前苏联专利SU1342418A3 Method of producing 6-methyl-3,4-dihydro-1,2,3-oxathiazine-4-on-2,2-dioxide or potassium salt thereo

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专利摘要:
6-Methyl-3,4-dihydro-1,2,3-oxathiazin-4-on-2,2-dioxid wird dadurch hergestellt, daß man a) in einem inerten organischen Lösungsmittel ein darin zumindest teilweise lösliches Salz der Amidosulfonsäure mit der mindestens etwa äquimolaren Menge eines Acetoacetylierungsmittels in Gegenwart eines Amin- oder Phosphin-Katalysators umsetzt, und daß man das dabei gebildete Acetoacetamid-N- sulfonat oder auch die freie Sulfonsäure b) durch die Einwirkung der mindestens etwa äquimolaren Menge S03, gegebenenfalls in einem inerten anorganischen oder organischen Lösungsmittel, zu dem hier in der Säureform anfallenden 6-Methyl-3,4-dihydro-1,2,3-oxathiazin-4-on-2,2-dioxid cyclisiert; aus der Säureform können gewünschtenfalls c) durch Neutralisation mit Basen die jeweiligen Salze gewonnen werden. Die nicht-toxischen Salze - insbesondere das Kaliumsalz - sind wertvolle synthetische Süßstoffe.
公开号:SU1342418A3
申请号:SU853867759
申请日:1985-03-21
公开日:1987-09-30
发明作者:Клаус Карл；Линкис Адольф；Ройшлинг Дитер
申请人:Хехст Аг (Фирма)；
IPC主号:

专利说明:

113
This invention relates to a process for the preparation of 6-methyl-3, 4-dihydro-1,2,3-oxathiazin-4-one-2,2-dioxide or its potassium salt, which have a sweet taste and are used in the food industry, and to the method of obtaining new intermediate products - ammonium acetoacetamide-N-sulfonates ..
The aim of the invention is to simplify the process, increase its safety and increase the yield of the target product.
This goal is achieved by reacting the quaternary ammonium salt of amidosulfonic acid with 4–30 mol,% excess diketene, and forming a new intermediate product — the corresponding ammonium acetoacetamide K – sulfonate is treated with 4–20 fold molar excess sulfur. anhydride.
I. Preparation of ammonium acetoacetamide-N-sulfonates.
Example 1
ABOUT
®
HN (CH,),
.e;
Trimethylammonium- (adetoacetamide-N-sulfonate).
9.7 g (0.1 mol) of amidosulfonic acid are added to a solution of 12 ml (0.125 mol) of trimeishtamine in 100 ml of glacial acetic acid and stirred until all is dissolved. Then 8 ml (0.104 mol) are added dropwise. Dictene at 25-30 ° C while cooling. 16 hours after the slow addition of ether, the reaction product precipitates and is sucked off, yield 22 g (92%). Melting point 101 ° C.
NMR (DMSO, db): 2.2 (CKj-CO); 2.8 (N-CH3); 3.45 (-CHj.
IR (KBr): 1045, 1240, 147 1660, -1720. ABOUT
®
HN (sn5) fg
About zoz
PRI mme R 2. Dimethylethylammonium (acetoacetamide-K-sulfonate). .
80 g (1.096 mol) are added dropwise to 80 g (0.825 mol) of amidosulfonic acid suspended in 500 ml of glacial acetic acid while cooling.

five
0
0
50
five
0
five
82
dimethylethylamine. When all is dissolved, while cooling at 25-35 ° C, 80 ml (1.038 mol) of diketene is added. After 16 hours, the residue is evaporated and the residue is triturated with acetone, and crystallization takes place. Yield 110 g (43%). Melting point 73-75 C.
From the mother liquor receive the remainder of the reaction product in the amount of 128 g (50%) in the form of syrup.
NMR (CDCl 2): 1.5 (OH,); 2.2 (CH3-CO) ;, 2.8 (N-CK,); 3.5 (-SK ,, - WITH)
IR spectra (KBr): 1050, 1240, 1475, 1690. 1730. ABOUT
LS,.
A f) Q o °
. . PRI me R 3. Triethylammonium t-acetoacetamide-I-sulfonate ;.
9.7 g (O, 1 mol) of the amidosulfonic acid are dissolved in 100 ml of methylene chloride together with 16 ml (0.12 mol) of triethylamine. Then 8 ml (0.104 mol) of diketene are added dropwise. Additionally stirred for 2 hours at 0 C and 2 hours at room temperature. Then, by adding hexane, the reaction product is precipitated and the remaining syrup is washed with further hexane. After drying in vacuo, 27-28 g (95.7-99%) remain. After a longer time, the syrup begins to crystallize.
NMR (CDClOS: 1.33 (-CH3); 2.2 (CHj-CO); 3.2 (N-CH); 3.5 ().
1Z-spectrum (pure substance): 1040, 1230, 1450, 1650, 1670 cm
Analogously to example 3, examples 4-7 are carried out.
The result is as follows:
ABOUT
HN (H-propyl),

PRI me R 4. Three- (n-propyl-ammonium (acetoacetamide-K-sulfonate). Vcode 92-97%,
NMR (CDC1): 2.3 (-CH -CO2); 3.6 (-SNg-CO).
IR spectrum (1040, 1260, 1420, 1700, 1740.
PRI me R 5.
г®-1
HN (H-BH),
Three- (n-butyl) -ammonium (acetoacem ™ amide-K-sulfonate). Yield 91-96%.
NMR {CDCl) 8: 2.25 (CH, -CO); 3.5 (.
IR spectrum (CHjClJ: 1040, 1250, 1420, 1700, 1740 cm.
II p and me 6.
O®
, 1JAN HN (CH,) j benzyl
- SO
about
Dimethylbenzylammonium acetoacetate-amide-N-sulfonate). The output of 92-97%
NMR (CDC1,) S: 2.2 (COCH,); 2.75 (P-CH,); 3.5 (); 4.3 {P-CH-A); 7.35 (aromatic).
IR spectrum (): 1040, 1260, 1270, 1430, 1470, 1700, 1740,
PRI me R 7.
O r & L (IZOPROPIL) 2 ETNL j
f
Diisopropylethylammonium- (acetoacetate amide-K-sulfonate), Yield 91-95%.
NMR (CDClJS: 1.3 and 1.4 (-CH,); 2.2 (COCH,); 3.5 ().
IR spectrum (): 1040, 1210, 1250, 1420, 1700, 1740 cm.
Example
ABOUT
LATER
And zoz about
Triethylammonium- (acetoacetamide-N-sulfonate),
9.7 g (0.1 mol) of amidosulfonic acid are suspended in 100 ml of acetone and 16 ml (0.12 mol) of triethylamine are added. When almost all is dissolved, 8 ml of diketone are added dropwise at 0 ° C. After that, while stirring at room temperature, they are allowed to react, and everything dissolves. After 16 hours, the reaction product was isolated with hexane as a syrup and was purified by stirring with hexane. After drying in vacuo, 27-28 g of syrup (95.7-99%) remain, which slowly crystallizes on standing.
NMR (CDCl 3) S: 1.3 (-CH,); 2.2 (CHj-CO); 3.55 (-CHj-CO).
IR (pure substance): 1040 1230, 1450, 1670.
42418
PRI me R 9.
Lsyn ®Вн
5 1 I / CN
L sop
Tetrabutylammonium- (acetoacetamide-N-sulfonate).
.Q 15.5 g (0.16 mol) of amidosulfonic acid in 10 ml of methanol and 50 ml of water
105 ml (0.16 mol) of a 40% aqueous solution of tetrabutylammonium hydroxide are mixed. Then evaporate to dryness. The residue is dissolved in 100 ml of methylene chloride and the pH is adjusted to a value of 9-10 with triethylamine. 10 ml of diketene are then added dropwise. After 12 hours, the pH was adjusted again to a value of 9-10 and the addition of diketea was repeated, and after 16 hours it was evaporated, and the residue crystallized. A slurry of crystals is filtered off with suction and washed with ethyl acetate and 2g of ether. The yield of 34.6 g (52%). Melting point 97-98 ° C.
NMR (CDClI) S: 1.33 - (CH,); 2.2 (COCHj); 3.2 (); 3.5 ().
IR spectrum (): 890, 1040, 1255, 1410.
Example 10
20
thirty
ABOUT
©
. HN t,
35
ABOUT
SO-:
Triethylammonium- (acetoacetamide-N-sulfonate).
19.4 g (0.2 mol) of amidosulfonic acid and 15.4 ml (0.2 mol) of diketene are placed in 200 ml of methylene chloride at. For 45 minutes, 29 ml (0.21 mol) of triztilamine are added dropwise with cooling and stirring. The mixture is then stirred for 30 minutes at 0 ° C and then the reaction mixture is left to stand at room temperature overnight. After evaporation of the solvent and drying in vacuum, the reaction product is obtained in the form of a syrup. Crystallization is carried out from acetone. Yield 53-56 g (94-99%). Melting point 55-58 s.
NMR (CDClI) S: 1.33; (- CH,); 2.2 (CHj-CO); 3.2 (N-CHt); 3.5 (). IR (clear): 1040, 1230, 1450,
-f
1670 cm product.
g ® t
Hn t
Example o
Lh
l sop about
Triethylagdanium- (acetoacetamide-N- - -sulfonate).
19.4 g (0.2 mol) of amidosulfonic acid, 15.4 ml (0.2 mol) of diketene and 1.14 ml (0.02 mol) of glacial acetic acid are placed at 0 ° C in 100 m of methylene chloride. For 45 minutes, 29 ml (0.21 mol) of triethylamine are added dropwise with cooling and stirring. Then it is further stirred at 0 ° C for 30 minutes and after that the reaction mixture is left to stand at room temperature overnight. After extracting the solvent, the residue is washed with diethyl ether and then dried in vacuo. Crystallization is carried out from acetone. The yield of 52-55 g (92-97,5%). Melting point 55-58 C.
NMR (CDC1) 8: 1.33 (-CH,); (CH, -CO); 3.5 ().
QC (pure product): 1040, 1230, 1450, 1670 cm.
PRI me R 12.

about
Lh
L $ 0Z®
.®
HN (CH,) C, HJ
ABOUT
Dimethylphenylammonium- (acetoacetate-amide-K-sulfonate).
To 9.7 g (100 mmol) of amidosulfonic acid in 100 ml of glacial acetic acid
acids are added 15.1 ml (120 mmol)
S, K is dimethylaniline and stirred until all is dissolved. Then, 8 ml (104 mmol) of diketene is added, and after 16 hours, 2 ml of diketene is added once more to the solution. When diketen disappears, the solution is concentrated and the product is precipitated by trituration with ether. Yield 88-92%. NMR (CDClI) S: 2.2 (COCH); 3.5
()
IR (SNGSXg): 1040, 1250, 1430, 1700, 1740 cm
Example 13

tr HjK (isopropyl)
24186
Ammonium (acetoacetamide M sulfonate). 10 ml of diketene and 1 ml of pyridine are added to a suspension of 4 g (100 mmol) of ammonium dosulphonate in 100 ml of glacial acetic acid with good stirring. After 17 h, the target product is sucked off. Yield 17 g (86%). Decomposition occurs, starting at about 125 C.
Example 14
ten
ABOUT
A nh
®
(isopropyl)
A, SOf
Diisopropylammonium- (acetoacetamide-N-sulfonate).
19.4 g (0.2 mol) of amidosulfonic acid in 200 ml of CH, C1 is neutralized. 28 ml (0.2 mol) of diisopropylamine. After the addition of 0.81 ml (10 mmol) of pyridine, 15.4 ml (0.2 mol) of diketene are added dropwise at 0 ° C. Then it is further stirred for 30 minutes at 0 ° C and then the reaction mixture is left to stand at room temperature overnight. After evaporation of the solvent and drying in vacuo, the reaction product is obtained in the form of a solution of 45-48 g (80-85%).
IR (pure product): 1040, 1280, 1450, 1670 cm
Example 15
Og
.. HjN - tert-butyl
sof
N-sulAonat).
about
T-butylammonium- (acetoacetamide 19, 4 g (0.2 mol) of amidosulfonic acid in 100 MP of DMF is neutralized with 21 m (0.2 mol) of tert.-butylamine. After adding 0.81 ml (10 mmol) of pyridine
45 at 15 ° C. 15.4 ml (0.2 mol) of diketene are added dropwise. Then additionally stirred for 3 h at room temperature. For processing, the reaction product is precipitated with
50 500 ml of diethyl ether. For eyes. Stir in syrup and rub with acetone. Yield 42 g (83%).
IR (pure substance): 1035, 1230, 1450, 1670 cm-.
55 II Preparation of 6-metsh-3,4-dihydro-1,2,3, -oxathiazin-4-one-2,2-dioxide or its potassium salts.
Example 16. K8 ml (200 mmol of liquid BOz in 100 ml at
7
-30 ° C and with good stirring over 60 minutes, 12.7 g (50 mmo) of dimethylethylammonium (acetacetamide-K-sulfonate) in 110 ml of methylene chloride are added dropwise. After 30 minutes, 50 ml of ethyladetate and 50 g of ice are added to the solution. The organic phase is separated, and the aqueous phase is extracted twice more with ethyl acetate. After drying over sodium sulfate, the combined organic phases are concentrated and dissolved in methanol. When the solution is neutralized with a methanol solution of KOH, the potassium salt of 6-methyl-3,4-dihydro-1,2,3-oxat azin-4-one-2,2-dioxide precipitates. The yield is 7.3 grams (73%). , ,
Example 17. K8 ml (200 mmol of liquid 80 in 50 ml of SO at -30 ° C with good stirring for 60 min. 12.7 g (50 mmol) of dimethylethylammonium- (acetoacetamide-H-sulfonate) are added dropwise in 110 ml of CH2Cl. After 30 minutes after evaporation of 80 ml, 50 ml of ethyl acetate and 50 g of ice are added to the solution. The organic phase is separated and the aqueous is extracted twice more with ethyl acetate. The combined organic phases are dried and dried over sodium sulfate and concentrated in methanol. a solution of KOH precipitates 6-methyl potassium salt , 4-dihydro-1,2,3-oxa-thiazin-4-one-2,2-dioxide. Yield 8.3 g (83%).
Example 18. To 12 ml (300 mmol of liquid SOj in 100 ml, 12.7 g (50 mmol) of dimethyl ethyl ammonium (acetoacetamide-I-sulfonate) in 110 ml are added dropwise in 60 ml with and with good stirring) in 110 ml. After 30 minutes to the solution 50 ml of ethyl acetate and 50 g of ice are added. The organic phase is separated and the aqueous phase is extracted twice more with ethyl acetate. The combined organic phases are dried and dried over sodium sulfate and concentrated in methanol to neutralize the solution with methanolic KOH. -methyl-3, 4-dihydro-1,2,3-oxathiase in 4-OH-2,2-dioxide. Yield 7.6 g (76%)
Example 19. K4 ml (100 mmol) of liquid SO, 4.24 g (16.7 mmol) dimethylphenol 4.24 g (16.6 mmol) are drenched in 100 ml at -30 ° C with good stirring for 20 minutes dimethylethyl ammonium- (acetoacetamide-K-sulfonate) in 35 ml. Thereafter, 4 ml (100 mmol) of SOj is added to the solution, and then 4.24 g (16.7 mmol of dimethylstilammonium- (acetoacetamide-N-sulfonate) in 35 ml are added dropwise over 20 minutes with good stirring at -30 €) Then add 4 ml (100 mmol SOj), then at -30 ° C and under good stirring for 20 min, 4.24 g (16.6 mmol) of dimethylethy ammonium (acetoacetamide-I-sulfonate) in 35 ml are added dropwise. 20 minutes the solution is treated analogously to example 16. The output of 8.7 g (87%).
Example 20. K2.4 ml (.60 mmol SO, in 100 ml of CH., Cl2 with 12.7 g (50 mmol) of dimethyl ethyl ammonium- (acetoacetamide-N-sulfonate) in 110 ml) with and with good stirring in 60 ml. At the same time, after 12, 24, 34 and 48 min (see the circumstances), 2.4 ml (60 mmol) of SOj are added. And then after 20 min, the solution is treated as in Example 16. A yield of 8.8 g (88%).
Example 21. Proceed as in Example 20, but first take 2.4 ml (60 mmol) of SO in 50 ml of S0, j. Yield 8.8 g (88%).
EXAMPLE 22 12.8 g (160 mmol of solid VO is dissolved in 150 ml of methylene chloride. After cooling the solution to -45 - -55 ° C for 8 min, 8.4 g (.26 mmol) tripropyl ammonium (acetoacetamide-I-sulfonate) in 25 ml of methylene chloride. After 4 h at -45 55 ° C, it is treated as in Example 16. The yield is 2.8 g (54%
Example 23. To 20 ml (500 mmol of liquid SOj in 500 ml of methylene chloride at -30 ° C and with good stirring, .125 ml of a solution of trisylammonium-acetoacetamceram-And-sulfonate) (0.1 mol) was added dropwise within 60 min After the next 60 minutes at -30 ° C, the solution is treated as in Example 16. The yield is 17.1 g (85%).
Example 24. 125 ml of a solution of triethylammonium- (acetoacetamide-K-sulfonate) (0.1 mol, methylene chloride) are introduced into 250 ml of methylene chloride at -30 ° C. 20 ml (500 mmol) of liquid SOg are added over 60 minutes, dissolved in 250 ml of methylene chloride. After the next 60 minutes at -30 ° C
9134
treated similarly to the example. 16. Yield 14.9 g (74%).
And pmimep 25. To 4.8 MP (120 mmol) liquid SOj in 500 ml of methylene chloride at -25 ° C over a period of 60 minutes, 125 ml of a solution of triethyl ammonium- (acetoacetate-N-sulfonate) are added dropwise (, 0, mole methylene chloride ). The next four portions of 4.8 ml (120 mmol) of liquid SO are added at 12-minute intervals. After 60 min at -25 ° C, the procedure is carried out analogously to Example 16, Yield 18.3 g (91%).
PRI me R 26. 50 ml of methylene chloride are placed in a reaction vessel at -30 ° C. With good cooling and stirring at the same time and evenly for 30 minutes, dropwise
a solution of 28.1 g (0.1 mol) of tri-ethyl ammonium-acetoacetamide-H-sulfonate) in 50 ml of methylene chloride and 24 ml of liquid SO j in 50 ml of methylene chloride. After the next 30 minutes at -25 - -30 ° C, 110 ml of water is carefully added at the same temperature. The methylene chloride is then distilled off and the reaction product is extracted with 80 ml of isobutyl acetate. The organic phase is then mixed with 20 ml of water and with good stirring with 4N. KOH solution is adjusted to a pH of 0.84-058 (pH - meter glass electrodes: Ingold 405-60- J7). After separation and extraction of the aqueous phase with 20 ml of isobutyl
15 g-s of water is added to the combined isobutyl acetate phase and, with stirring, neutralized with 4N. KOH solution to pH 5-7. The partially precipitated potassium salt is filtered off with suction and then combined with the aqueous phase of the filtrate. Evaporation of the water under vacuum gives 18.1 g (90%) of the sweet substance.
Example 27. 50 ml-CH 2 are preliminarily placed (in a reaction vessel) at -30 ° C. Then, a solution of 28.1 g (0.1 mol) of triethylammonium (acetoacetamide-N-sulfonate) in 50 ml and 24 ml of liquid SOj in 50 ml of methylene chloride with intensive cooling (Iopropanol / dry ice) is added simultaneously and evenly. Immediate processing as in Example 26 (extraction agent, isopropyl acetate) gives 17.9 g (89%) of the sweet substance.
Example 28. 12.4 ml of 60% oleum (200 mmol SOj) precursor
ABOUT
) | g

20 25 „, 35
40

45 50 55
but added to 200 ml of methylene chloride at -25 ° C. 62.5 ml of a solution of triethylammonium (acetoacetamide-K-sulfonate) (50 mmol, methylene chloride) are added dropwise within 30 minutes. After the next 60 minutes at -25 ° C, it was treated in the same manner as in Example 16. The yield was 4.7 g (47%).
PR and I m p 29. 200 ml of collidine at 30 C are carefully mixed with 8 ml (200 mmol) of liquid BO. Then 16.2 g (50 mmol) of tripropyl-ammonium (acetoacetamide-11-sulfonate) are added and the reaction mixture is heated at about 100 ° C for 20 hours. Most of the collidine is then distilled off in vacuo and the residue is dissolved in ethyl acetate . After acidification with sulfuric acid, the aqueous phase is extracted well with ethyl acetate. The organic phases are dried over sodium sulfate and evaporated in vacuo. The residue is dissolved in methanol and neutralized with a methanolic potassium hydroxide solution. The sweetened matter that is shed is sucked off and dried. Yield 2.2 g (22%). I
Comparative example
35.42 g (250 mmol) are placed in 250 ml,. At 60.5 minutes, 62.5 ml of a solution of triethylammonium - (acetoacetamide-M-sulfonate) in methylene chloride with a sulfonate content of 0.05 mol are added dropwise. After the next 60 minutes at -25 ° C, the solution is treated as in Example 16. In the reaction product using thin layer chromatography, traces of 6-methyl-3, 4-dihydro-1,2,3-oxathiazin-4-2.2 -dioxide, according to its potassium salt.

权利要求:
Claims (2)
[1]
1. A method of producing 6-methyl-3, 4-dihydro-1,2,3-oxathiazin-4-one-2,2-dioxind or its potassium salt by reacting the amide derivative, hydroxy acid with an acetoacetylating agent in a solvent, such as ice on acetic acid, methylene chloride or dimethylformamide, or their mixture at temperatures from 0 to 30 ° C, if necessary in the presence of an amine as a catalyst, followed by cyclization of the acetoacetamide derivative formed in an inert solvent and released.
the desired product in free form or in the form of potassium salt, characterized in that, in order to simplify the process, maintain its safety and yield the target product, the ammonium salt of amidosulfonic acid of the general formula
NH,
I And g ® / X 1
Р5 R, N (Rj Rj
SO
R, R and R, each hydrogen, or R, is hydrogen or lower alkyl; R. - lower alkyl and
R, hydrogen, lower alkyl, phenyl or
benzyl,
as a derivative of amidosulfonic acid, it is reacted with a 4-30 mol% by weight of diketene as an acetoacetylating agent, the resulting ammonium acetoacetate-amide-S-sulfonate of the general formula
rVe n, ® (“,) in,
A so h o
where R ,, R2 and R have the indicated meanings,
subjected to cyclization by reacting with a 4–20 fold molar excess of sulfuric anhydride in an organic medium, such as methylene exporter, J. Sereda Order 4447/58
Compiled by Z. Latypova Tehred I. Popovich
Corrector
Circulation 371 Subscription
VNIIPI USSR State Committee
for inventions and discoveries 113035, Moscow, Zh-35, Raushsk nab., 4/5
Production and printing company, Uzhgorod, st. Project, 4
342418
12
Read, or inorganic, such as liquid sulphurous anhydride, solvent, or their mixtures at temperatures from -55 to -25 C.
[2]
2. A method for producing ammonium acetocetamide-P-sulfonates of the general formula
ABOUT
ten
.R ..
Where
or
R, is hydrogen or lower alkyl; Rj is lower alkyl and R, is hydrogen, lower alkyl, phenyl or benzyl,
characterized in that the ammonium salt of amidosulfonic acid of the general formula
Kh
where R ,, R and R,
®
R, N (,
have the indicated values,
is reacted with a 4-30 mol.% -% excess diketene in an inert organic solvent, such as ice on acetic acid, methylene chloride or dimethylformamide, or a mixture of them at a temperature from 0 to 30 ° C, if necessary the presence of an amine as a catalyst.
Proofreader But King

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ZA852116B|1985-11-27|

US4607100A|1986-08-19|

CS249549B2|1987-03-12|

引用文献:

公开号 | 申请日 | 公开日 | 申请人 | 专利标题

DE2001017C3|1970-01-10|1978-05-18|Hoechst Ag, 6000 Frankfurt|3,4-Dihydro-1,23-oxathiazin-4on-2,2-dioxides, their manufacture and use|

NL157304B|1970-01-10|1978-07-17|Hoechst Ag|PROCESS FOR THE PREPARATION OF SWEETENING PRODUCTS, PREPARING FORMED PRODUCTS OBTAINED BY APPLICATION OF THIS PROCEDURE, AND PROCESS FOR PREPARING SWEETENING COMPOUNDS.|

DE2228423C3|1972-06-10|1982-05-13|Hoechst Ag, 6000 Frankfurt|3,4-Dihydro-1,2,3-oxathiazin-4-ones and process for their preparation|

DE2434549A1|1974-07-18|1976-01-29|Hoechst Ag|PROCESS FOR THE PREPARATION OF THE SWEET SUBSTANCE 6-METHYL-3,4-DIHYDRO-1,2,3-OXATHIAZIN4-ON-2,2-DIOXIDE|

DE2434564A1|1974-07-18|1976-01-29|Hoechst Ag|METHOD FOR THE PREPARATION OF 6-METHYL3,4-DIHYDRO-1,2,3-OXATHIAZIN-4-ON-2,2-DIOXIDE AND ITS USE AS A SWEET|

DE2453063A1|1974-11-08|1976-05-13|Hoechst Ag|METHOD FOR PRODUCING ACETOACETAMIDE-N-SULFOFLUORIDE|

DE3410440A1|1984-03-22|1985-09-26|Hoechst Ag, 6230 Frankfurt|METHOD FOR PRODUCING 6-METHYL-3,4-DIHYDRO-1,2,3-OXATHIAZINE-4-ON-2,2-DIOXIDE AND ITS NON-TOXIC SALTS|

DE3429039A1|1984-08-07|1986-02-20|Hoechst Ag, 6230 Frankfurt|METHOD FOR PRODUCING 6-METHYL-3,4-DIHYDRO-1,2,3-OXATHIAZINE-4-ON-2,2-DIOXIDE AND ITS NON-TOXIC SALTS|

DE3527070A1|1985-07-29|1987-01-29|Hoechst Ag|METHOD FOR PRODUCING 6-METHYL-3,4-DIHYDRO-1,2,3-OXATHIAZINE-4-ON-2,2-DIOXIDE|DE3410233A1|1984-03-21|1985-09-26|Hoechst Ag, 6230 Frankfurt|METHOD FOR PRODUCING CRYSTALLINE SALTS OF ACETOACETAMIDE-N-SULFOFLUORID|

DE3410440A1|1984-03-22|1985-09-26|Hoechst Ag, 6230 Frankfurt|METHOD FOR PRODUCING 6-METHYL-3,4-DIHYDRO-1,2,3-OXATHIAZINE-4-ON-2,2-DIOXIDE AND ITS NON-TOXIC SALTS|

DE3527070A1|1985-07-29|1987-01-29|Hoechst Ag|METHOD FOR PRODUCING 6-METHYL-3,4-DIHYDRO-1,2,3-OXATHIAZINE-4-ON-2,2-DIOXIDE|

DE3531359A1|1985-09-03|1987-03-12|Hoechst Ag|METHOD FOR PRODUCING 6-METHYL-3,4-DIHYDRO-1,2,3-OXATHIAZINE-4-ON-2,2-DIOXIDE AND ITS CLEANING THEREOF|

DE3531358A1|1985-09-03|1987-03-12|Hoechst Ag|METHOD FOR PRODUCING THE NON-TOXIC SALTS OF 6-METHYL-3,4-DIHYDRO-1,2,3-OXATHIAZINE-4-ON-2,2-DIOXIDS|

TW223067B|1992-03-17|1994-05-01|Hoechst Ag|

DE10013259A1|2000-03-17|2001-09-20|Nutrinova Gmbh|New stable complexes of acesulfame with trace elements e.g. zinc or copper, useful as taste-masked form of trace elements for use in foods, feedstuffs, pharmaceuticals or cosmetics|

DE10130298A1|2001-06-22|2003-01-23|Nutrinova Gmbh|Antimicrobial acesulfame complexes, process for their preparation and their use|

DE10130504B4|2001-06-25|2005-02-03|Nutrinova Nutrition Specialties & Food Ingredients Gmbh|Xanthine and phenazone acesulfame H complexes with improved taste, process for their preparation and their use|

JP2003026671A|2001-07-13|2003-01-29|Daicel Chem Ind Ltd|Method of producing oxadiazines|

CN1336363A|2001-07-25|2002-02-20|张元宾|Synthesis of potassium acetylsulfanilate|

DE10253773B3|2002-11-19|2004-06-24|Nutrinova Nutrition Specialties & Food Ingredients Gmbh|Use of acesulfamic acid as acidulant, useful in foods, beverages, pharmaceuticals and cosmetics, provides lower pH than standard food acids at equal acidic taste|

US20060062747A1|2002-11-19|2006-03-23|Nutrinova Nutrition Specialties & Food Ingredients Gmbh|Use of sweetener acids for the microbiological stabilization of foodstuffs, cosmetic products, consumer goods and pharmaceutical productions|

US8043647B1|2003-03-10|2011-10-25|Perry Stephen C|Sugar replacement|

DE10330025A1|2003-07-03|2005-01-20|Nutrinova Nutrition Specialties & Food Ingredients Gmbh|Process for the preparation of a sweetener salt based on aspartame and acesulfame|

JP2005263779A|2004-02-17|2005-09-29|Daicel Chem Ind Ltd|Method for producing 3,4-dihydro-1,2,3-oxathiazine-4-one-2,2-dioxide compound or its salt|

CN100516054C|2006-09-24|2009-07-22|张家港浩波化学品有限公司|Sulphonation ring closure process of synthesizing potassium acetylsulfamilate and special device for the same|

CN100410246C|2006-09-24|2008-08-13|张家港浩波化学品有限公司|Hydrolysis process of synthesizing potassium acetylsulfamilate and special device for the same|

CA2729943A1|2008-07-08|2010-01-14|Board Of Regents, The University Of Texas System|Novel inhibitors of proliferation and activation of signal transducer and activator of transcription |

CN102264761A|2008-12-23|2011-11-30|先灵公司|Purification of recombinantly produced interferon|

EP2407146A1|2010-07-15|2012-01-18|Nutrinova Nutrition Specialties & Food Ingredients GmbH|Use of acesulfame K as a flavour modulator|

US9024016B2|2012-06-08|2015-05-05|Nutrinova Nutrition Specialists & Food Ingredients GmbH|Process for producing acesulfame potassium|

CN103450114B|2013-08-19|2015-09-02|苏州浩波科技股份有限公司|The chloro-6-methyl isophthalic acid of 5-, the synthetic method of 2,3-Yang oxazine-4 -one-2,2-dioxide|

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法律状态:

优先权:

申请号 | 申请日 | 专利标题

DE19843410439|DE3410439A1|1984-03-22|1984-03-22|METHOD FOR THE PRODUCTION OF 6-METHYL-3,4-DIHYDRO-1,2,3-OXATHIAZINE-4-ON-2,2-DIOXIDE AND ITS NON-TOXIC SALTS AND THE ACETOACETAMONE-N-SULDE-N-SULESSALTS)|

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