Wu Kendall, Kim Hee-Tae, Rodriquez Jenny L, Hilsenbeck Susan G, Mohsin Syed K, Xu Xiao-Chun, Lamph William W, Kuhn John G, Green Jeff E, Brown Powel H
Breast Center, Department of Medicine, Baylor College of Medicine, Houston, Texas 77030, USA.
Cancer Epidemiol Biomarkers Prev. 2002 May;11(5):467-74.
Retinoids have been used in the clinic for the prevention and treatment of human cancers. They regulate several cellular processes including growth, differentiation, and apoptosis. Previously, we demonstrated that a pan-agonist retinoid 9-cis retinoic acid was able to suppress mammary tumorigenesis in the C3(1)-SV40 T-antigen (Tag) transgenic mouse model. However, significant toxicity was seen with this naturally occurring retinoid. We hypothesized that the cancer preventive effects of retinoids could be dissected from the toxic effects by using receptor-selective retinoids. In this study, we used TTNPB, an retinoic acid receptor-selective retinoid, and LGD1069, an retinoid X receptor-selective retinoid, to preferentially activate retinoic acid receptors and retinoid X receptors. In vitro, both compounds were able to inhibit the growth of T47D breast cancer cells. We then determined whether these retinoids prevented mammary tumorigenesis. C3(1)-SV40 Tag mice were treated daily by gastric gavage with vehicle, two different doses of TTNPB (0.3 or 3.0 microg/kg), or two different doses of LGD1069 (10 or 100 mg/kg). Mice were treated from approximately 6-8 weeks to 7-8 months of age. Tumor size and number were measured twice each week, and toxicities were recorded daily. Our data show that LGD1069 suppresses mammary tumorigenesis in C3(1)-SV40 Tag transgenic mice with no observable toxicity, whereas TTNPB had a modest chemopreventive effect, yet was very toxic. Median time to tumor development was 129 days in vehicle-treated mice versus 156 days in mice treated with 100 mg/kg LGD1069 (P = 0.05). In addition, tumor multiplicity was reduced by approximately 50% in mice treated with LGD1069 (2.9 for vehicle, 2.4 for 10 mg/kg LGD1069, and 1.4 for 100 mg/kg, P < or = 0.03). TTNPB-treated mice showed a delayed median time to tumor development (131 days for vehicle versus 154 days for 3.0 microg/kg TTNPB; P < or = 0.05), but no changes were seen in tumor multiplicity. However, toxicity (skin erythema, hair loss) was seen in all of the mice treated with TTNPB. These data demonstrate that receptor-selective retinoids suppress mammary tumorigenesis in transgenic mice and that preventive effects of retinoids can be separated from their toxicity, demonstrating that receptor-selective retinoids are promising agents for the prevention of breast cancer.
维甲酸已在临床上用于预防和治疗人类癌症。它们调节包括生长、分化和凋亡在内的多个细胞过程。此前,我们证明了一种泛激动剂维甲酸9-顺式维甲酸能够在C3(1)-SV40 T-抗原(Tag)转基因小鼠模型中抑制乳腺肿瘤发生。然而,这种天然存在的维甲酸具有明显的毒性。我们推测,通过使用受体选择性维甲酸,可以将维甲酸的癌症预防作用与毒性作用区分开来。在本研究中,我们使用了一种视黄酸受体选择性维甲酸TTNPB和一种视黄酸X受体选择性维甲酸LGD1069,以优先激活视黄酸受体和视黄酸X受体。在体外,这两种化合物都能够抑制T47D乳腺癌细胞的生长。然后,我们确定这些维甲酸是否能预防乳腺肿瘤发生。通过胃管给C3(1)-SV40 Tag小鼠每日灌胃给予溶剂、两种不同剂量的TTNPB(0.3或3.0微克/千克)或两种不同剂量的LGD1069(10或100毫克/千克)。小鼠从大约6 - 8周龄治疗至7 - 8月龄。每周测量两次肿瘤大小和数量,每天记录毒性情况。我们的数据表明,LGD1069可抑制C3(1)-SV40 Tag转基因小鼠的乳腺肿瘤发生,且无明显毒性,而TTNPB具有适度的化学预防作用,但毒性很大。溶剂处理组小鼠肿瘤发生的中位时间为129天,而接受100毫克/千克LGD1069治疗的小鼠为156天(P = 0.05)。此外,接受LGD1069治疗的小鼠肿瘤多发性降低了约50%(溶剂组为2.9,10毫克/千克LGD1069组为2.4,100毫克/千克组为1.4,P≤0.03)。接受TTNPB治疗的小鼠肿瘤发生的中位时间延迟(溶剂组为131天,3.0微克/千克TTNPB组为154天;P≤0.05),但肿瘤多发性未见变化。然而,所有接受TTNPB治疗的小鼠均出现了毒性(皮肤红斑、脱发)。这些数据表明,受体选择性维甲酸可抑制转基因小鼠的乳腺肿瘤发生,且维甲酸的预防作用可与其毒性相分离,这表明受体选择性维甲酸是预防乳腺癌很有前景的药物。
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