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胃癌:鉴定抑制可成药靶点的 microRNAs 和介导临床前模型疗效的 microRNAs。

Gastric Cancer: Identification of microRNAs Inhibiting Druggable Targets and Mediating Efficacy in Preclinical Models.

机构信息

Large Molecule Research, Roche Pharma Research and Early Development (pRED), Roche Innovation Center Munich, Penzberg, Germany;

Pharmaceutical Sciences, Roche Pharma Research and Early Development (pRed), Roche Innovation Center Basel, Basel, Switzerland.

出版信息

Cancer Genomics Proteomics. 2021 Jul-Aug;18(4):497-514. doi: 10.21873/cgp.20275.

Abstract

In addition to chemotherapy, targeted therapies have been approved for treatment of locally advanced and metastatic gastric cancer. The therapeutic benefit is significant but more durable responses and improvement of survival should be achieved. Therefore, the identification of new targets and new approaches for clinical treatment are of paramount importance. In this review, we searched the literature for down-regulated microRNAs which interfere with druggable targets and exhibit efficacy in preclinical in vivo efficacy models. As druggable targets, we selected transmembrane receptors, secreted factors and enzymes. We identified 38 microRNAs corresponding to the criteria as outlined. A total of 13 miRs target transmembrane receptors, nine inhibit secreted proteins and 16 attenuate enzymes. These microRNAs are targets for reconstitution therapy of gastric cancer. Further target validation experiments are mandatory for all of the identified microRNAs.

摘要

除了化疗,靶向治疗已被批准用于治疗局部晚期和转移性胃癌。治疗效果显著,但应实现更持久的反应和生存改善。因此,确定新的靶点和新的临床治疗方法至关重要。在这篇综述中,我们搜索了文献中干扰可药物治疗靶点并在临床前体内疗效模型中显示疗效的下调 microRNAs。作为可药物治疗靶点,我们选择了跨膜受体、分泌因子和酶。我们确定了 38 个符合上述标准的 microRNAs。共有 13 个 miR 靶向跨膜受体,9 个抑制分泌蛋白,16 个减弱酶。这些 microRNAs 是胃癌再构成治疗的靶点。所有鉴定的 microRNAs 都需要进行进一步的靶标验证实验。

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