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首页> 外文期刊>American Journal of Pathology >Brk Protects Breast Cancer Cells from Autophagic Cell Death Induced by Loss of Anchorage
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Brk Protects Breast Cancer Cells from Autophagic Cell Death Induced by Loss of Anchorage

机译:Brk保护乳腺癌细胞免受因失去锚固而导致的自噬细胞死亡

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摘要

Brk, a tyrosine kinase expressed in a majority of breast tumors, but not normal mammary tissue, promotes breast carcinoma cell proliferation. Normal epithelial cells are dependent on cell–cell or cell–matrix interactions for survival and undergo apoptosis after disruption of these interactions. Tumor cells are less sensitive to the induction of apoptosis and are predicted to have the potential to disseminate. We investigated whether Brk has further roles in breast tumor progression by relating its expression to tumor grade and demonstrating its role in the regulation of carcinoma cell survival under non-adherent conditions. Brk expression was determined by reverse transcription PCR on RNA extracted from surgical samples of human breast cancers. Breast carcinoma cell survival in suspension culture was examined when Brk protein levels were suppressed by RNA interference. Additionally, the effect of experimentally overexpressing Brk in otherwise Brk-negative breast carcinoma cells was assessed. Brk mRNA expression was notably higher in grade 3 breast tumors, as compared with lower tumor grades. In suspension culture, Brk suppression increased the rate of cell death, as compared with controls, and this cell death program exhibited characteristics of autophagy but not of apoptosis. Conversely, experimental expression of Brk in Brk-negative cells increased cell survival whereas kinase-inactive Brk did not. Therefore, Brk enhances breast carcinoma cell survival in suspension, suggesting a role for Brk in supporting breast cancer cell dissemination.
机译:Brk是一种在大多数乳腺肿瘤中表达的酪氨酸激酶, 而不是正常的乳腺组织,可促进乳腺癌细胞 的增殖。正常上皮细胞的存活取决于细胞-细胞 或细胞-基质的相互作用,并在破坏这些相互作用后发生凋亡 。肿瘤细胞对凋亡诱导的敏感性较低,并被预测具有传播的潜力。我们通过将Brk 的表达与肿瘤等级相关联并证明其在癌细胞存活的 调节中的作用来研究Brk 在乳腺肿瘤进展中是否还有其他作用。在非贴壁条件下,对人乳腺癌手术样本中提取的 RNA进行反转录PCR测定 Brk。 乳腺癌细胞的存活率当RNA干扰抑制Brk蛋白水平时,检查了悬浮培养物中的 。另外,实验性地过表达Brk 在否则为Brk阴性的乳房中的作用评估了癌细胞。 Brk mRNA在3级乳腺肿瘤中的表达明显高于 。在悬浮培养中, Brk抑制与对照相比 增加了细胞死亡的速率,并且该细胞死亡程序表现出自噬的特征 ,但没有凋亡。相反,Brk阴性细胞中Brk的实验性 表达增加了细胞存活率,而对激酶无活性的Brk则没有。因此,Brk增强了悬液中 乳腺癌细胞的存活率,表明Brk在支持乳腺癌细胞扩散中的作用。

著录项

  • 来源
    《American Journal of Pathology》 |2009年第3期|1226-1234|共9页
  • 作者单位

    From the Brunel Institute for Cancer Genetics and Pharmacogenomics,Biosciences, School of Health Sciences and Social Care, Brunel University, Uxbridge;

    the School of Biological Sciences,University of East Anglia, Norwich;

    the School of Biological Sciences,University of East Anglia, Norwich;

    From the Brunel Institute for Cancer Genetics and Pharmacogenomics,Biosciences, School of Health Sciences and Social Care, Brunel University, Uxbridge;

    the School of Biological Sciences,University of East Anglia, Norwich;

    the Cancer Research United Kingdom Centre for Cancer Therapeutics,McElwain Laboratories, the Institute of Cancer Research, Sutton;

    the Cancer Research United Kingdom Centre for Cancer Therapeutics,McElwain Laboratories, the Institute of Cancer Research, Sutton;

    and Academic Development Services,Royal Holloway, University of London, Egham, United Kingdom;

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