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雌激素受体α(ERα)和雌激素受体β(ERβ)的相互表达与雌激素介导的肠道肿瘤发生调节相关。

Reciprocal expression of ERalpha and ERbeta is associated with estrogen-mediated modulation of intestinal tumorigenesis.

作者信息

Weyant M J, Carothers A M, Mahmoud N N, Bradlow H L, Remotti H, Bilinski R T, Bertagnolli M M

机构信息

Department of Surgery and Pathology, Weill College of Medicine of Cornell University, New York, New York, USA.

出版信息

Cancer Res. 2001 Mar 15;61(6):2547-51.

Abstract

Menopausal hormone replacement therapy has been widely used to alleviate the symptoms of menopause and to decrease the detrimental effects of ovarian hormone loss on bone density and cardiovascular health. Multiple studies of colorectal cancer epidemiology also support a role for hormone replacement therapy in prevention of colorectal cancer. We studied the effect of ovariectomy and estrogen replacement on tumor formation in C57BL/6J-Min/+ (Min/+) mice, animals that bear a germline mutation in murine Apc. These mice develop multiple intestinal tumors that show loss of wild-type Apc protein. After ovariectomy, intestinal adenomas in Min/+ mice increased by 77% (P = 0.0004). Ovariectomized Min/+ mice that were treated with a replacement dose of 17beta-estradiol had the same number of tumors as Min/+ mice that were neither castrated nor treated with estrogen replacement (P = 0.85). Examination of estrogen receptor (ER) levels in intestinal tissue by immunoblot showed changes in relative expression levels of ERalpha and ERbeta, with highest ERalpha and lowest ERbeta expression in the normal-appearing intestine of Min/+ mice, and lowest ERalpha and highest ERbeta expression in the enterocytes of animals that received 17beta-estradiol. These results suggest that endogenous estrogens protect against Apc-associated tumor formation and that tumor prevention by 17beta-estradiol is associated with an increase in ERbeta and a decrease in ERalpha expression in the target tissue.

摘要

更年期激素替代疗法已被广泛用于缓解更年期症状,并减少卵巢激素丧失对骨密度和心血管健康的有害影响。多项结直肠癌流行病学研究也支持激素替代疗法在预防结直肠癌方面的作用。我们研究了卵巢切除和雌激素替代对C57BL/6J-Min/+(Min/+)小鼠肿瘤形成的影响,这些小鼠携带鼠源Apc基因的种系突变。这些小鼠会发展出多个肠道肿瘤,且野生型Apc蛋白缺失。卵巢切除后,Min/+小鼠的肠道腺瘤增加了77%(P = 0.0004)。接受17β-雌二醇替代剂量治疗的去卵巢Min/+小鼠的肿瘤数量与未阉割且未接受雌激素替代治疗的Min/+小鼠相同(P = 0.85)。通过免疫印迹检测肠道组织中的雌激素受体(ER)水平,结果显示ERα和ERβ的相对表达水平发生了变化,在Min/+小鼠外观正常的肠道中ERα表达最高而ERβ表达最低,在接受17β-雌二醇的动物的肠细胞中ERα表达最低而ERβ表达最高。这些结果表明内源性雌激素可预防与Apc相关的肿瘤形成,并且17β-雌二醇的肿瘤预防作用与靶组织中ERβ增加和ERα表达减少有关。

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