• 专利附录
  • 专利说明
  • 权利要求
  • 类似技术
  • 同族专利
  • 引用文献
  • 法律状态
  • 优先权
    • 专利摘要:
    A process for preparing 10-methyl-2,9-dioxatricyclo[4,3,1,03,7] decane derivatives is disclosed, wherein a 10-methylen-3-iodomethyl compound of the formula <IMAGE> is hydrogenated to obtain a mixture of the corresponding epimeric 10 beta - and 10 alpha -methyl-3-iodomethyl compounds, the pure 10 alpha - and 10 beta -methyl epimers are separated and recovered from this mixture and are reacted with a secondary amine. Optionally, the substituent in the 4-position of the resulting 10 alpha - or 10 beta -methyl-3-aminomethyl compounds are further changed.
    公开号:SU724084A3
    申请号:SU772511707
    申请日:1977-08-19
    公开日:1980-03-25
    发明作者:Асаи Акийи;БАН Иван;Давид Самуэль;Виллиброрд Тис Петер
    申请人:Кали-Хеми Фарма Гмбх (Фирма);
    IPC主号:
    专利说明:

    -2, 9-dioxatricyclo (4, 3, 1,) decane of the general formula
    3
    OCOCHj
    where Rj and RJ have the indicated meanings,
    subjected to catalytic hydrogenation with hydrogen in the presence of platinum oxide in an organic solvent medium, followed by separation of the reaction mixture from a 10-methyl derivative of a compound of general formula 1a with crystallization and a 10-methyl derivative of a compound of general formula 16 by chromatography of residue obtained from crystallization solution
    and each of the isomers obtained. subjected to amination with piperidine in the presence of sodium bicarbonate at boiling followed by isolation of the target product in free form or in the form of a salt.
    As the organic solvent, it is preferable to use acetoacetic ester, methanol, ethanol or propanol.
    The crystallization of the 10-methyl derivative of the compound of general formula 1a is preferably carried out from methanol after separation of the catalyst. The crystal from the atom is then recrystallized several times from methanol. The AU-Methyl derivative of the compound of general formula 16 is separated from the crystallization mother liquor, which is evaporated to dryness, and the residue is taken up in ether / hexane (1: 9) and chromatographed on silica gel.
    Example. Preparation of 3-piperidinomethyl-4, 8-oxy-8-methoxy-10P n -methyl-2, 9-dirxatricyclo (4, 3, 1, O) decanhydrohydrogen tartrate.
    A. Preparation of 3-iodomethyl-4-acetoxy-8-methoxy-10, b-methyl-2, 9-dioxatricyclo (4, 3, 1.0) decane.
    A solution of 800 g of 3-iodomethyl-4-acetoxy-8-methoxy-10-methylene-2, 9-diox satricyclo (4, 3, 1, O) on 3 acetoacetic ester is added to a suspension of 35 g of pre-hydrogenated platinum oxide in 300 ml of ethyl ether. Hydrogenation is carried out at room temperature and normal pressure. At first, hydrogen is absorbed very quickly, it runs very slowly under the end. After absorbing the theoretical amount of hydrogen (47.2 L)
    the reaction mixture is filtered under nitrogen through asbestos. After evaporation, 804 g of crude product is obtained (100% of the theoretical). After repeated recrystallization from methanol, 542 pure 10-methyl derivative was isolated (67% of the theoretical). The general formula is CjjHiqOOj, mol. at. 382, 19, m.p. 129С, + 24,5 ° (CHjOH).
    B. Preparation of 3-piperidine6methyl-4, L-oxy-8-methoxy-10 P-methyl-2, 9-dioxatricyclo- (4,3,1,) decane.
    54 g of NaHCOj are suspended in a solution of 191 g of 3-iodomethyl-4-acetoxy-8-methoxy-1O ft-methyl-2, 9-dioxatricyclo (4, 3, 1, O) decane in 250 ml of piperidine. The suspension is boiled with vigorous stirring under reflux. Light liquid (reaction mixture) for. 30 minutes turns into a viscous, yellow-colored gruel. At the end of the amination (about 4-5 hours), the reaction mixture, cooled to room temperature, is transferred to 500 ml of water, mixed with 20.0 ml of 30% sodium alkali and extracted four times in 400 ml portions of ether. The combined organic phases are dried, clarified with activated carbon and evaporated in vacuo.
    The crude product is purified through silica gel with a mixture of n-hexane / diethylamine yield 146, 2 g (98.3% of theoretical). The general formula is С ij, Н N0, mol.v. 297.4, mp. 60-61 ° C (recrystallization from petrol, ester ether); 6, 8 ° (CHjOH).
    B. Preparation of 3-piperidinomethyl-4J. Hydroxy-8-methoxy-10A-methyl-2, 9-dioxatricyclo- (4,3,1,0) decane-hydrogen de-arthrate.
    146.2 g of 3-piperidinome.yl-4, ft-ca-8-methoxy-10 j-methyl-2, 9-dioxatricyl (4, 3, 1, O -) dec-ana is dissolved in 50 mL of ethanol and mixed with a solution of 72 g of L (+) tartaric acid in 1500 ml of ethanol with vigorous stirring. After precipitation occurs, it is stirred for another 1 hour at 0 ° C, filtered and the precipitate is washed with cold ethanol. The substance is dried in vacuum at 60 ° C, yield 213 g (95% of the theoretical). The general formula is С 20 И 33 NO, р, mol. at. 447.46, mp. l83.C, 6.5 (N.O.), G ° -11.6 ° (CHjOH) .2 g
    PRI mme R 2. Preparation of 3-piperidinomethyl-4 -Hxy-8-methoxy-104 -methyl-2, 9-dioxatricyclo (4.3.1, O) decanhydrohydrogen tartrate.
    A. - Isolation of 3-iodomethyl-4 p-acetoxy-8-methoxy-1 O-methyl-2, 9-dioxtricyclo (4,3,1, O) decane.
    The 3-iodomethyl-4 pi-acetoxy-8-methoxy-10 B-methyl-2, 9-dioxatricyclo (4, 3, 1., 0) decane from Example 1A combined methanol mother liquor was evaporated. The residue, 250 g of red-brown oil, is dissolved in 700 ml of methanol and left to stand for 24 hours at 0 ° C, while the residual product crystallizes out. The filtered crystallisate (120 g) contains about 10% 10 (h-methyl derivative identified by NMR. These 120 g of crystallized material are not subjected to further processing.
    The filtrate is evaporated and the residue (130 g of a red-brown oil) is purified on a chromatographic column, passing through a 25-fold amount of silica gel, with ether / hexane (1: 9) as an elution liquid. Separate fractions are tested for purity through DS. After combining and subsequent evaporation, 80 g of a light, yellow oil are obtained. This oil is dissolved in water / acetone (1: 9). The saturated solution is cooled before and, adding a crystal, causes crystallization. After washing twice, 53 g of the desired epimer of the desired product are recovered. General formula mol. at. 382.19, mp 60-65 ° C, 1, ° + 28.5 (CHjOH).
    B. Preparation of 3-piperidinomethyl-4fe-oxy-8-methoxy-10-methyl-2,9-. -dioxatricyclo (4,3,1, -) decane.
    Amination of 3-iodomethyl.-4 and-acetoxy-8-methoxy-1 About d, -methyl-2, 9-di. Oxatricyclo (4, 3, 1, O) of dean was carried out by the method described in Example 1B, yield 40.8 f (99% of the theoretical). General formula C,
    m.p. 0 ° C, 7.5 mol.v. 297.4 (CHjOH).
    B. Preparation of acidic 3-piperidinomethyl-4-hydroxy-8-methox-10 ok-methyl-2, 9-dioxatricyclo (4,3,1,) decane tartrate. A solution of 40 g of 3-piperidinomethyl-4-hydroxy-8-methoxy-1O-methyl-2.9. Dioxatricyclo (4, 3, 1) decane 150 ml of ethanol is mixed with vigorous stirring dropwise with a solution of 20 g L (+ ) tartaric acid in 400 ml of ethanol. After the addition is complete, the reaction mixture is stirred at 0 ° C for 1 h, then filtered and the precipitate is washed with cold ethanol. The crystallisate is dried in a vacuum drying oven at a yield of 57 g (95% of the theoretical). The general formula is CaoH3H SCO mol. at. 44 7 46, m.p. 182-185 ° С, - 11.9 ° (CHjOH
    权利要求:
    Claims (4)
    [1]
     1. Method for preparing 10 P -methyls or 10 -methyl-2,9-dioxatricyclo (4,3,1,) decans of the general formula
    or
    CIS-R,
    .И1 | Н
    he (16)
    where R is piperidyl;
    one of the radicals Rj is a hydrogen atom, and the other methoxy group, or their salts, characterized in that 3-iodomethyl-4 / -acetoxy-1O-methylene-2, 9-dioxatricyclo (4,3,1,) decane of the general formula
    0
    .3
    five
    9 CHz-J
    illlllH
    bcocH}
    where R have the indicated meanings, is subjected to catalytic hydrogenation with hydrogen, in the presence of platinum oxide in the medium of organic solvent, followed by extraction from the reaction mixture
    10 ft -methyl derivative of the compound of general formula 1a by crystallization and
    Q 10 a sc-methyl derivative of the compound of general formula 16 by chromatography of the residues obtained from crystallization mother liquors,
    and each of the resulting isomers e is subjected to amination with piperidine in the presence of sodium bicarbonate at boiling, followed by a recovery of the desired product in free form or as a salt.
    [2]
    2. Method POP.1, distinguished by 60 y and with the fact that acetoacetic ether, methanol, and ethanol are used as the organic solvent
    or propanol.
    [3]
    3. The method according to claim 1, about t and h and y and y so that the crystallization of the iop-methyl derivative of the compound of general formula 1a is carried out in methanol. .
    [4]
    4. The method according to claim 1, is distinguished by the fact that chromatography 10 (i-methyl derivative of compound of general formula 16 is carried out on silica gel ether / hexane. Sources of information taken into account in the examination of i. USSR patent for application no. 2455502/23-04, class C 07 D 493/08, 02.21.76.
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    同族专利:
    公开号 | 公开日
    NO771806L|1978-11-07|
    US4182889A|1980-01-08|
    FR2389628B2|1981-01-23|
    IE45756L|1978-11-04|
    IE45756B1|1982-11-17|
    BE857981R|1978-02-20|
    ES461131A2|1978-06-01|
    GB1581263A|1980-12-10|
    DE2719916C2|1987-03-19|
    DE2719916A1|1978-11-09|
    PH15677A|1983-03-11|
    ATA554377A|1979-02-15|
    JPS6160078B2|1986-12-19|
    AU512406B2|1980-10-09|
    FI772488A|1978-11-05|
    NO146360B|1982-06-07|
    ZA774753B|1978-06-28|
    DK273977A|1978-11-05|
    NO146360C|1982-09-15|
    SE7709317L|1978-11-05|
    AU2779477A|1979-02-15|
    AT352139B|1979-09-10|
    DD132871A6|1978-11-15|
    SE439310B|1985-06-10|
    GR70658B|1982-12-03|
    NL7706640A|1978-11-07|
    CH638213A5|1983-09-15|
    MX4851E|1982-11-01|
    FR2389628A2|1978-12-01|
    JPS53137995A|1978-12-01|
    JPS61197584A|1986-09-01|
    CA1130300A|1982-08-24|
    引用文献:
    公开号 | 申请日 | 公开日 | 申请人 | 专利标题
    US3812154A|1969-12-08|1974-05-21|Kali Chemie Ag|Dioxatricyclodecanes|
    DE2129507C3|1971-06-15|1980-02-14|Kali-Chemie Ag, 3000 Hannover|Process for the preparation of 8-alkoxy-3halomethyl-4-acetoxy-10-methylene-2,9dioxatricyclo decanes|
    FI56533C|1973-02-08|1980-02-11|Kali Chemie Pharma Gmbh|SAETT ATT FRAMSTAELLA NYA 4ALPH CARBAMYLOXY-8-ALCOXY-10-METHYLENE-3-METHYL-2,9-DIOXATRICYCLO -DECANER|DE2547205C2|1975-10-22|1983-12-08|Kali-Chemie Pharma Gmbh, 3000 Hannover|2,9-Dioxatricyclo [4,3,1,0 → 3 → →, → → 7 →] decane and process for their preparation|
    DE3335827A1|1983-10-01|1985-04-18|Kali-Chemie Pharma Gmbh, 3000 Hannover|NEW 2,6-DIOXA-BICYCLO--OCTAN-7-YL- ACETALDEHYDE|
    DE3335826A1|1983-10-01|1985-04-18|Kali-Chemie Pharma Gmbh, 3000 Hannover|NEW N-3, 8 )) - UNDECANE -5-YL) -TRYPTAMINE DERIVATIVES|
    SE510643C2|1997-06-27|1999-06-14|Astra Ab|Thermodynamically stable omeprazole sodium form B|
    DE10130145A1|2001-06-22|2003-01-02|Wella Ag|Cationic dyes, processes for their preparation and colorants containing these compounds|
    法律状态:
    优先权:
    申请号 | 申请日 | 专利标题
    DE2719916A|DE2719916C2|1977-05-04|1977-05-04|
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