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  • Key words 10-Propargyl-10-deazaaminopterin  (1)
  • Key words Protein farnesylation inhibitor  (1)
  • 1
    Digitale Medien
    Digitale Medien
    A new analogue of 10-deazaaminopterin with markedly enhanced curative effects against human tumor xenografts in mice (1998)
    Springer
    Cancer chemotherapy and pharmacology 42 (1998), S. 313-318 
    Details
    ISSN: 1432-0843
    Schlagwort(e): Key words 10-Propargyl-10-deazaaminopterin ; Cytotoxicity ; Efficacy ; Human tumors
    Quelle: Springer Online Journal Archives 1860-2000
    Thema: Medizin
    Notizen: Abstract Purpose: These studies sought to evaluate the biochemical and cellular pharmacokinetic properties, cytotoxicity and antitumor efficacy of a new analogue of 10-deaza-aminopterin (PDX) against human tumors. Methods: Studies were conducted with a group of human tumor cell lines in culture examining PDX and other folate analogues as permeants for mediated membrane transport, as inhibitors of dihdrofolate reductase and as substrates for folylpolyglutamate synthetase. These same analogues were examined for their cytotoxicity following a 3-h pulse exposure, in experiments providing a value for IC50. Other studies with these analogues were conducted in nude mice bearing subcutaneously implanted human tumors. Treatment of the mice was initiated 4 days after implantation of the tumor using a schedule of administration of one dose per day for 5 days. The tumors were measured 6 days after cessation of therapy and compared to controls for assessment of response. Results: In the CCRF-CEM cell system, PDX was 2- to 3-fold less effective as an inhibitor of dihydrofolate reductase than aminopterin (AMT), methotrexate (MTX) or edatrexate (EDX) but much more effective as a permeant for one-carbon, reduced folate transport inward (PDX 〉AMT ≃ EDX 〉MTX) and substrate for folylpolyglutamate synthetase (PDX 〉AMT 〉EDX 〉MTX). As predicted by these results, PDX was 15- to 40-fold more cytotoxic than MTX and 3- to 4-fold more cytotoxic than the highly potent EDX following a 3-h pulse exposure in culture of CCRF-CEM cells and cells from a panel of three human breast and two human nonsmall-cell (NSC) lung cancers. The same relative differences were shown for the therapeutic efficacy of these three analogues at equitoxic doses in studies with the human MX-1 and LX-1 tumors and the human A549 NSC lung tumor xenografted in nude mice. On a schedule of qd × 5 given 3–4 days posttransplant, MTX was minimally active (modest tumor growth delay) against all three tumors. EDX was highly active (25–35% complete regressions and 5–10% cures) against the MX-1 and LX-1 tumors but very modestly active (no regressions) against the A549 tumor. In contrast, PDX was even more active (75–85% complete regressions and 25–30% cures) than EDX against the MX-1 and LX-1 tumors and highly active (30% complete regressions and 20% cures) against the A549 tumor. Conclusions: These studies showed significantly enhanced antitumor properties of PDX compared with MTX and EDX. Based upon these results, clinical trials of PDX in patients with metastatic breast and NSC lung cancer appear to be warranted.
    Materialart: Digitale Medien
    URL: http://dx.doi.org/10.1007/s002800050823
    Bibliothek Standort Signatur Band/Heft/Jahr Verfügbarkeit
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  • 2
    Digitale Medien
    Digitale Medien
    A peptidomimetic inhibitor of ras functionality markedly suppresses growth of human prostate tumor xenografts in mice. Prospects for long-term clinical utility (2000)
    Springer
    Cancer chemotherapy and pharmacology 46 (2000), S. 79-83 
    Details
    ISSN: 1432-0843
    Schlagwort(e): Key words Protein farnesylation inhibitor ; Human prostate tumors ; Efficacy
    Quelle: Springer Online Journal Archives 1860-2000
    Thema: Medizin
    Notizen: Abstract Purpose: These studies sought to evaluate the antitumor properties of an inhibitor of ras functionality, L-744,832, which acts at the level of its associated protein farnesyltransferase. Methods: Studies were carried out to measure the effects of L-744,832 alone and in combination with paclitaxel (PTXL) against TSU-PR1, DU-145 and PC-3 human prostate tumors xenografted to NCR-nu1 (AT) mice. Tumor-bearing mice were treated on a schedule of daily for 5 days ×2 or 3 with the MTD of L-744,832 and every 3–4 days ×4 with the MTD of PTXL starting 3–5 days after tumor implantation. Tumor volume in millimeters (4/3πr3) was measured 3–5 days after cessation of treatment and the increase in tumor volume in treated and control groups compared. Statistical analysis was carried out by the Chi-squared test. Results: L-744,832 at its MTD markedly inhibited the growth of all three tumors (T/C for increase in tumor mass varied from 11% to 15% and inhibition of growth had a rapid onset (within 1–2 days) and was independent of ras gene status. Estimated tumor doubling times were 8–12-fold greater in treated animals than in control animals. Treatment with L-744,832 for as long as 3 weeks had no untoward effects on the mice as determined by gross examination or necropsy. Administration of L-744,832 with this same dose and schedule potentiated the growth-inhibitory effect of PTXL at its MTD and induced some regression of TSU-PR1 with no obvious deleterious effects on the mice. Conclusions: L-744,832 could be safely administered over a protracted period of time to mice at doses which were markedly inhibitory to the growth of three human prostate tumor xenografts and in combination with PTXL was also well tolerated and brought about some regression of the TSU-PR1 tumor. Overall, these results suggest that L-744,832 could be clinically useful for long-term treatment of early-stage prostate cancer in patients and as an adjunct to cytotoxic therapy for late stages of this disease.
    Materialart: Digitale Medien
    URL: http://dx.doi.org/10.1007/s002800000126
    Bibliothek Standort Signatur Band/Heft/Jahr Verfügbarkeit
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