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一种用于鉴定胰腺癌中新型功能相关靶基因的多步骤高内涵筛选方法。

A multistep high-content screening approach to identify novel functionally relevant target genes in pancreatic cancer.

作者信息

Buchholz Malte, Honstein Tatjana, Kirchhoff Sandra, Kreider Ramona, Schmidt Harald, Sipos Bence, Gress Thomas M

机构信息

Clinic for Gastroenterology, Endocrinology, Metabolism and Infectiology, Philipps-University Marburg, Marburg, Germany.

Department of Pathology and Neuropathology, University Hospital Tübingen, Tübingen, Germany.

出版信息

PLoS One. 2015 Apr 7;10(4):e0122946. doi: 10.1371/journal.pone.0122946. eCollection 2015.

Abstract

In order to foster the systematic identification of novel genes with important functional roles in pancreatic cancer, we have devised a multi-stage screening strategy to provide a rational basis for the selection of highly relevant novel candidate genes based on the results of functional high-content analyses. The workflow comprised three consecutive stages: 1) serial gene expression profiling analyses of primary human pancreatic tissues as well as a number of in vivo and in vitro models of tumor-relevant characteristics in order to identify genes with conspicuous expression patterns; 2) use of 'reverse transfection array' technology for large-scale parallelized functional analyses of potential candidate genes in cell-based assays; and 3) selection of individual candidate genes for further in-depth examination of their cellular roles. A total of 14 genes, among them 8 from "druggable" gene families, were classified as high priority candidates for individual functional characterization. As an example to demonstrate the validity of the approach, comprehensive functional data on candidate gene ADRBK1/GRK2, which has previously not been implicated in pancreatic cancer, is presented.

摘要

为了促进对在胰腺癌中具有重要功能作用的新基因进行系统鉴定,我们设计了一种多阶段筛选策略,以便根据功能高内涵分析的结果,为选择高度相关的新候选基因提供合理依据。该工作流程包括三个连续阶段:1)对原发性人胰腺组织以及一些具有肿瘤相关特征的体内和体外模型进行系列基因表达谱分析,以鉴定具有明显表达模式的基因;2)在基于细胞的检测中,使用“反向转染阵列”技术对潜在候选基因进行大规模并行功能分析;3)选择单个候选基因,进一步深入研究其细胞作用。共有14个基因被列为进行个体功能表征的高优先级候选基因,其中8个来自“可成药”基因家族。作为证明该方法有效性的一个例子,本文展示了此前未涉及胰腺癌的候选基因ADRBK1/GRK2的综合功能数据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/971c/4388713/fed71277cce1/pone.0122946.g002.jpg

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