AU6711690A - 1,4,10,13-tetraoxa-7,16-diazacyclooctadecane derivatives, pharmaceutical compositions containing them and their use for the removal of toxic metal ions and radioactive isotopes from the living organism - Google Patents

1,4,10,13-tetraoxa-7,16-diazacyclooctadecane derivatives, pharmaceutical compositions containing them and their use for the removal of toxic metal ions and radioactive isotopes from the living organism

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AU6711690A
AU6711690A AU67116/90A AU6711690A AU6711690A AU 6711690 A AU6711690 A AU 6711690A AU 67116/90 A AU67116/90 A AU 67116/90A AU 6711690 A AU6711690 A AU 6711690A AU 6711690 A AU6711690 A AU 6711690A
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hydrogen
formula
metal
tetraoxa
group
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AU645507B2 (en
Inventor
Erno Brucher
Jozsef Emri
Bela Gyori
Bela Kanyar
Odon Kiraly
Zoltan Kovacs
Laszlo B Sztanyik
Laszlo Varga
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ORSZAGOS "FREDERIC JOLIOT-CURIE" SUGARBIOLOGIA ES SUGAREGESZSEGUGYI KUTATO INTEZET
Kossuth Lajos Tudomanyegyetem
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Orszagos Frederic Joliot Curie Sugarbiologia Es Sugaregeszsegugyi Ki
Kossuth Lajos Tudomanyegyetem
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    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D273/00Heterocyclic compounds containing rings having nitrogen and oxygen atoms as the only ring hetero atoms, not provided for by groups C07D261/00 - C07D271/00
    • C07D273/08Heterocyclic compounds containing rings having nitrogen and oxygen atoms as the only ring hetero atoms, not provided for by groups C07D261/00 - C07D271/00 having two nitrogen atoms and more than one oxygen atom
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D273/00Heterocyclic compounds containing rings having nitrogen and oxygen atoms as the only ring hetero atoms, not provided for by groups C07D261/00 - C07D271/00
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/33Heterocyclic compounds
    • A61K31/395Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P39/00General protective or antinoxious agents
    • A61P39/02Antidotes
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P43/00Drugs for specific purposes, not provided for in groups A61P1/00-A61P41/00

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  • Chemical & Material Sciences (AREA)
  • Organic Chemistry (AREA)
  • Health & Medical Sciences (AREA)
  • Animal Behavior & Ethology (AREA)
  • Veterinary Medicine (AREA)
  • Public Health (AREA)
  • Medicinal Chemistry (AREA)
  • General Health & Medical Sciences (AREA)
  • Pharmacology & Pharmacy (AREA)
  • Life Sciences & Earth Sciences (AREA)
  • General Chemical & Material Sciences (AREA)
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  • Chemical Kinetics & Catalysis (AREA)
  • Toxicology (AREA)
  • Engineering & Computer Science (AREA)
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  • Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
  • Medicines Containing Antibodies Or Antigens For Use As Internal Diagnostic Agents (AREA)
  • Medicinal Preparation (AREA)
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Description

1 , 4 , 10 , 13-TETRA0XA-7 , 16-DIAZACYCL00CTADECANE DERIVATIVES , PHARMA- CEUTICAL COMPOSITIONS CONTAINING THEM AND THE IR USE FOR THE REMOVAL OF TOXIC METAL IONS AND RADIOACTIVE ISOTOPES FROM THE LIVING ORGANISM
The invention relates to partially novel 1,4,10,13-tetraoxa- -7,16-diazacyclooctadecane derivatives and the use of such com¬ pounds for the decorporation of metal ions, mainly radioactive isotopes damaging the living organism. More particularly, the invention relates to metal complexes, salts and double salts of l,4,10,13-tetraoxa-7,16-diazacyclooctadecaπe derivatives of the formula (I)
(I) wherein
Q1 and Q2 mean hydrogen or a group of the formula (III).
COO"
-C—R
I
COO" in the groups of the formula (III)
R substituents independently represent hydrogen, a C^_5 straight or branched chain alkyl group, a C2_5 straight or branched chain alkenyl group, phenyl or phenyl-C-^alkyl group, the two latter ones optionally being substituted on their aro¬ matic part by one or more halogen(s), C-^alkyl, C-^alk- oxy, cyano or πitro group(s), with the proviso that at least one of Q-'- and Q2 is other than hydrogen;
Me stands for an alkaline metal or alkaline earth metal or transition metal ion; q is 0 or 1;
M and N, independently from each other, stand for hydrogen or an alkaline metal, alkaline earth metal or optionally substi¬ tuted ammonium ion; m, π and p are integers each being equal to the charge of N, M or
Me, respectively; s and r are, independently from each other, 0, 1, 2, 3 or 4, with the proviso that
(i) r, s and q cannot simultaneously be 0; and (ii) the number of hydrogens in the meaning of M or N may be 0, 1 or 2, as well as pharmaceutical compositions containing these co - pounds.
From the compounds of the formula (I), those containing hydrogen as Q^ and Cr are used mainly as intermediates. When administered into the organism, the compounds of the formula (I), independently whether they are new or not, are capable to form a stable complex with radioactive metal ions, above all with radio¬ active strontium and cerium being present in the blood circula¬ tion and extracellular space, and then to be eliminated.
From the compounds of the formula (I), the novel ones con¬ tain a group of the formula (III), wherein either R is other than hydrogen; or, q is 1 when R is hydrogen, i.e. the complexes; further, wherein M and N are other than sodium or lithium ion when q is 0.
Thus, on the one hand, the present invention relates to com¬ pounds of the formula (I), wherein 0- and Q2 mean hydrogen or a group of the formula (III), with the proviso that at least one of them is other than hydrogen; and in the groups of the formula (III) the R substituents independently mean hydrogen, a C]__5 straight or branched chain alkyl group, a C2_5 straight or branched chain alkenyl group, phenyl or phenyl-C^.^alkyl group, the two latter ones optionally being substituted on their aro¬ matic part by one or more halogεn(s), C^alkyl, ι_5al - oxy, cyano or nitro group(s);
Me stands for an alkaline metal or alkaline earth metal or transition metal ion; o is 0 or 1;
M and N, independently from each other, stand for hydrogen or an alkaline metal, alkaline earth metal or optionally substi¬ tuted ammonium ion; m, π and p are integers each being equal to the charge of N, M or
Me, respectively; s and r are, independently from each other, 0, 1, 2, 3 or 4, with the proviso that
(i) r, s and q cannot simultaneously be 0;
(ii) the number of hydrogens in the meaning of M or N may be
0, 1 or 2; (iii) q is 1 when R means hydrogen; and (iv) M and N are other than sodium or lithium ions when q is
0. Returning to the substituents of the formula (I), R as a Cj^alkyl group may be of straight or branched chain such as a methyl, ethyl, n-propyl, isopropyl, π-butyl, sec-butyl, tert-bu- tyl, π-pentyl or isopentyl group, preferably a methyl or ethyl group; R as a C2_5alkenyl group may be e.g. a vinyl or propenyl group; R as group may contain one of the alkyl moieties defined above, preferably a methyl group.
Me as an alkaline metal ion means preferably sodium or potassium ion; Me as an alkaline earth metal ion preferably stands for calcium or magnesium ion; and Me as a transition metal ion may be e.g. the ion of a metal belonging to the 3d, 4d or 5d group, preferably iroπ(II) (ferrous) or zinc ions. M and N as al- kaline metal or alkaline earth metal ions are preferably the above ions; whereas the optionally substituted ammonium ion con¬ tains 1,2,3 or 4 above-identified alkyl, phenyl or pheπylalkyl group(s) (supposed that no steric hindrance occurs). Due to their toxicity, the compounds containing a tetramethylammonium ion, cannot be used for administering into a living organism.
It is known that, on nuclear explosions or nuclear reactor disasters, very dangerous radioactive isotopes such as iodiπe-131 (131I), stroπtium-89 and -90 (89Sr and 90Sr) as well as cesiu - 134 and -137 (1 4Cs and 137Cs) and cerium-141 and -144 (141Ce and l44Ce) may get into the atmosphere /see e.g. in: Nuclear and Radiochemistry", John Wiley and Sons, pages 158 to 166 (1981/.
When these isotopes get to the lungs by inhalation or to the digesting tract by intake of contaminated food or fluid or tϋ the blood circulation or lymphatic system after resorption through the skin, they are deposited and accumulated in the tissues and finally, they lead to severe health injuries /"Summary Report on the Post Accident Review Meeting on the Chernobyl Accident" Safety Series No. 75, IAEA, Vienna (1986)/.
After the radioactive contamination, strontium begins to be built in to the bones in several hours, and there is no more pos¬ sibility to elinimate (decorporate) the strontium deposited from the organism. Thus, the protection against radioactive strontium is particularly problematic.
The only possible way of protection is to inhibit the fixation of strontium to the tissues, above all to bone tissues by introducing a suitable strontium-specific complexing agent to the organism, thus binding in a stable form the isotope occuring in the blood circulation or extracellular space and decorporating it from the organism. The solving of this problem is made more difficult thereby that the calcium complexes of complexing agents known from the literature, e.g. ethylenediaminetetraacetic acid or diethylene- triaminepeπtaacetic acid, are substantially more stable than
5 their strontium complexes /A. Catsch: "Radioactive Metal Mobiliz¬ ation in Medicine", Ed. Charles C. Thomas, Springfield, Illinois (1964); A. Catsch: "Dekorporierung radioaktiver und stabiler Me- tallionen", Therapeutische Grundlageπ, Ed. Thiemig, Munich (1968); A. Catsch: "Removal of Transuranium Element by Chelatiπg
10 Agents", in: Diagnosis and Treatment of Incorporated Radio- nuclides, IAEA Publication No. STI/PUB/411, IAEA, Vienna, page 295 (1976)/.
A new possibility for the research has been recognized by the synthesis of the crown ether and cryptand type molecules.
1.5 Namely, the mechanism of complex formation is in this case dif¬ ferent from that of the earlier known complexing agents as due to the structure of the new complex forming molecule, the metal ions get to holes with well-defined sizes and therefore, the stability of the complex formed essentially depends on the size of the
20 metal ion.
The first promising results were obtained during the inves¬ tigations on 4,7,13,16,21,24-hexaoxa-l,10-diazabicyclo 8,8,j3/- hexacosane forming a strontium complex with a stability constant of several orders of magnitude higher than that of its calcium 5 complex /"Coordination Chemistry of Macrocyclic Compounds", Ed. G.A. Melson, Plenum Press (1979)/. However, by using this com¬ pound in animal experiments it could only be proven that the complex formed with the ligand outside the organism was not dissociated in the organism after administration, but no evidence 0 was obtained that radioactive strontium could be removed from the organism as a stable complex formed with the ligand. In addition, the ligand proved to be highly toxic /W.H. Mϋller: Naturwiss. 31_, 248 (1970); W.H. Mϋller and W.A. Mϋller: Naturwiss. ^, 455 (1974); W.H. Mϋller et al.: Naturwiss. 6£, 96 (1977); J. Kπajfl et al.: 12th Ann. Meeting of ESRB, Budapest (1976); 3. Batsch et al.: Nukleonika 23_, 305 (1978)/.
The compounds of the formula (I), being salts when q is 0 and complexes when q is 1, possess specific complexing properties enabling them to bind and decorporate metal ions being harmful to the organism, mainly the radioactive strontium and cerium getting to the living organism and being present in the blood circulation as well as in the extracellular space of the organism. By admin¬ istering the pharmaceutical compositions containing the compounds of the formula (I) as active ingredients to humans or animals, the depositions of the radioactive strontium into tissue parts can be prevented and thereby severe health injuries induced by the radiation load of the organism can be avoided or diminished.
F. de Jong et al. published a method for the preparation of N,N'-bis(dicarboxymethyl)-l,4,10,13-tetraoxa-7,16-diazacycloocta- decaπe tetralithium salt /Rec. Trav. Chim. Pays-Bas 102, 164 (1983)/. According to this method, the corresponding cryptand was reacted with methyl 2-bromomalonate and the ester derivative obtained was hydrolyzed to give the lithium salt in a yield of not more than 15%. According to the British patent specification No. 2,024,822 the lithium salt thus prepared can be used in the form of a composition being useful for enhancing the solubility of barium sulfate in the petroleum industry. The corresponding tetrasodium salt is also mentioned in the same specification although it is not described in a specific example. The double salt of the tetrasodium salt with sodium bromide as well as the therapeutic utility of this double salt have been published in the Hungarian patent application No. 2614/89.
The water-soluble salts and complexes of formula (I) accord- ing to the invention, wherein Q1, Q2, R, Me, M, N, , n, p, r, s and q are as defined above, can be prepared on the analogy of the reaction mentioned above by reacting the corresponding halogen- ated dicarboxylic acid of the formula (II),
COOH I X-C- I COOH wherein R is as defined above and X stands for halogen, prefer¬ ably bromine, or a reactive derivative, suitably an ester, there¬ of with l,4,10,13-tetraoxa-7,16-diazacyclooctadecane in an organic solvent medium and then hydrolyziπg the thus-obtained product by a strong base, e.g. sodium hydroxide or by a mixture of suitable molar ratio of a strong base and a hydroxide or salt, preferably a halide, of a complex-forming metal.
Alternatively, the water-soluble salts and complexes of the compounds of the formula (I), wherein M and N stand for hydrogen or an alkaline metal or alkaline earth metal ion and Me means an alkaline earth metal ion, can be synthetized also by reacting l,4,10,13-tetraoxa-7,16-diazacycloαctadecaπe with a 2-halodicarb- oxylic acid of formula (II) preferably with 2-bromomaloπic acid in an aqueous medium at a pH of 6 to 13 in the presence of the alkaline metal or alkaline earth metal hydroxide corresponding to the salt to be prepared.
The complexes of formula (I), wherein q is 1, can be obtain¬ ed by reacting an alkaline metal salt of the formula (I), wherein q is 0 and M as well as N stand for alkaline metal ions, prefer- ably the tetrasodium salt, with an equivalent amount of a complex-forming metal halide, suitably metal chloride.
The action of the compounds of formula (I) according to the invention, which manifests itself as an increase in the elimina¬ tion of metal ions damaging the living organism, was investigated y using radioactive strontium or cerium ions on Swiss mice and Wistar rats of both sexes.
The elimination was studied on radioactive isotopes intro¬ duced in various rooutes to various sites, e.g. to the blood cir¬ culation, abdominal cavity, lungs, muscles or subcutaneous con- nective tissue of the experimental animals. The compound increas¬ ing the elimination of the isotopes was administered daily once or two times in the form of an injection, powder or liquid aerosol or plaster to the organism of the experimental animals. Thereafter, whole body activity measurements were performed and - Q -
retention curves were taken up which then were compared to the results obtained in the control group.
The retention curves obtained were analysed on a computer. "Nonlinear Regression by the Code of BMDP-3R" (BMDP Statistical Software Manual, UCLA, Los Angeles, 1990, Chief Ed. ... 3. Dixon) computer software was used for this purpose. It could be stated from the results obtained that the curves could be described by a two-component descending exponential function. Two data were cal¬ culated for characterizing the effectivity. One of these was the so-called F factor indicating the increase in the elimination in relation to the control and meaning the multiplication of the isotope elimination under effect of the test compound in relation to the untreated animals /see column (C) in Table 1/.
For the illustrative comparison of the compounds according to the invention additional characteristic data, the so-called El values are given which were obtained by multiplying the extent of isotope elimination as percentage related to the control group (effectivity, E) with the acute toxicity value (LD5 /3Q, inno¬ cuous, I) /see column (D) in Table 1/. Although the El value is numerically not identical to the therapeutic ratio (safety index) , it indicates in all cases to a weak or excellent activity of a product.
It is considered to be an important experimental observation that no radioactive strontium if any could be detected in the bones of the animals treated with an active compound of the invention; a residual activity of 5 to 10% measured as whole-body retention was found in the soft parts and liver of the animals whereas a major part (65 to 70%) of the retention measured in the organism of the control animals was built in to the bones. Similar results were obtained by administering the test com¬ pounds in various routes to the organism.
It has been proven that an excellent effectivity was shown by compounds of the formula (I), wherein O-'- and Q2 are the same and R stands for hydrogen. From these compounds N,N'-bis(dicarb- oxymethyl)-l,4,10,13-tetraoxa-7,16-diazacyclooctadecane calcium complex disodium salt showed a particularly outstanding effect. The importance of the effective compounds of formula (I) is further pronounced by their very advantageous therapeutic ratio. Due to its low toxicity and high decorporating effectivity, the calcium complex disodium salt mentioned above is particularly preferred.
The compounds of formula (I) can be converted to pharmaceu¬ tical compositions by using the common carriers and other auxili- ary materials in a known manner. The useful carriers, excipients, disintegrating, binding and other additive materials are de¬ scribed in detail in a number of relating handbooks.
The investigations on the effectivity of the compounds of Examples 1 to 16 showed that, after administration, the active ingredient was absorbed and exerted a decorporating effect either in the form of an iπjectable solution or in the form of a sub- lingual tablet, dragde, capsule, eπtero-solvent tablet, powder or liquid aerosol or transdermal plaster. The effective dose was found to be 1.0 to 200 /umol/kg of body-weight, preferably 10 to 100 /umol/kg of body-weight, which was administered in one or more portions, preferably in two subdoses.
The pharmaceutical compositions containing the compounds of formula (I) as active ingredient are useful also for the preven¬ tion of building-in to the organism of metal ions being harmful to the living organism.
The invention is illustrated in detail by the aid of the following non-limiting Examples.
Example 1 Preparation of N,N'-bis(dicarboxymethyl)-l,4,10,13-tetraoxa-7,16- -diazacyclooctadecane tetrasodium salt a) 2.74 g (14.98 mmol) of 2-bromomalonic acid are neutral¬ ized in 1.0 ml of water by adding sodium hydroxide solution of 7.410 mole/litre concentration in the presence of phenolphthalein indicator. Then 1.75 g (3.69 mmol) of N-dicarboxymethyl- -l,4,10,13-tetraoxa-7,16-diazacyclooctadecane disodium salt con¬ taining 14.10% by weight of sodium bromide (intermediate) obtained in a preceding reaction, then 1.95 g (7.43 mmol) of l,4,10,13-tetraoxa-7,16-diazacyclooctadecaπe are added to the above solution. The reaction mixture is maintained at 60°C for 10 to 11 hours while adding 2,02 ml of sodium hydroxide solution of 7.410 mole/litre concentration (14.98 mmol) in 0.1 ml portions. After termination of the reaction the solution is filtered off when necessary, sodium bromide is added, then it is evaporated, dried under reduced pressure and extracted in several portions with a total of 20 to 25 ml of methyleπe chloride.
The extract is evaporated to dryπess, 10 to 15 ml of petro¬ leum ether are added and after filtration the precipitate is dried in a stream of nitrogen. 2.27 g (4.82 mmol) of the product obtained containing 13.3% by weight of sodium bromide (inter¬ mediate) are used in the next manufacturing production batch. The identifying data of the intermediate are as follows: 1H-NMR spectrum (200 MHz, D20, <Tppm): 3.87 (IH, s); 3.67 (18H, m); 2.78-2.92 (8H, m). The residue of the methylene chloride extract is extracted with 60 ml of anhydrous ethanol until the extract is practically free from solid material. The residue of the extraction is dissolved in 6 to 7 ml of water and after adding sodium bromide it is evaporated to dryπess and dried. Thereafter, it is extracted by using 30 ml of anhydrous ethanol as described above. The two ethanolic extracts are combined and evaporated to dryπess to give 4.89 g of double salt containing 2.71 moles of sodium bromide. The yield is 94.1% calculated for the macrocycle used. The identifying data for the double salt are as follows: IR spectrum (KBr, cm-1): 2950, 2868 (m,Υ c_H); 1605 (vs,
Tcoo/as>; 1430 <m» Tcoo/s)-
Other characteristic but unidentified frequencies: 1350 (s), 1320
(s), 1095 (s), 928 (w).
1H-NMR spectrum (200 MHz, D20, <Tppm): 4.00 (2H, s); 3.70 (8H, s) ; 3.63 (8H, t) ; 2.92 (8H) , t) . b) Sodium bromide is removed from the double salt by extrac¬ tion with 50 ml of 95% by weight ethanol. The extraction residue is dried and made free from ethanol under reduced pressure to give 3.22 g of product. The yield is 93.2% calculated for the macrocycle used.
The identifying data of the product are as follows: 1H-NMR spectrum (200 MHz, D20, <Tppm): 3.95 (2H, s); 3.64 (8H, s); 3.60 (8H, t); 2.85 (8H, t) .
13C-NMR spectrum (50 MHz, D20, <Tppm): 179.95 (£=0); 76.45 (N-CH- (C00)2); 71.66 and 70.84 (0-CH2); 54.06 (N-rJH2).
Example 2 Preparation of N,N'-bis(dicarboxymethyl)-l,4,10,13-tetraoxa- -7,16-diazacyclooctadecaπe tetrasodium salt containing disodium hydroxy maloπate
The process described in Example 1 is followed by using 2.84 g (15.54 mmol) of 2-bromomaloπic acid, 2,02 g (4.11 mmol) of N- dicarboxymethyl-l,4,10,13-tetraoxa-7,16-diazacyclooctadecane di¬ sodium salt containing 16.87% by weight of sodium bromide and 2.01 g (7.66 mmol) of l,4,10,13-tetraoxa-7,16-diazacycloocta- decaπe, except that the reaction mixture is maintained at 50°C and the sodium hydroxide is portionwise added during 10 hours. The amount of monosubstituted intermediate obtained by extraction with methylene chloride is 2.17 g (4.41 mmol) and contains sodium bromide in an amount of 16.93% by weight. The product weighes 3.92 g, the yield is 96.5% calculated for the macrocycle used. The product contains 1.6% by weight of disodium hydroxymalonate.
The ^-H-NMR spectrum of the product (200 MHz, D20, cTppm) agrees with that of the product of Example 1, except that a resonance signal also appears at 4.31 (s) which is characteristic of hydroxymalonate.
Example 3 Preparation of N,N'-bis(dicarboxymethyl)-l,4,10,13-tetraoxa-7,16- -diazacyclooctadecane tetrapotassiu salt a) After neutralizing 1.32 g (7.22 mmol) of 2-bromomalonic acid in 1.0 ml of water by adding potassium hydroxide solution of 5.760 mole/litre concentration in the presence of phenolphthalein indicator, 1.25 g (4.77 mmol) of l,4,10,13-tetraoxa-7,16-diaza- cyclooctadecane are added. The reaction mixture is heated at 50°G for 26 hours while adding an equivalent amount of potassium hydr¬ oxide solution of 5.760 mole/litre concentration in portions. After evaporating the reaction mixture the solid residue is dried under reduced pressure and then extracted with a total of 20 ml of methylene chloride in several portions. After evaporation the residue is dried to give 0.35 g (1.73 mmol) of N-dicarboxymethyl- -l,4,10,13-tetraoxa-7,16-diazacyclooctadecane dipotassium salt containing 16.7% by weight of potassium bromide (intermediate). This product can be used in a next manufacturing batch. The residue of the methylene chloride extraction is extracted with 60 ml of anhydrous ethanol and after evaporation of the extract the residue is dried to give 2.18 g of product, i.e. a yield of 94.0% calculated for the macrocycle used.
The product is a double salt formed with potassium bromide which contains 29.97% by weight of potassium bromide.
1H-NMR spectrum of the intermediate (200 MHz, D20, <Tppm): 3.86 (IH, s); 3.63 (16H, m); 2.89 (4H, t); 2.78 (4H, m). ^H-NMR spectrum of the double salt formed with potassium bromide (200 MHz, D205 S"ppm): 3.99 (2H, s); 3.69 (8H, s); 3.63 (8H, t); 2.86 (8H, t). b) A pure potassium bromide-free product can be prepared by extracting the product obtained as described above with 97% by volume ethanol to give 1.16 g of product, i.e. a yield of 75.6% calculated for the macrocycle used. -H-NMR spectrum of the title product (200 MHz, D 0, T'ppm): 4.00 (2H, broad s); 3.70 (8H, broad s); 3.65 (8H, broad); 2.88 (8H, broad). Example 4 Preparation of N,N'-bis(dicarboxymethyl)-l,4,10,13-tetraoxa-7,16- -diazacyclooctadecane magnesium complex disodium salt
0.30 g (1.46 mmol) magnesium chloride hexahydrate dissolved in 2.0 ml of water is added to a solution containing 0.81 g (1.46 mmol) of product prepared according to Example 1 b) in 3.0 ml of water. After 30 minutes the solution is evaporated under reduced pressure and the residue is dried to give 0.93 g (97.8%) of title product containing 17.99% by weight of sodium chloride. 1H-NMR spectrum of the title product (200 MHz, D20 in the pres¬ ence of NaOD, (Tppm): 4.00 (2H, s); 3.67 (8H, s); 3.62 (8H, broad); 2.30 (8H, broad).
13C-NMR spectrum (50 MHz, D20, i-Tppm): 179.71 (£=0); 71.88 and 71.05 (0-CH2); 54.51 (N-£H2). Note: due to deuteration the resonance signal of £H(C00)2 is absent.
Example 5 Preparation of N, '-bis(dicarboxymethyl)-l,4,10,13-tetraoxa-7,16- -diazacyclooctadecaπe calcium complex disodium salt containing sodium chloride
The process described in Example 4 is followed by using 0,92 g (1.65 mmol) of product obtained according to Example 1 b) and 0.24 g (1.65 mmol) of calcium chloride dihydrate to give 1.08 g (98.2%) of title product containing 17.57% by weight of sodium chloride.
1H-NMR spectrum of the product (200 MHz, D 0 , - _pm) : 3.90 (4H, broad) ; 3.53 (14H , broad) ; 2.92 (4H , coalesced t) ; 2.72 (4H, coalesced t) . 13C-NMR spectrum (50 MHz , D20 , <Tppm) : 179.23 (£=0) ; 82.38 (£H(C00)2) ; 71.62 (0-£H2) ; 55.63 (N-£H2) .
Example 6 Preparation of N , N ' -bis(dicarboxymethyl ) -1 , 4 , 10 , 13-tetraoxa-7 ,16- -diazacyclooctadecaπe calcium complex disodium salt containing disodium hydroxymalonate and sodium chloride After neutralizing 3.44 g (18.825 mmol) of 2-bromomaloπic acid in 1.0 ml of water by adding sodium hydroxide solution of 8.360 mole/litre concentration in the presence of phenolphthalein indicator, 2.010 g (7.65 mmol) of l,4,10,13-tetraoxa-7,16-diaza- cyclooctadecaπe are added. The reaction mixture is heated at 30 to 45°C for 43 to 4G hours while adding sodium hydroxide solution (1.83 ml) required to form the disubstituted compound. There¬ after, the reaction mixture is maintained at 60°C for 22 to 25 hours while portionwise adding sodium hydroxide solution in an amount required to hydrolyze the uπreacted 2-bromomalonate. After termination of the reaction the solution is evaporated, then Example 1 b) is followed to obtain 4.720 g of dry crude product containing 12.0% by weight of disodium alonate and practically no sodium bromide. The crude product may be worked up in any of the following two ways: a) The crude product is dissolved in a mixture of 3.0 ml of water and 7.5 ml of calcium chloride solution of 1.000 mole/litre concentration. 12.0 ml of 99.7% by volume ethanol and 0.85 ml of calcium chloride are added to the above solution under stirring, then the ethanol content of the solution is adjusted to 90% by volume by adding 105 ml of 99.7% by volume ethanol. After vigorously stirring the suspension obtained for 30 to 60 minutes with heating and then filtering off the solid precipitate, the filtrate is evaporated under reduced pressure and the half-dry product is dried at 75 to 85°C under reduced pressure to give 4.48 g (90.6%) of the title product containing 14.0% by weight of sodium chloride and 1.08% by weight of disodium hydroxymalonate.
The -H-NMR spectrum of the product (200 MHz, D20, f"ppm) is in agreement with that of the product of Example 5, except that a resonance signal also appears at 4.31 ppm (IH, s) which is characteristic of hydroxymalonate. b) The crude product is worked up as described under a) above, except that after adding the first portion (7.50 ml) of the calcium chloride solution an additional portion of 3.10 ml of calcium chloride solution of 1 .000 mole/litre concentration is added to the reaction mixture, the ethanol content of the mixture is adjusted to 90% by volume by adding 114 ml of ethanol and the product is dried in nitrogen stream to give 5.00 g (94.9%) of
5 product containing also 19.5 mol% of calcium salt of the calcium complex (as calculated for the total of macrocycle) in addition to the disodium salt of the calcium complex.
The product contains 13.2% by weight of sodium chloride, 7.35% by weight of water and a negligible amount of disodium
10 hydroxymalonate.
The iH-NMR spectrum of the product (200 MHz, D20 , ^""ppm) is in agreement with that of the product of Example 5.
Example 7 Preparation of N , N ' -bis(dicarbαxymethyl ) -1 , 4 , 10 , 13-tetraoxa-7 , 16-
1.5 -diazacyclooctadecaπe calcium complex diammonium
0. 5 ml of water , 2 .04 ml of 0 .998 mole/litre calcium chloride solution and then 30 ml of anhydrous ethanol are added to 0.554 g (1.000 mmol) of tetrasodium salt obtained according to Example 1 b) . The solution is evaporated to about the third of
20 its original volume and anhydrous ethanol is added in a sufficient amount to adjust the ethanol concentration of the solution to 95-96% by volume. Thereafter the solution is warmed, stirred for 30 minutes , the sodium chloride precipitated is filtered off and washed with anhydrous ethanol. To the combined
25 filtrate 0.554 g (1.000 mmol ) of tetrasodium salt and 0.214 g
(4.000 mmol) of ammonium chloride and then water is added in an amount dissolving the solid materials . After evaporating the solution, the residue is made free from water at 75 to 80°C under reduced pressure to give 1.452 g (98.1%) of title product
30 containing 19.91% by weight of sodium chloride and 7.33% by weight of water. A pure chic ide-free product can be prepared by extraction with anhydrous ethanol.
1-H-NMR spectra of the chloride-free and sodium chloride-contain¬ ing product (200 MHz, D20, σ ppm) are identical: 3.90 (4H, broad m); 3.73 (14H, broad ); 2.92 (4H, broad t); 2.72 (4H, broad t).
Example 8 Preparation of N, '-bis(dicarboxymethyl)-l, ,10,13-tetraoxa-7,16- -diazacyclooctadecane calcium complex calcium salt After neutralizing 1.743 g (9.53 mmol) of 2-bromomalonic acid in 2.0 ml of water by adding calcium hydroxide in portions in the presence of phenolphthalein indicator, 1.000 g (3.01 mmol) of l,4,10,13-tetraoxa-7,16-diazacyclooctadecaπe is added. The reaction mixture is heated at 40, 45 and finally at 50°C for a total of 72 hours, then the reaction mixture is heated at 60°C for 24 hours while portionswise adding 0.85 g (11.47 mmol) of calcium hydroxide under vigorous stirring. Then, the precipitate (the major part of which is calcium hydroxymalonate) is filtered off and washed with 4 to 5 ml of water in 3 portions. The combined filtrate is evaporated under reduced pressure and then 2x35 ml of methylene chloride are distilled off from the evaporation residue to obtain a solid product which is dried at 75 to 85° under reduced pressure. In this way the title product is obtained in a yield of 2.710 g (89.7%) with a calcium bromide content of 31.5% by weight.
The 1H-NMR spectrum of this product (200 MHz, D20,<Tppm) is iden¬ tical with that of the product prepared according to Example 5. IR spectrum (KBr, cm-1): 2920, 2880 ( , ^ C_H); 1615 (vs, Other characteristic but unidentified frequencies: 1355, 1290
(m), 1250 (m), 1085 (vs), 950 (m).
Example 9
Preparation of N,N'-bis(dicarboxymethyl)-!,4,10,13-tetraoxa-7,16-
-diazacyclooctadecane iron(II) complex disodium salt The process described in Example 4 is followed by using
0.747 g (1.35 mmol) of product prepared according to Example l b) and 0.268 g (1.35 mmol) of ferrous chloride tetrahydrate, except that the oxidation of ferrous ions to ferric ions is prevented during the preparation is prevented by using nitrogen atmosphere. In this way the title product is obtained in a yield of 0.835 g (91.0%) with a sodium chloride content of 17.16% by weight.
The ^H-NMR spectrum of the product cannot be evaluated due to the presence of the paramagnetic ferrous ion. IR spectrum ( KBr , cm- 1 ) : 2910 , 2880 (m , .^ C_H) ; 1630 (vs ,
^ coo/as) ; 1400 (s> coo/s> -
Other characteristic but unidentified frequencies: 1355 (m), 1330 (m), 1100 (s), 930 (m). Example 10 Preparation of N,N'-bis(dicarboxymethyl)-l,4,10,13-tetraoxa-7,16- -diazacyclooctadecaπe zinc complex disodium salt
The process described in Example 4 is followed by using 0.735 g (1.32 mmol) of product prepared according to Example 1 b) and 0.180 g (1.32 mmol) of anhydrous zinc chloride to give 0.89 g (97.5%) of title product containing 16.92% by weight of sodium chloride.
1H-NMR spectrum (200 MHz, D20, ~ppm): 3.6 -4.2 (18H, broad t band system); 3.10 (8H, broad t). Example 11 Preparation of N,N'-bis(dicarboxymethyl)-l,4,10,13-tetraoxa-7,16- -diazacyclooctadecane trisodium salt
1.72 ml of hydrochloric acid solution of 1.048 mole/litre concentration are added to a solution of 1.000 g (1.804 mmol) of tetrasodium salt obtained according to Example 1 b) in 5.0 ml of water under cooling (at 0 to 5°C), then the solution is evapor¬ ated, the residue is made free from water by using methylene chloride then is dried at 60°C under reduced pressure to give 1.069 g (96.7%) of title product containing 9.5% by weight of sodium chloride. XH-NMR spectrum (200 MHz, D20, fppm): 4.18 (2H, s); 3.79 (16H, m, broad); 3.29 (8H, broad s).
The spectrum of the product taken uP in D20 in the presence of NaOD is in agreement with the spectrum given in Example 1 b). IR spectrum (KBr, cm-1): 2940, 2850, 1655, 1605 (vs,
Other characteristic but unidentified frequencies: 1345 (s), 1320
(s), 1120 (s), 1100 (s); 930 (m) .
Example 12 Preparation of N-dicarboxymethyl-N'-(l,l'-dicarboxyethyl)-l,4,- 10,13-tetraoxa-7,16-diazacyclooctadecane tetrasodium salt
After neutralizing 3.003 g (15.25 mmol) of bromomethyl- malonic acid in 0.5 ml of water by adding sodium hydroxide solu¬ tion of 8.360 mole/litre concentration at 0 to 5°C in the pres- eπce of phenolphthalein indicator, 2.000 g (7.62 mmol) of l,4,10,13-tetraoxa-7,16-diazacyclooctadecane are added. The solu¬ tion is maintained at 20 to 25°C for 8 to 10 days while portion- wise adding 1.82 ml (15.25 mmol) of sodium hydroxide solution of 8.360 mole/litre concentration. After termination of the reac- tion, the mixture is stirred at 55 to 60°C for 30 minutes, then evaporated. The dry residue is extracted in several portions with a total volume of 25 to 30 ml of methylene dichloride. After evaporating the extract, the residue is treated with ether and the solid precipitate is filtered off. The material remaining after the extraction with ether contains also a little amount of 1,4,10,13— etraoxa-7,16-diazacyclooctadecane which can be removed by dissolving the product in methylene dichloride and precipitating by ether. In this way a purified N-(l,l'- dicarboxyethyl)-1,4,10,13—tetraoxa-7,16-diazacyclooctadecane disodium salt containing 13.81% by weight of sodium bromide (intermediate) is obtained in a yield of 1.390 g (37.2%).
After evaporation of the ethereal extract 1.159 g of pure 1,4,10,13-tetraoxa-7,16-diazacyclooctadecane are recovered. Thus, the actual yield of the reaction corresponds to 38.5%. 1H-NMR spectrum of the intermediate (200 MHz, D 0, <Tppm): 3.66 (16H, m); 2.82 (4H, t); 2.72 (4H, t); 1.36 (3H, s).
By using the above intermediate the disubstituted derivative is obtained as follows.
After neutralizing 0.483 g (2.64 mmol) of 2-bromomalonic acid in 0.5 ml of water by adding sodium hydroxide solution of 0.360 mole/litre concentration in the presence of phenolphthalein indicator, 1.002 g (2.04 mmol) of the above intermediate coπtaiπ- iπg 13.81% by weight of sodium bromide are added, then the reac¬ tion mixture is maintained at 30 to 45°C for 72 hours and at 50 to 60 °C for 24 hours while portionwise adding 0.32 ml (2.64 mmol) of sodium hydroxyde solution of 8.360 mole/litre concentra¬ tion. After termination of the reaction the solution is evaporated and the residue is dried at 75 to 80°C under reduced pressure. After extracting the dry residue with anhydrous ethanol, the ethanolic extract is evaporated to dryπess under reduced pressure and dried to give 1.323 g (83.0%) of the double salt formed with 2.06 moles of sodium bromide. A sodium bromide-free product can be obtained from the double salt by extraction with 96% by volume of ethanol as described in Example 1 b) to give 0.532 g (54.5%) of the title product.
The 'H-NMR and IR spectra of the double salt are practically identical with those of the title product.
IR spectrum (KBr, cm"1): 2960, 2870 (m,^c_H); 1645, 1600 (vs,
Other characteristic but unidentified frequencies: 1355 (s), 1315 (s), 1095 (s), 930 (m). -H-NMR spectrum (200 MHz, D20, <Tppm): 3.89 (IH, s); 3.68 (16H, m); 2.92 (4H, t); 2.78 (4H), t); 1.41 (3H, s).
Example 13 Preparation of N-dicarboxymethyl-N'-djl'-dicarboxypropyD-l^,- 10,13-tetraoxa-7,16-diazacyclooctadecane tetrasodium salt sodium bromide double salt
The process described in Example 12 is followed by using 1.608 g (7.62 mmol) of 2-bromoethylmalonic acid and 1.000 g (3.81 mmol) of 1,4,10,13-tetraoxa-7,16-diazacyclooctadecane to give 0.517 g (26.2%) of N-(l,l'-dicarboxypropyl)-l,4,10,13-tetraoxa- -7,16-diazacyclooctadecane disodium salt containing 15.61% by weight of sodium bromide.
After evaporation of the ethereal extract 0.508 g of 1,4,10,13-tetraoxa-7,16-diazacyclooctadecane are recovered. Thus the actual yield is 53.3%. l-H-NMR spectrum of the intermediate (200 MHz, D20, cTpp ): 3.68 (16H, m); 2.88 (4H, t); 2.82 (4H, t); 1.84 (2H, q); 0.90 (3H, t). The title double salt containing 3.10 moles of sodium bromide is obtained in a yield of 0.475 g (52.7%) by using 0.517 g (1.00 mmol) of the above intermediate containing 15.61% by weight of sodium bromide and 0.229 g (1.20 mmol) of 2-bromo- alonic acid. 1H-NMR spectrum of the title double salt (200 MHz, D20, cTppm) : 3.88 (IH, s); 3.67 (16H, m); 2.91 (4H, t); 2.86 (4H, t); 1.84 (2H, q); 0.88 (3H, t).
Example 14 Preparation of N-dicarboxymethyl-N'-(benzyl-dicarboxymethyl)- 1,4,10,13-tetraoxa-7,16-diazacyclooctadecane tetrasodium salt containing disodium hydroxymalonate The process described in Example 12 is followed, except that the reaction is carried out in a water/ethaπol mixture of 1:1 volume ratio by using 2.081 g (7.62 mmol) of 2-bromo-2-beπzylma- lonic acid and 1.000 g (3.81 mmol) of 1,4,10,13-tetraoxa-7,16-di¬ azacyclooctadecane to obtain 0.372 g (17.4%) of N-(benzyl-dicarb- oxymethyl)-1,4,10,13-tetraoxa-7,16-diazacyclooctadecane disodium salt containing 11.21% by weight of sodium bromide (inter¬ mediate).
After evaporation of the ethereal extract 0.714 g of 1,4,10,13-tetraoxa-7,16-diazacyclooctadecane are recovered. Thus, the actual yield becomes 60.9%.
1H-NMR spectrum of the intermediate (200 MHz, D20, Tppm): 7.45 (2H, d); 7.29 (3H, ); 3.68 (12H, m); 3.57 (4H, t); 3.47 (2H, s); 2.78 (8H, m).
The title double salt containing 0.42 mole of disodium hydr- oxymaloπate is obtained by using 0.372 g (0.662 mmol) of the above intermediate containing 11.21% by weight of sodium bromide and 0.161 g (0.880 mmol) of 2-bromomaloπic acid. For obtaining the product, first an extraction with methylene chloride and then extraction with abs. ethanol are carried out to give the title salt in a yield of 0.432 g (91.4%).
1H-NMR spectrum of the title product (200 MHz, D20, <Tppm): 7.43 (2H, d); 7.29 (3H, m); 3.90 (IH, s); 3.64 (16H, broad); 3.34 (2H, s); 2.91 (4H, t); 2.80 (4H, t). Example 15
Preparation of N,N*-bis(l,1'-dicarboxyethyl)-l, ,10,13-tetraoxa- -7,16-diazacyclooctadecane tetrasodium salt
After neutralizing 3.11 g (14.79 mmol) of bromomethylmalonic acid dissolved in 1.0 ml of water by adding sodium hydroxide solution of 0.360 mole/litre concentration at 0 to 5°C in the presence of phenolphthalein indicator, 3.52 g (6.565 mmol) of N- -(1,1'-dicarboxyethyl)-l,4,10,13-tetraoxa-7,16-diazacycloocta¬ decane disodium salt containing 18.6% by weight of sodium bromide (intermediate) are added, then the reaction mixture is maintained at 20 to 25°C for 10 to 12 days while portioπwise adding 1.77 ml (14.79 mmol) of sodium hydroxide solution of 8.360 mole/litre concentration. Before termination of the reaction, the mixture is heated at 55 to 60°C for 30 minutes and then evaporated. The dry residue is extracted in several portions with .a total of 45 to 50 ml of methylene chloride. The extract is evaporated, the residue is treated with ether, the precipitate is filtered off and dried. In this way 2.08 g (4.29 mmol) of intermediate containing 14.0% by weight of sodium bromide are recovered which can be used in a next manufacturing batch. The solid material remaining after the extraction with methylene chloride is dried at 75 to 80°C under reduced pressure. After extraction of the dry residue with 55 to 60 ml of anhydrous ethanol, the ethanolic extract is evaporated to dryness under reduced pressure and dried to give 3.90 g (22.2%) of double salt containing 78.2% by weight of sodium bromide. The yield calcu¬ lated for the intermediate used up in the reaction is 64.3%. l-H-NMR spectrum of the double salt (200 MHz, D20, <fppm): 3.67 (8H, s); 3.64 (8H, t) ; 2.73 (8H, t); 1.36 (6H, s). A sodium bromid-free product is obtained from 3.90 g of double salt containing 73.2% by weight of sodium bromide by extraction with 96% by volume ethanol as described in Example 1 b). In this way 0.489 g (57.5%) of title product is obtained.
After evaporation and drying and a repeated extraction with anhydrous ethanol, a double salt containing 80 to 90% by weight of sodium bromide is obtained from the filtrate containing 96% by volume ethanol. This double salt can be utilized in a next manu¬ facturing batch. XH-NMR spectrum of the title product (200 MHz, D20, <Tppm): 3.70 (16H, broad m); 2.71 (8H, coalesced t); 1.34 (6H, broadened s).
Example 16 Preparation of N,N'-bis(benzyl-dicarboxymethyl)-l,4,10,13- -tetraoxa-7,16-diazacyclooctadecane tetrasodium salt sodium bro- ide double salt
The process described in Example 15 is followed; by carrying out the reaction with 0.362 g (1.324 mmol) of 2-bromo-2-benzylma- lonic acid and 0.372 g (0.662 mmol) of onosubstituted interme¬ diate containing 11.21% by weight of sodium bromide in a water/ethanol mixture of 1:1 volume ratio, a double salt contain¬ ing 4.2 moles of sodium bromide is obtained in a yield of 0.085 g (11.1%).
0.296 g of intermediate containing 11.21% by weight of sodium bromide is recovered. Thus, the yield calculated for the intermediate used up in the reaction is 54.2%. l-H-NMR spectrum of the title product (200 MHz, D20, <Tppm): 7.64 (4H, d); 7.45 (6H, m); 3.65 (12H, m); 3.52 (4H, t); 3.31 (4H, s); 2.68 (8H, t). Example 17
The acute toxicity values of the products prepared according to Examples 1 to 16 were determined on laboratory mice and rats in the following manner. Solutions containing the compounds in various concentrations were prepared by using physiological saline solution or glucose solution of 5% by weight concentration and the active agents were administered in various concentrations into the blood circulation of the animals by injecting them slowly during 3 to 5 minutes. Groups consisting of 6 to 10 animals (Swiss mice and Wistar rats of both sexes) each were used for the various dose levels. Thereafter, the animals were observed for 30 days. The LD5Q/3Q value (i.e. the dose causing the death of 50% of the experimental animals within 30 days) was determined from the number of animals died during this period by using probit analysis /D.3. Fiππey: Probit Analysis (2nd ed.) Cambridge University Press (1952)/. These values expressed in mmol/kg of body-weight for the active agents according to the invention are summarized in column (B) of Table 1. Table 1
Characteristic data of the products according to the invention (A) (B) (C) (D)
The radioactive isotope elimination-increasing effects of compounds prepared according to Examples 1 to 16 were compared on Swiss mice as described hereinafter. An activity of 37 to 74 kBq (1 to 2 /uCi) of radioactive strontium (Sr-85Cl2) or radioactive cerium (Ce-1 4Cl3), respectively, was administered into the abdominal cavity of the animals which were then divided into treatment groups consisting of 5 to 10 animals each. At 30 to 60 minutes after administration of the isotope, the animals of the treated groups were intra¬ venously (i.v.) given the active agent used in an amount to achieve a concentration of 50 to 100 /umol/kg of body-weight in the animal organism for each treatment. The animals of the con¬ trol groups were similarly treated with the carrier (sterile phy- siological saline or glucose solution of 5% by weight concentra¬ tion) without active agent.
The amount of radioactivity introduced to the animal organ¬ ism was determined immediately after administration of the iso¬ tope, then these measurements were repeated daily or in every two or three days in a device constructed for the purpose of whole- body measurements on small animals. The counts observed were related to the starting activity value of the zero (0) day and a so-called retention/time correlation was obtained by considering the activity retained in the organism. The change of activity of the animal organism in the time is illustrated in Figure 1 where the time (in days) elapsed after the treatment is shown on the abscissa and the whole-body retention as percentage is plotted on the ordinate. It can be seen that the rate of elimination of Sr- 85 administered into the abdominal cavity of control animals was slow: within 1 day only 15%, within 4 days 25% and within 7 days 30% of the activity were eliminated from their organism and the elimination was even more delayed in the later period. On the contrary, within 1 day 40%, within 4 days 65% and within 7 days 67% of the radioactivity introduced were excreted from the animal organism after a single treatment with 100 /umol/kg of the active agent prepared according to Example 13. Even more advantageous results were obtained by using the product prepared according to Example 5 which gave elimination values of 81, 84 and 85%, respectively, within the intervals mentioned above. Based on analysis carried out in the above manner, it was stated that the retention curves could be described by a two-component descending exponential function. The F factors and El values relating to the products according to the Examples mentioned above are summarized in the columns (C) and (D), respectively, of Table 1. It is obvious that the effectivities of various decorporating agents, particularly on the basis of their El values, are highly differ¬ ent. In our opinion, the agents with an El value of 0 to 5 are weak, those with an El value of 5 to 50 have a medium effect, those with an El value of 50 to 100 are good and those with an El value above 100 are excellent. Example 19 a) The whole-body retention curves illustrated in Figure 2 show the elimination of radioactive strontium introduced through the trachea into the lungs of Wistar rats after intraperitoneal (i.p.) administration of the compound described in Example 6 b). It can be seen from the pattern of the upper curve of Figure 2 that the radioactive strontium was eliminated to a low grade from the organism of control animals treated only with the solvent. Not more than 30 to 35% of the starting activity were eliminated in the days following the inner contamination. On the contrary, the whole-body load significantly decreased from 90% (measured on the controls) to 20% both in the group treated once with 50 /umol/kg of body weight of the agent according to the invention (middle curve) or in the group treated twice in 3-hour interwal (lower curve) within 1 day following the treatment. The rapid elimination of the isotope was continued in the days following the treatment, and reached 88 to 90% in the once-treated group and 94 to 96 in the twice-treated group. It is also an important experimental result that hardly any or no radioactive strontium could be detected in the bones of the animals treated with the active agent according to the invention and killed at the end of the experiment. The residual activity of 5 to 10% measured as whole-body retention was found in the soft parts and liver of the animals whereas the major part (65 to 70%) of the retention found in the controls were built in to the bones. Similarly advantage¬ ous results were obtained by administering the compounds accord¬ ing to the invention in an intravenous route or into the subcuta- neous connective tissue. b) The compounds of the invention increasing the isotope elimination were tried to remove other radioactive metals, firstly cerium-144 (belonging to the group of the rare earth elements) from the animal organism. In this Example the elimina- tion of Ce-1 Cl3, introduced to the lungs of female Wistar rats, is illustrated as a function of the time elapsed after a single dose or after a treatment repeated at a 24-hour interval (see Figure 3). The results obtained prove that the compounds accord¬ ing to the invention can advantageously be used also for the removal of this radioactive compound having a relatively low solubility in body fluids from the lungs. At the end of the experiment, i.e. on the 30th day, 40% of the introduced starting activity were present in the control animals whereas 14% were detected in the group treated i.p. once with the active agent according to the invention; and the whole-body retention decreased to 5.6% on effect of treatments with the active agent by 60 minutes and then by 24 hours after administration of the isotope. The beginning abrupt but later delayed pattern of whole- body retention curves of the treated groups is likely due to solubility relations of the radioactive contaminating compound and the elimination properties of the metal complex. Example 20 The effect of compounds according to the invention on the elimination of isotopes after administration into the blood cir¬ culation, abdominal cavity or subcutaneous connective tissue have been described in Example 17 to 19. From the viewpoint of human therapy and even more of the effective and rapid protection of a greater population it was important to justify that the compounds according to the invention are useful to decorporate internal radioisotope contaminations also by other routes of administra¬ tion.
Wistar rats were used for this purpose. In a part of the examinations radiostrontium was administered into the abdominal cavity of the animals and after 60 minutes the active agent according to the invention was given through the rachea into the lungs. The compounds indicated in Table 1 with an El value above 100 were used as active agents. Thereafter, the whole-body activ¬ ities were measured for 30 days. It turned out on evaluation of the whole-body retention curves, plotted in the usual manner, that the active agents according to the invention exerted a good effect on the elimination after inhalation in a powder or liquid aerosol form. The retention of 91% measured in the control ani¬ mals was diminished to 15% on the first day, and became lower than 10% on the 3rd day in the treated animals. An F factor value of 7.9 and El value of 164 (c.f. Table 1) were found which sup¬ ported the above statements.
The possibility of adsorption of the active agents according to the invention from the epithelial surface was studied in addi- tioπal experiments. A 3x3 cm area of the dorsal skin of rats was depilated. After administering radioactive strontium through the trachea into the lungs of the anaesthetized animals, whole-body activities were measured, then the active agent was applied in solution on the dorsal skin area previously depilated and cleaned. The area containing the active agent was covered with an adhesive plaster. It could be stated from daily measurements of the whole-body activites that the active agents according to the invention exterted their isotope-mobilizing effect through the skin, too. By considering all the measurement values, an F factor value of 2.5 and El value of 105 to 110 were obtained.
On the basis of the above experimental results the active agents according to the invention can be used also in the form of pharmaceutical compositions such as subliπgual tablet, supposi- tory, entεrosolvent dragee or capsule or transdermal plaster.

Claims (10)

Claims :
1. Compounds of the formula (I),
(I) wherein Q1 and Q2 mean hydrogen or a group of the formula (III), with the proviso that at least one of them is other than hydrogen; and in the groups of the formula (III), the
COO"
I
-C—R I COO"
R substituents independently mean hydrogen, a Ci c straight or branched chain alkyl group , a C2_5 straight or branched chain alkenyl group, phenyl or pheπyl-C^alkyl group, the two latter ones optionally being substituted on their aro¬ matic part by one or more halogen(s) , C^alkyl , C^alk- oxy, cyano or nitro group(s) ;
Me stands for an alkaline metal or alkaline earth metal or transition metal ion ; q is 0 or 1 ;
M and N, independently from each other, stand for hydrogen or an alkaline metal, alkaline earth metal or optionally substi¬ tuted ammonium ion; , n and p are integers each being equal to the charge of M, N or
Me, respectively; s and r are, independently from each other, 0, 1, 2, 3 or 4, with the proviso that
(i) r, s and q cannot simultaneously be 0; (ii) the number of hydrogens in the meaning of M or N may be
0, 1 or 2; (iii) q is 1 when R means hydrogen; and
(iv) M and N are other than sodium or lithium ions when q is 0.
2. A compound of the formula (I) as claimed in claim 1, wherein Q1 and Q2 are the same and R means hydrogen.
3. N,N'-bis(dicarboxymethyl)-l,4,10,13-tetraoxa-7,16-diaza¬ cyclooctadecane calcium complex disodium salt.
4. A composition useful for the decorporation of metal ions, mainly radioactive isotopes, being harmful to the living organ¬ ism, which comprises an effective amount of at least one compound of the formula (I),
(1)
wherein
Q1 and Q2 mean hydrogen or a group of the formula (III), COO"
I
- C— R
COO" in the groups of the formula (III)
R substituents independently represent hydrogen, a C-j^ straight or branched chain alkyl group, a C2_5 straight or branched chain alkenyl group, phenyl or phenyl-C^alkyl group, the two latter ones optionally being substituted on their aro¬ matic part by one or more halogeπ(s), C^alkyl, C^alk- oxy, cyano or nitro group(s), with the proviso that at least one of Q1 and Q2 is other than hydrogen; Me stands for an alkaline metal or alkaline earth metal or transition metal ion; q is 0 or 1;
M and N, independently from each other, stand for hydrogen or an alkaline metal, alkaline earth metal or optionally substi- tuted ammonium ion; , n and p are integers each being equal to the charge of M, N or
Me, respectively; s and r are, independently from each other, 0, 1, 2, 3 or 4, with the proviso that (i) r, s and q cannot simultaneously be 0; and
(ii) the number of hydrogens in the meaning of M or N may be 0, 1 or 2.
5. A composition as claimed in claim 4 characterized by a tablet, dragέe, capsule, suppository, injectable solution, powder or liquid aerosol or transdermal plaster form.
6. A composition as claimed in claim 4 or 5, which comprises as active ingredient a compound of the formula (I), wherein Q1 and Q2 are the same and R stands for hydrogen.
7. A composition as claimed in claim 4 or 5, which comprises N,N'-bis(dicarboxymethyl)-l,4,10,13-tetraoxa-7,16-diazacycloocta¬ decane calcium complex disodium salt as active ingredient.
8. Use of the compounds of the formula (I),
(I) wherein
G1 and Q2 mean hydrogen or a group of the formula (III),
C00"
I
-C—R
COO"
(III) in the groops of formula (III) the
R substituent independently represent hydrogen, a _ι_ straight or branched chain alkyl group, a C2_5 straight or branched chain alkenyl group, phenyl or phenyl-C^alkyl group, the two latter ones optionally being substituted on their aro¬ matic part by one or more halogen(s),. C^alkyl, C^alk- oxy, cyano or nitro group(s), with the proviso that at least one of Q1 and Q2 is other than hydrogen;
Me stands for an alkaline metal or alkaline earth metal or transition metal ion; q is 0 or 1;
M and N, independently from each other, stand for hydrogen or an alkaline metal, alkaline earth metal or optionally substi¬ tuted ammonium ion; m, π and p are integers each being equal to the charge of M, N or Me, respectively; s and r are, independently from each other, 0, 1, 2, 3 or 4, with the proviso that
(i) r, S and q cannot simultaneously be 0; and (ii) the number of hydrogens in the meaning of M or N may be
0, 1 or 2 for the decorporation of metal ions, mainly radioactive isotopes, being harmful to the living organism.
9. Use of a compound of the formula (I), wherein Q1 and Q2 are the same and R means hydrogen, for the decorporation of metal ions, mainly radioactive isotopes, being harmful to the livging organism.
10. Use of N,N'-bis(dicarboxymethyl)-l,4,10,13-tetraoxa- 7,16-diazacyclooctadecane calcium complex disodium salt for the decorporation of metal ions, mainly radioactive isotopes, being harmful to the living organism.
AU67116/90A 1990-01-16 1990-11-07 1,4,10,13-tetraoxa-7,16-diazacyclooctadecane derivatives, pharmaceutical compositions containing them and their use for the removal of toxic metal ions and radioactive isotopes from the living organism Ceased AU645507B2 (en)

Applications Claiming Priority (2)

Application Number Priority Date Filing Date Title
HU145/90 1990-01-16
HU90145A HU210667B (en) 1990-01-16 1990-01-16 Process for producing n,n'-bis(dicarboxy-methyl)-1,4,10,13-tetraoxa-7,16-diaza-cyclooktadecane derivatives, salts and complexes thereof and pharmaceutical compositions containing them

Publications (2)

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AU6711690A true AU6711690A (en) 1991-08-05
AU645507B2 AU645507B2 (en) 1994-01-20

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CA (1) CA2048627A1 (en)
HU (2) HUT73493A (en)
IN (1) IN171733B (en)
RU (1) RU2060256C1 (en)
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CA2092434A1 (en) * 1990-09-27 1992-03-28 Wolfgang J. Wrasidlo Chelating agents
HUP1100731A2 (en) 2011-12-30 2013-06-28 Stratoxer S Kft Complex forming compounds
EA201201241A1 (en) * 2012-06-19 2013-12-30 Елена Владимировна ОРЛОВА BIO SAFETY NANOCOMPOSITE POLYMER SORBENT FOR SELECTIVE BINDING OF Sr AND Cs ISOTOPES FROM LIQUID MEDIA AND RAW MATERIAL FOR ITS MANUFACTURE

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US4190462A (en) * 1978-07-04 1980-02-26 Shell Oil Company Dissolving barium sulfate scale with aqueous solutions of salts of carboxymethyl monocyclic macrocyclic polyamines
US4597903A (en) * 1984-08-21 1986-07-01 University Of Maryland Process for the direct preparation of N,N-disubstituted derivatives for 4,13-diaza-18-crown-6
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HU9502769D0 (en) 1995-11-28
EP0463123A1 (en) 1992-01-02
WO1991010655A1 (en) 1991-07-25
HU900145D0 (en) 1990-03-28
JPH04505626A (en) 1992-10-01
UA35547C2 (en) 2001-04-16
KR970009042B1 (en) 1997-06-03
IN171733B (en) 1992-12-26
HU210667B (en) 1998-03-30
AU645507B2 (en) 1994-01-20
RU2060256C1 (en) 1996-05-20
HUT73493A (en) 1996-08-28
CA2048627A1 (en) 1991-07-17

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