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CN101607957B - Intermediate for preparing 3-halo-4,5-dihydro-1h-pyrazoles - Google Patents

Intermediate for preparing 3-halo-4,5-dihydro-1h-pyrazoles Download PDF

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CN101607957B
CN101607957B CN2009101394048A CN200910139404A CN101607957B CN 101607957 B CN101607957 B CN 101607957B CN 2009101394048 A CN2009101394048 A CN 2009101394048A CN 200910139404 A CN200910139404 A CN 200910139404A CN 101607957 B CN101607957 B CN 101607957B
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alkyl
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amino
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CN101607957A (en
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G·D·安尼斯
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FMC Agro Singapore Pte Ltd
FMC Corp
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EI Du Pont de Nemours and Co
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Abstract

This invention relates to a method for preparing 3-halo-4,5-dihydro-1H-pyrazole compound of Formula (I), comprising contacting with HX1 a different 4,5-dihydro-1H-pyrazole compound of Formula (II), wherein X1 is halogen and L, R, k and X2 are as defined in the disclosure. This invention also discloses preparation of compounds of Formula (III) wherein X1, R3, R6, R7, R8a, R8b, and n are as defined in the disclosure.

Description

Be used to prepare 3-halo-4, the midbody of 5-dihydro-1 h-pyrazole
The application is dividing an application of following application: the applying date: on July 29th, 2003; Application number: 03818171.1 (PCT/US2003/023820); Denomination of invention: the same.
Background of invention
Still need other preparation 3-halo-4 at present, the method for 5-dihydro-1 h-pyrazole.These compounds comprise useful as intermediates, and said midbody is used to prepare crop protection agent, medicine and other fine chemical product.
More existing preparation 3-halos-4, the report of 5-dihydro-1 h-pyrazole method.For example, J.P.CHUPP, J.Heterocyclic Chem.1994,31, the 1377-1380 report is through making corresponding oxo pyrazoles alkane and phosphoryl chloride prepared in reaction 3-chloro-4,5-dihydro-1 h-pyrazole.M.V.Gorelik et al..Joumal of Organic Chemistry U.S.S.R.1985,21,773-781 (Zhumal Organicheskoi Khimii 1985; 21 (4); The English translation of 851-859) disclose, through amino-4 from corresponding 3-, the 5-dihydro-1 h-pyrazole prepares the diazonium salt midbody; Thereby preparation 3-chloro-4, the 5-dihydro-1 h-pyrazole.K.K.Bach et al.; Tetrahedron 1994; 50 (25), 7543-7556 announces, prepares 3-chloro-4 through making propenoate and the cycloaddition of hydrazine acyl chlorides midbody dipole; The 5-dihydro-1 h-pyrazole, wherein hydrazine acyl chlorides midbody forms the hydrazone generation decarboxylation chlorization of oxoethanoic acid with N-chlorosuccinimide.Still need the alternate method, especially have wider chemical structure ubiquity and use the low-cost compositions and methods of industrial business supply.
Summary of the invention
The present invention relates to prepare the 3-halo-4 of formula I, the method for 5-dihydro-1 h-pyrazole compound:
Figure GA20175791200910139404801D00021
Wherein L is optional substituted carbon part;
Each R independently is selected from optional substituted carbon part;
K is the integer of 0-4;
And X 1Be halogen.
Present method comprises makes 4 of formula II, 5-dihydro-1 h-pyrazole compound and formula HX 1Compound in being fit to solvent, react:
Figure GA20175791200910139404801D00022
X wherein 2Be OS (O) mR 1, OP (O) p(OR 2) 2Or be different from X 1Halogen;
M is 1 or 2;
P is 0 or 1;
R 1Be selected from alkyl and haloalkyl and optional by 1 to 3 substituted phenyl of substituting group that is selected from alkyl and halogen; And
Each R 2Independently be selected from alkyl and haloalkyl and optional by 1 to 3 substituted phenyl of substituting group that is selected from alkyl and halogen.
The invention still further relates to the method for preparing the formula III compound:
Figure GA20175791200910139404801D00031
X wherein 1Be halogen;
Each R 3Independent is C 1-C 4Alkyl, C 2-C 4Thiazolinyl, C 2-C 4Alkynyl, C 3-C 6Naphthenic base, C 1-C 4Haloalkyl, C 2-C 4Haloalkenyl group, C 2-C 4Halo alkynyl, C 3-C 6Halogenated cycloalkyl, halogen, CN, NO 2, C 1-C 4Alkoxyl group, C 1-C 4Halogenated alkoxy, C 1-C 4Alkylthio, C 1-C 4Alkyl sulphinyl, C 1-C 4Alkyl sulphonyl, C 1-C 4Alkylamino, C 2-C 8Dialkyl amido, C 3-C 6Cycloalkyl amino, (C 1-C 4Alkyl) (C 3-C 6Naphthenic base) amino, C 2-C 4Alkyl-carbonyl, C 2-C 6Alkoxy carbonyl, C 2-C 6Alkyl amino-carbonyl, C 3-C 8Dialkyl amino carbonyl or C 3-C 6Trialkylsilkl;
Z is N or CR 5
R 5Be H or R 3
R 6Be CH 3, F, Cl or Br;
R 7Be F, Cl, Br, I or CF 3
R 8aBe C 1-C 4Alkyl;
R 8bBe H or CH 3And
N is the integer of 0-3,
This method is used the compound of following formula I a:
R wherein 4Be H or optional substituted carbon part.
Present method be characterized as the compound (i.e. the formula I compound of a subclass) for preparing formula Ia through top said method.
Detailed Description Of The Invention
In the present invention, term " carbon part " is meant carbon atom and 4, the substituting group that 5-dihydro-1 h-pyrazole ring skeleton links to each other.Because carbon part L and R (comprise R 4) substituting group for being separated by reactive center, they can comprise a large amount of various carbon type groups by modern synthetic organic chemistry method preparation.Method of the present invention can generally be applicable to various formula I initial compounds and formula II product.Those skilled in the art can find that some group is responsive to hydrogen halide, and can under reaction conditions, be transformed.Those skilled in the art also can find, some group is an alkalescence, and can with the hydrogen halide salify, therefore method of the present invention possibly also need other hydrogen halide.
Therefore " carbon part " comprises alkyl, thiazolinyl and alkynyl, and they can be straight or branched." carbon part " also comprises carbocyclic ring and heterocycle, and they can be saturated, fractional saturation or complete unsaturated ring.And if satisfy the Huckel rule, unsaturated ring can be an aromatic ring.The carbocyclic ring of carbon part and heterocycle can form the multi-loop system that comprises a plurality of rings that are connected together.Term " carbocyclic ring " is meant that the atom that forms the ring skeleton is the ring of carbon.Term " heterocycle " is meant that at least one ring skeletal atom is not the ring of carbon." saturated carbon ring " is that finger ring skeleton carbon atom is through singly-bound ring connected to one another; Except as otherwise noted, remaining carbon valency is occupied by Wasserstoffatoms.Term " aromatic ring system " complete unsaturated carbocyclic of expression and heterocycle, at least one ring is an aromatics in the multi-loop system.Aromatics is represented each annular atoms basically on same plane, and has and the vertical p track of plane of a loop, and on the ring (4n+2) individual πDian Zi is arranged, and n is 0 or positive integer, meets the Buckel rule.Term " aromatic carbocyclic system " comprises that at least one ring is the carbocyclic ring of aromatics in Wholly aromatic carbocyclic ring and the multi-loop system.Term " non-aromatic carbocyclic system " complete saturated carbon ring of expression and unsaturated carbocyclic partially or completely, wherein in the loop systems not ring aromatic ring is arranged.Term " aromatic heterocycle system " and " hetero-aromatic ring " comprise that at least one ring is the heterocycle of aromatics in Wholly aromatic property heterocycle and the multi-loop system.Complete saturated heterocyclic of term " non-aromatic heterocyclic system " expression and unsaturated heterocycle partially or completely have no ring that aromatic ring is arranged in the unsaturated heterocycle.Term " aryl " representes that at least one ring is carbocyclic ring or the heterocycle that aromatic ring and other part of this aromatic ring and molecule are connected.
About L, R and R 4Carbon part be optional substituted.The term of relevant these carbon parts " optional substituted " is meant not have replacement or have at least one non-hydrogen substituent carbon part.The optional substituting group of illustrative comprises that alkyl, thiazolinyl, naphthenic base, cycloalkenyl group, aromatic group, hydroxycarbonyl group, formyl radical, alkyl-carbonyl, alkenyl carbonyl, alkynyl carbonyl, alkoxy carbonyl, hydroxyl, alkoxyl group, alkenyloxy, alkynyloxy group, cycloalkyloxy, aryloxy, alkylthio, thiazolinyl sulfenyl, alkynyl sulfenyl, cycloalkylthio, arylthio, alkyl sulphinyl, thiazolinyl sulfinyl, alkynyl sulfinyl, naphthenic base sulfinyl, aryl sulfonyl kia, alkyl sulphonyl, thiazolinyl alkylsulfonyl, alkynyl alkylsulfonyl, naphthene sulfamide base, aryl sulfonyl, amino, alkylamino, alkenyl amino, alkynyl amino, arylamino, aminocarboxyl, alkyl amino-carbonyl, alkenyl amino carbonyl, alkynyl aminocarboxyl, aromatic yl aminocarbonyl, alkyl amino-carbonyl, alkenyl amino carbonyl, alkynyl aminocarboxyl, fragrant amino carbonyl oxygen base, alkoxycarbonyl amino, alkenyloxy carbonylamino, alkynyloxy group carbonylamino and aryloxycarbonyl are amino, and each substituting group is optional further to be replaced; And halogen, cyanic acid and nitro.Further optional substituting group independently is selected from the above groups of enumerating with regard to substituting group itself such as substituting group, thereby forms L, R and R 4New substituting group is like haloalkyl, haloalkenyl group and halogenated alkoxy.Further for instance, alkylamino can further be replaced by alkyl, forms dialkyl amido.Substituting group also can link together; Figuratively speaking; Each substituting group from two substituting groups is perhaps removed one or two Wasserstoffatoms from a substituting group and said supportive molecular structure; Said then group couples together and produces ring texture and polynuclear plane, and said ring texture and polynuclear plane condense or additional being connected supported on the said substituent molecular structure.For example, hydroxyl adjacent on the phenyl ring is connected with methoxyl group, forms and contain-O-CH 2-O-group condense the dioxolane structure.The coupled molecular structure of hydroxyl couples together, and can form the cyclic ethers that comprises epoxide.The illustrative substituting group also comprises oxygen, when it links to each other with carbon, forms the carbonyl functional group.Form thiocarbonyl functionality when equally, sulphur links to each other with carbon.In carbon part L or R, substituting group connects can form ring or polynuclear plane.Carbon part L and R illustrative embodiment are: comprise at least two R parts in the same substituting group or comprise L part and at least one R part (promptly forming loop systems).Because 4, the 5-pyrazoline partly constitutes a ring, in same group, comprise the R part of two vicinals or comprise two vicinal L and R part, can form thick two ring or multi-loop systems.In same substituting group, comprise two and can form spirane structure together with position R part.
In the present invention; No matter " alkyl " is to use separately or the use of compound part of speech; Like " alkylthio " or " haloalkyl ", include straight chained alkyl or branched-chain alkyl, for example methyl, ethyl, n-propyl, sec.-propyl or different butyl, amyl group or hexyl isomer.The said substituting group 1-2 of term " 1-2 alkyl " expression instead position can be independent selected alkyl." thiazolinyl " comprises normal olefine or branched-chain alkene, like vinyl, 1-propenyl, 2-propenyl and different crotonyl, pentenyl and hexenyl isomer." thiazolinyl " also comprises the polyenoid alkyl, for example 1, and 2-propadiene base and 2,4-hexadienyl." alkynyl " comprises straight or branched alkynes, like ethynyl, 1-proyl, 2-propynyl and different butynyl, pentynyl and hexyn isomer." alkynyl " also can comprise a plurality of triple-linked parts, as 2, and 5-hexadiyne base." alkoxyl group " comprises for example methoxyl group, oxyethyl group, positive propoxy, isopropoxy and different butoxy, pentyloxy and hexyloxy isomer." alkenyloxy " comprises straight or branched alkenyloxy part.The instance of " alkenyloxy " comprises H 2C=CHCH 2O, (CH 3) 2C=CHCH 2O, (CH 3) CH=CHCH 2O, (CH 3) CH=C (CH 3) CH 2O and CH 2=CHCH 2CH 2O." alkynyloxy group " comprises straight or branched alkynyloxy group part.The instance of " alkynyloxy group " comprises HC ≡ CCH 2O, CH 3C ≡ CCH 2O and CH 3C ≡ CCH 2CH 2O." alkylthio " comprises side chain or straight chain alkylthio part, for example methylthio group, ethylmercapto group and different rosickyite bases, butylthio, amyl group sulphur and own sulfenyl isomer." alkyl sulphinyl " comprises two kinds of optically active enantiomorphs of alkyl sulphinyl group.The instance of " alkyl sulphinyl " comprises CH 3S (O), CH 3CH 2S (O), CH 3CH 2CH 2S (O), (CH 3) 2CHS (O) and different butyl sulfinyls, amyl group sulfinyl and hexyl sulfinyl isomer.The instance of " alkyl sulphonyl " comprises CH 3S (O) 2, CH 3CH 2S (O) 2, CH 3CH 2CH 2S (O) 2, (CH 3) 2CHS (O) 2With different butyl alkylsulfonyls, amyl group alkylsulfonyl and hexyl alkylsulfonyl isomer.Instance above the definition of terms such as " alkylamino ", " thiazolinyl sulfenyl ", " thiazolinyl sulfinyl ", " thiazolinyl alkylsulfonyl ", " alkynyl sulfenyl ", " alkynyl sulfinyl ", " alkynyl alkylsulfonyl " is similar.The instance of " alkyl-carbonyl " comprises C (O) CH 3, C (O) CH 2CH 2CH 3And C (O) CH (CH 3) 2
The instance of " alkoxy carbonyl " comprises CH 3OC (=O), CH 3CH 2OC (=O), CH 3CH 2CH 2OC (=O), (CH 3) 2CHOC (=O) with different butoxy carbonyls or pentyloxy carbonyl isomer." naphthenic base " comprises for example cyclopropyl, cyclobutyl, cyclopentyl and cyclohexyl.Term " cycloalkyloxy " comprises the same group that links to each other through Sauerstoffatom, like cyclopentyloxy and cyclohexyloxy." cycloalkyl amino " is meant that amino nitrogen atom links to each other with a Wasserstoffatoms with group of naphthene base, comprises as cyclopropyl is amino, cyclobutyl is amino, cyclopentyl is amino and cyclohexyl is amino." (alkyl) (naphthenic base) amino " is meant that the Wasserstoffatoms on the nitrogen is by the substituted group of alkyl in the cycloalkyl amino; Instance comprises (methyl) (cyclopropyl) amino, (butyl) (cyclobutyl) amino, (propyl group) cyclopentyl amino, (methyl) cyclohexyl amino etc." cycloalkenyl group " comprises for example cyclopentenyl and cyclohexenyl and has the group that surpasses two keys, like 1 base and 1 base.
Term " halogen " no matter uses separately or compound part of speech is used, and like " haloalkyl ", comprises fluorine, chlorine, bromine or iodine.One or two desirable subrogating can be independent selected halogen on the said substituting group of term " 1-halogen " expression.And when being used for compound word like " haloalkyl ", said alkyl can be partially or completely replaced by halogen, said halogen atom can be identical also can be different.The instance of " haloalkyl " comprises F 3C, ClCH 2, CF 3CH 2And CF 3CCl 2
The total number of carbon atoms in the substituting group is by prefix " C i-C j" expression, wherein i and j for example are 1 to 3 numeral; C for example 1-C 3Alkyl representes that methyl is to propyl group.
Though do not have clear and definite size restriction for formula I that is fit to the inventive method and II, preferred formula II comprises 4-100 carbon atom, is more preferably 4-50, most preferably be 4-25, and comprise 3-25 heteroatoms, more preferably 3-15, most preferably 3-10.Heteroatoms is selected from halogen, oxygen, sulphur, nitrogen and phosphorus usually.Two heteroatomss among formula I and the II are pyrazoline theheterocyclic nitrogen atoms; X 1Be halogen, X 2Contain at least one heteroatoms.
Though (comprise R for L and R 4) there is not clear and definite size restriction, L and R (comprise R 4) in the alkyl chain of optional substituted moieties generally include 1-6 carbon atom, more preferably 1-4 carbon atom most preferably is 1-2 carbon atom.L and R (comprise R 4) in optional substituted thiazolinyl generally include 2-6 carbon atom with alkynyl alkenyl or alkynyl chain partly, more preferably 2-4 carbon atom most preferably is 2-3 carbon atom.
Equally, for R 1And R 2The group of listing does not have clear and definite size restriction, but alkyl comprises verivate such as alkoxyl group and haloalkyl, is generally C 1-C 6, C more preferably 1-C 4, most preferably be C 1-C 2
As stated, carbon part L, R and R 4Can be aromatic ring or aromatic ring system (except other group).The instance of aromatic ring or aromatic ring system comprises that 8 yuan, 9 yuan or 10 yuan of phenyl ring, 5 yuan or 6 yuan of hetero-aromatic rings, aromatics condense two carbon-loop systems and aromatics condenses two heterocyclic ring systems for 8 yuan, 9 yuan or 10 yuan, and each ring or loop systems are optional in the second cycle line system is substituted.About the term of these L and R carbon part " optional replacement () " refer to that carbon part is not substituted or has at least one non-hydrogen substituting group.These carbon parts can be replaced by its optional substituting group that can hold maximum number, and the Wasserstoffatoms on its all commutable carbon or the nitrogen-atoms is replaced by non-hydrogen substituting group.Preferred optional substituting group number (when existing) is 1-4.Optional by the U-1 in the instance of 1-4 the substituted phenyl of substituting group such as the example displaying 1, wherein R vBe optional non-hydrogen substituting group, r is the integer of 0-4.The optional instance that is condensed two carbon-loop systems by 8 yuan, 9 yuan or 10 yuan of 1-4 the substituted aromatics of substituting group comprises optional by 1-4 the substituted naphthyl of substituting group, like U-85 in the example displaying 1, and chooses wantonly by 1-4 substituting group substituted 1; 2,3, the 4-tetralyl; Show U-86, wherein R in 1 like example vBe any substituting group, r is the integer of 0-4.Choose wantonly by the instance of 1-4 substituted 5 yuan or the 6 yuan hetero-aromatic rings of substituting group and comprise the ring of example displaying 1U-2 to U-53, wherein R vFor any substituting group and r are the integer of 1-4.The optional instance that is condensed two heterocyclic ring systems by 8 yuan, 9 yuan or 10 yuan of 1-4 the substituted aromatics of substituting group comprises example displaying 1U-54 to U-84, wherein R vIt for any substituting group and r 0 to 4 integer.The instance of other L and R comprises optional by 1-4 the substituted phenmethyl of substituting group, shows 1U-87 like example, and optional by 1-4 the substituted benzoyl-of substituting group, shows 1U-88, wherein R like example vBe any substituting group, r is the integer of 0-4.
Though have R at structure U-1 structural formula in the U-85 VGroup, but notice that they not necessarily exist, because they are optional substituting groups.Need substituting group to fill its valent nitrogen-atoms with H or R vTo its replacement.Notice that some U groups can only be less than 4 R vGroup replace (like U-14, U-15, U-18 can only be by a R to U-34 to U-21 and U-32 vReplace).Note as (R v) rAnd the binding site between the U is not when cannot being shown fixingly, (R v) rCan be connected in any commutable carbon atom and nitrogen-atoms on the U group.Notice that when the binding site on the U group cannot not be shown fixingly the U group can be connected in formula I and II rest part through optional attachable carbon atom on the U group through replacing Wasserstoffatoms.
Example shows 1
Figure GA20175791200910139404801D00091
Figure GA20175791200910139404801D00101
Figure GA20175791200910139404801D00111
Figure GA20175791200910139404801D00121
As stated, carbon part L, R and R 4Maybe be for (except other group) saturated or fractional saturation carbocyclic ring and heterocycle, they further are optionally substituted.Refer to that about the term of these L and R carbon part " optional substituted " carbon part is not substituted or at least one non-hydrogen substituting group arranged.These carbon parts can be replaced by its optional substituting group that can hold maximum number, and the Wasserstoffatoms on its all commutable carbon or the nitrogen-atoms is replaced by non-hydrogen substituting group.In general, optional substituting group number (when existing) is 1-4.Saturated or fractional saturation isocyclic instance comprises optional substituted C 3-C 8Naphthenic base and optional substituted C 3-C 8Naphthenic base.Saturated or fractional saturation heterocyclic instance comprises 5 yuan or 6 yuan of non-aromatic heterocyclics, its optional one or two ring integral part that comprises, this part be selected from C (=O), SO or S (O) 2, said heterocycle is optional to be substituted.The instance of such L and R carbon part comprises that G-1 is to G-35 in the example displaying 2.Notice that when the connection site on these G groups cannot not be shown fixingly the G group can through replacing Wasserstoffatoms, be connected in formula I and II rest part through optional commutable carbon or nitrogen-atoms on the G group.Said optional substituting group can be connected in any commutable carbon atom and nitrogen-atoms (said substituting group does not show that in example 2 mark, because they are optional substituting group) through replacing Wasserstoffatoms.Note comprising when being selected from G-24 Q to the ring of G-31, G-34 and G-35 as G 2Can be selected from O, S, NH or substituted N.
Example shows 2
Figure GA20175791200910139404801D00131
Note L, R and R 4Carbon part can be optional substituted.As implied above, except other group, L and R carbon part can comprise further optional by 1-4 U group or the G group that substituting group is substituted usually.Like this; L and R carbon part can comprise and be selected from U or G group and its of U-1 to U-88 or G-1 to G-35 and further replaced by other substituting group; Said substituting group comprises 1-4 U or G group (they can be identical or different), makes it have core U or G group and optional further substituted substituting group U or G group like this.It should be noted that especially to comprise and choose wantonly by 1-3 the optional substituted U group L carbon part of other substituting group.For example, L can be the U-41 group.
Shown in flow process 1, according to the method for the invention, 4 of formula II, 5-dihydro-1 h-pyrazole and HX 1Reaction forms different formula I3-halos-4,5-dihydro-1 h-pyrazole compound.
Flow process 1
Wherein L, R, X 1, X 2With the definition among k invention summary together.
Above-mentioned being reflected in the suitable solvent carried out.Reach the optimum solvent and should be non-nucleophilicity solvent, it is to HX 1The compound of relative inertness and solubilized formula II.Suitable solvent comprises methylene bromide, methylene dichloride, acetate, ETHYLE ACETATE and acetonitrile.Reaction can under atmospheric pressure or carried out near being higher than under the normal atmosphere under the normal atmosphere or in pressurized vessel.Starting raw material HX 1Can add in the reaction mixture of formula II compound and solvent with the form of gas.X in formula II compound 2During for halogen such as Cl, the HX that preferred reaction produces 2Remove through spraying or other appropriate method.In addition, can at first make starting raw material HX 1Be dissolved in its highly soluble inert solvent (for example acetate), then directly or in solution, contact with the compound of formula II.Work as X in the compound of formula II equally 2During for halogen such as Cl, need substantially exceed the HX of monovalent usually 1(like 4 to 10 equivalents), this depends on the level of conversion of expectation.Work as X 2Be OS (O) mR 1Or OP (O) p(OR 2) 2The time, the HX of monovalent 1High conversion can be provided, but when the compound of formula II contains at least one basic functionality (like nitrogen heterocyclic ring), need to surpass the HX of monovalent usually 1Reaction can be carried out between 0 to 100 ℃, most convenient be temperature (10-40 ℃ according to appointment) near surrounding environment, most preferably be about 20 to 30 ℃.Add lewis acid catalyst and (, be used to prepare formula I, wherein X like aluminum bromide 1Be Br) can promote reaction.The product of formula I separates with usual method well known to those skilled in the art, comprises extraction, distillation and crystallization.
The preferred initial compounds of the inventive method comprises formula II compound, and wherein m is 2, and p is 1.X in preferred 2Be halogen or OS (O) mR 1The formula II initial compounds of (preferably wherein m is 2) its.Further preferred initial compounds is such formula II compound: X wherein 2Be Cl or OS (O) mR 1, m is 2, R 1Be C 1-C 6Alkyl, CF 3Or optional be selected from C by 1 to 3 1-C 4The substituted phenyl of the substituting group of alkyl, more preferably R 1Be C 1-C 2Alkyl, phenyl or 4-aminomethyl phenyl.The special preferable methods of the present invention comprises uses such formula II initial compounds: X wherein 2Be Cl or OS (O) 2R 1, and R 1Be methyl, phenyl or 4-aminomethyl phenyl.In the formula II initial compounds that the special preferable methods of the present invention is used, X 2Be Cl or OS (O) 2R 1, and R 1Be phenyl or 4-aminomethyl phenyl.
The preferred product of the inventive method comprises such formula I compound: X wherein 1Be Cl, Br or I.Preferred product comprises such formula I compound: X wherein 1Be Cl or Br.Most preferred product comprises wherein X 1Formula I compound for Br.The useful especially embodiment of the inventive method comprises preparation I compound, wherein X 1Be Cl or Br, said formula I compound obtains with formula II compound, X in its Chinese style II compound 2Be OS (O) 2R 1, R wherein 1For example be methyl, phenyl or 4-aminomethyl phenyl, more preferably phenyl or 4-aminomethyl phenyl.
The preferred process of the present invention comprises such method: its Chinese style II initial compounds is formula IIa, and formula I product is formula Ia, shown in the following surface current journey 2.
Flow process 2
Figure GA20175791200910139404801D00161
X wherein 1And X 2Cotype I and II definition;
Each R 3Independent is C 1-C 4Alkyl, C 2-C 4Thiazolinyl, C 2-C 4Alkynyl, C 3-C 6Naphthenic base, C 1-C 4Haloalkyl, C 2-C 4Haloalkenyl group, C 2-C 4Halo alkynyl, C 3-C 6Halogenated cycloalkyl, halogen, CN, NO 2, C 1-C 4Alkoxyl group, C 1-C 4Halogenated alkoxy, C 1-C 4Alkylthio, C 1-C 4Alkyl sulphinyl, C 1-C 4Alkyl sulphonyl, C 1-C 4Alkylamino, C 2-C 8Dialkyl amido, C 3-C 6Cycloalkyl amino, (C 1-C 4Alkyl) (C 3-C 6Naphthenic base) amino, C 2-C 4Alkyl-carbonyl, C 2-C 6Alkoxy carbonyl, C 2-C 6Alkyl amino-carbonyl, C 3-C 8Dialkyl amino carbonyl or C 3-C 6Trialkylsilkl;
R 4Be H or optional substituted carbon part;
Z is N or CR 5
R 5Be H or R 3And
N is selected from 1 to 3 integer.
The formula Ia of those skilled in the art will appreciate that is the subclass compound of formula I, and formula IIa is the subclass compound of formula II.
Though for the method for flow process 2, the various optional substituted carbon part of having introduced in the ester of formula Ia as R 4Be useful, but common R 4For containing the group of 18 carbon atoms at most, and it is selected from alkyl, thiazolinyl and alkynyl; And phenmethyl and phenyl, each group is optional to be replaced by alkyl and halogen.R 4Most preferably be C 1-C 4Alkyl.
It should be noted that in the method shown in the flow process 2 that Z is N, n is 1, R 3For Cl or Br and on 3.It should be noted that the method shown in the flow process 2 equally, wherein X 2Be halogen or OS (O) 2R 1, preferred R 1Be methyl, phenyl or 4-aminomethyl phenyl.It should be noted that the method shown in the flow process 2 equally, wherein X 1Be Br or Cl and preferred X 1Be Br.Especially it should be noted that the method shown in the flow process 2, wherein X 1Be Br, X 2Be Cl or OS (O) mR 1, m is 2, R 1Be phenyl or 4-aminomethyl phenyl.
(like Z is N and/or R in formula IIa compound, to have basic functionality 3Be alkylamino, dialkyl amido, cycloalkyl amino or (alkyl) (naphthenic base) amino) time, the typical case needs to surpass the HX of monovalent 1Reaching satisfied transformation efficiency, though this moment X 2Be OS (O) mR 1Or OP (O) p(OR 2) 2Z is N in formula IIa, R 3Not alkylamino, dialkyl amido, cycloalkyl amino or (alkyl) (naphthenic base) amino, and X 2Be S (O) 2R 1The time, use as few as 1.5 to 2 normal HX 1Can reach splendid transformation efficiency.
X wherein 2For the formula II initial compounds of halogen can be from corresponding formula 1 compound, shown in flow process 3.
Flow process 3
Figure GA20175791200910139404801D00171
X wherein 2Be halogen, L, R and k ditto define.
The compound of formula 1 is handled with halide reagent, in solvent, obtained corresponding formula II halogenated compound usually.The available halide reagent comprises phosphoryl halogen, phosphorus trihalide, phosphorus pentahalides, THIONYL CHLORIDE 97, dihalo trialkyl phosphorane, dihalo phenylbenzene phosphorane, oxalyl chloride, carbonyl chloride, sulfur tetrafluoride and (diethylamino) sulfur trifluoride.Be preferably phosphoryl halogen and phosphorus pentahalides.Transform for reaching fully, will use 0.33 normal phosphoryl halogen (mol ratio that is phosphoryl halogen and formula 1 is at least 0.33) at least with respect to formula 1 compound, preferably between 0.33 and 1.2 equivalents.Transform for reaching fully, will use 0.20 normal phosphorus pentahalides at least with respect to formula 1 compound, preferably between 0.20 and 1.0 equivalents.The typical solvent of this halogenating reaction comprises halogenated alkane such as methylene dichloride, chloroform, chlorobutane and analogue; Aromatic solvent such as benzene, YLENE, chlorobenzene and analogue; Ether such as THF, P-Dioxane, diethyl ether and analogue; Polar aprotic solvent such as acetonitrile, N, dinethylformamide and analogue.Can choose the adding organic bases wantonly, like triethylamine, pyridine, N, accelerine and analogue.Also can choose the adding catalyzer wantonly, like N, dinethylformamide.Preferable methods is that solvent is acetonitrile and does not have alkali.Typically, when using acetonitrile, do not need alkali or catalyzer.The carrying out of preferred method is for sneaking into the compound of formula 1 in acetonitrile.In the suitable time, add halide reagent again, mixture is placed on the temperature of requirement and accomplishes down to reaction.The type reaction temperature is about 20 ℃ and arrives between the boiling point of acetonitrile that the type reaction time is for being less than 2 hours.Use mineral alkali such as sodium hydrogencarbonate, sodium hydroxide and analogue then, or use organic bases, like sodium acetate, the neutralization reaction material.The product that needs is that formula II compound can separate through method well-known to those having ordinary skill in the art, comprises extraction, crystallization and distillation.
Shown in flow process 4, R wherein 1Be 0S (O) mR 1Or OP (O) p(OR 2) 2Formula II initial compounds can be equally from corresponding formula 1 compound, its preparation method is to make it and X 3S (O) mR 1(2) or X 3P (O) p(OR 2) 2(3) react respectively, wherein X 3Be the nucleophilic reaction leavings group.Halogen such as Cl are to X 3Particularly useful.To X 3S (O) mR 1X equally usefully 3Be OS (O) mR 1(be that formula 2 is R 1S (O) mOS (O) mR 1); Work as R 1Be CF 3The time X 3Be OS (O) mR 1Particularly useful.From the aspect of reaction feasibility and relatively low cost, X 3For Cl is usually preferred.
Flow process 4
Figure GA20175791200910139404801D00181
X wherein 2Be OS (O) mR 1Or OP (O) p(OR 2) 2, X 3Be leavings group, L, R, R 1, k, m and p ditto define.
In the method, formula 1 compound is having in the presence of solvent or the alkali and formula 2 compound (X usually 2Be OS (O) mR 1The time) or formula 3 compound (X 2Be OP (O) p(OR 2) 2The time) reaction.Suitable solvent comprises methylene dichloride, THF, acetonitrile and analogue.Suitable alkali comprises tertiary amine (like triethylamine, N, the N-diisopropylethylamine) and ion alkali such as salt of wormwood and analogue.Preferred alkali is tertiary amine.Usually use monovalent (it is excessive slightly to be preferably, like 5-10%) formula 2 compounds or formula 3 compounds and the alkali that relates to formula 1 compound at least to transform fully.Usually be reflected at approximately-50 ℃ and under the temperature between the solvent boiling point, carry out, more preferably about 0 ℃ to (promptly about 15 to 30 ℃) between the envrionment temperature.Typical reaction was accomplished in several hours to several days; Reaction process can be used technical monitoring well-known to those having ordinary skill in the art, as thin-layer chromatography with 1The HNMR spectroscopic analysis.Reaction mixture subsequently is as with water washing, dry organic phase and evaporating solvent.Needed product is that formula II compound can separate through method well-known to those having ordinary skill in the art, comprises extraction, crystallization and distillation.
Because formula IIa is the subclass compound of formula II, formula IIa compound can pass through flow process 3 and 4 described methods, and from corresponding formula 1a compound, back one compound is the subclass compound of formula 1.
Figure GA20175791200910139404801D00191
R wherein 3, R 4, Z and n cotype IIa definition.
Formula 1 compound can be through many modern compound method methodology well-known to those having ordinary skill in the art.For example, formula 1a compound can be shown in flow process 5, from formula 4 and formula 5 compound.
Flow process 5
Figure GA20175791200910139404801D00192
R wherein 3, R 4, Z and n cotype IIa definition.
In the method, the hydrazine compound of formula 4 and formula 5 compounds (can use fumaric acid esters or maleate or their mixture) are having reaction in the presence of alkali and the solvent.Said alkali is typically metal alkoxide, like sodium methylate, potassium methylate, sodium ethylate, potassium ethylate, potassium tert.-butoxide, trimethyl carbinol lithium and analogue.Should use above 0.5 normal alkali formula 4 compounds, between the preferred 0.9-1.3 equivalent.Should use to surpass 1.0 normal formula 5 compounds, between the preferred 1.0-1.3 equivalent.Can use polar protic organic solvent and polar non-proton organic solvent, like alcohol, acetonitrile, THF, N, dinethylformamide, methyl-sulphoxide and analogue.Preferred solvent is an alcohol, like methyl alcohol and ethanol.Special alcohols is pure identical with the pure and mild alkoxide base of forming fumaric acid esters or maleate.Carry out this reaction normally mixing type 4 compounds and alkali in solvent.Mixture can be heated or cooled desired temperatures, with for some time adding formula 5 compounds.Common temperature of reaction is 0 ℃ and arrives between the boiling point of solvent for use.Reaction can be carried out under superatmospheric pressure, to improve the boiling point of solvent.Usually preferred temperature is between 30-90 ℃.The time of adding formula 5 compounds can be soon to the time of heat passage permission.Typical case's joining day is between 1 minute to 2 hours.Optimum reacting time and joining day, the compound characteristic was different changes according to formula 4 and formula 5.After the adding, reaction mixture remains on following for some time of temperature of reaction.According to temperature of reaction, the required hold-time possibly be 0 to 2 hour.Usually the hold-time is 10 to 60 minutes.Pass through then to add organic acid, like acetate and analogue, or mineral acid, example hydrochloric acid, sulfuric acid and analogue, acidification reaction material.According to reaction conditions and separate mode, on the formula 1a compound-CO 2R 4Functional group can be hydrolyzed to-CO 2H; For example, exist water can promote this hydrolysis in the reaction mass.If form carboxylic acid (CO 2H), can adopt esterification process well known in the art, make that carboxyl is reverse to be converted into-CO 2R 4, R wherein 4For example be C 1-C 4Alkyl.Needed product is that formula 1a compound can separate through method well-known to those having ordinary skill in the art, like crystallization, extraction or distillation.
Can think, utilize description those skilled in the art of front can farthest utilize the present invention.Therefore, embodiment subsequently only is illustrative, and limits the disclosure of invention never in any form.Step in following examples has been explained the per step program in the whole synthetic method for transformation, and the starting raw material in per step can be through the specific preparing method's preparation described in other embodiment or the step.Except the chromatography solvent mixture or have in addition the explanation, per-cent is weight percentage.Except as otherwise noted, the part of chromatography solvent mixture or per-cent are volume percent. 1The HNMR spectral representation is the downfield ppm of tetramethyl-silicomethane; " s " expression is unimodal, and " d " expression is bimodal, and " t " representes three peaks, and " q " representes four peaks, and " m " representes multiplet, and two of " dd " expressions are bimodal, and " dt " representes two three peaks, and " br s " expression is wide unimodal.
Embodiment 1
Through replace the chlorine preparation with bromine
3-bromo-1-(3-chloro-2-pyridyl)-4,5-dihydro-1 h-pyrazole-5-ethyl formate
Steps A: preparation 2-(3-chloro-2-pyridyl)-5-oxo-3-pyrazolidine-ethyl formate
In the 2-L that mechanical stirring device, TM, addition funnel, reflux exchanger and nitrogen inlet are housed four neck flasks, add straight alcohol (250mL) and sodium ethylate ethanolic soln (21%, 190mL, 0.504mol).Mixture is heated to backflow under about 83 ℃.(68.0g 0.474mol) handles to use 3-chloro-2 (1H)-pyridone hydrazone then.The mixture reheat refluxed about 5 minutes.Yellow slurry drips diethyl maleate again, and (88.0mL 0.544mol) handled about 5 minutes.Return velocity obviously increases in the adding method.All starting raw materials dissolve when adding completion.The gained orange-red solution keeps refluxing about 10 minutes.After being cooled to 65 ℃, reaction mixture with glacial acetic acid handle (50.0mL, 0.873mol).Form deposition.Mixture water (650mL) dilution makes resolution of precipitate.Orange solution cools off in ice bath.Product begins deposition in the time of 28 ℃.Slurry was 2 ℃ of held 2 hours.Product is through filtering separation, with aqueous ethanolic solution (40%, 3 * 50mL) washs, and on filter about 1 hour of dry air.The title product that obtains is the bright orange powder (70.3g, 55% productive rate) of highly crystalline. 1HNMR does not observe tangible impurity.
1H?NMR(DMSO-d 6)δ1.22(t,3H),2.35(d,1H),2.91(dd,1H),4.20(q,2H),4.84(d,1H),7.20(dd,1H),7.92(d,1H),8.27(d,1H),10.18(s,1H)。
Step B: preparation 3-chloro-1-(3-chloro-2-pyridyl)-4,5-dihydro-1 h-pyrazole-5-ethyl formate
In the 2-L that mechanical stirring device, TM, reflux exchanger and nitrogen inlet are housed four neck flasks, add acetonitrile (1000mL), 2-(3-chloro-2-pyridyl)-5-oxo-3-pyrazolidine ethyl formate (being the product of steps A) (91.0g; 0.337mol) and phosphoryl chloride (35~mL, 0.375mol).When adding phosphoryl chloride, mixture is heated to 25C and forms deposition from 22C self.The glassy yellow slurry was heated to 83 ℃ of refluxed 35 minutes, and deposition is dissolving therefore.The gained orange solution keeps refluxing 45 minutes, thereby becomes blackish green.Replace reflux exchanger with still head, the 650mL solvent is removed in distillation.In second 2-L four neck flask that mechanical stirring device is housed, add sodium hydrogencarbonate (130g, 1.55mol) and water (400mL).Spissated reaction mixture joined in the sodium hydrogencarbonate slurry with 15 minutes.The two-phase mixture vigorous stirring of gained 20 minutes stops venting this moment.Mixture stirred 50 minutes with methylene dichloride (250mL) dilution then.Mixture is handled with 545 super-cells (11g), removes by filter the isolating black gunk of inhibitory phase.Because filtrating knows that phase-splitting is slow; With methylene dichloride (200mL) and water (200mL) dilution, use more
Figure GA20175791200910139404801D00222
545 (15g) to handle again it.Filtering mixt, filtrating is transferred to separating funnel.Separate heavier deep green organic layer.Again filter debris layer (rag layer) (50mL) and add organic phase.This organic solution (800mL) is handled slurry magnetic agitation 30 minutes with Tai-Ace S 150 (30g) and silica gel (12g).Filter slurry, remove Tai-Ace S 150 and silica gel, solution becomes dark blue-green.Filter cake washs with methylene dichloride (100mL).Filtrating concentrates with Rotary Evaporators.Product is a stantienite look oil (92.0g, 93% productive rate). 1The observable impurity of HNMR only has 1% starting raw material and 0.7% acetonitrile.
1HNMR(DMSO-d6)δ1.15(t,3H),3.26(dd,1H),3.58(dd,1H),4.11(q,2H),5.25(dd,1H),7.00(dd,1H),7.84(d,1H),8.12(d,1H)。
Step C: preparation 3-bromo-1-(3-chloro-2-pyridyl)-4,5-dihydro-1 h-pyrazole-5-ethyl formate
To 3-chloro-1-(3-chloro-2-pyridyl)-4, (8.45g feeds hydrogen bromide in methylene bromide 29.3mmol) (85mL) solution to 5-dihydro-1 h-pyrazole-5-ethyl formate (being the product of step B).Stop air-flow after 90 minutes, reaction mixture washs with sodium bicarbonate aqueous solution (100mL).Dry and reduction vaporization organic phase obtains oily title product (9.7g, 99% productive rate), and product leaves standstill crystallization.
1H NMR (CDCl 3) δ 1.19 (t, 3H), 3.24 (in the ABX system 1/2 of AB, J=9.3,17.3Hz, 1H), 3.44 (in the ABX system 1/2 of AB; J=11.7,17.3Hz, 1H), 4.18 (q, 2H), 5.25 (the X part among the ABX, 1H; J=9.3,11.9Hz), 6.85 (dd, J=4.7,7.7Hz, 1H), 7.65 (dd; J=1.6,7.8Hz, 1H), 8.07 (dd, J=1.6,4.8Hz, 1H).
Embodiment 2
Through replace the preparation of toluenesulphonic acids base with bromine
3-bromo-1-(3-chloro-2-pyridyl)-4,5-dihydro-1 h-pyrazole-5-ethyl formate
Steps A: preparation 1-(3-chloro-2-pyridyl)-4,5-. dihydro-3-[[(4-aminomethyl phenyl) alkylsulfonyl] oxygen base]-1H-pyrazoles-5-ethyl formate
Under 0 ℃; To 2-(3-chloro-2-pyridyl)-5-oxo-3-pyrazolidine ethyl formate (being the product of embodiment 1 steps A) (10.0g; 37.1mmol) and Tosyl chloride (7.07g, 37.1mmol) drip in the mixture in methylene dichloride (100mL) triethylamine (3.75g, 37.1mmol).Add once more Tosyl chloride (0.35g, 1.83mmol) and triethylamine (0.19g, 1.88mmol).Make reaction mixture rise to room temperature and stirred overnight then.Mixture is used methylene dichloride (200mL) dilution and again with water washing (3 * 70mL).Drying is also evaporated organic phase, stays oily title product (13.7g, 87% productive rate), and product slowly forms crystallization.With the product of ethyl acetate/hexane recrystallization in 99.5-100 ℃ of fusion.
IR(nujol):1740,1638,1576,1446,1343,1296,1228,1191,1178,1084,1027,948,969,868,845cm -1
1HNMR (CDC 13) δ 1.19 (t, 3H), 2.45 (s, 3H), 3.12 (in the ABX system 1/2 of AB, J=17.3,9Hz, 1H), 3.33 (in the ABX system 1/2 of AB; J=17.5,11.8Hz, 1H), 4.16 (q, 2H), 5.72 (the X part among the ABX, J=9,11.8Hz, 1H); 6.79 (dd, J=4.6,7.7Hz, 1H), 7.36 (d, J=8.4Hz, 2H), 7.56 (dd, J=1.6; 7.8Hz, 1H), 7.95 (d, J=8.4Hz, 2H), 8.01 (dd, J=1.4,4.6Hz, 1H).
Step B: preparation 3-bromo-1-(3-chloro-2-pyridyl)-4,5-dihydro-1 h-pyrazole-5-ethyl formate
To 1-(3-chloro-2-pyridyl)-4, [[(4-aminomethyl phenyl) alkylsulfonyl] oxygen base]-(5g feeds hydrogen bromide in methylene bromide 11.8mmol) (50mL) solution to 1H-pyrazoles-5-ethyl formate (being the product of steps A) to 5-dihydro-3-.Air-flow stops after 60 minutes, and reaction mixture washs with sodium bicarbonate aqueous solution (50mL).Dry and reduction vaporization organic phase obtains oily title product (3.92g, 100% productive rate), and product leaves standstill crystallization.Product 1HNMR spectrum is identical with embodiment 1 step C product.
Embodiment 3
Through preparing with bromine substituted benzenesulfonic acid base
3-bromo-1-(3-chloro-2-pyridyl)-4,5-dihydro-1 h-pyrazole-5-ethyl formate
Steps A: preparation 1-(3-chloro-2-pyridyl)-4,5-dihydro-3-[(phenyl sulfonyl) oxo]-1H-pyrazoles-5-ethyl formate
Under 0 ℃; With 1 hour to 2-(3-chloro-2-pyridyl)-5-oxo-3-pyrazolidine ethyl formate (being embodiment 1, the product of steps A) (5.0g, 18.5mmol) and benzene sulfonyl chloride (3.27g; 18.5mmol) drip in the mixture in methylene dichloride (20mL) triethylamine (1.85g, 18.5mmol).Temperature does not allow above 1 ℃.Continued stirred reaction mixture 2 hours, add again benzene sulfonyl chloride (0.5g, 1.85mmol).(0.187g is 1.85mmol) to mixture further to drip triethylamine again.Restir 0.5 hour, mixture distribute between water (100mL) and methylene dichloride (100mL).Dry (MgSO 4) and evaporate organic layer, obtain orange solids title product (7.18g, 94% productive rate).With the product of ethyl acetate/hexane recrystallization in 84-85 ℃ of fusion.
IR(nujol):1737,1639,1576,1448,1385,1346,1302,1233,1211,1188,1176,1088,1032,944,910,868,846cm -1
1H NMR (CDCl 3) δ 1.19 (t, 3H), 3.15 (in the ABX system 1/2 of AB, J=8.8,17.3Hz, 1H), 3.36 (in the ABX system 1/2 of AB, J=11.8; 17.3Hz, 1H), 4.17 (q, 2H), 5.23 (the X part of ABX, J=8.8,11.8Hz, 1H); 6.78 (dd, J=2.8,4.8Hz, 1H), 7.71-7.55 (m, 4H), 8.01 (dd; J=1.6,4.6Hz, 2H), 8.08 (dd, J=1.0,2.6Hz, 2H).
Step B: preparation 3-bromo-1-(3-chloro-2-pyridyl)-4,5-dihydro-1 h-pyrazole-5-ethyl formate
With 1-(3-chloro-2-pyridyl)-4,5-dihydro-3-[(phenyl sulfonyl) oxygen base]-1H-pyrazoles-5-ethyl formate (being the product of steps A) (1.0g, and the acetic acid soln of acetic acid soln 2.44mmol) (4mL) adding hydrogen bromide (33%, 1.2g, 4.89mmol).After about 1 hour reaction mixture is added in the saturated sodium bicarbonate aqueous solution (100mL).Mixture with ethyl acetate extraction (2 * 50mL), dry (MgSO 4) and evaporation merging extract, obtain oily title product (0.69g, 85% productive rate), the slow crystallization of product. 1HNMR spectrum is identical with the product of embodiment 1 step C.
Combine with method well known in the art through methods described herein, formula II compound can be converted into formula I compound, like the formula Ia that lists in the table 1 and the explanation of formula IIa.That uses in the table is abbreviated as: t is uncle, and s is secondary, and n is for just, and i is different, and Me is a methyl, and Et is an ethyl, and Pr is a propyl group, and i-Pr is a sec.-propyl, and t-Bu is the tertiary butyl, and Ph is a phenyl.
Table 1
X 1Be Br; X 2Be OS (O) 2Ph
Figure GA20175791200910139404801D00262
X 1Be Br; X 2Be OS (O) 2Ph-4-Me
Figure GA20175791200910139404801D00263
X 1Be Br; X 2Be OS (O) 2Me
Figure GA20175791200910139404801D00271
X 1Be Br, X 2Be Cl
Figure GA20175791200910139404801D00272
X 1Be Cl; X 2Be OS (O) 2Ph-4-Me
Figure GA20175791200910139404801D00281
X 1Be Br; X 2Be OS (O) 2Me
Figure GA20175791200910139404801D00282
X 1Be Br
Figure GA20175791200910139404801D00283
3-halo-4 of the present invention, 5-dihydro-1 h-pyrazole preparation method can be used for preparing various formula I compounds, and these compounds are useful intermediates of the agent of preparation crop protection, medicine and other fine chemical product.Example shows that 3 have listed 3-halo-4 that can be prepared according to the methods of the invention, the instance of 5-dihydro-1 h-pyrazole, and said examples of compounds can be from having OS (O) mR 1(like OS (O) 2CH 3Or OS (O) 2Ph), OP (O) p(OR 2) 2((OMe) like OP (O) 2) or different halogenic substituent (replace Br like Cl, or Br replacing Cl) is corresponding 4, the preparation of 5-dihydro-1 h-pyrazole, useful 3-halo-4 when being included in the compound that preparation has fungicidal, weeding or plant growth regulating purposes, 5-dihydro-1 h-pyrazole.These embodiment are as the scope of explanation rather than restriction the inventive method different application.Other can be used for preparing medicinal products by compound prepared according to the methods of the invention, like anti-inflammatory agent, transformation reactions suppressor factor, anticonvulsive agent, tranquilizer etc.
Example shows 3
Figure GA20175791200910139404801D00301
Figure GA20175791200910139404801D00311
In compound that can be prepared according to the methods of the invention, formula Ia compound is particularly useful to preparation formula III compound.
Figure GA20175791200910139404801D00312
Wherein Z, X 1, R 3Ditto define with n; R 6Be CH 3, F, Cl or Br; R 7Be F, Cl, Br, I or CF 3R 8aBe C 1-C 4Alkyl; R 8bBe H or CH 3Preferred Z is N, and n is 1, R 3For Cl or Br and on 3.
The formula III compound is useful during as sterilant; The U.S. Patent application of for example applying for 60/324 referring to September 27 calendar year 2001 disclosed PCT publication number WO 01/70671 and September 21 calendar year 2001; 173; The U.S. Patent application 60/369,661 of the U.S. Patent application 60/323,941 of application on September 21 calendar year 2001 and application on April 2nd, 2002.The method for preparing formula 8 and formula III compound is seen the U.S. Patent application 60/400352 [BA9308 US PRV] of application on July 31st, 2002; The U.S. Patent application 60/446438 [BA9308 US PRV1] of on February 11st, 2003 application, they by reference integral body be attached among this paper; And the U.S. Patent application 60/369,660 of application on April 2nd, 2002.
The formula III compound can be through method shown in the flow process 6-9 from corresponding formula Ia compound.
Shown in flow process 6, formula Ia compound is chosen wantonly in the presence of acid, uses oxidizer treatment.
Flow process 6
Figure GA20175791200910139404801D00321
R wherein 3, R 4, Z, X 1Definition with n cotype Ia.
Formula Ia compound is preferably as the starting raw material of this step, wherein R 4Be C 1-C 4Alkyl.Oxygenant can be hydrogen peroxide, organo-peroxide, Potassium Persulphate, Sodium Persulfate, ammonium persulfate, potassium hydrogen persulfate (like
Figure GA20175791200910139404801D00322
) or potassium permanganate.Be to transform fully, should use at least one normal oxygenant, be preferably from about one to two equivalent to the compound of formula Ia.Typical this oxidizing reaction is carried out in the presence of solvent.Solvent can be ether such as THF, P-Dioxane and analogue, organic ester such as ETHYLE ACETATE, methylcarbonate and analogue, or polar aprotic solvent such as N, dinethylformamide, acetonitrile and analogue.The acid that this oxidation step is fit to use comprises mineral acid such as sulfuric acid, phosphoric acid and analogue, organic acid such as acetate, phenylformic acid and analogue.When using acid, should use above 0.1 normal acid formula Ia compound.For transforming fully, can use one to five normal acid.To Z wherein is CR 5Formula Ia compound, preferred oxidant is that hydrogen peroxide and oxidation are preferably carried out under anacidity.To Z wherein is the formula Ia compound of N, and preferred oxidant is that Potassium Persulphate and oxidation are preferably carried out in the presence of sulfuric acid.Reaction is carried out passing through mixing type Ia compound and acid in the solvent of needs, if use acid.Add oxygenant with suitable speed subsequently.Usually temperature of reaction to obtain to accomplish the reasonable reaction time of reaction, preferably is less than 8 hours for from being low to moderate 0 ℃ of boiling point to height to solvent.The product of expectation is that formula 6 compounds can separate through method well-known to those having ordinary skill in the art, comprises extraction, chromatography, crystallization and distillation.
R in formula 6 carboxylic acid cpds 4During for H, it can be through the corresponding formula 6 ester cpds preparation of hydrolysis, wherein R 4For example be C 1-C 4Alkyl.Carbonate can be through many methods, comprise the nucleophilic cracking under the anhydrous condition or relate to the hydrolysis method of using acid or alkali (about the summary of method referring to T.W.Greene and P.G.M.Wuts, Protective Groups in OrganicSynthesis; 2nd ed., John Wiley & Sons, Inc.; New York; 1991, pp.224-269), be converted into carboxylic acid cpd.To formula 6 compounds, preferred bases catalytic hydrolysis method.Suitable alkali comprises basic metal (like lithium, sodium or potassium) oxyhydroxide.For example, ester is dissolvable in water water and pure like the alcoholic acid mixture.After with sodium hydroxide or potassium hydroxide treatment, ester is by sylvite or the sodium salt of saponification so that carboxylic acid to be provided.With strong acid example hydrochloric acid or sulfuric acid acidation, the carboxylic acid of acquisition formula 6, wherein R 4Be H.The method that this carboxylic acid can be known is by one of skill in the art separated, and comprises extraction, distillation and crystallization.
With the pyrazole carboxylic acid of formula 6, wherein R 4Be H,, obtain the benzoxazinone of formula 8 with the anthranilic acid coupling of formula 7.In flow process 7, through in the presence of tertiary amine such as triethylamine or pyridine, to R 4Add methylsulfonyl chloride successively in the pyrazole carboxylic acid for the formula 6 of H, add the anthranilic acid of formula 7 then, add tertiary amine and methylsulfonyl chloride for the second time again, directly prepare the benzoxazinone of formula 8.
Flow process 7
R wherein 3, R 6, R 7, X 1, Z and n be with the definition of formula III.
This method obtains benzoxazinone productive rate preferably usually.
Flow process 8 is described the another kind of method of preparation formula 8 benzoxazinones, relates to formula 10 pyrazoles acyl chlorides and formula 9 isatoic anhydride couplings, directly obtains formula 8 benzoxazinones.
Flow process 8
Figure GA20175791200910139404801D00342
R wherein 3, R 6, R 7, X 1, Z and n be with the definition of formula III.
For example pyridine or pyridine/acetonitrile equal solvent is fit to this reaction.The acyl chlorides of formula 10 can be through currently known methods as with THIONYL CHLORIDE 97 or oxalyl chloride chlorination, from corresponding R 4For the acid of the formula 6 of H obtains.
The compound of formula III can be through making formula 8 benzoxazinone and the C of formula 11 1-C 4Alkylamine and (C 1-C 4Alkyl) (methyl) amine prepared in reaction is shown in flow process 9.
Flow process 9
Figure GA20175791200910139404801D00351
R wherein 3, R 6, R 7, R 8a, R 8b, X 1, Z and n ditto define.
This reaction can be carried out and in various suitable solvents, carry out under solvent-free, and solvent comprises acetonitrile, THF, diethyl ether, methylene dichloride or chloroform, and best temperature of reaction is the reflux temperature from the room temperature to the solvent.Benzoxazinone and amine reaction produce generally being reflected at of anthranilamide has write up in the chemical literature.Summary about the benzoxazinone chemistry is seen Jakobsen et al., BIORGANIC AND MEDICINAL CHEMISTRY 2000,8,2095-2103 and the reference of listing thereof.Also can be referring to Coppola, J.HeterocyclicChemistry 1999,36,563-588.

Claims (7)

1. Formula Il a compound:
Figure F2009101394048C00011
Each R wherein 3Independent is C 1-C 4Alkyl, C 2-C 4Thiazolinyl, C 2-C 4Alkynyl, C 3-C 6Naphthenic base, C 1-C 4Haloalkyl, C 2-C 4Haloalkenyl group, C 2-C 4Halo alkynyl, C 3-C 6Halogenated cycloalkyl, halogen, CN, NO 2, C 1-C 4Alkoxyl group, C 1-C 4Halogenated alkoxy, C 1-C 4Alkylthio, C 1-C 4Alkyl sulphinyl, C 1-C 4Alkyl sulphonyl, C 1-C 4Alkylamino, C 2-C 8Dialkyl amido, C 3-C 6Cycloalkyl amino, (C 1-C 4Alkyl) (C 3-C 6Naphthenic base) amino, C 2-C 4Alkyl-carbonyl, C 2-C 6Alkoxy carbonyl, C 2-C 6Alkyl amino-carbonyl, C 3-C 8Dialkyl amino carbonyl or C 3-C 6Trialkylsilkl;
R 4Be H or C 1-C 4Alkyl;
X 2Be OS (O) mR 1
M is 1 or 2;
R 1Be selected from C 1-C 2Alkyl, phenyl or 4-aminomethyl phenyl;
Z is N or CR 5
R 5Be H or R 3And
N is the integer of 1-3.
2. the compound of claim 1, wherein R 4Be C 1-C 4Alkyl.
3. the compound of claim 2, wherein Z is N, n is 1, R 3For Cl or Br and on 3.
4. the compound of claim 3, wherein m is 2, R 1Be phenyl or 4-aminomethyl phenyl.
5. the compound of claim 4, wherein R 4Be ethyl, R 3Be Cl and R 1Be phenyl.
6. the compound of claim 4, wherein R 4Be ethyl, R 3Be Cl and R 1Be the 4-aminomethyl phenyl.
7. the compound of claim 1, wherein Z is N, R 4Be ethyl, R 3Be 3-Cl and X 2Be OS (O) 2Ph or OS (O) 2Ph-4-Me.
CN2009101394048A 2002-07-31 2003-07-29 Intermediate for preparing 3-halo-4,5-dihydro-1h-pyrazoles Expired - Lifetime CN101607957B (en)

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