Contribution of allelic imbalance to colorectal cancer

Palin, Kimmo; Pitkänen, Esa; Turunen, Mikko; Sahu, Biswajyoti; Pihlajamaa, Päivi; Kivioja, Teemu; Kaasinen, Eevi; Välimäki, Niko; Hänninen, Ulrika A.; Cajuso, Tatiana; Aavikko, Mervi; Tuupanen, Sari; Kilpivaara, Outi; Berg, Linda van den; Kondelin, Johanna; Tanskanen, Tomas; Katainen, Riku; Grau, Marta; Rauanheimo, Heli; Plaketti, Roosa‐Maria; Taira, Aurora; Sulo, Päivi; Hartonen, Tuomo; Dave, Kashyap; Schmierer, Bernhard; Botla, Sandeep K.; Sokolova, Maria; Vähärautio, Anna; Gladysz, Kornelia; Ongen, Halit; Dermitzakis, Emmanouil T.; Bramsen, Jesper B.; Ørntoft, Torben F.; Andersen, Claus Lindbjerg; Ristimäki, Ari; Lepistö, Anna; Renkonen–Sinisalo, Laura; Mecklin∥, Jukka–Pekka; Taipale, Jussi; Aaltonen, Lauri A.

doi:10.1038/s41467-018-06132-1

Cited by 29 publications

(64 citation statements)

References 38 publications

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“…3Retrotransposon insertion distribution in LRP1B and DLG2 . Mapping of retrotransposon insertions identified in 202 colorectal tumors, HPV integration hotspots reported in 135 cervical cancers and allelic imbalance breakpoints identified in 1,699 CRCs 31,36 . Figure plotted with genoPlotR 64 .…”

Section: Resultsmentioning

confidence: 99%

“…We observed recurrent insertions in 12 out of 21 genes with high probability of being fragile as estimated in another study 30 (Supplementary Data 3). Since common fragile sites are prone to copy number alterations (CNAs) 35 , we evaluated whether retrotransposition and CNAs—in this study detected as AI 36 —were correlated (Supplementary Data 3). Fragile sites with high frequency of insertions seemed to display lower frequency of AI (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…We utilized 196 colorectal tumors with complete information on molecular and clinical variables that were included in the model (Table 2, Supplementary Data 5). We applied a multiple linear regression model for log-transformed insertion counts, and hypothesized that the number of somatic insertions may be associated with tumor location, TP53 mutation, MSI, genomic fraction of AI 36 and CIMP. The model was adjusted for mean sequencing coverage, tumor stage, sex and age at diagnosis (Table 2).…”

Section: Resultsmentioning

confidence: 99%

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Retrotransposon insertions can initiate colorectal cancer and are associated with poor survival

et al. 2019

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Genomic instability pathways in colorectal cancer (CRC) have been extensively studied, but the role of retrotransposition in colorectal carcinogenesis remains poorly understood. Although retrotransposons are usually repressed, they become active in several human cancers, in particular those of the gastrointestinal tract. Here we characterize retrotransposon insertions in 202 colorectal tumor whole genomes and investigate their associations with molecular and clinical characteristics. We find highly variable retrotransposon activity among tumors and identify recurrent insertions in 15 known cancer genes. In approximately 1% of the cases we identify insertions in APC , likely to be tumor-initiating events. Insertions are positively associated with the CpG island methylator phenotype and the genomic fraction of allelic imbalance. Clinically, high number of insertions is independently associated with poor disease-specific survival.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

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Retrotransposon insertions can initiate colorectal cancer and are associated with poor survival

et al. 2019

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“…Pooled CRISPR/Cas9-mediated knockout screens were performed in each cell line, using guide RNAs (sgRNAs) targeting 3,179 genes including all TR proteins studied in the VIPER analysis 12 , as well as selected core essential and non-essential genes, as positive and negative controls 33,34 (Extended Data Fig. 6b).…”

Section: Pda Master Regulators Are Enriched In Essential Genesmentioning

confidence: 99%

Developmental and MAPK-responsive transcription factors drive distinct malignant subtypes and genetic dependencies in pancreatic cancer

Laise

Turunen

Garcia³

et al. 2020

Preprint

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Despite extensive efforts to characterize the transcriptional landscape of pancreatic ductal adenocarcinoma (PDA), reproducible assessment of subtypes with actionable dependencies remains challenging. Systematic, network-based analysis of regulatory protein activity stratified PDA tumours into novel functional subtypes that were highly conserved across multiple cohorts, including at the single cell level and in laser capture microdissected (LCM) samples. Identified subtypes were characterized by activation of master regulator proteins representing either gastrointestinal lineage markers or transcriptional effectors of morphogen pathways. Single cell analysis confirmed the existence of Lineage and Morphogenic states but also revealed a dominant population of more differentiated Oncogenic Precursor (OP) cells , present in all sampled patients, yet not apparent from bulk tumor analysis. Master regulators were validated by pooled, CRISPR/Cas9 screens, demonstrating both subtype-specific and universal dependencies. Conversely, ectopic expression of Lineage MRs, such as OVOL2, was sufficient to reprogram Morphogenic cells, thus providing a roadmap for the future targeting of patient-specific dependencies in PDA.

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“…Cancer genomes harbor large-scale chromosomal aberrations and are characterized by aneuploidy 27,28 . To understand the gross chromosomal aberrations in the transformed tumorigenic CMT and CMT+sgTP53 iHeps compared to normal HFs, we performed spectral karyotyping, which showed a normal diploid male (46,XY) in HFs and aneuploid karyotypes in transformed iHeps (Fig.…”

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confidence: 99%

Cellular transformation by combined lineage conversion and oncogene expression

Sahu

Pihlajamaa

Zhang

et al. 2019

Preprint

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Cancer is the most complex genetic disease known, with mutations in more than 250 genes contributing to different forms of the disease 1,2,3 . Most human driver mutations are specific to particular types of cancer, at least in part due to differences in expression pattern between cell types, and the diversity of mutational mechanisms across different human tissues 4 . However, the fact that many apparently oncogenic mutations fail to transform differentiated cells in culture suggests that tumorigenesis is triggered by a specific combination of three elements: the set of driver mutations, the cellular lineage, and the state of differentiation of the cells along the lineage. Here we show that a combination of oncogenes that is characteristic of liver cancer cells (CTNNB1, TERT and MYC) induces cellular senescence in human fibroblasts, and in primary human hepatocytes. However, reprogramming fibroblasts to a liver progenitor fate, induced hepatocytes (iHeps) makes them sensitive to transformation by the same oncogenes. The transformed iHeps are highly proliferative, tumorigenic in nude mice, and bear gene expression signatures of liver cancer. Temporal analysis of the tumorigenic program using single-cell RNA-seq and RNA velocity analysis revealed that the cells progress along a common path to transformation, invariably acquiring liver progenitor cell identity prior to expressing markers characteristic of liver tumor cells. These results, together with analysis of chromatin accessibility using ATAC-seq and NaNoMe-seq indicate that lineage-determining factors act by defining a cell fate and associated chromatin state that are permissive for transformation. Taken together, our results indicate that cell identity is a key determinant in transformation, and establish a paradigm for defining the molecular states of distinct types of human cancer.Cancer genetics and genomics have identified a large number of genes implicated in human cancer 1,2,3 . Although some genes such as p53 and PTEN are commonly mutated in many different types of cancer, most cancer genes are more lineage-specific. It is well

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Contribution of allelic imbalance to colorectal cancer

Cited by 29 publications

References 38 publications

Retrotransposon insertions can initiate colorectal cancer and are associated with poor survival

Retrotransposon insertions can initiate colorectal cancer and are associated with poor survival

Developmental and MAPK-responsive transcription factors drive distinct malignant subtypes and genetic dependencies in pancreatic cancer

Cellular transformation by combined lineage conversion and oncogene expression

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