BACKGROUND:Clinical and experimental evidence suggest that estrogen has a role in the natural history of desmoid tumor (DT) and colorectal carcinoma.

METHODS:The biological effects of LY117018, a nonsteroidal antiestrogen benzothiophene derivative, were assessed on a human adenocarcinoma cell line (HCT8 cells), and on DT cells and colorectal cancer derived fibroblasts in primary culture.

RESULTS:LY117018 inhibited cell proliferation and collagen type I synthesis in DT cells. The compound also reduced cell growth in HCT8 cells and colorectal cancer fibroblasts. Binding experiments revealed the presence of estrogen binding sites in DT cells and frozen tissues but LY117018 did not displace [3H]17 beta E2 binding to DT cells.

CONCLUSIONS:Present results demonstrate that LY117018 inhibits epithelial and fibroblastic colon cancer cells proliferation and proliferation and differentiation of desmoid cells in vitro. The lack of displacement of [3H]17 beta E2 binding to desmoid cells by LY117018 suggests the existence of distinct LY117018 binding sites.

译文

背景 : 临床和实验证据表明,雌激素在结膜瘤 (DT) 和大肠癌的自然史中起作用。
方法 : 非甾体类抗雌激素苯并噻吩衍生物LY117018的生物学作用,在人腺癌细胞系 (HCT8细胞) 以及原代培养物中的DT细胞和大肠癌衍生的成纤维细胞上进行了评估。
结果 :LY117018抑制DT细胞中的细胞增殖和I型胶原合成。该化合物还降低了HCT8细胞和大肠癌成纤维细胞的细胞生长。结合实验表明,在DT细胞和冷冻组织中存在雌激素结合位点,但LY117018并未取代 [3H] 17βe2与DT细胞的结合。
结论 : 目前的结果表明,LY117018在体外抑制上皮和成纤维细胞结肠癌细胞的增殖以及结膜样细胞的增殖和分化。LY117018缺乏与结膜细胞结合的 [3H] 17βe2的位移,表明存在不同的LY117018结合位点。

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