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首页> 美国卫生研究院文献>British Journal of Cancer >Synergistic inhibition of prostate cancer cell lines by a 19- nor hexafluoride vitamin D3 analogue and anti-activator protein 1 retinoid
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Synergistic inhibition of prostate cancer cell lines by a 19- nor hexafluoride vitamin D3 analogue and anti-activator protein 1 retinoid

机译:19或六氟化物维生素D3类似物和抗激活剂蛋白1类维生素A对前列腺癌细胞系的协同抑制作用

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The secosteroid hormones, all- trans- and 9- cis -retinoic acid and vitamin D3, have demonstrated significant capacity to control proliferation in itro of many solid tumour cell lines. Cooperative synergistic effects by these two ligands have been reported, and it is, therefore, possible that greater therapeutic effects could be achieved if these compounds were administered together. The role of retinoid-dependent anti-activator protein 1 (anti-AP-1) effects in controlling cancer cell proliferation appears significant. We have utilized an anti- AP-1 retinoid [2-(4,4-dimethyl-3,4-dihydro-2H-1 benzopyran-6-yl)carbonyl-2-(4-carboxyphenyl)-1,3,-dithiane; SR11238], which does not transactivate through a retinoic acid response element (RARE), and a potent vitamin D3analogue [1α,25(OH)2-16-ene-23-yne-26,27-F6-19-nor -D3, code name LH] together at low, physiologically safer doses against a panel of prostate cancer cell lines that represent progressively more transformed phenotypes. The LNCaP (least transformed) and PC-3 (intermediately transformed) cell lines were synergistically inhibited in their clonal growth by the combination of LH and SR11238, whereas SR11238 alone was essentially inactive. DU-145 cells (most transformed) were completely insensitive to these analogues. LNCaP cells, but neither PC-3 nor DU-145, underwent apoptosis in the presence of LH and SR11238. Transactivation of the human osteocalcin vitamin D response element (VDRE) by LH was not enhanced in the presence of SR11238, although the expression of E-cadherin in these cells was additively up-regulated in the presence of both compounds. These data suggest the anti-AP-1 retinoid and the vitamin D3 analogue may naturally act synergistically to control cell proliferation, a process that is interrupted during transformation, and that this combination may form the basis for treatment of some androgen-independent prostate cancer. © 1999 Cancer Research Campaign
机译:甾醇类固醇激素,全反式和9-顺式视黄酸和维生素D3已显示出显着的能力来控制许多实体瘤细胞系中的增殖。已经报道了这两个配体的协同协同作用,因此,如果将这些化合物一起给药,则可能获得更大的治疗效果。类视黄醇依赖性抗激活蛋白1(抗AP-1)的作用在控制癌细胞增殖中的作用似乎很重要。我们已经利用了抗AP-1类视黄醇[2-(4,4-二甲基-3,4-二氢-2H-1苯并吡喃-6-基)羰基-2-(4-羧基苯基)-1,3,-双硫烷SR11238],不会通过视黄酸反应元件(RARE)进行反式激活,并且不会产生有效的维生素D3类似物[1α,25(OH)2-16-ene-23-yne-26,27-F6-19-nor -D3 ,代号LH],同时以低,生理上更安全的剂量对抗代表逐渐转化的更多表型的一组前列腺癌细胞系。 LHaP(最少转化的)和PC-3(中等转化的)细胞系通过LH和SR11238的组合被协同抑制了其克隆生长,而单独的SR11238则基本上没有活性。 DU-145细胞(转化最多的)对这些类似物完全不敏感。 LNCaP细胞(但PC-3和DU-145均不存在)在LH和SR11238的存在下发生凋亡。在SR11238的存在下,LH对人骨钙素维生素D反应元件(VDRE)的反式激活并未增强,尽管在两种化合物的存在下,这些细胞中E-钙粘蛋白的表达也被上调。这些数据表明,抗AP-1类视黄醇和维生素D3类似物可以自然地协同作用来控制细胞增殖,这一过程在转化过程中被中断,并且这种结合可能构成治疗某些雄激素非依赖性前列腺癌的基础。 ©1999癌症研究运动

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