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  • 1
    Electronic Resource
    Electronic Resource
    Glutathione-S-transferase Activates Novel Alkylating Agents (1994)
    s.l. : American Chemical Society
    Journal of medicinal chemistry 37 (1994), S. 1501-1507 
    Details
    ISSN: 1520-4804
    Source: ACS Legacy Archives
    Topics: Chemistry and Pharmacology
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1021/jm00036a016
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    Paper (German National Licenses)
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  • 2
    Electronic Resource
    Electronic Resource
    Affinity Fingerprinting (1995)
    [s.l.] : Nature Publishing Company
    Nature biotechnology 13 (1995), S. 965-966 
    Details
    ISSN: 1546-1696
    Source: Nature Archives 1869 - 2009
    Topics: Biology , Process Engineering, Biotechnology, Nutrition Technology
    Notes: [Auszug] We often think that a ligand binding to its target is finding the key that fits a lock. While this simile is useful for describing the complementarity of binding surfaces, it breaks down when one considers that there are literally thousands of ligands that can bind to a particular target—with ...
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1038/nbt0995-965
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    Paper (German National Licenses)
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  • 3
    Electronic Resource
    Electronic Resource
    Peptide mimetic drugs: A comment on progress and prospects (1996)
    [s.l.] : Nature Publishing Company
    Nature biotechnology 14 (1996), S. 709-709 
    Details
    ISSN: 1546-1696
    Source: Nature Archives 1869 - 2009
    Topics: Biology , Process Engineering, Biotechnology, Nutrition Technology
    Notes: [Auszug] The need for “translating” information from protein and peptide structures into the sort of small organic molecules typical of traditional Pharmaceuticals has long been a high-priority goal for pharmaceutical research. The progress made, due largely to the application of new technical ...
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1038/nbt0696-709
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    Paper (German National Licenses)
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  • 4
    Electronic Resource
    Electronic Resource
    Isozyme specificity of novel glutathione-S-transferase inhibitors (1993)
    Springer
    Cancer chemotherapy and pharmacology 33 (1993), S. 63-70 
    Details
    ISSN: 1432-0843
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Abstract A systematically diversified set of peptide analogs of the reaction product of glutathione with an electrophilic substrate have been tested as isozyme-specific inhibitors of human glutathione-S-transferase (GST). The potency of the best of the inhibitors is in the 0.5 to 20 micromolar range, with kinetics indicative of competitive inhibition with glutathione at the active site. The specificity observed among three recombinant-derived GST isozymes at both low and high potency ranged from negligible to high (at least 20-fold over the next most sensitive isozyme). These results define a novel strategy for the design of drugs targeting cells with elevated levels of particular GST isozymes, such as tumor cells for which elevated levels of GST are believed to be an important cause of chemotherapeutic drug resistance.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/BF00686025
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  • 5
    Electronic Resource
    Electronic Resource
    Isozyme-specific glutathione S-transferase inhibitors potentiate drug sensitivity in cultured human tumor cell lines (1996)
    Springer
    Cancer chemotherapy and pharmacology 37 (1996), S. 363-370 
    Details
    ISSN: 1432-0843
    Keywords: Key words GST inhibitor ; Potentiate ; Drug sensitivity
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Abstract  Novel glutathione (GSH) analogs, previously shown to inhibit glutathione S-transferase (GST) activity at about 1 μM in vitro, were tested for their ability to potentiate the killing of cultured tumor cells by chemotherapeutic drugs. When tested at doses up to 200 μM, the analogs were neither toxic nor capable of potentiating drug toxicity unless the diethyl ester (DEE) form was used for treatment of the cells. HPLC analysis revealed rapid internalization of the DEE and intracellular conversion to a monoethyl ester form that accumulated in the cell, followed by a more gradual loss of the second ester to generate the active parent form. For the four GSH analogs tested, the ability of the DEE forms to potentiate chlorambucil (CMB) toxicity in HT-29 human colon adenocarcinoma cells strongly correlated with the in vitro ability of the parent form to inhibit recombinant human P1-1. This isozyme is the dominant form of GST present in HT-29 cells. Of the four analog DEEs tested, γ-glutamyl-S-(benzyl)cysteinyl-R(−)-phenyl glycine (TER 117) DEE was the most effective in potentiating CMB toxicity in several cell lines: HT-29, HT4-1 (HT-29 subclone), SKOV-3 ovarian carcinoma, and SK VLB (vinblastine-resistant variant of SKOV-3) cells. γ-Glutamyl-S-(octyl)cysteinyl-glycine (TER 143) DEE potentiated mitomycin C (MTC) toxicity in HT4-1 and SK VLB cells while TER 117 DEE did not. TER 117 DEE enhanced melphalan effects on xenografts of HT4-1 in mice to a similar extent as that achieved with the previously described nonspecific GST inhibitor, ethacrynic acid. Taken together, our results indicate that cell-permeable analogs of GSH can potentiate cytotoxicity of common chemotherapeutic drugs and this effect has a strong positive correlation with the ability of the analogs to inhibit specific GST isozymes.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/s002800050398
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  • 6
    Electronic Resource
    Electronic Resource
    Reduced [3H]-tetrodotoxin binding in the nap ts paralytic mutant of Drosophila (1982)
    Springer
    Molecular genetics and genomics 187 (1982), S. 172-173 
    Details
    ISSN: 1617-4623
    Source: Springer Online Journal Archives 1860-2000
    Topics: Biology
    Notes: Summary The temperature-sensitive paralytic mutant of Drosophila, nap ts, has been shown to have defects in axonal physiology which suggest that it codes for a component of the voltage-sensitive sodium channel. Ligand binding studies using tritiated tetrodotoxin, a sodium channel antagonist, show a decrease in the apparent number of sodium channels in nap ts, providing additional support for this hypothesis.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/BF00384402
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