced with a rotational speed of 2000 rpm (RZR 2102, Heidolph). At a stirring speed of 2000 rpm a solution of 195.5 g of Basonat® TU 75E (polyfunctional tolylene diisocyanate adduct of TDI and polyol, 75% strength by weight in ethyl acetate, BASF Aktiengesellschaft) in 1080.8 g of Miglyol was added over the course of 90 minutes. After the end of the addition the dispersion was heated to 6O⁰C over the course of 15 minutes and stirred for a further 60 minutes. Thereafter the reac¬ tion mixture was cooled to room temperature over the course of 15 minutes. 5.1 g of 2-aminomethylpropanol (Merck, 95%) were added and stirring was continued at room temperature for 40 minutes. The dispersion obtained was milky blue and according to microscopic evaluation contained individual capsules predominantly 1-5 μm in diame¬ ter. The viscosity was 219 mPas (100 s^'1) and the solids content was 20 percent by weight. UV-Vis spectroscopy indicated an encapsulation efficiency of 18%.

Comparative example 2:

Using the method of comparative example 1 a microcapsule dispersion was prepared, but the Basonat® in solution in Miglyol was added not at a uniform rate over

90 minutes but instead in a linearly descending gradient over the same period of time. The dispersion obtained was milky blue and according to microscopic evaluation con¬ tained individual capsules predominantly 1-5 μm in diameter. The viscosity was 240 mPas (100 s^"1) and the solids content was 20 percent by weight. UV-Vis spectros¬ copy indicated an encapsulation efficiency of 35%.

Comparative example 3:

By the method of comparative example 1 a microcapsule dispersion was prepared, using 44 g of Sicovit® Cochineal Red 80 A(E 124, C.I 16255, BASF Aktiengesellschaft) instead of C.I. 42090 (BASF Aktiengesellschaft). The dispersion obtained was milky red and according to microscopic evaluation contained individual capsules predomi- nantly 1-5 μm in diameter. The viscosity was 219 mPas (100 s^"1) and the solids content 20 percent by weight. UV-Vis spectroscopy indicated an encapsulation efficiency of 7%.

Comparative example 4: By the method of comparative example 2 a microcapsule dispersion was prepared, using 44 g of Sicovit® Cochineal Red 80 A(E 124, C.I 16255, BASF Aktiengesellschaft) instead of C.I. 42090 (BASF Aktiengesellschaft). The dispersion obtained was milky red and according to microscopic evaluation contained individual capsules predomi¬ nantly 1-5 μm in diameter. The viscosity was 153 mPas (100 s^"1) and the solids content 20 percent by weight. UV-Vis spectroscopy indicated an encapsulation efficiency of 51%.

Claims

1. A microcapsule dispersion comprising microcapsules in a hydrophobic solvent, wherein the microcapsules have a capsule core, comprising at least one water- soluble organic substance, and a capsule shell, and wherein the capsule shell comprises reaction products of

a) at least one di-, oligo- and/or polyisocyanate and b) at least one polyfunctional amine selected from the group consisting of poly- vinylamines, polyethylenimines and polyoxyalkylenamines having a number- average molecular weight of from 600 to 380 000 g/mol and c) if appropriate, one or more different alkyldiamines having 2 to 10 carbon at¬ oms.

2. The microcapsule dispersion according to claim 1 , wherein the capsule shell is composed of reaction products of

3. The microcapsule dispersion according to claim 1 or 2, wherein the capsule shell is formed using one or more different alkyldiamines having 2 to 10 carbon atoms.

4. The microcapsule dispersion according to any one of claims 1 to 3, wherein the at least one polyfunctional amine has a number-average molecular weight of from 800 to 70 000 g/mol.

5. The microcapsule dispersion according to any one of claims 1 to 4, wherein the at least one polyfunctional amine is a polyvinylamine.

6. The microcapsule dispersion according to any one of claims 1 to 5, wherein the isocyanate is an oligo- and/or polyisocyanate containing urethane, isocyanurate, allophanate, urea and/or biuret structures.

7. The microcapsule dispersion according to any one of claims 1 to 6, wherein the at least one di-, oligo- and/or polyisocyanate is selected from the group consisting of tetramethylene diisocyanate, hexamethylene diisocyanate, dodecamethylene diisocyanate, 1 ,4-diisocyanatocyclohexane, 4,4'-di(isocyanatocyclohexyl)- methane, trimethylhexane diisocyanate, tetramethylhexane diisocyanate, 1- isocyanato-3,3,5-trimethyl-5-(isocyanatomethyl)cyclohexane (IPDI), 2,4-tolylene diisocyanate and 2,6-tolylene diisocyanate, tetramethylxylylene diisocyanate, 2,4'- diisocyanatodiphenylmethane and 4,4'-diisocyanatodiphenylmethane.

8. The microcapsule dispersion according to any one of claims 1 to 7, wherein the water-soluble organic substances comprise dyes.

9. The microcapsule dispersion according to any one of claims 1 to 8, wherein the hydrophobic solvent is composed of from 50 to 100% by weight of glycerol ester oils and from 0 to 50% by weight of solvents miscible with glycerol ester oils.

10. The microcapsule dispersion according to any one of claims 1 to 9, wherein the hydrophobic solvent is composed of glycerol ester oils.

11. The microcapsule dispersion according to any one of claims 1 to 10, wherein the capsule core comprises water as hydrophilic solvent.

12. A process for preparing a microcapsule dispersion according to any one of claims 1 to 11 , wherein an emulsion of the hydrophilic solvent in the hydrophobic solvent is prepared with the aid of a surface-active substance, the hydrophilic phase com¬ prising the water-soluble organic substance and the at least one polyfunctional amine and also, if desired, one or more different alkyldiamines having 2 to 10 car¬ bon atoms, and di-, oligo- and/or polyisocyanates are added to the emulsion.

13. The process according to claim 12, wherein the di-, oligo- and/or polyisocyanates are added to the emulsion continuously at a rate which decreases as reaction progresses.

14. The process according to claim 12 or 13, wherein as surface-active substance a linear block copolymer having a hydrophobic structural unit with a length of more than 5 nm (50 A) is used which is defined by the following formula:

C_w(-B-A-B_y-)_XD_Z

in which

A is a hydrophilic structural unit having a solubility in water at 25°C of 1% by weight or more, having a number-average molecular weight of from 200 to 50 000 g/mol and being selected such that it is bonded covalently to B; B is a hydropho¬ bic structural unit which has a number-average molecular weight of from 300 to 60 000 g/mol, has a solubility in water at 25°C of less than 1% by weight and can be bonded covalently to A;

C and D are end groups, which can be A or B and the same group or different groups; w is 0 or 1 ; x is an integer of 1 or greater; y is 0 or 1 , and z is 0 or 1.

15. The process according to claim 14, wherein the linear block copolymer is a 12- hydroxystearic acid block copolymer.

16. The process according to claim 12 or 13, wherein as surface-active substance C₁₂-C₁₈ sorbitan fatty acid esters are used.

17. The process according to claim 12 or 13, wherein as one surface-active sub¬ stance a mixture comprising Ci₂-C₁₈ sorbitan fatty acid esters and linear block co¬ polymers according to claim 14 is used.

18. Microcapsules obtainable by removing the hydrophobic solvent from a microcap- sule dispersion according to any one of claims 1 to 11.