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Distinct TP63 Isoform-Driven Transcriptional Signatures Predict Tumor Progression and Clinical Outcomes.

Cancer Res.. 2018; 
Abbas Hussein A,Bui Ngoc Hoang Bao,Rajapakshe Kimal,Wong Justin,Gunaratne Preethi,Tsai Kenneth Y,Coarfa Cristian,Flores El
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ORF cDNA Clones/MolecularCloud Genscript. DNp63a ORF was cloned into pcDNA3.1-Myc-empty plasmid. Cells were collected 48 hours Get A Quote

摘要

TP63 is required to maintain stem cell pluripotency and suppresses the metastatic potential of cancer cells through multiple mechanisms. These functions are differentially regulated by individual isoforms, necessitating a deeper understanding of how the distinct transcriptional programs controlled by these isoforms affect cancer progression and outcomes. In this study, we conducted a pan-cancer analysis of The Cancer Genome Atlas to identify transcriptional networks regulated by TAp63 and ΔNp63 using transcriptomes derived from epidermal cells of TAp63 and ΔNp63 mice. Analysis of 17 cancer developmental and 27 cancer progression signatures revealed a consistent tumor suppressive pattern for TAp63. In cont... More

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