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首页> 外文期刊>Journal of Cancer Research and Clinical Oncology >DC-CLM, a cadherin-like molecule cloned from human dendritic cells, inhibits growth of breast cancer cells.
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DC-CLM, a cadherin-like molecule cloned from human dendritic cells, inhibits growth of breast cancer cells.

机译:DC-CLM是从人树突状细胞中克隆的一种钙粘蛋白样分子,可抑制乳腺癌细胞的生长。

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PURPOSE. To identify the characteristics and function of a cadherin-like molecule, cloned from a human dendritic cell (DC) cDNA library and designated DC-derived cadherin-like molecule (DC-CLM). METHODS. The mRNA expression of DC-CLM in tissues and cells was analyzed by Northern blot and RT-PCR, respectively. In order to express DC-CLM in target cells, we constructed a pcDNA3.1/DC-CLM expression vector and transfected it into MCF-7 human breast cancer cells. Tumor growth was demonstrated by cell proliferation and colony formation. RESULTS. DC-CLM cDNA encoded a protein of 260 amino acids and the gene was localized to chromosome 5q31. The predicted protein possessed a definitive cadherin-specific sequence motif and shared homology with classical cadherin. However, no transmembrane segment was observed in DC-CLM. Northern blot revealed the ubiquitous nature of DC-CLM transcripts in human tissues, with high expression in heart, brain, prostate, testis and ovary. RT-PCR demonstrated that DC-CLM was widely expressed in hematopoietic and epithelial tumor cell lines, but was not expressed in MCF-7. Interestingly, DC-CLM expression was upregulated in DC activated by lipopolysaccharides. DC-CLM expression in the stable transfectant (MCF-7/DC-CLM) was confirmed by RT-PCR and Western blot. DC-CLM protein was found to be secreted by MCF-7/DC-CLM but not expressed on the membrane of MCF-7/DC-CLM. DC-CLM transfection resulted in significant inhibition of in vitro growth and colony formation of MCF-7 cells. CONCLUSIONS. A cadherin-like molecule DC-CLM was cloned from human DC and it may be a soluble cadherin-like molecule for tumor suppression. DC-CLM was upregulated in activated DC and may be involved in the effector function of activated DC.
机译:目的。为了鉴定类钙粘蛋白样分子的特征和功能,从人树突状细胞(DC)cDNA库中克隆并命名为DC衍生的钙粘蛋白样分子(DC-CLM)。方法。分别通过Northern印迹和RT-PCR分析DC-CLM在组织和细胞中的mRNA表达。为了在靶细胞中表达DC-CLM,我们构建了一个pcDNA3.1 / DC-CLM表达载体,并将其转染到MCF-7人乳腺癌细胞中。细胞增殖和集落形成证明了肿瘤的生长。结果。 DC-CLM cDNA编码一个260个氨基酸的蛋白质,该基因定位在5q31染色体上。预测的蛋白质具有确定的钙粘着蛋白特异性序列基序,并且与经典钙粘着蛋白具有同源性。然而,在DC-CLM中未观察到跨膜片段。 Northern印迹揭示了DC-CLM转录本在人组织中的普遍存在,在心脏,大脑,前列腺,睾丸和卵巢中高表达。 RT-PCR显示DC-CLM在造血和上皮肿瘤细胞系中广泛表达,但在MCF-7中不表达。有趣的是,DC-CLM表达在脂多糖激活的DC中上调。通过RT-PCR和Western印迹证实了稳定转染子(MCF-7 / DC-CLM)中的DC-CLM表达。发现DC-CLM蛋白由MCF-7 / DC-CLM分泌,但未在MCF-7 / DC-CLM的膜上表达。 DC-CLM转染可显着抑制MCF-7细胞的体外生长和集落形成。结论。从人DC中克隆了钙粘蛋白样分子DC-CLM,它可能是一种可溶的钙粘蛋白样分子,用于抑制肿瘤。 DC-CLM在激活的DC中上调,可能与激活的DC的效应子功能有关。

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