Synthesis and cytotoxicity of metal 4-methyl-8-quinolinethiolates

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It has been found that the nature of the substituent, its position in the quinoline ring, and the nature of the metal significantly affect the antitumor activity and toxicity of metal 8-quinolinethiolates. The most cytotoxic towards human fibrosarcoma HT-1080 and mouse hepatoma MG-22A tumor cells are the 6-methoxy-8-quinolinethiolates of rhodium, osmium, iridium, indium, antimony, and bismuth, however these are highly toxic towards normal mouse embryonic NIH 3T3 fibroblasts. The iridium 5-methyl-8-quinolinethiolate is somewhat less active to MG-22A cells but shows quite good selectivity of action because of its markedly lower toxicity.Keywords: metal 3-and 5-methyl-8-quinolinethiolates, metal 2-and 6-methoxy-8-quinolinethiolates, synthesis, toxicity, cytotoxicity.After more than 40 years, platinum complexes occupy a high profile place in the arsenal of antitumor agents [1-3]. During this time there have appeared problems connected with their use, i.e. high overall toxicity leading to unwanted side effects and resistance to platinum preparations in a series of tumors which can develop during the time of chemotherapy. Attempts have been made to overcome these observations by changing the ligands in the platinum complexes and, more recently, by exchanging the metal [4,[7][8][9][10][11].In this respect the most promising proved to be ruthenium complexes which have low overall toxicity and are selectively accumulated in the tumor cells [4,7,[12][13][14][15][16][17][18]. Two of them have carried on to clinical investigation [14,19,20]. At the same time their rhodium and osmium analogs have shown even greater cytotoxicity towards A549 lung and T47D mammary gland carcinoma cells [21].We have shown that not only ruthenium, rhodium, and osmium but also iridium complexes [22,23] with an 8-quinolinethiol [22,23] or 8-quinolineselenol [24,25] ligand show high cytotoxicity to HT-1080 human fibrosarcoma and MG-22A mouse hepatoma tumor cells. However, all of these compounds showing high activity towards tumor cells are also toxic to normal NIH 3T3 mouse embryonic fibroblasts [22]. The toxicity of the highly active rhodium and iridium 8-quinolinethiolates can be markedly decreased by the introduction into their molecules of a methyl group at the 4 position of the quinoline ring [23]. It was also found that substituents in different positions of the quinoline ring can increase the selectivity of action of di(8-quinolyl) disulfides [26]. __________________________________________________________________________________________

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confidence: 94%

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confidence: 99%

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confidence: 99%

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Synthesis and cytotoxicity of methyl-and methoxy-substituted metal 8-quinolinethiolates

Lukevics

Zaruma

Ashaks

et al. 2008

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“…Several rhodium complexes have revealed a greater toxicity towards A549 lung carcinoma and T47D mammary gland cells than their ruthenium analogs [22] and this points to the promise of novel antitumor agents amongst rhodium compounds [23][24][25][26]. A series of osmium complexes has also shown comparable cytotoxicity towards various tumor cells [22,[27][28][29][30][31] We have found that iridium complexes [32][33][34][35] as well as those of ruthenium, rhodium, and osmium show a high cytotoxicity towards human fibrosarcoma HT-1080 and mouse hepatoma MG-22A cells with the use of 8-quinolinethiol [32][33][34] or 8-quinolineselenol [35] as ligand. Certain polypyridyl complexes of iridium actively inhibit the growth of human MCF-7 (mammary gland cancer) and HT-29 (large intestine cancer) tumor cells [36].…”

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confidence: 99%

“…The toxicity of the complexes can be varied by the introduction of a substituent into the quinoline ring [35,51] but, as in the case of analogous 8-quinolinethiolates [32][33][34], the selectivity of the substituent is low.…”

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confidence: 99%

Synthesis and cytotoxicity of methyl-substituted 8-quinolineselenolates of ruthenium, rhodium, osmium, and iridium

Lukevics

Zaruma

Ashaks

et al. 2009

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A series of 2-methyl, 4-methyl, and 2,4-dimethyl-8-quinolineselenolates of ruthenium, rhodium, osmium, and iridium has been synthesized and their cytotoxicity towards HT-1080 (human fibrosarcoma) and MG-22A (mouse hepatoma) tumor cells studied. It was found that all of the osmium complexes had a high cytotoxicity towards both cell lines. Their toxicity towards the normal mouse embryonic fibroblasts NIH-3T3 depends on the position and number of methyl groups in the quinoline ring and decreases in the order 2-Me > 4-Me > 2,4-Me 2 . The greatest selectivity in cytoxic activity is noted for iridium 4-methyl-8-quinolineselenolate and ruthenium 2-methyl-8-quinolineselenolate.The successful use of platinum complexes in tumor chemotherapy together with the presence of unwanted side effects on the one hand and the resistance of several tumors to this preparation on the other [1] has encouraged an extended study of antitumor activity in the complexes of other metals [2].From the viewpoint of creating novel antitumor agents it has been found that the complexes and organometallic derivatives of ruthenium have low overall toxicity and are selectively accumulated in tumor cells [3][4][5][6][7][8][9][10][11][12][13][14][15][16][17][18][19][20]. Two of these have already been investigated clinically [2-4] and porphyrin containing ruthenium complexes (which show high phototoxicity towards melanoma cells) are promising agents for the photodynamic chemotherapy of tumors [21].Similar complexes of rhodium, osmium, and iridium have also shown a photosensitization effect towards melanoma cells [21]. Several rhodium complexes have revealed a greater toxicity towards A549 lung carcinoma and T47D mammary gland cells than their ruthenium analogs [22] and this points to the promise of novel antitumor agents amongst rhodium compounds [23][24][25][26]. A series of osmium complexes has also shown comparable cytotoxicity towards various tumor cells [22,[27][28][29][30][31].

Synthesis and cytotoxicity of pyridine and quinoline oxorhenium(V) complexes with tridentate (NS2, S3)/monodentate (s) coordination*

Segal

Zablotskaya

Knieß

et al. 2012

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New oxorhenium complexes with tridentate 3-thia-and 3-methylazapentane-1,5-dithiolate and monodentate pyridine and quinoline derivatives have been synthesized. As a result of investigation of biological activity a high cytotoxicity was found for the synthesized complexes in relation to tumor cells. The specificity of the 2-pyridylthiolato [3-(N-methyl)azapentane-1,5-dithiolato]oxorhenium(V) cytotoxic action towards cells of mouse hepatoma MG-22A on a background of low acute toxicity was established.Keywords: oxorhenium(V) complexes, pyridine, quinoline, rhenium, cytotoxicity.Derivatives of quinoline and pyridine are widely used for the synthesis of various medicinal agents including antitumor medications (rogletimide, peldesin, pazelliptine, oxysuran, ledacrine, lurtotecane, emitefur, brequinar, aconiazide, etc.) [1]. As structural fragments they also form part of the structure of the antitumor antibiotics nigrin [1], bruneomycin [2], and antitumor alkaloids camptothecin [3] and meridin [4]. On the other hand, a series of transition metal complexes [5,6], including quinoline-containing [7-10], and also complexes of rhenium [11][12][13], display antitumor activity and are potentially biological transporting agents for medications [14,15].In the present work, with the aim of studying the effect of the ligand nature on antitumor properties, neutral oxorhenium(V) complexes have been synthesized in which the oxorhenium(V) framework ReO 3+ is coordinated with the tridentate 3-thia-and 3-methylazapentane-1,5-dithiolate, and also with the monodentate 2-mercaptopyridine and 2-mercaptoquinoline. The formation of the complexes was carried out by "3+1" methodology using two different rhenium precursors 1 and 2 depending on the neutral donor atom of the tridentate ligand.Chloro(3-thiapentane-1,5-dithiolato)oxorhenium(V) (4) was obtained from tetra-n-butylammonium perrhenate as an intermediate for the synthesis of 2-pyridylthiolato(3-thiapentane-1,5-dithiolato)oxorhenium(V) (6). As a result of its reaction with pyridine-2-thiol (5) in refluxing acetonitrile, the chlorine atom in compound 4 was successfully replaced by a pyridylthiol residue with the formation of the corresponding rhenium complex 6 in high yield. An alternative approach was used