Article citationsMore>>
de Bono, J.S., Oudard, S., Ozguroglu, M., Hansen, S., Machiels, J.P., Kocak, I., Gravis, G., Bodrogi, I., Mackenzie, M.J., Shen, L., Roessner, M., Gupta, S. and Sartor, A.O. (2010) Prednisone plus Cabazitaxel or Mitoxantrone for Metastatic Castration-Resistant Prostate Cancer Progressing after Docetaxel Treatment: A Randomised Open-Label Trial. The Lancet, 376, 1147-1154.
https://doi.org/10.1016/S0140-6736(10)61389-X
has been cited by the following article:
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TITLE:
Switching of GnRH Agent from Agonist to Antagonist in Patients with Castration-Resistant Prostate Cancer
AUTHORS:
Shinji Fukui, Yasushi Nakai, Yoriaki Kagebayashi, Shoji Samma
KEYWORDS:
CRPC, GnRH Antagonist, PSA, FSH
JOURNAL NAME:
Open Journal of Urology,
Vol.6 No.12,
December
21,
2016
ABSTRACT: Objectives: To evaluate the efficacy of
alteration from gonadotropin-releasing hormone (GnRH) agonist to antagonist in
patients with castration-resistant prostate cancer (CRPC). Methods: Fourteen
patients with CRPC were switched from GnRH agonist to GnRH antagonist. CRPC was
defined as 3 consecutive rises of PSA values under androgen deprivation therapy
despite a testosterone level at the castration level. No patient underwent a
change in oral anti-androgen agent or any additional therapy. Patients who showed
increase of the PSA value within 10% or showed decrease in the PSA value
compared to the baseline were defined as responders. We measured serum PSA,
testosterone, follicular stimulating hormone (FSH), and leutenizing hormone
(LH) at the time of alteration and 3 months after alteration. Results: The mean
age at diagnosis was 74.8 ± 6.3 years with a mean initial PSA level of 537.3 ±
999.1 ng/mL. The mean age at alteration to GnRH antagonist was 81.4 years with
a mean PSA level of 28.6 ng/mL. Two out of 14 patients (14%) were judged as
responders based on PSA after alteration to GnRH antagonist, although they did
not show any further reduction of the serum testosterone level (remain less
than 0.03). Six patients showed further reduction of the serum FSH level after
alteration; however, they showed no PSA response (from 46.4 ± 42.6 to 69.4 ±
70.3). Conclusions: The switch from GnRH agonist to GnRH antagonist affected
14% of the patients (2 out of 14 patients) with CRPC at 3 months based on PSA.
Larger and longer-term studies are required to determine the efficacy of
alteration to GnRH antagonist in patients with CRPC.
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