NO882368L - Phosphine. - Google Patents

Description

The present invention relates to new phosphine compounds that have tumor cell growth-inhibiting activity, pharmaceutical compositions containing an effective, tumor cell growth-inhibiting amount of such a phosphine compound, and a method for treating tumor cells that are sensitive to such a compound by providing tumor cell growth-inhibiting amounts of a phosphine compound to a host animal affected by such tumor cells.

The heterocyclic phosphine compounds of this invention are not known. Cariati et al., Inorg. Chim. Acta, 1 (2), 315-318 (1967); Bates et al., Inorg Chim. Acta, 81 (2), 151 - 156

(1984) and McAuliffe et al., J.C.S. Dalton, 1730 (1979), describes bis|_1 , 2-bis (dif enylph osf in ) ethanej gold (I) chloride .

The digold compounds in some of the pharmaceutical mixtures of this compound are known. Sadler et al., J. Chem. Soc, Dalton Trans, 969 - 974 (1 984), proposes the synthesis of di-., chlorobis[i,2-bis(diphenylphosphine)ethane]digold(I), but is unable to isolate the compound. Schmidbaur et al., Chem.

Ber, 110, 2751 - 2557 (1977), describes dichlorobis[i,2-bis(dife-nylph osf in ) methane]] digold (I). Stringer et al., abstracts of the 15th Middle Atlantic Regional Meeting of the American Chemical Society, January 7-9, 1981, Washington, D.C., describe the synthesis of dichlorobisf 1 , 2-bis (diethylph osf in ) ethane] digulK I ), and diper-chloratobis[i,2-bis(diethylphosphine)ethane]digold(I), establishing that these three compounds were examined for activity in adjuvant-induced arthritis in the Charles River wistar rat. However, there is no mention in Stringer et al. the publication that such compounds actually have anti-arthritis or some other therapeutically useful biological activity.

Struck et al., J. Med. Chem., 9, 414-416 (1966), describes cytotoxic activity for 1,2-bis(diphenylphosphine)ethane which is used as a starting material for the preparation of some of the pharmaceutical compositions and methods of treatment in this invention.

None of the aforementioned publications describe or suggest the compounds, pharmaceutical mixtures or methods of treatment in the present invention.

This invention relates to methods with the formula

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in which:

R is the same and is 2-pyridyl, 4-pyridyl, 2-thienyl or 2-furyl;

X is the same and is halogen or thiosugar;

M is 0 or 1, provided that when M is 1, R is 2-pyridyl or 4-pyridyl; and

A is a straight or branched alkanediyl chain with from one to six carbon atoms.

When X is thiosugar, the bond of X to the gold atom goes through the sulfur atom of the thiosugar.

This invention also relates to a compound of the formula

in which:

R<1> is the same and is 2-pyridyl;

A is the same and is a straight or branched alkanediyl chain of from one to six carbon atoms; and

X^ is the same and is halogen.

This invention therefore relates to a pharmaceutical mixture comprising an effective, tumor cell growth-inhibiting amount of an active ingredient and an inert, pharmaceutically acceptable carrier or diluent, in which the mixture is useful for inhibiting the growth of animal tumor cells which are sensitive to the active ingredient, and where the active ingredient is a compound of formula (I) or a compound of the formula:

in which:

2 R is the same and is phenyl, ethyl or 2-pyridyl; A is a straight or branched alkanediyl chain of from one to six carbon atoms; Y is a chain between the four P atoms with the structure

and

X is halogen;

provided that when Y is

and a pharmaceutically acceptable carrier.

Another aspect of this invention relates to a method of inhibiting the growth of animal tumor cells sensitive to compounds of formula (I) or formula (III), wherein an animal affected by the tumor cells is given an effective tumor cell growth inhibitory amount of a compound of formula (I) or formula (III).

One skilled in the art will see that all the compounds of formula (II)

is covered by the framework of formula (III).

By the term "thiosugar" is meant any 1-thioaldose. Examples of such thiosugars are 1-thioglucose, 1-thiogalactose, 1-thiomannose, 1-thioribose, 1-thiomaltose, 1-thiofucose, tetra-O-acetyl-1-thioglucose, tetra-O-acetyl-1-thiomannose, tetra -O-acetyl-1-thiogalactose, tri-O-acetyl-1-thioribose, hepta-O-acetyl-1-thiomaltose and tri-O-acetyl-1-thiofucose.

All the compounds of formulas (I), (II) and (III) can be prepared by methods available to a person skilled in the art.

In general, compounds of formula (I) in which M is 0 can be prepared by reacting the corresponding heterocycle in an anhydrous ethyl ether with an organolithium reagent such as n-butyllithium in a non-reactive organic solvent with the corresponding compound of the formula:

where A is defined as above.

All the necessary heterocycles, organolithium reagents

and formula A compounds can be purchased, e.g. from Strem Chemicals, Inc., Newburyport, Massachusetts.

In general, the starting materials for the compounds of formula (I) in which M is 1 and X is chlorine are the corresponding diphosphinohydrocarbons of formula (I) in which M is 0. To obtain the digold products of formula (I) a corresponding diphosphinohydrocarbon is reacted bon with formula (I) either directly with chlorosulfuric acid tetrahydrate or a reduced form of the acid hydrate produced by treatment with thiodiglycol in a corresponding non-reactive organic solvent.

To obtain the compounds of formula (I), in which X is thiosugar, the corresponding compound of formula (I) in which X is chlorine is reacted with the corresponding sodium thiosugar. The necessary sodium-umthiosugars can be purchased, e.g. from Sigma Chemical Co., St. Louis, Missouri, or prepared by conventional techniques.

Formula (I) compounds in which X is bromine are prepared by

reacting the corresponding ligand of formula (I) wherein M is 0 with bromogold acid hydrate (available for example from Strem Chemicals, Inc., Newburyport, Massachusetts), which has been reduced by treatment with thiodiglycol; or by reacting the corresponding ligand of formula (I) in which M is 0 with bromogold acid hydrate directly in a corresponding non-reactive organic solvent. Alternatively, compounds of formula (I) in which X is bromine are prepared by reacting the corresponding compound of formula (I) in which X is chlorine, with sodium bromide in a suitable organic solvent such as aqueous ethanol or DMF.

Formula (I) compounds X is iodine are prepared by treating the corresponding compound of formula (I) in which X is chlorine or bromine with sodium iodide in a corresponding organic solvent such as acetone.

In general, compounds of formula (II) can be obtained by reacting the corresponding compound of formula (I) in which M is 0 or 1 with the corresponding compound of formula (I) in which M is 0 in a corresponding non-reactive organic solvent.

In general, the compounds of formula (III) in which Y is

is prepared by reacting one mole of the corresponding ligand of formula: with one mole of the corresponding gold complex of formula:

in which R"^ is the same and is phenyl or ethyl; X<1> is halogen and A is as defined above, in a non-reactive organic solvent.

All the necessary formula B ligands can be purchased, e.g. from Stren Chemicals, Inc., Newburyport, Massachusetts.

The formula C gold complexes in which X^ is chlorine are readily prepared by reacting the corresponding ligand of formula B with chlorosulfuric acid tetrahydrate which has been reduced by treatment with thiodiglycol. Formula C gold complexes in which X 1 is chlorine can also be easily prepared by reacting the corresponding ligand of formulas B directly with chlorosulfuric acid hydrate in a corresponding non-reactive organic solvent.

Complexes of formula C in which X^ is bromine are prepared by reacting the corresponding ligand of formula B with bromogold acid hydrate (which can be purchased, for example, from Strme Chemicals, Inc., Newburyport, Massachusetts) which has been reduced by - treatment with thiodiglycol, or by reacting the corresponding ligand of formula B directly with bromogold acid hydrate in a corresponding non-reactive organic solvent. Alternatively, formula C complexes in which X^ is bromine are prepared by reacting the corresponding compound of formula C in which X^ is chlorine with sodium bromine

f

mid in a suitable organic solvent such as aqueous ethanol or DMF-

Formula (III) compounds, in which X is bromine, are prepared by reacting one mole of the corresponding compound of formula C, in which X^ is bromine, with one mole of the corresponding compound of formula B. Alternatively, formula (III)- compounds wherein X is bromine by reacting the corresponding formula (III) compound wherein X 1 is chlorine with sodium bromide in a suitable organic solvent such as aqueous ethanol or DMF.

Compounds of formula (III) in which X^ is iodine are prepared

by reacting the corresponding compound of formula (III) wherein X is chlorine or bromine, with sodium iodide in a suitable organic solvent, such as acetone.

Compounds of formula (I) and (III) have tumor cell growth inhibitory activity which has been demonstrated in at least one animal tumor model.

P388 lymphocyte leukemia is currently the most widely used animal tumor model for investigating antitumor agents and for detailed assessment of active compounds. This tumor system is widely accepted as an antitumor agent investigation tool because it is sensitive to practically all clinically active antineoplastic agents, quantitative and reproducible, suitable for large-scale investigation, and predictable for activity in other animal tumor models. Drugs that are highly active in intraperitoneal (ip) P388 leukemia are generally active in other tumor models as well. The antitumor activity of compounds of formula (I) and (III) is demonstrated in the P388 leukemia mouse model using the following protocol: 10 P388 leukemia cells are inoculated ip into B 6D2F^ mice. Twenty-four hours later, if the tumor inoculum is found to be free of bacterial contamination (as determined by 24 hours of incubation in thioglycollate medium), animals are statistically divided into groups of 6 and housed in shoebox cages. The compound to be examined is dissolved in saline if it is soluble therein or in a minimal volume of either N,N-dimethylacetamide (DMA) or 95% ethanol (depending on solubility). An equal volume of salt water is added to these compounds dissolved in an organic carrier, and if the drug falls out of the solution, an equal volume of polyethoxylated castor oil is added and then salt water up to such a concentration that the desired dose is delivered in 0.5 ml. The final concentration of DMA, ethanol and/or polyethoxylated castor oil is -10%. Dilutions for lower doses are made with saline, like this

that there is an increase in the proportion of organic solvents in the carrier with decreasing dose. These carriers provide soluble formulations (or suspensions). The formulations are prepared immediately before injection. The compound is given ip on days 1 through 5 (ie, treatment begins 24 hours after tumor inoculation). Each experiment contains three groups of 6 animals as untreated controls and animals treated with a positive control, cisplatin, at two dose levels. The animals are weighed as one group on days 1,

5 and 9, and the average weight change (& weight) is used

as a measure of toxicity. Each experiment also contains an inoculum titration - - groups of eight mice inoculated

5 0

ip with 10 to 10 P388 leukemia cells. The titration is used to calculate cell killing achieved by treatment with drugs. The animals are checked daily for mortality and the experiments are terminated after 45 days. The end point is mean survival time (MST) and increase in lifetime (ILS) which is the percentage increase in MST compared to untreated controls. Untreated controls inoculated ip with 10 P388 leukemia cells generally survive an average of 9 to 11 days. A medicine is considered active if it gives - 25% ILS.

A summary of the investigation of several compounds of formula (I) in the in vivo ip P388 model is shown in the following Table A.

Based on the data presented in Table A, compounds of formula (I) showed significant anti-tumor activity in the in vivo P388 leukemia tumor assay.

A summary of the results of several compounds of formula (III) in the in vivo ip P388 model is shown in the following table B.

Based on data given in Table B, compounds of formula (III) showed significant anti-tumor activity in the in vivo ip P388 leukemia tumor assay. It should be noted that the 4-pyridylanalog of compound #10 in Table B was also tested twice in the ip P388 leukemia assay, but showed insufficient anti-tumor activity (ie, < 25%) in both trials.

The cytotoxic activity of two compounds of formula (III) was investigated in vivo using B16 melanoma cells.

In this system, groups pp B6D2F1~ mice are inoculated ip with 0.5 ml

of a 10% medium of the B16 melanoma prepared from pooled sc tumors excised at 14-21 days from C57B1/6 donor mice. Daily treatment begins 24 hours after tumor implantation, and continues daily for ten (10) days. The route of administration for the drug is ip. The mice are checked daily for survival for sixty (60) days. Anti-tumour activity is determined by prolongation of mean survival time. An ILS of 25% shows activity in this tumor model.

A summary of the measurements of two compounds of formula (III) in the in vivo ip B 16 melanoma assay is shown in Table C.

The pharmaceutical composition in this invention comprises

an effective tumor cell growth inhibitory amount of a compound of formula (I) or formula (III) and an inert pharmaceutically acceptable carrier or diluent. These mixtures are prepared in unit dosage form suitable for parenteral administration.

Mixtures for parenteral administration contain sterile aqueous or non-aqueous solutions, suspensions or emulsions. The mixture may be in the form of a solution of the active ingredient in a minimum volume of dimethylacetamide or ethanol, e.g. 5 volume percent brought up to volume with peanut oil or normal saline solution. Polyethoxylated castor oil, e.g. 2 to 5 percent by volume can also be used to solubilize the active ingredient. In addition, the mixture can be in the form of a slurry with e.g. hydroxypropyl cellulose or other suitable suspending agent. As an emulsifier, e.g. lecithin is used. The mixture can also be in the form of a sterile solid which can be dissolved in a sterile injectable medium immediately before use.

Freireich et al., Cancer Chemo. Rept., 50, 219-244 (1966) compared the quantitative toxicity of 18 anti-scratch drugs in 6 species after correcting the data to a uniform treatment core for five consecutive days. This analysis showed that mouse, rat, dog, human, monkey had essentially the same maximum tolerated dose (MTD) compared on a mg/m<2>body surface basis. This investigation indicated that phase I clinical trials could safely be initiated at a third-party dose of the animal MTD. The mouse was as applicable as any other species in this respect as a basis for calculation. The correct therapeutically effective dose for a compound produced according to the invention can therefore be easily determined by a person skilled in the art from simple experimentation with laboratory animals, preferably mice.

It will be clear that the actual preferred dosages

of compounds of formula (I) or formula (III) used in the compositions of this invention will vary depending on the particular compound used, the particular formulated composition, the form of administration, and the particular site, host and disease being treated. The internal route of administration should be chosen to ensure that an effective tumor cell growth inhibitory amount of the compound of formula (i) or formula (III) contacts the tumor. Optimum dosages for a given set of conditions can be determined by the person skilled in the art using usual dosage determination experiments based on the above-mentioned experimental data. For parenteral administration of a compound of formula (III) or a gold-containing compound of formula (I), the generally used dose is from approx. 5 to approx. 100 mg/m<2>body surface per day for one to five days, repeated approximately every four weeks for four

ready for treatment. For parenteral administration of a non-gold-containing compound of formula (I), the dose used is preferably from approx. 15 to approx. 600 mg/m<2>body surface per day for 5 days, repeated every four weeks for four courses of treatment.

The method of inhibiting the growth of animal tumor cells which are sensitive to a compound of formula (I) or formula (III) according to this invention consists in giving a host animal affected by the tumor cells an effective tumor cell growth-inhibiting amount of a compound of formula (I) or formula (III).

EXAMPLES

The following examples illustrate the chemical preparation of several compounds of formula (I) and formula (III) which can be used in the mixtures and the method of this invention and as such must not be considered as limiting the scope thereof. All temperatures are in °C.

EXAMPLE 1

1, 2-bis(di-2- pyridylphosphino) ethane

Under an argon atmosphere, 2-bromopyridine (30.9 g, 0.19 mol) in aqueous ethyl ether (50 mL) was added to n-butyllithium (0.19 mol)

in hexane (73 mL) while maintaining the temperature below -50°C. After stirring for 1 hour, a further 7.5 g of 2-bromopyridine was added,

and the mixture was stirred for 30 minutes. An ether solution (100 ml)

of 1,2-bis(dichlorophosphino)ethane (10 g, 43 mmol), from Strem Chemicals, Inc., Newburyport, Mass., was added and the mixture was stirred for 1 hour at -50°C, then allowed to warm to room temperature overnight. Saturated aqueous ammonium chloride was isolated and dissolved in chloroform, dried (Na 2 SO 4 ), filtered and the solvent was removed to give a dark residue. The residue was treated with acetone and then the acetone was cooled to give a light yellow solid (4.5 g). Recrystallization from acetone gave 2.64 g of the title compound, mp 134 - 135°C: EXAMPLE 2

1, 2-bis(di-4-pyridylphosphino)ethane

Under an argon atmosphere, 4-bromopyridine (30.9 g, 0.19 mol) in anhydrous ethyl ether (50 mL) was added to n-butyllithium (0.19 mol) in hexane (73 mL) while maintaining the temperature below -50° C. After stirring for 1 hour, an additional 7.5 g of 4-bromopyridine was added, and the mixture was stirred for 30 minutes. An ethereal solution (100 mL) of 1,2-bis(dichlorophosphino)ethane (10 g, 43 mmol), from Strem Chemicals, Inc., Newburyport, Massachusetts was added

and the mixture was warmed to room temperature overnight. After 18 hours at room temperature, aqueous saturated ammonium chloride was added and the solid was removed. The remaining solid in the flask was collected, dissolved in chloroform, treated with activated carbon, filtered and the solvent removed. Flash chromatography (SiCl 2 , 7% methanol/methylene chloride) of the residue gave a small amount of the desired product, m.p. 183 - 185°C.

EXAMPLE 3

1, 2-bis(di-2-thienylphosphino) ethane

Under argon at room temperature, thiophene (16 g,

0.19 mol) in anhydrous ethyl ether (50 ml) to a hexane (73 ml) solution of n-butyllithium (0.19 mol) which had been diluted with ether (50 ml). After stirring for 1 hour, the mixture was cooled to 0°C. Then 1,2-bis(dichlorophosphino)ethane (10 g, 0.043 mol)

from Strem Chemicals, inc., Newburyport, Mass., in 50 mL of ether added, and the mixture was allowed to warm to room temperature and stirred for 2 hours. Saturated aqueous ammonium chloride solution was added and the solids collected. This was dissolved in chloroform, washed with water, dried (MgSO 4 ), filtered and the solvent concentrated to give a solid which was collected and dried to give 4.2 g, m.p. 108 - 110°C. Chromatography (fSiO2, 2:1 CC14/CH2C12) gave the title product in analytical purity after crystallization from ethanol, m.p. 114 - 115°C.

EXAMPLE 4

1. 2-bis(di-2-furylphosphino)ethane

Furan (12.9 g, 0.19 mol) in anhydrous ethyl ether (50 mL) was added to a hexane (73 mL) solution of n-butyllithium (0.19 mol) diluted with ether (50 mL) and kept at room temperature. The mixture was stirred for 2 hours, cooled to 0°C, and 1,2-bis-dichlorophos-fino)ethane (10 g, 0.043 mol) from Strem Chemicals, Inc., Newburyport, Massachusetts in 50 mL of ether added. The mixture was stirred for 18 hours and warmed to room temperature. Saturated aqueous ammonium chloride was added and the mixture was stirred for 1 hour. The solid was removed. The mixture was extracted with ether,

and then chloroform and the extracts were combined. The solid from the combined organic extracts was removed and the solvent removed in vacuo. The residue was treated with hot hexane, cooled and the solid collected (4.7 g). Recrystallization from ethanol gave 1.5 g of the title product as needles, m.p. 94 - 96°C.

EXAMPLE 5

When using the procedure in example 1 to convert

the corresponding heterocycle with the corresponding formula (A) compound, the following compounds of formula are prepared

(I) :

a. 1,2-bis(di-2-pyridylphosphino)methane

b. 1,2-bis(di-2-pyridylphosphino)propane

c. 1,2-bis(di-2-pyridylphosphino)butane

d. 1,2-bis(di-2-pyridylphosphino)pentane

e. 1,2-bis(di-2-pyridylphosphino)hexane f. 1,2-bis(di-4-pyridylphosphino)methane

g. 1,2-bis8di-4-pyridylphosphino)propane

h. 1,2-bis(di-4-pyridylphosphino)butane

i. 1,2-bis(di-4-pyridylphosphino)pentane

j. 1,2-bis(di-4-pyridylphosphino)hexane

k. 1,2-bis(di-2-thienylphosphino)methane

1. 1,2-bis8di-2-thienylphosphino)propane

m. 1,2-bis(di-2-thienylphosphino)butane

n. 1,2-bis(di-2-thienylphosphino)pentane

o. 1,2-bis(di-2-thienylphosphino)hexane

p. 1,2-bis(di-2-furylphosphino)methane

q. 1,2-bis(di-2-furylphosphino)propane

r. 1,2-bis(di-2-furylphosphino)butane

pp. 1,2-bis(di-2-furylphosphino)pentane

t. 1,2-bis(di-2-furylphosphino)hexane

EXAMPLE 6

A specific embodiment of a mixture prepared according to the invention, an active ingredient, such as one part of the compound from example 1, is dissolved in five parts of dimethylacetamide and five parts of polyethoxylated castor oil, and then normal saline qs and given parenterally at a dose of 30 mg/m <2>to a host animal affected by tumor cells sensitive to this compound.

EXAMPLE 7

DichlorbisCl, 2-bis(diphenylphosphino) ethane digold

a) p - f 1 ,2-bis(diphenylphosphino) ethane] bis [chlor or gold (I )J

Hydrochloric acid hydrate (1.6 g, 3.8 mmol) in ethanol (20 mL)

was added to bis(1,2-diphenylphosphino)ethane (1.83 g, 4.5 mmol)

from Strem Chemicals, Inc., Newburyport, Mass., in 1:1 chloroform/ethanol (40 mL) maintained at room temperature. After one hour the white precipitate was collected, dissolved in methylene chloride, filtered and ethanol added to initiate precipitation. After

standing, the product was collected and dried to give 0.97 g (50%) of the title gold complex which had a melting point of 291 - 293°C.

(b) Dichlorobis[i,2-bis(diphenylphosphino)ethane]digold

A solution of 1,2-bis(diphenylphosphino)ethane (2.31 g, 5.8 mmol) from Strem Chemicals, Inc., Newburyport, Mass., in chloroform (100 mL) was added to a slurry of ,2-bis(diphenylphosphino)ethane]bischlorogold) (5.0 g, 5.8 mmol) prepared as described above in chloroform (500 mL) kept at room temperature. After 45 minutes, the reaction mixture became homogeneous (clear) and the solvent was removed in vacuo. The residue was dissolved in a minimum amount of chloroform and ether was added. After cooling, the precipitate was collected and dried to give 3.0 g (41%) of the title product, m.p. 298 - 302°C.

EXAMPLE 8

Dichlorbis 1, 2-bis(diethylphosphino) ethane digold

a) y~[l,2-bis(diethylphosphino)ethane] bis[chlorosulfur (I )]]

Chlorosulfuric acid tetrahydrate (7.88 g) in water (35 ml) was reduced with thiodiglycol (5.5 g) in ethanol (12 ml) at 0°C in the usual manner. A solution of 1,2-bis(diethylphosphino)ethane (2.06 g) from Strem Chemicals, Inc., Newburyport, Mass., in ethanol

(15 ml) was added. After stirring for 1 hour, the reaction mixture was poured into 400 ml of ice water and extracted with methylene chloride.

The combined extracts were dried (MgSO 4 ), filtered and cooled overnight. The resulting solid was collected and air-dried to give 3.0 g of the title product, m.p. 168 - 170°C.

b) Dichlorobis 1,2-bis(diethylphosphino)ethane digold

Addition of 1,2-bis(diethylphosphino)ethane (0.31 g, 1.49

mmol) from Strem Chemicals, Inc., Newburyport, Massachusetts,

in a single portion to a solution of yl-£1,2-bis(diethylphosphino)-ethane]bischlorogold) (1.0 g, 1.49 mmol) as described above in chloroform (200 mL) was carried out, and the resulting clear solution for 30 minutes. The solvent was removed in vacuo, the residue crystallized from chloroform/ether to give 1.0 g (77%) of the title product, m.p. 211 - 214°C.

EXAMPLE 9

Using the procedure of Example 7 (b) or Example 8 (b) to react the corresponding gold complex of formula

(C) (prepared according to the method of example 7 (a) or 7 (a) by using the corresponding haloauric acid hydrate) with the

corresponding ligands of formula (B), the following compounds of formula (III) are prepared, wherein is chlorine or bromine; and/or by reacting the corresponding compound of formula (III), wherein X is chlorine, with sodium bromide in a corresponding organic solvent such as aqueous ethanol or DMF, the following compounds of formula (III) wherein X is bromine are prepared; and by reacting the corresponding compound of formula (III) in which X^ is chlorine or bromine with sodium iodide in a corresponding organic solvent, such as acetone, the following compounds of formula (III) in which X 1 is iodine are prepared: a) dichlorobisfl, 2-bis(diphenylphosphino)methanej digold b ) dichlorobis[ 1,2-bis(diphenylphosphino)propane] digold

c) dichlorobis Tl,2-bis(diphenylphosphino)butane]digold

d) dichlorobis^1,2-bis(diphenylphosphino)pentane]digold

e) dichlorobisL"! , 2-bis (dif enyl phosphino ) hexane] digold

f) dichlorobis[1,2-bis(diethylphosphino)methane]digold

g) dichlorobis[1,2-bis(diethylphosphino)propane]digold

h) dichlorobis[1,2-bis(diethylphosphino)butane]digold

i) dichlorobis[i,2-bis(diethylphosphino)pentane]digold

j) dichlorobis £1 ,2-bis(diethylphosphino)hexane]digold k ) diiodobis jj , 2-bis ( diphenylphosphino ) ethane] digold 1) dibrombis £1 , 2-bis (diphenylphosphino ) ethanej digold

EXAMPLE 10

As a specific embodiment of a mixture prepared

in this invention, an active ingredient such as one part of the compound from example 7 is dissolved in 5 parts dimethylacetamide and 5 parts polyethoxylated castor oil and then normal saline solution qs, and given parenterally in a dose of 5 mg/m<2> to an affected host animal of tumor cells that are sensitive to this compound.

EXAMPLE 11

y- [ i , 2- bis( di- 2- pyridylphosphino) ethane! bis (chlorine gold)

Under an argon atmosphere, 2-bromopyridine (30.95 g, 0.19 mol) in anhydrous ethyl ether (50 mL) was added to n-butyllithium (0.19 mol) in hexane (73 mL) while maintaining the temperature below -50° C. After stirring for 1 hour, an additional 7.5 g of 2-bromopyridine was added and the mixture was stirred for 30 minutes. An ethereal solution (100 mL) of 1,2-bis(dichlorophosphino)ethane (10 g, 43 mmol) from Strem Chemicals, Inc., Newburyport, Mass., was added and the mixture was stirred for 1 hour at -50°C, and then allowed to warm to room temperature overnight. Saturated aqueous ammonium chloride was added and the mixture was stirred for 1 hour. The solid was collected and dissolved in chloroform, dried (Na 2 SO 4 ), filtered and the solvent was removed to give a dark residue. The residue was treated with acetone and the acetone was cooled to give a pale yellow solid (4.5 g). Recrystallization from acetone gave 2.64 g of 1,2-bis(di-2-pyridylphosphino)ethane, m.p. 134 - 135°C.

Thiodiglycol (1 g, 8.18 mmol) in water (10 mL)/methanol (30 mL) was added to chlorosulfuric acid tetrahydrate (0.88 g, 2.14 mmol) in water (10 mL) kept at 0 °C. After stirring for 15 minutes, 1,2-bis(di-2-pyridylphosphino)ethane, (0.43 g, 1.07 mmol) prepared as described above in acetone (50 mL)/chloroform (10 mL) was added, and the mixture was stirred for 2 hours. Methanol was added and the product was collected and slurried with Cf 2 C 2 /CHCl 2 , diluted with methanol and cooled. The resulting solid was collected and dried to give 0.38 g (41%) of the title product, m.p. 292 - 293°C.

EXAMPLE 12

y- Li , 2- bis ( di- 2- pyridyl f osphino ) ethane"] bis l( 1 - thio( l- D- glucopyrano-sato- S) gold

A mixture of sodium thioglucose (0.33 g, 1.5 mmol) from Sigma Chemical Company, St. Louis, Missouri, and ji-[i , 2-bis(di-2-pyridylphosphino)ethane]bis(chlorosulfur) (0 .6 g, 0.69 mol), prepared as described in Example 1, in chloroform (75 ml)/methanol (75 ml)/water (10 ml) was stirred at room temperature for 2 hours and the solvent evaporated. The residue was dissolved in chloroform and the precipitate was collected. The solid was dissolved in methanol, filtered and the solvent evaporated. The residue was dissolved in acetone, cooled and the precipitate was collected and dried to give 0.49 g (60%)

of the title compound as a white, amorphous solid.

EXAMPLE 13

U- D, 2- bis( di- 4- pyridylphosphino) ethane] bis( chlorogold)

Under an argon atmosphere, 4-bromopyridine (30.95 g, 0.19 mol) in anhydrous ethyl ether (50 mL) was added to n-butyllithium (0.19 mol) in hexane (73 mL) while maintaining the temperature below -50° C. After stirring for 1 hour, an additional 7.5 g of 4-bromopyridine was added and the mixture was stirred for 30 minutes. An ether solution (100 ml)

of 1,2-bis(dichlorophosphino)ethane (10 g, 43 mmol) from Strem Chemicals, Inc., Newburyport, Massachusetts was added and the mixture was stirred for 1 hour at -50°C, then allowed to warm to room temperature overnight. After 18 hours at room temperature, aqueous saturated ammonium chloride was added and the solid was removed. The remaining solid in the flask was collected, dissolved in chloroform, treated with activated carbon, filtered and then the solvent was removed. Flash chromatography (SiG^, 7% methanol/methylene chloride) of the residue gave a small amount of 1-2-bis(di-4-pyridylphosphino)ethane, m.p. 183 - 185°C.

Thiodiglycol (2 g, 16.4 mmol) in water (10 mL)/methanol (30 mL) was added to chlorosulfuric acid tetrahydrate (1.58 g, 3.83 mmol)

in water (10 ml) kept at 0°C. After stirring for 15 min, 1-2-bis(di-4-pyridylphosphino)ethane (0.77 g, 1.9 mmol) prepared as described above in CH 2 Cl 2 (10 mL)/methanol (30 mL) was added and the mixture was stirred for 1 hour. Methanol was added and the precipitate collected and stirred in acetonitrile, filtered and dried to give 0.75 g (45%) of the title product, m.p. 241 - 242°C.

EXAMPLE 14

Chlorbis[1,2-bis(di-2-pyridylphosphino)ethane] gold

To a suspension of |-t- [i , 2-bis ( di-2-pyridyl phosphino )-ethane]bis-(chlorosulfur) (0.12 g, 0.14 mmol) in CH 2 Cl 2 (25 mL) and the mixture was stirred at room temperature for 18 h and gave a clear solution. The solvent was evaporated and the residue was dissolved in methanol and diluted with ethyl ether. After cooling, the precipitate was collected and dried to give 0.28 g (98%) of the title product, m.p. 257 - 258°C.

EXAMPLE 15

a) By using the method described in example 11 or 13 by directly heating the corresponding halogold acid hydrate with the corresponding diphosphinohydrocarbon compound of formula (I) in which M is 0 in a corresponding non-reactive organic solvent or by reacting the corresponding halogold acid hydrate which has been reduced by treatment with tidiglycol with the corresponding compound of formula (I) in which M is 0, the following compounds of formula (I) are prepared in which

M is 1 and X is chlorine or bromine; or by reacting the corresponding compound of formula (I) in which M is 1 and X is chlorine with sodium bromide in a suitable organic solvent, such as aqueous ethanol or DMF, the following compounds of formula (I) are prepared in which M is 1 and X is bromine; or by reacting the corresponding compound of formula (I) in which M is 1 and X is chlorine or bromine with sodium iodide in a suitable organic solvent such as acetone, the following compounds of formula (I) are prepared in which M is 1 and X is iodine:

i) y - [i , 1 - bis ( di-2-pyridyl f osphino ) me tan] bis - ( chloro gold)

ii) U-["1,3-bis(di-2-pyridyl phosphino) propane] bis - (chlorine gold)

iii) ^-[1,4-bis(di-2-pyridyl phosphino)butane]bis(chlorosulfur)

iv) p- [i , 5-bis ( di-2-pyridyl phosphino ) pentanj bis ( kl or gold)

v) }J-[1,6-bis( di-2-pyridyl phosphino ) hexane] bis ( chlorine or gold)

vi) |4-[1,2-bis( di-2-pyridyl phosphino ) ethane bis (bromogold)

vii) |4-(j,2-bis(di-2-pyridyl phosphino)ethane]bis (iodogold)

viii) \i- f_ 1 , 2-bis (di-4-pyridyl osphino )methane] bis (chlorosulphur)

ix) ^-[1,2-bis(di-4-pyridylphosphino)propane]bis(chlorogold)

x ) \ i- [i , 2-bis (di-4-pyridyl f osphino ) butane] bis (chlorosulfur)

xi) £l , 2-bis ( di-4-pyridyl f osphino ) pentanj bis (chlorosulfur)

xii ) |4- [_1 , 2-bis (di-4-pyridyl phosphino ) hexane] bis (chlorogold)

xiii ) |J-(j , 2-bis (di-4-pyridyl f osphino ) ethane] bis (bromo gold)

xiv) |J-(j , 2-bis (di-4-pyridyl f osphino ) ethanej bis ( iodide gold)

b) Using the method described in example 14 by reacting the corresponding compound of formula (I) in which R is 2-pyridyl, prepared as described above with the corresponding compound of formula (I) in which M is 0 prepared as described above, the following compounds of formula (I) are prepared, in which M is 1: i) chlorobis[i,1-bis(di-2-pyridylphosphino)methane] gold ii) chlorobisf_1,3-bis(di-2-pyridyl f osf ino ) propane] gold iii) chlorobis jj ,4-bis(di-2-pyridylphosphino)butane]gu11

iv) chlorobis[J ,5-bis(di-2-pyridylphosphino)pentane]gold v) chlorobis[j ,6-bis(di-2-pyridylphosphino)hexane]gold vi) iodobis[i , 2-bis (di- 2-pyridylphosphino)ethane]gold vii)bromobis[i,2-bis(di-2-pyridylphosphino)ethane]gold

EXAMPLE 16

By using the procedure from example 12 and converting

the corresponding formula (I) compound in which X is chlorine, prepared according to the method in example 11, 13 or 15, with the corresponding thiosugar, the following formula (I) compounds are prepared, in which X is thiosugar:

a) yl - [i , 1 - bis (di-2-pyridyl f osphino ) methane] bis ( 1 -thio-(i-D-gluco-pyranosato-S) gold b) ja - [i , 3-bis (di-2-pyridyl phosphino ) propaneJbis ( 1 -thio-(i-D-gluco-pyranosato-S)gold c) yJ-jj , 4-bis (di-2-pyridyl phosphino ) butanjbis ( 1-thio- fi>-D-gluco- pyranosato-S)gold d ) }-!- (j , 5-bis (di-2-pyridyl f osphino ) petnanjbis ( 1 -thio-fS-D-gluco- pyranosator-S)gold e ) fi- [i , 6-bis (di-2-pyridyl phosphino ) hexane"] bis ( 1 -thio-(?-D-gluco- pyranosato-S)gold f) |i-[j,2-bis( di-2-pyridyl f osphino ) et an"] bis ( 1 -thio- P-D-galacto-pyranosator-S)gold g) H-^ 1 ' 2-bis(di-2-pyridylphosphino)ethane]bis(1-thio-Ø-D-mannopy-ranosato-S)gold h) /2-bis(di-2-pyridylphosphino)ethanej bis(1 -tio-ft-D-ribofu-ranosato-S)gold

i ) H ~ 0 ' 1 ~ki-s (di-4-pyridyl f osf ino ) me tan"] bis ( 1 -thio-$-D-gluco-pyranosato-S)gold

j ) |4- [i , 2-bis (di-4-pyridyl phosphino ) ethane bis ( 1 -thio-(i-D-gluco-pyranosato-S)gold

k ) u - {j , 3-bis (di-4-pyridyl f osphino ) propane] bis ( 1 -thio-(J-D-gluco-pyranosato-S)gold

1) j-l- [i , 4-bis (di-4-pyridyl f osphino ) butane^bis ( 1 -thio-fr-D-gluco-pyranosato-S)gold

m) [4-[1,5-bis( di-4-pyridyl phosphino ) pentane] bis ( 1 -thio-S-D-gluco-pyranosato-S) gold

n) - Ij i 6-bis (di-4-pyridyl phosphino ) hexane] bis ( 1-thio-(1-D-gluco-pyranosato-S) gold

o) Ji-[1,2-bis( di-4-pyridyl phosphino ) ethane] bis ( 1-thio-(5-D-galacto-pyranosato-S) gold

p) p-[1,2-bis(di-4-pyridyl phosphino)ethane bis(1-thio-fj-D-manno-pyranosato-S)gold

q ) JlU 0 , 2-bis ( di-4-pyridyl f osphino ) ethane] bis ( 1 -thio-D-ribof urano-sato-S) gold

EXAMPLE 17

A specific embodiment of a mixture containing

an active ingredient such as a portion of the compound from Example 11, is dissolved in 5 parts dimethylacetamide and 5 parts polyethoxylated castor oil and then normal saline qs, and given parenterally in a single dose of 5 mg/m<2> to a host animal affected by tumor cells that are sensitive to this connection.

Claims (4)

1. Analogy method for the preparation of a therapeutically active compound of formula in which all R are the same and are 2-pyridyli_ 4-pyj[idyJLJ_2^^ 2-furyl; and A is a straight or branched alkylene residue having from one to six carbon atoms; characterized by reacting the corresponding heterocycle in an anhydrous ethyl ether with an organolithium reagent such as n-butyllithium in a non-reactive, organic solvent with the corresponding compound of the formula where A is defined as above. 2. Method according to claim 1, in which the preparation of compounds of formula (I) in which A is ethylene, characterized in that correspondingly substituted starting materials are used. 3. Process according to claim 2 for the preparation of compounds in which R is 2-thienyl, characterized by using correspondingly substituted starting materials. 4. Method according to claim 2 for the preparation of compounds in which R is 2-furyl, characterized by using correspondingly substituted starting materials.