Crabtree Judy S, Peano Bryan J, Zhang Xiaochun, Komm Barry S, Winneker Richard C, Harris Heather A
Endocrinology & Reproductive Disorders Division, Women's Health and Musculoskeletal Biology, Wyeth Research, Collegeville, PA 19426, USA.
Mol Cell Endocrinol. 2008 Jun 11;287(1-2):40-6. doi: 10.1016/j.mce.2008.01.027. Epub 2008 Feb 12.
Selective estrogen receptor modulators (SERMs) have the unique potential to provide estrogenic effects in the skeletal and cardiovascular system, while minimizing/eliminating side effects on reproductive organs. However, despite the unifying characteristic of mixed estrogen receptor (ER) agonist/antagonist activity, compounds within this class are not interchangeable. In order to define and compare the effects of SERMs on different hormone-responsive tissues, we evaluated effects of bazedoxifene acetate (BZA), lasofoxifene (LAS) and raloxifene (RAL) in the mammary gland and uterus of the ovariectomized mouse. Endpoints measured included those regulated by estradiol alone (uterine wet weight, uterine G protein-coupled receptor 105 (GPR105) mRNA expression and mammary gland indoleamine-pyrrole 2,3 dioxygenase (INDO) mRNA expression) as well as others that required the combination of estradiol and progesterone (uterine serine protease inhibitor Kazal type 3 (Spink3) mRNA expression, mammary gland morphology and mammary gland defensin beta1 (Defbeta1) mRNA expression). The three SERMs tested had variable agonist and antagonist activity on these endpoints. In the uterus, the SERMs were mixed agonists/antagonists on estradiol-induced wet weight increase, whereas all three SERMs were estrogen receptor antagonists on GPR105 mRNA expression. However, in the presence of progesterone, BZA and RAL were agonists on Spink3 expression, while LAS was primarily an antagonist. In the mammary gland, BZA and RAL were predominantly agonists on the endpoint of mammary morphology and all three SERMs were clear agonists on Defbeta1 mRNA expression, an E+P-dependent marker. Finally, LAS and RAL had mixed agonist/antagonist activity on INDO mRNA expression, while BZA had only antagonist activity. These results demonstrate that compounds with small structural differences can elicit distinct biological responses, and that in general, SERMs tended to behave more as antagonists on endpoints requiring estrogen alone and agonists on endpoints requiring the combination of estrogen and progesterone.
选择性雌激素受体调节剂(SERMs)具有独特的潜力,可在骨骼和心血管系统中发挥雌激素样作用,同时将对生殖器官的副作用降至最低/消除。然而,尽管这类化合物具有混合雌激素受体(ER)激动剂/拮抗剂活性这一统一特征,但该类别中的化合物并非可相互替代。为了定义和比较SERMs对不同激素反应性组织的影响,我们评估了醋酸巴多昔芬(BZA)、拉索昔芬(LAS)和雷洛昔芬(RAL)对去卵巢小鼠乳腺和子宫的影响。所测量的终点包括仅由雌二醇调节的指标(子宫湿重、子宫G蛋白偶联受体105(GPR105)mRNA表达和乳腺吲哚胺-吡咯2,3-双加氧酶(INDO)mRNA表达)以及其他需要雌二醇和孕酮共同作用的指标(子宫丝氨酸蛋白酶抑制剂Kazal型3(Spink3)mRNA表达、乳腺形态和乳腺防御素β1(Defbeta1)mRNA表达)。所测试的三种SERMs在这些终点上具有不同的激动剂和拮抗剂活性。在子宫中,SERMs对雌二醇诱导的湿重增加表现为混合激动剂/拮抗剂,而所有三种SERMs对GPR105 mRNA表达均为雌激素受体拮抗剂。然而,在孕酮存在的情况下,BZA和RAL对Spink3表达为激动剂,而LAS主要为拮抗剂。在乳腺中, BZA和RAL在乳腺形态终点上主要为激动剂,并且所有三种SERMs在Defbeta1 mRNA表达上均为明显的激动剂,Defbeta1 mRNA表达是一种依赖雌二醇和孕酮的标志物。最后,LAS和RAL在INDO mRNA表达上具有混合激动剂/拮抗剂活性,而BZA仅具有拮抗剂活性。这些结果表明,结构差异较小的化合物可引发不同的生物学反应,并且一般而言,SERMs在仅需要雌激素的终点上倾向于表现为拮抗剂,而在需要雌激素和孕酮共同作用的终点上表现为激动剂。
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