Bontenbal M, Foekens J A, Lamberts S W, de Jong F H, van Putten W L, Braun H J, Burghouts J T, van der Linden G H, Klijn J G
Division of Endocrine Oncology (Department of Medical Oncology), Dr Daniel den Hoed Kliniek, Rotterdam, The Netherlands.
Br J Cancer. 1998;77(1):115-22. doi: 10.1038/bjc.1998.18.
Suppression of the secretion of prolactin, growth hormone and insulin-like growth factor 1 (IGF-1) might be important in the growth regulation and treatment of breast cancer. Because oestrogens may counteract the anti-tumour effects of such treatment, the combination of an anti-oestrogen (tamoxifen), a somatostatin analogue (octreotide) and a potent anti-prolactin (CV 205-502) might be attractive. In this respect, we performed a first exploratory long-term study on the feasibility of combined treatment and possible clear differences in endocrine and anti-tumour effects during such combined treatment vs standard treatment with tamoxifen alone. Twenty-two post-menopausal patients with metastatic breast cancer (ER and/or PR positive or unknown) were randomized to receive either 40 mg of tamoxifen per day or the combination of 40 mg of tamoxifen plus 75 microg of CV 205-502 orally plus 3 x 0.2 mg of octreotide s.c. as first-line endocrine therapy. An objective response was found in 36% of the patients treated with tamoxifen alone and in 55% of the patients treated with combination therapy. Median time to progression was 33 weeks for patients treated with tamoxifen and 84 weeks for patients treated with combination therapy, but the numbers are too small for hard conclusions. There was no difference in overall post-relapse survival between the two treatment arms. With respect to the endocrine parameters, there was a significant decrease of plasma IGF-1 levels in both treatment arms, whereas during combined treatment plasma growth hormone tended to decrease and plasma prolactin levels were strongly suppressed; in some patients insulin and transforming growth factor alpha (TGF-alpha) decreased during the triple therapy. Although there was no significant difference in mean decrease of plasma IGF-1 levels between the two treatment arms, combined treatment resulted in a more uniform suppression of IGF-1. Therefore, the addition of a somatostatin analogue and an anti-prolactin may potentially enhance the efficacy of anti-oestrogens in the treatment of breast cancer owing to favourable endocrine and possible direct anti-tumour effects. Large phase III trials using depot formulations (to increase the feasibility) of somatostatin analogues are warranted to demonstrate the potential extra beneficial anti-tumour effects of such combination therapy.
抑制催乳素、生长激素和胰岛素样生长因子1(IGF-1)的分泌可能在乳腺癌的生长调节和治疗中具有重要意义。由于雌激素可能会抵消此类治疗的抗肿瘤作用,抗雌激素(他莫昔芬)、生长抑素类似物(奥曲肽)和强效抗催乳素药物(CV 205-502)联合使用可能具有吸引力。在这方面,我们进行了一项初步探索性长期研究,以探讨联合治疗的可行性以及联合治疗与单独使用他莫昔芬的标准治疗相比,在内分泌和抗肿瘤效果方面可能存在的明显差异。22例绝经后转移性乳腺癌患者(雌激素受体和/或孕激素受体阳性或情况不明)被随机分为两组,一组每天接受40mg他莫昔芬治疗,另一组接受40mg他莫昔芬联合75μg CV 205-502口服加3×0.2mg奥曲肽皮下注射作为一线内分泌治疗。单独使用他莫昔芬治疗的患者中有36%出现客观缓解,联合治疗的患者中有55%出现客观缓解。单独使用他莫昔芬治疗的患者中位进展时间为33周,联合治疗的患者为84周,但由于样本量太小,难以得出确凿结论。两个治疗组的总体复发后生存率没有差异。在内分泌参数方面,两个治疗组的血浆IGF-1水平均显著下降,而在联合治疗期间,血浆生长激素趋于下降,血浆催乳素水平受到强烈抑制;在一些患者中,三联治疗期间胰岛素和转化生长因子α(TGF-α)下降。尽管两个治疗组血浆IGF-1水平的平均下降幅度没有显著差异,但联合治疗导致IGF-1的抑制更为均匀。因此,由于有利的内分泌作用和可能的直接抗肿瘤作用,添加生长抑素类似物和抗催乳素可能会增强抗雌激素在乳腺癌治疗中的疗效。有必要进行大型III期试验,使用生长抑素类似物的长效制剂(以提高可行性)来证明这种联合治疗潜在的额外有益抗肿瘤效果。
