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用于鉴定癌症新型治疗靶标的细胞表面蛋白质组学。

Cell-surface proteomics for the identification of novel therapeutic targets in cancer.

机构信息

a Princess Margaret Cancer Centre , University Health Network , Toronto , Canada.

b The Centre for Drug Research and Development, Division of Biologics , Vancouver , Canada.

出版信息

Expert Rev Proteomics. 2018 Mar;15(3):259-275. doi: 10.1080/14789450.2018.1429924. Epub 2018 Jan 23.

Abstract

Cancer is the second most common cause of death worldwide and its heterogeneity complicates therapy. Standard cytotoxic regiments disrupt rapidly dividing cells, regardless of their neoplastic status. The introduction of less toxic targeted therapies has partially contributed to the observed decrease in cancer-related mortality. Cell-surface proteins represent attractive targets for therapy, due to their easily-accessible localization and their involvement in essential signaling pathways, often dysregulated in cancer. Despite their clinical appeal, cell-surface proteins are often underrepresented in standard proteomic data sets, due to their poor solubility and lower expression levels compared to intracellular proteins. Areas covered: This review will summarize some of the available techniques for enriching the cell-surface proteome, and discuss their advantages, limitations and applicability to clinical sample-testing. Moreover, we discuss currently available strategies for the development of novel targeted therapies in cancer. Expert commentary: The interest in elucidating the cancer-associated surfaceome is growing and will likely benefit from recent advancements in instrument sensitivity, method development, and a growing body of high-quality proteomics databases. Multiomics studies, in combination with functional validations (e.g. dropout screens), and evaluation of the healthy surfaceome, will likely aid in the selection of relevant targets for future therapy development.

摘要

癌症是全球第二大常见死因,其异质性使治疗复杂化。标准细胞毒性方案会破坏快速分裂的细胞,而不管其肿瘤状态如何。毒性较低的靶向治疗的引入部分促成了癌症相关死亡率的下降。细胞表面蛋白因其易于接近的定位及其参与经常失调的癌症中的重要信号通路而成为有吸引力的治疗靶点。尽管具有临床吸引力,但与细胞内蛋白相比,细胞表面蛋白在标准蛋白质组学数据集通常代表性不足,因为它们的溶解度较差且表达水平较低。

涵盖领域

这篇综述将总结一些用于富集细胞表面蛋白质组的现有技术,并讨论它们的优点、局限性以及对临床样本测试的适用性。此外,我们还讨论了目前用于开发癌症新型靶向疗法的策略。

专家评论

阐明与癌症相关的表面组学的兴趣正在增长,并且可能受益于仪器灵敏度、方法开发方面的最新进展,以及越来越多的高质量蛋白质组学数据库。多组学研究,结合功能验证(例如缺失筛选)和健康表面组学的评估,可能有助于为未来的治疗开发选择相关靶点。

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