Luque Raúl M, Villa-Osaba Alicia, L-López Fernando, Pozo-Salas Ana I, Sánchez-Sánchez Rafael, Ortega-Salas Rosa, de Lecea Luis, Álvarez-Benito Marina, López-Miranda José, Gahete Manuel D, Castaño Justo P
Department of Cell Biology, Physiology, and Immunology, University of Córdoba, Reina Sofía University Hospital, Maimonides Biomedical Research Institute of Córdoba (IMIBIC), Córdoba, Spain.
CIBER Fisiopatología de la Obesidad y Nutrición (CIBERobn), Córdoba, Spain.
Breast Cancer Res. 2016 Mar 8;18(1):29. doi: 10.1186/s13058-016-0689-1.
Somatostatin (SST) and cortistatin (CORT), two structurally and functionally related peptides, share a family of widespread receptors (sst1-5) to exert apparently similar biological actions, including endocrine/metabolic regulation and suppression of tumor cell proliferation. However, despite their therapeutic potential, attempts to apply SST-analogs to treat breast cancer have yielded unsatisfactory results. Actually, the specific roles of SST and CORT in mammary gland tumorigenesis (MGT), particularly in relation to metabolic dysregulation (i.e. obesity), remain unknown.
The role of endogenous SST and CORT in carcinogen-induced MGT was investigated under normal (lean) and obesity conditions. To that end, SST- and CORT-knockout (KO) mice and their respective littermate-controls, fed low-fat (LF) or high-fat (HF) diets, were treated with 7,12-dimethyl-benza-anthracene (DMBA) once a week (wk) for 3 wk, and MGT was monitored for 25 wk. Additionally, we examined the effect of SST or CORT removal in the development of the mammary gland.
Lack of SST did not alter DMBA-induced MGT incidence under lean conditions; conversely, lack of endogenous CORT severely aggravated DMBA-induced MGT in LF-fed mice. These differences were not attributable to altered mammary gland development. HF-diet modestly increased the sensitivity to DMBA-induced carcinogenesis in control mice, whereas, as observed in LF-fed CORT-KO, HF-fed CORT-KO mice exhibited aggravated tumor incidence, discarding a major influence of obesity on these CORT actions. In marked contrast, HF-fed SST-KO mice exhibited much higher tumor incidence than LF-fed SST-KO mice, which could be associated with higher mammary complexity.
Endogenous SST and CORT distinctly impact on DMBA-induced MGT, in a manner that is strongly dependent on the metabolic/endocrine milieu (lean vs. obese status). Importantly, CORT, rather than SST, could represent a major inhibitor of MGT under normal/lean-conditions, whereas both neuropeptides would similarly influence MGT under obesity conditions. The mechanisms mediating these different effects likely involve mammary development and hormones, but the precise underlying factors are still to be fully elucidated. However, our findings comprise suggestive evidence that CORT-like molecules, rather than classic SST-analogs, may help to identify novel tools for the medical treatment of breast cancer.
生长抑素(SST)和可体松(CORT)是两种在结构和功能上相关的肽,它们共有一族广泛分布的受体(sst1 - 5),以发挥明显相似的生物学作用,包括内分泌/代谢调节和抑制肿瘤细胞增殖。然而,尽管它们具有治疗潜力,但尝试应用SST类似物治疗乳腺癌的结果并不理想。实际上,SST和CORT在乳腺肿瘤发生(MGT)中的具体作用,特别是与代谢失调(即肥胖)相关的作用,仍然未知。
研究了内源性SST和CORT在正常(瘦)和肥胖条件下致癌物诱导的MGT中的作用。为此,将SST和CORT基因敲除(KO)小鼠及其各自的同窝对照小鼠,分别喂食低脂(LF)或高脂(HF)饮食,每周一次用7,12 - 二甲基苯并蒽(DMBA)处理3周,并监测MGT 25周。此外,我们研究了去除SST或CORT对乳腺发育的影响。
在瘦的条件下,缺乏SST不会改变DMBA诱导的MGT发生率;相反,缺乏内源性CORT会严重加重低脂饮食喂养的小鼠中DMBA诱导的MGT。这些差异并非归因于乳腺发育的改变。高脂饮食适度增加了对照小鼠对DMBA诱导的致癌作用的敏感性,而正如在低脂饮食喂养的CORT - KO小鼠中观察到的那样,高脂饮食喂养的CORT - KO小鼠表现出更高的肿瘤发生率,排除了肥胖对这些CORT作用的主要影响。与之形成鲜明对比的是,高脂饮食喂养的SST - KO小鼠比低脂饮食喂养的SST - KO小鼠表现出更高的肿瘤发生率,这可能与更高的乳腺复杂性有关。
内源性SST和CORT对DMBA诱导的MGT有明显影响,其方式强烈依赖于代谢/内分泌环境(瘦与肥胖状态)。重要的是,在正常/瘦的条件下,CORT而非SST可能是MGT的主要抑制剂,而在肥胖条件下,这两种神经肽对MGT的影响相似。介导这些不同作用的机制可能涉及乳腺发育和激素,但确切的潜在因素仍有待充分阐明。然而,我们的研究结果提供了提示性证据,即类似CORT的分子而非经典的SST类似物,可能有助于确定乳腺癌医学治疗的新工具。
Zotero 插件
