CN104693118A - N-deethyl chasmanine derivative - Google Patents

N-deethyl chasmanine derivative Download PDF

Info

Publication number
CN104693118A
CN104693118A CN201310656143.3A CN201310656143A CN104693118A CN 104693118 A CN104693118 A CN 104693118A CN 201310656143 A CN201310656143 A CN 201310656143A CN 104693118 A CN104693118 A CN 104693118A
Authority
CN
China
Prior art keywords
compound
pharmaceutically acceptable
climing
peaceful
ethyl
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Pending
Application number
CN201310656143.3A
Other languages
Chinese (zh)
Inventor
不公告发明人
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Shanghai Yizhi Pharmaceutical Technology Co Ltd
Original Assignee
Shanghai Yizhi Pharmaceutical Technology Co Ltd
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by Shanghai Yizhi Pharmaceutical Technology Co Ltd filed Critical Shanghai Yizhi Pharmaceutical Technology Co Ltd
Priority to CN201310656143.3A priority Critical patent/CN104693118A/en
Publication of CN104693118A publication Critical patent/CN104693118A/en
Pending legal-status Critical Current

Links

Classifications

    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D221/00Heterocyclic compounds containing six-membered rings having one nitrogen atom as the only ring hetero atom, not provided for by groups C07D211/00 - C07D219/00
    • C07D221/02Heterocyclic compounds containing six-membered rings having one nitrogen atom as the only ring hetero atom, not provided for by groups C07D211/00 - C07D219/00 condensed with carbocyclic rings or ring systems
    • C07D221/22Bridged ring systems

Abstract

The invention relates to a N-deethyl chasmanine hydrochloride or pharmaceutically acceptable solvates thereof and applications thereof in preparation of cardiotonics and anti-heart-failure medicines.

Description

N-takes off ethyl and looks into this climing peaceful derivative
Invention field
The present invention relates to medicinal chemistry art, specifically, the present invention relate to N-take off ethyl look into this climing peaceful derivative and pharmacy application.
Background technology
For now, although cardiotonic drug and cardiotonic agents have a variety of, these medicines existing easily cause many and heavy untoward reaction, and the result for the treatment of of existing medicine is still not ideal enough.Chinese invention patent application publication No. is describe the active compound that some have cardiotonic drug and anti-heart failure in the patent documentation of CN102977020 A.
Summary of the invention
The invention discloses the compound that some is new, the preparation method of these compounds, the pharmacy application of the pharmaceutical composition containing these compounds and these compounds and composition.
These compounds show good water-soluble stability and solid form stability.Some compound of these compounds shows special good stability.It has very high solvability to these compounds in water compared with corresponding free alkali.
It is higher that these compounds show its activity in surprise because of synergy between the two compared with corresponding free alkali.
To be effective preparation provide advantage with using in a large number for the surprising and significant stability of these compounds, water-soluble, biological activity.
Therefore, the invention provides a kind of formula III compound:
{(Ⅰ)H}+Ⅱ ˉ;
Wherein the chemical structure of I is as follows:
Wherein II is hydrochloric acid;
And/or pharmaceutically acceptable solvate, wherein:
II --represent counter ion.
Suitable counter ion II --the ion provided by pharmaceutically acceptable acid is provided.
Preferred counter ion are salt acid ions.
Formula III compound is salt.
Suitable pharmaceutically acceptable solvate is hydrate.
In addition, present invention also offers the preparation method of formula III and/or pharmaceutically acceptable solvate.This method comprises formula I compound:
With counter ion II defined above --source is reacted, and after this if necessary, then prepares its pharmaceutically acceptable solvate.
Suitable counter ion II --source is pharmaceutically acceptable mineral acid.
Preferred source of counter ions is hydrochloric acid.
Formula I compound and counter ion II --reaction between source is normally carried out under conventional salt formation condition, such as, in a solvent, be generally C1---C4 alkanol solvent as ethanol, can provide under the arbitrary temp generating required suitable rate, usually, at the temperature of the temperature such as solvent refluxing raised, be conveniently with the molar weight about waited but preferably with the counter ion II of the amount of skipping over --by formula I compound and counter ion II when source --source mixes then crystallization and goes out required product (III).
The pharmaceutically acceptable solvate of formula III compound can be prepared by the chemical process of routine.
Formula I compound can be prepared by the method described in the patent documentation of CN 102977020A according to Chinese invention patent application publication No..
Suitable source of counter ions knownly can easily to obtain through commercial sources.
The stability of the compounds of this invention can measure by normal quantitative analysis method; The stability of such as solid chemical compound can measure with the stability test accelerated, and such as dsc (DSC), thermo-gravimetric analysis (TGA) is tested with the thermoisopleth in intensification.This test comprises room temperature storage test.(wherein within known period under temperature and humidity control condition storage test compound).The quantitative analysis of test compound is before storage period, in storage period or after storage period.Relative to the stability of suitable reference standard determination test compound.
As mentioned above, it has significantly high solvability to compound of the present invention in water compared with corresponding free alkali.The ordinary method of such mensuration the compounds of this invention stability be in aqueous included in known temperature condition and known during in measure by the degree being settled out parent free alkali in the aqueous solution of test compound, we find that formula III compound demonstrates good aqueous stability.Particularly wherein II --the formula III compound of the salt acid group represented is stable especially in aqueous.More surprisingly wherein II --the formula III compound of the salt acid group represented is abnormal stable in aqueous.
Described test compound quantitative analysis test in conventional manner, can use chromatography usually, and such as high pressure lipuid chromatography (HPLC) is carried out.
As mentioned above, compound of the present invention has practical therapeutic activity.
Therefore, the invention provides the formula III compound as therapeutic active substance and/or pharmaceutically acceptable solvate.
Like this, the invention provides the formula III compound as cardiotonic drug and anti-heart failure and/or pharmaceutically acceptable solvate.
Formula III compound and/or pharmaceutically acceptable solvate can himself form be used, and preferably also can the form of pharmaceutical composition containing pharmaceutically acceptable carrier use.
Therefore, present invention also offers a kind of pharmaceutical composition containing formula III compound and/or pharmaceutically acceptable solvate and pharmaceutically acceptable carrier.
Term used herein " pharmaceutically acceptable " comprises the compound, composition and the component that use people and animal doctor, and such as, term " pharmaceutically acceptable salt " comprises the upper acceptable salt of animal doctor.
Suitable pharmaceutical composition is the composition of unit dosage, such as oral liquid, tablet, capsule, injection liquid, sprays.
Optimum pharmaceutical composition is oral liquid, sprays.
According to the convention on the medicine of routine, carrier can comprise thinner, weighting agent, disintegrating agent, wetting agent, lubricant, tinting material, seasonings or other conventional additives.
Optimum composition is configured to unit dosage.
Usually, activeconstituents can aforementioned pharmaceutical compositions form be used.
Present invention also offers a kind of containing the application on the medicine of production cardiotonic drug and anti-heart failure of formula III compound and/or pharmaceutically acceptable solvate.
Provide embodiments of the invention below for further illustrating and describing the present invention in more detail.
Embodiment 1
N-takes off ethyl and looks into this climing peaceful hydrochloride
Compound N-Tuo ethyl is looked into this climing peaceful 0.42 gram (1mmol) and hydrochloric acid 1ml is dissolved in the ethanol 10 milliliters of boiling.This hot solution is through diatomite filtration, then Slow cooling under mild agitation, a few hours are left standstill in the temperature environment of 0-5 DEG C, precipitation N-takes off ethyl and looks into this climing peaceful hydrochloride crystal, leach N-to take off ethyl and look into this climing peaceful hydrochloride crystal, dry with cold washing with alcohol and under 50 DEG C of vacuum conditions, obtain 0.45 gram of product.Embodiment 2
N-takes off ethyl and looks into this climing peaceful hydrochloride
Compound N-Tuo ethyl is looked into this climing peaceful hydrochloride 0.42 gram and hydrochloric acid 1ml in the ethanol 10 milliliters of backflow, to be stirred to solid all to dissolve.Add gac, by this hot solution through diatomite filtration, in stirring, be cooled to room temperature.In the temperature environment of 0-5 DEG C, leave standstill a few hours, separate out N-and take off ethyl and look into this climing peaceful hydrochloride crystal, leach N-and take off ethyl and look into this climing peaceful hydrochloride crystal, dry under 50 DEG C of vacuum conditions with cold washing with alcohol, obtain 0.43 gram of product.
The present invention can summarize with other the specific form without prejudice to spirit of the present invention or principal character.Therefore, no matter from which point, above-mentioned embodiment of the present invention all can only be thought explanation of the present invention and can not limit the present invention.

Claims (2)

1.N-takes off ethyl and looks into this climing peaceful (I) hydrochloric acid (II) salt (III);
HCl
(Ⅱ)
{(Ⅰ)H}+Ⅱ ˉ
(Ⅲ)
2. the application of compound in the medicine preparing cardiotonic drug and/or anti-heart failure of claim 1.
CN201310656143.3A 2013-12-06 2013-12-06 N-deethyl chasmanine derivative Pending CN104693118A (en)

Priority Applications (1)

Application Number Priority Date Filing Date Title
CN201310656143.3A CN104693118A (en) 2013-12-06 2013-12-06 N-deethyl chasmanine derivative

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
CN201310656143.3A CN104693118A (en) 2013-12-06 2013-12-06 N-deethyl chasmanine derivative

Publications (1)

Publication Number Publication Date
CN104693118A true CN104693118A (en) 2015-06-10

Family

ID=53340713

Family Applications (1)

Application Number Title Priority Date Filing Date
CN201310656143.3A Pending CN104693118A (en) 2013-12-06 2013-12-06 N-deethyl chasmanine derivative

Country Status (1)

Country Link
CN (1) CN104693118A (en)

Similar Documents

Publication Publication Date Title
CN104710422A (en) Cytisine derivative
CN103833757A (en) Salt of methoxy-canthin-6-tone derivative
CN103626773A (en) Salt of vasicine derivative
CN104693118A (en) N-deethyl chasmanine derivative
CN104693117A (en) A chasmanine derivative
CN104693116A (en) N-deethyl diacetyl chasmanine derivative
CN103772475A (en) Conimine derivative salts
CN104693197A (en) Anisodine derivative
CN103833758A (en) Salt of hydroxyl canthin-6-one derivative
CN103833747A (en) Salt of coptisine derivative
CN104710418A (en) Oleracein E derivativen
CN104710370A (en) Pymetrozine derivative
CN103833748A (en) Salt of thalicarpine urbaini derivative
CN104710353A (en) Pyridine alkaloid derivative
CN103121993A (en) Salt of 2,6-dichloro-3-fluorophenyl derivative
CN104693212A (en) A lycobetaine derivative
CN104710362A (en) Isocorydione derivatives
CN104693202A (en) Sophoridine N-oxide derivative
CN104447552A (en) Pharmaceutical use of corydine derivative
CN104710416A (en) Tetrahydropalmatine derivative
CN104387381A (en) Drug application of hydroxyl phenanthroquinolizidine derivatives
CN103864807A (en) Salts of dioxo-dehydrocrebanine derivative
CN103508952A (en) Salts of N-nornuciferine derivatives
CN103508951A (en) Salts of 2-hydroxy-1-methoxyaporphine derivative
CN103772470A (en) Salts of conessine derivative

Legal Events

Date Code Title Description
C06 Publication
PB01 Publication
WD01 Invention patent application deemed withdrawn after publication

Application publication date: 20150610