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1

Digitale Medien

Stereoselective pharmacokinetics of ifosfamide and its 2- and 3-N-dechloroethylated metabolites in female cancer patients (1996)

Granvil, Camille P. ; Ducharme, Julie ; Leyland-Jones, Brian ; [weitere]

Springer

Cancer chemotherapy and pharmacology 37 (1996), S. 451-456

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ISSN: 1432-0843

Schlagwort(e): Key words Ifosfamide enantiomers ; N-Dechloroethylation ; Metabolism ; Enantioselective pharmacokinetics

Quelle: Springer Online Journal Archives 1860-2000

Thema: Medizin

Notizen: Abstract The pharmacokinetics of the R and S enantiomers of ifosfamide (IFF) and of its 2- and 3-N-dechloroethylated metabolites (2-DCE-IFF and 3-DCE-IFF) were investigated in 14 cancer patients treated with a 3-h infusion of (R,S)-IFF (3 g/m2) with mesna uroprotection. An enantioselective gas chromatographic-mass spectrometric (GC-MS) assay was used to determine the concentrations in plasma and urine. The AUCs of (R)-IFF were significantly larger than those of (S)-IFF (2480±200 vs 1960±150 μM . h). The terminal half-lives (7.57±0.99 h) and mean residence times (11.17±1.10 h) of (R)-IFF were significantly longer than those of (S)-IFF, 6.03±0.82 h and 9.37±0.88 h, respectively. The mean volume of distribution at steady state of (R)-IFF (25.68±0.80 l/m2) was slightly smaller than that of (S)-IFF (27.35±0.89 l/m2). While the renal clearances of (R)-IFF and (S)-IFF were similar, the nonrenal clearance was significantly lower for (R)-IFF (30.20±2.70 vs 41.40±3.55 ml/m2 per min) as was total clearance (41.52±2.90 vs 52.37±3.75 ml/m2 per min). The AUC values for all of the DCE metabolites from (S)-IFF were significantly greater than those from (R)-IFF with 47% of the measured AUC accounted for by DCE from (S)-IFF compared to only 20% for (R)-IFF. Therefore, the enantioselective difference in IFF elimination can be partially explained by differences in N-dechloroethylation.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/s002800050411

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2

Digitale Medien

Flavone acetic acid (LM 975, NSC 347512) A novel antitumor agent (1987)

O'Dwyer, Peter J. ; Shoemaker, Dale ; Zaharko, Daniel S. ; [weitere]

Springer

Cancer chemotherapy and pharmacology 19 (1987), S. 6-10

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ISSN: 1432-0843

Quelle: Springer Online Journal Archives 1860-2000

Thema: Medizin

Notizen: Summary Flavone acetic acid (FAA) is a synthetic flavonoid compound which has recently begun clinical trials as an antitumor agent based on its striking activity in solid tumor model systems. The pharmacologic behavior of FAA in animals appears to be predictive of both its cytotoxic efficacy and its toxicity to normal tissues (principally the central nervous system and gastrointestinal tract). The design and conduct of phase I studies in man are based upon these principles, with the goal of maximizing their safety and efficacy.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/BF00296246

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3

Digitale Medien

A strategy for the development of two clinically active cisplatin analogs: CBDCA and CHIP (1990)

Foster, Brenda J. ; Harding, Bonnie J. ; Wolpert-DeFilippes, Mary K. ; [weitere]

Springer

Cancer chemotherapy and pharmacology 25 (1990), S. 395-404

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ISSN: 1432-0843

Quelle: Springer Online Journal Archives 1860-2000

Thema: Medizin

Notizen: Summary The antitumor agent cisplatin has a broad antitumor spectrum and has been incorporated into regimens that are curative for some malignant diseases. However, one of the major limitations to its clinical usefulness is the incidence of severe toxicities involving several major organ systems. Therefore, much enthusiasm has been generated for the development of cisplatin analogs that demonstrate an improved therapeutic index in some preclinical models. The two most promising analogs are CBDCA (carboplatin) and CHIP (iproplatin). The preclinical and early clinical trial results have demonstrated that these two compounds show activity in cisplatin-responsive tumors. The preclinical background providing the rationale for the clinical development of these two analogs is described. We suggest a means of screening for each analog's clinical antitumor activity and determining the analogs' utility against specific malignant diseases compared with that of the parent compound or standard treatment.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/BF00686049

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4

Digitale Medien

Anthracycline analogs The past, present, and future (1986)

Weiss, Raymond B. ; Sarosy, Gisele ; Clagett-Carr, Kathleen ; [weitere]

Springer

Cancer chemotherapy and pharmacology 18 (1986), S. 185-197

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ISSN: 1432-0843

Quelle: Springer Online Journal Archives 1860-2000

Thema: Medizin

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/BF00273384

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5

Digitale Medien

Letter to the editors (1987)

Mathé, Georges ; Carter, S. K. ; McElwain, T. J. ; [weitere]

Springer

Cancer chemotherapy and pharmacology 19 (1987), S. 350-350

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ISSN: 1432-0843

Quelle: Springer Online Journal Archives 1860-2000

Thema: Medizin

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/BF00261488

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6

Digitale Medien

Comparative studies between the effects of mitozolomide and two novel tetrazepinones PYRCL and QUINCL on NIH:OVCAR-3 cells (1998)

Jean-Claude, Bertrand Jacques ; Mustafa, Amir ; Damian, Z. ; [weitere]

Springer

Cancer chemotherapy and pharmacology 42 (1998), S. 59-67

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ISSN: 1432-0843

Schlagwort(e): Key words Tetrazepinones ; Cell cycle arrest ; DNA damage ; OVCAR-3 cells

Quelle: Springer Online Journal Archives 1860-2000

Thema: Medizin

Notizen: Abstract Cytotoxicity, reduction of macromolecule synthesis and cell cycle perturbations by two novel 3-(2-chloroethyl)-tetrazepinones, PYRCL and QUINCL were compared with those produced by the structurally related 3-(2-chloroethyl)-tetrazinone, mitozolomide, in the OVCAR-3 cell line. Methods: Macromolecule synthesis was determined by incorporation of 3H-thymidine, 3H-uridine and 3H-leucine into acid-precipitable fractions of OVCAR-3 cell extracts. Maxam-Gilbert sequencing was used to compare the DNA alkylating sites induced by the tetrazepinones, with those created by mitozolomide. Alkaline sucrose-density sedimentation was employed to detect genomic DNA damage. Also, the effects of the tetrazepinones on the cell cycle were determined by univariate flow cytometry. Results: At 3 h post-treatment, mitozolomide appeared as a selective inhibitor of DNA synthesis, while both tetrazepinones inhibited the synthesis of all three macromolecules. At 24 h post-treatment, the inhibition of DNA synthesis was observed to increase in cells treated with mitozolomide, while it decreased in those previously exposed to the tetrazepinones. Also at 24 h post-treatment, mitozolomide induced accumulation of cells in S(late)/G2M at low concentrations and in S-middle at high concentrations. In contrast, at the same recovery time, cells treated with the tetrazepinones accumulated specifically in G2M, the strength of the block being dose-dependent. At an equimolar concentration, the tetrazepinones induced weaker guanine N-7 alkylation than mitozolomide. By 24 h after treatment, cells exposed to the tetrazepinones showed significantly greater DNA fragmentation than those previously treated with mitozolomide. Conclusion: In summary, based on (a) their effects on DNA, RNA, protein synthesis and on the cell cycle, (b) their alkylating power and (c) their interactions with DNA, the 3-(2-chloroethyl)tetrazepinones appeared to kill tumor cells by a novel mechanism which may significantly differ from that of their 3-(2-chloroethyl)-tetrazinone counterpart, mitozolomide.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/s002800050785

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7

Digitale Medien

Echinomycin: The first bifunctional intercalating agent in clinical trials (1985)

Foster, Brenda J. ; Clagett-Carr, Kathleen ; Shoemaker, D. Dale ; [weitere]

Springer

Investigational new drugs 3 (1985), S. 403-410

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ISSN: 1573-0646

Schlagwort(e): Echinomycin ; intercalator ; Quinomycin A

Quelle: Springer Online Journal Archives 1860-2000

Thema: Chemie und Pharmazie , Medizin

Notizen: Summary Echinomycin is a quinoxaline antibiotic that was originally isolated from Streptomyces echinatus. Based on its antitumor activity against two i.p. implanted murine tumors, the B16 melanoma, and the P388 leukemia, it was brought into clinical trials by the National Cancer Institute. Recent studies on its cytotoxic action have related its antitumor activity with its ability to bifunctionally intercalate with double stranded DNA. Toxicologic studies were carried out in CDF1 mice and beagle dogs using intravenous injections. For the mice studies the dose ranges were 288–692 mcg/kg (864–2076 mcg/m2) by single bolus, and 112–254 mcg/kg/day (336–762 mcg/m2/day) for five consecutive days. In the dog, dose ranges studied were 8.9–89.4 mcg/kg (178–1788 mcg/m2) by single bolus, and 3.4–33.5 mcg/kg/day (68–670 mcg/m2/day) for five consecutive days. The major toxic effects were found in the gastrointestinal, hepatic, and lymphoreticular systems. These were reversible at all but the highest dose, in dogs that had been treated for five consecutive days. Phase I clinical trials using various intravenous schedules were sponsored by the National Cancer Institute. Nausea, vomiting, reversible liver enzyme abnormalities, and allergic reactions were the most common toxicities encountered. Based on results from these studies, the National Cancer Institute has recently begun phase II trials in a broad range of diseases. These trials will further characterize echinomycin's toxic effects and its antitumor activity.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/BF00170766

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8

Digitale Medien

Didemnin B (1986)

Chun, Hoo G. ; Davies, Barbara ; Hoth, Daniel ; [weitere]

Springer

Investigational new drugs 4 (1986), S. 279-284

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ISSN: 1573-0646

Schlagwort(e): didemnin B

Quelle: Springer Online Journal Archives 1860-2000

Thema: Chemie und Pharmazie , Medizin

Notizen: Abstract A new class of marine compounds, the didemnins, with potent antitumor activity has been identified. They share the novel structure of a cyclic depsipeptide. Among three structurally related compounds, didemnin B is by far the most potent in its in vitro cytotoxicity and in vivo antitumor activity (0.001 μg/ml inhibits the growth of L1210 leukemia cells by 50%). It also demonstrates good antitumor activity against B16 melanoma and moderate activity against M5076 sarcoma and P388 leukemia. The compound also has good antiviral and potent immunosuppressive properties. Although the precise mechanism of action for the cytotoxicity remains unknown, the agent inhibits protein synthesis more than DNA synthesis and the inhibition of protein synthesis is closely correlated with inhibition of L1210 cell growth. Toxicology studies in CD2F1 mice, Fischer 344 rats and beagle dogs reveal that major target organs are the lymphatics, gastrointestinal tract, liver and kidney. Phase I trials are currently in progress under the auspices of the National Cancer Institute.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/BF00179597

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9

Digitale Medien

Merbarone: an antitumor agent entering clinical trials (1987)

Glover, Alice ; Chun, Hoo G. ; Kleinman, Larry M. ; [weitere]

Springer

Investigational new drugs 5 (1987), S. 137-143

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ISSN: 1573-0646

Schlagwort(e): merbarone

Quelle: Springer Online Journal Archives 1860-2000

Thema: Chemie und Pharmazie , Medizin

Notizen: Summary Merbarone was developed to clinical trial stage on the basis of its ‘curative’ activity against P388 and L1210 leukemias and moderate activity against B16 melanoma and M5076 sarcoma. Its activity appears to be schedule-dependent favoring a longer duration of administration. The mechanism of action of merbarone is not yet established but it does induce single strand breaks in DNA apparently without binding to DNA. The pharmacokinetic data in the dog indicate that clearance mechanisms may be saturable. Merbarone is hydroxylated at the 4′ position in the rat, mouse and dog, and glucuronidated in the dog. Parent drug and the hydroxy metabolite are excreted in the urine. If saturable clearance mechanisms also pertain to man, this will mean that infusion rate (and therefore steady state concentrations reached) may be a significant factor in determining acute toxicity. Preclinical toxicology studies revealed that major target tissues are in the lymphoid organs, bone marrow, gastrointestinal tract and kidney. Some behavioral signs of reversible central nervous system toxicity were observed. Phase I trials have commenced using only a 5-day continuous intravenous infusion schedule based on the preclinical data. The pharmacokinetic information from these trials will be crucial for further clinical development of the compound, including selection of the optimal schedule(s) for phase II/III evaluation.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/BF00203538

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10

Digitale Medien

Arabinosyl-5-azacytosine: A novel nucleoside entering clinical trials (1987)

Grem, Jean L. ; Shoemaker, D. Dale ; Hoth, Daniel F. ; [weitere]

Springer

Investigational new drugs 5 (1987), S. 315-328

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ISSN: 1573-0646

Schlagwort(e): arabinosyl-5-azacytosine ; deoxycytidine kinase ; cytosine arabinoside ; 5-azacytidine

Quelle: Springer Online Journal Archives 1860-2000

Thema: Chemie und Pharmazie , Medizin

Notizen: Abstract Arabinosyl-5-azacytosine is a new compound which has been selected by the Division of Cancer Treatment, National Cancer Institute for clinical development as an antineoplastic agent based on its high degree of activity against a broad range of tumor types in preclinical studies. Therapeutic activity has been observed against murine and human leukemias, transplantable murine solid tumors, and human tumor xenografts. Arabinosyl-5-azacytosine exhibited a broader spectrum of activity against human solid tumors than cytosine arabinoside. Arabinosyl-5-azacytosine is phosphorylated to the nucleotide level by deoxycytidine kinase. Upon further anabolism to the triphosphate level, it can be incorporated into DNA. The mechanism of cytotoxicity is thought to be related to inhibition of DNA synthesis. Leukemic and solid tumor cell lines that are resistant to cytosine arabinoside due to deletion of deoxycytidine kinase activity are cross-resistant to arabinosyl-5-azacytosine. Unlike cytosine arabinoside, arabinosyl-5-azacytosine does not readily undergo deamination. Schedule dependence has been demonstrated in mice bearing L1210 leukemia, with superior activity seen with multiple doses administered on each treatment day compared to administration of larger but less frequently administered doses. From preliminary data in solid tumor models, however, antitumor activity did not appear to be superior with continuous infusion compared to that observed on a bolus schedule. Preclinial toxicology studies indicated that the bone marrow and gastrointestinal tract were the main target organs. A single large dose of arabinosyl-5-azacytosine could be tolerated by both mice and dogs. When administered as a continuous infusion, the toxicity was related to both the dose and duration of exposure, suggesting that toxicity resulted from a critical time above a threshold concentration as opposed to the total area under the concentration-time curve. Phase I clinical trials have been initiated to determine the maximum tolerated dose on a low dose continuous infusion schedule for 72 hours and also on a high dose short infusion daily times five schedule.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/BF00169970

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