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首页> 外文期刊>Journal of oncology >Modulation of ERQC and ERAD: A Broad-Spectrum Spanner in the Works of Cancer Cells?
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Modulation of ERQC and ERAD: A Broad-Spectrum Spanner in the Works of Cancer Cells?

机译:ERQC和ERAD的调制:癌细胞作品中的广谱扳手?

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摘要

Endoplasmic reticulum glycoprotein folding quality control (ERQC) and ER-associated degradation (ERAD) preside over cellular glycoprotein secretion and maintain steady glycoproteostasis. When cells turn malignant, cancer cell plasticity is affected and supported either by point mutations, preferential isoform selection, altered expression levels, or shifts to conformational equilibria of a secreted glycoprotein. Such changes are crucial in mediating altered extracellular signalling, metabolic behavior, and adhesion properties of cancer cells. It is therefore conceivable that interference with ERQC and/or ERAD can be used to selectively damage cancers. Indeed, inhibitors of the late stages of ERAD are already in the clinic against cancers such as multiple myeloma. Here, we review recent advances in our understanding of the complex relationship between glycoproteostasis and cancer biology and discuss the potential of ERQC and ERAD modulators for the selective targeting of cancer cell plasticity.
机译:内质网糖蛋白折叠质量控制(ERQC)和内质网相关降解(ERAD)控制细胞糖蛋白分泌并维持稳定的糖蛋白稳定。当细胞变为恶性时,癌细胞的可塑性受到点突变、优先异构体选择、表达水平改变或分泌糖蛋白构象平衡的影响和支持。这种变化在介导细胞外信号、代谢行为和癌细胞粘附特性的改变方面至关重要。因此,可以想象,对ERQC和/或ERAD的干扰可用于选择性地损害癌症。事实上,ERAD晚期抑制剂已经在临床上用于治疗多发性骨髓瘤等癌症。在这里,我们回顾了我们对糖蛋白稳态和癌症生物学之间复杂关系的理解的最新进展,并讨论了ERQC和ERAD调节剂在选择性靶向癌细胞可塑性方面的潜力。

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  • 来源
    《Journal of oncology 》 |2019年第4期| 共1页
  • 作者单位

    Univ Leicester Dept Mol &

    Cell Biol Leicester Inst Struct &

    Chem Biol Henry Wellcome Bldg;

    Univ Leicester Dept Mol &

    Cell Biol Leicester Inst Struct &

    Chem Biol Henry Wellcome Bldg;

    CNR Inst Sci Food Prod Unit Lecce Via Monteroni I-73100 Lecce Italy;

    Univ Leicester Dept Mol &

    Cell Biol Leicester Inst Struct &

    Chem Biol Henry Wellcome Bldg;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 肿瘤学 ;
  • 关键词

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