Cancer mutations in enriched RBP motifs.

Slides:

Advertisements

Similar presentations

Homozygous deletions within chromosome 9q23.

Advertisements

Figure 1. Exploring and comparing context-dependent mutational profiles in various cancer types. (A) Mutational profiles of pan-cancer somatic mutations,

Clinical trial matching.

The Functional Impact of Alternative Splicing in Cancer

Empirical mutation-selection phase diagram of tumor evolution.

binding sites 58 of the 473 unambiguously assigned phosphorylation sites are predicted by Scansite to be sites for binding. 50 of these correspond.

Fig. S3 Human genome consensus coding sequence

Ewing sarcoma tumors acquire somatic aberrancies with treatment.

Empirical mutation-selection phase diagram of tumor evolution.

by Bartlomiej Przychodzen, Andres Jerez, Kathryn Guinta, Mikkael A

WES detects a limited number of clinically targetable alterations in patients with advanced cancer. WES detects a limited number of clinically targetable.

High-throughput analysis of informative CpG sites for the four studied tumor suppressor genes (A-D). High-throughput analysis of informative CpG sites.

The Functional Impact of Alternative Splicing in Cancer

Diverse abnormalities manifest in RNA

Whole-exome sequencing identifies NF1 mutations in tumors of melanoma patients exhibiting resistance to vemurafenib. Whole-exome sequencing identifies.

Volume 48, Issue 5, Pages (December 2012)

Histology and genomic copy number alterations in TRAMP tumors.

Functional enrichment of differentially expressed genes.

Distribution of informative SNPs with LOH (black bars) on each chromosome (rows, oriented p-arm at the bottom and q-arm at the top of each chromosome)

Robustness of TRU, Proximal-proliferative (PP), and Proximal-inflammatory (PI) classification. Robustness of TRU, Proximal-proliferative (PP), and Proximal-inflammatory.

Patterns and regulation of age‐related splicing changes.

Phylogenetic and convergence analyses of rpoB mutations.

CaQTL analysis identifies genetic variants affecting human islet cis-RE use. caQTL analysis identifies genetic variants affecting human islet cis-RE use.

Association of specific phylotypes with walnut consumption and carcinogen exposure (Study 2). Association of specific phylotypes with walnut consumption.

A: Spectrum of 136 somatic HNF1A mutations observed in 75 HCA samples (top) and in 364 MODY3 individuals (bottom) (data from Ellard and Colclough [25]).

Schematic of proteins identified by RNA affinity purification-coupled LC-MS/MS and the hnRNPH-associated protein network recruited by the G-containing.

Xing Hua, Haiming Xu, Yaning Yang, Jun Zhu, Pengyuan Liu, Yan Lu

Temporal analysis of clonal evolution in typical FL and matched TFL samples. Temporal analysis of clonal evolution in typical FL and matched TFL samples.

Integrated mRNA and microRNA expression and DNA methylation clusters.

KIT mutations in GISTs. A, amino acid sequence of KIT exon 11 mutations in clinical GIST biopsies. –, amino acids that are deleted; italicized amino acids,

Relationship between the expression of immune-related genes and burdens of somatic mutation. Relationship between the expression of immune-related genes.

Predictive value of the FGFR3 mutation assay increases with multiple consecutive FGFR3-positive urine samples. Predictive value of the FGFR3 mutation assay.

Personalized genomic analyses for cancer mutation discovery and interpretation by Siân Jones, Valsamo Anagnostou, Karli Lytle, Sonya Parpart-Li, Monica.

Regional association plot of genotyped and imputed SNPs in proximity to rs , summarizing evidence of interaction with at least weekly heartburn or.

Somatic mutational rates and survival analysis of IBD-CRC.

Transcripts enriched and depleted in NB TICs compared with SKPs and other tumor tissues. Transcripts enriched and depleted in NB TICs compared with SKPs.

Temporal and spatial dissection of mutation spectra in esophageal adenocarcinoma samples. Temporal and spatial dissection of mutation spectra in esophageal.

Comparison of the frequency of nucleotide variation in the mtDNA D-loop region between stomach and other tumor cell lines. Comparison of the frequency.

Two-way, unsupervised hierarchical clustering representing the 60 tumor cell lines (vertical axis) and the analyzed total, phospho- and cleaved proteins.

Dual-color FISH analysis of 16p13

Association between BRCA1 transcript level and cisplatin sensitivity, BRCA1 promoter methylation, and NtAI. Association between BRCA1 transcript level.

Ki-67 expression in M31- and H3-treated tumors (A) and respective Ki-67 labeling indices in the two groups of tumors (B). Ki-67 expression in M31- and.

Number of identical D-loop DNA clones detected in 10 DNA clones derived from liver tumor tissues. Number of identical D-loop DNA clones detected in 10.

Representative photograph of somatic mutations detected by PCR-SSCP.

Clustering analysis of DTC-associated genes.

The long tail of mutational hotspots in cancer.

Location of the ER mutations and frequencies per cohort.

A and B, two blocks from the original specimen used for TMA demonstrated areas with varying patterns of ALK rearrangement and KRAS mutation status. A and.

Frequently mutated genes in colorectal cancer.

Global mutational landscape of the 170 lung adenocarcinoma patients (discovery cohort). Global mutational landscape of the 170 lung adenocarcinoma patients.

Concordance between the genomic landscape identified by whole-exome sequencing of plasma cfDNA and tumor; DNA and recurrence of KDR/VEGFR2 oncogenic mutations.

The primary axis scores of each sample from a constrained ordination of principal coordinates (CAP) for the temperature profile of each city are indicated.

Landscape of genomic alterations identified by WES in biopsies of patients with advanced PDAC. Co-mutation plot displaying integrated genomic data for.

Enrichment of two rare SNPs among ABC DLBCL tumors.

Germline variants influencing primary tumor type.

ERCC2 mutation mapping and distribution across tumor types.

Correlations between APOBEC expression and immune cell markers across 22 cancer types. Correlations between APOBEC expression and immune cell markers across.

Distinct subtypes of CAFs are detected in human PDAC

Venn diagram showing the overlap of PD-L1 overexpression, MSI-NGS–high, and TML-high in all gastrointestinal tumors, with all three markers tested (N =

EZH2-driven lung cancer as a molecularly distinct entity.

Detection of BRCA reversion mutations in pretreatment cfDNA and tumor biopsy. Detection of BRCA reversion mutations in pretreatment cfDNA and tumor biopsy.

Gene expression heatmap of non–T-cell-inflamed, intermediate, and T-cell–inflamed testicular germ cell tumors from TCGA. Genes are on the row, and samples.

High genomic fidelity of SCLC PDX models derived from both CTCs and biopsies. High genomic fidelity of SCLC PDX models derived from both CTCs and biopsies.

Driver pathways and key genes in OSCC

Integrated analysis of gene expression and copy number alterations.

Molecular characterization of esophagogastric tumors.

TME characteristics of TCGA-STAD subtype and cancer somatic genome.

Coincidence and prognostic significance of PD-1+ and CD103+ cells in HGSC. Serial sections from the 490-case TMA were stained with antibodies to CD103.

Characteristic gene expression patterns distinguish LCH cells from other immune cells present in LCH lesions. Characteristic gene expression patterns distinguish.

Small RNA sequencing data quality.

Presentation transcript:

Cancer mutations in enriched RBP motifs. Cancer mutations in enriched RBP motifs. We provide the proportion of samples separated by tumor type (y axis) that have a mutated motif in 5SS (A), 3SS (B), CDS (C), and INTRON (D) SMRs. In each SMR type, we show the enriched motifs. For 5SS and 3SS, we indicate the consensus 5′ or 3′ splice-site sequences (5SSC/3SSC). The proportions are color coded by tumor type. We show the mutation patterns on SRSF10 motifs in 3SS (E), CDS (F), and INTRON (G) SMRs. Top, We indicate in dark red the position of the mutations and in light red the positions covered by motif. The bar plots below show the proportion of somatic mutations (y axis) that fall on each position along the motif logo. In orange indicate those somatic mutations that coincide with a germline SNP (with a different substitution pattern, as the exact matching substitutions were removed). Below we show for each position the number of motifs with each type of substitution indicated with a color code below. Babita Singh et al. Mol Cancer Res 2018;16:1112-1124 ©2018 by American Association for Cancer Research