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Bioinformatics And The Cell by Xuhua Xia

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1Bioinformatics Of Non Small Cell Lung Cancer And The Ras Proto-oncogene

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  • Title: ➤  Bioinformatics Of Non Small Cell Lung Cancer And The Ras Proto-oncogene
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  • Language: English

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The book is available for download in "texts" format, the size of the file-s is: 156.27 Mbs, the file-s for this book were downloaded 29 times, the file-s went public at Tue Dec 15 2020.

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2Bioinformatics And The Cell : Modern Computational Approaches In Genomics, Proteomics, And Transcriptomics

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“Bioinformatics And The Cell : Modern Computational Approaches In Genomics, Proteomics, And Transcriptomics” Metadata:

  • Title: ➤  Bioinformatics And The Cell : Modern Computational Approaches In Genomics, Proteomics, And Transcriptomics
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  • Language: English

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The book is available for download in "texts" format, the size of the file-s is: 885.96 Mbs, the file-s for this book were downloaded 15 times, the file-s went public at Fri Apr 22 2022.

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3A Bioinformatics Approach Reveals Novel Interactions Of The OVOL Transcription Factors In The Regulation Of Epithelial - Mesenchymal Cell Reprogramming And Cancer Progression.

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This article is from BMC Systems Biology , volume 8 . Abstract Background: Mesenchymal to Epithelial Transition (MET) plasticity is critical to cancer progression, and we recently showed that the OVOL transcription factors (TFs) are critical regulators of MET. Results of that work also posed the hypothesis that the OVOLs impact MET in a range of cancers. We now test this hypothesis by developing a model, OVOL Induced MET (OI-MET), and sub-model (OI-MET-TF), to characterize differential gene expression in MET common to prostate cancer (PC) and breast cancer (BC). Results: In the OI-MET model, we identified 739 genes differentially expressed in both the PC and BC models. For this gene set, we found significant enrichment of annotation for BC, PC, cancer, and MET, as well as regulation of gene expression by AP1, STAT1, STAT3, and NFKB1. Focusing on the target genes for these four TFs plus the OVOLs, we produced the OI-MET-TF sub-model, which shows even greater enrichment for these annotations, plus significant evidence of cooperation among these five TFs. Based on known gene/drug interactions, we prioritized targets in the OI-MET-TF network for follow-on analysis, emphasizing the clinical relevance of this work. Reflecting these results back to the OI-MET model, we found that binding motifs for the TF pair AP1/MYC are more frequent than expected and that the AP1/MYC pair is significantly enriched in binding in cancer models, relative to non-cancer models, in these promoters. This effect is seen in both MET models (solid tumors) and in non-MET models (leukemia). These results are consistent with our hypothesis that the OVOLs impact cancer susceptibility by regulating MET, and extend the hypothesis to include mechanisms not specific to MET. Conclusions: We find significant evidence of the OVOL, AP1, STAT1, STAT3, and NFKB1 TFs having important roles in MET, and more broadly in cancer. We prioritize known gene/drug targets for follow-up in the clinic, and we show that the AP1/MYC TF pair is a strong candidate for intervention.

“A Bioinformatics Approach Reveals Novel Interactions Of The OVOL Transcription Factors In The Regulation Of Epithelial - Mesenchymal Cell Reprogramming And Cancer Progression.” Metadata:

  • Title: ➤  A Bioinformatics Approach Reveals Novel Interactions Of The OVOL Transcription Factors In The Regulation Of Epithelial - Mesenchymal Cell Reprogramming And Cancer Progression.
  • Authors: ➤  
  • Language: English

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The book is available for download in "texts" format, the size of the file-s is: 32.61 Mbs, the file-s for this book were downloaded 71 times, the file-s went public at Thu Oct 23 2014.

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4Bioinformatics : Information Transduction And Processing Systems From Cell To Whole Body : Proceedings Of The International Symposium On Information Transduction And Processing In Biological Systems, From Cell To Whole Body, Takamatsu, Kagawa, Japan, 12-16 March 1989

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This article is from BMC Systems Biology , volume 8 . Abstract Background: Mesenchymal to Epithelial Transition (MET) plasticity is critical to cancer progression, and we recently showed that the OVOL transcription factors (TFs) are critical regulators of MET. Results of that work also posed the hypothesis that the OVOLs impact MET in a range of cancers. We now test this hypothesis by developing a model, OVOL Induced MET (OI-MET), and sub-model (OI-MET-TF), to characterize differential gene expression in MET common to prostate cancer (PC) and breast cancer (BC). Results: In the OI-MET model, we identified 739 genes differentially expressed in both the PC and BC models. For this gene set, we found significant enrichment of annotation for BC, PC, cancer, and MET, as well as regulation of gene expression by AP1, STAT1, STAT3, and NFKB1. Focusing on the target genes for these four TFs plus the OVOLs, we produced the OI-MET-TF sub-model, which shows even greater enrichment for these annotations, plus significant evidence of cooperation among these five TFs. Based on known gene/drug interactions, we prioritized targets in the OI-MET-TF network for follow-on analysis, emphasizing the clinical relevance of this work. Reflecting these results back to the OI-MET model, we found that binding motifs for the TF pair AP1/MYC are more frequent than expected and that the AP1/MYC pair is significantly enriched in binding in cancer models, relative to non-cancer models, in these promoters. This effect is seen in both MET models (solid tumors) and in non-MET models (leukemia). These results are consistent with our hypothesis that the OVOLs impact cancer susceptibility by regulating MET, and extend the hypothesis to include mechanisms not specific to MET. Conclusions: We find significant evidence of the OVOL, AP1, STAT1, STAT3, and NFKB1 TFs having important roles in MET, and more broadly in cancer. We prioritize known gene/drug targets for follow-up in the clinic, and we show that the AP1/MYC TF pair is a strong candidate for intervention.

“Bioinformatics : Information Transduction And Processing Systems From Cell To Whole Body : Proceedings Of The International Symposium On Information Transduction And Processing In Biological Systems, From Cell To Whole Body, Takamatsu, Kagawa, Japan, 12-16 March 1989” Metadata:

  • Title: ➤  Bioinformatics : Information Transduction And Processing Systems From Cell To Whole Body : Proceedings Of The International Symposium On Information Transduction And Processing In Biological Systems, From Cell To Whole Body, Takamatsu, Kagawa, Japan, 12-16 March 1989
  • Author: ➤  
  • Language: English

“Bioinformatics : Information Transduction And Processing Systems From Cell To Whole Body : Proceedings Of The International Symposium On Information Transduction And Processing In Biological Systems, From Cell To Whole Body, Takamatsu, Kagawa, Japan, 12-16 March 1989” Subjects and Themes:

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Downloads Information:

The book is available for download in "texts" format, the size of the file-s is: 808.28 Mbs, the file-s for this book were downloaded 24 times, the file-s went public at Mon Jul 27 2020.

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ACS Encrypted EPUB - ACS Encrypted PDF - Abbyy GZ - Cloth Cover Detection Log - DjVuTXT - Djvu XML - Dublin Core - Item Tile - JPEG Thumb - JSON - LCP Encrypted EPUB - LCP Encrypted PDF - Log - MARC - MARC Binary - Metadata - OCR Page Index - OCR Search Text - PNG - Page Numbers JSON - Scandata - Single Page Original JP2 Tar - Single Page Processed JP2 ZIP - Text PDF - Title Page Detection Log - chOCR - hOCR -

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