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  • 1
    Electronic Resource
    Electronic Resource
    Kinetics of tissue disposition of cis-ammine/cyclohexylamine-dichloroplatinum(II) and cisplatin in mice bearing FSaIIC tumors (1994)
    Springer
    Cancer chemotherapy and pharmacology 35 (1994), S. 38-44 
    Details
    ISSN: 1432-0843
    Keywords: Key words Alicyclic mixed amine complex ; Pharmacokinetics ; Tissue distribution
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Abstract  The clinical potential of mixed amine platinum(IV) complexes has been identified, and interest in this new class of antitumor agents has been heightened by demonstration of their activity in cisplatin-resistant neoplasms. These tetravalent platinum agents are expected to undergo a reductive reaction to form the corresponding platinum(II) drug prior to eliciting biological activity. cis-Ammine/cyclohexylamine-dichloroplatinum(II) is one such product that we evaluated with cisplatin in vivo, and we found the two complexes given i.v. or i.p. to have comparable activities against a solid murine fibrosarcoma. Following i.v. administration of the two compounds at equitoxic dose levels (20 mg/kg) to tumor-bearing mice, platinum levels in the plasma were consistently higher for cisplatin. Tissue platinum levels, in contrast, were comparable between the agents or higher for the mixed amine analog at the earliest (3-h) time point. The temporal profiles determined for the concentrations over 48 h were tissue- and/or drug-specific and could be described by terminal-phase constants or half-lives of platinum in most tissues. In the plasma, kidney, lung, and jejunum, platinum levels arising from both compounds decayed with half-lives of 24 – 92 h. The terminal-phase constants of platinum determined in the heart for the two complexes were not significantly different from zero, indicative of levels remaining steady, whereas the constants were negative in the spleen, indicative of an increase in tissue drug concentration. In the tumor, liver, and testes, positive values for the decay-phase constants corresponding to half-lives of 47, 256, and 79 h, respectively, were seen with the mixed amine complex; this pattern contrasted with that found for cisplatin, for which the terminal-phase constant was either zero or negative. In vitro binding studies demonstrated the mixed amine complex to be more reactive. Thus, the presence of one ammine and one cyclohexylamine carrier ligand in the mixed amine complex, as opposed to the diammine ligands in cisplatin, leads to an increase in drug distribution and an alteration in the kinetics of tissue binding and removal of platinum.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/BF00686282
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    Paper (German National Licenses)
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  • 2
    Electronic Resource
    Electronic Resource
    Kinetics of tissue disposition ofcis-ammine/cyclohexylamine-dichloroplatinum(II) and cisplatin in mice bearing FSallC tumors (1994)
    Springer
    Cancer chemotherapy and pharmacology 35 (1994), S. 38-44 
    Details
    ISSN: 1432-0843
    Keywords: Alicyclic mixed amine complex ; Pharmacokinetics ; Tissue distribution
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Abstract The clinical potential of mixed amine platinum(IV) complexes has been identified, and interest in this new class of antitumor agents has been heightened by demonstration of their activity in cisplatin-resistant neoplasms. These tetravalent platinum agents are expected to undergo a reductive reaction to form the corresponding platinum(II) drug prior to eliciting biological activity.cis-Ammine/cyclohexylamine-dichloroplatinum(II) is one such product that we evaluated with cisplatin in vivo, and we found the two complexes given i.v. or i.p. to have comparable activities against a solid murine fibrosarcoma. Following i.v. administration of the two compounds at equitoxic dose levels (20 mg/kg) to tumor-bearing mice, platinum levels in the plasma were consistently higher for cisplatin. Tissue platinum levels, in contrast, were comparable between the agents or higher for the mixed amine analog at the earliest (3-h) time point. The temporal profiles determined for the concentrations over 48 h were tissue-and/or drug-specific and could be described by terminalphase constants or half-lives of platinum in most tissues. In the plasma, kidney, lung, and jejunum, platinum levels arising from both compounds decayed with half-lives of 24–92 h. The terminal-phase constants of platinum determined in the heart for the two complexes were not significantly different from zero, indicative of levels remaining steady, whereas the constants were negative in the spleen, indicative of an increase in tissue drug concentration. In the tumor, liver, and testes, positive values for the decay-phase constants corresponding to half-lives of 47, 256, and 79 h, respectively, were seen with the mixed amine complex; this pattern contrasted with that found for cisplatin, for which the terminal-phase constant was either zero or negative. In vitro binding studies demonstrated the mixed amine complex to be more reactive. Thus, the presence of one ammine and one cyclohexylamine carrier ligand in the mixed amine complex, as opposed to the diammine ligands in cisplatin, leads to an increase in drug distribution and an alteration in the kinetics of tissue binding and removal of platinum.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/BF00686282
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    Paper (German National Licenses)
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  • 3
    Electronic Resource
    Electronic Resource
    Ammine/amine platinum (II) complexes effective in vivo against murine tumors sensitive or resistant to cisplatin and tetraplatin (1994)
    Springer
    Journal of cancer research and clinical oncology 120 (1994), S. 571-577 
    Details
    ISSN: 1432-1335
    Keywords: Ammine/amine platinum complex ; Structure/efficacy relationship ; Drug resistance
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Abstract Three homologous series, each differing from the other in the coordinated amine ligand class, namely alicyclic, heterocyclic or isoaliphatic, were highly effective against wild-type murine leukemia L1210/0 cells in vivo (T/C=171%–426% at optimal doses). Of the 13 complexes comprising the three series, 3 were inactive in the cisplatin-resistant L1210/DDP model, but the other 10 maintained good efficacy (T/C=131%–167%). Longterm survivors, frequently observed with these complexes in the L1210/0 model, were also seen in the L1210/DDP model but to a lesser extent. In the homologous alicyclic series, which contained six analogs, as the alicyclic ring size increased, potency against L1210/0 and L1210/DDP cells also increased up to cyclohexylamine, and then declined. Four ammine/alicyclic amine analogs were evaluated against L1210/DACH cells, which are cross-resistant to tetraplatin, and the clinically predictive M5076 reticulosarcoma. Although the congeners were ineffective or minimally effective in prolonging the survival time of L1210/DACH-bearing mice (T/C=111%–134%), 20%–40% cure rate was consistently observed and suggested that the compounds possessed a low inherent ability to circumvent resistance in these tumor cells also. In the solid M5076 model, activity was greatest (tumor growth delays of about 25 days) for the alicyclic homologs containing the ammine/cyclobutylamine or ammine/cyclopentylamine carrier ligand combination. In summary, ammine/amine platinum (II) analogs have demonstrated promise at the preclinical level in their ability to circumvent acquired resistance, which is a major drawback of cisplatin use in treating cancer.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/BF01212810
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  • 4
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    p16INK4A immunohistochemical staining and predictive value for progression of cervical intraepithelial neoplasia grade 1: A prospective study in China (2013)
    Wiley-Blackwell
    Details
    Publication Date: 2013-09-18
    Description: p16 INK4A is strongly expressed in tissues diagnosed as cervical intraepithelial neoplasia (CIN) and cancer in women infected with human papillomavirus (HPV), but few prospective studies have evaluated p16 INK4A as a marker for the risk of low-grade CIN (CIN1) progression. We investigated the prevalence of p16 INK4A immunostaining by CIN grade and whether overexpression of p16 INK4A in CIN1 predicts future risk for high-grade CIN in Chinese women. 6,557 Chinese women aged 30-49 years were screened from 2003 to 2005 using cytology and carcinogenic HPV test. Colposcopy was performed on women with any abnormal result. p16 INK4A Immunostaining was performed on biopsies from all women with CIN1, as well as randomly selected women with normal or CIN grade 2 and worse (CIN2+) biopsies. Women with CIN1 were followed up without treatment. Colposcopy was performed on all untreated women at a 2-year interval. The prevalence of p16 INK4A staining was 2.7%, 42.7%, 75.5%, 79.6% and 100% among women with normal, CIN1, 2, 3 and cancer biopsies respectively (P〈0.001). HPV positivity was strongly associated with p16 INK4A staining (OR=12.8; 95% CI: 5.2-31.6). p16 INK4A staining of CIN1 biopsies at baseline was associated with an increased risk of finding high-grade CIN over two years of follow up (OR=1.43; 95% CI: 0.52, 3.91). The two-year cumulative incidence of CIN2+ for p16 INK4A positive women was higher at 10.71% than for p16 INK4A negative women at 1.30% (crude RR=8.25, 95%CI: 1.02, 66.62). p16 INK4A overexpression is strongly associated with grade of CIN and risk of progression to high-grade CIN in women with low-grade lesions. © 2013 Wiley Periodicals, Inc.
    Print ISSN: 0020-7136
    Electronic ISSN: 1097-0215
    Topics: Biology , Medicine
    Published by Wiley-Blackwell
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  • 5
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    Nanoporous Cobalt(II) MOF Exhibiting Four Magnetic Ground States and Changes in Gas Sorption upon Post-Synthetic Modification (2014)
    American Chemical Society (ACS)
    Details
    Publication Date: 2014-03-18
    Description: Journal of the American Chemical Society DOI: 10.1021/ja500191r
    Print ISSN: 0002-7863
    Electronic ISSN: 1520-5126
    Topics: Chemistry and Pharmacology
    Published by American Chemical Society (ACS)
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  • 6
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    Isospin dependence of nuclear multifragmentation in statistical model (2011)
    Institute of Physics (IOP)
    Details
    Publication Date: 2011-06-11
    Description: The evolution of nuclear disintegration mechanisms with increasing excitation energy, from compound nucleus to multifragmentation, has been studied by using the Statistical Multifragmentation Model (SMM) within a micro-canonical ensemble. We discuss the observable characteristics as functions of excitation energy in multifragmentation, concentrating on the isospin dependence of the model in its decaying mechanism and break-up fragment configuration by comparing the A 0 = 200, Z 0 = 78 and A 0 = 200, Z 0 = 100 systems. The calculations indicate that the neutron-rich system ( Z 0 = 78) translates to a fission-like process from evaporation later than the symmetric nucleus at a lower excitation energy, but gets a larger average multiplicity as the excitation energy increases above 1.0 MeV/u.
    Print ISSN: 1674-1137
    Topics: Physics
    Published by Institute of Physics (IOP)
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