CN1270955A - Preparation of 1,5-di-o-coffeic acyl quininic acid derivative - Google Patents

Preparation of 1,5-di-o-coffeic acyl quininic acid derivative Download PDF

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CN1270955A
CN1270955A CN 99105113 CN99105113A CN1270955A CN 1270955 A CN1270955 A CN 1270955A CN 99105113 CN99105113 CN 99105113 CN 99105113 A CN99105113 A CN 99105113A CN 1270955 A CN1270955 A CN 1270955A
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CN1093529C (en
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董俊兴
金文涛
许天林
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Institute of Radiation Medicine of CAMMS
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Abstract

The present invention relates to the preparation of 1,5-di-o-coffeic acyl quininic acid derivative, especially 1,5-di-o-coffeic acyl quininic acid.

Description

1, the preparation method of 5-two-O-coffeic acyl quininic acid derivative
The present invention relates to 1,5-two-O-coffeic acyl quininic acid derivative, especially 1, the preparation method of 5-two-O-caffeoylquinic acids.
Coffee mesitoyl quinine acid compounds extensively exists in the plants such as herbal medicine, fruit, vegetables.They have antiviral, antitumor, multiple biological activity such as protection liver etc.We discover, di-coffee mesitoyl quinine acid compounds, and particularly 1,5-two-O-caffeoylquinic acids, and derivative has significant inhibitory effect to hepatitis B virus (HBV) and virus of AIDS (HIV).But present dicaffeoylquinic acid derivative, especially 1, the source of 5-two-O-caffeoylquinic acids is also mainly by plant extract, and dicaffeoylquinic acid is lower in plant content.In addition, though also have at present the report 1, the chemical synthesis process of 5-two-O-coffeic acyl quininic acid derivative, by this method obtain 1, the synthetic yield of 5-two-O-caffeoylquinic acids is very low.Therefore, seek new preparation 1, the preparation method of 5-O-coffeic acyl quininic acid derivative is very necessary.
The purpose of this invention is to provide 1,5-two-O-coffeic acyl quininic acid derivative, especially 1, the preparation method of 5-two-O-caffeoylquinic acids.
The present invention relates to formula I1, the preparation method of 5-two-O-coffeic acyl quininic acid derivative:
Figure A9910511300051
Wherein: R 1And R 2Can be identical or different, represent hydrogen, C 1-6Alkyl, C nH 2n-1CO or R 1And R 2Lump together expression-CH 2-;
R 3Expression hydrogen, C 1-6Alkyl, benzyl or basic metal or alkaline-earth metal;
R 4And R 6Can be identical or different, be respectively H or coffee acyl;
N is the integer of 1-6; This method comprises:
1) with formula II compound, wherein R 1' and R 2' can be identical or different, represent C nH 2n-1OCO, C nH 2n-1CO or R 1' and R 2' lump together expression-CO-,-CCl 2-; X is a halogen;
With the reaction of formula III compound,
R wherein 3' represent H, C 1-6Alkyl, benzyl or basic metal or alkaline-earth metal; R 4' and R 5' can be identical or different, represent H, C 1-6Alkyl or C 6-10Aryl or R 4' and R 5' represent C with adjacent carbon atom 3-7Carbocyclic ring is as-(CH 2) 5-; Production IV compound, wherein, R 1', R 2', R 3', R 4' and R 5' as above definition; With
Figure A9910511300063
2) with 1) in obtain formula IV compound hydrolysis.
Used in the present invention term " basic metal " is meant Li, Na or K.
Used in the present invention term " alkaline-earth metal " is meant Mg, Ca, Ba etc.
Used in the present invention term " halogen " is meant chlorine, bromine, fluorine or iodine.
Term " C 1-6Alkyl " be meant the straight or branched alkyl that contains 1-6 carbon atom, as methyl, ethyl, propyl group, sec.-propyl, butyl, isobutyl-, the tertiary butyl, amyl group, neo-pentyl, hexyl etc.
Say that more specifically according to the present invention 1, the preparation of 5-two-O-coffeic acyl quininic acid derivative can prepare by the reaction scheme shown in following:
Figure A9910511300071
Wherein in step 1,
Formula II compound and the reaction of formula III compound are to follow under the stirring, in the alkali existence or not, under the decompression, are 50-160 ℃ in temperature, and the reaction times is to carry out under 10-60 minute.Wherein used alkali is selected from organic bases or mineral alkali, as BaCO 3, K 2CO 3, Na 2CO 3, NaHCO 3, KHCO 3Deng.
Or the reaction of formula II compound and formula III compound is following under the stirring, in organic solvent, in the presence of alkali, in-4 ℃ to 100 ℃, reaction times is to carry out in 1-48 hour, and wherein organic solvent is selected from pyridine, triethylamine, dimethyl formamide, methyl-sulphoxide, methylene dichloride, trichloromethane, benzene, toluene, acetonitrile, propionitrile etc., alkali is selected from organic bases or mineral alkali, as pyridine, and diamino-pyridine, triethylamine, K 2CO 3, Na 2CO 3, KHCO 3, NaHCO 3Deng.
In step 2,
Formula IV compound can be used rare organic acid such as acetic acid,diluted or diluted mineral acid such as dilute hydrochloric acid earlier, uses dilute alkaline soln subsequently, as NaHCO 3, Na 2CO 3, KHCO 3, K 2CO 3, NaOH etc., hydrolysis.
According to the present invention, preferably make 1 of following formula representative, 5-two-O-caffeoylquinic acids (being called for short compd A later on) by the inventive method:
Figure A9910511300081
By following embodiment the present invention is explained in further detail, but should be understood that these embodiment and do not mean that any restriction the present invention.Synthesizing of embodiment 1. compd As
With 449mg 3,4-O-carbonyl coffee acyl chlorides and 254mg 3,4-O-isopropylidene quininic acid sodium fully grinds evenly, add in the flask, under vacuum decompression, in oil bath, be heated to 100 ℃ earlier, slowly rise to 140 ℃ then, heat and under vacuum state, be cooled to room temperature after 20 minutes.Reaction product adds 5,0m1 80% acetate and heated in boiling water bath 30 minutes, removes solvent under reduced pressure.(elutriant is CHCl3-MeOH-H to the about 800mg of residue with the silica gel column chromatography separation 2O, 90: 35: 6), get the about 450mg of compd A.FAB-MS:m/z609,499,355,337,193,163;EI-MS:m/z354,336,180,163。 1H-NMR:δ19.6(dd),2.36(dd),2.48(dd),2.50(dd),3.75(ddd),4.24(ddd),5.37(ddd),6.20(d),6.25(d),6.80(d),6.81(d),6.96(dd),6.97(dd),7.11(d),7.13(d),7.50(d),7.53(d); 13C-NMR:δ35.4,37.3,69.4,71.3,72.9,80.6,115.4,115.9,116.3,116.7,123.1,127.8,146.6,146.7,146.8,149.3,166.9,167.6。Synthesizing of embodiment 2. compd As
With 449mg 3,4-O-carbonyl coffee acyl chlorides and 254mg 3,4-O-isopropylidene quininic acid sodium and 100mg Dimethylamino pyridine (DMAP) are dissolved among the 40ml DMF, and room temperature is crossed liquid.In reaction product, add each 150ml of entry and ethyl acetate, shaking out.Get the upper strata and remove ethyl acetate under reduced pressure, residue adds 50ml 80% acetate and heated in boiling water bath 30 minutes, removes solvent under reduced pressure.(elutriant is CHCl3-MeOH-H to the about 800mg of residue with the silica gel column chromatography separation 2O, 90: 35: 6), get the about 450mg of compd A.FAB-MS:m/z609,499,355,337,193,163;EI-MS:m/z354,336,180,163。 1H-NMR:δ19.6(dd),2.36(dd),2.48(dd),2.50(dd),3.75(ddd),4.24(ddd),5.37(ddd),6.20(d),6.25(d),6.80(d),6.81(d),6.96(dd),6.97(dd),7.11(d),7.13(d),7.50(d),7.53(d); 13C-NMR:δ35.4,37.3,69.4,71.3,72.9,80.6,115.4,115.9,116.3,116.7,123.1,127.8,146.6,146.7,146.8,149.3,166.9,167.6。Synthesizing of embodiment 3. compd As
With 559mg 3,4-O-dichloro methylene radical coffee acyl chlorides and 254mg 3,4-O-isopropylidene quininic acid sodium fully grinds evenly, add in the flask, under vacuum decompression, in oil bath, be heated to 100 ℃ earlier, slowly rise to 140 ℃ then, heat and under vacuum state, be cooled to room temperature after 20 minutes.Reaction product adds 50ml 80% acetate and heated in boiling water bath 30 minutes, removes solvent under reduced pressure.(elutriant is CHCl3-MeOH-H to the about 800mg of residue with the silica gel column chromatography separation 2O, 90: 35: 6), get the about 450mg of compd A.FAB-MS:m/z609,499,355,337,193,163;EI-MS:m/z354,336,180,163。 1H-NMR:δ19.6(dd),2.36(dd),2.48(dd),2.50(dd),3.75(ddd),4.24(ddd),5.37(ddd),6.20(d),6.25(d),6.80(d),6.81(d),6.96(dd),6.97(dd),7.11(d),7.13(d),7.50(d),7.53(d); 13C-NMR:δ35.4,37.3, 69.4,71.3,72.9,80.6,115.4,115.9,116.3,116.7,123.1,127.8,146.6,146.7,146.8,149.3,166.9,167.6。Synthesizing of embodiment 4. compd As with 559mg 3,4-O-dichloro methylene radical coffee acyl chlorides and 254mg 3,4-O-isopropylidene quininic acid sodium and 100mg Dimethylamino pyridine (DMAP) are dissolved among the 40ml DMF ambient temperature overnight.In reaction product, add each 150ml of entry and ethyl acetate, shaking out.Get the upper strata and remove ethyl acetate under reduced pressure, residue adds 50ml 80% acetate and heated in boiling water bath 30 minutes, removes solvent under reduced pressure.(elutriant is CHCl3-MeOH-H to the about 800mg of residue with the silica gel column chromatography separation 2O, 90: 35: 6), get the about 450mg of compd A.FAB-MS:m/z609,499,355,337,193,163;EI-MS:m/z354,336,180,163。 1H-NMR:δ19.6(dd),2.36(dd),2.48(dd),2.50(dd),3.75(ddd),4.24(ddd),5.37(ddd),6.20(d),6.25(d),6.80(d),6.81(d),6.96(dd),6.97(dd),7.11(d),7.13(d),7.50(d),7.53(d); 13C-NMR:δ35.4,37.3,69.4,71.3,72.9,80.6,115.4,115.9,116.3,116.7,123.1,127.8,146.6,146.7,146.8,149.3,166.9,167.6。Embodiment 5.1,5-two-O-(3,4-two-O-ethanoyl) caffeoylquinic acids synthetic
With 565mg 3,4-two O-ethanoyl coffee acyl chlorides and 254mg 3,4-O-isopropylidene quininic acid sodium and 100mg Dimethylamino pyridine (DMAP) are dissolved among the 40ml DMF ambient temperature overnight.In reaction product, add each 150ml of entry and ethyl acetate, shaking out.Get the upper strata and remove ethyl acetate under reduced pressure, residue adds 50ml 80% acetate and heated in boiling water bath 30 minutes, removes solvent under reduced pressure.(elutriant is CHCl3-MeOH-H to the about 900mg of residue with the silica gel column chromatography separation 2O, 90: 35: 6), get the about 550mg of compd A.FAB-MS:m/z609,499,355,337,193,163;EI-MS:m/z354,336,180,163。 1H-NMR:δ1.96(dd),2.08(s),2.36(dd),2.48(dd),2.50(dd),3.75(ddd),4.24(ddd),5.37(ddd),6.39(d),6.38(d),6.85(d),6.86(d),6.98(dd),6.99(dd),7.08(d),7.09(d),7.62(d),7.64(d); 13C-NMR:δ21.9,22.0,35.4,37.3,69.4,71.3,72.9,80.6,116.4,116.9,117.5,116.7,123.3,127.6,147.6,146.7,147.8,148.4,166.9,167.6,168.1,168.2。

Claims (10)

1. formula I1, the preparation method of 5-two-O-coffeic acyl quininic acid derivative:
Figure A9910511300021
R wherein 1And R 2Can be identical or different, expression hydrogen, C 1-6Alkyl, C nH 2n-1CO-or R 1And R 2Lump together expression-CH 2-etc.;
R 3Expression H, C 1-6Alkyl, benzyl or alkalies and alkaline earth (as: Li, Na, K, Mg, Ca, Ba) etc.;
R 4And R 5Can be identical or different, be respectively H or coffee acyl,
N is the integer of 1-6;
This method comprises:
1) with formula II compound, wherein R 1' and R 2' can be identical or different,
Figure A9910511300022
Represent C nH 2n-1OCO, C nH 2n-1CO or R 1' and R 2' lump together representative-CO-,-CCl 2X is a halogen; With the reaction of formula III compound, wherein R 3' represent H, C 1-6Alkyl, benzyl or basic metal or
Figure A9910511300023
Alkaline-earth metal R 4' and R 5' can be identical or different, represent H, C 1-6Alkyl or C 6-10Aryl or R 4' and R 5' represent C with adjacent carbon atom 3-7Carbocyclic ring, production IV compound, wherein R 1', R 2', R 3', R 4' and R 5' as above definition; With
2) with 1) in the formula IV compound that obtains be hydrolyzed.
2. according to the process of claim 1 wherein that reaction is under agitation in the step 1), under alkali exists or do not exist and reduces pressure, under temperature 50-160 ℃ and reaction times 10-60 minute, carry out.
3. according to the method for claim 2, wherein reaction is carried out having in the presence of the alkali, and alkali is selected from BaCO 3, K 2CO 3, Na 2CO 3, KHCO 3Or NHCO 3
4. according to the process of claim 1 wherein that the step 1) reaction is in organic solvent, in the presence of alkali, follow and stir in-4 ℃ to 100 ℃, the reaction times is to carry out under 1-48 hour.
5. according to the method for claim 4, wherein organic solvent is selected from pyridine, triethylamine, dimethyl formamide, methyl-sulphoxide, methylene dichloride, trichloromethane, benzene, toluene, acetonitrile or propionitrile.
6. according to the method for claim 4 or 5, wherein alkali is selected from pyridine, Dimethylamino pyridine, triethylamine, K 2CO 3, Na 2CO 3, KHCO 3Or Na 2HCO 3Deng.
7. according to the process of claim 1 wherein step 2) in hydrolysis be earlier with the acid solution of dilution, be hydrolyzed with the alkaline solution that dilutes again.
8. according to the method for claim 7, wherein acid is selected from acetate or hydrochloric acid, and alkali is selected from NaHCO 3, Na 2CO 3, KHCO 3, K 2CO 3, NaOH.
9. according to the process of claim 1 wherein that basic metal or alkaline-earth metal are selected from Li, Na, K, Mg, Ca, Ba.
10. according to the method for claim 1, make following formula 1,5-two-O-dicaffeoylquinic acid,
Figure A9910511300041
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Cited By (5)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN101302159B (en) * 2008-05-16 2011-09-21 浙江大学 Method for synthesizing monobenzoyl quinate compound
CN102626404A (en) * 2012-03-22 2012-08-08 华东理工大学 Application of dicaffeoylquinic acid compound
CN101284799B (en) * 2007-03-23 2013-04-03 浙江医药股份有限公司新昌制药厂 Nitrogen-contained derivates of caffeoylquinic acid, method for preparing same, pharmaceutical compositions thereof and uses
CN106431928A (en) * 2015-08-12 2017-02-22 赵庆春 Caffeoylquinic acid derivative and application of caffeoylquinic acid derivative as medicine for repairing and protecting neurons
CN115598251A (en) * 2022-10-20 2023-01-13 山东省分析测试中心(Cn) Qualitative analysis method for isomers of hydroxybenzoyl quininic acid and hydroxycinnamoyl quininic acid

Family Cites Families (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN1087608C (en) * 1996-08-29 2002-07-17 中国人民解放军军事医学科学院放射医学研究所 Use of dicafeoyl quininic acid in treatment of hepatitis B and diseases associated with retrovirus and cafeoyl quininic acid derivs.

Cited By (6)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN101284799B (en) * 2007-03-23 2013-04-03 浙江医药股份有限公司新昌制药厂 Nitrogen-contained derivates of caffeoylquinic acid, method for preparing same, pharmaceutical compositions thereof and uses
CN101302159B (en) * 2008-05-16 2011-09-21 浙江大学 Method for synthesizing monobenzoyl quinate compound
CN102626404A (en) * 2012-03-22 2012-08-08 华东理工大学 Application of dicaffeoylquinic acid compound
CN106431928A (en) * 2015-08-12 2017-02-22 赵庆春 Caffeoylquinic acid derivative and application of caffeoylquinic acid derivative as medicine for repairing and protecting neurons
CN106431928B (en) * 2015-08-12 2020-06-19 中国人民解放军北部战区总医院 Caffeoylquinic acid derivative and application thereof as neuron repair and protection medicament
CN115598251A (en) * 2022-10-20 2023-01-13 山东省分析测试中心(Cn) Qualitative analysis method for isomers of hydroxybenzoyl quininic acid and hydroxycinnamoyl quininic acid

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