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  • Cell & Developmental Biology  (2)
  • 3D external beam radiotherapy  (1)
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  • 1
    Electronic Resource
    Electronic Resource
    3D Interstitial HDR Brachytherapy Combined with 3D External Beam Radiotherapy and Androgen Deprivation for Prostate Cancer Preliminary Results (2000)
    Springer
    Strahlentherapie und Onkologie 176 (2000), S. 361-367 
    Details
    ISSN: 1439-099X
    Keywords: Key Words: Prostate cancer ; HDR brachytherapy ; 3D external beam radiotherapy ; Androgen deprivation ; Dose volume histograms ; Schlüsselwörter: Prostatakarzinom ; HDR-Brachytherapie ; Externe 3D-Radiotherapie ; Androgendeprivation ; Dosis-Volumen-Histogramme
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Description / Table of Contents: Hintergrund: Auswertung der Praktikabilität, Verträglichkeit und Effektivität einer neuen interstitiellen 3D-HDR-Brachytherapie-Technik, kombiniert mit externer 3D-Radiotherapie und Androgendeprivation beim Prostatakarzinom. Patienten und Methoden: Von Januar 1997 bis August 1998 behandelten wir 35 Patienten mit Prostatakarzinomen im Stadium cT1–3 N0 M0. Die Daten von 32 Patienten mit einer Nachbeobachtungszeit von zwölf bis 28 Monaten (median: 18 Monate) wurden ausgewertet. Nach ultraschallgesteuerter transrektaler Implantation von vier nicht parallelen Nadeln erfolgte die CT-gestützte 3D-Brachytherapie-Planung (“Offenbach-System”). Alle Patienten erhielten vier Fraktionen der 3D-Brachytherapie mit einer Einzeldosis von 5 oder 7 Gy im Abstand von jeweils 14 Tagen. Anschließend erfolgte die externe 3D-Radiotherapie bis 39,6 oder 45,0 Gy. Alle Patienten erhielten zusätzlich eine Androgendeprivation, die zwei bis 19 Monate vor der Brachytherapie eingeleitet und drei Monate nach Abschluss der externen Radiotherapie abgesetzt wurde. Ergebnisse: Bei 29/32 Patienten (91%) sank der posttherapeutische PSA-Wert unter 1,5 ng/ml, davon bei 25 Patienten auf unter 0,5 ng/ml, bei vier Patienten auf 0,5 bis 1,5 ng/ml. Zwei Patienten entwickelten ein biochemisches Rezidiv. Die transrektale Implantation wurde sehr gut toleriert. Ein Patient entwickelte akute Grad-3-Toxizitäten des Harntraktes, kein Patient akute gastrointestinale Nebenwirkungen größer als Grad 1. Eine Grad-3-Spättoxizität des Harntraktes zeigte ein Patient, gastrointestinale Spättoxizitäten entwickelte kein Patient. Alle 140 Dosis-Volumen-Histogramme der 3D-HDR-Brachytherapie wurden ausgewertet. Schlussfolgerung: Die neue 3D-HDR-Brachytherapie-Technik, kombiniert mit externer 3D-Radiotherapie und Androgendeprivation, stellt eine praktikable, bisher gut verträgliche und effektive Therapiemodalität nach Kurzzeitnachbeobachtung von median 18 Monaten dar.
    Notes: Background: Evaluation of feasibility, tolerance and efficiency for a new 3D interstitial HDR brachytherapy technique combined with 3D external beam radiotherapy and androgen deprivation for prostate cancer. Patients and Methods: Between January 1997 and August 1998 we treated 35 patients with Stage cT1–3 N0 M0 prostate cancer. Thirty-two patients with a follow-up of 12 to 28 months (median: 18 months) were evaluated. After ultrasound-guided transrectal implantation of 4 non-parallel needles, CT based 3D brachytherapy treatment planning (“Offenbach system”) was performed. All patients received 4 fractions brachytherapy using a fractional dose of 5 or 7 Gy. Time between each fraction was 14 days. After brachytherapy 3D external irradiation followed up to 39.6 or 45.0 Gy. All patients received androgen deprivation, starting 2 to 19 months before brachytherapy, ending 3 months after 3D external radiotherapy. Results: Posttreatment PSA levels dropped to 〈 1.5 ng/ml in 29/32 patients (91%). In 25 patients PSA levels were 〈 0.5 ng/ml, in 4 patients 0.5 to 1.5 ng/ml. In 2 patients we noted biochemical relapse. Transrectal implantation was very well tolerated. Grade 3 acute urinary toxicity occurred in 1 patient. We noted no Grade 2 or higher acute gastrointestinal toxicity. One patient developed a Grade 3 late urinary toxicity. No patient showed late gastrointestinal side effects. All 140 dose-volume histograms for 3D HDR brachytherapy were analyzed. Conclusions: The new 3D HDR brachytherapy technique, combined with 3D external irradiation and androgen deprivation, is a feasible, so far well tolerated and effective treatment in the short-time follow-up of median 18 months.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/PL00002344
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  • 2
    Electronic Resource
    Electronic Resource
    Multiple mechanisms of growth inhibition by cyclic AMP derivatives in rat GH1 pituitary cells: Isolation of an adenylate cyclase-deficient variant (1981)
    New York, NY [u.a.] : Wiley-Blackwell
    Journal of Cellular Physiology 109 (1981), S. 289-297 
    Details
    ISSN: 0021-9541
    Keywords: Life and Medical Sciences ; Cell & Developmental Biology
    Source: Wiley InterScience Backfile Collection 1832-2000
    Topics: Biology , Medicine
    Notes: GH pituitary cells have been widely utilized for studies of hormone response mechanisms. Studies reported here were motivated by the desirability of isolating characterized GH clones defective in cyclic AMP synthesis or action. Spontaneously occurring GH1 cell variants resistant to the growthinhibitory effects of cyclic AMP analogs were isolated. Characterization of four variants showed that these were deficient in adenosine kinase and had acquired resistance to the cytotoxic effects of purine nucleoside derivatives formed in the culture medium. A second-stage selection was undertaken with mutagenized adenosine kinase-deficient cells. One 8 Br cAMP-resistant variant was found to have normal cyclic AMP-dependent protein kinase activity but exhibited altered adenylate cyclase activity. Activation of cyclase activity by fluoride, guanyl nucleotides, cholera toxin, and hormone (VIP) was subnormal in the variant. Mndependent cyclase activity was also subnormal, suggesting that the 8 Br cAMP-resistant variant may have a deficiency in the catalytic moiety of adenylate cyclase.Surprisingly, adenosine 3′ :5′ -monophosphate and 5′ -monophosphate derivatives were found to be equally potent in growth-inhibiting adenosine kinasedeficient cells. Cross-resistance to 8 Br AMP was observed in the 8 Br cAMP-resistant variant. We conclude that cyclic AMP derivatives inhibit growth of GH cells by an unanticipated mechanism that is, nonetheless, related to endogenous cyclic AMP synthesis.
    Additional Material: 9 Ill.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1002/jcp.1041090212
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  • 3
    Electronic Resource
    Electronic Resource
    Paradoxical effects of protein synthesis inhibitors on uridine uptake in cultured cells: Possible role of uncharged tRNA in regulating metabolism (1980)
    New York, NY [u.a.] : Wiley-Blackwell
    Journal of Cellular Physiology 103 (1980), S. 489-502 
    Details
    ISSN: 0021-9541
    Keywords: Life and Medical Sciences ; Cell & Developmental Biology
    Source: Wiley InterScience Backfile Collection 1832-2000
    Topics: Biology , Medicine
    Notes: Previous studies (J. Biol. Chem, 253: 99-105, 1978) showed that thyrotropin-releasing hormone (TRH) acutely stimulated uridine uptake in pituitary cell (GH4C1) cultures. Studies on the role of protein synthesis in this response to TRH led to the finding that an inhibitor of ribosomal translation, cycloheximide, also stimulated uridine uptake acutely. Studies reported here attempt to determine the mechanism of cycloheximide action and whether cycloheximide and hormone stimulation of uridine uptake occurred by similar pathways. The experiments presented indicate that: (1) seven inhibitors of ribosomal translation stimulated uridine uptake; (2) in contrast, inhibition of protein synthesis at tRNA aminoacylation resulted in reduced rates of uridine uptake; (3) inhibition of tRNA aminoacylation blocked cycloheximide but not TRH stimulation of uptake; (4) cycloheximide stimulation of uptake was restricted to amino acid-depleted cultures; (5) amino acid supplementation stimulated uridine uptake with a time-course identical to that of cycloheximide; (6) cycloheximide and amino acid supplementation promoted reacylation of cellular tRNAs in amino acid-depleted cultures; and (7) cycloheximide stimulation of uridine uptake resulted from enhanced nucleoside phosphorylation rather than increased uridine transport. We conclude that cycloheximide and amino acid stimulation of uridine phosphorylation may be mediated through a common pathway involving the extent of amino-acylation of cellular tRNAs. Furthermore, cycloheximide and TRH stimulate uridine phosphorylation by pathways that are distinguishable. It is apparent that not all cellular effects of cycloheximde can be attributed solely to inhibition of the synthesis of proteins.
    Additional Material: 7 Ill.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1002/jcp.1041030314
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