P38

Q3 Medicine Ejc Supplements Pub Date : 2015-11-01 DOI:10.1016/j.ejcsup.2015.08.087
S. Semina, M. Krasil’nikov
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引用次数: 0

Abstract

The efficiency of endocrine therapy for tumors is limited by the development of hormone resistance and progression of tumor cells to hormone-independent phenotype. Among these tumors – breast cancers, for which hormone therapy is one of the most common and effective methods of treatment, but only in cases, when the tumors retain their hormonal dependence. The mechanism of hormonal independence was found to be based on the fundamental properties of cancer cell including both downregulation of specific hormone receptors, and affecting of intracellular signalling, particularly – estrogen-independent growth signaling pathways. However, the role of the intercellular interactions in the progression of hormonal resistance is still unclear.

We hypothesize, that the formation of the clone of the hormone-resistant cells in the tumor, and the subsequent common growth of the hormone-resistant and sensitive cells may lead to spread the hormonal resistance to the sensitive cells – as a result of the secretion of the specific factors acting in the paracrine manner or via the direct cell–cell contacts. Here, using the estrogen-dependent breast cancer cells MCF-7 and the resistant subline MCF-7/T developed by long-term cultivation of MCF-7 cells in the presence of antiestrogen tamoxifen, we investigated the possible changes in the hormonal sensitivity of these cells caused by the co-cultivation in vitro. For this purpose MCF-7/T cells were transfected with the plasmid containing the gene of the green fluorescent protein (GFP), and GFP-positive hormone-resistant subline MCF-7/T/GFP+ was developed. The GFP expression should allow to distinguish the resistant and parental cells during co-cultivation.

To study the influence of the co-cultivation on the cell sensitivity to tamoxifen the parent MCF-7 cells (GFP-negative) were co-cultivate with the resistant MCF-7/T/GFP+/cells for 10 days, then the cells were treated with tamoxifen and the efficiency of growth inhibitory tamoxifen action was determined. We found, that the co -cultivation of the parent and resistant cells lead to increase in the resistance of the parent cell to tamoxifen, indicating the important role of the contacts, direct or indirect, between hormone sensitive and resistant cells in the development of hormone resistance.

In general, we evaluate the established results as the first evidence of the possible involvement of the cell–cell underrelations in the realization of the hormonal response, and suppose that the next investigations will give a new insights in the molecular mechanisms of this effects and its role in the formation of the hormone-resistant phenotype of the tumors.

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P38
肿瘤的内分泌治疗效率受到激素抵抗的发展和肿瘤细胞向激素不依赖型发展的限制。在这些肿瘤中——乳腺癌,激素治疗是最常见和最有效的治疗方法之一,但只有在肿瘤保持对激素依赖的情况下。激素独立的机制被发现是基于癌细胞的基本特性,包括特异性激素受体的下调和细胞内信号传导的影响,特别是不依赖雌激素的生长信号通路。然而,细胞间相互作用在激素抵抗过程中的作用仍不清楚。我们推测,肿瘤中激素抵抗细胞克隆的形成,以及随后激素抵抗细胞和敏感细胞的共同生长可能导致激素抵抗向敏感细胞扩散,这是由于特定因子以旁分泌方式或通过直接细胞-细胞接触分泌的结果。本研究利用雌激素依赖性乳腺癌细胞MCF-7和MCF-7细胞在抗雌激素的他莫昔芬存在下长期培养而形成的耐药亚群MCF-7/T,在体外研究共同培养对这些细胞激素敏感性可能产生的变化。为此,用含有绿色荧光蛋白(GFP)基因的质粒转染MCF-7/T细胞,形成了绿色荧光蛋白阳性的激素抗性亚群MCF-7/T/GFP+。在共培养过程中,GFP的表达应该能够区分抗性细胞和亲本细胞。为了研究共培养对细胞对他莫昔芬敏感性的影响,将GFP阴性的MCF-7亲本细胞与耐药的MCF-7/T/GFP+/细胞共培养10 d,然后用他莫昔芬处理细胞,测定他莫昔芬抑制生长的效果。我们发现,亲本和抗性细胞的共同培养导致亲本细胞对他莫昔芬的抗性增加,这表明激素敏感细胞和抗性细胞之间的直接或间接接触在激素抗性的发展中起着重要作用。总的来说,我们将现有的结果评价为可能参与激素反应实现的细胞-细胞欠关系的第一个证据,并假设下一步的研究将在这种作用的分子机制及其在肿瘤激素抗性表型形成中的作用方面提供新的见解。
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来源期刊
Ejc Supplements
Ejc Supplements 医学-肿瘤学
自引率
0.00%
发文量
0
审稿时长
3.7 months
期刊介绍: EJC Supplements is an open access companion journal to the European Journal of Cancer. As an open access journal, all published articles are subject to an Article Publication Fee. Immediately upon publication, all articles in EJC Supplements are made openly available through the journal''s websites. EJC Supplements will consider for publication the proceedings of scientific symposia, commissioned thematic issues, and collections of invited articles on preclinical and basic cancer research, translational oncology, clinical oncology and cancer epidemiology and prevention. Authors considering the publication of a supplement in EJC Supplements are requested to contact the Editorial Office of the EJC to discuss their proposal with the Editor-in-Chief. EJC Supplements is an official journal of the European Organisation for Research and Treatment of Cancer (EORTC), the European CanCer Organisation (ECCO) and the European Society of Mastology (EUSOMA).
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