2014
DOI: 10.1186/s13059-014-0428-9
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Metastatic tumor evolution and organoid modeling implicate TGFBR2as a cancer driver in diffuse gastric cancer

Abstract: BackgroundGastric cancer is the second-leading cause of global cancer deaths, with metastatic disease representing the primary cause of mortality. To identify candidate drivers involved in oncogenesis and tumor evolution, we conduct an extensive genome sequencing analysis of metastatic progression in a diffuse gastric cancer. This involves a comparison between a primary tumor from a hereditary diffuse gastric cancer syndrome proband and its recurrence as an ovarian metastasis.ResultsBoth the primary tumor and … Show more

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Cited by 116 publications
(78 citation statements)
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“…In addition, miR-21-5p may contribute to osteosarcoma metastasis via its target genes. EGFR has been demonstrated to be associated with metastasis of osteosarcoma to the lungs (37), whereas TGFBR2 has been associated with metastasis of gastric cancer cells (51), and suppressive TPM1 may alter TGF-β tumor suppressor function and thus promote metastasis of tumor cells (52). Therefore, it is possible that miR-21-5p exerts a regulatory effect on metastasis via regulation of the expression of its target genes.…”
Section: Discussionmentioning
confidence: 99%
“…In addition, miR-21-5p may contribute to osteosarcoma metastasis via its target genes. EGFR has been demonstrated to be associated with metastasis of osteosarcoma to the lungs (37), whereas TGFBR2 has been associated with metastasis of gastric cancer cells (51), and suppressive TPM1 may alter TGF-β tumor suppressor function and thus promote metastasis of tumor cells (52). Therefore, it is possible that miR-21-5p exerts a regulatory effect on metastasis via regulation of the expression of its target genes.…”
Section: Discussionmentioning
confidence: 99%
“…[63][64][65] Emerging studies are now being performed to study patterns of GC tumor evolution and clonality, occurring either within the primary tumor, or between primary lesions and metastatic sites. 54,66 Such results will be crucial for identifying molecular events associated with GC progression rather than initiation, and may suggest improved strategies for managing patients with advanced metastatic GC.…”
Section: Genetics and Molecular Pathogenesis Of Gastric Cancermentioning
confidence: 99%
“…Organoids are established by dissociating and embedding tissue in an cell-free extracellular matrix (matrigel or collagen), which can be expanded in a growth factor-enriched medium [150]. Organoids from pancreatic [151], colon [152154], gastric [155], prostate cancer [156] and brain tumors/metastasis [157] have been established, and have the advantage of 3D growth of normal and cancer tissue, recapitulating copy number and mutation spectra, as well as other physiologically relevant aspects of disease progression in vitro [150158]. Organoids can be established in culture from needle biopsies within a relative short time period, and have also been generated from circulating tumor cells [156].…”
Section: The Use Of In Vitro and In Vivo Models For Guiding Precisionmentioning
confidence: 99%