ZIB

1

Electronic Resource

In vitro cytotoxicity of GC sequence directed alkylating agents related to distamycin (1993)

Lee, Moses ; Rhodes, Andrea L. ; Wyatt, Michael D. ; [et al.]

s.l. : American Chemical Society

Journal of medicinal chemistry 36 (1993), S. 863-870

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ISSN: 1520-4804

Source: ACS Legacy Archives

Topics: Chemistry and Pharmacology

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1021/jm00059a011

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2

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Pharmacokinetics of 4-demethoxydaunorubicin in cancer patients (1990)

Zanette, Luisa ; Zucchetti, Massimo ; Freshi, Andrea ; [et al.]

Springer

Cancer chemotherapy and pharmacology 25 (1990), S. 445-448

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ISSN: 1432-0843

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The clinical pharmacokinetics of 4-demethoxydaunorubicin was investigated in 28 cancer patients who received the drug orally. The majority of the patients were elderly (median age, 72 years). Nine of them also received an i. v. dose, and the bioavailability of the oral dose ranged between 9% and 39%. 4-Demethoxydaunorubicin peak levels were achieved 2–4 h after the oral dose in most patients. The drug was rapidly and extensively metabolized to 4-demethoxy-13-hydroxydaunorubicin, which is probably as active as the parent drug. The metabolite levels were much higher and longer lasting than the parent drug, suggesting that it may play an important role in the drug's pharmacological effects.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00686057

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3

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A limited sampling model for the pharmacokinetics of etoposide given orally (1993)

Gentili, Donatella ; Zucchetti, Massimo ; Torri, Valter ; [et al.]

Springer

Cancer chemotherapy and pharmacology 32 (1993), S. 482-486

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ISSN: 1432-0843

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract A limited sampling model of etoposide after oral administration to estimate the area under the plasma concentration-time curve from 0 to 24 h (AUC) by determination of the drug plasma levels at only two time points was developed by a multiple regression analysis on a training data set of 15 patients receiving oral doses ranging from 54 to 90 mg/m2. The equation describing the model is AUC (μg ml−1 h)=5.183 (μg ml−1 h)+1.193 (h)×C1h (μg/ml)+8.439 (h)×C4h (μg/ml) (R 2=0.93,P=0.0001), whereC 1h andC 4h represent the plasma etoposide concentrations at 1 and 4 h, respectively. The model was validated prospectively on a test data set of 13 patients receiving oral doses ranging from 52 to 87 mg/m2 and, additionally, on a data set of 7 patients receiving oral doses ranging between 176 and 200 mg/m2, investigated in a previous study. Validation on both test data sets gave a relative mean predictive error of 0.1% and a relative root mean square error of 15.8% and 16.7%, respectively. The present study shows that it is possible to obtain a good estimate of the plasma AUC after oral administration of etoposide using a two-time-point sampling model. The model can be used to monitor the etoposide AUC in patients receiving chronic oral treatment.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00685894

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4

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Changes in doxorubicin distribution and toxicity in mice pretreated with the cyclosporin analogue SDZ PSC 833 (1995)

Gonzalez, Odalys ; Colombo, Tina ; Fusco, Maurizio ; [et al.]

Springer

Cancer chemotherapy and pharmacology 36 (1995), S. 335-340

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ISSN: 1432-0843

Keywords: MDR ; Pgp ; SDZ PSC 833

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract SDZ PSC 833 (PSC 833) is a cyclosporin A analogue that is under clinical investigation in combination with doxorubicin (Dx) or other anticancer agents as a type-1 multidrug resistance (MDR-1)-reversing agent. The present study was focused on the effects of PSC 833 on the distribution and toxicity of Dx in non-tumor-bearing CDF1 male mice. Mice were given PSC 833 i.p. at 30 min before i.v. Dx treatment. Dx levels were determined by a high-performance liquid chromatography (HPLC) assay at different times during a 72-h period following Dx treatment in the serum, heart, intestine, liver, kidney, and adrenals of mice. In all tissues, Dx area under the concentrationtime curve (AUC) values were much greater in mice receiving 10 mg/kg Dx in combination with 12.5 or 25 mg/kg PSC 833 than in mice receiving Dx alone. The highest increase in Dx concentrations was found in the intestine, liver, kidney, and adrenals. Lower, albeit significant, differences were found in the heart. PSC 833 did not appear to influence either urinary or fecal Dx elimination or Dx metabolism to a great extent. Doses of PSC 833 devoid of any toxicity potentiated the acute and delayed toxicity of Dx dramatically. The mechanism responsible for this enhanced toxicity has not yet been elucidated but is likely to be related to an increased tissue retention of Dx due to inhibition of the P-glycoprotein (Pgp) pump by PSC 833, as has recently been proposed for cyclosporin A.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00689051

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5

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Metabolism and pharmacokinetics of p-(3,3-dimethyl-1-triazeno) benzoic acid in M5076 sarcoma-bearing mice (1989)

Benfenati, Emilio ; Farina, Pierluigi ; Colombo, Tina ; [et al.]

Springer

Cancer chemotherapy and pharmacology 24 (1989), S. 354-358

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ISSN: 1432-0843

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The pharmacokinetics of the anticancer agent p-(3,3-dimethyl-1-triazeno) benzoic acid (pCOOH-DMT), a drug now in phase I clinical trial in Europe, was investigated in C57 Bl female mice with M5076 reticulum-cell sarcoma that were treated i.v. with 200 mg/kg pCOOH-DMT. The drug disappeared from plasma with a terminal half-life of about 2.5 h. Plasma clearance was approximately 6 ml/min per kg. Distribution studies showed some differences in drug levels in different tissues. The highest levels were found in the tumor, liver, kidney and lung; lower levels were found in the spleen and gut, and the lowest, in the brain. The N-desmethyl derivative of pCOOH-DMT was not detectable in plasma or tissues of mice treated with the drug. Therefore, the previous evidence of low N-demethylation of pCOOH-DMT was confirmed. pCOOH-DMT glucuronide was identified by mass spectrometry and quantified by high-performance liquid chromatography (HPLC) in plasma, tissues and urine samples. pCOOH-DMT glucuronide appears to be the major urinary metabolite of pCOOH-DMT in mice. Another metabolite identified by mass spectrometry and quantified by HPLC in some tissues and urine was pCOOH-DMT glycinate.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00257441

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6

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O 6-Methylguanine-DNA methyltransferase activity and induction of novel immunogenicity in murine tumor cells treated with methylating agents (1992)

Bianchi, Roberta ; Citti, Lorenzo ; Beghetti, Rita ; [et al.]

Springer

Cancer chemotherapy and pharmacology 29 (1992), S. 277-282

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ISSN: 1432-0843

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary To investigate the mechanism of the generation of immunogenic tumor variants by mutagenic drugs, murine leukemia cells exhibiting different sensitivity to killing by the alkylator 1,3-bis(2-chloroethyl)-1-nitrosourea (BCNU) and different ability to repairO 6-methylguanine in their DNA were treated in vitro with a series of methylating agents, including triazene derivatives, temozolomide, and streptozotocin. At the population level, we found that BCNU-resistant cells (L1210/BCNU) that appeared to be cross-resistant to killing by a dimethyltriazene and expressed high levels ofO 6-methylguanine-DNA methyltransferase activity (mer+ phenotype) failed to generate highly immunogenic variant sublines on repeated exposure to the methylating agents. In contrast, all cells (L1210) that were susceptible to DNA alkylation damage and deficient inO 6-methylguanine repair (mer−) developed immunogenic variant sublines. A noticeable exception was represented by streptozotocin treatment, which was equally effective in mer+ and mer− cells. At the clonal level, a single exposure to streptozotocin or a triazene derivative resulted in a high incidence (33% and 50%, respectively) of immunogenic cell generation in mer− cells only. In mer+ cells, streptozotocin treatment led to a 33% incidence of immunogenic clones only when the cells were concurrently exposed toO 6-methylguanine as a free base. The activity ofO 6-methylguanine-DNA methyltransferase in mer+ cells was greatly reduced by treatment withO 6-methylguanine or streptozotocin, and the combination of the two drugs led to enzyme levels similar to those observed in mer− cells. Taken together, these data suggest that the mechanism ofO 6-alkylation may be operative in the induction of novel tumor-cell antigenicity by methylating agents.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00685945

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7

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Phase I clinical and pharmacological study of oral methoxymorpholinyl doxorubicin (PNU 152243) (1999)

Sessa, Cristiana ; Zucchetti, Massimo ; Ghielmini, Michele ; [et al.]

Springer

Cancer chemotherapy and pharmacology 44 (1999), S. 403-410

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ISSN: 1432-0843

Keywords: Key words Phase I ; Methoxymorpholinyl doxorubicin ; Anthracycline analogs ; Hematotoxicology ; Oral chemotherapy

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Purpose: The methoxymorpholinyl doxorubicin analogue PNU 152243 was brought into clinical studies because of preclinical observations of its non-cross-resistance in mdr tumor cells, dose-limiting neutropenia, lack of cardiotoxicity, and antitumor activity after oral administration. Methods: PNU 152243 was given orally every 4 weeks to 21 adults with a variety of solid tumors at doses ranging from 59 to 940 μg/m2. Antiemetic prophylaxis with 5-HT3 antagonists and steroids, given i.v. on day 1 and orally on days 2–8, was required beginning with the dose of 118 μg/m2. The plasma pharmacokinetics of PNU 152243 were determined by an HPLC method with fluorescence detection. The in vitro myelotoxic effects on granulocyte macrophage-colony forming cells (GM-CFC) of the plasma from 11 patients, obtained 4 and 6 h after treatment at all dose levels, were also assessed. Results: Neutropenia was the main hematologic toxic effect and the maximum tolerated dose (MTD) for myelotoxicity was 940 μg/m2, with neutropenia grade 3–4 in two of three patients. Dose-dependent nausea and vomiting were dose-limiting and the MTD for gastrointestinal toxicity was fixed at 820 μg/m2, with grade 4 vomiting in one of two patients. Other frequent toxic effects were diarrhea and fatigue. Peak levels of PNU 152243 were achieved 4 h after dosing. Dose-dependent Cmax and AUCExp, and significant interpatient variability of the main pharmacokinetic parameters were found. Very low levels of the 13-dihydrometabolite PNU 155051 were detected only at the highest doses. The hematotoxicity tests showed a 〈70% colony growth inhibition with no correlation between the growth inhibition effect and the degree of myelotoxicity in the same patient. Plasma concentrations of PNU 152243 were 1000 times lower than the concentration inhibiting the growth of 70% of colonies. No objective tumor responses were seen. Conclusions: Owing to the occurrence of severe and prolonged nausea and vomiting, the clinical development of oral PNU 152243 was discontinued. The higher-than-expected neutropenia and its lack of relationship with plasma levels of PNU 152243 and its 13-dihydroderivative PNU 155051 might be related to the formation of potent cytotoxic metabolites present in human plasma at undetectable concentrations and with prolonged half-life, as suggested by hematotoxicity tests performed with plasma from patients in GM-CFC assays.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/s002800050996

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8

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Dose-dependent pharmacokinetics of PMM in the rat (1981)

Colombo, Tina ; Torti, Laura ; D'Incalci, Maurizio

Springer

Cancer chemotherapy and pharmacology 5 (1981), S. 201-203

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ISSN: 1432-0843

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Concentrations of pentamethylmelamine (PMM) and some metabolites were determined in plasma of rats treated with 10 and 50 mg PMM/kg IV. The areas under the plasma levels curve after these doses were 241 and 1,827 μg/mlxmin; plasma clearances were 0.042 and 0.027 l·kg-1·min-1, respectively. These data suggest that PMM pharmacokinetics is dose-dependent in the rat. The N-demethylated metabolite levels were not proportional to the administered dose.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00258481

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9

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The pharmacokinetics of liposomal encapsulated daunorubicin are not modified by HAART in patients with HIV-associated Kaposi's sarcoma (2000)

Fumagalli, Luca ; Zucchetti, Massimo ; Parisi, Idria ; [et al.]

Springer

Cancer chemotherapy and pharmacology 45 (2000), S. 495-501

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ISSN: 1432-0843

Keywords: Key words Antiretroviral therapy ; Kaposi's sarcoma ; Liposomal daunorubicin ; Pharmacokinetics ; Protease inhibitors

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Purpose: To investigate the pharmacokinetics of liposomal daunorubicin (DaunoXome) administered alone or in combination with antiviral therapy including protease inhibitors (PI) to HIV-positive patients affected by Kaposi's sarcoma (KS). Patients and methods: A group of 18 patients with extensive or rapidly progressing AIDS-related KS received DaunoXome at a dose of 40 mg/m2 alone or in association with a triple combination therapy consisting of one PI plus two nucleoside reverse transcriptase inhibitors (NRTI). Daunorubicin pharmacokinetics were determined in a total of 23 cycles, 6 with DaunoXome alone, 9 in combination with indinavir, 6 with ritonavir and 2 with saquinavir. Plasma samples were obtained at different times during the 72 h after DaunoXome administration. Daunorubicin and daunorubicinol plasma levels were determined by high-performance liquid chromatography. Results: After the DaunoXome infusion, daunorubicin was rapidly cleared from the body following, in most cases, a one-compartment open kinetic model. The daunorubicin peak concentrations, clearances and elimination half-lives were (means ± SD): 16.3 ± 2.8 μg/ml, 0.3 ± 0.1 l/h per m2 and 5.6 ± 2.6 h after DaunoXome alone; 15.1 ± 4.9 μg/ml, 0.5 ± 0.3 l/h per m2 and 5.8 ± 2.1 h after the combination with indinavir; and 14.5 ± 2.8 μg/ml, 0.4 ± 0.2 l/h per m2 and 6.5 ± 3.9 h after the combination with ritonavir. In all groups, daunorubicinol plasma levels were approximately 25–30 times lower than those of the parent drug. Conclusion: Our data show that there are no significant differences in the pharmacokinetic parameters of daunorubicin in patients receiving DaunoXome in combination with indinavir and ritonavir compared with those in patients not receiving PIs. Therefore in patients affected by AIDS-related KS treated with Highly Active AntiRetroviral Therapy (HAART) there is no pharmacokinetic justification for reducing the doses of DaunoXome.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/s002800051025

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Pharmacokinetics of VP16-213 in Lewis lung carcinoma bearing mice (1982)

Colombo, Tina ; Broggini, Massimo ; Torti, Laura ; [et al.]

Springer

Cancer chemotherapy and pharmacology 7 (1982), S. 127-131

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ISSN: 1432-0843

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The pharmacokinetics of VP16 have been investigated in Lewis lung bearing mice after i.v. doses of 13 and 40 mg/kg. At both doses the plasma elimination half-life was around 30 min. The lowest VP16-213 levels were in brain and primary tumor. Drug concentrations were much higher in metastases than in primary tumor. The highest concentrations were in small intestine, liver and kidney. Drug levels in the liver were disproportionally higher after 40 mg/kg, the AUC value being approximately 12 times greater than after 13 mg/kg. Urinary excretion of VP16-213 as unchanged drug accounted for 20–30% of the administered dose in the 60 h after treatment. The concentration cytotoxicity curve was very steep and apparently similar for cells derived from primary tumor or metastases grown in vitro.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00254534

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