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Core Signaling Pathways in Human Pancreatic Cancers Revealed by Global Genomic Analyses

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TLDR
It is found that pancreatic cancers contain an average of 63 genetic alterations, the majority of which are point mutations, which defined a core set of 12 cellular signaling pathways and processes that were each genetically altered in 67 to 100% of the tumors.
Abstract
There are currently few therapeutic options for patients with pancreatic cancer, and new insights into the pathogenesis of this lethal disease are urgently needed. Toward this end, we performed a comprehensive genetic analysis of 24 pancreatic cancers. We first determined the sequences of 23,219 transcripts, representing 20,661 protein-coding genes, in these samples. Then, we searched for homozygous deletions and amplifications in the tumor DNA by using microarrays containing probes for approximately 10(6) single-nucleotide polymorphisms. We found that pancreatic cancers contain an average of 63 genetic alterations, the majority of which are point mutations. These alterations defined a core set of 12 cellular signaling pathways and processes that were each genetically altered in 67 to 100% of the tumors. Analysis of these tumors' transcriptomes with next-generation sequencing-by-synthesis technologies provided independent evidence for the importance of these pathways and processes. Our data indicate that genetically altered core pathways and regulatory processes only become evident once the coding regions of the genome are analyzed in depth. Dysregulation of these core pathways and processes through mutation can explain the major features of pancreatic tumorigenesis.

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Surgery for chronic pancreatitis decreases the risk for pancreatic cancer: A multicenter retrospective analysis

TL;DR: It is confirmed that chronic pancreatitis is an important risk factor for the development of pancreatic cancer in Japan and patients who underwent surgery for the treatment of Chronic pancreatitis had significantly lower incidences of pancreating cancer.
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HP1-Assisted Aurora B Kinase Activity Prevents Chromosome Segregation Errors

TL;DR: It is shown that heterochromatin protein 1 (HP1) is an essential CPC component required for full Aurora B activity and identified a molecular basis for chromosome segregation errors in cancer cells.
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Opportunities and Challenges for Pancreatic Circulating Tumor Cells

TL;DR: Advances in the detection, isolation, and analysis of CTCs have increased the understanding of the dissemination and progression of pancreatic cancer, but standardization of methodologies and prospective studies are needed for this emerging technology to have a significant effect on clinical care.
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Analysis of the intra- and intertumoral heterogeneity of hypoxia in pancreatic cancer patients receiving the nitroimidazole tracer pimonidazole.

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Circulating biomarkers for early diagnosis of pancreatic cancer: facts and hopes.

TL;DR: A number of novel circulating biomarkers that show promising diagnostic value have been discovered using advances in sequencing techniques and "omics" analyses, and Panels comprising several biomarkers may also exhibit better diagnostic performance.
References
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TL;DR: This work has been supported by the Department of the Army and the National Institutes of Health, and the author acknowledges the support and encouragement of the National Cancer Institute.
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Book

Pancreatic Cancer

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