1999
DOI: 10.1038/sj.pcan.4500317
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Intermittent versus continuous hormone deprivation in metastatic prostate cancer: preliminary data from an ongoing European study

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Cited by 6 publications
(5 citation statements)
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“…Intermittent treatment was stopped when PSA levels decreased below 4 ng/ml and signs of clinical progression disappeared, and restarted when there was evidence of progression or PSA levels rose above 10 ng/ml. Preliminary results from this study showed that intermittent therapy was acceptable to most patients, and that intermittent therapy was not associated with the early development of hormone independence 32 . There was no significant difference in the incidence of progression between patients receiving intermittent therapy and those receiving continuous therapy.…”
Section: Hormonal Therapy Alonementioning
confidence: 72%
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“…Intermittent treatment was stopped when PSA levels decreased below 4 ng/ml and signs of clinical progression disappeared, and restarted when there was evidence of progression or PSA levels rose above 10 ng/ml. Preliminary results from this study showed that intermittent therapy was acceptable to most patients, and that intermittent therapy was not associated with the early development of hormone independence 32 . There was no significant difference in the incidence of progression between patients receiving intermittent therapy and those receiving continuous therapy.…”
Section: Hormonal Therapy Alonementioning
confidence: 72%
“…Preliminary results from this study showed that intermittent therapy was acceptable to most patients, and that intermittent therapy was not associated with the early development of hormone independence. 32 There was no significant difference in the incidence of progression between patients receiving intermittent therapy and those receiving continuous therapy.…”
Section: Intermittent Androgen Deprivationmentioning
confidence: 88%
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“…Progression to a hormone‐refractory state appears due to the fact that apoptosis induced by androgen ablation is not able to eradicate all malignant cells, the remaining cells losing their apoptotic potential [30]. The emergence of androgen‐independent prostate cancer cells may arise from the selection of pre‐existing clones of androgen‐independent cells resistant to apoptosis generated randomly by genetic instability of tumours (clonal selection hypothesis) or from the upregulation of androgen‐repressed adaptive mechanisms and growth factors (adaptation hypothesis) [31].…”
Section: Intermittent Adtmentioning
confidence: 99%
“…However, phase II studies should be regarded mainly as a demonstration of the feasibility of the approach. Several phase III studies are currently comparing tumour progression, safety and quality of life with intermittent or continuous MAB in patients with metastatic prostate cancer 58,68 …”
Section: Pharmacokineticsmentioning
confidence: 99%