• 专利附录
  • 专利说明
  • 权利要求
  • 类似技术
  • 同族专利
  • 引用文献
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  • 优先权
    • 专利摘要:
    New and valuable process for the manufacture of 2,1,3-thiadiazin-4-one-2,2-dioxide derivatives by reaction of anthranilic acid amide or aminopyridine carboxamide derivatives with sulfur trioxide derivatives to give the sulfamic acid salts, followed by cyclization of these salts.
    公开号:SU715021A3
    申请号:SU782587400
    申请日:1978-03-09
    公开日:1980-02-05
    发明作者:Меркле Ханс;Мюллер Альбрехт;Цоллер Карл
    申请人:Басф Аг (Фирма);
    IPC主号:
    专利说明:

    The invention relates to a method for producing derivatives of 2,1,3-thiadiazin-4-one-2,2-dioxide of the general formula
    where R 1 is alkyl with 1-4 carbon atoms;
    R 2 is hydrogen or alkyl with 1–3 carbon atoms, galbgenalkyl with 2–3 carbon atoms, alkoxyalkyl with 2–3 carbon atoms;
    R 3 is hydrogen, halogen, trifluoromethyl, methyl, methoxy;
    Y is a group —CH “-> unsubstituted or substituted with halogen, methyl, methoxy, 2 q trifluoromethyl or
    Y = group -N =.
    It is known to obtain 2,1,3-benzothiadazin-4-one — 2,2— dioxides by reacting the corresponding esters of anthranilic acid with sulfamic acid halides [1].
    It is known to obtain compounds of the general formula (1), for example, 3-alkyl-2,1,3-benzothiadiazin-4-one-2.2 dioxide by reacting anthranilic acid with alkylamidosulfonyl chlorides in the presence of tertiary amines followed by cyclization of sulfamides with phosgene [2].
    The purpose of the invention is to increase the selectivity of the process.
    This goal is achieved due to the fact that the carboxylic acid amide of the general formula o n (2)
    NHR 2 where R 1 , R 2 , R 3 y have the previously given meanings, are reacted with sulfur trioxide or with chlorosulfonic acid in the presence of an organic base or with adduct
    volume of sulfur trioxide with an organic base to obtain a sulfamic acid salt and a base of the General formula
    ^ K- ^ OzN base (3)
    I ί>
    R where R 1 , R 2 , R 3 and Y have the meanings given above, followed by cyclization of the resulting sulfamic acid salt or free sulfamic acid in the presence of is anhydride or acid halide.
    According to the invention, use readily available and cheap starting materials is easier, much more economical than the known processes, the desired product 2 0 very high purity and in high yields. So, the purity of the obtained products is 96-100%. According to the literature, tll. the compounds of formula (1) is 128133 ° C. According to the invention, the same 25 product is obtained, with tl. 132-136 ° C.
    When implementing the proposed method, it is possible to use, for example, the following organic bases: trialkylamines, for example trimethylamine, triethylamine, dimethylethylamine, zc dimethylpropylamines, dimethylbutylamines, dimethylcyclohexylamine, tributylamine, N-methylmorpholine, N-ethylmorpholine, N-methylpiperidine; tert-amines, for example N-ethylimidazole, N-methylpyrrole, pyridine, alkylpyridines, quinol 35 , lutidine, quinaldine; Ν, Ν-dialkylanilines, e.g. dimethylaniline. diethylaniline, methylethylaniline; N-alkyldaphenylamines, for example N-methyldiphenylamine, N-ethyldaphenylamine; Ν, Μ-dialkylamides, for example dimethylformamide, 4 q dimethylacetamide; tetraalkylureas, for example tetramethyl and tetraethylurea; Schiff bases, for example, isopropylidene isopropyl amine.
    This compound may find use as bases for sulfonation aminopiridinkarbono- 45 O acids.
    For cyclization of salts of sulfamic acid of the formula (3), for example, organic acid halides, for example • acetyl chloride, are used. esters of chloroformic acid, imidoyl chlorides; carboxylic acid anhydrides, for example, acetic anhydride, inorganic acid halides, for example phosgene, phosphorus pentachloride, phosphoroxychloride, 55 bromine trifluoride or inorganic acid anhydrides, for example phosphorus pentoxide.
    The reaction is advisable weight · thus: 0.8-1.5, preferably
    0.95-13, a mole of sulfur trioxide is reacted with 0.95-2 mol of one of these bases at temperatures from -20 to 100 ° C, preferably -10, -30 ° C, in an inert solvent or diluent under the reaction conditions, for example, an aliphatic, if appropriate, chlorinated hydrocarbon, such as methylene chloride, chloroform, carbon tetrachloride, 1,2-dichloroethane, dichloropropanes, aromatic, if appropriate, chlorinated hydrocarbons, such as benzene, toluene, chlorobenzenes, dichlorobenzene; a hydrocarbon like gasoline, hexane, heptane, octane; ether, as diethyl ether, amide, as dimethylformamide, or in mixtures of the above solvents. The base used for the reaction can also simultaneously serve as a solvent during the reaction. In a solution or suspension of the sulfur trioxide adduct to the base at -20100 ° С, preferably -10 - 30 ° С, add 1 mol of amide or hydrazide of one of the listed anthranilic acids or aminopyridinecarboxylic acids in pure form, in the form of a suspension or solution, for example, in one of these solvents. After a few minutes, a sulfamic acid salt with a base is formed, which, depending on the reaction conditions, is obtained in the form of a suspension or solution. Sulfamic acid can be obtained by adding the adduct of sulfur trioxide to the base in pure form in suspension or solution of a compound of structural formula (2). The mixture is stirred for another 30 minutes -2 hours at room temperature, then adding 1-3 equivalents of one of the listed acid chlorides or acid anhydrides, after which the reaction mixture is stirred at room temperature to the boiling point of the solvent from 30 minutes to 2 hours. Then the reaction mixture is hydrolyzed water and recycle. Salts of sulfamic acid can also be isolated from the reaction mixture, for example, by filtration or removal of the solvent, followed by cyclization of the salts. In addition, sulfamic acid can be isolated from the salt, for example, with hydrogen chloride, followed by cyclization of the free acid. For economic and industrial reasons, the interaction and cyclization should be carried out sequentially without highlighting the intermediate stage.
    The method can be carried out intermittently and continuously, without pressure or under pressure.
    The compounds obtained by the proposed method are plant protection products, in particular 3-isopropyl-2,13 benzotaadiazin-4-one-2,2 dioxide and its sodium and ammonium salts.
    71
    Example la) 17.6 parts by weight sulfur trioxide is added over a period of 30 minutes at 0 ° C. to a solution of 21.5 parts of picolin in 300 parts of 1,2-dichloroethane.
    After 20 minutes, 33.65 parts of anthranilic acid isopropylamide are added in one go. A fine-crystalline precipitate forms from the solution formed after a short time, which is isolated by stirring for 1 h by filtration. After drying under high vacuum, 702 parts of the colorless picolinic salt of 1 - (isopropylamidocarbonyl) phenylsulfamic acid, mp. 147 u C.
    b) In suspension of picolin salt at room temperature for 5 minutes 15 21 parts of phosphoroxychloride are added, slowly heating the reaction mixture under reflux to a boil to form a brown solution. After boiling for 2 hours under reflux, the reaction mixture is hydrolyzed with water. 20 s ical organic phase was washed with water and then extracted three times with dilute aqueous sodium hydroxide solution. Get 3 — isopropyl-2,13 — benzothiadiazine — 4 — he — 2,2 — dioxide, so pl. 134 ° C.
    Example 2. A suspension of picolinic salt obtained analogously to 25 example 1 is added over 40 minutes to a solution of 30 parts of phosphoroxychloride in 100 parts of dichloroethane heated to reflux to form a light brown solution. Then another 30 half an hour is stirred, cooled and hydrolyzed at 20 ° C using 100 parts of water, then processing analogously to example 1. Receive 47 parts of dioxide 3-isopropyl-2,1,3-benzothiadiazin-4-one-2,2 , mp 135 ° C. 3 5
    Example 3. a) 9.0 parts of sulfur trioxide are added for 10 minutes at 0 ° C to 11.2 parts of picolin in 100 parts of 1,2-dichloroethane, then they are kneaded for 20 minutes, allowing the temperature to rise to 15 ° С , add at one time 17.92 hours 40 Ν, Ν — anthranilic acid dimethylhydrazide; the temperature does not change. The resulting colorless suspension was stirred for 1.5 hours at room temperature, followed by filtration. After drying under high vacuum at 45 20 ° C, 35.1 hours. The colorless picolinic salt of 2- (N, №dimepshgidrazidokarbonil) fenilsulfaminovoy acid aphids. 153 ° C.
    b) To a suspension of the picolinic salt of the obtained sulfamic acid at room temperature, add 11 parts of phosphoroxychloride, slowly heating the reaction mixture under reflux. After boiling the reaction mixture for 1 h under reflux, yellow ‘the product is hydrolyzed with water. The 55 organic phase is washed with water and then extracted several times with a dilute caustic solution. soda. Collected extracts acidify, semi
    5021 6 A valuable precipitate is filtered off with suction and dried, yielding 225 parts of yellow dioxide. 3-dimethyl-2,13-benzothiadiazine-H — she-2.2, mp 168 ° C, from toluene.
    Example 4. 9 parts of sulfur trioxide for 15 minutes at 0 ° C are added to the solution for 11 hours. picolina in 100 parts of 1.2 — dichloroethane. Then, 19.2 parts of 8-methylantrianilic acid isopropylamide are added, stirring the resulting suspension for 1 hour at room temperature. Then 15.4 parts of phosphoroxychloride are added, the reaction solution is boiled for 2 hours under reflux and processed in the usual way to obtain 24 parts of 8-methyl — 3-isopropyl — 2.13-benzothiadiazine-4-one-2.2, t pl. 124 ° C.
    Example 5. 9 parts of sulfur trioxide are added to a solution of 12 parts of triethylamine in 100 parts of 1,2-dichloroethane over 15 minutes at 20 ° C. Then, after half an hour, 17.8 parts of anthranilic acid isopropylamide were added to the yellow reaction solution. The resulting suspension was stirred at room temperature for another hour, then 12 parts of phosphoroxychloride was added and the mixture was stirred under reflux. After normal processing, 22 parts of 3-isopropyl — 2.13 — benzothiadiazine — 4 — she-2.2 dioxide are obtained, m.p. 134 ° C.
    Example 6. 8.5 parts of sulfur trioxide are added for 14 minutes at 10 ° C. to a solution of 14 parts of Ν, Ν-dimethylcyclohexylamine in 100 parts of 1,2-dichloroethane. In 20 minutes. add
    17.8 parts of anthranilic acid isopropylamide. Initially, a voluminous suspension gradually turns into a brown solution. Then it is kneaded for another 90 minutes, 15 parts of phosphoroxychloride are added and the mixture is refluxed for 2 hours to obtain 23 parts of 3-isopropyl-2,1,3-benzothiadiazin-4 — she-2.2 dioxide, mp. 134 ° C.
    Example 7. 9. parts of sulfur trioxide for 15 minutes at 0 ° C are added dropwise to a solution of 15 parts of dimethylaniline in 100 parts of dichloroethane. Then, 17.8 parts of anthranilic acid isopropylamide are added to the greenish-yellow solution. The brown reaction solution was stirred for 2 hours at room temperature, then 15 parts of phosphoroxychloride was added and 2 hours was heated under reflux. After that, it is cooled to 20 ° C and processed in the usual way, obtaining 22.8 parts of dioxide 3 — isopropyl — 2,1,3 — benzothiadiazine — 4 — she — 2.2, so pl. 133 ° C.
    Example 8. Within 10 minutes at 0 ° C, 9 hours of sulfur trioxide is added to the solution.
    14.9 parts of quinoline in 150 parts of dichloroethane. After an hour and a half, a colorless suspension is added at room temperature, 17.8 parts of isopropyl715021 anthranilic acid amide are added and the mixture is stirred for another 2 hours. After this, 12 parts of phosphoroxychloride are added, they are kept at room temperature for several minutes, and then thin-layer chromatography can be used to prove the presence of dioxide 3 —Isopropyl — 2.13 — benzothiadiazine — 4 — she-2.2. Then an additional 2 hours were stirred at 55 ° C and overnight at room temperature. After normal processing, 23.2 parts of dioxide-3 — isopropyl-2,13-10-benzothiadazin-4-one-23, aphids are obtained. 136 ° C.
    Example 9. 9 parts of sulfur trioxide are added dropwise over 15 minutes at 0 ° C. to 18 parts of tetramethyl urea in 100 parts of di ·. hporetana. To this small amount of crystallizate, a colorless solution, 17.8 parts of anthranilic acid isopropylamide are added. After a while, a brown solution forms, in which after 1 h of exposure at room temperature 20 to 15 parts of phosphoroxychloride are added. Thin-layer chromatography showed half an hour later that the reaction solution contained large amounts of 3-isopropyl-2,13-benzothiadiazine-4 — she-2.2 dioxide. By boiling for 25 hours under reflux, the cyclization is completed, after which the mixture is processed in the usual way, to obtain 20.5 parts of 3 -isoprosh-2,13-benzothiadiazin-4-one — 2.2, t. pl. 132 ° C. thirty
    Example 10. To a suspension of picoline salt (0.2 mol), analogously to example 2, 20 parts of phosphorus pentachloride are added, stirring the orange suspension initially at room temperature (through a short period of time, thin-layer chromatography proves the presence of 3-isopropyl dioxide 2,13-benzothia. Diazin-4-one-2.2). Then, the reaction solution was heated under reflux for 40 min to obtain an orange-40 red solution. After. conventional processing. 1 43.0 parts of 3-ieopronil-2.13-benzothiadiazin-4-one-2.2 dioxide, m.p. 134 ° C.
    Example I. To 0.2 mol of a suspension of pico } 5 linear salt (analogously to Example 1), 28 parts of phosphorus pentoxide are added; while lumps form in suspension. Then, it is heated under reflux for 2 hours, and the reaction mixture does not completely go into the Q state of the solution. After ordinary processing, 35 parts of Z-isopropyl-2,13-benzothiadi-1 azin-4-one — 2.2, tll. 134 ° C.
    EXAMPLE 12 A suspension of sulfamic acid salt is prepared in the same manner as in Example 5S ru 1. Then, 0.5 parts of dimethylformamide are added, and then phosgene gas is introduced at room temperature for 2 hours. After that, 100 parts of water are hydrolyzed and processed in the usual way. Get 20 parts of dioxide 3 — isopropyl-2,13 — benzothiadiazine — 4-one — -2.2, so pl. 132 ° C.
    Example 13. To the suspension of the sulfamic acid salt in Example 12, 10 parts of acetic anhydride are added and the mixture is refluxed for 2 hours. After ordinary processing, 15 parts of 3-isopropyl — 2,13-benzothiadiazine — 4 — she — 2.2 dioxide are obtained.
    Example 14. In the suspension of the sulfamic acid salt indicated in Example 12, 5 parts of acetyl chloride were added and the mixture was heated under reflux for 2 hours. After ordinary processing, 10 parts of 3 — isopropyl — 2.1 3 — benzothiadazin-4-one-2.2 dioxide are obtained.
    Example 15. 9 parts of sulfur trioxide are added over a period of 10 minutes at 0 ° C. to a solution of 15 parts of picolin in 150 parts of 1,2-dichloroethane. After mixing for 20 minutes, 17.9 g of 2-amino-pyridine-3-carboxylic acid isopropylamide are added in one go. The resulting colorless suspension is stirred for 2 hours at room temperature, after which 15.4 parts of phosphoroxychloride are added, 2 hours are heated under reflux; while the reaction mixture goes into a brown solution. Then it is hydrolyzed with water, the organic phase is washed and dried with sodium sulfate. After that, the filtered organic phase was evaporated to dryness to obtain 21.5 parts of 3-isopropyl-1-H-pyridino-(3,2-е) - 2,13-thiaziazin-4-one-2.2 dioxide, t pl. 190 ° C.
    In a similar manner, the compounds of formula (1) were obtained in which R 1 , R 2 and R 3 are shown in table. values.
    R 1 '. R 2 R 3 Melting point, 0 C, or refractive index (n ^ 5 ) 4 2. 3 4- sun 3 n - 207 s 2 n 5 N - 181 ns 3 n, N - 191-192 ns 4 n 9 n - 124 -C 4 H 9 n - 153-154 i-propyl CH 3 OCH 2 - 1,542 sun 3 ns 3 n, - 39 i-SzN, ’CHS - 54-55
    Continuation of the table.
    <1 2 3 4 1 — C 3 H 7 iC 3 H 7 - 44–45 <—C 3 n 7 HCV 2 H 4 - 1,5648 1-C 3 H 7 sun 3 6-Vg 135-137 C 2 H 5 sun 3 6-Vg 104-105 i — C 3 H 7 C 2 H 5 - 56-58
    Example 16. 9.6 g of SO 3 are added to a solution of 18.6 g of c-picoline in 300 g of 13-dichloroethane. for 15 minutes at 0 ° C. Then 21.25 g of 3-chloroanthranilic acid isopropylamide is added to the reaction mixture and the resulting suspension is stirred for one hour at room temperature. Then add 153 g of phosphorus oxychloride and cook the reaction mixture for 4 hours under reflux, and then prepare in the usual way.
    Get 24.7 g of dioxide 8-chloro-3 -isopropyl 5 saw-2,13-benzothiadiazine-4-one — 2.2 L · C.
    Example 17. 9.6 g of SO 3 are added to a solution of 18.6 g (β-picoline in 300 g of 1,2-dichloroethane for 15 minutes at 0 ° C. 20.8 g of isopropyl- 3 θ yes 3 are added to the reaction mixture -metoksiantranilovoy acid and stirred for one hour at room temperature. Then was added 153 g of phosphorus oxychloride and boiled under reflux for 3 hours, after something or, prepared in the usual obrazom- obtained 25 g of 8-methoxy-dioxide 35 -3 -isopropyl-2 , 13 — benzothiadiazine — 4 — she — 2.2, mp 111 ° C.
    Example 18. 98 g of SO 3 was added to a solution of 18.6 g of oC-picoline in 300 g of 1,2-dichloroethane over 15 minutes at 0 ° C. 24.6 g of 3-trifluoromethylanthranilic acid isopropylamide are added to the reaction mixture and stirred for one hour at room temperature. Then add 153 g of phosphorus oxychloride and cook for 4 hours under reflux, after which they are prepared in the usual way. Get 25 g of dioxide 8-trifluoromethyl-3-isopropyl-2,13-benzothiadiazine-4 — she — 2.2, so pl. 94 ° C.
    Example 19. 14 g of chlorosulfonic acid is added to a solution of 30 g of cL-picoline in 400 g of 1,2-dichloroethane over 15 minutes at 0 ° C. To the reaction mixture was added 17.8 g of anthranilic acid isopropylamide and stirred for one hour at room temperature. Then add 15.4 g of phosphorus oxychloride and cook for 4 hours under reflux. Conventional preparation yields 18 g of 3-isopropyl-2,13-benzothiadiaein-4-one -2,2 dioxide, mp. 136 ° C.
    Example 20. 10 parts of SO 3 are added to 20 parts of оС-picoline in 300 ml of 1,2-dichloroethane for 15 minutes at 0 ° C. After stirring for 20 minutes at 0 ° C., 17.82 hours are added. isthropylamide anthranilic acid. The fine crystalline white suspension formed after several minutes was stirred for one hour and 153 parts of phosphoroxychloride were immediately added. The reaction mixture was then heated for 3 hours under reflux (83 ° C).
    The yellow solution thus obtained is cooled and prepared in the usual manner. Get 23.8 parts of dioxide Z-isopropyl-2,13 — benzothiadiazine — 4 — she — 2,2, so pl. 137 ° C.
    权利要求:
    Claims (2)
    [1]
    the volume of sulfur trioxide with an organic base to obtain the salt of sulfamic acid and the base of the general formula 1 1 CK - R K- &gt; OCH-oc o5o // "(3) where R, R, R and Y have the previously mentioned values, followed by cyclization of the sulfate acid or free sulfamic acid in 1d in the presence of anhydride or acid halide. According to the invention, readily available cheap raw materials are used and simpler, much more economical than with the known methods, target products of very high purity and with high yields are obtained. Thus, the purity of the products obtained is 96-100%. According to literary data, tll. Compounds of formula (1) are between 128 and 133 C. According to the invention, the same product is obtained from T.Sh1. 132-136 ° C. In the implementation of the proposed method, the following organic bases are used, for example: trialkylamines, for example, trimethylamine, triethylamine, dimethylethylamine, dimethylpropylamines, dimethylbutylamine, dimethylcyclohexylamine, fibutylamine, N-methyl morpholine, N-ethylmeloxylamine; ; tert-amines, for example N-ethylimidazole. N-methylpyrrole, pyridine, alkylthridine, quino lin, lutidine, quinaldine; N, N-daalkylaniline, for example dimethylaniline ,. diethylashsh, methyl ethylaniline; M-alkyldaphenylamines, for example, L-methyldiphenylamine, .M-ethyldiphenylamine; M, N-dialkylamides, for example dimethylformamide, dimethyl acetamide; tetraalkyl ureas, for example tetramethyl and tetraethyl urea; Schiff bases, for example isoproshdeneisopropylamine. In the sulfonation of aminoiridinecarboxylic acids, eg, compounds can be used as bases. For the cyclization of sulfamic acid salts of formula (3), for example, organic acid halides, for example acetyl chloride, are used. chloroformate esters, imidoyl chlorides; carbonic anhydrides of Bbix acids, for example acetic anhydride, acid halides of inorganic acids, for example phosgene, phosphorus pentachloride, phosphorus oxychloride bromine trifluoride, or inorganic acid anhydrides, for example phosphorus pentoxide. The reaction of interaction is expedient in this way: 0.8-1.5, preferably 14 0.95-13, the mol of sulfur trioxide is reacted with 0.95-2 mol of one of the listed bases at temperatures from -20 to 100 ° C, preferably -10, -30 ° C, in an inergic solvent or diluent under the reaction conditions, for example an aliphatic, if appropriate, chlorinated hydrocarbon, such as methylene chloride, chloroform, carbon tetrachloride, 1,2-dichloroethane, dichloropropanes, somatic, in appropriate case chlorinated hydrocarbon, like benzene, toluo Chlorobenzenes, dahlorbenzol; hydrocarbons like gasoline, hexane, heptane, octane; ether, as diethyl ether, amide, as dimethylformamide, or in mixtures of previously educed solvents. The base used for the reaction can also simultaneously serve as a solvent during the reaction. To a solution or suspension of sulfur trioxide adduct to the base at -20100 ° G, preferably -10 - 30 ° C, add 1 mole of the amide or hydrazide of one of the listed anthranilic acids or aminopyridine scarboxylic acids in a pure form, in the form of a suspension or solution, for example, in one of the indicated solvents. After a few minutes, a sulfamic acid salt forms with the base, obtained depending on the reaction conditions in the form of a suspension or solution. Sulfamic acid can be obtained by adding the sulfur trioxide adduct to the base in pure form in a suspension or solution of the compound of structural formula (2). The mixture is stirred for another 30 minutes to 2 hours at room temperature, then adding 1-3 equivalents of one of the listed acid chlorides or acid anhydrides, after which the reaction mixture is stirred at temperatures from room temperature to a boiling point of solvent from 30 minutes to 2 hours. Then the reaction mixture hydrolyzed with water and recycled. Salts of sulfamic acid can also be isolated from the reaction mixture, for example, by filtration or removal of the solvent, followed by cyclization of the salts. In addition, sulfamic acid can be isolated from the salt, for example, hydrogen chloride, followed by cyclization of the free acid. For economic and industrial reasons, the interaction and cyclization should be carried out sequentially without isolating the intermediate stage. The method can be carried out intermittently and continuously, without pressure or under pressure. The compounds obtained by the proposed method are plant protection agents, in particular 3-isopropyl-2.13-benzothiadiazin-4-one-2, 2 dioxide and its sodium and ammonium salts. 57 Example 1. a) 17 weight.h. sulfur dioxide at 30 ° C for 30 minutes is added to a solution of 21.5 parts of picoline in 300 parts of 1,2-dichloroethane. After 20 minutes, 33.65 parts of ashranilic acid isopropylamide was added at a time. From the solution formed after a short time, a fine-crystalline precipitate is discharged, which is stirred, stirring for 1 h, by filtration. After drying under high vacuum, 70 D of colorless picolinic salt of 1 - (isopropylamidocarboket) -phenylsulfamic acid, T.Sh1 are obtained. . b) Suspend picopyne salt at room temperature for 5 minutes. 21 parts of phosphorus oxychloride are added, slowly heating the reaction mixture under reflux to a boil to form a brown solution. Proc. 2 hours under reflux the reaction mixture is hydrolyzed with water. The organic phase is washed with water and then extracted three times with aqueous dilute sodium hydroxide solution. Get 3-isoprop ffl-2,13-benzotiadiazin-4-one-2,2-dioxide, T.PL. 134 ° C. Example 2. A suspension of the picoline salt obtained analogously to Example 1 was added over 40 minutes to a solution of 30 parts of phosphoroxychloride in 100 parts of dichloromethane heated under reflux to boiling to form a light brown solution. Then, it is stirred for another half hour, cooled and hydrolyzed at 20 ° C using 100 parts of water, processing then as in Example 1. 47 parts of D-isoprop L-2,1,3-benzothiadiazin-4-one-2.2 dioxide are obtained. T.SH1. 135 ° C. Example 3. a) 9.0 parts of sulfur trioxide are added over 10 minutes at 0 ° C to 11.2 parts of picoline per 100 hours. 1,2-dichloroethane is added, then the mixture is stirred for 20 minutes, allowing the temperature to rise to 15 ° C, 17.92 parts of N, N-dimethylhydrazide anthranilic acid are added at a time; the temperature does not change. The resulting colorless slurry for 1.5 hours is incubated at room temperature, followed by filtration. After drying under high vacuum at 20 ° C., 35.1 parts of the colorless picolinic salt of 2- (M, M dimethylhydrazidocarbonyl) phenylsulfamic acid are obtained, mp. 153 ° C. B) To the suspension of the picolinic salt of the resulting sulfamic acid, 11 parts of phosphoroxychloride are added at room temperature, slowly heating the reaction mixture under reflux. After boiling the reaction mixture for 1 h under reflux, the yellow product was hydrolyzed with water. The organic phase is washed with water and then extracted several times with a dilute caustic solution. soda. The collected extracts are acidified, and the precipitate obtained is aspirated and dried, with about 22 parts of yellow dioxide. 3-d methylamino2, 13-benzothiadiazin-α-2,2, so pl. 168 ° C, from toluene. Example 4. 9 parts of sulfur trichoxy are added to a solution of 11 parts picoline in 100 parts of 1.2-dichloroethane over 15 minutes. Then 19.2 parts of isopropyl amide of 8-methane-trianilic acid are added, stirring the slurry for 1 hour at room temperature. Then 15.4 parts of phosphorus oxychloride are added, the reaction solution is boiled under reflux for 2 hours and it is worked up in the usual way to obtain 24 parts of 8-methyl-3-isopropyl-2,13-benzothiadiazin-4-one-2 dioxide, 2, t. Roi. 124 ° C. Example5.9h. sulfur dioxide for 15 minutes at 20 ° C is added to a solution of 12 parts of triethylamine in 100 hours of 1,2-dichloroethane. Then, after half an hour, 17.8 parts of HsonporouiaNowa anthranilic acid are added to the yellow reaction solution. Stir for another 1 hour stirring at room temperature, then add 12 parts of phosphoroxychloride and stir for 2 hours under reflux. After the usual processing of half-casings 22 hours of dioxide, 3-isoproshosh-2,13-benzothiadiazin-4-one-2, 2, so pl. 134 ° C. EXAMPLE 6 8.5 parts of sulfur trioxide are added to a solution of 14 parts of N, N-dimethyl-cyclohexutamine per 100 parts of 1,2-dichloroethane over 15 minutes at 10 ° C. After 20 minutes, 17.8 hours are added. izoprohoshal {3 and anthranilic acid. Initially, the bulky nocTeneifflO suspension turns into a brown solution. Then another 90 minutes are added, 15 parts of phosphorus oxychloride are added and the mixture is heated under reflux for 2 hours, 23 parts of diochroxy 3-isoprosh-2, 1,3-benzothiadnaein-4-one-2.2. T.PL. 134 ° C. Example 7. 9. parts of sulfur trioxide for 15 minutes at 0 ° C are added dropwise to a solution of 15 parts of dimethylanil per 100 parts of dichloroethane. Then, 17.8 parts of propylene and anthrachosic acid are added to the greenish-yellow solution. The coryicene reaction solution is stirred for 2 hours at room temperature, then 15 parts of phosphoroxychloride are added and 2 hours are heated under reflux. After that, it is cooled to 20 ° C and processed in the usual way to obtain 22.8 parts of 3-isopropyl-2,1,3-benzothiadiazin-4-one-2.2 dioxide, m.p. 33 ° C. Example 8. Within 10 minutes at 0 ° C, 9 hours of sulfur trioxide are added to a solution of 14.9 hours. X1sholine in 150 hours of dichloroethane. After a half hour, add to the colorless suspension at a constant temperature of 17.8 parts of isopropyl anthranilic acid and stir for 2 hours. After this, add 12 parts of phosphorus oxychloride, keep it at a temperature of several minutes, then thin-layer chromatography can be proved 3-isopropyl-2,13 benzothiaadaazin-H-one-2 dioxide. Then, for another 2 hours, stir 1 FIP temperature of 55 ° C and overnight at room temperature. After processing, 23.2 parts of dioxide-3-nzopropyl-2,1-benzothiadiazin-4-one-2, 2, t.Sh1 are obtained. 136 ° C. Example 9. 9 parts of sulfur trioxide are added in a manner of 15 minutes at 18 parts of tetramethyl urea per 100 parts of dihporethia. To this colorless solution containing a small amount of a crystalline solution was added 17.8 parts of ayranilic acid isogofoslamide. After some time, a brown11 solution is formed, into which after 1 h of aging. At the room temperature, 15 parts of phosphorus oxychloride are added. Thin-layer chromatography shows in half an hour that large amounts of 3-isopropyl-2,13-benzothiadiazine 4-one-2, 2 are contained in the reaction solution. By refluxing the cyclization for 2 hours, the cyclization is completed, after which the mixture is processed in the usual way, yielding 20.5 parts of the 3-isoprog 1p-2,13-benzothiadiazin-4 - «-2 -2, T. Ш1. 132 ° C., Example 10. 20 parts of phosphorus chloride were added to a slurry of picoline salt (0.2 mol) as in Example 2 while stirring the orange suspension initially at room temperature (after a short period of time, thin layer chromatography can be shown 3-isoprotein-1, 2, 13-benzothiadiazin-4 (she-2.2). Then the reaction solution is heated under reflux for 40 minutes to obtain an orange-red solution. After. conventional non-processing. 43.0 parts are obtained. 7-euproximate 2,13-benzothiadiazin-4-one-2.2, tll. 134C. PRI me R and. 28 parts of phosphorus pentoxide are added to 0.2 mol of the suspension of the picoline salt (as in Example 1); at the same time lumps form in suspension. Then it is heated under reflux for 2 hours, and the reaction mixture does not fully enter the state of solution. After usual processing, 35 parts of 3-iso-propyl-2,13-benzothiadi-i azin-4-one-2.2 dioxide are obtained. 134 ° C. EXAMPLE 12 A suspension of a sulfamic acid salt is prepared in the same manner as in Example 1. Then 0.5 parts of dimethylformamide is added, after which phosgene gas is introduced at room temperature for 2 hours. After that, 100 parts of water are hydrolyzed and processed by the usual method HNi-C 8. Get 20 hours of dioxide 3-isoprohosh-2L 3-benzothiadiazin-4-one -2.2, so pl. 132 ° C. Example 13. In the suspension of the sulfamic acid salt given in Example 12, 10 parts of acetic anhydride were added and the mixture was heated under reflux for 2 hours. After usual processing, 15 parts of 3-isoprosh-2,13-benzothiadiazin-4-one-2.2 dioxide are obtained. Example 14. In the suspension of family sushi acid indicated in Example 12, 5 parts of acetyl chloride are added and the mixture is heated under reflux for 2 hours. After the usual processing, 10 parts of 3-isopropyl-2, 13-benzothiadiazin-4-one-2.2 dioxide are obtained. Example 15. 9 parts of sulfur trioxide are added for 10 hours at 0 ° C to the solution of IS Ch. Picoscia in 150 parts of 1,2-dichloroethane. After stirring for 20 minutes, 17.9 g of 2-amino-pyridine-3-carboxylic acid isoproshamide are added in one cree. The obtained colorless suspension is stirred for 2 hours at room temperature, after which 15.4 parts of phosphoroxychloride are added, the mixture is heated for 2 hours with refluxing; at the same time, the reaction mixture turns into a brown solution. Then the hydrolysis of gkgg water, the organic phase gfomshakzt and svdvat sodium sulfate. Thereafter, the filtered organic phase is evaporated to dryness, yielding 21.5 parts of 3-isoprosh-1-H-pyridino- (3,2-e) -2,13-thioadiax-4-she-2, 2, t. square . Compounds of formula (1) are obtained in a similar way, in which the inverters R and R are listed in Table. value. CzN, H 191-192 C. NoH 124,153-154 ropyl CH3 OCHj - 1,542 H-CsN - 3N, P p & m ep 16. 9.6 g of 80z are added to a solution of 18.6 ° C-picoline in 300 g 1D-dichloroethane c. for 15 minutes at 0 ° C. 21D5 g of 3-chlororanthranilic acid isopropylamide is then added to the reaction mixture and the resulting suspension is stirred for one hour at room temperature. Then 153 g of phosphorus oxychloride are added and the reaction mixture is boiled under reflux for 4 hours, after which it is prepared in the usual way. 24.7 g of dioxide 8-hlrr-3-isopr PSh1-2,13-benzothiadiazin-4-one-2.2, t are obtained. square 82 Example 17. 9.6 g of 5O3 are added to a solution of 18.6 th (. - picoline in 300 g of 1,2-dichloroethane over 15 minutes at. To the reaction mixture is added 20.8 g of 3-methoxyaccranic acid isopropylamide and stirred for one hour at room temperature. Then 153 g of phosphorus oxychloride is added and refluxed for 3 hours, after which it is prepared: in the usual manner. 25 g of 8-methoxy-3 -isopropyl-2,13 dioxide are obtained -Benzothiamid-1-4-a-2.2 t., melting point 111 ° C. Example 18. 9.6 g of D3 are added to a solution of 18.6 g of o1.-picoline in 300 g of 1,2-dichloroethane over 15 minutes at 0 ° C. 24.6 g of isopropyl amide 3-trifluoromethyl-anthracic acid are added to the reaction mixture and the mixture is stirred for 1 hour at room temperature, 153 g of phosphoroxychloride are then added and the mixture is heated under reflux for 4 hours, and then prepared in the usual manner. 8-trifluorometh-1 -3-isopropyl-2,13-benzothiadiazin-4-one-2, 2 dioxide, mp: 94 ° C. Example 19.14G of chlorosulfonic acid is added to a solution of 30 g o (, picoline in 400 g 1 , 2-dichloroethane for 15 min at 0 ° C. 17.8 g of antranilic isopropylamide is added to the reaction mixture and stirred for one hour at room temperature. Then 15.4 g of phosphorus oxychloride is added and cooked for 4 hours under reflux; 1nick. An ordinary preparation will receive 18 G of 3-isopropyl-2,13 dioxide - J-H30 thiadiazn-4-one-2, 2, m. 136 ° C. Example 20. 10 hours 50s are added to 20 hours. OL-picoline in 300 ml of 1,2-dichloroethane over 15 minutes at 0 ° C. After stirring for 20 minutes at 0 ° C, 17.82 hours are added. anthranilic acid isopropylamide. The fine white crystalline suspension, which forms after a few minutes, is stirred for an hour and 153 parts of phosphorus oxychloride are immediately added. The reaction mixture is then heated for 3 hours under reflux (83 ° C). The resulting yellow solution is cooled and prepared in the usual way. 233 parts of 3-isopropyl-2,13-benzothiadiazole {n-4-one-2, 2, m.p. 137 ° C. The invention The method of obtaining derivatives of 2,13-thiadiazin-4-one-2, 2-dioxide of the general formula </ BR> where R is alkyl with 1-4 carbon atoms; R is hydrogen or alkyl with 1-3 carbon atoms, haloalkyl with 2-3 carbon atoms, alkoxyalkyl with 2-3 carbon atoms; R is hydrogen, halogen, trifluoromethyl, methyl, methoxy; Y is a -CHf group, unsubstituted or mixed with halogen, methyl, methoxy, trifluoromethyl, or Y is an -N group, characterized in that, in order to increase the selectivity of the process, the amidarboxylic acid of general formula II have the given values, interact with sulfur trioxide or with chlorosulfonic acid in the presence of organic bases or with sulfur trioxide adducts with an organic base with R. R, R n In the nmenug given above, cyclis iey Vani common salt or free acid formulysulfaminovoy sulfa0 N.mnnovoy acid in the presence of I galogenangidII row or acid anhydride. V N Sources of information,., Taken into account in the examination of Y If - OCH-OCHOOOWLe (3,} 1. USSR Patent N 509233, class C 07 D 285/16, published 1975.
    [2]
    2. Patent of the USSR NO 514571, with Q-J Q 285/16, published. 1976 (prototype).
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    同族专利:
    公开号 | 公开日
    NL188947C|1992-11-16|
    NL971033I1|1997-10-01|
    NL7802662A|1978-09-12|
    JPS6238352B2|1987-08-17|
    GB1595029A|1981-08-05|
    BE864705A|1978-09-11|
    HU178438B|1982-05-28|
    NL971036I1|1997-10-01|
    BR7801459A|1978-10-31|
    ATA171878A|1979-08-15|
    SE436743B|1985-01-21|
    TR19681A|1979-10-05|
    FI780694A|1978-09-11|
    IT7848362D0|1978-03-09|
    PL108030B1|1980-03-31|
    NL971035I1|1997-10-01|
    CA1086728A|1980-09-30|
    IL54092D0|1978-04-30|
    AU3351078A|1979-08-30|
    DK105178A|1978-09-11|
    DE2710382C2|1983-12-22|
    NL971034I1|1997-10-01|
    US4175184A|1979-11-20|
    AU514429B2|1981-02-12|
    FR2383177B1|1983-01-07|
    YU54178A|1982-08-31|
    DD134092A5|1979-02-07|
    ZA781380B|1979-03-28|
    AR230835A1|1984-07-31|
    JPS53112888A|1978-10-02|
    DK145378B|1982-11-08|
    FI68233C|1985-08-12|
    NL188947B|1992-06-16|
    GR66117B|1981-01-16|
    FI68233B|1985-04-30|
    DK145378C|1983-04-05|
    DE2710382A1|1978-09-14|
    SE7802669L|1978-09-11|
    IT1104109B|1985-10-14|
    IN147927B|1980-08-16|
    PL205164A1|1979-02-12|
    IL54092A|1980-09-16|
    NL971038I1|1997-10-01|
    CS204023B2|1981-03-31|
    FR2383177A1|1978-10-06|
    AT355588B|1980-03-10|
    CH633545A5|1982-12-15|
    NL971037I1|1997-10-01|
    ES467704A1|1978-10-16|
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    DE1120456B|1958-10-01|1961-12-28|Geigy Ag J R|Process for the preparation of new 4-oxo-3, 4-dihydro-2, 1, 3-benzothiadiazine-2, 2-dioxydes|
    FR1354761A|1959-09-30|1964-03-13|Geigy Ag J R|Novel 3-oxo-1.2.6-thiadiazine 1.1-dioxides and their preparation|
    US3217001A|1963-08-19|1965-11-09|American Home Prod|Derivatives of 1h-2, 1, 3-benzothiadiazin-4-one 2-oxide and intermediates therefor|
    DE2105687C2|1971-02-08|1981-09-24|Basf Ag, 6700 Ludwigshafen|Process for the preparation of 3-substituted 2,1,3-benzothiadiazin-4-one-2,2-dioxides|
    US3989507A|1973-11-05|1976-11-02|The Dow Chemical Company|1H-pyrido thiadiazin-4-one-2,2-dioxides and derivatives thereof|
    DE2357063C2|1973-11-15|1986-07-17|Basf Ag, 6700 Ludwigshafen|Process for the preparation of N-isopropyl-2,1,3-benzothiadiazin-4-one-2,2-dioxide|
    US4014888A|1975-04-28|1977-03-29|The Dow Chemical Company|Substituted pyridine carboxylic acids and derivatives|US5136085A|1990-11-28|1992-08-04|Glaxo Inc.|Synthesis of 2-aminobenzophenones|
    DE19505036A1|1995-02-15|1996-08-22|Basf Ag|Process for the preparation of ammonium salts of 3-isopropyl-2,1,3-benzothidadizin-4-one-2,2-dioxide|
    DE19735682A1|1997-08-19|1999-02-25|Basf Ag|Single step production of a benzothiadiazinone di:oxide|
    US7288554B2|2001-08-15|2007-10-30|E.I. Du Pont De Nemours And Company|Ortho-substituted aryl amides for controlling invertebrate pests|
    EP1467988B1|2002-01-22|2013-07-17|E.I. Du Pont De Nemours And Company|Quinazolineones for invertebrate pest control|
    CN101973961B|2010-09-26|2012-06-27|合肥星宇化学有限责任公司|Preparation method for bentazone|
    法律状态:
    优先权:
    申请号 | 申请日 | 专利标题
    DE2710382A|DE2710382C2|1977-03-10|1977-03-10|Process for the preparation of 2,1,3-benzothiadiazin-4-one-2,2-dioxide derivatives|
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