间歇性雄激素抑制治疗前列腺癌的临床经验:至少3年随访。

Molecular urology Pub Date : 1999-01-01
Goldenberg, Gleave, Taylor, Bruchovsky
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引用次数: 0

摘要

本报告回顾了间歇性雄激素抑制治疗前列腺癌的前瞻性II期评估的长期随访。本方案共纳入87例患者。在本报告发表时,已有50名男性被跟踪调查了至少3年。治疗开始联合雄激素阻断,并持续至少6个月,直到观察到血清PSA最低点。然后停止用药,直到血清PSA升高到10至20 ng/mL之间的平均值。这种治疗和不治疗的循环被重复,直到PSA的调节变得不依赖于雄激素。研究的总时间为40 - 126个月,平均为65.5个月。长期随访的第一个周期的停药期与在治疗开始前报告性功能正常或接近正常的男性的幸福感和性欲和效力的恢复有关。第1、2、3、4周期的平均停药时间(百分比)分别为15个月(54%)、10个月(48%)、8个月(45%)、7个月(40%)。研究小组包括9名因局部晚期癌症放射治疗后PSA浓度升高而接受治疗的患者。这些患者在治疗周期1和2中分别平均停药22个月和13个月。6例根治性前列腺切除术后PSA值升高且随访超过36个月的患者在治疗周期1和2中分别平均停药19个月和11个月。在87例患者中,23例在治疗中位数32个月时病情进展为雄激素独立,13例在治疗中位数48个月时因癌症特异性死亡。前列腺癌可通过间歇性雄激素抑制来控制。这种方法在患者停止治疗时改善了生活质量,降低了毒性和费用。II期试验表明,对患者预后没有负面影响。目前正在进行随机方案,以确定这种治疗是否对局部复发或转移性癌症患者的生存产生有利或不利的影响。
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Clinical Experience with Intermittent Androgen Suppression in Prostate Cancer: Minimum of 3 Years' Follow-Up.

This report reviews the long-term follow-up of a prospective Phase II evaluation of intermittent androgen suppression in the treatment of prostate cancer. A total of 87 patients have been entered in this protocol. At the time of this report, 50 men have been followed for a minimum of 3 years. Treatment was initiated with combined androgen blockade and continued for at least 6 months until a serum PSA nadir was observed. Medication was then withheld until the serum PSA increased to mean values between 10 and 20 ng/mL. This cycle of treatment and no treatment was repeated until the regulation of PSA became androgen independent. The total time in the study ranges from 40 to 126 months, with a mean of 65.5 months. The off-treatment period in the first cycle for the men with long-term follow-up was associated with an improvement in the sense of well-being and recovery of libido and potency in men who reported normal or near-normal sexual function before the start of therapy. The average time off therapy (percentage time off therapy) for cycles 1, 2, 3, and 4 was 15 months (54%), 10 months (48%), 8 months (45%), and 7 months (40%), respectively. The study group included 9 patients treated because of a rising PSA concentration after radiation therapy for locally advanced cancer. These patients have been off therapy for an average of 22 and 13 months in treatment cycles 1 and 2, respectively. Six patients with rising PSA values after radical prostatectomy and with follow-up exceeding 36 months have been off therapy for an average of 19 and 11 months in treatment cycles 1 and 2, respectively. Of the 87 patients, 23 have had their disease progress to androgen independence at a median of 32 months of treatment, and 13 have died cancer-specific deaths at a median of 48 months. Prostate cancer is amenable to control by intermittent androgen suppression. This approach affords an improved quality of life when the patient is off therapy, with reduced toxicity and costs. Phase II trials suggest that there is not a negative impact on patient outcome. Randomized protocols are currently in progress to determine whether survival is affected in a beneficial or adverse way by such treatment in men with locally recurrent or metastatic cancer.

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Farewell and Thank You Neural computation in urology: an orientation. Genetic adaptive neural network to predict biochemical failure after radical prostatectomy: a multi-institutional study. Predictive modeling techniques in prostate cancer. Application of Cre-loxP system to the urinary tract and cancer gene therapy.
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