Process for crystallizing the organic substances from steroidal origin and the thus obtained compounds

Information

  • Patent Grant
  • 5266712
  • Patent Number
    5,266,712
  • Date Filed
    Friday, August 14, 1992
    31 years ago
  • Date Issued
    Tuesday, November 30, 1993
    30 years ago
Abstract
A process for crystallizing a pharmaceutically active steroidal product, without mechanical procedure, to obtain a homogeneous granulometric class which may be prepared beforehand, wherein the product which is desired to be crystallized is dissolved in a ternary mixture made of a lipophilic solvent, a hydrophilic solvent and a surface active agent at a temperature close to the boiling point of the mixture of solvents and wherein the mixture of solvents is allowed to revert to a temperature where the crystallization initiates, then, the thus-formed crystals are recovered.
Description

This invention relates to the field of pharmacotechnology and more particularly it relates to a process for obtaining active ingredients for pharmaceutical use having a determined size of crystals, by means of a crystallization method.
It is in fact known that the size of crystals of a pharmaceutical active ingredient plays an important role when dry or fluid pharmaceutical formulation are realized, to insure a reproducible manufacture of the formulation and hence a constant resorption.
The fact has been frequently cited in the litterature that the variations in the kinetics of dissolution are due either to alterations in the crystalline structure or of the surface properties, of the crystals, or to modifications of the extent of the surface of contact put in action (G. GILLARD Labo. Pharm. Probl. and Techn. 309 (1981) 359-369).
To improve the kinetics of dissolution of the active ingredients of drugs showing a limited solubility, a decrease of the size of the particles are often employed.
This problem is usually solved by the use of a mechanical proceeding such as grinding or micronizing (pounded by jet of air).
A study conducted on various progestatives by Muttenrauch and Cowork (STP Pharma 5(10) 1989, 642-646) has shown that the role played by the size of the crystals on the rate of dissolution was closely linked to the solubility of the organic substances.
It has been often disclosed on a large number of molecules of therapeutic use, that the size of particles and the physico-chemical properties of the active-ingredients resulting from these treatments determine the bioavailability of the pharmaceutical formulation containing them through modifications of the rates and speed of dissolution (cf. FDA paper guidelines, Manuf Control Form ANDA'S (1985). However these methods of pounding are not appropriate to pulverize all active ingredients, some of which have low melting points and become pasty or elastic. Other active ingredients because of their physical properties cannot be micronized (80% <10 .mu.m) and this despite several passages in the pounder. It has been described, namely by Nakagawa and cowork (Chem. Pharm. Bull. 30 (1982) 242) that the specific surface and the crystallinity have a great influence on the chemical stability at the solid state, of the pulverized compound.
The rate of dissolution is also dependant up on the cristallinity of the compound B. A. Hendricken disclosed it in Int. J. of Pharm. 60 243-252 (1990). Other investigators have studied the effects of mechanical treatments, such as grinding, on the physico-chemical properties of various active ingredients contained in the composition of a pharmaceutical formulation for therapeutic purpose. These workers noticed that the active ingredients show some alterations in the physico-chemical properties due to these treatments.
Among them it may be cited:
loss of cristallinity (ascertained using X-rays diffraction)
variations of the specific surface SW which may become double or triple.
a drop in the chemical stability determined through differential thermical analysis of the temperature of decomposition (for some active ingredients it has been noted drops in the melting points of 10.degree. to 15.degree. C.)
a variation in the surface properties which do not make always easy the manufacture of a mixture of powders. It has more precisely described in the previously-cited Gillard's work that the morphometric, electrical and rheological properties are very significant for the realization of a homogeneous mixture and namely these having a good flowing capacity.
All these changes in the physico-chemical characteristics on various active ingredients have been very precisely described by M. OTSUKA and N. KANENIWA in International J. of Pharmaceutics 62 (1990) 65-73 and in the references cited in this article. Moreover it cannot be forgot ten the influence of the decrease in the size of the particles produced by grinding on the hardness of tablets obtained from these compounds (cf. Y. SAGAWA J. Powder Technol. Jap. 20 (1983) 737-743).
This is why the experimental results from Tawashi (STP Pharma. 6(5) (1990) 299-302) supplied with an illustration of the relation-ship which exists between decrease in the size of the particles and morphological aspects of thus resulting fragments. The result of the mechanism of reduction in the size depending on the utilized means on the measurements of the fragments substantially relate to the evidence of the irregularity of the surfaces of the particles and the relation-ship which exist between the surfaces and physical behaviour of powders during the manufacture of pharmaceutical formulations. Through appearance of the surface, through its influence on the capacity of flowing of the product, constitutes one of the significant factors which have an influence on the qualities of a mixture of powders in order to realize such a pharmaceutical formulation. The effect of the mechanism of reduction in the size also plays an important role on the solubility of the active ingredient.
Other studies have moreover shown that the crystalline form of an active ingredient could still undergo a transformation (crystallisation) or a deformation (such a plastic) during the compression (cf. C. FUHRER, STP Pharma. 6(5) (1990) 294-298).
The grinding may also results in replacing the crystals with agglomerates equivalent to smaller crystals, which do not improve in any manner neither the solubility nor the rate of dissolution of the active ingredient.
Moreover a grinding when mechanical as it is the case with crusher with knifes, may introduce some dirts of the products with metallic particles or with oil.
This invention has then as a subject matter to find a solution which is more satisfactory than the grinding, to obtain a granulometric range of crystals which may be used in the pharmaceutical industry while achieving at will, crystals of a determined size with a quasi constant percentage and which avoids the use of damaging methods for the decrease of the size of particles such as the various publications mentioned and such as the applicant itself, could state it on the experienced active ingredients.
It appeared thus possible to arrive to a solution of this physical problem relating to crystallization and to obtain in this way a homogenous granulometric class of crystals without it would be necessary to have recourse to a grinding or to a sieving and without even modifying the cristalline system of the starting material. This has been ascertained through microscopy and thermal differential analysis (TDA).
The applicant has then searched, to avoid the use of a proceeding of grinding, to exert an influence on the various parameters which control the phenomena of crystallization and namely to modify the constituents of the mass to be crystallized. These procedures have as a goal to exert an influence namely on decisive parameters such as mass transfers and heat transfers. It is known, in fact, that mass transfer is due to a phenomenon of diffusion of the molecules from the liquid mass to the surface of the crystals and that heat transfer is caused by the diffusion of the heat of crystallization (energy of binding released during the period of formation of the crystal) from the surface of crystals to the mass of liquid. A sufficient command of the surimposition of both transfers allows to exert an influence on the growth of the crystals and this to avoid the factor of vicinity of crystals during their formation in concentrated solution.
The latter parameter intervenes for disturbing the regular growth of crystals while causing the formation of agglomerates.
This invention has then as a subject matter a process for crystallizing which through this influence on the parameters of crystallization authorizes without mechanical proceeding, to obtain a homogeneous granulometric range according which the product which is to be crystallized is as a preliminary, dissolved in a ternary mixture made of a lipophilic solvent, a hydrophilic solvent and a surfactant, at a temperature near the boiling point of the mixture of solvents and the resulting solution is cooled to a temperature, where the crystallisation initiates, the thus-formed crystalls which are of the same crystalline system as those at first utilized before they are dissolved in the mixture of solvents but are of the desired size.
Similar processes, except they are in a binary mixture, have already been described for recrystallizing mineral salts such as for example CHIANESE A and cowork. Process Technol. Proc. 89--Vol. 6 (ind. cryst. 87) 261-264 such as sodium perborate, wherein the said authors use a surfactant in water, to recrystallize the said salt, or BLASZCZAK J. and cowork. Kryst. Przem. Krajowe Symp. Mater Konf. 3rd (56 WYAM) 89--95-101 on hydrated Aluminium fluoride.
In the litterature they are also found many publications which study the crystallization to obtain the active ingredients in a well-defined crystalline system, such as for example G.A.J.M.T Sas and cowork which use a process through precipitation to obtain an active ingredient crystallized in the monoclinic system (Eur. Pat. Appl. 389.035) or then to resolve polymorphic forms such as Terfenadin (2 crystalline forms) cf. T. G. Fawcett and al. (U.S. Pat. No. 4,742,175) other scientists have prepared microcrystalls by precipitation in an "anti-solvent"- Schmitt W. achieves this process for microcrystallizing, in dissolving the active ingredient in a hydrosoluble solvent and injecting the aqueous solution into cold carbon dioxide- Microcrystals are thus obtained (PCT Int. Applic. WO 90/03782--CA (1990) 113, 178284 k).
In the process according to this invention, the hydrophilic solvent is selected in such a manner to be miscible or soluble in the lipophilic solvent, to insure a homogeneous solution. Preferably the hydrophilic solvent is an aqueous mixtures of solvents and more particularly water added to a polar solvent and/or a lower alkyl ester.
After numerous searches it appears to be advantageous to select from the family of alkanols (i.e. methanol, ethanol, butanol, isopropanol), of ketons (such as acetone, methylethylketone, and methyl isobutylketone) ethyl acetate, isobutyl acetate inter alia and water, the percentage of which in the binary mixture ranges between 0 and 12%.
The surfactant is preferably a anionic surfactant selected among the polyoxy ethylenic esters of sorbitan and fatty acids having at least 8 carbon atoms, the polyoxy ethylenic ethers of fatty alcohols having at least 8 carbon atoms and the polyoxy ethylenic esters of stearic acid.
The anionic surfactant is selected among those which have an amphiphilic character, but with a predominant hydrophilic character having a HLB>12, such as for example the polyoxy ethylenic esters of sorbitan and a fatty acid such as the TWEENS 20 to 40, the polyoxy ethylenic ethers of fatty alcohols such as the BRIJ 56, 58, 78, 96, 97, 98 and 99, G 3816 and 3820, G 3910 and 3920 or ETHYLAN D 254 to 257, RENEX, CREMOPHOR or of the type PLURONIC (F 68).
The polyoxy ethylenic esters of stearic acid such as the MYRJS 49, 51, 52, 53 and 59 are also suitable because they further improve the dissolution of the active ingredients, they allow to get very-concentrated solutions during the crystallization and to decrease also the, temperature of recrystallization for obtaining the supersaturation of the medium.
As a function of the series of active ingredients to be used, it appears advantageous to utilize a ternary mixture consisting of the previously cited solvents containing from 1 to 12% water and 0,01 to 10% of the surfactant and most preferably from 0.05 to 5%.
This ternary mixture may be produced at once or through several succesive steps in dissolving first the active ingredient in one of the solvents, in adding optionally the surfactant then in making complete the mixture with the other solvent. The volume and the nature of the ternary mixture to be used for the recrystallization, will be selected as a function of the granulometric class to be searched for the studied pharmaceutical form and as a function of the expected yield.
For a definite active ingredient, it will be necessary to establish a ternary diagramm of the mixture to be used and to define the proportion of the solvents which constitute this mixture.
The volume of the ternary mixture depends on the solubility of the active ingredient at reflux temperature in this mixture. A good solubility is required to obtain relatively high concentrations in the mass since this one is an influent factor of the growth of the crystals in the course of cooling.
The presence of water is necessary for some surfactants to insure a good repartition of these ingredients in the liquid mass and thus to promote its incorporation in the network, to form liquid and solid masses in the course of recrystallization and thus to influence the interfacial tension liquid/solid. The effect of vicinity in the course of crystallization may disturb the regular growth of the crystals and lead to groupings having not any clear shape. It is merely the well ordered disposal in the space of the particles composing it, which distinguish the crystals from the amorphous substances wherein the arrangement of the particles is anarchic.
The temperature of heating of the ternary mixture plays an important role. The ternary mixture containing the active ingredient to be crystallized, is lead to a temperature as close as possible from the boiling point of the said mixture in order to insure an high concentration of the substance to be crystallized and in order to be in a position to decrease at most as possible, the temperaure of recrystallization of the said substance.
The size of the thus obtained crystal also varies as a function of the concentration and the ratio lipophilic solvent/hydrophilic solvent. The amount of hydrophilic solvent goes through an optimal value such as for example with the progestative derivatives, between 2 a 5% in the presence of a solvent of the ketonic kind such as methyl ethylketone to obtain a class of crystals the granulometry of which lies between 35 and 70 .mu.m and preferably around 5% to restrict this class between 35 and 55 .mu.m.
With 7.5% of the previously used solvent, the class of crystals raises a new to between 70 and 100 .mu.m. This increase in the content of hydrophilic solvent leads to crystals with higher size. Moreover when operating in a more or less diluted medium, the crystals are caused to be of more or less extended size and to be a function of the nature of the utilized tenside. It appears that the general rule according to which, smaller crystals are obtained if the concentration of the active ingredient is more significant in a medium of crystallization containing only one solvent, is not always verified in this process of crystallization.
The rate of cooling, the temperature of initiation of the recrystallization, the nature of the ternary mixture and the concentration of the active ingredient, are the parameters needed for the selection of a determined granulometry. The cariage of frigories as well as the stirring of the medium will have to be previously defined for each study. The isolation of the active ingredient by filtration is to be carried out at temperatures which may range from +45.degree. to -10.degree. C.
The scale up of this process in the industry for particular compounds, gave rise to some shifts in the granulometric classes. For example for Promestriene at the level of 1 g, crystals of about 50 .mu.m have been obtained, whilst for a batch of 60 kg the same experimental conditions supplied crystals with a granulometry of about 150 .mu.m. Accordingly an adjustment is required when the process has to be adapted to the industrial production.
The active ingredient to be crystallized is preferably a compound having a steroidal structure and particulary a derivative of estrane androstane, pregnane, 19-nor pregnane and cholestane.
Among the derivatives of estrane, it may be cited estradiol, estrone, estriol, 19-nor Testosterone as well as their esters and/or their ethers. A more precise example of derivative of estrane is the 3-propyl ether of the 17-methyl ether of estradiol (Promestriene) or 19-nor Testosterone, Undecanoate.
Among the derivatives of androstane, it may be cited Testosterone, its ethers and ethers in position 17, the substituted Testosterone in position 4,6,7 or 16 such as for exemple 4-chloro Testosterone, 6-methyl Testosterone, 7-methyl Testosterone, the fatty acid esters of Testosterone such as Testosterone cyclopentyl acetate or cyclohexyl propionate, the derivatives of androsta 2-ene substituted in position 17 such as 17-.beta.-acetoxy-17.alpha.-ethynyl-5.alpha.-androsta-2-ene.
Among the derivatives of pregnane it may be cited progesterone, its enolic ethers, the cyclic or linear enamines, the 17.alpha.-hydroxy derivatives thereof, the esters of 17.alpha.-hydroxy progesterone, the progesterones substituted in position 1, in position 6, in position 7 or in position 16.
Among the 21-hydroxy pregnenic derivatives, it may be cited the cortisone derivatives such as cortisone, cortisol, prednisone, medrol, dexamethasone, .beta.-methasone or Triamcinolone.
Among the derivatives of 19-nor progesterone it may be cited 17.alpha.-hydroxy 19-nor progesterone, its ethers in position 17, its esters in position 17 as well as the substituted 19-nor progesterones such as 6-methyl 17.alpha.-hydroxy 19-nor progesterone, its ethers in position 17, its esters in position 17, as well as 6-methyl-3,20-dioxo-17.alpha.-hydroxy 19-nor-pregna-4,6-diene and its esters.
Among the cholestanic derivatives it may be cited the biliary acids, cholesterol and its esters, ergosterol, stigmasterol and Calciferol.
The micro-crystalline compounds obtained according to the process of this invention are use ful active ingredients of dry pharmaceutical composition such as uncoated tablets, tablets with slow release, soft gelatine capsules, granulates; or in liquid pharmaceutical compositions such as drinkable suspension or injectible suspensions for intramuscular or intra-articular administration, in vaginal preparations such as suspension, bio-adhesive gels, suppositories or vaginal suppositories.





BRIEF DESCRIPTION OF THE DRAWINGS
FIGS. 1-21 are illustrative of the various test results from the examples. FIG. 1 illustrates the transition enthalpy for solid/liquid transitions of the microcrystallized product. The differential thermic analysis of the raw product, ground product, and microcrystallized product are shown in FIGS. 2-6. FIGS. 7, 11, 12, 15 and 16 show the results of granulometric analysis as determined by a laser granulometer Coulter LS 130. Results of differential thermic analysis of Nomegestrol acetate, before and after grinding, are illustrated by FIGS. 8 and 9, respectively. FIGS. 13 and 14 demonstrate the chromatographic analysis by HPLC of Nomegestrol acetate, before and after grinding, while FIG. 10 illustrates the thermogravimetric analysis of the starting material. FIGS. 17-20 show the granulometric analysis for batches 23, 27, 33 and 35, respectively. (See Example XII) FIG. 21 is a comparison of the dissolution curves.





The following examples illustrate this invention without limiting it in any manner. They show the interest of this process in comparison with the conventional grinding.
EXAMPLE I
Microcrystalls of Hydrocortisone
10 g of hydrocortisone are dissolved at reflux temperature in 10 volumes of a solvent mixture formed of:
95.8% methylethylketone
4% water
0.2% Tween 20
It is kept to reflux for 5 to 10 mn under stirring and it has to be sure it no longer remain any particle suspended. Under stirring, the mass is cooled to -10.degree. C. This temperature is maintained for one hour and the resulting crystals are dried. The crystals are washed with water and further dried under reduced pressure, at a temperature close to 50.degree.-60.degree. C. The thus formed crystals are of 25.times.30 .mu.m for the biggest ones to 5.times.10 .mu.m for the smallest ones.
MPk: 221.5.degree.-222.degree. C.
[.alpha.].sub.D (methanol)=+156.degree..+-.2.degree.
EXAMPLE II
Microcristalls of Dexamethasone Acetate
10 g dexamethasone acetate are dissolved at reflux temperature in 4 vol. of a solvent mixture made of:
89.0% methylethyl ketone
10.5% water
0.5% MIRJ 51
The reflux is kept for 30 mn. The insoluble particles are filtered and the filtrate is cooled to -15.degree. C. This temperature is maintained for 1 hour before drying the crystalline mass. The crystals are washed with water then dried at 60.degree. C. under reduced pressure. The size of the thus formed crystals extends from 80.times.50 .mu.m for the biggest ones to 8.times.10 .mu.m for the smallest ones.
MPk=226.degree.-227.degree.
[.alpha.].sub.D (methanol)=+84.degree..+-.2.degree.
EXAMPLE III
Microcrystalls of Dexamethasone Acetate
10 g of Dexamethasone acetate are dissolved at reflux temperature into 4 vol. of a solvent made of:
87.6% acetone
12.0% water
0.4% TWEEN 20
Isolation is carried out as described in the preceding example and crystals are obtained the range of which extends from 200.times.75 .mu.m for the biggest ones to 160.times.50 .mu.m for the smallest ones.
MPk=228.degree. C.
[.alpha.].sub.D (methanol)=+86.degree..+-.2.degree.
EXAMPLE IV
Microcrystalls of Prednisone
10 g prednisone are dissolved in 5 vol. of a solvent mixture made of:
94.8% methylethyl ketone
5.0% water
0.2% TWEEN 20
Isolation of the crystals is performed as described in the foregoing examples (cooling to -10.degree. C.). It is obtained crystals the maximum size of which, is about 55.times.40 .mu.m and the minimal size of which is 35.times.24 .mu.m.
MPk=240.degree..+-.1.degree. C.
[.alpha.].sub.D (methanol)=+167.degree..+-.4.degree.
EXAMPLE V
Microcrystalls of Nomegestrol Acetate
10 g Nomegestrol acetate are dissolved at the reflux temperature in 6 Vol. of a solvent mixture made of:
94.9% methanol
5.0% water
0.1% TWEEN 20
The temperature is let to revert very slowly under stirring using external cooling to -5.degree. C. This temperature is maintained for 15 mn. The crystalline mass is separated, dried then washed with water and dried again under reduced pressure.
The thus-formed crystals range from 50.times.25 .mu.m for the bulkiest ones to 10.times.10 .mu.m for the smallest ones.
EXAMPLE VI
Microcrystalls of Nomegestrol Acetate
The procedure of example I is followed but using 2 vol. of a ternary solvent mixture made of:
92.4% methylethyl ketone
7.5% water
0.1% TWEEN 20
The microcrystals are recovered, the size of which ranges from 100.times.100 .mu.m for the bulkiest ones to 65.times.35 .mu.m for the smallest ones.
EXAMPLES VII
Microcrystalls of Nomegestrol Acetate
The same procedure than at example I is used but utilizing 2 vol. of a ternary solvent mixture made of:
94.9% methylethyl ketone
5.0% water
0.1% TWEEN 20
The microcrystals are recovered, the size of which ranges from 55.times.40 .mu.m for the bulkiest ones to 35.times.25 .mu.m for the smallest ones.
EXAMPLE VIII
Microcrystals of Nomegestrol Acetate
The same procedure than at example I has been used but using 2 vol. of a ternary solvent mixture formed of:
87.9% methylethyl ketone
12.0% water
0.1% TWEEN 20
The microcrystals are recovered, the size of which ranges from 150.times.65 for the bulkiest ones to 90.times.50 .mu.m for the smallest ones.
EXAMPLE IX
Microcrystalls Of Nomegestrol Acetate
The same procedure than at example I is used but utilizing 1,5 vol. of a ternary solvent mixture made of:
94.9% methylethyl ketone
5.0% water
0.1% TWEEN 20
The microcrystals are recovered the size of which ranges from 120.times.40 .mu.m for the bulkiest ones to 75.times.50 .mu.m for the smallest ones.
EXAMPLE X
Microcrystalls Of Promestriene
The same procedure than at example I is used but dissolving one part of Promestriene in 4 vol. of a ternary solvent mixture made of:
94.9% ethanol at 100%
5.0% water
0.1% TWEEN 20
The crystals are recovered, the size of which ranges from 300.times.100 .mu.m for the bulkiest ones to 100.times.50 .mu.m for the smallest ones.
EXAMPLE XI
Microcrystalls Of Promestriene
The same procedure than at the fore going example has been followed in dissolving 30 kg Promestriene in 3 vol. of a ternary solvent mixture made of:
______________________________________94.8% methylethyl ketone (i.e 85.320 l) 5.0% water (i.e 4.500 l) 0.2% TWEEN 20 (i.e 0.180 l)______________________________________
The mixture is cooled to -10.degree. C. After 15 mn at this temperaure, the thus-formed crystals are filtered. They were washed with water and dried in a oven at about 35.degree. under reduced pressure. The thus recovered crystals have a size which ranges from 125.times.100 .mu.m for the bulkiest ones to 80.times.50 .mu.m for the smallest ones.
The compounds which have been used for these studies (raw compounds, ground compounds and microcrystallised compounds) have been controlled through differential thermic analysis.
Separated studies comparing a raw product and a ground product (Ref. C.114 and C.114B) comparing two ground compounds (C.108B and C.114B) and comparing a raw compound and a microcrystallized product (C.109 and C.109M) have given the following results:
between the tested products from the batches C.108B, C.114B and C.114 in similar experimental conditions in the field of temperatures ranging from 12.degree. to 142.degree. C., these three compounds show through differential thermic analysis with temperature scanning, similar behaviours (see FIGS. 2,3,4,5 and 6).
The melting of these compounds appears to be similar between them, with temperature located in the neighborhood of 64.degree. C. and a melting enthalpy ranging from 72 to 74 joules/g.
The microcrystallized product has a melting temperature of 64.57.degree. C. and melting enthalpy located at 73.2 joules/g, thus very close to that of the other compounds.
EXAMPLE XII
Microcrystalls of Nomegestrol Acetate
Two assays of crystallization have been carried out along the procedure of this invention, starting from 30 kg of Nomegestrol acetate.
The starting material is dissolved in 4 vol. of a ternary solvent made of:
94.9% methanol
5.0% water
0.1% TWEEN 20
The resulting crystalline product is recovered and shows the granulometric range as follows (as determined with a laser granulometer Coulter LS 130):
assay 1: batch 037 MC 2
assay 2: batch 037 MC 3 (see FIG. 7)
For these two assays the results are statistically similar for a definite granulometric range, all the particles of which are inferior to 400 .mu.m.
On the contrary when grinding various industrial batches, it has been stated a large irregularity in the range of the granulometric classes (cf. curves of the batches 23, 27, 33 and 35 in FIGS. 17 to 20).
EXAMPLE XIII
Assays have been performed on larger patches of Nomegestrol acetate using 40, 60 and 90 kg respectively, according to the procedure disclosed in example XII. The results have been as good as the preceding ones.
Even an assay with 90 kg (Ref. S4-- batch 3) has given the following granulometric analysis (see FIG. 16).
EXAMPLE XIV
Microcrystalls of Progesterone
This study has been performed as in the preceding examples, by dissolving the starting material at the reflux temperature in 6 vol. of a solvent made of:
93.4% ethanol
6.0% water
0.6% TWEEN 40
The thus formed crystals are separated in the cold and washed with water then dried. The thus produced crystalls range from 150.times.80 .mu.m for the bulkiest ones to 10.times.20 .mu.m for the smallest ones.
MPk=125.degree..+-.2.degree.
[.alpha.].sub.D (dioxan)=+170.degree..+-.4.degree.
EXAMPLE XV
Microcrystalls of 17.beta.-Acetoxy 17.alpha.-Ethynyl 5.alpha.-.DELTA.2-Androsten
As described in the preceding examples, the product has been processed in dissolving it at the reflux temperature in 4 vol. of a mixture made of:
96.0% ethyl acetate
3.2% water
0.8% TWEEN 20
The crystals are recovered as previously described in the preceding examples. The thus produced crystals has a mean granulometry of 40 to 60 .mu.m.
MPk=125.degree.-129.degree.
EXAMPLE XVI
Microcrystalls of Androstanolone (4-Dihydro Testosterone)
The product is processed as in the previously cited examples, in dissolving the starting material at the reflux temperature in 7.5 vol. of a solvent made of:
91.8% methanol
8.0% water
0.2% TWEEN 20
The thus formed crystals are separated in the cold, then are washed with water and dried. The crystals show a mean granulometry of 120 .mu.m.
MPk=182.degree..+-.2.degree.
[.alpha.] (ethanol)=+30.degree..+-.2.degree.
A differential thermic analysis has been performed on industrial batches of Nomegestrol acetate before grinding, after grinding and after microcrystallization:
sample A and B for Nomegestrol acetate before grinding (FIG. 8)
sample C and D for Nomegestrol acetate after grinding (FIG. 9)
samples E and F for Nomegestrol acetate after microcrystallisation
The microcrystallization, subject of this invention, has been performed on the raw material before grinding.
RESULTS
The assays temperatures range from 290.degree. to 525.degree. K. It has not been found any solid/solid transition. The solid/liquid transition has been found depending on the sample from 178.1.degree. to 179.1.degree. C.
The transition enthalpy is about 6.8 joules/g. The intervals of temperature for the transitions solid/liquid have been found the smallest for the samples E and F, resulting from the microcrystallized compound according to the therein claimed process (FIG. 1).
A thermogravimetric analysis has been performed on a sample (B) of starting material. With this kind of product at assay temperatures ranging from 25.degree. to 700.degree. C., the loss of mass is about total at 400.degree. C. (FIG. 10).
It has been also possible to study the granulometric classes resulting from the process of microcrystallization, by means of an image scanner fitted with a logiciel VIDS IV.
On the industrially recrystallized product according to the process of example XII (batch 037 MC 2) it has been performed a study with this kind of material. The obtained results are expressed in .mu.m for the dimensions (parameters and length) and in .mu.m.sup.2 for the surfaces.
This kind of analysis allows a clear confirmation of the results obtained by Laser granulometry. In a field of small particles, it has been made out particles from 9 to 16 .mu.m, which are values similar to that observed by Laser granulometry.
Analysis of the bulkiest particles has supplied with dimensions close to 70 .mu.m, values also obtained with Laser granulometer.
The chromatographic analysis by HPLC allows to show the baneful influence of the grinding. For Nomegestrol acetate the damaging may be evaluated to about 0.2%.
Some examples of industrial batches evidence this phenomena:
batches before grinding (Ref. 028 and 031)--(see FIG. 13)
batches after grinding (Ref. 028B and 031B)--(see FIG. 13)
The analysis by HPLC have been carried out at two disterict wawe lenghthes (245 and 290 nm) to have a better separation of the impurities of the type 3-keto .DELTA.-4 pregnene from that of the type 3-keto .DELTA.4,6-pregnadien.
To overcome this damaging, several methods have been contemplated:
one consisting in grinding while cooling the apparatus
the other one using the method of crystallization according to this invention.
In order to be comparative and to be able to validate the method according to this invention, both techniques have been put into practice on a same batch of active ingredient ##STR1##
The batches designated as 037-MC 1 a 3 are three assays of recrystallization on industrial batches (30 kg) in order to confirm the validity of the disclosed method, as regard to the granulometric class (FIGS. 7,11 and 12).
The HPLC analysis on the so produced compounds have been performed under the same conditions than those previously described.
These tests fully demonstrate that:
the grinding, even performed under cooling, does not prevent that the compound fall into disrepair (cf. FIG. 14).
the crystallization according to the process of this invention, allows to obtain an active ingredient of better quality and that in the wanted granulometric class without the need to recurse to a grinding method (FIG. 15).
This phenomenon of chemical alteration is also stated on other steroidal compounds to a more or less extent, depending on the considered active ingredient.
The following examples related to formulations illustrate the use of the microcrystallized compounds of this invention and more particularly of the compounds derived from pregnane.
The disclosed granulometric class is the most representative of the cited compound (i.e.>80%).
EXAMPLE XVII
Tablets with Belated Release
Unit formulation for various dosologies
______________________________________microcrystallized Nomegestrol acetate 1.25 to 10.00 mg(200 to 300 .mu.m) fromAerosil 200 0.37 to 0.50 mgPrecirol ATO 5 1.85 to 2.25 mgMethocel E.4 55.0 to 70.00 mgAvicel PH 101 10.00 to 20.00 mgLactose enough for 1 tablet of 185.00 to 200.00 mg______________________________________
EXAMPLE XVIII
Tablets with Fast Release
Unit formulation for various dosologies
______________________________________microcrystallized Nomegestrol acetate 1.25 to 10.00 mg(<50 .mu.m)Aerosil 200 0.37 to 0.50 mgPrecirol ATO 5 1.85 to 2.00 mgAvicel PH 102 50.00 to 70.00 mgExplotab or Polyplasdone XL 5.00 to 25.00 mgLactose enough for a tablet of 185 to 225.00 mg______________________________________
EXAMPLE XIX
Tablets of Nomegestrol Acetate
Unit formulation for various dosologies
______________________________________microcrystallized Nomegestrol acetate 1.25 to 10.00 mg(200 to 300 .mu.m)Aerosil 200 0.37 to 0.50 mgPrecirol ATO 5 1.85 to 2.25 mgAvicel PH 101 55.00 to 70.00 mgLactose enough for a tablet of 185.00 to 220.00 mg______________________________________
The analysis of the results by the function of distribution of Weibull(D. GIBASSIER and COWORK--STP PHARMA 1(10) (1985) 967-973) evidence a significant difference between these three formulations.
The shapes of dissolution curves, as shown by the parameter .beta. of this function, give 0.148 for a formulation with fast release, 1.015 for a formulation with normal release and 1.914 for a formulation with delayed release (cf. FIG. 21).
The process of this invention thus allows the realization of granulometric classes of an active ingredient appropriate to the needs of the formulation to be realized.
It is ascertained that these two pharmaceutical compositions which have been realized from industrial raw materials, have an equivalent bioavailability.
EXAMPLE XX
Injectible depot formulation based on Medroxyprogesterone or on Nomegestrol in the form of their acetates.
Unit formulation for 1 flask of 5 ml:
______________________________________microcrystallized Medroxy progesterone acetate 500.00 mgor microcrystallized Nomegestrol acetate(15 to 40 .mu.m)Polyethylene glycol 4000 200.00 mgPreservatives 0.006 mgSodium chloride/Sodium Citrate 0.15 mgDistilled water for injection 5.00 mg______________________________________
EXAMPLE XXI
Vaginal or Gynaecologic Capsule
a) unit formulation for a capsule
______________________________________microcrystallized progesterone 50 to 500.00 mg(200 to 300 .mu.m)Vaseline (pharmacopeia) 200.00 mgSorbitol sesquioleate 200.00 mgSynthetic perhydrosqualene 1.85 g______________________________________
Dry coating: gelatine, glycerol, preservative, for a soft gelatine capsule weighing 2.55 g
b) vaginal suppository
______________________________________microcrystallized Nomegestrol acetate 20.00 mgvithepsol H35 or H37 enough for a suppository of 2.8 g______________________________________
EXAMPLE XXI
Bioadhesive Gel for Cutaneous or Gynaecologic Use
Formula for 100 g:
______________________________________microcrystallized Progesterone 2.0 to 3.0 gPolyethylene glycol 4.0 to 6.0 gCarboxypolyvinyl polymer 0.5 to 1.0 gPreservatives 0.3 mgTriethanolamine enough for pH 6.5Purified water 100.0 g______________________________________
EXAMPLE XXIII
Bioadhesive Gynaecologic Foam Formula for a Dispenser (2.5 ml) of 50 g
______________________________________microcrystallized Progesterone 2.0 to 5.0 gCarboxypolyvinyl polymer 0.5%Isobutane 5.5%Excipient base F25/1 enough for 50.0 g______________________________________
Shake the suspension before use.
Dispensed dosage from 100 to 250 mg.
EXAMPLE XXIV
Implants
Formulation for 100 g of material to be extruded:
______________________________________Nomegestrol acetate 5.0 gPoly (orthocarbonates) enough for 100.0 g______________________________________
The temperature of the mixture shall not excede 185.degree. C. in order not to impair the crystalline form of the active ingredient.
EXAMPLE XXV
Intra-uterine Device with Reservoir
Device with a Silastic reservoir of 2.5 to 3.5 cm length for a thickness of 0.4 to 0.8 mm and a diameter of 2 mm.
The preparation is formulated as a suspension as follows:
For 100 g of suspension:
______________________________________microcrystallized Progesterone (80-250 .mu.m) 0.600 to 1.0 gsuspended intosuspending agent 0.5 gsynthetic Perhydrosqualene 100.0 g______________________________________
EXAMPLE XXVI
Patches
Content of the reservoir. Preparation for 100 g:
______________________________________microcrystallized Nomegestrol acetate 0.5 g(80-250 .mu.m)Carboxy polyvinylic polymer 0.2 gColloidal silica 0.2 gSilicone oil enough for 100.0 g______________________________________
Examples of Formulation of Estrane Derivatives
EXAMPLE XXVII
Tablets
Unit formulation:
______________________________________microcrystallized Estradiol (10-50 .mu.m) 1.0 to 2.0 mgKollidone 25 10.0 to 20.0 mgKollidon 90 5.0 to 10.0 mgAvicel PH 102 25.0 to 50.0 mgPEG 6000 1.0 to 2.0 mgPrecirol ATO 5 1.5 to 3.0 mgPolyplasdone XL 2.5 to 5.0 mgLactose enough for 1 tablet______________________________________
EXAMPLE XXVIII
Bioadhesive Gels based on Estradiol or Promestriene
Formulation for 100 g of gel:
______________________________________microcrystallized Estradiol or Promestriene 1.0 to 2.0 gPropylene glycol 5.0 to 10.0 gCarboxypolyvinyl polymer 0.5 to 1.0 gPreservatives 0.3 mgTriethanolamine enough for pH 6.0 to 6.5Purified water enough for 100.0 g______________________________________
EXAMPLE XXIX
Vaginal Capsules
Formulation for one capsule:
______________________________________microcrystallized Estradiol 1.0 mgLabrafil M 1944 CS 0.5 gPerhydrosqualene 1.3 g______________________________________
Dry coating: gelatine, glycerol, preservatives for a soft gelatine capsule of 2.1 g
EXAMPLE XXX
Patches
Content of the reservoir: formula for 100 g
______________________________________microcrystallized Estradiol (80-100 .mu.m) 0.5 to 1.0 gAerosil 0.5 gsynthetic Perhydrosqualene enough for 100.0 g______________________________________
EXAMPLES OF FORMULATION WITH COMPOUNDS DERIVED FROM ANDROSTANE
EXAMPLE XXXI
Formulation as tablets-unit formulation for a 380 mg tablet:
______________________________________microcrystallized 17.beta.-acetoxy 17.alpha.-ethynyl 20.0 mg5.alpha.-androst-2enAvicel PH 101 91.20 mgAerosil 0.45 mgPrecirol ATO 5 7.60 mgExplotab 4.30 mgLactose 256.45 mg______________________________________
This formulation shows a better availability than that previously disclosed in the literature.
EXAMPLE XXXII
Gynaecologic Gel
Formulation for 100 g:
______________________________________microcrystallized Androstanolone 2.50 g(dihydrotestosterone)Propylene glycol 2.50 gTranscutol 5.00 gPreservatives 0.08 gViscosity agent (such as TEA) 0.25 gCarboxypolyvinyl polymers 1.50 gPurified water enough for 100.00 g______________________________________
EXAMPLE XXXIII
Oral Capsule
______________________________________microcrystallized Testosterone Heptylate 50.00 mgOleic acid enough for 1 capsule 250.00 mg______________________________________
Coating: gelatine, preservatives, glycerol
EXAMPLES OF FORMULATION WITH COMPOUNDS DERIVED FROM 21-HYDROXY PREGNENES
EXAMPLE XXXIV
Tablets for the Oral Way
Unitary formulation for each tablet:
______________________________________microcrystallized Prednisone (80-150 .mu.m) 2.50 mgAvicel PH 102 50.00 mgAerosil 1.80 mgPrecirol ATO 5 2.00 mgLactose enough for one tablet 128.70 mg______________________________________
EXAMPLE XXXV
Tablets for the Oral Way
Unitary formulation for each tablet:
______________________________________microcrystallized Prednisone (80-150 .mu.m) 0.50 mgAvicel PH 102 50.00 mgAerosil 1.70 mgPrecirol ATO 5 2.00 mgLactose enough for on tablet 130 mg______________________________________
EXAMPLE XXXVI
Gel for Cutaneous Application
Formulation for 100 g:
______________________________________microcrystallized Dexamethasone acetate 0.05 to 0.10 gPolyethylene glycol 5.00 gCarboxypolyvinyl Polymer 1.00 gTriethanolamine enough for pH 6.5Purified water enough for 100.0 g______________________________________
EXAMPLE XXXVII
INJECTIBLE SUSPENSION
Unit formulation for a 2 ml ampul:
______________________________________microcrystallized Dexamethasone acetate 10.0 mg(>80 .mu.m)______________________________________
Suspension solution:
______________________________________Polysorbate 80 0.015 gSodium carboxymethyl cellulose 0.010 gSodium chloride 0.010 gPurified water for injection enough for 2.00 ml______________________________________
______________________________________FIG. 1______________________________________DEE C108BInitial temperature: 285.2KFinal temperature: 379.3KScanning rate: 2.00 C/mnAmplification range: 1.000 mVSample mass: 37.200 mgSampling rate: 2.08 sStorage: 1357 points______________________________________FIG. 2______________________________________Glass transition determinationTemperature range for Tg Determination:Beginning temperature: 61.79 C.End temperature: 66.63 C.The three Glass temperatures are: 64.0 C. 64.79 C. 65.38 C.Cp variation: 6.64 Cal/g C.Integration with a linear base linePeak start: 62.06 C.Peak end: 74.23 C.Onset temperature: 64.89 C.Enthalpy: -.27672E + 004 mJ or -.66202E/003 mcal -.74389E + 002 J/g or -.17796E + 002 cal/gEndothermic peaktop of peak temperature: 66.56 C.______________________________________FIG. 3______________________________________01/08/90DEE C114BInitial temperature: 285.2KFinal temperature: 525.0KScanning rate: 2.00 C/mnAmplification range: 1.000 mVSample mass: 25.400 mgSampling rate: 3.68 sStorage: 1955 pointsGlass transition determinationTemperature range for Tg Determination:Beginning temperature: 62.29 C.End temperature: 66.57 C.The three Glass temperatures are: 64.10 C. 64.55 C. 64.98 C.Cp variation: 4.56 Cal/g C.Integration with a linear base linePeak start: 62.16 C.Peak end: 75.38 C.Onset temperature: 64.62 C.Enthalpy: -.18837E + 004 mJ or -.45064E/003 mcal -.74161E + 002 J/g or -.17742E + 002 cal/gEndothermic peaktop of peak temperature: 66.44 C.______________________________________FIG. 4______________________________________07/08/90DEE C109Initial temperature: 285.2KFinal temperature: 415.2KScanning rate: 2.00 C/mnAmplification range: 1.000 mVSample mass: 42.200 mgSampling rate: 2.08 sStorage: 1875 pointsFin storage: 1875 points in file 4Peak start: 61.16 C.Peak end: 73.61 C.Onset temperature: 64.75 C.Enthalpy: -.30705E + 004 mJ or -.73458E/003 mcal -.72762E + 002 J/g or -.17407E + 002 cal/gEndothermic peaktop of peak temperature: 66.69 C.Glass transition determinationTemperature range for Tg Determination:Beginning temperature: 61.16 C.End temperature: 66.68 C.The three Glass temperatures are: 63.70 C. 64.22 C. 65.24 C.______________________________________FIG. 5______________________________________DEE C114Initial temperature: 285.2KFinal temperature: 415.2KScanning rate: 2.00 C/mnAmplification range: 1.00 mVSample mass: 61.600 mgSampling rate: 2.08 sStorage: 1875 pointsGlass transition determinationTemperature range for Tg Determination:Beginning temperature: 57.84 C.End temperature: 67.04 C.The three Glass temperatures are: 63.60 C. 64.31 C. 65.52 C.Cp variation: 5.24 Cal/g C.Integration with a linear base linePeak start: 77.00 C.Peak end: 64.78 C.Enthalpy: -.45478E + 004 mJ or -.10879E/004 mcal -.73828E + 002 J/g or -.17662E + 002 cal/gEndothermic peaktop of peak temperature: 66.90 C.______________________________________FIG. 6______________________________________07/08/90DEE 109MCInitial temperature: 285.2KFinal temperature: 415.2KScanning rate: 2.00 C/mnAmplification range: 1.000 mVSample mass: 35.800 mgSampling rate: 2.08 sStorage: 1875 pointsFin. Storage: 1875 points in file 5Integration with a linear base linePeak start: 61.75 C.Peak end: 73.26 C.Onset temperature: 64.65 C.Enthalpy: -.26206E + 004 mJ or -.62695E/003 mcal -.73203E + 002 J/g or -.17512E + 002 cal/gEndothermic peaktop of peak temperature: 66.90 C.Glass transition determinationTemperature range for Tg Determination:Beginning temperature: 61.65 C.End temperature: 67.04 C.The three Glass temperatures are: 64.40 C. 64.57 C. 65.59 C.Cp variation: 7.48 Cal/g C.______________________________________FIG. 7______________________________________Ref. 9007033Coulter .RTM. LS Particle size analysis A0890.S18Filename: A0890.S18 Group ID: A0-890Sample ID: TX 066 LOT 037 MC2 Run number: 6Operator: A.P.C. SIMMComments: DISPERSION: glycerol & U. SOUND COULTRONICS FRANCEStart time: 10:42 25 aug 1990Run length: 90 secondsObscuration: 6%PIDS Obscur: 30%Optical model: Fraunhofer PIDS includedPC: Version 1.10 13:07 Fri Mar 02 1990 Volume Statistics (Arithmetic) 10890.S18Calculations 0.10 .mu.m to 834.40 .mu.mfromVolume 100.0 %Mean 22.49 .mu.m 95% Conf. 19-42-25-56 .mu.m limits:Median 19.72 .mu.m Std. Dev: 15-67 .mu.mMean/median 1.341 Variance: 245.5 .mu.m.sup.2RatioMode 29.60 .mu.m Coef. var: 69.66 % Skewness: 7.016e-001 Right skewed Kurtois: -1.088e-001 Platy- kurtic% 10.00 25.00 50.00 75.00 90.00Size .mu.m 45.20 32.64 19.72 10.10 3.771______________________________________FIG. 8______________________________________DATA TREATMENT OF A CURVE STDRED: SCANNINGMODE: INTEGRATION, CRYSTALLINITY AND GLASSTRANSITION DETERMINATIONS11/04/90THERAMEX AInitial temperature: 290.2KFinal temperature: 525.2KScanning rate: 2.00 C/mnAmplification range: 10.00 mVSample mass: 51.300 mgSampling rate: 1.92 sStorage: 3671 pointsGlass transition determinationTemperature range for Tg Determination:Beginning temperature: 172.9 C.End temperature: 181.5 C.The three Glass temperatures are: 176.9 C. 178.7 C. 179.9 C.Pente = : -13.2346027168Integration with a linear base linePeak start: 173.9 C.K1 = 2.490S(K.sub. 1) = -3.1655Peak end: 191.1 C.K2 2760S(K.sub.2) -3.1354Enthalpy: -3.487E + 003 mJ or -1.626E/001 mcal or -6.797E + 001 J/gEndothermic peakTP = 181.881617top of peak temperature: 180.1 C.11/04/90THERAMEX BInitial temperature: 290.2KFinal temperature: 525.2KScanning rate: 5.00 C/mnAmplification range: 2.500 mVSample mass: 15.600 mgSampling rate: .80 sStorage: 3524 pointsIntegration with a linear base linePeak start: 169.6 C.K1 2356S(K.sub.1) -2.3444Peak end: 199.5 C.K2 2806S(K.sub.2) -1.8524Enthalpy: -1.052E + 003 mJ or -1.618E/001 mcal -6.748E + 001 J/gEndothermic peakTP = 181.919107A6top of peak temperature: 180.2 C.Glass transition determinationTemperature range for Tg Determination:Beginning temperature: 169.5 C.End temperature: 181.5 C.The three Glass temperatures are: 176.4 C. 178.1 C. 179.5 C.Pente: -6.4818199304______________________________________FIG. 9______________________________________11/04/90THERAMEX CInitial temperature: 290.2KFinal temperature: 525.2KScanning rate: 5.00 C/mnAmplification range: 2.500 mVSample mass: 10.500 mgSampling rate: .80 sStorage: 3524 pointsIntegration with a linear base linePeak start: 173.6 C.K1 2417S(K.sub.1) -1.7128Peak end: 199.5 C.K2 2807S(K.sub.2) -1.4299Enthalpy: -7.215E + 002 mJ or -1.644E/001 mcal or -6.872E + 001 J/gEndothermic peakTP = 180.985774333top of peak temperature: 179.2 C.Glass transition determinationTemperature range for Tg Determination:Beginning temperature: 173.5 C.End temperature: 180.5 C.The three Glass temperatures are: 177.2 C. 178.9 C. 179.4 C.Pente: -11.8392024107THERAMEX DInitial temperature: 290.2KFinal temperature: 525.2KScanning rate: 5.00 C/mnAmplification range: 2.500 mVSample mass: 15.900 mgSampling rate: .80 sStorage: 3524 pointsIntegration with a linear base linePeak start: 175.5 C.K1 2446S(K.sub.1 ) -2.4676Peak end: 194.5 C.K2 2731S(K.sub.2) -2.3127Enthalpy: -1.114E + 003 mJ or -1.677E/001 mcal or -7.011E + 001 J/gEndothermic peakTP 181.252441top of peak temperature: 179.0 C.Glass transition determinationTemperature range for Tg Determination:Beginning temperature: 173.5 C.End temperature: 181.0 C.The three Glass temperatures are: 178.0 C. 179.1 C. 179.7 C.Pente: -21.4280794192______________________________________FIG. 11______________________________________Ref. 9007032COULTER .RTM. LS Particle size analysis A0889.S01Filename: A0889.S01 Group ID: A0-889Sample ID: TX 066 LOT 037 MC1 Run number: 1Operator: A.P.C SIMMComments: DISPERSION: NONIDET & U. SOUND COULTER FRANCEStart time: 11.55 24 aug 1990Run length: 91 secondsObscuration: 5%PIDS Obscur: 23%Optical model: Fraunhofer PIDS includedPC: Version 1.10 13:07 Fri Mar 02 1990 Volume Statistics (Arithmetic) 10889.S01Calculations 0.10 .mu.m to 834.40 .mu.mfromVolume 100.0 %Mean 32.93 .mu.m 95% Conf. 29-02-26-84 .mu.m limits:Median 31.12 .mu.m Std. Dev: 18-96 .mu.mMean/median 1.058 Variance: 396.4 .mu.m.sup.2RatioMode 44.70 .mu.m Coef. var: 60.61 % Skewness: 3.640e-001 Right skewed Kurtois: -5.857e-001 Platy- kurtic% 10.00 25.00 50.00 75.00 90.00Size .mu.m 65.21 47.02 31.12 17.07 7.810______________________________________FIG. 12______________________________________Operator: FP Sample: MC216 Oct. 1991 16:03Field area: 30543.81 Calibration: 0.2717 mcm/pixelField 1: Class 2:Feat. Area Perimeter Long dimsn.______________________________________1 60.181 34.189 13.0552 96.954 38.947 14.8273 45.634 26.169 9.25514 69.116 33.109 12.7725 58.409 30.959 12.1076 53.277 29.411 10.8187 37.807 28.331 12.3758 49.732 29.488 11.2739 59.295 29.303 10.78810 48.292 27.650 9.638111 49.474 27.094 10.22912 39.727 27.849 11.14513 57.818 31.689 11.84814 32.490 24.579 9.638115 44.231 25.782 9.491416 29.832 22.428 7.955017 102.086 40.780 15.91018 46.188 30.739 13.05819 47.443 30.379 12.26120 50.877 28.224 10.233Total 1078.86 597.098 228.675Mean 53.943 29.855 11.434St Dev. 18.281 4.4267 1.9422______________________________________FIG. 13______________________________________N.M.A. 028-028B 031-031B028001.DT3 05-30-1991 13:50:40Y-scale 008 AU/FS Sample name tx(1-00-1)Sampling 21 msec *4 Paper speed 4 mm/mintimeSense normalResolu- 3 nm Column ultrosphere DDS 4,6 mmtion ID $250 mmTime 2.4-25 min Packing material C18rangeInterval 1 sec Mobile phase Acetonitrile 360Baseline OFF Flow MeOH 240 1,3 ml/min rateSmooth- 5 points Pressure 2.300 psiingDrift .002 Slope H.sub.2 O 400 .0001 AU/ AU/min minWidth .001 min Height .0002 AUTime 30 min Min. area .00002 AU*double min Minus OFF peak______________________________________
Claims
  • 1. A process for crystallizing a product comprising a pharmaceutically active ingredient of steroidal structure to obtain without any mechanical procedure a homogenous class of product which may be prepared beforehand comprising dissolving the product to be crystallized in a ternary mixture of a lipophilic solvent, a hydrophilic solvent and a surface active agent at a temperature close to the boiling point of the ternary mixture, allowing the ternary mixture to cool to a temperature where crystallization occurs and recovering the resulting crystals.
  • 2. A process according to claim 1 wherein the active ingredient is an estrane derivative.
  • 3. A process according to claim 2 wherein the estrane derivative is selected from the group consisting of estradiol, estrone, estriol, 19-nor Testosterone, the 3-mono ethers of the same, the 3, 17-diethers of these compounds and the esters of these compounds.
  • 4. A process according to claim 1 wherein the active ingredient is an androstane derivative.
  • 5. A process according to claim 4 wherein the derivative of androstane is selected from the group consisting of Testosterone, ethers of Testosterone, esters of Testosterone, Testosterones substituted by a halogen or a lower alkyl in position 4, 6, 7 or 16 and the 17.alpha.-ethynyl-17.beta.-acetoxy-5.alpha.-androst-2-ene.
  • 6. A process according to claim 1 wherein the active ingredient is a pregnane derivative.
  • 7. A process according to claim 6 wherein the pregnane derivative is a steroidal compound selected from the group consisting of progesterone, enolic ethers of progesterone, cyclic or linear enamines of progesterone, 17.alpha.-hydroxy progesterones, esters of 17.alpha.-hydroxy progesterone, progesterones substituted by an alkyl, a trifluoromethyl or a halogen in position 1,6,7 and/or 16 and the ethers or esters thereof.
  • 8. A process according to claim 1 wherein the active ingredient is a 19-nor pregnane derivative.
  • 9. A process according to claim 8 wherein the derivative of 19-nor pregnane is a steroidal derivative selected from the group consisting of 17.alpha.-hydroxy-19-nor-progesterone, the ethers in position 17 of 17.alpha.-hydroxy-19-nor-progesterone, 6-methyl-17.alpha.-hydroxy-19-nor-progesterone, ethers in position 17 of 6-methyl-17.alpha.-hydroxy-19-nor-progesterone, esters in position 17 of 6-methyl-17.alpha.-hydroxy-19-nor-progesterone, 6-methyl-3,20-dioxo-17.alpha.-hydroxy-19-nor-pregna-4,6-diene and the esters in position 17 of 6-methyl-17.alpha.-hydroxy-19-nor-pregna-4,6-diene and the 17.alpha.- and 21-methyl or ethyl analogs of 6-methyl-3,20-dioxo-19-nor-pregna-4,6-diene.
  • 10. A process according to claim 1 wherein the active ingredient is a derivative of cholestane.
  • 11. A process according to claim 1 wherein the active ingredient is a derivative of 21-hydroxy .DELTA.4-pregnene.
  • 12. A process according to claim 10 wherein the 21-hydroxy .DELTA.4-pregnenic derivative is a corticosteroid selected from the group consisting of Cortisone, Prednisone, Dexamethasone, Betamethasone, Triamcinolone, Medrol, Cortivazol, their esters in position 17, their diesters in positions 17 and 21 and their esters in position 21.
  • 13. A process according to claim 1 wherein the lipophilic solvent is selected from the group consisting of alkanols, ketones, alkyl esters and cyclic ethers in which the hydrophilic solvent has to be miscible in an amount up to 12%.
  • 14. A process according to claim 13 wherein the hydrophilic solvent is selected in such a manner to be miscible with the lipophilic solvent in order to insure a homogeneous solution.
  • 15. A process according to claim 13 wherein the hydrophilic solvent is an aqueous mixture made of one or several oxygenated solvents.
  • 16. A process according to claim 13 wherein the hydrophilic solvent is selected from the group consisting of water and/or polar solvents and/or lower alkyl esters of cycloalkylcarboxylates.
  • 17. A process according to claim 1 wherein the surface active agent is an anionic surfactive agent.
  • 18. A process according to claim 17 wherein the anionic surfactive agent is soluble in the lipophilic solvent or in the hydrophilic solvent and necessarily at the same time in the mixture of both solvents.
  • 19. A process according to claim 1 wherein the anionic surface active agent is selected from the group consisting of the polyoxyethylenic esters of sorbitan and fatty acids, having at least 8 carbon atoms the polyoxyethylenic esters of stearic acid and the copolymers of ethylene oxide and propylene oxide.
  • 20. A process according to claim 1 wherein the ternary mixture, made of a lipophilic solvent, a hydrophilic solvent and a surface active agent, is realized in one or several steps.
  • 21. A process according to claim 1 wherein the concentration of the surface active agent in the ternary mixture lies between 0.01 and 10%.
  • 22. A process according to claim 21 wherein the concentration in surface active agent in the ternary mixture lies between 0.05 and 5%.
  • 23. A process according to claim 1 wherein the ternary mixture containing the active ingredient to be crystallized, is heated to a temperature as close as possible to the boiling point of the mixture of solvent in order to insure the highest possible concentration of the compound to be crystallized and to decrease the temperature of crystallisation of the said compound.
  • 24. The microcrystallized products of the process according to claim 1.
Priority Claims (1)
Number Date Country Kind
90 13981 Nov 1990 FRX
PCT Information
Filing Document Filing Date Country Kind 102e Date 371c Date
PCT/FR91/00888 11/12/1991 8/14/1992 8/14/1992
Publishing Document Publishing Date Country Kind
WO92/08730 5/29/1992
US Referenced Citations (4)
Number Name Date Kind
2096744 Hildebrandt et al. Oct 1937
2897216 Oliveto et al. Jul 1959
3007923 Muller et al. Nov 1961
3053865 Taub et al. Sep 1962