CA2006666A1 - Condensed quinoline system compound and process of preparation thereof - Google Patents
Condensed quinoline system compound and process of preparation thereofInfo
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- CA2006666A1 CA2006666A1 CA 2006666 CA2006666A CA2006666A1 CA 2006666 A1 CA2006666 A1 CA 2006666A1 CA 2006666 CA2006666 CA 2006666 CA 2006666 A CA2006666 A CA 2006666A CA 2006666 A1 CA2006666 A1 CA 2006666A1
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Abstract
ABSTRACT OF THE DISCLOSURE
Novel condensed quinoline system compounds such as indenoquinoline system compounds, indoloquinoline system compounds, benzothienoquinoline system compounds and benzofuranoquinoline system compounds, and a process for preparation of theses compounds are provided. The present invention is also directed to salts of the above compounds.
The compounds of the present invention are effective for inhibition of KB-cell growth and prolongation of life span in cancer inplated mouse.
Novel condensed quinoline system compounds such as indenoquinoline system compounds, indoloquinoline system compounds, benzothienoquinoline system compounds and benzofuranoquinoline system compounds, and a process for preparation of theses compounds are provided. The present invention is also directed to salts of the above compounds.
The compounds of the present invention are effective for inhibition of KB-cell growth and prolongation of life span in cancer inplated mouse.
Description
20()6666 TITLE OF THE INVENTION
Condensed Quinoline System Compound and Process of Preparation thereof BACKGROUND OF THE INVENTION
Field of the Invention The present invention relates to novel quinoline Rystem compounds and a process for preparing the ~ame and more particularly, relates to novel indenoquinoline system compounds (Z = CH,), indoloquinoline system compounds t2 =
NH), benzothienoquinoline system compounds (Z = S) and benzofuranoquinoline system compound~ (~ = S), and a process for preparation thereof.
Description or the Related Art In 1972, B. F. Cain, G. J. Atwell and R. N. Sealye synthesized acridine derivatives each having an alkylamino group at position 9 of acridine, and found that some of them had antileukemia activities. (See J. Med. Chem. vol.15, 611 (1972?) B. F. Cain, G. J. Atwell and R. N. Sealye replaced the alkylamino group at the 9-position of acridine with another molecule or group, and found that N-14-(9-acridylamino)-3-methoxyphenyl)methanesulfonamide (Amsacrine) has the highest carcinostatic function. (Refer to J. Med. Chem.
vol.17, 922 (19743) G. W. Rewcastle, B. C. Baguley, G. J. Atwell and W. A.
200~;666 Denny modified Amsacrine molecule to synthesize derivatives each having acridine ring introduced with methyl group or N-methylcarbamoly group, and found that the derivatives have strong carcinostatic activities. (See J. Med. Chem.
vol. 30, 1576 (1987)) We previously synthesized indenoquinoline system compounds having high carcinostatic activities, and filed a patent application relating thereto (Japanese Patent disclosure No. 63-1~1369).
Eurther, we synthesized benzofuranoquinoline and benzothieoquinoline system compounds having similar high carcinostatic activities, and filed another patent application relating thereto (Japane~e Patent disclosure No. 63-238079).
We also filed a patent application directing to indoloquinoline and benzoacridine ~ystem compounds, a process for preparation thereof and use of the same as anticancer agents (Japanese Patent disclosure No. 63 -56883).
SUMMARY OF THE INVENTION
An object of the present invention is to provide novel quinoline system compounds with strong carcinostatlc activities.
The present invention is based on our further investigations on various condensed quinoline system compounds, and we found novel condensed quinoline system ` 2006666 compounds and a process for preparing thereof.
According to this invention, there is provided a sondensed quinoline system compound represented by the following formula II]:
X Y
NH
~ 1 M
In the formula, L represents a lower alkoxyl group or a dimethylamino group, M represents a hydroxyl group, a methoxycarbonyl group or- NHQ (in this formula, Q
represents hydrogen, - SO,CH,, - COOCH,, - COCH,, CH,SO,Na or - CH,COOH), X represents hydrogen or a lower alkyl group, Y represents hydrogen, a lower alkyl group, halogen, - NO2 or - NHR (in this formula, R represents hydrogen, - COCH., - SO,CH,, OAc /o~
AcO~ (in this formula, Ac represents acetyl) or ~ - OAc OAc OH
, ~ representu oxygen, uulfur, CN. or NN.
OH
The present invention will now be described in detail.
In the formula [I ], the lower alkoxyl ~roup means an alkoxyl group having l to 6 carbon atoms. Examples of the alkoxyl group include methoxy, ethoxy, propoxy, butoxy and pentoxy. The lower alkyl means an alkyl group having l to 6 carbon atoms. Examples of the alkyl group include methyl, ethyl, n-propyl, iso-propyl, n-butyl, tert-butyl, n-pentyl, n-hexyl. Examples of halogen include fluorine, chlorine, bromine and iodine.
The present invention includes salts, in particular pharmaceuticaly acceptable salts of the compound represented by formula lIl. Examples of the salts include salts of inorganic acids such as hydrochloric acid, phosphoric acid, bromic acid and sulfuric acid, and salts of organic acids such as benzoic acid, citric acid, succinic acid, acetic acid, tartaric acid and maleic acid.
In the case of indenoquinoline system compounds represented by formula [I] wherein Z is CH,, preferably, L
is a lower alkoxyl group or a dimethylamino group, M is NHQ (in this formula, Q represents hydrogen, - SO,CH,, -COOCH,, - CH, SO, Na or - CH. COOH), X is hydrogen or a lower alkyl group, Y is hydrogen or a lower alkyl group. The position of X (7- to 10-position~ and that of Y ~1- to 4-position) are not limited, but it is preferred that X is located at 10-positlon and Y is located at 1-, 2- and 3-position.
In the case of indoloquinoline system compounds represented by formula 1I] wherein Z is NH, preferably, L is a lower alkoxyl group, M is a hydroxyl group, a methoxycarbonyl group or - NHQ (in this formula, Q
represents - SO.CH,, - COOCH3, - COCH,), X is hy~rogen or a lower alkyl group, Y is hydrogen, a lower alkyl group, halogen, - NO2 or - NHR (in this formula, R represents OAc OH
-- COCH,,-- SO, CH,, ~
) OAC OH
OAc OH
The position of X (7- to 10-position) and that of Y
(1- to 4-position) are not limited, but it is preferred that X is located at 10-position and Y is located at 1-, 2- and 3-position.
In the case of benzothienoquinoline system compounds 20(~66~,6 represented by formula 1I] wherein Z is sulfur, preferably, L is a lower alkoxyl group, M is - NHQ (in this formula, Q
represents - SO.CH3), X is hydrogen or a lower alkyl group, Y is hydrogen or a lower alkyl group. The position of X
~7- to lO-position) and that of Y (l- to 4-position) are not limited, but it is preferred that X is located at lO-position and Y is located at l-, 2- and 3-position.
In the case of benzofuranoquinoline sy3tem compounds represented by formula II] wherein Z is oxygen, preferably, L is a lower alkoxyl group, M is - N8Q (in this formula, Q
represents - SO,CH,), X is hydrogen or a lower alkyl group, Y i8 hydrogen or a lower alkyl group. The position of X
(7- to lO-positionj and that of Y (l- to 4-position) are not limited, but it is preferred that X is located at lO-position and Y is located at l-, 2- and 3-position.
A process for preparation of the compounds of this invention will be explained in view of schemes l to 4 below:
Z~O
~3 ~ ~o + r<, m o Z~
\_ / \ _ ~)~ < ~ >
' 2006666 ~
, oC~
P: ~ 3 CD ~
~= I
0~ ~
,~
~o :æo ~q æ:::
o :æc~ ~ Z; .F
ZO()6666 ~ ~
U:~ J
~lô ~>
:C ~
C_~ O
51 ~ 1 ~ ~ôl =~ ~A~
; ~ I
~5~;~0 Z006666~ ~
o ~
~^ _~>
.. ~
B e ~
., ~z ol ~0 wô
o ~o '' ~z~o ~ 1 0 ~
Scheme 1: Indenoquinoline compound (z = CH,) Indenoquinoline compounds represented by formula lIal can be synthesized by the method shown in Scheme 1.
Anthranilic acid shown by formula (10) is reacted with indanone shown by formula (11) to obtain indenol3,2-b]-6, ~1-dihydroquinoline-6-one shown by formula (12). The reaction condition should be changed in accordance with kinds of subs~ituents X and Y, and this reaction can be conducted, for example, in the absence or presence of solvent such as para-cymene and at a temperature of from 100 to 200C -Compound (12) is then reacted with phosphorus oxychloride to obtain indeno~3,2-b]quinoline shown by formula (13). This reaction is suitably carried out at a reflux temperature.
Thus obtained compound (13) i8 reacted with an aniline derivative shown by formula (14) to obtain an indenoquinoline compound represented by formula [Ia]. This reaction can be conducted by heating under reflux in the presence of solvent such as dimethylformamide (DMF), pyridine, ethoxyethanol or dioxane, in an atmosphere of inert gas. The reaction product is optionally purified by a conventional method such as recrystallization.
Salts of indenoquinoline compound represented by formula [Ial can be obtained by addition of an acid such as hydrochloric acid to the reaction solution before, during or after the reaction with the aniline derivative.
Condensed Quinoline System Compound and Process of Preparation thereof BACKGROUND OF THE INVENTION
Field of the Invention The present invention relates to novel quinoline Rystem compounds and a process for preparing the ~ame and more particularly, relates to novel indenoquinoline system compounds (Z = CH,), indoloquinoline system compounds t2 =
NH), benzothienoquinoline system compounds (Z = S) and benzofuranoquinoline system compound~ (~ = S), and a process for preparation thereof.
Description or the Related Art In 1972, B. F. Cain, G. J. Atwell and R. N. Sealye synthesized acridine derivatives each having an alkylamino group at position 9 of acridine, and found that some of them had antileukemia activities. (See J. Med. Chem. vol.15, 611 (1972?) B. F. Cain, G. J. Atwell and R. N. Sealye replaced the alkylamino group at the 9-position of acridine with another molecule or group, and found that N-14-(9-acridylamino)-3-methoxyphenyl)methanesulfonamide (Amsacrine) has the highest carcinostatic function. (Refer to J. Med. Chem.
vol.17, 922 (19743) G. W. Rewcastle, B. C. Baguley, G. J. Atwell and W. A.
200~;666 Denny modified Amsacrine molecule to synthesize derivatives each having acridine ring introduced with methyl group or N-methylcarbamoly group, and found that the derivatives have strong carcinostatic activities. (See J. Med. Chem.
vol. 30, 1576 (1987)) We previously synthesized indenoquinoline system compounds having high carcinostatic activities, and filed a patent application relating thereto (Japanese Patent disclosure No. 63-1~1369).
Eurther, we synthesized benzofuranoquinoline and benzothieoquinoline system compounds having similar high carcinostatic activities, and filed another patent application relating thereto (Japane~e Patent disclosure No. 63-238079).
We also filed a patent application directing to indoloquinoline and benzoacridine ~ystem compounds, a process for preparation thereof and use of the same as anticancer agents (Japanese Patent disclosure No. 63 -56883).
SUMMARY OF THE INVENTION
An object of the present invention is to provide novel quinoline system compounds with strong carcinostatlc activities.
The present invention is based on our further investigations on various condensed quinoline system compounds, and we found novel condensed quinoline system ` 2006666 compounds and a process for preparing thereof.
According to this invention, there is provided a sondensed quinoline system compound represented by the following formula II]:
X Y
NH
~ 1 M
In the formula, L represents a lower alkoxyl group or a dimethylamino group, M represents a hydroxyl group, a methoxycarbonyl group or- NHQ (in this formula, Q
represents hydrogen, - SO,CH,, - COOCH,, - COCH,, CH,SO,Na or - CH,COOH), X represents hydrogen or a lower alkyl group, Y represents hydrogen, a lower alkyl group, halogen, - NO2 or - NHR (in this formula, R represents hydrogen, - COCH., - SO,CH,, OAc /o~
AcO~ (in this formula, Ac represents acetyl) or ~ - OAc OAc OH
, ~ representu oxygen, uulfur, CN. or NN.
OH
The present invention will now be described in detail.
In the formula [I ], the lower alkoxyl ~roup means an alkoxyl group having l to 6 carbon atoms. Examples of the alkoxyl group include methoxy, ethoxy, propoxy, butoxy and pentoxy. The lower alkyl means an alkyl group having l to 6 carbon atoms. Examples of the alkyl group include methyl, ethyl, n-propyl, iso-propyl, n-butyl, tert-butyl, n-pentyl, n-hexyl. Examples of halogen include fluorine, chlorine, bromine and iodine.
The present invention includes salts, in particular pharmaceuticaly acceptable salts of the compound represented by formula lIl. Examples of the salts include salts of inorganic acids such as hydrochloric acid, phosphoric acid, bromic acid and sulfuric acid, and salts of organic acids such as benzoic acid, citric acid, succinic acid, acetic acid, tartaric acid and maleic acid.
In the case of indenoquinoline system compounds represented by formula [I] wherein Z is CH,, preferably, L
is a lower alkoxyl group or a dimethylamino group, M is NHQ (in this formula, Q represents hydrogen, - SO,CH,, -COOCH,, - CH, SO, Na or - CH. COOH), X is hydrogen or a lower alkyl group, Y is hydrogen or a lower alkyl group. The position of X (7- to 10-position~ and that of Y ~1- to 4-position) are not limited, but it is preferred that X is located at 10-positlon and Y is located at 1-, 2- and 3-position.
In the case of indoloquinoline system compounds represented by formula 1I] wherein Z is NH, preferably, L is a lower alkoxyl group, M is a hydroxyl group, a methoxycarbonyl group or - NHQ (in this formula, Q
represents - SO.CH,, - COOCH3, - COCH,), X is hy~rogen or a lower alkyl group, Y is hydrogen, a lower alkyl group, halogen, - NO2 or - NHR (in this formula, R represents OAc OH
-- COCH,,-- SO, CH,, ~
) OAC OH
OAc OH
The position of X (7- to 10-position) and that of Y
(1- to 4-position) are not limited, but it is preferred that X is located at 10-position and Y is located at 1-, 2- and 3-position.
In the case of benzothienoquinoline system compounds 20(~66~,6 represented by formula 1I] wherein Z is sulfur, preferably, L is a lower alkoxyl group, M is - NHQ (in this formula, Q
represents - SO.CH3), X is hydrogen or a lower alkyl group, Y is hydrogen or a lower alkyl group. The position of X
~7- to lO-position) and that of Y (l- to 4-position) are not limited, but it is preferred that X is located at lO-position and Y is located at l-, 2- and 3-position.
In the case of benzofuranoquinoline sy3tem compounds represented by formula II] wherein Z is oxygen, preferably, L is a lower alkoxyl group, M is - N8Q (in this formula, Q
represents - SO,CH,), X is hydrogen or a lower alkyl group, Y i8 hydrogen or a lower alkyl group. The position of X
(7- to lO-positionj and that of Y (l- to 4-position) are not limited, but it is preferred that X is located at lO-position and Y is located at l-, 2- and 3-position.
A process for preparation of the compounds of this invention will be explained in view of schemes l to 4 below:
Z~O
~3 ~ ~o + r<, m o Z~
\_ / \ _ ~)~ < ~ >
' 2006666 ~
, oC~
P: ~ 3 CD ~
~= I
0~ ~
,~
~o :æo ~q æ:::
o :æc~ ~ Z; .F
ZO()6666 ~ ~
U:~ J
~lô ~>
:C ~
C_~ O
51 ~ 1 ~ ~ôl =~ ~A~
; ~ I
~5~;~0 Z006666~ ~
o ~
~^ _~>
.. ~
B e ~
., ~z ol ~0 wô
o ~o '' ~z~o ~ 1 0 ~
Scheme 1: Indenoquinoline compound (z = CH,) Indenoquinoline compounds represented by formula lIal can be synthesized by the method shown in Scheme 1.
Anthranilic acid shown by formula (10) is reacted with indanone shown by formula (11) to obtain indenol3,2-b]-6, ~1-dihydroquinoline-6-one shown by formula (12). The reaction condition should be changed in accordance with kinds of subs~ituents X and Y, and this reaction can be conducted, for example, in the absence or presence of solvent such as para-cymene and at a temperature of from 100 to 200C -Compound (12) is then reacted with phosphorus oxychloride to obtain indeno~3,2-b]quinoline shown by formula (13). This reaction is suitably carried out at a reflux temperature.
Thus obtained compound (13) i8 reacted with an aniline derivative shown by formula (14) to obtain an indenoquinoline compound represented by formula [Ia]. This reaction can be conducted by heating under reflux in the presence of solvent such as dimethylformamide (DMF), pyridine, ethoxyethanol or dioxane, in an atmosphere of inert gas. The reaction product is optionally purified by a conventional method such as recrystallization.
Salts of indenoquinoline compound represented by formula [Ial can be obtained by addition of an acid such as hydrochloric acid to the reaction solution before, during or after the reaction with the aniline derivative.
2~0ti6~6 Scheme 2: Indoloquinoline compound (Z = NH) Indenoquinoline compounds represented by formula [Ib]
can be synthesized by the method shown in Scheme 2.
Anthranilic acid shown by formula (lO) is reacted with chloroacetyl chloride to obtain N(chloroacetyl)anthranilic acid shown by formula (15). This reaction is suitably carried out by heating under reflux in a solvent such as benzene.
Thus obtained compound (15) is reacted with an aniline derivative shown by formula tl6) to obtain an anthranilic acid shown by formula (17). This reaction is suitalby conducted by heating at a temperature from about 50 to 100C
in a solvent such as dimethylformamide.
Compound (17) is reacted with polyphosphoric acid to obtain an indoloquinoline derivative shown by formula (18).
This reaction is suitalby conducted by heating at a temperature from about 100 to 150 C in the presence of excess amount of polyphosphoric acid.
Compound (18) is reacted with phosphorus oxychloride in the presence of phosphorus pentachloride to obtain a chloride of indoloquinoline derivative shown by formula (19). This reaction is suitably carried out by heating preferably at a reflux temperature.
Thus obtained compound (19) i9 reacted with an aniline derivative shown by formula (14) to obtain an indoloquinoline compound represented by formula [Ib]. This reaction can be conducted by heating, preferably at a reflux temperature, in the presence of solvent such as dimethylformamide (DMF), pyridine, ethoxyethanol or dioxane, in an atmosphere of inert gas. The reaction product is optionally purified by a conventional method such as recrystallization. Salts of indoloquinoline compound represented by formula [Ib] can be obtained by addition of an acid such as hydrochloric acid to the reaction solution before, durin~ or after the reaction with the aniline derivative.
Scheme 3: senzothieno _ noline compound (z = S) senzothienoquinoline compounds represented by formula [Ic] can be synthesized by the method shown in Scheme 3.
A thiol derivative shown by formula (20) is reacted with butyl bromoacetate by a conventional method and then hydrolyzed to obtain a -phenythioacetic acid shown by formula (21). Compound (21) is reacted with thionyl chloride by a conventional method to obtain an acetyl chloride shown by formula (22).
Compound (22) is reacted with anthranilic acid shown by formula (lO) to obtain an anthranilic acid derivative shown by formula (23). This reaction can be carried out by dissolving anthranilic acid (10) in an aqueous solution of an alkali hydroxide such as sodium hydroxide, droping compound (22) into this solution and stirring the resulting solution. The droping and stirring are preferably conducted under cooling, for example in an ice bath.
The resultant anthranilic acid derivative (23) is reacted with polyphosphoric acid to obtain an benzothienoquinoline derivative shown by formula (24). This reaction is suitalby conducted by heating at a temperature from about 100 to 150 C in the presence of excess amount of polyphosphoric acid.
Compound (24) is reacted with phosphorus oxychloride to obtain a chloride of benzothienoquinoline derivative shown by ~ormula (25). This reaction is sultably carried out by heating under reflux in the presence of excess amount of phosphorus oxychloride.
Thus obtained compound (25) is reacted with an aniline derivative shown by formula (14) to obtain a benzothienoquinoline compound represented by formula ~Ic].
This reaction can be conducted by heating, for exampl at a reflux temperature, in the presence of solvent such as dimethylformamide (DMF), pyridine, ethoxyethanol or dioxane, in an atmosphere of inert gas. The reaction product i8 optionally purified by a conventional method such as recrystallization.
Salts of benzothienoquinoline compound represented by formula [Icl can be obtained by addition of an acid such as hydrochloric acid to the reaction solution before, during or after the reaction with the aniline derivative.
Scheme 4: ~enzofuranoquinoline compound (Z = O) BenzofuranoqUinoline compounds represented by formula lId] can be synthesized by the method shown in Scheme 4.
Phenoxyacetic acid shown by formula (26) is reacted l 4 200~i6~i6 with thionyl chloride by a conventional method to obtain phenoxyacetyl chloride shown by formula ~27).
Phenoxyacetyl chloride (27) is reacted with anthranilic acid shown by formula ~10) to obtain an anthranilic acid derivative shown by formula (28). This reaction can be carried out by dissolving anthranilic acid (10) in an aqueous solution of an alkali hydroxide such as sodium hydroxide, droping chloride (28) into this aqueous solution and stirring the resulting solution.
The resultant anthranilic acid derivative ~28) is reacted with polyphosphoric acid to obtain an benzofuranoquinoline derivative shown by formula (29). This reaction can be conducted by heating at a temperature of from about 100 to 150 C in the presence of excess amount of polyphosphoric acid.
Compound (29) is reacted with phosphorus oxychloride to obtain a chloride of benzofuranoquinoline derivative shown by formula (30). This reaction can be carried out by heating in the presence of excess amount of phosphorus oxychloride at a reflux temperature.
Thus obtained compound (30) is reacted with an aniline derivative shown by formula (14) to obtain a benzofuranoquinoline compound represented by formula lId].
This reaction can be conducted by heating, for exampl at a reflux temperature, in the presence of solvent such as dimethylformamide (DMF), pyridine, ethoxyethanol or dioxane, in an atmosphere of inert gas. The reaction product is optionally purified by a conventional method such as recrystallization.
Salts of benzofuranoquinoline compound represented by ' formula lId] can be obtained by addition of an acid such as hydrochloric acid to the reaction solution before, during or after the reaction with the aniline derivative.
Starting materials used in the above-mentioned method are known compounds or compounds easily obtainable by known methods.
The novel condensed quinoline system compounds of this invention suppress proliferation of cancer cells and exhibit effects in prolonging the life of animals with cancer and therefore, are expected to be utilized as unticancer agents.
The present invention will now be de~cribed more in detail with reference to Examples.
Synthesis of hydrochlorate of 6-4-~methanesulfonamide-2-methoxyanilino)-1,10-dimethylindeno[3,2-b]quinoline:
/ CH. CH, \
''' 1',~
NH HCQ
OCH, NH- SO,CH3 7-Methyl-1-indanone 5 g (34.0 mmol) and 3-methylanthranilic acid 11.0 g (85.0 mmol) were dissolved in 20 ml of paracymene and heated under reflux at 200 to 220 C
for 4 hours. After reflux, paracymene was distilled under the reduced pressure and the resulting residue was recrystallized from toluene to obtain 1,10-dimethylindenol3,2-b]-6,11-dihydroquinoline-6-one 890 mg (yield: 12%). 7-Methyl-1-indanone was synthesized by the method reported by B. R. Holt and J. London ~Zh. Obshch.
Khim., 20, 1245(1950)~ .
The resultant compound 890 mg (3.41 mmol) was refluxed with phosphorus oxychloride 10 ml for 2 hours and unreacted phosphorus oxychloride was distilled off. The residue was poured into ice water and neutralized with KOH. Then the neutralized solution was subjected to extraction with chloroform, and the resulting chloroform solution was washed with an aqueous solution saturated with NaCl and dried with anhydrous MgSO,. The solvent in the dried solution was then distilled off. The residue was recrystallized from dichloromethane/hexane to obtain 6-chloro-1,10-dimethylindenone 780 mg (yield: 82%) (melting point: 161 to 162 C )-Then the resulting compound 750 mg and 4-amino-3-methoxyanilinemethanesulfonaminde 610 mg were dissolved in 10 ml of ethoxyethanol under heating. One drop of conc.
hydrochloric acid was added to the solution and heated with agitation for 2 hours. Deposited precipitate was collected by filtration and recrystallized from dimethylformamide/methanol to obtain the above captioned compound (hydrochlorate) 680 mg (yield : 51%).
Melting point: 232 to 233C
I R ~ cm : 3520, 3330, 1320, 1150 'H-NMR(CF,COOD) ~
2.92,3.11(6H, each s, CH, X 2 ) 3.33(3H, s, SO~CHl) 3.52(2H, s, CH,) 3.93(2H, s, OCH,) 7.01-7.40(5H, m, aromatic H, NH) 7.48-7.95(7H, m, aromatic H ) ... . . . . . . .. .
20~)6666 Synthesis of hydrochlorate of 6-4-(methanesulfonamide-2-methoxyanilio)-10-methylindeno[3,2-b]quinoline:
NH . HC.e [~ OCH9 NH-- SO~ CH3 1-Indanone 1 g (7.6 mmol) and 3-methylanthranilic acid 1.1 g (7.3 mmol) were ais~olved in 20 ml of paracymene and refluxed at 200 C for 30 minutec. After reflux, the reaction solution was cooled and deposited crystals were colloected by filtration and washed with pyridine and ether to obtain 10-methylindeno[3,2-b]-6,11-dihydroquinoline-6-one (melting point: 300 nc or more) 960 mg (yield: 53%).
The resultant compound 950 mg ~3.85 mmol) was refluxed with phosphorus oxychloride 10 ml for 2 hours and unreacted phosphorus oxychloride was distilled off. The residue was poured into ice water and neutralized with 10~ KOH. Then the neutralized solution was subjected to extraction with chloroform, and the resulting chloroform solution was washed .
;~006666 with water and dried with anhydrous MgSO.. The solvent in the dried solution was then di~tilled off to obtain 6-chloro-10-methylindenone 800 mg (yield: 82%) (melting point:
131 to 133 DC )~ Then the resulting compound 700 mg and 4-amino-3-methoxyanilinemethanesulfonaminde 700 mg (3.30 mmol) were dissolved in 8 ml of ethoxyethanol under heating.
Two drops of conc. hydrochloric acid were added to the solution and heated for 4 hours. Deposited precipitate was filtered and recrystallized from methanol to obtain the above captioned compound (hydrochlorate) 320 mg (yield ;
26.4%).
Melting point: 251 to 2S3C
1 R ~ N i~l cm~~: 3340, 1320, 1150 'H-NMR(CFlCOOD) ~ :
2.92(3H, s, CH,) 3.33(3H, s, SO,CH,) 3.52(2H, s, CH,) 3.93(3H, s, OCH,) 7.01-7.40(5H, m, aromatic H, NH) 7.48-7.95(7H, m, aromatic H ) 8.10-8.40(2H, m, aromatic H ) Synthesis of hydrochlorate of 6-(4-methoxycarbamoyl-2-methoxyanilino)-indeno[3,2-blquinoline:
200666~i NH
~,~CII, ~-UC~
NHCOOCH~
6-Chloroindenol 3, 2-b]quinoline ~synthesized by a method described in Japanese Patent Disclosure No.63-101369) 700 mg (2.8 mmol) and 4-methoxycarbamoyl-2-methoxyaniline 650 mg were added to 5 ml of ethoxyethanol.
Two drops of conc. hydrochloric acid were added to this solution and reated under reflux for 3 hours. After the reaction, deposited precipitate was filtered and washed with ether to obtain the above captioned hydrochlorate 610 ~g (yield : 49%).
4-Methoxycarbamoyl-2-methoxyaniline was synthesized by the method of G. W. Rew castle (J. Med. Chem., 30, 1576 (1987)).
Melting point: 244 to 246~C
I R v Nu~ol cm-~: 3450, 1730 'H-NMR(DMSO-d6) ~ :
3.40(2H, s, CH,) 3.82(6H, s, OCH~, COOCH,) 7.11-7.30(2H, m, aromatic H ) 7.38-7.80(6H, m, aromatic H ) 7.96-8.65(4H, m, aromatic H, NH) 9.72-9.85(1H, br, N~) Synthesis of hydrochlorate of 6-(4-amino-2-methoxyanilino)-indenot3,2-b]quinolines 10 ~
NH
l ~ OC~ NC e NH~
6-(4-Methoxycarbamoyl-2-methoxyanilino)-indenol3,2-blquinoline (415 mg, 1 mmol) synthesized in Example 3 was dissolved in 4ml of CH3SO3H. Then, 0.37 ml (5 mmol) of (CHJ),S was added to the resulting solution and stirred at 35 ~C for 1.5 hours. The reaction solution was neutralized with KHCOa and the product was extracted with ethyl acetate. The obtained extract solution was dried with MgSO4 and the solvent was distilled off to obtain the objective product quantitatively.
Melting Point: 246 to 251 ~C (decomp,) X0066~6 I R ~ Nulol cm~l: 3470(NH,), 3440, 3290(NH) NMR(CDC~ , + DMSO - d.)~
3.20-3.43(2H, m, CH,) 3.72(3H, s, OCH~) 6.14-7.56(11H, m, aromatic H, NH, NH,) 7.90-8.33(3~, m, aromatic ~ ) Synthesis of hydrochlorate of 6-(4-methanesulfonamide-anilino)-indenol3,2-blquinoline:
In accordance with the procedures of Example 2 excepting that anthranilic,acid was used in place of 3-methylanthranilic acid, hydrchlorate of 6-(4-methanesulfonamide-anilino)-indenol3,2-b]quinoline was obtained.
NH
O H~ CQ
NHSO,CH3 Melting Point: lB5 to 188 C
I R v Nulol cm~~ 3560, 1335, 1145 NMR(DMSO- d5) ~
3.08(3H, s), 3.70(2H, s), 7.00-7.31(4H, m), 7.31-7.80(5H, m), 8.15-8.50(3H, m) Synthesis of hydrochlorate of 6-( 4-methanesulfonamide-2-dimethylaminoanilino)-indeno~3,Z-b]quinoline:
10 ~ ~
NH
~5 I ~ ~(C~ C~
NHSO,CH9 6-Chloroindeno[3,2-b]quinoline ~592 mg, 2 mmol) synthesized in Example 3 and hydrochlorate of 4-amino-3- 0 dimethylaminoanilinemethanesulfonamide 519 mg ~2 mmol) were added to 10ml of ethoxyethanol and three drops of conc.
hydrochloric acid were added to this solution. Thu~
obtained solution was heated under reflux for 11 hours.
After refluxi deposited crystals were collected and washed 5 with ether to obtain the objective product 520 mg ~yield:
59%).
Melting point: 262 to 265 C
I R ~ NuJol cm~~ 3340, 1330, 1143 ~., NMR(DMSO- d,) ~
2~69(6H, s, NMe,) 3.15(3H, 9~ SO,Me) 3.20-3.38(2H, m, CH,) 6.80-7.83~8H, m, aromatic H ) 8.11-8.98(3H, m, aromatic H ) 9.89-10.03~1H, br, NN) 10.34-10.51(1H, br, NHSO~- ) Synthesis of hydrochlorate of 6-(4-sodium sulfonmethylamino-2-methoxyanilino)-indeno[3,2-b]quinoline:
[ ~ > ~
NH
~OJ
20~ ~
NHCH,SO,Na 6-(4-Amino-2-methoxyanilino)-indenoE3,2-b]quinoline (353 mg, 1 mmol) synthesized in Example 4 was dissolved in 60ml oP ethanol. 30 ml of ethanl solution (ethanol:
water=8:2) of HOCH.SO,Na ~150 mg, 1.1 mmol) was added to this solution. The resulting reaction mixture was heated at 60 to 70 C for 10 minutes. After heating, deposited crystals were collected by filtration and washed with ethanol and ether to obtain the objective product 339 mg (yield: 75~
The product was identified by confirming generation of SO, when the product was heated in 10% HCl solution at 100 C .
Synthesis of hydrochlorate of 6-(4-carboxymethylamino-2-methoxyanilino)-indeno[3,2-b]quinoline:
NH
~c~ J~c~
NHCH, COOH
~
6-(4-Amino-2-methoxyanilino)-indeno[3,2-b~quinoline (500 mg, 1.4 mmol) synthesized in Example 4 was dissloved in Sml of dried DMF and 500 mg (3.5 mmol) of K,CO, was added to this solution. To this mixing solution, BrCH,COOCH3 0.16ml (1.5mmol) was added and heated at 50 to 60 C for 2 hours. After heating, the reaction mixture was poured into ice water and subjected to extraction with ethyl acetate.
The extract solution was dried with MgSO4 and the solvent was distilled off to obtain quantitatively 6-(4-methylcarboxymethylamino-2-methoxyanilino)-indeno[3,2-b]quinoline.
426 mg (1 mmol) of this product was dissloved in 20%
NaOH-methanol solution 10 ml and ag~tated for 2 hours at room temperature. After agitation, the reaction mixture was neutralized with 10% HCl solution and then methanol was distilled off. Then 1 ml of 10% HCl solution was added to the residue to acidify and deposited crystals were collected by filtration to obtain the objective product (hydrochlorate) 306 mg (yield: 74~).
Physical properties of 6-(4-methylcarboxymethylamino-2-methoxyanilino)-indeno[3,2-b]quinbline:
Melting point: 260 to 270 C (decomp) I R ~ N~ol cm~~ 1740(C,O), 3400(NH) m~ ~
'H-NMR(CDC~
3.42(2H, s, CH,) 3.77(6H, s, OCH3) 3.90(2H, s, CH,) 6.01-6.42(4H, m, aromatic H, NH) 7.18-7.70(4H, m, aromatic H, NH) 7.99-8.32(3H, m, aromatic H) 5 Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-methoxyanilino)-10-methylindolo[3,2-b]quinoline:
CH, \
NH HC~
~ OCH~ ~
NH- SO,CH9 3-Methylanthranilic acid 10 g (0.07 mol) was dissolved in dried benzene lOOml. To thi~ solution, chloroacetylchloride 5.81 ml (0.07 mol) was added.dropwise at room temperature and heated under reflux for two hours.
After cooling, deposited crystals were collected by filtration and recrystallized from benzene-toluene to obtain 3-methyl-N(chloroacetyl)anthranilic acid 11.7 g (yield:
79~).
Then, 3 g (0.01 mol) of this compound was dissolved in 5 ml tO.04 ml) of aniline and 5 ml of dimethylformamide and heated at 80 to 90 C for 4 hours. Cold water was added to the reaction solution, and deposited crystals were collected by filtration, washed with ether and recrystallized from toluene to obtain 3-methyl-N(phenylaminoacetyl)anthranilic acid 2.6 g (yield: 70~).
The resulting compound 2.5 g (7.8 mmol) was mixed with .
polyphosphoric acid 50 g and heated at 120 C for 2 hours.
After heating, the reaction mixture was poured into cold water. The resulting solution was neutralized with potassium hydrogencarbonate and deposited crystals were collected by filtration to obtain 11-methylindolo[3,2-b]-6,11-dihydroquinoline-6-one 1.7 g (yield: 77%).
The resultant compound 1.7 g (6 mmol) was added to phosphorus pentachloride 1.25 g (6 mmol) and phosphorus oxychloride 30 ml, and hèated under reflux for 2 hours.
Unreacted phosphorus oxychloride was distilled off, and the residue was poured into ice water and neutralized with 10%
NaOH solution. Then the neutralized solution was subjected to extraction with chloroform, and the resulting chloroform solution was washed with water, dried with anh~drous MgSO4 and the solvent was distilled off. The residue was recrystallized from dichloromethane/methanol to obtain 6-chloro-10-methylindolol3,2-b]quinoline (melting point: 228 to 230 C ) 1.2 g (yield: 66%).
Then the resulting compound 800 mg (3.1 mmol) and 4-amino-3-methoxyanilinemethanesulfonaminde 684 mg (3.6 mmol) were dissolved in 10 ml of ethoxyethanol. One drop of conc.
;i hydrochloric acid was added to this solution and heated under reflux for 4 hours. After cooling, precipitate was collected, washed with ether and chloroform and recrystallized from methanol to obtain the objective compound (hydrochlorate) 870 mg (yiled : 72%).
Melting point: 260 to 263 C
' .
, .
2 0 ~ 66 6 6 I R ~ Nulol cm~l 3120, 1325, 1160 m- I
NMR~CDC~ g ~ DMSO - d5) ~ :
3.14t3H, S, CH,) 3.31(3H, s, SO,CH,) 3.8S(3H, s, OCH,) 7.09-7,45(2H, m, aromatic H ) 7. 53-8.18(8H, m, aromatic H ) 8.~3-9.04(1H, m, NH) 9.21-9.46(1H, m, NH) 10.49-10.60(1H, br, NH) EXAMPLE lO
Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-methoxyanilino)-1,10-dimethylindolol3,2-b]quinoline:
,~ 15 J CH3 CH, \
~J, ~
- NH HC~
[~C ,1 NH- SO,CHg 3-Methyl-N(chloroacetyl)anthranilic acid 7.5 g (33 mmol)(synthesized from 3-methylanthranilic acid by the same procedures as those of Example 9) and m-toluidine 11 ml '' .
!
Z00~6~i6 0.10 mol) were dissolved in 60 ml of dimethylformamide and heated at 90 C for 4 hours. The reaction solution was poured into ice water and extracted with ether. The ; resulting ether solution was extracted with 10% sodium hydroxide and the resluting aqueous solution was neutralized with 10% HCl solution. The neutralized solution was extracted with ether, and the ether solution was washed with water and dried. The solvent was distilled off and the residue was recrystallized from benzene-toluene to obtain 3-methyl-N[(3-methylphenyl)acetyl]anthranilic acid 4.8 9 (yield: 49~).
The resulting compound 5.1 9 (0.02 mmol) was mixed with polyphosphoric acid 200 9 and heated at 120 C for 2 ., ~; hours. After heating, the reaction mixture was poured into I5 ice water. The resulting solution was neutralized with an aqueous solution saturated with potassium hydrogencarbonate and deposited crystals were collected by filtration to obtain a mixture of 1, 10-dimethyl-6,11-dihydroindolo[3,2-, b]-quinoline-6-one and 3, 10-dimethyl-6,11-dihydroindolo[3,2-b]-quinoline 6-one (3.9 g (yield: 8~.5~)).
The resulting mixture 3.8 g (5 mmol) was added to phosphorus oxychloride 20 ml and heated under reflux for 2 ~ hours. Unreacted phosphorus oxychloride was distilled off - under the reduced pressure, and the residue was poured into ice water and neutralized with 10~ potassium hydrogencarbonate solution. Then the neutralized solution was subjected to extraction with ethylacetate. The ~. ' ' Z0()6666 resulting ethylacetate solution was washed with an aqueous solution saturated with NaCl and dried with MgSO~, and the solvent in the dried solution was distilled off. Thus obtained residue was subjected to silica gel column chromatography and separated with hexane (eluent) to obtain 6-chloro-1,10-dimethylindolo[3,2-b]quinoline 620 mg (yield:
15~) and 6-chloro-3,10-dimethylindolol3,2-b]quinoline 560 mg (yield: 14%).
The resulting 6-chloro-1,10-dimethylindolo[3,2-b]quinoline 400 mg (1.43 mmol) and 4-amino-3-methoxyanilinemethanesulfonaminde 340 mg (1.5 mmoll were dissolved in 6 ml of ethoxyethanol. Two drops of conc.
hydrochloric acid were added to this solution and heated under reflux for 3 hours. After cooling, precipitate was collected by filtration to obtain the objective compound (hydrochlorate) 450 mg (yiled : 63%).
Melting point: 202 to 205C
I R v N U I I ~ - I 1320, 1150 ~ . ,~
NMR ( CF, COOD ) 2.98(3H, s, CH,) 3.12(3H, s, CH3) 3.47(3H, s, SO,CH,) 3.95(3H, 9, OCH~) 7.05-8.03(10H, m, aromatic H, NH) ; 8.38-8.S5(1H, m, aromatic H ) Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-' , methoxyanilino)-3,10-dimethylindolo[3,2-blquinoline:
cu ~
NH HC~
~ ~ OCH, NH- SO.CH9 6-Chloro-3,10-dimethylindolo[3,2-b~quinoline 560 mg (1.43 mmol) obtained in Example 10 and 4-amino-3-methoxyanilinemethanesulfonaminde 340 mg (1.5 mmol) were dissolved in 6 ml of ethoxyethanol. Two drops of conc.
hydrochloric acid were added to this solution and heated under reflux for 3 hours. After cooling, precipitate was collected by filtration to obtain the objective compound (hydrochlorate) 420 mg (yield : 59%).
Melting point: 198 to 200~C
R i~ Nuiol cm~l 1320, 1150 m~ I .
NMR(CF,COOD) 2.54(3H, s, CH3) 2.93(3H, s, CH3) 3.39(3H, s, SO,CH3) ~00~.6~,6 3.98(3H, s, OCH,) 7.14-7.96(9H, m, aromatic H, NH) 8.16-8.47(2H, m, aromatic H ) Synthesis of hydrochlorate of 2-chloro-6-(4-methanesulfonamide-2-methoxyanilino)indolol3,2-b]quinoline:
10 /[~C,Q\
NH
~ C~ ce NH-SO,CH, N(chloroacetyl)anthranilic acid 3.2 9 (0.02 mol) and p-chloroaniline 3.95 9 (0.00S mol) were dissolved in 4 ml of dimethylformamide and heated at 80 to 90 C for 4 hours.
The reaction solution was poured into ice water and deposited crystals were collected by filtration. These crystals were washed with ether and recrystallized from ethanol to obtain N-[(4-chlorophenylamino)acetyl~-anthranilic acid 2.2 g (yield: 72.2%).
The resulting compound 2.28 9 (7.52 mmol) was mixed with polyphosphoric acid 75 9 and heated at 120 DC for 2 Z006~i66 hours. After heating, the reaction mixture was poured into ice water and deposited crystal~ were collected by filtration to obtain 2-chloroindolo[3,2-bl-6,11-dihydroquinoline-6-one 1.6 g (yield: 80%).
The resulting compound 1.34 9 (5 mmol) was added to phosphorus oxychloride 10 ml and heated under reflux for 3 hours. An excess amount of phosphorus oxychloride was distilled off, and the residue was poured into ice water and neuralized with potassium hydrogencarbonate. Then the neutralized solution was subjected to extraction with chloroform. The resulting chloroform solution was washed with an aqueous solution saturated with NaCl and dried with anhydrous MgSO., and the solvent in the dried solution was distilled off. Thus obtained residue was recrystallized from chloroform-methanol to obtain 2,6-dichloroindolo[3,2-b]-quinoline (melting point: 221 to 222C ) l.1 9 (yie}d: 74%).
This compound 861 mg (3.01 mmol) and 4-amino-3-methoxyanilinemethanesulfonaminde 680 mg (4.5 mmol) were dissolved in 8 ml of ethoxyethanol. TwO drops af conc.
hydrochloric acid were added to this solution and heated under reflux for 3 hours. After cooling, deposited orystals were collected by filtration to obtain the objective compound ~hydrochlorate) 1.01 mg (yiled : 60%).
Melting point: 203.5 to 204C (decomp.) I R ~ Nu~ol cm~~ : 3360, 1320, 1150 m I
NMR(DMSO-d~) ~
2qo6666 3.06(3H, s, SO,CH3) 3.52(3H, s, OCH,) 7.01-7.80(7H, m, aromatic H ) 8.11-8.38(2H, m, aromatic H ) 8.61-8.70~1H, m, NH) 10.04-10.13(1H, m, NH) 10.51-10.72(1H, m, NH) Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-methoxyanilino)-2-methylindolo[3,2-b]quinoline:
~ r~
NH
~ ~ CU, ~ . NC8 NHSO,CH3 N(chloroacetyl)anthranilic acid 3.2 9 ~0.02 mol) and p-toluidine 3.4 9 (0.005 mol) were dissolved in 4 ml of dimethylformamide and heated at 90 C for 3 hours. The reaction solution was poured into ice water and deposited crystals were collected by filtration. These crystals were washed with ether and recrystallized from ethanol to obtain N-[(4-methylphenylamino)acetyl]anthranilic acid 2.6 g (yield: 70%).
The resulting compound 2.1 9 (7.02 mmol) was mixed with polyphosphoric acid 70 g and heated at 120C for 2 hours. After heating, the reaction mixture was poured into ice water and deposited crystals were collected by filtration to obtain 2-methylindolo~3,2-b~-6,11-dihydroquinoline-6-one 1.2 g (yield: 80~).
This compound 1.1 g (4 mmol) was added to phosphorus oxychloride 8 ml and heated under reflux for 3 hours. An excess amount of phosphorus oxychloride was distilled off, and the residue was poured into ice water and neutralized with potassium hydrogencarbonate. Then the neutralized solution was subjected to extraction with chloroorm. The resulting chloroform solution was washed with an aqueous solution saturated with NaCl, dried with anhydrous MgSO, and the solvent in the dried solution was distilled off. Thus obtained residue was recrystallized from chloroform-methanol to obtain 2-mehyl-6-chloroindolo~3,2-b]quinoline (melting point: 201 to 203 C ) 1.2 g (yield: 66%).
The resulting compound 660 mg (2.51 mmol) and 4-amino-3-methoxyanilinemethanesulfonaminde 560 mg ~2.6S mmol ) were dissolved in 8 ml of ethoxyethanol. Two drops of conc.
hydrochloric acid were added to this solution and heated under reflux for 2 hours. After cooling, deposited crystals were collected by filtration and recrystallized from methanol to obtain the objective compound Z0~6666 (hydrochlorate) 870 mg (yiled : 72%).
Melting point: 214 to 217C
'H-NMR(DMSO-d,) 2.48(3H, s, CH,) 3.05~3H, 5, SO.Me ) 3.56(3H, s, OCH,) 6.85-7.50~7H, m, aromatic H ) 8.05-8.46(3H, m, aromatic H ) 9.71-9.82(1H, m, NH) 10.24-10.30tlH, m, NH) 10.98-11.10(lH, br, NH) Synthesis of hydrochlorate of 6-(4-methoxycarbamoyl-2-methoxyanilino)indolo[3,2-b]quinoline:
NH
~ 3"OC~ IICQ
NH-COOCH, Hydrochlorate of 4-methoxycarbamoyl-2-methoxyaniline 3.3 g lsynthesized by the method of Rewcastle et al. (Jounal of Medical Chemistry(1987) vol. 30, 1576-1581)] and 6-.
chloroindoloj3,2-b]quinoline 3.0 g (12 mmol) were dissolved in 35 ml of ethoxyethanol and heated under reflux for 4 hours. After cooling, deposited crystals were collected by filtration and washed with ether and chloroform. Thus obtained crystals were added to CHICN-KHCO3 solution and to this solution, a large amount of water was added and deposited crystals were collected by filtration. The~e crystals were recrystallized from methanol and dichloromethane to obtain the objective compound 3.3 g (yield : 67~).
Melting point: 178 to 181 C
I R NU 1 I cm~~: 3390, 1716 .. ~
NMR(DMSO- d,) 3.71~ 3.75(6H, each s, OMe X 2) 6.85-7.10(2H, m, aromatic H) 7.10-8.02(6H, m, aromatic H) 8.02-8.72(3H, m, aromatic H) 9.72(1H, br, NH) 11.03(1H, br, -NH) Synthesis of hydrochlorate of 6-~4-acetoamino-2-methoxyanilino)indolol3,2-b]quinoline:
200~666 NH
[~ocn~ uce NH-COCH, 6-(4-Methoxycarbamoyl-2-methoxyanilino)indolo[3,2-b]-quinoline obtained in Example 14 was dissolved in methanesulfonic acid S ml in a stream of argon. Then dimethylsulfide 0.37ml was added dropwise to this solution in an ice bath and stirred at room temperature for one day.
After reaction, the solution was neutralized with potassium hydrogencarbonate in a stream of argon and etracted with ethyl acetate. The resulting ethyl acetate solution was washed with water, dried with anhydrous MgSO~
and the solvent was distilled off to obtain 6-(4-amino-2-methoxyanilino)indolo~3,2-b]quinoline. This compound was dis610ved in acetic anhydride 0.27 ml/acetic acid 5 ml without purification andjreacted by adding gradually with zinc powder 250 mg. After agitation for one hour, the reaction solution was added with water and neutralized with potasisum hydrogencarbonate. Deposited precipitate was collected by filtration and dissloved in methanol. After ` Z00~i666 addition with hydrochloric acid, the resulting methanol solution was concentrated under the reduced pressure to obtain the objective compound (hydrochlorate) 330 mg (yield: 76~).
Melting point: 168 to 173C
I R NuJo~ cm~~: 1650 0- .
NMR(CF.COOD + CDCQ ,) ~ :
2.36(3H, 8, -COCH,) 3.87(3H, s, -OCH,) 6 . 94-8.44(14H, m, aromatic H, NH) ExAMeLE 16 Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-methoxyanilino)-1-mehtylindolol3,2-blquinoline:
CH
H
NH
~ ~ OC I ~ ~CQ
NH-SO,CH3 N(chloroacetyl)anthranilic acid 6 . 4 g (15 mmol) ~synthesized from anthranilic acid by the same procedures as those of Example 9) and m-toluidine 9.5 ml (0.09 mol) were dissolved in 60 ml of dimethylformamide and heated at ' 80 to 90 ~C for 4 hours. The reaction mixture was poured into ice water and extracted with ether. The resulting ether solution was extracted with 10~ sodium hydroxide and the resulting aqueous solution was neutralized with 10% HCl solution. The neutralized solution was extracted with ether, and the ether solution was washed with water and dried. The solvent of dried solution was distilled off and the residue was recrystallized from benzene-hexane to obtain Nl(3-methylphenyl)acetyllanthranilic acid 4.7 9 (yields 57%).
The resulting compound 5.0 g (0.02 mmol) was mixed with polyphosphoric acid 176 9 and heated at 120 C for 2 hours. After heating, the reaction mixture was poured into ice water. The resulting solution was neutralized with an aqueous solution saturated with potassium hydrogencarbonate and deposited crystals were collected by filtration to obtain a mixture of 1-methyl-6,11~dihydroindolo[3,2-b~-quinoline-6-one and 3-methyl-6,11-dihydroindolo[3,2-b]-quinoline-6-one ~4.1 9 (yields 83%)).
The resulting mixture 4.1 9 (16 mmol) was added to phosphorus oxychloride 20 ml and heated under reflux for 2 hours. Unreacted phosphorus oxychloride was distilled off under the reduced pressure, and the residue was poured into ice water and neutralized with an aqueous solutin saturated ;20066~,6 with potassium hydrogencarbonate. Then the neutralized solution was subjected to extraction with ethyl acetate.
The resulting ethyl acetate solution was washed with an aqueous solution saturated with NaCl, dried with MgSO4 and the solvent in the dried solution was distilled off. Thus obtained residue was subjected to silica gel column chromatography and separated with hexane ~eluent) to obtain 6-chloro-1-methylindolol3,2-blquinoline (melting point: 170 to 172C ) 450 mg ~yield: 10%) and 6-chloro-3-methylindolo[3,2-b]quinoline (melting point: 193 to 194C ) 380 mg (yield: 8.4~).
The resulting 6-chloro-1-methylindolol3,2-b]o3uinoline 400 mg (l.S1 mmol) and 4-amino-3-methoxyaniline methanesulfonaminde 360 mg (1.75 mmol) were dissolved in 6 ml of ethoxyethanol. Two drops of conc. hydrochloric acid were added to this solution and heated under reflux for 3 hours. After cooling, precipitate was collected by filtration to obtain the ob~ective compound (hydrochlorate) 520 mg (yield : 71%).
Melting point: 214 to 217C
NMR(CFlCOOD) ~ :
3.06(3H, s, CH,) 3.33(3H, s, SO,CH3) 3.73(3H, s, OCH3) 7.08-7.46(7H, m, aromatic H, NH) 7.60-8.56(6H, m, aromatic H) Synthesis of hydrochlorate of 6-(4-methanesulfoneamide-2-methoxyanilino)-3-mehtylindolo[3,2-b]quinoline:
~ cn,~
NH
~ ~ CH, J Nce NH-SO,CH3 6-Chloro-3-methylindolo[3,2-b]quinoline 350 mg t1.31 mmol) obtained in Example 16 and 4-amino-3-methoxyaniline methanesulfonaminde 310 mg (1.42 mmol) were dissolved in 6 ml of ethoxyethanol. Two drops of conc. hydrochloric acid were added to this solution and heated under reflux for 2 hours. After cooling, precipitate was collected by filtration to obtain the objective compound (hydrochlorate) 430 mg (yield : 68%).
Melting point: 215 to 217 C
NMR(CF,COOD ) ~ :
2.48(3H, s, CH,) 3.38(3H, s, SO,CHl) 3.95(3H, s, OCHI) 7.07-7.50(6H, m, aromatic H, NH) 7.60-8.47t7H, m, aromatic H, NH) ... , . . .. . . , . . .. ... ~. .. . .. . . ~ . . . . . , Synthesis of 6-(4-methanesulfonamide-2-methoxyanilino)-2-nitroindolol3,2-blquinoline:
5 ~/110, NH
~
NHSOa CH, Fuming nitric acid (d=1.42) was added dropwise to 6-chloroindolol3,2-b]quinoline 2.S2 g (0.01 mol) at 0 C . The resulting mixture was left overnight at room temperature and then poured into ice water. Deposited crystals were collected by filteration, washed with an aqueous solution saturated with KHCO1 and recrystallized from tetrahydrofuran and CH~ Cl~ to obtain 6-chloro-2-nitroindolol3,2-b]quinoline (melting point: 280 to 290C
(decomp.)) 2.50 g (yield: 84%).
This compound 5.9 g (0.02 mol) and 4-amino-3-methoxyanilinemethanesulfonaminde hydrochlorate 6 g (0.024 ; mol) were dissolved in 10 ml of ethoxyethanol and heated ~ under reflux for 6 hours. After cooling, precipitate was collected by filtration and added to chloroform. This chloroform was neutralized with an aqueous solution saturated with KHCO3 and then chloroform was distilled off.
Z0~66~i6 The residue was recrystallized from methanol to obtain the objective compound 6 g ~yield : 61~).
Melting point: 300 C or more MS m/e 478 (M~ ) Synthesis of hydrochlorate of 2-fluoro-6-(4-methanesulfonamide-2-methoxyanilino)indolo[3,2-b]quinoline:
I ~ ~ ~ F
NH
15 ~ OC~ ~C~
N(chloroacetyl)anthranilic aaid 4.0 g (8 mmol) and p-fluoroaniline 5.3 ml (56 mmol) were dissolved in 4 ml of dimethylformamide and heated at 80 to 90C for 4 hours. The reaction solution was poured into ice water and deposited crystals were collected by filtration. These crystals were washed with ether and recrystallized from ethanol to obtain N-[(4-fluorophenylamino)acetyllanthranilic acid (melting point: 217 to 219 C ) 2.4 g (yield: 46~).
The resulting compound 2.26 g (7.5 mmol) was mixed 2~066~6 with polyphosphoric acid 75 g and heated at 120C for 2 hours. After heating, the reaction mixture was poured into ice water and deposited crystals were collected by filtration to obtain 2-fluoromethylindolol3,2-bl-6,11-dihydroquinoline-6-one 1.35 g.
The resulting compound 1.0 g was added to phosphorus oxychloride 10 ml and heated under roflux for 3 hours. An excess amount of phosphorus oxychloride was distilled off.
The residue was poured into ice water, neutralized with potassium hydrogencarbonate and deposited crystals were collected by filtration. The crystals were subjected silica gel column chromatography to obtain 6-chloro-2-fluoroindolol3,2-b]quinoline (melting point: 201 to 204 C ) 470 mg (yield: 43%).
This compound 400 mg (3.01 mmol) and 4-amino-3-methoxyanilinemethanesulfonaminde 400 mg (1.6 mmol) were dissolved in 10 ml of ethoxyethanol and heated under reflux for 3 hours. After cooling, deposited crystals were collected by filtration to obtain the objective compound (hydrochlorate) 660 mg (yiled : 95~).
Melting point: 260 C (decomp.) I R ~ N~iol cm l 1150, 1318tSOICH3), 3250~NH,) m~ -NMR(DMSO- d6) ~ :
3.12(3H, s, CH3) 3.66(3~, s, C~3) 6.80-8.02(10H, m, aromatic H ) Synthesis of hydrochlorate of 6-(4-hydroxy-2-methoxyanilino) indolol3,2-blquinoline:
5 [~
NH
,o ~ ~ c~ ce OH
1.4 9 (8.3 mmol) of 4-hydroxy-2-methoxyaniline hydrochlorate synthesized by the method of J. L. Jurlina et al. [J. Med. Chem., 19B7, Vol. 30, No.3] and 6-chloroindolol3,2-blquinoline 1.75 9 (6.9 mmol) were dissolved in 10ml of ethoxyethanol and heated under reflux for 4 hours. Deposited crystals were collected by20 filtration and washed with ether to obtain the objective compound ~hydrochlorate) 1.8 g (yield: 78%).
Melting point~ 259 to 263 C (decomp.) 'H-NNR(CF3COOD) ~
3.91(3H, s, OCH,) 7.10-8.54(14H, m, aromatic H, NH) Synthesis of 6-(4-aceto-2-methoxyanilino)indolol3,2-~0~)~i666 b]quinoline:
H
NH
OCOCH, 600 mg (1.5 mol) of hydrochlorate of 6-(4-hydroxy-2-methoxyanilino)indolol3,2-b]quinoline obtained in Example 20, anhydrous K, C03 2.1 g and acetic anhydride 0.46 ml were dissolved in 90 ml of dimethylformamide and agitated at room temperature for 1.5 hours. The reaction solution was poured into ice water, and deposited crystals were collected by filtration and recrystallized from tetrahydrofuran and CH, Cl2 to obtain the objective compound 510 mg (yield: 77%).
Melting point: 224 to 230 C (decomp.) 'H-NMR(CF,COOD) ~ :
2.S6(3H, B, COCH,) 3.95(3H, s, OCH3) 6.90-8.61(13H, m, aromatic H, NH) Synthesis of 2-amino-6-(4-methanesulfonamide-2-methoxyanilino)indolol3,2-b]quinoline ~ NH2 NH
NHSO,CH, 6-(4-Methanesulfonamide-2-methoxyanilino)-2-nitroindolol3,2-blquinoline 2 g (3.6 mmol) obtained in Example 18 was dissolved in 150 ml of acetic acid. 10% Pd-C 50 mg was added to this solution and the above compound was reduced by hydrogen for 5 hours. After removal of Pd-C, acetic aoid was distilled off, and the residue was neutralized with an aqueous solution saturated with KHCO9 and extracted with chlorofornl. The resulting chloroform solution was washed with an aqueous solution saturated with NaCl, dried with anhydrous MgSO~ and the solvent was distilled off. The residue was recrystallized from mehtanol and dichloromethane to obtain the objective compound 1.36 g (yield: 78%).
Melting point: 251 to 256 ~C (decomp.) Acetate ~ H-NMR(CF. COOD) Z00666~
2.23(3H, S, CH3CO) 3.32(3H, s, SO,CH,) 3.96~3H, s, OCN,) 7.12-8.46~14H, m, aromatic H, NH) Synthesis of N- (4-l(7-(2,3,4, 6-tetra-O-acetylglycosyl-1-amino)-1 OH-indolo[3, 2-blquinoline-11-yl)amino 1-3-methoxyphenyl) methanesulfonamide OAc 0--r H OAc NH
~ OCHg NHSO,CH, 1-sromo-2, 3,4, 6-tetra-O-acetylglucose 450 mg (1 mmol) was dissloved in dried pyridine 1 ml and dried dimethyformamide 10 ml and stirred overnight in an atmosphere of argon. Then, to this solution, dimethylformamide solution containing 240 mg (0.5 mmol) of 2-amino-6-(4-methanesulfonamide-2-methoxyanilino) indolo[3,2-blquinoline obtained in Example 22 was added and reacted for 24 hours at room temperature. The reaction solution was poured into ice water and extracted with chloroform. The solvent was distilled off from the resulting chloroform solution and the residue was subjected to silica gel column chromatography to obtain the objective compound 210 mg (yield: 30~) from the dichloromethane:hexane (1:5) eluate.
Melting point: 172 to 178 C ( decomp.) ' H-NMR(DMSO-d, ) 2.08(12H, s, COCH, X 4) 2.96(3H, s, SO. CH, ) 4.04(3H, s, OCH, ) 4.16-4.64(3H, m, 4' -H, CH,OAc) 5.11-5.39(2H, m, 2' -H, 3' -H) 5.71-6.00(1H, m, 5' -H) 6.48-6.68(1H, m, 1' -H) 7.14-7.79(10H, m, aromatic H, NH) 8.09-8.74(3H, m, aromatic H) ExAMeLE 24 Synthesis of N- (4-l (7-(glycosyl-1-amino)-10H-indolol3,2-blquinoline-11-yl)amino]-3-methoxyphenyl) methanesulfonamide 200fi666 r~
O
~( ~ N~
H OH
NH
.
I0 NHSO.CHl 120 mg ~0.14 mmol) of N- ~4-[~7-(2,3,4,6-tetra-O-acetylglycosyl-1-amino)-10H-indolo[3,2-blquinoline-11-yl) amino]-3-methoxyphenyl~ methanesulfonamide obtained in Example 23 was dissolved in methanol 20 ml and an aqueous ammonium solution (NH, H,O) 20 ml. The resulting solution was agitated for 3 days and during this agitation, ammonia was added to this solution every 3 hours. The reaction solution was neutralized with 10% aqueous acetic acid solution and methanol was distilled off from the neutralized solution. Deposited crystals were collected by filtration and recry~tallized from methanol and dichloromethane to obtain the objective compound 75 mg (yield: 87~)~
Melting point: 201 to 205 C (decomp.) lH-NMR(CD3OD+ DMSO-d~) 2.96(3H, s, SO,CH,) 3.73(2H, s, CH,OH ) 4.04(3H, s, OCH,) 4.55(6H, m, 4 ' -H, 5' -H and OH X 4) 5.03-5.12(2H, m, 2' -H and 3' -H) 6.36-6.52(1H, m, 1' -H) 6.58-6.64(1H, m, aromatic H) 7.14-7.79~10H, m, aromatic H, NH) 7.94-8.56(3H, m, aromatic H) Synthesis of 2-methylcarbamoyl 6-(4-methanesulfonamide-2-methoxyanilino)indolo[3,2-blquinoline UNCOCU.
NH
OCH, NHSO~CH~
500 mg (1.1 mmol) of 2-amino-6-(4-methanesulfonamide-2-methoxyanilino)indolo[3,2-blquinoline obtained in Example 22 was dissolved in dried pyridine 10 ml and acetic anhydride 2 ml and heated at 80 to 90C for 6 hours. The reaction solution was poured into ice water and extracted with chloroform. The resulting chloroform solution was washed with water and dried with anhydrous MgSO,. The solvent was distilled off and the residue was recrystallized from tetrahydrofuran and dichlromethane to obtain the objective compound 470 mg ~yield: 75%) Melting point: 223 to 226 C (decomp.) H-NMR(CF,COOD) ~
2.08(3H, s, COCH,) 3.28(3H, s, SO.OH,) 3.80(3H, s, OCH,) 7.08-7.86(9H, m, aromatic H, NH) 7.89-8.48~5H, m, aromatic H, NH) Synthesis of hydrochlorate of 2-methanesulfonamide-6-(4-methanesulfonamide-2-methoxyanilino)indolol3,2-b]quinoline 1 5 ~ 0, C
NH
,oc~ IIC~
NH-SO, CH, 500 mg (1.1 mmol) of 2-amino-6-(4-methanesulfonamide-2-methoxyanilino)indolo[3,2-b]quinoline obtained in Example 22 was dissolved in dried pyridine 10 ml and to this solution, CH,SO,Cl 132 mg (1.05 equivalent) was added dropwise at 0 C . After addition, the reaction solution was agitated for 3 hours and poured into ice water. Deposited crystals were collected by filtration and recrystallized from chloroform and methanol to obtain the objective compound 520 mg (yield: 90%).
Melting point: 251 to 255 ~ (decomp.) 'H-NMR(CF,COOD) ~
2.90(3H, s, 7-NHSO,CH3) 3.31(2H, 5, 4' -NHSO,CH,) 3.82(313., s, OC~I,) 7.01-7.25(3H, m, aromatic H) 7.25-7.99(8H, m, aromatic H, NH) 8.02-8.41(3H, m, aromatic H) Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-methoxyanilino)-10-methylbenzofuranol3,2-b]quinoline ~0~
NH
~oc~l J~c~
NH-SO,CH3 3-Methylanthranilic acid 5 g (33 mmol) ~as dissolved in 10% aqueous sodium hydroxide solution 27 ml and to this 200~666 solution, phenoxyacetyl chloride 6.2 g (36 mmol) was added dropwise at C . The resulting solution was stirred at room temperature for 1 hour and acidified with 10%
hydrochloric acid solution. Deposited crystals were collected by filtration, washed with water and recrystallized from ethanol to obtain 3-methyl-N-(phenoxyacetyl)anthranilic acid (melting point: 174 to 176 C) 4.4 g (yield: 47%).
This compound 7.6 g (27 mmol) was mixed with polyphosphoric acid 60 g and heated with stirring at 120 to 130C for 1.5 hours. The reaction mixture was poured into ice water and neutralized with potassium hydrogencarbonate.
Deposited crystals were collected by filtration to obtain 10-methyl-6,11-dihydrobenzofuranol3,2-b]quinoline-6-one 5.0 g (yield: 74%). Then, this compound 5.0 g was added to phosphorus oxychloride 50 ml and heated under reflux for 1 hour. Unreacted phosphorus oxychloride was distilled off under the reduced pressure, and the residue was neutralized with an aqueous KOH solution and extracted with chloroform.
The resulting chloroform solution was washed with water and dried, and then the solvent was distilled off. The residue was recrystallized from benzene to obtain 6-chloro-10-methylbenzofurano[3,2-blquinoline (melting point: 137 to 139 C ) 4.1 g (yield: 54~).
This compound 1.8 9 (5.0 mmol) and 4-amino-3-methoxyanilinomethanesulfonamide 1.6 g (7.4 mmol) were dissolved in 15 ml of ethoxyethanol and heated under reflux for 15 hours. Deposited crystals were collected by filtration and washed with ether to obtain the objective compound ~hydrochlorate) 0.8 9 (yield: 36%).
Melting point: 25S to 2S9C
I R ~ ~U~O~ cm~~: 1640~S=O), 3300(NH) m~ ~
H-NMR (CDC~ 9 + DMSO-d,) ~ s 2.96(6H, s, 4-CH3, SO,CH,) 3.93(3H, s, OCH,) 6.70-6.95 ~ 7.18-7.75 ~ 8.S5-8.95(12H, m, aromatic H, NHX 2) Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-methoxyanilino)-1,10-dimethylbenzofurano[3,2-b]quinoline CH, CH, ~ ' T [~ i NH
~ ~ ocn ,,~ ~ NCQ
NH-SO~CH3 3-Methylanthranilic acid 1.0 9 (6 mmol) was dissolved in 10% aqueous sodium hydroxide solution 27 ml and to this soulution, 2-methylphenoxyacetyl chloride 1.3 9 ` Z006666 (7.3 mmol) was added dropwise at 0 C . The resulting solution was stirred at room temperature for 5 minutes and acidified with 10~ hydrochloric acid solution. Deposited crystals were collected by filtration, washed with hot water and recrystallized from ethanol to obtain 3-methyl-N-(2-methylphenoxyacetyl)anthranilic acid (melting point: 133 to 136C) 1.7 9 (yield: 83%).
This compound 19.4 9 (65 mmol) was mixed with polyphosphoric acid 650 g and heated with stirring at 120 C
for 2 hours. The reaction mixture was poured into ice water and deposited crystals were collected by filtration to obtain a mixture (6.4 g) of 1,10-dimethyl-6,11-dihydrobenzofuranol3,2-b]quinoline-6-one and 3,10-dimethyl-6,11-dihydrobenzofuranol3,2-b]quinoline-6-one. Then, this mixture 6.4 9 was added to phosphorus oxychloride 25 ml and heated under reflux for 0.5 hours. Unreacted phosphorus oxychloride was distilled off under the reduced pressure, and the residue was poured into ice water and extracted with ethyl acetate. The resulting ethyl acetate solution was dried with anhydrous MgS0,, and then the solvent was distilled off. The residue was subjected to silica gel column chromatography to obtain 6-chloro-1,10-dimethylbenzofurano[3,2-b]quinoline (melting point: 165 to 168C ) 0.9 9 (yield: 14%) and 6-chloro-3,10-dimethylbenzofurano~3,2-b]quinoline (melting point: 164 to 168 C ) 2.2 g (yield: 33 %).
Then, the l,10-dimethyl compound 0.5 9 (1.6 mmol) and Z00~6~;6 4-amino-3-methoxyanilinemethanesulfonamide hydrochlorate 0.5 g (2.0 mmol) were dissolved in 5 ml of ethoxyethanol and heated under reflux for 2 hours. The reaction solution was neutralized with an aqueous solution saturated with KHCO3 and extracted with ethyl acetate. The resulting ethyl acetate solution was dried with anhydrous MgSO, and the solvent was distilled off. The residue was subjected to silica gel column chromatography to obtain the objective compound (hydrochlorate) 0.3 g (yield: 38~).
Melting point: 211 to 213C
I R ~ N`ulol cm~~ 3510, 3300, 1320 .. . Il H-NM~ (CF,COOD) ~ :
2.93(3H, s, CB3 ) 3.15(3H, s, CH,) 3.33(3H, s, SO.CHl) 3.87(3H, s, OCH,) 6.95-8.10(8H, m, aromatic H) 8.15-8.45(1H, dd, J=8.2Hz, aromatic H) Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-methoxyanilino)-3,10-dimethylbenzofurano~3,2-blquinoline ~ CH, 5 ~[~\Cil-NH
~ ,OCN, ~ ce NHSO, CH9 0.35 9 (1.2 mmol) of 6~chloro-3,10-dimethyl-benzofuranol3,2-b]quinoline obtained in Example 28 and 4-amino-3-methoxyanilinemethanesulfonamide hydrochlorate 0.4 g (1.8 mmol) were dissolved in 5 ml of ethoxyethanol and heated under reflux for 6 hours. After cooling, deposited crystals were collected by filtration and washed with ethanol to obtain the objective compound 0.4 g (yield: 61%).
Meltign point:l79 to 184C
'H-NMR (CF,COOD) 2.59(3H, s, CH, ) 2.87~3H, S, CH, ) 3.28(3H, s, SO,CH,) 3.84(3H, s, OCH~) 7.00-8.27(9H, m, aromatic H) Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-,.
.
:' :
Z0066fi6 methoxyanilino)-1-methylbenzofurano[3,2-blquinoline . CH, \
NH
~ ~ OC~ Ce NH-SO,CH, Anthranilic acid 7.95 g (58 mmol) was dissolved in 10%
aqueous sodium hydroxide solution 48 ml and to this 15 solution, 3-methylphenoxyacetyl chloride 11.8 g (64 mmol) was added dropwise at C . The resulting solution was stirred at room temperature for 5 minutes and acidified with 10% hydrochloric acid solution. Deposited crystals were collected by filtration and washed with hot water to obtain N-(3-methylphenoxyacetyl)anthranilic acid 14.0 g (yield:
68%).
This compound 14.0 9 (44 mmol) was mixed with polyphosphoric acid 467 9 and heated with stirring at 120 ~C
for 2 hours. The reaction mixture was poured into ice water, and deposited crystals were collected by filtration and washed with 10 % KHC09 solution and water to obtain a mixture (6.S g) of 1-methyl-6,11-dihydrobenzofuranol3,2-~006666 b]quinoline-6-one and 3-methyl-6,11-dihydrobenzofuranol3,2-blquinoline-6-one. Then, this mixture 6.5 9 was added to phosphorus oxychloride 20 ml and heated under reflux for 1 hour. Unreacted pho~phorus oxychloride was distilled off under the reduced pressure, and the residue was poured into ice water and neutralized with an aqueous solution saturated with KHCO.. Deposited crystals were collected by filtration and washed with water~. Thus obtained crystal~
were subjected to silica gel column chromatography to obtain 6-chloro-1-methylbenzofurano[3,2-blquinoline (melting point: 169 to 172 C ) 0.48 g (yield: 4%) from the hexane eluate and 6-chloro-3-methylbenzofurano~3,2-b]quinoline 3.42 ~ (yield: 26%) from the next eluate (~exane:ethyl acetate = 8:1).
~rhen, the l-methyl compound 0.45 9 (1.6 mmol) and 4-amino-3-methoxyanilinemethanesulfonamide 0.44 g (1.7 mmol) were dissolved in 5 ml of ethoxyethanol and heated under reflux for 3.3 hours. Deposited crystals were collected by filtration and washed with ethanol to obtain the objective compound (hydrochlorate) 0.6 g (yield: 76%), Melting point: 2S3 to 255 C
I ~ ~ N~ol cm~~ 3510, 3300, 1320 'H-NMR (DMSO-d6) ~ :
3.00(6H, s, CH3, SO,CH,) 3.69(3H, s, OCH,) 6.98-8.47(12H, m, aromatic H, NH) 20(~66~i6 Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-methoxyanilino)-3-methylbenzofuranol3,2-b]quinoline ~ ~ ~ C~.
NH
~ ,OCHJ ~ce NHSO,CH3 6-Chloro-3-methylbenzofuranol3,2-b]quinoline (0.4 g (1.6 mmol)) obtained in Example 30 and 4-amino-3-~ethoxyanilinemethanesulfoniamide hydrochlorate 0.44 g (1.7 mmol) were dissolved in 5 ml of ethoxyethanol and heated under reflux for 2 hours. Deposited crystals were collected by fil~ration and washed with ethanol to obtain the objective compound 0.64 g (yield: 81%).
Melting point: 213 to 215 C
H-NMR (DMSO-d.) ~ :
2.45~3H, s, CH,) 3.00(3H, s, SO,CHI) 3.65(3H, s, OCH3) 6.8S-8.20(10H, m, aromatic H) Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-~0~!666~
methoxyanilino)-10-methylbenzothieno[3,2-b]quinoline CH, \
' NH ~ 8C~
~ OCH9 NH-SO~CH, senzenethiol and butyl bromoacetate were reacted by a conventional method and then hydrolyzed to obtain a -phenylthioacetatic acid. a -phenylthioacetatic acid was reacted wlth thionyl chloride by a convention method to obtain a -phenylthioacetyl chloride. 3-Methylanthranilic acid 59 (33 mmol) was dissolved in 10% aqueous sodium hydroxide solution 27 ml and to thiq solution, a -phenylthioacetyl chloride 5.5 ml (33 mmol) was added dropwise at C . The resulting solution was stirred at room temperature for 1 hour and neutralized with 10~
hydrochloric acid solution. Deposited crystals were collected by filtration and recrystallized from ethanol and water to obtain 3-methyl-N-(phenylthioacetyl)anthranilic acid (melting point: 148 to 150 ~C) 8.8 g (yield: 89%).
This compound 4.6 g (15 mmol) was mixed with polyphosphoric acid 30 9 and heated with stirring at 120 to 130C for 2 hours. The reaction mixture was poured into ice water and neutralized with potassium hydrogencarbonate.
Deposited crystals were collected by filtration and washed with water to obtain 10-methylbenzothienol3,2-b]-6,11-dihydroquinoline-6-one 4.2 g (yield: 90~).
Then, this compound 4.2 g was added to phosphorus oxychloride 50 ml and heated under reflux for 2.5 hours.
Unreacted phosphorus oxychloride was distilled off under the reduced pressure, and the residue was poured into ice water, neutralized with an aqueous XHO solution and extracted with chloroform. The resulting chloroform solution was washed with water and dried, and then the solvent was distilled off. The residue was recrystallized from benzene to obtain 6-chloro-10-methylbenzothieno[3,2-blquinoline (melting point: 143 to 146C ) 4.1 9 (yield: 84 % ) .
Then, this compound 1 9 (3.7 mmol) and 4-amino-3-methoxyanilinemethanesulfonamide 1.2 9 (4.4 mmol) were dissolved in 12 ml of ethoxyethanol and heated under reflux for 1.5 hours. Deposited crystals were collected by filtration, stirred in chloroform with KHCO9 and extracted with chloroform. The resulting chloroform solution was dried with anhydrous MgSO, and the solvent was distilled off. The residue was recrystallized from acetone to obtain the objective compound (hydrochlorate) 0.8 g (yield: 48~).
Melting point: 220 to 223 C
Z0066~6 I R v N~l~l cm~~: 3400, 3250, 1320 m- ~
H-NMR (DMSO-d~
3.11(3H, s, 4-CH3) 3.28(3H, s, SO.CH,) 3.66(3H, s, OCH,) 6.63-8.70~12H, m, aromatic H, NHX 2) Synthesis of hydrochlorate of 6-(4-methane~ulfonamide-2-methoxyanilino)-l-methylbenzothienol3,2-b]quinoline NH ~ HC~
~o~ J
NH-SO,CH3 ~ ~
3-Methylbenzenethiol and butyl bromoacetate were reacted by a conventional method and then hydrolyzed to obtain 3-methyl-a -phenylthioacetatic acid~ 3-Methyl-a -phenylthioacetatic acid was reacted with thionyl chloride25 by a conventional method to obtain 3-methyl-a -phenylthioacetyl chloride. Anthranilic acid S.6 g (41 mmol) was dissolved in 10% aqueous sodium hydroxide solution 32 ml and to this solution, 3-methyl-a -phenylthioacetyl chloride (99C /3.3 mmHg) 8.9 g was added dropwise at 0C .
The resulting solution was stirred at room temperature for 20 minutes and neutralized with 10% hydrochloric acid solution. To this solution, ether was added, and deposited crystals were collected by filtration and washed with hot water to obtain N-(3-methylphenylthioacetyl)anthranilic acid ~melting point: 148 to 150 C) 11.2 g tyield: 25~).
This compound 15.8 g (50 mmol) was mixed with polyphosphoric acid 500 g and heated with stirring at 120 C
for 2 hours. The reaction mixture was poured into ice water and neutralized with an aqueous potassium hydrogencarbonate solution. Deposited crystals were collected by f iltration and washed with water to obtain crude 1-methylbenzothieno[3,2-b]-6,11-dihydroquinoline-6-one 10.5 g.
Then, this compound 10.5 9 was added to phosphorus oxychloride 50 ml and heated under reflux for 1 hour.
Unreacted phosphorus oxychloride was distilled off under the reduced pressure, and the residue was poured into ice - water, neutralized with an aqueous solution saturated with KHC0~ and extracted with chloroform. The resulting chloroform solution was dried with anhydrous MgS0~, and then the solvent wa~ distilled off. The residue was subjected to silica gel column chromatography to obtain 6-chloro-1-methylbenzothieno[3,2-b]quinoline (melting point: 143 to 146 C ) 0.8 g (yield: 6%).
- 20066fi6 Then, this compound 0.2 g (0.7 mmol) and 4-amino-3-methoxyanilinemethanesulfonamide 0.2 9 (0.8 mmol) were dissolved in 5 ml of ethoxyethanol and heated under reflux for 3 hours. Depo~ited crystals were collected by filtration and washed with ethanol to obtain the objective compound (hydrochlorate) 0.21 g (yield: 60%).
Melting point: 205 to 210 ~C
H-NMR ICF~COOD) ~ :
3.04(3H, 8, CH,) 3.33(3H, 8, SO.CH,) 3.93(3H, s, OCH,) 7.32-9.02(12H, m, aromatic H, NH) Test Example 1: Test for Antitumorigen Function Function for Inhibiting Multiplication of KB Cell (in vitro test) ' KB cells, carcinomatous cell tumors, were transferred to in vitro floatation incubator systems, and added respectively with compounds of Examples 1 to 33. The results of cultivation added with these compounds were compared with the results of the control which was not added with any compound.
~3 Experimental System:
Cell used: KB Cell (Originating from human mouth epidermal cancer) Culture medium: Eagles minimal essential medium (MEM) supplemented with 10% calf serum Cultivation: 37C carbon dioxide gas incubator (5% CO,) ~ Method of Experiment:
Day 0: KB cells were diluted in the culture medium to adjust the KB cell density to 2 x 10'/ml.
Three ml of the cell suspension was inoculated in each of 60 mm plastic dishes.
Two dishes per standard dosage were used.
Day 1: Test compound was added to the medium so that the final concentrations were set to 100, 30, 10, 3 and 1 ~ g/ml.
, Day 4: Cells were scraped off from the dish using trypsin, and the cell number was countered using a Corter counter.
~9 Criteria for Judgements In generally accordance with the ~tipulation~ set forth by the National Cancer Institute ~NCI), U.S.A., the concentration of compound neces~ary for exerting 50% growth inhibition (EDs~) compared to the contral was determined. A
compound was judged as effective when ED~o was less than 4 g/ml.
The results are shown below.
Table l: Results of Test on Carcinostatic Effect (Effect of Inhibiting growth of KB-Cell) _ Compound No. Tested Conc.(ED60)(~ 9/~ ) ¦
l < 0.3 2 < 0.3 4 < 0 3 7_ C 0 3 . 11 ':
Z0~6666 Table 1 (continuation) Compound No. Tested Conc.(ED~0)(~ g/~ ) i 8 < 0.3 9 ~ 0.3 < 0.3 11 < 0.3 12 < 0.3 13 < 0.3 14 < 0.3 < 0.3 16 < 0.3 17 < 0.3 18 < 0.3 , 19 < 0.3 < 0.3 21 < 0.3 22 < 0.3 23 < 0.3 24 < 0.3 < 0.3 26 < 0.3 27 0.38 28 < 0.3 ~' , .
' 20066~6 Table 1 (continuation) ., . Compound No. Tested Conc.(ED~0)(~ g/~ ) . _ . . 29 < 0.3 ;: 30 1.5 ~: 31 < 0.3 ; . 32 1.4 `- 10 33 < 0.3 .~. Reference 0 .~
Test Example 2: Effect on Prolongation of Life Span in ,~ Cancer inplanted Mouse and Acute Toxicity 15 Pharmacological effects of compounds of Examples 1 to . 33 were tested in in vitro systems using P-3B8 implanted mice. The results were compared to that of a control which ll was to added with any compound.
System used in experiment:
:~ ~ 20 Animal used: CDF mouse (6 mice/group) `~ Tumor: P-388 ~ Number of implanted cells: 10' cells/mouse ; Implanted site: i.p.
Day of administration: Day 1 and Day 5 .-: 25 Dosage: LD~o or 400 mgtkg/day at the maximum Criteria for Judgement:
The treatment was judged as effective when the ratio ' , ' . 7 3 .
20066fi6 of survival of the treated group to that of the control group (T/C ~) was 120% or more. The survival period of the control group was generally about 10 days. The results are ~ shown in Table 2.
Table 2: Effect on Prolongation of Life Span of Mouse implanted with P-38 Cancer Cells Compound Dosage (mg / kg~ Ratio of Life No. Tested Prolongation (%) 200240(cure 1/6) 1 100290(cure 1/6) _ 100257(cure 1/6) 12.5 134 ~!
! 400 165 i 200 172 1505 l335 6 200 247(cure 2/6) ' 100 169 'I
20~ 111 ~, 7 100 108 l 50 111 - 25 8 42oo 17558 100 _ 175 !
' Table 2 (continuation) Compound Dosage (mg / kg) Ratio of Life No. Tested Prolongation (%) 305(cure 4/6) 235(cure 1/6) 9 12.5 198 6.25 168 3.12 165 1.56 131 100 260(cure 1/6) 12.5 165 . 6.25 145 3.12 109 . I
315(cure 1/6) 11 25 294(cure 2/6) 12.5 315(cure 1/6) 315(cure 1/6) 12 25 242(cure 1/6) 12.5 231 .
; 12.5 189 l 200 221 I 14 10500 266(cure 1/6) _ 100 240(cure 1/6) ; 16 25 288~cure 2/6) 12.5 240(cure 2/6) . 12.5 153 : 50 70 12.5 164(cure 1/6) . I __ . .
. . .
Table 2 (continuation) Compound Dosage (mg / kg) Ratio of Life No. Tested Prolongation (~) 19 25 252(cure 2/6) 12.5 313(cure 3/6) 131(cure 1/6) 12.5 179 21 50 185(cure 1/6) . 25 17~
242(cure 1/6) 12.5 171 23 25 148(cure 1/6) 12.5 300(cure 2/6) 12.5 213~cure 2/6) _ 12.5 135 _ : 50 143 .
12.5 126 _ 400 310(cure 2/6) . 27 200 250(cure 1/6) i 100 230 . 28 100 269 : 50 204 ..
. 7 6 .
Table 2 (continuation) Compound Dosage ( mg / kg ) Ratio of Life No. Tested Prolongation (%) 29 200 269(cure 1/6) 100 204(cure 1/6) 400 219(cure 1/6) 31 200 175(cure 1/6) 400 280(cure 1/6) 33 200 255(cure 1/6)
can be synthesized by the method shown in Scheme 2.
Anthranilic acid shown by formula (lO) is reacted with chloroacetyl chloride to obtain N(chloroacetyl)anthranilic acid shown by formula (15). This reaction is suitably carried out by heating under reflux in a solvent such as benzene.
Thus obtained compound (15) is reacted with an aniline derivative shown by formula tl6) to obtain an anthranilic acid shown by formula (17). This reaction is suitalby conducted by heating at a temperature from about 50 to 100C
in a solvent such as dimethylformamide.
Compound (17) is reacted with polyphosphoric acid to obtain an indoloquinoline derivative shown by formula (18).
This reaction is suitalby conducted by heating at a temperature from about 100 to 150 C in the presence of excess amount of polyphosphoric acid.
Compound (18) is reacted with phosphorus oxychloride in the presence of phosphorus pentachloride to obtain a chloride of indoloquinoline derivative shown by formula (19). This reaction is suitably carried out by heating preferably at a reflux temperature.
Thus obtained compound (19) i9 reacted with an aniline derivative shown by formula (14) to obtain an indoloquinoline compound represented by formula [Ib]. This reaction can be conducted by heating, preferably at a reflux temperature, in the presence of solvent such as dimethylformamide (DMF), pyridine, ethoxyethanol or dioxane, in an atmosphere of inert gas. The reaction product is optionally purified by a conventional method such as recrystallization. Salts of indoloquinoline compound represented by formula [Ib] can be obtained by addition of an acid such as hydrochloric acid to the reaction solution before, durin~ or after the reaction with the aniline derivative.
Scheme 3: senzothieno _ noline compound (z = S) senzothienoquinoline compounds represented by formula [Ic] can be synthesized by the method shown in Scheme 3.
A thiol derivative shown by formula (20) is reacted with butyl bromoacetate by a conventional method and then hydrolyzed to obtain a -phenythioacetic acid shown by formula (21). Compound (21) is reacted with thionyl chloride by a conventional method to obtain an acetyl chloride shown by formula (22).
Compound (22) is reacted with anthranilic acid shown by formula (lO) to obtain an anthranilic acid derivative shown by formula (23). This reaction can be carried out by dissolving anthranilic acid (10) in an aqueous solution of an alkali hydroxide such as sodium hydroxide, droping compound (22) into this solution and stirring the resulting solution. The droping and stirring are preferably conducted under cooling, for example in an ice bath.
The resultant anthranilic acid derivative (23) is reacted with polyphosphoric acid to obtain an benzothienoquinoline derivative shown by formula (24). This reaction is suitalby conducted by heating at a temperature from about 100 to 150 C in the presence of excess amount of polyphosphoric acid.
Compound (24) is reacted with phosphorus oxychloride to obtain a chloride of benzothienoquinoline derivative shown by ~ormula (25). This reaction is sultably carried out by heating under reflux in the presence of excess amount of phosphorus oxychloride.
Thus obtained compound (25) is reacted with an aniline derivative shown by formula (14) to obtain a benzothienoquinoline compound represented by formula ~Ic].
This reaction can be conducted by heating, for exampl at a reflux temperature, in the presence of solvent such as dimethylformamide (DMF), pyridine, ethoxyethanol or dioxane, in an atmosphere of inert gas. The reaction product i8 optionally purified by a conventional method such as recrystallization.
Salts of benzothienoquinoline compound represented by formula [Icl can be obtained by addition of an acid such as hydrochloric acid to the reaction solution before, during or after the reaction with the aniline derivative.
Scheme 4: ~enzofuranoquinoline compound (Z = O) BenzofuranoqUinoline compounds represented by formula lId] can be synthesized by the method shown in Scheme 4.
Phenoxyacetic acid shown by formula (26) is reacted l 4 200~i6~i6 with thionyl chloride by a conventional method to obtain phenoxyacetyl chloride shown by formula ~27).
Phenoxyacetyl chloride (27) is reacted with anthranilic acid shown by formula ~10) to obtain an anthranilic acid derivative shown by formula (28). This reaction can be carried out by dissolving anthranilic acid (10) in an aqueous solution of an alkali hydroxide such as sodium hydroxide, droping chloride (28) into this aqueous solution and stirring the resulting solution.
The resultant anthranilic acid derivative ~28) is reacted with polyphosphoric acid to obtain an benzofuranoquinoline derivative shown by formula (29). This reaction can be conducted by heating at a temperature of from about 100 to 150 C in the presence of excess amount of polyphosphoric acid.
Compound (29) is reacted with phosphorus oxychloride to obtain a chloride of benzofuranoquinoline derivative shown by formula (30). This reaction can be carried out by heating in the presence of excess amount of phosphorus oxychloride at a reflux temperature.
Thus obtained compound (30) is reacted with an aniline derivative shown by formula (14) to obtain a benzofuranoquinoline compound represented by formula lId].
This reaction can be conducted by heating, for exampl at a reflux temperature, in the presence of solvent such as dimethylformamide (DMF), pyridine, ethoxyethanol or dioxane, in an atmosphere of inert gas. The reaction product is optionally purified by a conventional method such as recrystallization.
Salts of benzofuranoquinoline compound represented by ' formula lId] can be obtained by addition of an acid such as hydrochloric acid to the reaction solution before, during or after the reaction with the aniline derivative.
Starting materials used in the above-mentioned method are known compounds or compounds easily obtainable by known methods.
The novel condensed quinoline system compounds of this invention suppress proliferation of cancer cells and exhibit effects in prolonging the life of animals with cancer and therefore, are expected to be utilized as unticancer agents.
The present invention will now be de~cribed more in detail with reference to Examples.
Synthesis of hydrochlorate of 6-4-~methanesulfonamide-2-methoxyanilino)-1,10-dimethylindeno[3,2-b]quinoline:
/ CH. CH, \
''' 1',~
NH HCQ
OCH, NH- SO,CH3 7-Methyl-1-indanone 5 g (34.0 mmol) and 3-methylanthranilic acid 11.0 g (85.0 mmol) were dissolved in 20 ml of paracymene and heated under reflux at 200 to 220 C
for 4 hours. After reflux, paracymene was distilled under the reduced pressure and the resulting residue was recrystallized from toluene to obtain 1,10-dimethylindenol3,2-b]-6,11-dihydroquinoline-6-one 890 mg (yield: 12%). 7-Methyl-1-indanone was synthesized by the method reported by B. R. Holt and J. London ~Zh. Obshch.
Khim., 20, 1245(1950)~ .
The resultant compound 890 mg (3.41 mmol) was refluxed with phosphorus oxychloride 10 ml for 2 hours and unreacted phosphorus oxychloride was distilled off. The residue was poured into ice water and neutralized with KOH. Then the neutralized solution was subjected to extraction with chloroform, and the resulting chloroform solution was washed with an aqueous solution saturated with NaCl and dried with anhydrous MgSO,. The solvent in the dried solution was then distilled off. The residue was recrystallized from dichloromethane/hexane to obtain 6-chloro-1,10-dimethylindenone 780 mg (yield: 82%) (melting point: 161 to 162 C )-Then the resulting compound 750 mg and 4-amino-3-methoxyanilinemethanesulfonaminde 610 mg were dissolved in 10 ml of ethoxyethanol under heating. One drop of conc.
hydrochloric acid was added to the solution and heated with agitation for 2 hours. Deposited precipitate was collected by filtration and recrystallized from dimethylformamide/methanol to obtain the above captioned compound (hydrochlorate) 680 mg (yield : 51%).
Melting point: 232 to 233C
I R ~ cm : 3520, 3330, 1320, 1150 'H-NMR(CF,COOD) ~
2.92,3.11(6H, each s, CH, X 2 ) 3.33(3H, s, SO~CHl) 3.52(2H, s, CH,) 3.93(2H, s, OCH,) 7.01-7.40(5H, m, aromatic H, NH) 7.48-7.95(7H, m, aromatic H ) ... . . . . . . .. .
20~)6666 Synthesis of hydrochlorate of 6-4-(methanesulfonamide-2-methoxyanilio)-10-methylindeno[3,2-b]quinoline:
NH . HC.e [~ OCH9 NH-- SO~ CH3 1-Indanone 1 g (7.6 mmol) and 3-methylanthranilic acid 1.1 g (7.3 mmol) were ais~olved in 20 ml of paracymene and refluxed at 200 C for 30 minutec. After reflux, the reaction solution was cooled and deposited crystals were colloected by filtration and washed with pyridine and ether to obtain 10-methylindeno[3,2-b]-6,11-dihydroquinoline-6-one (melting point: 300 nc or more) 960 mg (yield: 53%).
The resultant compound 950 mg ~3.85 mmol) was refluxed with phosphorus oxychloride 10 ml for 2 hours and unreacted phosphorus oxychloride was distilled off. The residue was poured into ice water and neutralized with 10~ KOH. Then the neutralized solution was subjected to extraction with chloroform, and the resulting chloroform solution was washed .
;~006666 with water and dried with anhydrous MgSO.. The solvent in the dried solution was then di~tilled off to obtain 6-chloro-10-methylindenone 800 mg (yield: 82%) (melting point:
131 to 133 DC )~ Then the resulting compound 700 mg and 4-amino-3-methoxyanilinemethanesulfonaminde 700 mg (3.30 mmol) were dissolved in 8 ml of ethoxyethanol under heating.
Two drops of conc. hydrochloric acid were added to the solution and heated for 4 hours. Deposited precipitate was filtered and recrystallized from methanol to obtain the above captioned compound (hydrochlorate) 320 mg (yield ;
26.4%).
Melting point: 251 to 2S3C
1 R ~ N i~l cm~~: 3340, 1320, 1150 'H-NMR(CFlCOOD) ~ :
2.92(3H, s, CH,) 3.33(3H, s, SO,CH,) 3.52(2H, s, CH,) 3.93(3H, s, OCH,) 7.01-7.40(5H, m, aromatic H, NH) 7.48-7.95(7H, m, aromatic H ) 8.10-8.40(2H, m, aromatic H ) Synthesis of hydrochlorate of 6-(4-methoxycarbamoyl-2-methoxyanilino)-indeno[3,2-blquinoline:
200666~i NH
~,~CII, ~-UC~
NHCOOCH~
6-Chloroindenol 3, 2-b]quinoline ~synthesized by a method described in Japanese Patent Disclosure No.63-101369) 700 mg (2.8 mmol) and 4-methoxycarbamoyl-2-methoxyaniline 650 mg were added to 5 ml of ethoxyethanol.
Two drops of conc. hydrochloric acid were added to this solution and reated under reflux for 3 hours. After the reaction, deposited precipitate was filtered and washed with ether to obtain the above captioned hydrochlorate 610 ~g (yield : 49%).
4-Methoxycarbamoyl-2-methoxyaniline was synthesized by the method of G. W. Rew castle (J. Med. Chem., 30, 1576 (1987)).
Melting point: 244 to 246~C
I R v Nu~ol cm-~: 3450, 1730 'H-NMR(DMSO-d6) ~ :
3.40(2H, s, CH,) 3.82(6H, s, OCH~, COOCH,) 7.11-7.30(2H, m, aromatic H ) 7.38-7.80(6H, m, aromatic H ) 7.96-8.65(4H, m, aromatic H, NH) 9.72-9.85(1H, br, N~) Synthesis of hydrochlorate of 6-(4-amino-2-methoxyanilino)-indenot3,2-b]quinolines 10 ~
NH
l ~ OC~ NC e NH~
6-(4-Methoxycarbamoyl-2-methoxyanilino)-indenol3,2-blquinoline (415 mg, 1 mmol) synthesized in Example 3 was dissolved in 4ml of CH3SO3H. Then, 0.37 ml (5 mmol) of (CHJ),S was added to the resulting solution and stirred at 35 ~C for 1.5 hours. The reaction solution was neutralized with KHCOa and the product was extracted with ethyl acetate. The obtained extract solution was dried with MgSO4 and the solvent was distilled off to obtain the objective product quantitatively.
Melting Point: 246 to 251 ~C (decomp,) X0066~6 I R ~ Nulol cm~l: 3470(NH,), 3440, 3290(NH) NMR(CDC~ , + DMSO - d.)~
3.20-3.43(2H, m, CH,) 3.72(3H, s, OCH~) 6.14-7.56(11H, m, aromatic H, NH, NH,) 7.90-8.33(3~, m, aromatic ~ ) Synthesis of hydrochlorate of 6-(4-methanesulfonamide-anilino)-indenol3,2-blquinoline:
In accordance with the procedures of Example 2 excepting that anthranilic,acid was used in place of 3-methylanthranilic acid, hydrchlorate of 6-(4-methanesulfonamide-anilino)-indenol3,2-b]quinoline was obtained.
NH
O H~ CQ
NHSO,CH3 Melting Point: lB5 to 188 C
I R v Nulol cm~~ 3560, 1335, 1145 NMR(DMSO- d5) ~
3.08(3H, s), 3.70(2H, s), 7.00-7.31(4H, m), 7.31-7.80(5H, m), 8.15-8.50(3H, m) Synthesis of hydrochlorate of 6-( 4-methanesulfonamide-2-dimethylaminoanilino)-indeno~3,Z-b]quinoline:
10 ~ ~
NH
~5 I ~ ~(C~ C~
NHSO,CH9 6-Chloroindeno[3,2-b]quinoline ~592 mg, 2 mmol) synthesized in Example 3 and hydrochlorate of 4-amino-3- 0 dimethylaminoanilinemethanesulfonamide 519 mg ~2 mmol) were added to 10ml of ethoxyethanol and three drops of conc.
hydrochloric acid were added to this solution. Thu~
obtained solution was heated under reflux for 11 hours.
After refluxi deposited crystals were collected and washed 5 with ether to obtain the objective product 520 mg ~yield:
59%).
Melting point: 262 to 265 C
I R ~ NuJol cm~~ 3340, 1330, 1143 ~., NMR(DMSO- d,) ~
2~69(6H, s, NMe,) 3.15(3H, 9~ SO,Me) 3.20-3.38(2H, m, CH,) 6.80-7.83~8H, m, aromatic H ) 8.11-8.98(3H, m, aromatic H ) 9.89-10.03~1H, br, NN) 10.34-10.51(1H, br, NHSO~- ) Synthesis of hydrochlorate of 6-(4-sodium sulfonmethylamino-2-methoxyanilino)-indeno[3,2-b]quinoline:
[ ~ > ~
NH
~OJ
20~ ~
NHCH,SO,Na 6-(4-Amino-2-methoxyanilino)-indenoE3,2-b]quinoline (353 mg, 1 mmol) synthesized in Example 4 was dissolved in 60ml oP ethanol. 30 ml of ethanl solution (ethanol:
water=8:2) of HOCH.SO,Na ~150 mg, 1.1 mmol) was added to this solution. The resulting reaction mixture was heated at 60 to 70 C for 10 minutes. After heating, deposited crystals were collected by filtration and washed with ethanol and ether to obtain the objective product 339 mg (yield: 75~
The product was identified by confirming generation of SO, when the product was heated in 10% HCl solution at 100 C .
Synthesis of hydrochlorate of 6-(4-carboxymethylamino-2-methoxyanilino)-indeno[3,2-b]quinoline:
NH
~c~ J~c~
NHCH, COOH
~
6-(4-Amino-2-methoxyanilino)-indeno[3,2-b~quinoline (500 mg, 1.4 mmol) synthesized in Example 4 was dissloved in Sml of dried DMF and 500 mg (3.5 mmol) of K,CO, was added to this solution. To this mixing solution, BrCH,COOCH3 0.16ml (1.5mmol) was added and heated at 50 to 60 C for 2 hours. After heating, the reaction mixture was poured into ice water and subjected to extraction with ethyl acetate.
The extract solution was dried with MgSO4 and the solvent was distilled off to obtain quantitatively 6-(4-methylcarboxymethylamino-2-methoxyanilino)-indeno[3,2-b]quinoline.
426 mg (1 mmol) of this product was dissloved in 20%
NaOH-methanol solution 10 ml and ag~tated for 2 hours at room temperature. After agitation, the reaction mixture was neutralized with 10% HCl solution and then methanol was distilled off. Then 1 ml of 10% HCl solution was added to the residue to acidify and deposited crystals were collected by filtration to obtain the objective product (hydrochlorate) 306 mg (yield: 74~).
Physical properties of 6-(4-methylcarboxymethylamino-2-methoxyanilino)-indeno[3,2-b]quinbline:
Melting point: 260 to 270 C (decomp) I R ~ N~ol cm~~ 1740(C,O), 3400(NH) m~ ~
'H-NMR(CDC~
3.42(2H, s, CH,) 3.77(6H, s, OCH3) 3.90(2H, s, CH,) 6.01-6.42(4H, m, aromatic H, NH) 7.18-7.70(4H, m, aromatic H, NH) 7.99-8.32(3H, m, aromatic H) 5 Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-methoxyanilino)-10-methylindolo[3,2-b]quinoline:
CH, \
NH HC~
~ OCH~ ~
NH- SO,CH9 3-Methylanthranilic acid 10 g (0.07 mol) was dissolved in dried benzene lOOml. To thi~ solution, chloroacetylchloride 5.81 ml (0.07 mol) was added.dropwise at room temperature and heated under reflux for two hours.
After cooling, deposited crystals were collected by filtration and recrystallized from benzene-toluene to obtain 3-methyl-N(chloroacetyl)anthranilic acid 11.7 g (yield:
79~).
Then, 3 g (0.01 mol) of this compound was dissolved in 5 ml tO.04 ml) of aniline and 5 ml of dimethylformamide and heated at 80 to 90 C for 4 hours. Cold water was added to the reaction solution, and deposited crystals were collected by filtration, washed with ether and recrystallized from toluene to obtain 3-methyl-N(phenylaminoacetyl)anthranilic acid 2.6 g (yield: 70~).
The resulting compound 2.5 g (7.8 mmol) was mixed with .
polyphosphoric acid 50 g and heated at 120 C for 2 hours.
After heating, the reaction mixture was poured into cold water. The resulting solution was neutralized with potassium hydrogencarbonate and deposited crystals were collected by filtration to obtain 11-methylindolo[3,2-b]-6,11-dihydroquinoline-6-one 1.7 g (yield: 77%).
The resultant compound 1.7 g (6 mmol) was added to phosphorus pentachloride 1.25 g (6 mmol) and phosphorus oxychloride 30 ml, and hèated under reflux for 2 hours.
Unreacted phosphorus oxychloride was distilled off, and the residue was poured into ice water and neutralized with 10%
NaOH solution. Then the neutralized solution was subjected to extraction with chloroform, and the resulting chloroform solution was washed with water, dried with anh~drous MgSO4 and the solvent was distilled off. The residue was recrystallized from dichloromethane/methanol to obtain 6-chloro-10-methylindolol3,2-b]quinoline (melting point: 228 to 230 C ) 1.2 g (yield: 66%).
Then the resulting compound 800 mg (3.1 mmol) and 4-amino-3-methoxyanilinemethanesulfonaminde 684 mg (3.6 mmol) were dissolved in 10 ml of ethoxyethanol. One drop of conc.
;i hydrochloric acid was added to this solution and heated under reflux for 4 hours. After cooling, precipitate was collected, washed with ether and chloroform and recrystallized from methanol to obtain the objective compound (hydrochlorate) 870 mg (yiled : 72%).
Melting point: 260 to 263 C
' .
, .
2 0 ~ 66 6 6 I R ~ Nulol cm~l 3120, 1325, 1160 m- I
NMR~CDC~ g ~ DMSO - d5) ~ :
3.14t3H, S, CH,) 3.31(3H, s, SO,CH,) 3.8S(3H, s, OCH,) 7.09-7,45(2H, m, aromatic H ) 7. 53-8.18(8H, m, aromatic H ) 8.~3-9.04(1H, m, NH) 9.21-9.46(1H, m, NH) 10.49-10.60(1H, br, NH) EXAMPLE lO
Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-methoxyanilino)-1,10-dimethylindolol3,2-b]quinoline:
,~ 15 J CH3 CH, \
~J, ~
- NH HC~
[~C ,1 NH- SO,CHg 3-Methyl-N(chloroacetyl)anthranilic acid 7.5 g (33 mmol)(synthesized from 3-methylanthranilic acid by the same procedures as those of Example 9) and m-toluidine 11 ml '' .
!
Z00~6~i6 0.10 mol) were dissolved in 60 ml of dimethylformamide and heated at 90 C for 4 hours. The reaction solution was poured into ice water and extracted with ether. The ; resulting ether solution was extracted with 10% sodium hydroxide and the resluting aqueous solution was neutralized with 10% HCl solution. The neutralized solution was extracted with ether, and the ether solution was washed with water and dried. The solvent was distilled off and the residue was recrystallized from benzene-toluene to obtain 3-methyl-N[(3-methylphenyl)acetyl]anthranilic acid 4.8 9 (yield: 49~).
The resulting compound 5.1 9 (0.02 mmol) was mixed with polyphosphoric acid 200 9 and heated at 120 C for 2 ., ~; hours. After heating, the reaction mixture was poured into I5 ice water. The resulting solution was neutralized with an aqueous solution saturated with potassium hydrogencarbonate and deposited crystals were collected by filtration to obtain a mixture of 1, 10-dimethyl-6,11-dihydroindolo[3,2-, b]-quinoline-6-one and 3, 10-dimethyl-6,11-dihydroindolo[3,2-b]-quinoline 6-one (3.9 g (yield: 8~.5~)).
The resulting mixture 3.8 g (5 mmol) was added to phosphorus oxychloride 20 ml and heated under reflux for 2 ~ hours. Unreacted phosphorus oxychloride was distilled off - under the reduced pressure, and the residue was poured into ice water and neutralized with 10~ potassium hydrogencarbonate solution. Then the neutralized solution was subjected to extraction with ethylacetate. The ~. ' ' Z0()6666 resulting ethylacetate solution was washed with an aqueous solution saturated with NaCl and dried with MgSO~, and the solvent in the dried solution was distilled off. Thus obtained residue was subjected to silica gel column chromatography and separated with hexane (eluent) to obtain 6-chloro-1,10-dimethylindolo[3,2-b]quinoline 620 mg (yield:
15~) and 6-chloro-3,10-dimethylindolol3,2-b]quinoline 560 mg (yield: 14%).
The resulting 6-chloro-1,10-dimethylindolo[3,2-b]quinoline 400 mg (1.43 mmol) and 4-amino-3-methoxyanilinemethanesulfonaminde 340 mg (1.5 mmoll were dissolved in 6 ml of ethoxyethanol. Two drops of conc.
hydrochloric acid were added to this solution and heated under reflux for 3 hours. After cooling, precipitate was collected by filtration to obtain the objective compound (hydrochlorate) 450 mg (yiled : 63%).
Melting point: 202 to 205C
I R v N U I I ~ - I 1320, 1150 ~ . ,~
NMR ( CF, COOD ) 2.98(3H, s, CH,) 3.12(3H, s, CH3) 3.47(3H, s, SO,CH,) 3.95(3H, 9, OCH~) 7.05-8.03(10H, m, aromatic H, NH) ; 8.38-8.S5(1H, m, aromatic H ) Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-' , methoxyanilino)-3,10-dimethylindolo[3,2-blquinoline:
cu ~
NH HC~
~ ~ OCH, NH- SO.CH9 6-Chloro-3,10-dimethylindolo[3,2-b~quinoline 560 mg (1.43 mmol) obtained in Example 10 and 4-amino-3-methoxyanilinemethanesulfonaminde 340 mg (1.5 mmol) were dissolved in 6 ml of ethoxyethanol. Two drops of conc.
hydrochloric acid were added to this solution and heated under reflux for 3 hours. After cooling, precipitate was collected by filtration to obtain the objective compound (hydrochlorate) 420 mg (yield : 59%).
Melting point: 198 to 200~C
R i~ Nuiol cm~l 1320, 1150 m~ I .
NMR(CF,COOD) 2.54(3H, s, CH3) 2.93(3H, s, CH3) 3.39(3H, s, SO,CH3) ~00~.6~,6 3.98(3H, s, OCH,) 7.14-7.96(9H, m, aromatic H, NH) 8.16-8.47(2H, m, aromatic H ) Synthesis of hydrochlorate of 2-chloro-6-(4-methanesulfonamide-2-methoxyanilino)indolol3,2-b]quinoline:
10 /[~C,Q\
NH
~ C~ ce NH-SO,CH, N(chloroacetyl)anthranilic acid 3.2 9 (0.02 mol) and p-chloroaniline 3.95 9 (0.00S mol) were dissolved in 4 ml of dimethylformamide and heated at 80 to 90 C for 4 hours.
The reaction solution was poured into ice water and deposited crystals were collected by filtration. These crystals were washed with ether and recrystallized from ethanol to obtain N-[(4-chlorophenylamino)acetyl~-anthranilic acid 2.2 g (yield: 72.2%).
The resulting compound 2.28 9 (7.52 mmol) was mixed with polyphosphoric acid 75 9 and heated at 120 DC for 2 Z006~i66 hours. After heating, the reaction mixture was poured into ice water and deposited crystal~ were collected by filtration to obtain 2-chloroindolo[3,2-bl-6,11-dihydroquinoline-6-one 1.6 g (yield: 80%).
The resulting compound 1.34 9 (5 mmol) was added to phosphorus oxychloride 10 ml and heated under reflux for 3 hours. An excess amount of phosphorus oxychloride was distilled off, and the residue was poured into ice water and neuralized with potassium hydrogencarbonate. Then the neutralized solution was subjected to extraction with chloroform. The resulting chloroform solution was washed with an aqueous solution saturated with NaCl and dried with anhydrous MgSO., and the solvent in the dried solution was distilled off. Thus obtained residue was recrystallized from chloroform-methanol to obtain 2,6-dichloroindolo[3,2-b]-quinoline (melting point: 221 to 222C ) l.1 9 (yie}d: 74%).
This compound 861 mg (3.01 mmol) and 4-amino-3-methoxyanilinemethanesulfonaminde 680 mg (4.5 mmol) were dissolved in 8 ml of ethoxyethanol. TwO drops af conc.
hydrochloric acid were added to this solution and heated under reflux for 3 hours. After cooling, deposited orystals were collected by filtration to obtain the objective compound ~hydrochlorate) 1.01 mg (yiled : 60%).
Melting point: 203.5 to 204C (decomp.) I R ~ Nu~ol cm~~ : 3360, 1320, 1150 m I
NMR(DMSO-d~) ~
2qo6666 3.06(3H, s, SO,CH3) 3.52(3H, s, OCH,) 7.01-7.80(7H, m, aromatic H ) 8.11-8.38(2H, m, aromatic H ) 8.61-8.70~1H, m, NH) 10.04-10.13(1H, m, NH) 10.51-10.72(1H, m, NH) Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-methoxyanilino)-2-methylindolo[3,2-b]quinoline:
~ r~
NH
~ ~ CU, ~ . NC8 NHSO,CH3 N(chloroacetyl)anthranilic acid 3.2 9 ~0.02 mol) and p-toluidine 3.4 9 (0.005 mol) were dissolved in 4 ml of dimethylformamide and heated at 90 C for 3 hours. The reaction solution was poured into ice water and deposited crystals were collected by filtration. These crystals were washed with ether and recrystallized from ethanol to obtain N-[(4-methylphenylamino)acetyl]anthranilic acid 2.6 g (yield: 70%).
The resulting compound 2.1 9 (7.02 mmol) was mixed with polyphosphoric acid 70 g and heated at 120C for 2 hours. After heating, the reaction mixture was poured into ice water and deposited crystals were collected by filtration to obtain 2-methylindolo~3,2-b~-6,11-dihydroquinoline-6-one 1.2 g (yield: 80~).
This compound 1.1 g (4 mmol) was added to phosphorus oxychloride 8 ml and heated under reflux for 3 hours. An excess amount of phosphorus oxychloride was distilled off, and the residue was poured into ice water and neutralized with potassium hydrogencarbonate. Then the neutralized solution was subjected to extraction with chloroorm. The resulting chloroform solution was washed with an aqueous solution saturated with NaCl, dried with anhydrous MgSO, and the solvent in the dried solution was distilled off. Thus obtained residue was recrystallized from chloroform-methanol to obtain 2-mehyl-6-chloroindolo~3,2-b]quinoline (melting point: 201 to 203 C ) 1.2 g (yield: 66%).
The resulting compound 660 mg (2.51 mmol) and 4-amino-3-methoxyanilinemethanesulfonaminde 560 mg ~2.6S mmol ) were dissolved in 8 ml of ethoxyethanol. Two drops of conc.
hydrochloric acid were added to this solution and heated under reflux for 2 hours. After cooling, deposited crystals were collected by filtration and recrystallized from methanol to obtain the objective compound Z0~6666 (hydrochlorate) 870 mg (yiled : 72%).
Melting point: 214 to 217C
'H-NMR(DMSO-d,) 2.48(3H, s, CH,) 3.05~3H, 5, SO.Me ) 3.56(3H, s, OCH,) 6.85-7.50~7H, m, aromatic H ) 8.05-8.46(3H, m, aromatic H ) 9.71-9.82(1H, m, NH) 10.24-10.30tlH, m, NH) 10.98-11.10(lH, br, NH) Synthesis of hydrochlorate of 6-(4-methoxycarbamoyl-2-methoxyanilino)indolo[3,2-b]quinoline:
NH
~ 3"OC~ IICQ
NH-COOCH, Hydrochlorate of 4-methoxycarbamoyl-2-methoxyaniline 3.3 g lsynthesized by the method of Rewcastle et al. (Jounal of Medical Chemistry(1987) vol. 30, 1576-1581)] and 6-.
chloroindoloj3,2-b]quinoline 3.0 g (12 mmol) were dissolved in 35 ml of ethoxyethanol and heated under reflux for 4 hours. After cooling, deposited crystals were collected by filtration and washed with ether and chloroform. Thus obtained crystals were added to CHICN-KHCO3 solution and to this solution, a large amount of water was added and deposited crystals were collected by filtration. The~e crystals were recrystallized from methanol and dichloromethane to obtain the objective compound 3.3 g (yield : 67~).
Melting point: 178 to 181 C
I R NU 1 I cm~~: 3390, 1716 .. ~
NMR(DMSO- d,) 3.71~ 3.75(6H, each s, OMe X 2) 6.85-7.10(2H, m, aromatic H) 7.10-8.02(6H, m, aromatic H) 8.02-8.72(3H, m, aromatic H) 9.72(1H, br, NH) 11.03(1H, br, -NH) Synthesis of hydrochlorate of 6-~4-acetoamino-2-methoxyanilino)indolol3,2-b]quinoline:
200~666 NH
[~ocn~ uce NH-COCH, 6-(4-Methoxycarbamoyl-2-methoxyanilino)indolo[3,2-b]-quinoline obtained in Example 14 was dissolved in methanesulfonic acid S ml in a stream of argon. Then dimethylsulfide 0.37ml was added dropwise to this solution in an ice bath and stirred at room temperature for one day.
After reaction, the solution was neutralized with potassium hydrogencarbonate in a stream of argon and etracted with ethyl acetate. The resulting ethyl acetate solution was washed with water, dried with anhydrous MgSO~
and the solvent was distilled off to obtain 6-(4-amino-2-methoxyanilino)indolo~3,2-b]quinoline. This compound was dis610ved in acetic anhydride 0.27 ml/acetic acid 5 ml without purification andjreacted by adding gradually with zinc powder 250 mg. After agitation for one hour, the reaction solution was added with water and neutralized with potasisum hydrogencarbonate. Deposited precipitate was collected by filtration and dissloved in methanol. After ` Z00~i666 addition with hydrochloric acid, the resulting methanol solution was concentrated under the reduced pressure to obtain the objective compound (hydrochlorate) 330 mg (yield: 76~).
Melting point: 168 to 173C
I R NuJo~ cm~~: 1650 0- .
NMR(CF.COOD + CDCQ ,) ~ :
2.36(3H, 8, -COCH,) 3.87(3H, s, -OCH,) 6 . 94-8.44(14H, m, aromatic H, NH) ExAMeLE 16 Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-methoxyanilino)-1-mehtylindolol3,2-blquinoline:
CH
H
NH
~ ~ OC I ~ ~CQ
NH-SO,CH3 N(chloroacetyl)anthranilic acid 6 . 4 g (15 mmol) ~synthesized from anthranilic acid by the same procedures as those of Example 9) and m-toluidine 9.5 ml (0.09 mol) were dissolved in 60 ml of dimethylformamide and heated at ' 80 to 90 ~C for 4 hours. The reaction mixture was poured into ice water and extracted with ether. The resulting ether solution was extracted with 10~ sodium hydroxide and the resulting aqueous solution was neutralized with 10% HCl solution. The neutralized solution was extracted with ether, and the ether solution was washed with water and dried. The solvent of dried solution was distilled off and the residue was recrystallized from benzene-hexane to obtain Nl(3-methylphenyl)acetyllanthranilic acid 4.7 9 (yields 57%).
The resulting compound 5.0 g (0.02 mmol) was mixed with polyphosphoric acid 176 9 and heated at 120 C for 2 hours. After heating, the reaction mixture was poured into ice water. The resulting solution was neutralized with an aqueous solution saturated with potassium hydrogencarbonate and deposited crystals were collected by filtration to obtain a mixture of 1-methyl-6,11~dihydroindolo[3,2-b~-quinoline-6-one and 3-methyl-6,11-dihydroindolo[3,2-b]-quinoline-6-one ~4.1 9 (yields 83%)).
The resulting mixture 4.1 9 (16 mmol) was added to phosphorus oxychloride 20 ml and heated under reflux for 2 hours. Unreacted phosphorus oxychloride was distilled off under the reduced pressure, and the residue was poured into ice water and neutralized with an aqueous solutin saturated ;20066~,6 with potassium hydrogencarbonate. Then the neutralized solution was subjected to extraction with ethyl acetate.
The resulting ethyl acetate solution was washed with an aqueous solution saturated with NaCl, dried with MgSO4 and the solvent in the dried solution was distilled off. Thus obtained residue was subjected to silica gel column chromatography and separated with hexane ~eluent) to obtain 6-chloro-1-methylindolol3,2-blquinoline (melting point: 170 to 172C ) 450 mg ~yield: 10%) and 6-chloro-3-methylindolo[3,2-b]quinoline (melting point: 193 to 194C ) 380 mg (yield: 8.4~).
The resulting 6-chloro-1-methylindolol3,2-b]o3uinoline 400 mg (l.S1 mmol) and 4-amino-3-methoxyaniline methanesulfonaminde 360 mg (1.75 mmol) were dissolved in 6 ml of ethoxyethanol. Two drops of conc. hydrochloric acid were added to this solution and heated under reflux for 3 hours. After cooling, precipitate was collected by filtration to obtain the ob~ective compound (hydrochlorate) 520 mg (yield : 71%).
Melting point: 214 to 217C
NMR(CFlCOOD) ~ :
3.06(3H, s, CH,) 3.33(3H, s, SO,CH3) 3.73(3H, s, OCH3) 7.08-7.46(7H, m, aromatic H, NH) 7.60-8.56(6H, m, aromatic H) Synthesis of hydrochlorate of 6-(4-methanesulfoneamide-2-methoxyanilino)-3-mehtylindolo[3,2-b]quinoline:
~ cn,~
NH
~ ~ CH, J Nce NH-SO,CH3 6-Chloro-3-methylindolo[3,2-b]quinoline 350 mg t1.31 mmol) obtained in Example 16 and 4-amino-3-methoxyaniline methanesulfonaminde 310 mg (1.42 mmol) were dissolved in 6 ml of ethoxyethanol. Two drops of conc. hydrochloric acid were added to this solution and heated under reflux for 2 hours. After cooling, precipitate was collected by filtration to obtain the objective compound (hydrochlorate) 430 mg (yield : 68%).
Melting point: 215 to 217 C
NMR(CF,COOD ) ~ :
2.48(3H, s, CH,) 3.38(3H, s, SO,CHl) 3.95(3H, s, OCHI) 7.07-7.50(6H, m, aromatic H, NH) 7.60-8.47t7H, m, aromatic H, NH) ... , . . .. . . , . . .. ... ~. .. . .. . . ~ . . . . . , Synthesis of 6-(4-methanesulfonamide-2-methoxyanilino)-2-nitroindolol3,2-blquinoline:
5 ~/110, NH
~
NHSOa CH, Fuming nitric acid (d=1.42) was added dropwise to 6-chloroindolol3,2-b]quinoline 2.S2 g (0.01 mol) at 0 C . The resulting mixture was left overnight at room temperature and then poured into ice water. Deposited crystals were collected by filteration, washed with an aqueous solution saturated with KHCO1 and recrystallized from tetrahydrofuran and CH~ Cl~ to obtain 6-chloro-2-nitroindolol3,2-b]quinoline (melting point: 280 to 290C
(decomp.)) 2.50 g (yield: 84%).
This compound 5.9 g (0.02 mol) and 4-amino-3-methoxyanilinemethanesulfonaminde hydrochlorate 6 g (0.024 ; mol) were dissolved in 10 ml of ethoxyethanol and heated ~ under reflux for 6 hours. After cooling, precipitate was collected by filtration and added to chloroform. This chloroform was neutralized with an aqueous solution saturated with KHCO3 and then chloroform was distilled off.
Z0~66~i6 The residue was recrystallized from methanol to obtain the objective compound 6 g ~yield : 61~).
Melting point: 300 C or more MS m/e 478 (M~ ) Synthesis of hydrochlorate of 2-fluoro-6-(4-methanesulfonamide-2-methoxyanilino)indolo[3,2-b]quinoline:
I ~ ~ ~ F
NH
15 ~ OC~ ~C~
N(chloroacetyl)anthranilic aaid 4.0 g (8 mmol) and p-fluoroaniline 5.3 ml (56 mmol) were dissolved in 4 ml of dimethylformamide and heated at 80 to 90C for 4 hours. The reaction solution was poured into ice water and deposited crystals were collected by filtration. These crystals were washed with ether and recrystallized from ethanol to obtain N-[(4-fluorophenylamino)acetyllanthranilic acid (melting point: 217 to 219 C ) 2.4 g (yield: 46~).
The resulting compound 2.26 g (7.5 mmol) was mixed 2~066~6 with polyphosphoric acid 75 g and heated at 120C for 2 hours. After heating, the reaction mixture was poured into ice water and deposited crystals were collected by filtration to obtain 2-fluoromethylindolol3,2-bl-6,11-dihydroquinoline-6-one 1.35 g.
The resulting compound 1.0 g was added to phosphorus oxychloride 10 ml and heated under roflux for 3 hours. An excess amount of phosphorus oxychloride was distilled off.
The residue was poured into ice water, neutralized with potassium hydrogencarbonate and deposited crystals were collected by filtration. The crystals were subjected silica gel column chromatography to obtain 6-chloro-2-fluoroindolol3,2-b]quinoline (melting point: 201 to 204 C ) 470 mg (yield: 43%).
This compound 400 mg (3.01 mmol) and 4-amino-3-methoxyanilinemethanesulfonaminde 400 mg (1.6 mmol) were dissolved in 10 ml of ethoxyethanol and heated under reflux for 3 hours. After cooling, deposited crystals were collected by filtration to obtain the objective compound (hydrochlorate) 660 mg (yiled : 95~).
Melting point: 260 C (decomp.) I R ~ N~iol cm l 1150, 1318tSOICH3), 3250~NH,) m~ -NMR(DMSO- d6) ~ :
3.12(3H, s, CH3) 3.66(3~, s, C~3) 6.80-8.02(10H, m, aromatic H ) Synthesis of hydrochlorate of 6-(4-hydroxy-2-methoxyanilino) indolol3,2-blquinoline:
5 [~
NH
,o ~ ~ c~ ce OH
1.4 9 (8.3 mmol) of 4-hydroxy-2-methoxyaniline hydrochlorate synthesized by the method of J. L. Jurlina et al. [J. Med. Chem., 19B7, Vol. 30, No.3] and 6-chloroindolol3,2-blquinoline 1.75 9 (6.9 mmol) were dissolved in 10ml of ethoxyethanol and heated under reflux for 4 hours. Deposited crystals were collected by20 filtration and washed with ether to obtain the objective compound ~hydrochlorate) 1.8 g (yield: 78%).
Melting point~ 259 to 263 C (decomp.) 'H-NNR(CF3COOD) ~
3.91(3H, s, OCH,) 7.10-8.54(14H, m, aromatic H, NH) Synthesis of 6-(4-aceto-2-methoxyanilino)indolol3,2-~0~)~i666 b]quinoline:
H
NH
OCOCH, 600 mg (1.5 mol) of hydrochlorate of 6-(4-hydroxy-2-methoxyanilino)indolol3,2-b]quinoline obtained in Example 20, anhydrous K, C03 2.1 g and acetic anhydride 0.46 ml were dissolved in 90 ml of dimethylformamide and agitated at room temperature for 1.5 hours. The reaction solution was poured into ice water, and deposited crystals were collected by filtration and recrystallized from tetrahydrofuran and CH, Cl2 to obtain the objective compound 510 mg (yield: 77%).
Melting point: 224 to 230 C (decomp.) 'H-NMR(CF,COOD) ~ :
2.S6(3H, B, COCH,) 3.95(3H, s, OCH3) 6.90-8.61(13H, m, aromatic H, NH) Synthesis of 2-amino-6-(4-methanesulfonamide-2-methoxyanilino)indolol3,2-b]quinoline ~ NH2 NH
NHSO,CH, 6-(4-Methanesulfonamide-2-methoxyanilino)-2-nitroindolol3,2-blquinoline 2 g (3.6 mmol) obtained in Example 18 was dissolved in 150 ml of acetic acid. 10% Pd-C 50 mg was added to this solution and the above compound was reduced by hydrogen for 5 hours. After removal of Pd-C, acetic aoid was distilled off, and the residue was neutralized with an aqueous solution saturated with KHCO9 and extracted with chlorofornl. The resulting chloroform solution was washed with an aqueous solution saturated with NaCl, dried with anhydrous MgSO~ and the solvent was distilled off. The residue was recrystallized from mehtanol and dichloromethane to obtain the objective compound 1.36 g (yield: 78%).
Melting point: 251 to 256 ~C (decomp.) Acetate ~ H-NMR(CF. COOD) Z00666~
2.23(3H, S, CH3CO) 3.32(3H, s, SO,CH,) 3.96~3H, s, OCN,) 7.12-8.46~14H, m, aromatic H, NH) Synthesis of N- (4-l(7-(2,3,4, 6-tetra-O-acetylglycosyl-1-amino)-1 OH-indolo[3, 2-blquinoline-11-yl)amino 1-3-methoxyphenyl) methanesulfonamide OAc 0--r H OAc NH
~ OCHg NHSO,CH, 1-sromo-2, 3,4, 6-tetra-O-acetylglucose 450 mg (1 mmol) was dissloved in dried pyridine 1 ml and dried dimethyformamide 10 ml and stirred overnight in an atmosphere of argon. Then, to this solution, dimethylformamide solution containing 240 mg (0.5 mmol) of 2-amino-6-(4-methanesulfonamide-2-methoxyanilino) indolo[3,2-blquinoline obtained in Example 22 was added and reacted for 24 hours at room temperature. The reaction solution was poured into ice water and extracted with chloroform. The solvent was distilled off from the resulting chloroform solution and the residue was subjected to silica gel column chromatography to obtain the objective compound 210 mg (yield: 30~) from the dichloromethane:hexane (1:5) eluate.
Melting point: 172 to 178 C ( decomp.) ' H-NMR(DMSO-d, ) 2.08(12H, s, COCH, X 4) 2.96(3H, s, SO. CH, ) 4.04(3H, s, OCH, ) 4.16-4.64(3H, m, 4' -H, CH,OAc) 5.11-5.39(2H, m, 2' -H, 3' -H) 5.71-6.00(1H, m, 5' -H) 6.48-6.68(1H, m, 1' -H) 7.14-7.79(10H, m, aromatic H, NH) 8.09-8.74(3H, m, aromatic H) ExAMeLE 24 Synthesis of N- (4-l (7-(glycosyl-1-amino)-10H-indolol3,2-blquinoline-11-yl)amino]-3-methoxyphenyl) methanesulfonamide 200fi666 r~
O
~( ~ N~
H OH
NH
.
I0 NHSO.CHl 120 mg ~0.14 mmol) of N- ~4-[~7-(2,3,4,6-tetra-O-acetylglycosyl-1-amino)-10H-indolo[3,2-blquinoline-11-yl) amino]-3-methoxyphenyl~ methanesulfonamide obtained in Example 23 was dissolved in methanol 20 ml and an aqueous ammonium solution (NH, H,O) 20 ml. The resulting solution was agitated for 3 days and during this agitation, ammonia was added to this solution every 3 hours. The reaction solution was neutralized with 10% aqueous acetic acid solution and methanol was distilled off from the neutralized solution. Deposited crystals were collected by filtration and recry~tallized from methanol and dichloromethane to obtain the objective compound 75 mg (yield: 87~)~
Melting point: 201 to 205 C (decomp.) lH-NMR(CD3OD+ DMSO-d~) 2.96(3H, s, SO,CH,) 3.73(2H, s, CH,OH ) 4.04(3H, s, OCH,) 4.55(6H, m, 4 ' -H, 5' -H and OH X 4) 5.03-5.12(2H, m, 2' -H and 3' -H) 6.36-6.52(1H, m, 1' -H) 6.58-6.64(1H, m, aromatic H) 7.14-7.79~10H, m, aromatic H, NH) 7.94-8.56(3H, m, aromatic H) Synthesis of 2-methylcarbamoyl 6-(4-methanesulfonamide-2-methoxyanilino)indolo[3,2-blquinoline UNCOCU.
NH
OCH, NHSO~CH~
500 mg (1.1 mmol) of 2-amino-6-(4-methanesulfonamide-2-methoxyanilino)indolo[3,2-blquinoline obtained in Example 22 was dissolved in dried pyridine 10 ml and acetic anhydride 2 ml and heated at 80 to 90C for 6 hours. The reaction solution was poured into ice water and extracted with chloroform. The resulting chloroform solution was washed with water and dried with anhydrous MgSO,. The solvent was distilled off and the residue was recrystallized from tetrahydrofuran and dichlromethane to obtain the objective compound 470 mg ~yield: 75%) Melting point: 223 to 226 C (decomp.) H-NMR(CF,COOD) ~
2.08(3H, s, COCH,) 3.28(3H, s, SO.OH,) 3.80(3H, s, OCH,) 7.08-7.86(9H, m, aromatic H, NH) 7.89-8.48~5H, m, aromatic H, NH) Synthesis of hydrochlorate of 2-methanesulfonamide-6-(4-methanesulfonamide-2-methoxyanilino)indolol3,2-b]quinoline 1 5 ~ 0, C
NH
,oc~ IIC~
NH-SO, CH, 500 mg (1.1 mmol) of 2-amino-6-(4-methanesulfonamide-2-methoxyanilino)indolo[3,2-b]quinoline obtained in Example 22 was dissolved in dried pyridine 10 ml and to this solution, CH,SO,Cl 132 mg (1.05 equivalent) was added dropwise at 0 C . After addition, the reaction solution was agitated for 3 hours and poured into ice water. Deposited crystals were collected by filtration and recrystallized from chloroform and methanol to obtain the objective compound 520 mg (yield: 90%).
Melting point: 251 to 255 ~ (decomp.) 'H-NMR(CF,COOD) ~
2.90(3H, s, 7-NHSO,CH3) 3.31(2H, 5, 4' -NHSO,CH,) 3.82(313., s, OC~I,) 7.01-7.25(3H, m, aromatic H) 7.25-7.99(8H, m, aromatic H, NH) 8.02-8.41(3H, m, aromatic H) Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-methoxyanilino)-10-methylbenzofuranol3,2-b]quinoline ~0~
NH
~oc~l J~c~
NH-SO,CH3 3-Methylanthranilic acid 5 g (33 mmol) ~as dissolved in 10% aqueous sodium hydroxide solution 27 ml and to this 200~666 solution, phenoxyacetyl chloride 6.2 g (36 mmol) was added dropwise at C . The resulting solution was stirred at room temperature for 1 hour and acidified with 10%
hydrochloric acid solution. Deposited crystals were collected by filtration, washed with water and recrystallized from ethanol to obtain 3-methyl-N-(phenoxyacetyl)anthranilic acid (melting point: 174 to 176 C) 4.4 g (yield: 47%).
This compound 7.6 g (27 mmol) was mixed with polyphosphoric acid 60 g and heated with stirring at 120 to 130C for 1.5 hours. The reaction mixture was poured into ice water and neutralized with potassium hydrogencarbonate.
Deposited crystals were collected by filtration to obtain 10-methyl-6,11-dihydrobenzofuranol3,2-b]quinoline-6-one 5.0 g (yield: 74%). Then, this compound 5.0 g was added to phosphorus oxychloride 50 ml and heated under reflux for 1 hour. Unreacted phosphorus oxychloride was distilled off under the reduced pressure, and the residue was neutralized with an aqueous KOH solution and extracted with chloroform.
The resulting chloroform solution was washed with water and dried, and then the solvent was distilled off. The residue was recrystallized from benzene to obtain 6-chloro-10-methylbenzofurano[3,2-blquinoline (melting point: 137 to 139 C ) 4.1 g (yield: 54~).
This compound 1.8 9 (5.0 mmol) and 4-amino-3-methoxyanilinomethanesulfonamide 1.6 g (7.4 mmol) were dissolved in 15 ml of ethoxyethanol and heated under reflux for 15 hours. Deposited crystals were collected by filtration and washed with ether to obtain the objective compound ~hydrochlorate) 0.8 9 (yield: 36%).
Melting point: 25S to 2S9C
I R ~ ~U~O~ cm~~: 1640~S=O), 3300(NH) m~ ~
H-NMR (CDC~ 9 + DMSO-d,) ~ s 2.96(6H, s, 4-CH3, SO,CH,) 3.93(3H, s, OCH,) 6.70-6.95 ~ 7.18-7.75 ~ 8.S5-8.95(12H, m, aromatic H, NHX 2) Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-methoxyanilino)-1,10-dimethylbenzofurano[3,2-b]quinoline CH, CH, ~ ' T [~ i NH
~ ~ ocn ,,~ ~ NCQ
NH-SO~CH3 3-Methylanthranilic acid 1.0 9 (6 mmol) was dissolved in 10% aqueous sodium hydroxide solution 27 ml and to this soulution, 2-methylphenoxyacetyl chloride 1.3 9 ` Z006666 (7.3 mmol) was added dropwise at 0 C . The resulting solution was stirred at room temperature for 5 minutes and acidified with 10~ hydrochloric acid solution. Deposited crystals were collected by filtration, washed with hot water and recrystallized from ethanol to obtain 3-methyl-N-(2-methylphenoxyacetyl)anthranilic acid (melting point: 133 to 136C) 1.7 9 (yield: 83%).
This compound 19.4 9 (65 mmol) was mixed with polyphosphoric acid 650 g and heated with stirring at 120 C
for 2 hours. The reaction mixture was poured into ice water and deposited crystals were collected by filtration to obtain a mixture (6.4 g) of 1,10-dimethyl-6,11-dihydrobenzofuranol3,2-b]quinoline-6-one and 3,10-dimethyl-6,11-dihydrobenzofuranol3,2-b]quinoline-6-one. Then, this mixture 6.4 9 was added to phosphorus oxychloride 25 ml and heated under reflux for 0.5 hours. Unreacted phosphorus oxychloride was distilled off under the reduced pressure, and the residue was poured into ice water and extracted with ethyl acetate. The resulting ethyl acetate solution was dried with anhydrous MgS0,, and then the solvent was distilled off. The residue was subjected to silica gel column chromatography to obtain 6-chloro-1,10-dimethylbenzofurano[3,2-b]quinoline (melting point: 165 to 168C ) 0.9 9 (yield: 14%) and 6-chloro-3,10-dimethylbenzofurano~3,2-b]quinoline (melting point: 164 to 168 C ) 2.2 g (yield: 33 %).
Then, the l,10-dimethyl compound 0.5 9 (1.6 mmol) and Z00~6~;6 4-amino-3-methoxyanilinemethanesulfonamide hydrochlorate 0.5 g (2.0 mmol) were dissolved in 5 ml of ethoxyethanol and heated under reflux for 2 hours. The reaction solution was neutralized with an aqueous solution saturated with KHCO3 and extracted with ethyl acetate. The resulting ethyl acetate solution was dried with anhydrous MgSO, and the solvent was distilled off. The residue was subjected to silica gel column chromatography to obtain the objective compound (hydrochlorate) 0.3 g (yield: 38~).
Melting point: 211 to 213C
I R ~ N`ulol cm~~ 3510, 3300, 1320 .. . Il H-NM~ (CF,COOD) ~ :
2.93(3H, s, CB3 ) 3.15(3H, s, CH,) 3.33(3H, s, SO.CHl) 3.87(3H, s, OCH,) 6.95-8.10(8H, m, aromatic H) 8.15-8.45(1H, dd, J=8.2Hz, aromatic H) Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-methoxyanilino)-3,10-dimethylbenzofurano~3,2-blquinoline ~ CH, 5 ~[~\Cil-NH
~ ,OCN, ~ ce NHSO, CH9 0.35 9 (1.2 mmol) of 6~chloro-3,10-dimethyl-benzofuranol3,2-b]quinoline obtained in Example 28 and 4-amino-3-methoxyanilinemethanesulfonamide hydrochlorate 0.4 g (1.8 mmol) were dissolved in 5 ml of ethoxyethanol and heated under reflux for 6 hours. After cooling, deposited crystals were collected by filtration and washed with ethanol to obtain the objective compound 0.4 g (yield: 61%).
Meltign point:l79 to 184C
'H-NMR (CF,COOD) 2.59(3H, s, CH, ) 2.87~3H, S, CH, ) 3.28(3H, s, SO,CH,) 3.84(3H, s, OCH~) 7.00-8.27(9H, m, aromatic H) Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-,.
.
:' :
Z0066fi6 methoxyanilino)-1-methylbenzofurano[3,2-blquinoline . CH, \
NH
~ ~ OC~ Ce NH-SO,CH, Anthranilic acid 7.95 g (58 mmol) was dissolved in 10%
aqueous sodium hydroxide solution 48 ml and to this 15 solution, 3-methylphenoxyacetyl chloride 11.8 g (64 mmol) was added dropwise at C . The resulting solution was stirred at room temperature for 5 minutes and acidified with 10% hydrochloric acid solution. Deposited crystals were collected by filtration and washed with hot water to obtain N-(3-methylphenoxyacetyl)anthranilic acid 14.0 g (yield:
68%).
This compound 14.0 9 (44 mmol) was mixed with polyphosphoric acid 467 9 and heated with stirring at 120 ~C
for 2 hours. The reaction mixture was poured into ice water, and deposited crystals were collected by filtration and washed with 10 % KHC09 solution and water to obtain a mixture (6.S g) of 1-methyl-6,11-dihydrobenzofuranol3,2-~006666 b]quinoline-6-one and 3-methyl-6,11-dihydrobenzofuranol3,2-blquinoline-6-one. Then, this mixture 6.5 9 was added to phosphorus oxychloride 20 ml and heated under reflux for 1 hour. Unreacted pho~phorus oxychloride was distilled off under the reduced pressure, and the residue was poured into ice water and neutralized with an aqueous solution saturated with KHCO.. Deposited crystals were collected by filtration and washed with water~. Thus obtained crystal~
were subjected to silica gel column chromatography to obtain 6-chloro-1-methylbenzofurano[3,2-blquinoline (melting point: 169 to 172 C ) 0.48 g (yield: 4%) from the hexane eluate and 6-chloro-3-methylbenzofurano~3,2-b]quinoline 3.42 ~ (yield: 26%) from the next eluate (~exane:ethyl acetate = 8:1).
~rhen, the l-methyl compound 0.45 9 (1.6 mmol) and 4-amino-3-methoxyanilinemethanesulfonamide 0.44 g (1.7 mmol) were dissolved in 5 ml of ethoxyethanol and heated under reflux for 3.3 hours. Deposited crystals were collected by filtration and washed with ethanol to obtain the objective compound (hydrochlorate) 0.6 g (yield: 76%), Melting point: 2S3 to 255 C
I ~ ~ N~ol cm~~ 3510, 3300, 1320 'H-NMR (DMSO-d6) ~ :
3.00(6H, s, CH3, SO,CH,) 3.69(3H, s, OCH,) 6.98-8.47(12H, m, aromatic H, NH) 20(~66~i6 Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-methoxyanilino)-3-methylbenzofuranol3,2-b]quinoline ~ ~ ~ C~.
NH
~ ,OCHJ ~ce NHSO,CH3 6-Chloro-3-methylbenzofuranol3,2-b]quinoline (0.4 g (1.6 mmol)) obtained in Example 30 and 4-amino-3-~ethoxyanilinemethanesulfoniamide hydrochlorate 0.44 g (1.7 mmol) were dissolved in 5 ml of ethoxyethanol and heated under reflux for 2 hours. Deposited crystals were collected by fil~ration and washed with ethanol to obtain the objective compound 0.64 g (yield: 81%).
Melting point: 213 to 215 C
H-NMR (DMSO-d.) ~ :
2.45~3H, s, CH,) 3.00(3H, s, SO,CHI) 3.65(3H, s, OCH3) 6.8S-8.20(10H, m, aromatic H) Synthesis of hydrochlorate of 6-(4-methanesulfonamide-2-~0~!666~
methoxyanilino)-10-methylbenzothieno[3,2-b]quinoline CH, \
' NH ~ 8C~
~ OCH9 NH-SO~CH, senzenethiol and butyl bromoacetate were reacted by a conventional method and then hydrolyzed to obtain a -phenylthioacetatic acid. a -phenylthioacetatic acid was reacted wlth thionyl chloride by a convention method to obtain a -phenylthioacetyl chloride. 3-Methylanthranilic acid 59 (33 mmol) was dissolved in 10% aqueous sodium hydroxide solution 27 ml and to thiq solution, a -phenylthioacetyl chloride 5.5 ml (33 mmol) was added dropwise at C . The resulting solution was stirred at room temperature for 1 hour and neutralized with 10~
hydrochloric acid solution. Deposited crystals were collected by filtration and recrystallized from ethanol and water to obtain 3-methyl-N-(phenylthioacetyl)anthranilic acid (melting point: 148 to 150 ~C) 8.8 g (yield: 89%).
This compound 4.6 g (15 mmol) was mixed with polyphosphoric acid 30 9 and heated with stirring at 120 to 130C for 2 hours. The reaction mixture was poured into ice water and neutralized with potassium hydrogencarbonate.
Deposited crystals were collected by filtration and washed with water to obtain 10-methylbenzothienol3,2-b]-6,11-dihydroquinoline-6-one 4.2 g (yield: 90~).
Then, this compound 4.2 g was added to phosphorus oxychloride 50 ml and heated under reflux for 2.5 hours.
Unreacted phosphorus oxychloride was distilled off under the reduced pressure, and the residue was poured into ice water, neutralized with an aqueous XHO solution and extracted with chloroform. The resulting chloroform solution was washed with water and dried, and then the solvent was distilled off. The residue was recrystallized from benzene to obtain 6-chloro-10-methylbenzothieno[3,2-blquinoline (melting point: 143 to 146C ) 4.1 9 (yield: 84 % ) .
Then, this compound 1 9 (3.7 mmol) and 4-amino-3-methoxyanilinemethanesulfonamide 1.2 9 (4.4 mmol) were dissolved in 12 ml of ethoxyethanol and heated under reflux for 1.5 hours. Deposited crystals were collected by filtration, stirred in chloroform with KHCO9 and extracted with chloroform. The resulting chloroform solution was dried with anhydrous MgSO, and the solvent was distilled off. The residue was recrystallized from acetone to obtain the objective compound (hydrochlorate) 0.8 g (yield: 48~).
Melting point: 220 to 223 C
Z0066~6 I R v N~l~l cm~~: 3400, 3250, 1320 m- ~
H-NMR (DMSO-d~
3.11(3H, s, 4-CH3) 3.28(3H, s, SO.CH,) 3.66(3H, s, OCH,) 6.63-8.70~12H, m, aromatic H, NHX 2) Synthesis of hydrochlorate of 6-(4-methane~ulfonamide-2-methoxyanilino)-l-methylbenzothienol3,2-b]quinoline NH ~ HC~
~o~ J
NH-SO,CH3 ~ ~
3-Methylbenzenethiol and butyl bromoacetate were reacted by a conventional method and then hydrolyzed to obtain 3-methyl-a -phenylthioacetatic acid~ 3-Methyl-a -phenylthioacetatic acid was reacted with thionyl chloride25 by a conventional method to obtain 3-methyl-a -phenylthioacetyl chloride. Anthranilic acid S.6 g (41 mmol) was dissolved in 10% aqueous sodium hydroxide solution 32 ml and to this solution, 3-methyl-a -phenylthioacetyl chloride (99C /3.3 mmHg) 8.9 g was added dropwise at 0C .
The resulting solution was stirred at room temperature for 20 minutes and neutralized with 10% hydrochloric acid solution. To this solution, ether was added, and deposited crystals were collected by filtration and washed with hot water to obtain N-(3-methylphenylthioacetyl)anthranilic acid ~melting point: 148 to 150 C) 11.2 g tyield: 25~).
This compound 15.8 g (50 mmol) was mixed with polyphosphoric acid 500 g and heated with stirring at 120 C
for 2 hours. The reaction mixture was poured into ice water and neutralized with an aqueous potassium hydrogencarbonate solution. Deposited crystals were collected by f iltration and washed with water to obtain crude 1-methylbenzothieno[3,2-b]-6,11-dihydroquinoline-6-one 10.5 g.
Then, this compound 10.5 9 was added to phosphorus oxychloride 50 ml and heated under reflux for 1 hour.
Unreacted phosphorus oxychloride was distilled off under the reduced pressure, and the residue was poured into ice - water, neutralized with an aqueous solution saturated with KHC0~ and extracted with chloroform. The resulting chloroform solution was dried with anhydrous MgS0~, and then the solvent wa~ distilled off. The residue was subjected to silica gel column chromatography to obtain 6-chloro-1-methylbenzothieno[3,2-b]quinoline (melting point: 143 to 146 C ) 0.8 g (yield: 6%).
- 20066fi6 Then, this compound 0.2 g (0.7 mmol) and 4-amino-3-methoxyanilinemethanesulfonamide 0.2 9 (0.8 mmol) were dissolved in 5 ml of ethoxyethanol and heated under reflux for 3 hours. Depo~ited crystals were collected by filtration and washed with ethanol to obtain the objective compound (hydrochlorate) 0.21 g (yield: 60%).
Melting point: 205 to 210 ~C
H-NMR ICF~COOD) ~ :
3.04(3H, 8, CH,) 3.33(3H, 8, SO.CH,) 3.93(3H, s, OCH,) 7.32-9.02(12H, m, aromatic H, NH) Test Example 1: Test for Antitumorigen Function Function for Inhibiting Multiplication of KB Cell (in vitro test) ' KB cells, carcinomatous cell tumors, were transferred to in vitro floatation incubator systems, and added respectively with compounds of Examples 1 to 33. The results of cultivation added with these compounds were compared with the results of the control which was not added with any compound.
~3 Experimental System:
Cell used: KB Cell (Originating from human mouth epidermal cancer) Culture medium: Eagles minimal essential medium (MEM) supplemented with 10% calf serum Cultivation: 37C carbon dioxide gas incubator (5% CO,) ~ Method of Experiment:
Day 0: KB cells were diluted in the culture medium to adjust the KB cell density to 2 x 10'/ml.
Three ml of the cell suspension was inoculated in each of 60 mm plastic dishes.
Two dishes per standard dosage were used.
Day 1: Test compound was added to the medium so that the final concentrations were set to 100, 30, 10, 3 and 1 ~ g/ml.
, Day 4: Cells were scraped off from the dish using trypsin, and the cell number was countered using a Corter counter.
~9 Criteria for Judgements In generally accordance with the ~tipulation~ set forth by the National Cancer Institute ~NCI), U.S.A., the concentration of compound neces~ary for exerting 50% growth inhibition (EDs~) compared to the contral was determined. A
compound was judged as effective when ED~o was less than 4 g/ml.
The results are shown below.
Table l: Results of Test on Carcinostatic Effect (Effect of Inhibiting growth of KB-Cell) _ Compound No. Tested Conc.(ED60)(~ 9/~ ) ¦
l < 0.3 2 < 0.3 4 < 0 3 7_ C 0 3 . 11 ':
Z0~6666 Table 1 (continuation) Compound No. Tested Conc.(ED~0)(~ g/~ ) i 8 < 0.3 9 ~ 0.3 < 0.3 11 < 0.3 12 < 0.3 13 < 0.3 14 < 0.3 < 0.3 16 < 0.3 17 < 0.3 18 < 0.3 , 19 < 0.3 < 0.3 21 < 0.3 22 < 0.3 23 < 0.3 24 < 0.3 < 0.3 26 < 0.3 27 0.38 28 < 0.3 ~' , .
' 20066~6 Table 1 (continuation) ., . Compound No. Tested Conc.(ED~0)(~ g/~ ) . _ . . 29 < 0.3 ;: 30 1.5 ~: 31 < 0.3 ; . 32 1.4 `- 10 33 < 0.3 .~. Reference 0 .~
Test Example 2: Effect on Prolongation of Life Span in ,~ Cancer inplanted Mouse and Acute Toxicity 15 Pharmacological effects of compounds of Examples 1 to . 33 were tested in in vitro systems using P-3B8 implanted mice. The results were compared to that of a control which ll was to added with any compound.
System used in experiment:
:~ ~ 20 Animal used: CDF mouse (6 mice/group) `~ Tumor: P-388 ~ Number of implanted cells: 10' cells/mouse ; Implanted site: i.p.
Day of administration: Day 1 and Day 5 .-: 25 Dosage: LD~o or 400 mgtkg/day at the maximum Criteria for Judgement:
The treatment was judged as effective when the ratio ' , ' . 7 3 .
20066fi6 of survival of the treated group to that of the control group (T/C ~) was 120% or more. The survival period of the control group was generally about 10 days. The results are ~ shown in Table 2.
Table 2: Effect on Prolongation of Life Span of Mouse implanted with P-38 Cancer Cells Compound Dosage (mg / kg~ Ratio of Life No. Tested Prolongation (%) 200240(cure 1/6) 1 100290(cure 1/6) _ 100257(cure 1/6) 12.5 134 ~!
! 400 165 i 200 172 1505 l335 6 200 247(cure 2/6) ' 100 169 'I
20~ 111 ~, 7 100 108 l 50 111 - 25 8 42oo 17558 100 _ 175 !
' Table 2 (continuation) Compound Dosage (mg / kg) Ratio of Life No. Tested Prolongation (%) 305(cure 4/6) 235(cure 1/6) 9 12.5 198 6.25 168 3.12 165 1.56 131 100 260(cure 1/6) 12.5 165 . 6.25 145 3.12 109 . I
315(cure 1/6) 11 25 294(cure 2/6) 12.5 315(cure 1/6) 315(cure 1/6) 12 25 242(cure 1/6) 12.5 231 .
; 12.5 189 l 200 221 I 14 10500 266(cure 1/6) _ 100 240(cure 1/6) ; 16 25 288~cure 2/6) 12.5 240(cure 2/6) . 12.5 153 : 50 70 12.5 164(cure 1/6) . I __ . .
. . .
Table 2 (continuation) Compound Dosage (mg / kg) Ratio of Life No. Tested Prolongation (~) 19 25 252(cure 2/6) 12.5 313(cure 3/6) 131(cure 1/6) 12.5 179 21 50 185(cure 1/6) . 25 17~
242(cure 1/6) 12.5 171 23 25 148(cure 1/6) 12.5 300(cure 2/6) 12.5 213~cure 2/6) _ 12.5 135 _ : 50 143 .
12.5 126 _ 400 310(cure 2/6) . 27 200 250(cure 1/6) i 100 230 . 28 100 269 : 50 204 ..
. 7 6 .
Table 2 (continuation) Compound Dosage ( mg / kg ) Ratio of Life No. Tested Prolongation (%) 29 200 269(cure 1/6) 100 204(cure 1/6) 400 219(cure 1/6) 31 200 175(cure 1/6) 400 280(cure 1/6) 33 200 255(cure 1/6)
Claims (11)
1. A condensed quinoline system compound represented by the following formula [I] and salts therof.
(I) In the formula, L represents a lower alkoxy group or a dimethylamino group, M represents a hydroxyl group, methoxycarbonyl group or -NHQ (in this formula, Q
represents hydrogen, -SO,CH,, -COOCH,, -COCH,, -CH,SO,Na or -CH,COOH), X represents hydrogen or a lower alkyl group, Y
represents hydrogen, a lower alkyl group, halogen, -NO2 or -NHR (in this formula, R represents hydrogen, -COCH,, -SO,CH,, ( AC is an acetyl group) or Z represents oxygen, sulfur, CH, or NH.
(I) In the formula, L represents a lower alkoxy group or a dimethylamino group, M represents a hydroxyl group, methoxycarbonyl group or -NHQ (in this formula, Q
represents hydrogen, -SO,CH,, -COOCH,, -COCH,, -CH,SO,Na or -CH,COOH), X represents hydrogen or a lower alkyl group, Y
represents hydrogen, a lower alkyl group, halogen, -NO2 or -NHR (in this formula, R represents hydrogen, -COCH,, -SO,CH,, ( AC is an acetyl group) or Z represents oxygen, sulfur, CH, or NH.
2. A condensed quinoline system compound of claim 1 wherein Z is CH?, L is a lower alkoxyl group or a dimethylamino group, M is -NHQ (in the formula, Q is hydrogen, -SO?CH?, -COOCH?, -CH? SO? Na or -CH?COOH), X is hydrogen or a lower alkyl, Y is hydrogen or a lower alkyl group.
3. A condensed quinoline system compound of claim 1 wherein Z is NH, L is a lower alkoxyl group, M is hydroxyl group, a methoxycarbonyl group or -NHQ ( in the formula, Q
is -SO? CH?, -COOCH? or -COCH? ), X is hydrogen or a lower alkyl, Y is hydrogen, a lower alkyl group, halogen, -NO? or -NHR (in this formula, R is hydrogen, -COCH?, -SO? CH?, or .
is -SO? CH?, -COOCH? or -COCH? ), X is hydrogen or a lower alkyl, Y is hydrogen, a lower alkyl group, halogen, -NO? or -NHR (in this formula, R is hydrogen, -COCH?, -SO? CH?, or .
4. A condensed quinoline system compound of claim 1 wherein Z is sulfur, L is a lower alkoxyl group, M is -NHQ
(in the formula, Q is -SO2CH3 ), X is hydrogen or a lower alkyl group, Y is hydrogen or a lower alkyl group.
(in the formula, Q is -SO2CH3 ), X is hydrogen or a lower alkyl group, Y is hydrogen or a lower alkyl group.
5. A condensed quinoline system compound of claim 1 wherein Z is oxygen, L is a lower alkoxyl group, M is -NHQ
(in the formula, Q is -SO2 CH3 ), X is hydrogen or a lower alkyl group, Y is hydrogen or a lower alkyl group.
(in the formula, Q is -SO2 CH3 ), X is hydrogen or a lower alkyl group, Y is hydrogen or a lower alkyl group.
6. A condensed quinoline system compound of claim 1
7 9 wherein the salt is a pharmaceutically acceptable salt.
7. A condensed quinoline system compound of claim 1 wherein the salt is one selected from the group consisting of salts of hydrochloric acid, phosphoric acid, bromic acid, sulfuric acid, benzoic acid, citric acid, succinic acid, acetic acid, tartric acid and maleic acid.
7. A condensed quinoline system compound of claim 1 wherein the salt is one selected from the group consisting of salts of hydrochloric acid, phosphoric acid, bromic acid, sulfuric acid, benzoic acid, citric acid, succinic acid, acetic acid, tartric acid and maleic acid.
8. A process for preparation of a condensed quinoline system compound represented by formula [Ia] comprising reacting a 4-chloroindenoquinoline derivative represented by formula (12) (in the formula, X is hydrogen or a lower alkyl group, Y is hydrogen or a lower alkyl group) with an aniline derivative represented by formula (14) (in the formula, L is a lower alkoxyl group or a dimethylamino group, M is -NHQ (in the formula, Q is hydrogen, -SO2CH3, -COOCH3, -CH2SO2Na or -CH2COOH)).
[I a]
(In the formula, L, M, X and Y have the same definition as above.)
[I a]
(In the formula, L, M, X and Y have the same definition as above.)
9. A process for preparation of a condensed quinoline system compound represented by formula [Ib] comprising reacting a 4-chloroindenoquinoline derivative represented by formula (19) (in the formula, X is hydrogen or a lower alkyl group, Y is hydrogen, a lower alkyl group, halogen, -NO, or -NHR (in the formula, R is hydrogen, -COCH3, -- SO, CH3, or ) ) with an aniline derivative represented by formula (14) (in the formula, L is a lower alkoxyl group, M is a hydroxyl group, a methoxycarbonyl group or -NHQ (in the formula, Q
is hyarogen, -SO? CH,, -COOCH? or -COCH?)).
[I b]
(In the formula, L, M, X and Y have the same definition as above.)
is hyarogen, -SO? CH,, -COOCH? or -COCH?)).
[I b]
(In the formula, L, M, X and Y have the same definition as above.)
10. A process for preparation of a condensed quinoline system compound represented by formula [Ic] comprising reacting a benzothieno-4-chloroquinoline derivative represented by formula (25) (in the formula, X is hydrogen or a lower alkyl group, Y is hydrogen or a lower alkyl group) with an aniline derivative represented by formula (14) (in the formula, L is a lower alkoxyl group, M is -NHQ (in the formula, Q is -SO2CH3)).
[ I C ]
(In the formula, L, M, X and Y have the same definition as above.)
[ I C ]
(In the formula, L, M, X and Y have the same definition as above.)
11. A process for preparation of a condensed quinoline system compound represented by formula [Id] comprising reacting a benzofurano-4-chloroquinoline derivative represented by formula (30) (in the formula, X is hydrogen or a lower alkyl group, Y is hydrogen or a lower alkyl group) with an aniline derivative represented by formula (14) (in the formula, L is a lower alkoxyl group, M is -NHQ ( in the formula, Q is -SO2 CH3 ) ) .
[ I d ]
(In the formula, L, M, X and Y have the same definition as above.)
[ I d ]
(In the formula, L, M, X and Y have the same definition as above.)
Applications Claiming Priority (4)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP33067488 | 1988-12-27 | ||
| JP330674/1988 | 1988-12-27 | ||
| JP282298/1989 | 1989-10-30 | ||
| JP1282298A JP2659826B2 (en) | 1989-10-30 | 1989-10-30 | TIG welding electrode |
Publications (1)
| Publication Number | Publication Date |
|---|---|
| CA2006666A1 true CA2006666A1 (en) | 1990-06-27 |
Family
ID=26554542
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CA 2006666 Abandoned CA2006666A1 (en) | 1988-12-27 | 1989-12-27 | Condensed quinoline system compound and process of preparation thereof |
Country Status (1)
| Country | Link |
|---|---|
| CA (1) | CA2006666A1 (en) |
-
1989
- 1989-12-27 CA CA 2006666 patent/CA2006666A1/en not_active Abandoned
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