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随着衰老,大鼠的松果体褪黑素水平和 MT1 受体表达降低,与乳腺癌生长加速及对褪黑素的敏感性降低有关。

Declining melatonin levels and MT1 receptor expression in aging rats is associated with enhanced mammary tumor growth and decreased sensitivity to melatonin.

机构信息

Department of Structural and Cellular Biology, Tulane University School of Medicine, 1430 Tulane Ave, SL-49, New Orleans, LA 70112, USA.

出版信息

Breast Cancer Res Treat. 2011 May;127(1):91-8. doi: 10.1007/s10549-010-0958-0. Epub 2010 Jun 12.

DOI:10.1007/s10549-010-0958-0
PMID:20549340
Abstract

Serum melatonin (MLT) levels have been reported to diminish significantly by the 5th and 6th decades of life as the incidence of breast cancer increases. Given MLT's anti-cancer activity, we hypothesize that age-related decline in pineal MLT production leads to enhanced breast cancer development and growth as women age. In this study, we sought to determine whether the growth of tissue-isolated mammary tumors in young, adult, and old female Buffalo rats relates to the age-related changes in MLT and its MT1 receptor. Significant decreases in the peak nighttime serum MLT levels were observed in old as compared to adult and young rats. Significantly diminished nighttime and early morning levels of MT1-melatonin receptors were observed in uteri from old rats compared to adult and young rats. Growth rates in transplanted, tissue-isolated, carcinogen-induced mammary tumors are significantly increased in old rats as compared to adult or young rats. The growth-suppressive actions of exogenous MLT are diminished in old rats compared to adult and young rats. This decrease in tumor response correlates with reduced expression of the MT1 receptor in old as compared to young and adult rats. Thus, enhanced mammary tumor growth is associated with old age and diminished levels of MLT and MT1 receptor during old age, resulting in reduced sensitivity to exogenous MLT. Finally, our studies demonstrate that the tissue-isolated tumor model is viable model system in which to study the role of aging on breast cancer growth.

摘要

血清褪黑素 (MLT) 水平随着乳腺癌发病率的增加,在生命的第 5 和第 6 个十年中显著下降。鉴于 MLT 的抗癌活性,我们假设松果体 MLT 产生的年龄相关性下降导致女性年龄增长时乳腺癌的发展和生长增强。在这项研究中,我们试图确定年轻、成年和老年雌性布法罗大鼠组织分离的乳腺肿瘤的生长是否与 MLT 及其 MT1 受体的年龄相关变化有关。与成年和年轻大鼠相比,老年大鼠的夜间血清 MLT 水平峰值显著降低。与成年和年轻大鼠相比,老年大鼠子宫中夜间和清晨 MT1-褪黑素受体的水平明显降低。与成年或年轻大鼠相比,移植的、组织分离的、致癌物诱导的乳腺肿瘤的生长速度在老年大鼠中显著增加。与成年和年轻大鼠相比,外源 MLT 的生长抑制作用在老年大鼠中减弱。这种肿瘤反应的降低与 MT1 受体在老年大鼠中的表达减少相关,与年轻和成年大鼠相比。因此,增强的乳腺肿瘤生长与衰老以及衰老过程中 MLT 和 MT1 受体水平降低有关,导致对外源 MLT 的敏感性降低。最后,我们的研究表明,组织分离的肿瘤模型是一种可行的模型系统,可用于研究衰老对乳腺癌生长的作用。

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