Antitumor activity of titanocene amino acid complexes

Seven ionic titanocene -amino acid (aa) complexes [(C₅H₅)₂Ti(aa)₂]²⁺[X]₂ ^– with aa = glycine,l-alanine, 2-methylalanine,d-l-phenylalanine,d,l-4-fluorophenylalanine and X = Cl or AsF₆, were investigated for antitumor activity against fluid Ehrlich ascites tumor growing in CF1 mice. These complexes are the first stable model compounds of titanocene units with protein components, synthesized from a water-like, methanolic medium. All titanocene amino acid complexes induced antitumor activity which was manifested by maximum cure rates ranging from 30 to 70% and increases in life span from 78 to 276% in comparison with untreated control animals. The complexes containing chloride as anion X were more effective than the hexafluoroarsenate derivatives, which surprisingly showed a low substance toxicity. In all cases, the antitumor activity of the ionic titanocene amino acid complexes tested was less pronounced than that of the neutral parent compound [(C₅H₅)₂TiCl₂].     

Enhanced anti-cancer activities of some derivatives of titanocene dichloride

The compounds (eta5-C5H5)2TiCl2 (I), currently undergoing phase II trials, (eta5-C5H5)(eta5-C5H4CO2Me)TiCl2 (II) and C5H4CO2Me)2TiCl2 (III) are assessed for their efficacies against a small lung cancer cell line. It is found that the introduction of the electron withdrawing carbomethoxy group into the cyclopentadienyl rings increases the effectiveness of this class of drugs, such that III compares favorably with the well known cisplatin.     

Antitumor properties of vindesine-monoclonal antibody conjugates

Summary The anticancer alkaloid vindesine (VDS) was conjugated to four mouse monoclonal antibodies recognizing human tumor-associated antigens. The antibodies were 96.5 (antimelanoma, IgG2a); 791T/36 (antiosteogenic sarcoma, IgG2b); 11.285.14, and 14.95.55 (anticarcinoembryonic antigen, IgG1 and IgG2a respectively). Conjugates VDS-96.5 and VDS-791T/36 were tested in vitro and shown to be specifically cytotoxic for target cells expressing the appropriate antigen. The in vivo effects of the antibodies and conjugates were tested against human tumor xenografts in athymic or immunodeprived mice using multiple treatments. Conjugate VDS-96.5 retarded the initial growth of a melanoma xenograft, whereas free antibody was without effect. Similarly, VDS-791T/36 but not free antibody retarded the growth of osteogenic sarcoma 791T. The most marked antitumor effects observed were those obtained with VDS conjugates of the anti-CEA antibodies against a colorectal tumor xenograft. Antibody 14.95.55 suppressed tumor growth both alone and as a VDS conjugate, whereas 11.285.14 produced only a slight effect alone but an almost complete and lasting suppression of tumor growth as a VDS conjugate. Free VDS had little effect at nontoxic levels. Acute studies showed that VDS-11.285.14 conjugate was considerably less toxic than free VDS in Balb/c mice.     

Dimethyl titanocene Y: A valuable precursor for libraries of cytotoxic titanocene derivatives

Reaction of the known titanocene Y 2 with methyl lithium at −15 °C yields bis-[(p-methoxybenzyl)cyclopentadienyl]titanium(IV) dimethyl (dimethyl titanocene Y, 3), a hitherto unknown, surprisingly robust titanium (IV) dimethyl species. Dimethyl titanocene Y was utilized in the preparation of several bis-[(p-methoxybenzyl)cyclopentadienyl]titanium(IV) dicarboxylates by the reaction with the free carboxylic acids in fair to good yields. Cytotoxicity of all new compounds has been estimated in Hela S3 cells.     

Antitumor activity of some organomettalic bismuth(III)thiolates

The neutral organobismuth(III)bis(thiolates) CH₃Bi(SCH₃)₂ and CH₃Bi(p-SC₆H₄NH₂)₂ and the ionic mercaptoanilinium derivative [CH₃Bi(p-SC₆H₄NH₂CH₃)₂]²⁺2I⁻ were tested for antitumor properties in the fluid Ehrlich ascites tumor systems of mice. They all effected an optimum cure rate of 100% and were characterized by values of the therapeutic index ranging between 3.2 and 5.0.     

Antitumor properties of chemically detoxified killed Brucella abortus organisms

Summary Killed Brucella abortus organisms of the vaccinal strain B19 were detoxified by incubation in NaOH. A 24-h incubation in 0.01 M NaOH increased the LD₅₀ of smooth (S) and rough (R) organisms 2–3 times in normal mice and 50–100 times in adrenalectomized mice. This NaOH treatment did not alter the antitumor activity of Brucella abortus as shown in EL4 lymphoma- and Lewis carcinoma-grafted mice. After incubation in NaOH, S bacteria injected IV retained their ability to provoke spleen hypertrophy and antibody synthesis, and S and R organisms injected into he footpad had comparable ability to induce granulomas. NaOH treatment tended to diminish the mitogenic activity of R bacteria for spleen cell cultures.     

Synthesis,Ti(IV) intake by apotransferrin and cytotoxic properties of functionalized titanocene dichlorides

Functionalization of cyclopentadienyl (Cp) ligands and incorporation of these into a Ti(IV) center require careful design and selection of the appropriate synthetic routes to obtain the desired product in reasonably good yields. As part of our research efforts in the area of titanocene antitumor agents, we have revisited the synthesis of Cp rings with electron-withdrawing groups and their corresponding titanocene dichlorides, (Cp-R)₂TiCl₂ and (Cp-R)CpTiCl₂, where R is CO₂CH₃ and CO₂CH₂CH₃. These complexes were characterized by elemental analysis and ¹H and ¹³C NMR and IR spectroscopies. This report presents the first detailed synthetic route for (Cp-CO₂CH₂CH₃)CpTiCl₂ and provides an alternate route for synthesis of (Cp-R)₂TiCl₂ complexes. The ability of these complexes to deliver Ti(IV) to apotransferrin was investigated to elucidate how the functionalized Cp ligands affect the titanium intake by apotransferrin. The subject complexes transfer Ti(IV) to human apotransferrin, loading both N- and C-lobes. The antitumor activity of these complexes against HT-29 cancer colon cells was determined using a 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide assay. Carboethoxy Cp functionalization results in complexes with a toxicity comparable to that of titanocene dichloride. The carbomethoxy-functionalized complexes proved to be nonactive at the time intervals studied here, regardless of their ability to donate the titanium atom to human apotransferrin.     

Antitumor properties of nonstarch polysaccharides: Fucoidans and chitosans

This review deals with the pharmacology of nonstarch polysaccharides, namely fucoidans and chitosans, isolated from marine organisms. The work summarizes information from the international literature on the antitumor activities of native polysaccharides and their derivatives. The structures and physicochemical properties of these polysaccharides are described and the molecular mechanisms of their antitumor and antimetastatic effects are discussed.     

A new series of titanocene dichloride derivatives bearing chiral alkylammonium groups; assessment of their cytotoxic properties

A series of new, water soluble titanocene dichloride derivatives containing chiral alkylammonium groups have been synthesized and characterized and their cytotoxicities against the human lung cancer cell lines A549, H209 and H209/CP have been assessed. The potencies of the compounds vary greatly, with primary ammonium salts being particularly ineffective. However, mono- and dicationic derivatives containing chiral ephedrine-type functional groups are very effective, in particular the dicationic species.     

Antitumor properties and toxicity of a carminomycin and protein complex

The properties of carminomycin complexes with protein, a bovine serum albumin prepared with two different methods using glutaraldehyde or carbodiimine were studied. The complex prepared with the use of carbodiimine was biologically inactive. The complex prepared with the use of glutaraldehyde had a molecular mass of about 15 000 000 dalton, was more toxic than carminomycin and possessed proportionally higher antitumor activity and a wider antitumor spectrum. The studies on the use of the method of carminomycin complex formation with antitumor immunoglobulins are promising.     

Antifungal properties of some pyrazolyl-alkyl-sulfides

Four 5-amino-4-alkylthio-pyrazoles were synthesized and their antifungal activity was evaluated in vitro in Trichophyton mentagrophytes, Microsporum cookei and Candida albicans. The compounds slightly influenced the growth kinetics of the yeast, but at concentrations ranging from 20 to 40 g/ml completely prevented the mycelial growth of the two dermatophytes cultivated on Sabouraud's agar medium. An electron microscopic study, undertaken by using the most active compound, showed that in C. albicans mitochondria were the only cell targets affected whereas in the dermatophytes cell wall, plasmalemma and the main cytoplasmic organelles were damaged in various degrees. Since the most remarkable alterations were connected with membrane abnormalities, the cytological changes observed were tentatively interpreted as a consequence of the compound intrusion into the lipid bilayer of the membranes, since the drug is lipophilic in nature.Investigations supported by a grant from Consiglio Nazionale delle Ricerche of Italy (Contract No. 79.01871.04)     

Complexing properties of some pyrimidines

The synthesis of transition metal barbiturate, and thiobarbiturate complexes containing different functional groups of variable electronic character with CoII, NiII, CuII, PdII, and PtII have been prepared. The stereochemistry and the mode of bonding of the complexes were determined by elemental analysis and electronic and vibrational spectra together with their magnetic moment values. Electronic spin resonance of copper complexes were recorded. The Racah parameter of some cobalt and nickel complexes were calculated. Some of the complexes are of mixed stereochemistry. All the PdII or PtII complexes are of square planar geometries.     

New antitumor titanocene derivatives containing hydrophilic ligands

Four titanocene derivatives containing hydrophilic ligands were tested for antiproliferative activity against Ehrlich ascites tumor in mice. The new compounds (C₅H₅)₂TiCl(p-SC₆H₄NH₃⁺Cl^?) (I) and (C₅H₅)₂Ti(p-SC₆H₄NH₃⁺Cl^?)₂ (II), containing hydrochlorinated p-aminothiophenolate ligands, and the known compounds (C₅H₅)₂Ti(cis-OOCCHCHCOOH)₂ (III) and (C₅H₅)₂Ti(OOCCCl₃)₂ (IV) containing the carboxylic acid anions hydrogen- maleinate and trichloroacetate as acido ligands, induced maximum cure rates of 100%. The T.I. values amounted to 4.4–4.6 (I), 3.5–4.1 (II), 3.7– 3.8 (III) and 5.5 (IV), and were slightly increased in comparison to (C₅H₅)₂TiCl₂ (T.I. = 3.3). The complexes I–III were rather soluble in water and equally active in a DMSO/saline (1/9, v/v) mixture, in pure saline and in buffered solutions. In the case of IV, the toxicity was considerably low (LD₅₀,440 mg/kg; LD₁₀₀, 500 mg/kg) in relation to (C₅H₅)₂TiCl₂ (LD₅₀, 100 mg/kg; LD₁₀₀, 140 mg/kg).