GB2253396A - Imidazoacridines and their antineoplastic use - Google Patents

Imidazoacridines and their antineoplastic use Download PDF

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GB2253396A
GB2253396A GB9204315A GB9204315A GB2253396A GB 2253396 A GB2253396 A GB 2253396A GB 9204315 A GB9204315 A GB 9204315A GB 9204315 A GB9204315 A GB 9204315A GB 2253396 A GB2253396 A GB 2253396A
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Wieslaw Marek Cholody
Jerzy Kazimierz Konopa
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BTG International Ltd
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British Technology Group Ltd
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    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D471/00Heterocyclic compounds containing nitrogen atoms as the only ring hetero atoms in the condensed system, at least one ring being a six-membered ring with one nitrogen atom, not provided for by groups C07D451/00 - C07D463/00
    • C07D471/02Heterocyclic compounds containing nitrogen atoms as the only ring hetero atoms in the condensed system, at least one ring being a six-membered ring with one nitrogen atom, not provided for by groups C07D451/00 - C07D463/00 in which the condensed system contains two hetero rings
    • C07D471/06Peri-condensed systems
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P35/00Antineoplastic agents
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P35/00Antineoplastic agents
    • A61P35/02Antineoplastic agents specific for leukemia

Abstract

Compounds of formula I <IMAGE> in which: R represents: -OH or -OR', wherein R' represents C1-C6 alkyl, R1<a> and R1<b>, which may be identical or different, represent hydrogen or C1-C6 alkyl, unsubstituted or substituted by a hydroxyl, an amino, a N'-alkylamino or a N', N'-dialkylamino group, such N'-alkyl groups containing 1-4 atoms, n is 2-5 and R2 represents hydrogen, or straight chain C1-4 alkyl, in the form of a free base or a pharmaceutically acceptable acid addition salt or an N-oxide are useful in antineoplastic treatment and prophylaxis, especially of leukaemia.

Description

IMIDAZOACRIDINES AND THEIR ANTINEOPLASTIC USE Backqround of the Invention
I. Field of the invention This invention relates to substituted 5E(aminoalkyl)aminolimidazo [4,5,1-delacridin-6-ones and their antineoplastic use,
especially for the treatment of leukaemia, and processes for their production. 2. Description of t e related art
In the paper 115-1(aminoalkyl)aminolimidazo[4,5,1-de)acridin6-ones as a novel class of antineoplastic agents. Synthesis and Biological Activity", J. Med. Chem. 33, 49-52 (1990), W.M. Cholody, S. Martelli, J. Paradziej-Lukowicz and J. Konopa have briefly reviewed tricyclic ring antineoplastic agents and have described new compounds recited in the title. A later paper, by W. Cholody et I]., J. Med. Chem. 33, 2852-2856 (1990), entitled "8-substituted 5-E(aminoalkyl)aminol-6H-v-triazolo[5,4,1-del- acridin-6-ones as potential antineoplastic agents. Synthesis and Biological Activity", describes these compounds, which differ by the replacement of an optionally substituted imidazo C-atom by a triazolo N- atom (unsubstituted) and optionally by the introduction of an 8-substituent selected from nitro, chloro, methyl, methoxy and hydroxy. The results are described as clearly indicating that high antineoplastic activity of those triazolo ring compounds is related to the A ring hydroxylation. However, structure-activity relationships in relation to in vivo evaluation against murine leukaemia remained unclear. It is, therefore, still a problem to find other compounds with high antineoplastic, especially antileukaemic, activity.
Summary of the Invention
The present invention provides compounds of formula I:
R2--, C N 1 2 3 R 4 7 6 5 in which:
(I) 6 5 0 H N, (CH2)n N R a R b 1 1 R represents: -OH or -OR' wherein R' represents C]-C6 alky], e.g. methyl, a b R1 and R,, which may be identical or different, represent hydrogen or C,- C6 alky], e.g. methyl or ethyl, which is unsubstituted or is substituted by a hydroxy], an amino, a W-alkylamino or a N',N'-dialkylamino group, in which the or each 10 alkyl group has 1 - 4 carbon atoms, for example in the substituents: 2-hydroxyethy], 2-aminoethy], 2-M-al kyl amino) ethyl and 2-(N',N'dialkylamino)ethy], n is 2-5 and R2 represents hydrogen, or straight chain Cl-4 alky], in the form of the free bases, their pharmaceutically acceptable acid is addition salts or N-oxides thereof.
Description of the preferred embodiments
Rla and R1b are normally identical and represent alkyl groups e.g. C]-C6 alkyl groups, especially C]-C3 alkyl-, such as methyl or ethyl, n typically being 2 or 3.
The compounds of formula I in which Rla = R1b = methyl or ethyl, R2 = hydrogen or methyl and n is 2 or 3 are of particular interest in treating leukaemia. Of these compounds, those of 3 most interest are those in which:
Ex. 9 Ex. 10 Ex. 11 Ex. 12 Ex. 14 Ex. 15 Ex. 16 R = -OH; R = -OH; R = -OH; R = -OH; R = -OH; R = -OH; R = -OH; R,a = R1b = - CH3; R2 = H; Rla = R1b = - CH3; R2 = CH3; Rla = R1b = - CH2CH3; R2 = H; R,a. R1b = - CH2CH3; R2 = CH3; R,a = R1b = - CH3; R2 = CH3; R,a = R1b = - CH2CH3; R2 = H; R,a = R1b = - CH2CH3; R2 = CH3; n = 3.
n = 2. n = 2.
n = 2. n = 2. n = 3. n = 3.
The methyl ethers are generally less active, but among them the compounds in which n = 2, R2 = H and Rla = Rlb CH3 or CA, (Examples 1 and 2) are the most preferred.
Addition salts which are generally pharmaceutically acceptable, may be of an organic or inorganic acid. Examples of suitable acids for salt formation are: hydrochloric, sulfuric, phosphoric, acetic, citric, malonic, ascorbic, maleic, methanesulfonic, lactic, gluconic, glucuronic, and the like. Usually the compound I is present in the form of a hydrochloride, which could be a mono-, dior tri- salt or any mixture thereof. It can also be hydrated to variable extents.
It is known that N-oxides of chemotherapeutic anthraquinones having tertiary amino groups are useful as pro-drugs for antineoplastic therapy, being bioreductively activated within neoplastic tissue to form the active compound: see UK Patent Specification 2 237 283A (NRDC). Mild oxidation, under conditions which will not cause disruption of the imidazole ring, can be used to make N-oxides, of the imidazole N-atom or of a tertiary amine group present when Rla and Rlb are not hydrogen atoms.
Compounds of formula I (in which R2 represents hydrogen or a said alkyl group) may be produced as free bases or salts by treating a compound of formula II, optionally in the form of an acid addition salt thereof, H NH2 1 N R 0 H,W,(CH2)n N R a R b 1 1 01) respectively with formic acid or a compound of formula R2CON(CH3)2, preferably at elevated temperature, typically at reflux in the absence of added solvent. Salts can readily be converted to free bases and free bases to salts or N-oxides by methods known per se.
Compounds of formula II, optionally in the form of acid addition salts, may be produced from compounds of formula III by treatment thereof to reduce the nitro group to the corresponding amino group:
H N02 1 N 1 1 R n Kt (ED NRCLW] H' "(CH2)n 1 1 Compounds of formula III can be prepared as described in European Patent Application EP-A 145 226 (Warner-Lambert Company) or procedures analogous thereto. The reduction of the nitro group is preferably carried out by hydrazine hydrate, suitably in the presence of a catalyst, e.g. Raney Nickel, in a polar solvent such as tetrahydrofuran (THF). The intermediates II thus obtained are generally extremely unstable to oxygen, especially in those compounds wherein n represents 3 and are usually used as starting materials for conversion to compounds of formula I in the form of acid addition salts, for example hydrochlorides.
The present invention further includes within its scope an intermediate of formul.a II, preferably in the form of an acid addition salt.
Two methods are generally used for isolation of the final products. In the case of methoxy derivatives, the products may be extracted with benzene or chloroform from the reaction mixture after rendering the mixture alkaline and next transformed into dihydrochlorides. The hydroxy compounds may instead be isolated as hydrochloride salts directly from the reaction mixture after acidification with HCl.
Compounds of formula I are of interest for the treatment or prophylaxis of neoplasms (a term used herein to refer to any malignant tissue growth and therefore to include cancers and leukaemias), especially lymphoblastic leukaemias. All the compounds of the invention tested appear to have antileukaemic activity in the in vitro and/or in vivo tests reported hereinafter (see Table III). In.vivo tests of selected compounds of the invention against tumours in animals have shown that the compounds of Examples 11 and 12 are active against the MT-3 human mammary caninoma and the compounds of Examples 12 and 15 against colon 38 adenocarcinoma and B16 melanoma. In vitro data shows that compounds of Examples 10 and 16 have potent activity against renal cancer cell lines.
Accordingly, in a further aspect the present invention comprises a compound of formula I for use in therapy and, in a yet further aspect of the present invention, comprises the use of a compound of formula I for the manufacture of a medicament useful in antineoplastic treatment or prophylaxis.
The dosage form and amount can be readily established by reference to known antineoplastic treatment or prophylactic regimens. In general, however, the dosage of the compound of formula I usually lies within the range about O.1mg to about 50mg/kg, preferably 0.5mg to 10mg/kg.
The compound of formula I can be administered alone or in connection with, one or more pharmaceutically acceptable diluents or carriers therefor, and optionally, any other ingredients which may be therapeutic per se, synergistic with the compound of formula I, or both. Carrier(s) and diluents are, of course, pharmaceutically acceptable and compatible with the other ingredients of the formulation.
Formulations suitable for oral, rectal, topical or parenteral (including subcutaneous, intramuscular and intravenous) administration are included. Unit dosage forms may be prepared by known methods. All methods generally include the step of bringing the active compound into association with a carrier or diluent, as a suspension or solution, and optionally one or more accessory ingredients, e.g. buffers, flavouring agents, binders, surface is active agents, thickeners, anti-caking agents, lubricants and preservatives (including antioxidants).
Formulations of the present invention suitable for oral administration may be presented as capsules, cachets, tablets or lozenges, powder or granules; or a suspension. Tablets may be prepared by compressing the active compound in a free-flowing form such as a powder or granules, optionally mixed with conventional additives. A syrup may be made by adding the active compound to a concentrated, aqueous solution of a sugar, for example sucrose, optionally containing conventional additives. Formulations suitable for parenteral administration conveniently comprise a sterile aqueous preparation of the active compound which is preferably made isotonic.
The present invention is illustrated by the following Examples:- EXAMPLES
General Procedure Compounds of formula I, the subject of Examples 1 to 16, are produced by the route outlined in Scheme 1.
SCHEME 1 H N02 1 N 1 1 H2MCH2) NR CL R b - 1 1 OR) R n 1 1 R 0 CL 0 A.,( NR CIRb H CH2)n 1 1 H N02 1 DMF N R=OCH3 or OH R2C N 1 N R 0,N NR CL R b H '(CH2)n 1 1 (I) DMF = dimethylformamide, THF = tetrahydrofuran, = dimethylacetamide.
THF W2NH2W H NH2 1 formic acid or OMA N R 0 W, W, ( CH2)n N R aR b 1 1 In the following Examples melting points were taken on a Buchi 510 capillary melting points apparatus and are uncorrected. 1H NMR spectra were recorded on a Varian VXR-300 spectrometer operating at 300 MHz. Chemical shifts are reported as 8 units in ppm downfield from internal tetramethylsilane. NMR abbreviations used are as follows: br(broad), s(singlet), d(doublet), t(triplet), qu(quartet), qt(quintet), m(multiplet), ex(exchangeable with deuterium oxide). Quartets which by addition of deuterium oxide are transformed into triplets are labeled with. Single frequency decoupling was utilized to assign specific protons. Coupling constants are given in Hz. Microanalytical results, indicated by atomic symbols, are within 0.4% of the theoretical values.
EXAMPLE 1
A.]-[[2-(Diethylamino)ethyllaminol-7-methoxy-4-nitro-g(IOH)- acridinone.
A mixture of 4.57g (0.015 mol) 1-chloro-7-methoxy-4-nitro 9(100-acridinone, 25 m] DMF and 7.00g (0.06 mol) 2-diethy] aminoethylamine is stirred and heated at 600C for 30 minutes.100 m] 4TI. (vlv) MeOH-water solution is added to the reaction mixture, heated to boiling and after cooling left overnight in a refrigerator. The crystallized product is collected by filtration washed with water (150 mD and MeOH (50 m]) and dried to give 5.30g. (92%) analytically pure product as yellow needles: mp 178-1790C (lit.mp., European Patent Appl. EP-A 145226, Chem. Abstr. 1985, 103, 215182s., 179-180C); B. Preparation of 7substituted-4-amino-]-[[(dialkylamino)alkyllaminol9(10H)-acridinone Hydrochloride Salts.
To a mixture of nitro derivatives (0.01 mol), 200 m] THF, and about 2.5g of Raney Ni is added with stirring at room temperature then 2 m] hydrazine monohydrate. Stirring is continued for about 30 minutes. The catalyst is filtered off and washed with THF (50 m]). The filtrate is quickly treated with 10 m] concentrated hydrochloric acid and stirred for 10 minutes.
The yellow precipitate obtained is collected and washed with THF.
The product is recrystallized from a solution of MeOH (go%) dioxane made acidic with HC1 (pH-2).
C. Preparation of 5-[[2-(diethylamino)ethyliaminol-8-methoxyimidazo[4.5.1-del acridin-6-one Dihydrochloride.
A mixture of 1.71g (4 mmol) of the product from the procedure of Example 16 and 20 ml 95% formic acid is heated at reflux for 6h.
Acid is evaporated and the residue is dissolved in water (100 ml).
The solution is made basic (pH 9) by addition of sodium carbonate and product is extracted with chloroform (2 x 100 ml). The organic extracts are dried and evaporated to give a residue which is dissolved in EtOH. The solution is made acidic with HCl and product is crystallized by addition of acetone to give the title product.
EXAMPLE 2
Compound I: n=2, R=OCH3, R,a=R,b=CH 3, R2=H.
The procedures M, H and M of Example 1 are followed but dimethylaminoethylamine is used in place of diethYlaminoethy] amine in 1A.
EXAMPLE 3
Compound I: n=2, R=OCH3, R,a=R,b=CH3, R2=CH3.
The procedures M and 1B of Example 1 are followed using dimethylaminoethylamine in place of diethylaminoethylamine.
The product is then subjected to the following procedure (designated X):
A mixture of 2.14g (5 mmol) hydrochloride and 30 m] DMA is refluxed for 12h, 200 m] water is added to the reaction mixture, made basic with sodium hydroxide and the product is extracted with benzene (2.150 ml). The extracts are evaporated to dryness and the residue is dissolved in methanoldioxane O:D mixture. The solution is made acidic with gaseous HCl and the crystallized product is collected by filtration to give yellow crystals.
EXAMPLE 4
Compound 1: n=2, R=OCH3, R,a=R,b=CH2CH3, R2=CH3.
The procedures M and]B of Example 1 are followed and the product is subjected to procedure 3C.
EXAMPLE 5
Compound I: n=3, R=OCH3, R1a=R,b=CH3, R2=K The procedures M, H and 1C of Example 1 are followed but di methyl ami nopropyl ami ne is used in place of di ethyl ami noethyl amine in procedure M.
EXAMPLE 6
Compound I: n=3, R=OCH3, R,a=R,b=CH3, R2.CH3.
The procedure of Example 5 is followed but procedure 3C replaces procedure]C.
EXAMPLE 7
Compound I: n=3, R=OCH3, R,a=R,b=CH.CH3, R2=H.
The procedures M,]B and 1C of Example 1 are followed but diethylaminopropylamine is used in place of diethylaminoethy] amine in procedure M.
EXAMPLE 8
Compound I: n=3, R=OCH3, R,a=R,b=CH2CH3, R2=CH3.
The procedure of Example 7 is followed but procedure 3C replaces procedure 1C.
EXAMPLE 9 Compound I: n=2, R=OH, R,a=R,b=CH3, R.=H.
The procedure of Example 1 is followed but dimethylaminoethylamine is used in place of diethylaminoethylamine and 1-chloro-7hydroxy-4-nitro9(IOH)-acridone is used in place of 1-chloro-7-methoxy-4-nitro-9(10H)acridone in procedure M and procedure K is replaced by the following, designated 9C:
A mixture of 5 mmol of dihydrochloride salt and 20 ml of 95% formic acid is refluxed for 8h. Formic acid is evaporated and the residue is dissolved on heating in methanol. 3 ml conc. hydrochloric acid is added to the hot solution and the product is crystallized by addition of acetone. The product is collected by filtration and recrystallized from a methanol-acetone mixture.
EXAMPLE 10 Compound I: n=2, R=OH, R,a=Rlb=CH3, R2=CH3- The procedure of Example 9 is followed but the following procedure, designated IOC, replaces 9C:
A mixture of 5 mmol of dihydrochloride salt and 25 ml of DMA is refluxed for 12h. About 20 ml of the solvent is evaporated, 100 ml acetone is added to the residue and the solution is acidified with gaseous HC1. The precipitated product is collected by filtration and washed with acetone. Crude product is recrystallized (if necessary twice) from methanolacetone to give the respective dihydrochloride salt.
EXAMPLE 11 Compound I: n=2, R=OH, Rla=Rlb=CH2CH3, R2=H.
The procedure of Example 9 is followed but diethylaminoethy] amine is used in place of dimethylaminoethylamine in procedure M.
EXAMPLE 12
Compound I: n=2, R=OH, R,a=Rb=CH2CH3, R2=CH3.
The procedure of Example 10 is followed but diethylamino ethylamine is used in place of dimethylaminoethylamine in procedure M.
EXAMPLE 13
Compound I: n=3, R=OH, R,a=R,b=CH3, R2=H.
The procedure of Example 9 is followed but dimethylamino propylamine is used in place of dimethylaminoethylamine in procedure]A.
- 12 EXAMPLE 14 Compound I: n=3, R=OH, R,a=Rb=CH3, R,=CH3.
The procedure of Example 13 is followed but procedure IOC replaces procedure 9C.
EXAMPLE 15 Compound I: n=3, R=OH, R,a=R,b=CH2CH3, R2=H.
The procedure of Example 13 is followed but diethylaminopropylamine is used in place of dimethylaminopropylamine in procedure]A.
EXAMPLE 16 Compound I: n=3, R=OH, R,a=R1b=CH2CH3, R2=CH3.
The procedure of Example 15 is followed but procedure 1OC replaces procedure 9C.
Intermediates Melting points, yields and molecular formulae of starting compounds (III) and intermediates (ID are set forth in Table I.
- 13 TABLE I I-Substituted 4-Nitro-9(10H)-acridinones (III) and ISubstituted 4-Amino-7-methoxy-9-(10H)-acridinones (ID Compd n R R,a = mp,C yield,% molecular formula Rlb UID 2 OCH3 CH3 242-243d 96 Cl8H2ON404 2 OCH3 CH2CH3 178-17ge 92 C20H24N404 3 OCH3 CH3 165-166 94 ClqH22N404 If 3 OCH3 CH2CH3 153-154f 97 C2lH26N404 2 OH CH3 258-260 90 C17H18N404 2 OH CH2CH3 227-229 94 ClqH22N404 3 OH CH3 213-2149 82 C18H20N404 3 OH CH2CH3 208-210 86 C20H24N404 (ID 2 OCH3 CH3 240-243 dec. 79 C18H22N402.2HCI 2 OCH3 CH2CH3 227-231 dec. 74 C20H26N402.2HCI 3 OCH3 CH3 232-235 dec. 80 CIqH24N402.2HCl 3 OCH3 CH2CH3 180-185 dec. 84 C2lH28N402.3HC1 The analyses are within 0.4% of the theoretical val,ues for C, H and N.
Final Compounds Melting points, yields and molecular formulae of compounds of the invention are set forth in Table II, with reference to formula 1. It will be'appreciated that such compounds can readily be prepared as the free bases or as other acid addition salts and/or hydrates and therefore that the disclosure of Table II is not to be construed as limited by such particular forms of compound. NMR spectra of certain compounds are shown below.
Compound I: R=OCH3, R,a=R1b=CH2CH3, R2=H, n=2. (Ex.3) N NMR (free basO(Me2SO-dO G 9.13(s, 1H,CIA), 8.98Q,1H, ex,-NH-CH2), 8.36(d,IH,J=9.1,CIO-H), 7.98(d,IH,J=8.9,C3-H), 7.79(d,IH,J=3.0,C7-H), 7.52(dd,1H,J=9.1,J=3.0,C9-H), 6.80(d,IH, J=8.9,C4-H), 3.92(s,3H,-OCH3), 3.42(qu,2H,-NH-CH2-CH2-), 2.73(t, M-CH2-CH2-NEt2), 2.58(qu,4H,-N(CH2-CH3)2), 1.02(t,6H,-N(CH2 CH3)2).
Compound I: R=OCH3, R,a=R,b=CH2CH3, R2=CH3, n=2. (Ex.4) ]H NMR (free base) (Me2SO-dO & 8.98(t,IH,ex,-NH-CH2), 8.12(d,IH,J=9.2,CIO-H), 7.82(d,IH,J=3.2,C7-H), 7.80(d,1H,J=8.8, C3-H), 7.43(dd,1H,J=9.2,J=3.2,C9-H), 6.70(d,IH9J=8.8,C4-H), 3.91(s,3H,-OCH3), 3.38(qu,2H,-NH-CH2-CH2-), 3.00(5,3H,Cl-CH3), 2.72(t,2H,-CH2-CH2-NEt2), 2.58(qu,4H,-N(CH2-CH3)2), 1.03(t,6H, N(CH2-CH3)2)- Compound I: R=OH, R,a=R,b=CH2CH3, R2=H, n=2. (Ex.11) ]H NMR (free base) (Me2SO-dO & 10.00(s,IH,ex,C8-0H), 9.0Ms,1H,Cl-H), 8.99(t,IH,ex,-NH-CH2-), 8.26(d,IH,J=8.9,CIO-H), 7.95(d,IH,J=8.8,C3-H)., 7.72(d,1H,J=2.8,C7-H), 7.33(dd,1H,J=8.9, J=2-8,GA), 6.77(d,IH,J=8.8,C4-H), 3.40(qu,2H,-NH-CH2-CH2-), 2.70(t,2H,-CH2-CH2-NEt2), 2.56(qu,4H,-N(CH2-CH3)2), 1.01(t,6H, N(CH2-CH3)2).
Compound I: R=OH, R,a=Rb=CH.CH3, R2=CH3, n=2. (Ex.12) % NMR (free base) (ME2SO-dO 6 10.00(s,IH,ex,C8-0H), 9.02(t,IH,ex,-NH-CH2-), 8.11(d,IH,J=9.],(CIO-H, 7.8Ed,1H,J=8.8, C3-H), 7.79(d,IH,J=2.9,C7-H), 7.33(dd,1H,J=9.1,J=2.9,C9-H), 6.72(d,IH.,J=8.8,C4-H), 3.38(qu,2H,-NH-CH2-CH2), 3.02(s,3H,Cl CH3), 2.72(t,2H,-CH2-CH2-NEt2), 2.56(qu,4H,-N(CH2-CH3)2), 1.02(t, 6H,A(CH2-CH3)2).
- is - Compound I: R=OH,Rla=R1b=CH2CH3,R2=H, n=3. (Ex.15) ]H NMR (free base) (ME2SO-dO 6 10.02(br s,1H,ex,C8-OW, 9.10(s,1H,CIA), 8.93(t,IH,ex,-NH-CH2-), 8.27(d,IH,J=8.9,CIO-H), 7.97(d,IH,J=8.8,C3-H), 7.73(d,IHJ=2.8,C7-H), 7.34(dd,1H,J=8.9, J=2.8,GA), 6.81(d,1H,J=8.8,C4-H), 3.42(qu,2H,-NH-CH2-CH2-), 2.52(t,2H,CH2-CH2-NEt2), 2.48(qu,4H,-N(CH2,CH3)2), 1.78(qt,2H, CH2-CH2-CH2-), 0.96(t,6H,-N(CH2-CH3)2).
Compound I: R=OH, R,a=R,b=CH2CH3, R2=CH3, n=3. (Ex.16) ]H NMR (free base) (Me2SO-d6) & 10.0(br s,1H,ex,C8-ON), 8.91(t,IH,ex,-NH-CH2-), 8.08(d,1H,J=9.1,CIO-H), 7.80(d,1H,J=8.8, C3-H), 7.77(d,1H,J=3.0,C7-H), 7.32(dd,IH9J=9.1,J=3.0,C9-H), 6.70(d,IH,J=8.8,C4-H), 3.38(qu,2H,-NH-CH2-CH2-), 3.00(s,3H,Cl CH3), 2.48(m,6H,-CH2-CH2-N(CH2-CH3)2), 1.76(qt,2H,-CH2-CH2-CH2-).
TABLE II
Formulae, melting points and yields of 8-substituted 5-aminoimidazoF4.5.1delacridin-6-ones of formula I R2--, C N 2 3 4 D R (I) 7 6 5 0 H, W, (CH2)n N R a R b 1 1 EX n R R,a = R2 mp,OC yield formula c R 1 b % 1 2 OCH3 CH2CH3 H 250-254 decd 68 C21H20402.1.75HCl 2 2 OCH3 CH3 H 254-258 dec 90 C19H2ON402.1.5M 0.75H20 3 2 OCH3 CH3 CH3 255-259 dec 82 C20H22N402.2 KM20 4 2 OCH3 CH2CH3 CH3 238-241 dece 70 C22H28N402.2 HCl 3 OCH3 CH3 H 237-241 dec 70 C20H22N402.2 HCL0.2H20 6 3 OCH3 CH3 CH3 252-256 decf 68 C21H24N402.1.85 HCl 7 3 OCH3 CH2CH3 H 246-250 dec 72 C22H26N402.1.5 HCl 8 3 OCH3 CH2CH3 CH3 203-208 dec 64 C23H28N402.2 KM20 9 2 OH CH3 H 260-264 dec 77 C18H18N402.2 HCM20 2 OH CH3 CH3 268273 dec 68 C19H2ON402.2 HCL2H20 11 2 OH CH2CH3 H 250-255 decg 72 C20H22N402.2 HCIA20 12 2 OH CH2CH3 C H3 260-265 dech 78 C21H20402.1.5HCl 0.5H20 13 3 OH CH3 H 247-251 dec 70 C19H2ON402.2 HCl 14 3 OH CH3 CH3 268-271 deci 69 C20H22N402.2 HCL0.5H20 3 OH CH2CH3 H 269-272 deci 70 C21H21N402.2 KM20 16 3 OH CH2CH3 CH3 238-242 deck 66 C22H26N402.2 KM20 (c) Microanalyses are within 0.,V1. of the theoretical values for C, H and N. (d) Free base mp 191-193 OC. (e) Free base mp 156-158 OC. (f) Free base mp 156-158 T. (g) Free base mp 239-242 OC. (h) Free base mp 255-258 T. (i) Free base mp 242-245 T.
(j) Free base mp 222-225 'C. (k)Free base mp 240-245 T.
Bioloqical Tests In Vitro Cytoxicity Evaluation The mouse L1210 leukaemia cells (RPMl, USA) are grown in RPM1 1640 medium supplemented with 5% fetal calf serum and penicillin (1,000,000 units /litre) plus streptomycin (100 mg/litre) in controlled air-5% C02 humidified atmosphere at 370C. L1210 mouse leukemia cells are seeded at a density of 5xlO4 cells/ml. The tested compounds, dissolved in 50% ethanol, are added, at four different concentrations, to the cell suspensions. The cytotoxic activity (IC50 value) of the tested compounds is defined as their concentrations causing 50% growth inhibition after 48h, measured by cell protein contents and is determined from dose-response curves by the method of J. Konopa, A. Matuszkiewicz, M. Hrabowska, K.
Onoszko, Arzneim.-Forsch. 1974, 24, (1971).
In Vivo Antileukaemic Evaluation BDF, mice are injected ip with 106 P388 lymphotic leukemia cells on day 0 and treated ip on days 1-5 in accordance with the protocols described by the National Cancer Institute:
R.I. Geran, et al., Cancer Chemotherapy Reports, Part 3, 3(2), 1-103 (1972) [ISSN=0069-01391. The mean survival time (MST) for each treatment group (eight mice) is calculated and the percent of T/C was determined by using the following formula:
%T/C=[(MST treated)/(MST control)IxIOO.
Results of the Cytotoxicity Evaluation and Antileukaemic Evaluation are set forth in Table III:
- 18 TABLE III Formulae and activities against Murine L1210 in vitro and P388 leukemia in vivo of 8-substituted 5-aminolmidazo[4.5.1delacridin-6-ones of formula I R2--, C - N 1 2 CNI 3 R 8 7 6 5 H N, (CH2)n N R a R b 1 1 L1210 leukaemia P 388 leukaemia in vitro in vivo a optimal EX n R R, R IC50 dose % R 1 b 2 (Pg/M1) (PM) (mg.lkg.) TC 1 2 OCH3 CH2CH3 H 0.78( 0.02) 1.8 100 183,209 2 2 OCH3 CH3 H 0.65GO.07) 1.6 100 177,136 3 2 OCH3 CH3 CH3 0.34( 0.09) 0.77 150 127 4 2 OCH3 CH2CH3 CH3 0.70G0.40) 1.55 150 136,120 3 OCH3 CH3 H 3.50( 0.75) 8.25 150 164 6 3 OCH3 CH3 CH3 1.40( 0.60) 3.2 150 136 7 3 OCH3 CH2CH3 H 1.10( 0.32) 2.5 150 142 8 3 OCH3 CH2CH3 CH3 0.70( 0.17) 1.4 150 108 9 2 OH CH3 H 0.02( 0.01) 0.048 12.5 210,210 2 OH CH3 CH3 0.06GO.03) 0.135 12.5 200,250 11 2 OH CH2CH3 H 0.013( 0.008) 0.031 5 211,175 12 2 OH CH2CH3 CH3 0.11GO-08) 0.25 75 280,290 13 3 OH CH3 H 0.014( 0.005) 0.034 5 183 14 3 OH CH3 CH3 0.10( 0.07) 0.23 100- 255 3 OH CH2CH3 H 0.08GO.05) 0.18 25 309,230 16 3 OH CH2CH3 CH3 0.40( 0.21) 0.89 25 150,155 When two values are given, the second one represents the result obtained during repeated independent multidose assay.
1 9 - Free-radical testing Many anti-cancer compounds exhibit cardiotoxic side effects which are usually ascribed to the liberation of free radicals. Accordingly four representative compounds of the invention, those 05 of Examples 1, 11, 12 and 15, were tested in rat liver microsomes, in comparison with doxorubicin. Whereas 50OpM of doxorubicin in NADPH- supplemented rat liver microsomes, under nitrogen purging, gave an electron spin resonance (ESR) signal indicative of the presence of doxorubicin semiquinone free radical, the same molar 10 concentration (500^ of the four compounds of the invention gave no ESR spectrum over a three hour period.
Compounds of formula I:

Claims (10)

  1. R2--, C N 1
  2. 2 N1
  3. 3
  4. 4 R 8 7 6 0 H,N,, (CH2)n N R a R b 1 1 in which:
    (I) R represents: -OH or -OR', wherein R' represents C]-C6 al kyl, Rla and Rlb, which may be identical or different, represent hydrogen or CI-C6 alkyl, unsubstituted or substituted by a hydroxyl, an amino, a N'alkylamino or a N',N'-dialkylamino group, such N'-alkyl groups containing 1-4 carbon atoms, n is 2-
  5. 5 and R2 represents hydrogen, or straight chain CI-4 alkyl, in the form of a free base or a pharmaceutically acceptable acid addition salt, or an N-oxide thereof. 2. Compounds according to Claim 1, in which Rla and Rlb are identical. 3. Compounds according to claim I or 2, in which Rla or Rlb or both represent a Cl-C3 alkyl group. 4. Compounds according to claim 1, 2 or 3, in which n is 2 or 3. 5. Compounds according to claim 1, in which R = -OH, Rla = Rlb 20 methyl or ethyl, R2 = hydrogen or methyl and n is 2 or 3.
    - 21
  6. 6. A process for the production of a compound of formula I clai med in claim 1, wherein a compound of formula II, optionally in the form of an acid addition salt thereof, H NH2 1 N R' 0 H A,,( CH2)n N RaR b 1 1 (11) is treated with formic acid or an N,N-dialkylamide of formula R2CON(CH3)2, R2 representing straight chain CI-4 alkyl, and, if necessary, an acid addition salt is converted to the free base or the free base to a pharmaceutically acceptable acid addition salt or to an N-oxide.
  7. 7. Compounds according to claim I for use in therapy.
  8. 8. The use of a compound according to claim I for the manufacture of a medicament useful in antineoplastic treatment or prophylaxis.
  9. 9. A pharmaceutical composition which comprises a compound according to claim 1, 2, 3, 4 or 5, in association with a pharmaceutically acceptable diluent or carrier therefor.
  10. 10. Each of the individual compounds according to claim I hereinbefore set forth, in the form of free bases or any of their pharmaceutically acceptable acid addition salts.
    92FEB/79
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