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基于紫杉醇反应的合成细胞毒性相互作用的计算推断。

In Silico Inference of Synthetic Cytotoxic Interactions from Paclitaxel Responses.

机构信息

Seoul National University Biomedical Informatics (SNUBI), Division of Biomedical Informatics, Seoul National University College of Medicine, Seoul 110799, Korea.

Asan Medical Center, University of Ulsan College of Medicine, Seoul 05505, Korea.

出版信息

Int J Mol Sci. 2021 Jan 22;22(3):1097. doi: 10.3390/ijms22031097.

Abstract

To exploit negatively interacting pairs of cancer somatic mutations in chemotherapy responses or synthetic cytotoxicity (SC), we systematically determined mutational pairs that had significantly lower paclitaxel half maximal inhibitory concentration (IC) values. We evaluated 407 cell lines with somatic mutation profiles and estimated their copy number and drug-inhibitory concentrations in Genomics of Drug Sensitivity in Cancer (GDSC) database. The SC effect of 142 mutated gene pairs on response to paclitaxel was successfully cross-validated using human cancer datasets for urogenital cancers available in The Cancer Genome Atlas (TCGA) database. We further analyzed the cumulative effect of increasing SC pair numbers on the TP53 tumor suppressor gene. Patients with TCGA bladder and urogenital cancer exhibited improved cancer survival rates as the number of disrupted SC partners (i.e., SYNE2, SON, and/or PRY) of TP53 increased. The prognostic effect of SC burden on response to paclitaxel treatment could be differentiated from response to other cytotoxic drugs. Thus, the concept of pairwise SC may aid the identification of novel therapeutic and prognostic targets.

摘要

为了利用癌症体细胞突变在化疗反应或合成细胞毒性 (SC) 中的负相互作用对,我们系统地确定了具有显著降低紫杉醇半数最大抑制浓度 (IC) 值的突变对。我们评估了具有体细胞突变谱的 407 个细胞系,并在癌症药物敏感性基因组学 (GDSC) 数据库中估计了它们的拷贝数和药物抑制浓度。使用在癌症基因组图谱 (TCGA) 数据库中可获得的泌尿生殖系统癌症人类癌症数据集,成功地对 142 个突变基因对与紫杉醇反应的 SC 效应进行了交叉验证。我们进一步分析了随着 SC 对数量的增加对 TP53 肿瘤抑制基因的累积效应。随着 TP53 的破坏性 SC 伙伴(即 SYNE2、SON 和/或 PRY)数量的增加,TCGA 膀胱癌和泌尿生殖系统癌症患者的癌症生存率得到改善。SC 负担对紫杉醇治疗反应的预后作用可以与对其他细胞毒性药物的反应区分开来。因此,成对 SC 的概念可能有助于确定新的治疗和预后靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0ace/7865701/77eb1d877047/ijms-22-01097-g001.jpg

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