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用一种强效促黄体生成激素释放激素类似物治疗转移性前列腺癌。

The treatment of metastatic prostatic cancer with a potent luteinizing hormone releasing hormone analogue.

作者信息

Trachtenberg J

出版信息

J Urol. 1983 Jun;129(6):1149-52. doi: 10.1016/s0022-5347(17)52615-4.

Abstract

Metastatic prostatic cancer generally is treated by either castration or the administration of exogenous estrogens, both of which have significant clinical disadvantages. Luteinizing hormone releasing hormone analogues have been shown to suppress gonadal steroidogenesis in animals and humans. To assess the effect of the administration of a potent luteinizing hormone releasing hormone analogue, (D-Leu-6)luteinizing hormone releasing hormone (1-9) nonapeptide ethylamide, 9 patients with previously untreated stage D2 prostatic cancer were treated with this agent for 3 to 8 months. By 3 months of treatment all patients demonstrated a significant decrease in serum testosterone and a decreased peak serum luteinizing hormone and testosterone response to the acute administration of the analogue, with no change in baseline serum luteinizing hormone or prolactin. These data suggest that this analogue acts by decreasing the pituitary release of luteinizing hormone. No major adverse effects were noted with this treatment modality, and all patients were symptomatically improved and demonstrated a decrease or stabilization in tumor activity as measured by prostatic computerized tomography or ultrasound scan, prostatic acid phosphatase and bone scan. A representative case is presented. Luteinizing hormone releasing hormone analogues may prove to be valuable new agents in the treatment of advanced prostatic cancer.

摘要

转移性前列腺癌通常通过去势或给予外源性雌激素进行治疗,这两种方法都有明显的临床缺点。促黄体激素释放激素类似物已被证明在动物和人类中可抑制性腺类固醇生成。为了评估一种强效促黄体激素释放激素类似物,即(D-亮氨酸-6)促黄体激素释放激素(1-9)九肽乙酰胺的给药效果,对9例未经治疗的D2期前列腺癌患者使用该药物治疗3至8个月。治疗3个月时,所有患者血清睾酮均显著降低,血清促黄体激素峰值及对该类似物急性给药的睾酮反应均降低,而基线血清促黄体激素或催乳素无变化。这些数据表明该类似物通过减少垂体促黄体激素的释放发挥作用。这种治疗方式未观察到重大不良反应,所有患者症状均有改善,且通过前列腺计算机断层扫描或超声检查、前列腺酸性磷酸酶和骨扫描测量,肿瘤活性降低或稳定。现介绍一个典型病例。促黄体激素释放激素类似物可能被证明是治疗晚期前列腺癌的有价值的新药。

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