Your search keyword '"Jaime I. Davila"' showing total 32 results

1. Polymorphous Low-Grade Neuroepithelial Tumor of the Young (PLNTY): Molecular Profiling Confirms Frequent MAPK Pathway Activation

Author

Kay Minn, Jaime I. Davila, Cristiane M. Ida, Caterina Giannini, Robert B. Jenkins, Kevin C. Halling, Kar-Ming A Fung, Timothy J. Kaufmann, Jessica R. Balcom, Dong Kun Kim, Numrah Fadra, Asha Nair, Derek R. Johnson, Benjamin R. Kipp, Thomas M. Kollmeyer, Ida C.M., Johnson D.R., Nair A.A., Davila J., Kollmeyer T.M., Minn K., Fadra N.M., Balcom J.R., Fung K.-M.A., Kim D.K., Kaufmann T.J., Kipp B.R., Halling K.C., Jenkins R.B., and Giannini C.

Subjects

Adult, MAPK/ERK pathway, NTRK2, Mitogen-Activated Protein Kinase Kinase, Biology, medicine.disease_cause, BRAF, Pathology and Forensic Medicine, Polymorphous low-grade neuroepithelial tumor, Cellular and Molecular Neuroscience, Recurrence, Seizures, Chromosome instability, KIAA1549, Gene duplication, medicine, Humans, Receptor, trkB, Mitogen-Activated Protein Kinase Kinases, Mutation, Membrane Glycoproteins, Chromosome, Original Articles, General Medicine, Aneuploidy, medicine.disease, Seizure, Neoplasms, Neuroepithelial, Neuroepithelial cell, Neurology, FGFR2, Cancer research, Female, CD34, Membrane Glycoprotein, Neurology (clinical), Oligodendroglioma, Gene Fusion, Chromosomes, Human, Pair 9, V600E, Human, Transcription Factors

Abstract

Polymorphous low-grade neuroepithelial tumor of the young (PLNTY) is a recently described epileptogenic tumor characterized by oligodendroglioma-like components, aberrant CD34 expression, and frequent mitogen-activated protein kinase (MAPK) pathway activation. We molecularly profiled 13 cases with diagnostic histopathological features of PLNTY (10 female; median age, 16 years; range, 5–52). Patients frequently presented with seizures (9 of 12 with available history) and temporal lobe tumors (9 of 13). MAPK pathway activating alterations were identified in all 13 cases. Fusions were present in the 7 youngest patients: FGFR2-CTNNA3 (n = 2), FGFR2-KIAA1598 (FGFR2-SHTN1) (n = 1), FGFR2-INA (n = 1), FGFR2-MPRIP (n = 1), QKI-NTRK2 (n = 1), and KIAA1549-BRAF (n = 1). BRAF V600E mutation was present in 6 patients (17 years or older). Two fusion-positive cases additionally harbored TP53/RB1 abnormalities suggesting biallelic inactivation. Copy number changes predominantly involving whole chromosomes were observed in all 10 evaluated cases, with losses of chromosome 10q occurring with FGFR2-KIAA1598 (SHTN1)/CTNNA3 fusions. The KIAA1549-BRAF and QKI-NTRK2 fusions were associated respectively with a 7q34 deletion and 9q21 duplication. This study shows that despite its name, PLNTY also occurs in older adults, who frequently show BRAF V600E mutation. It also expands the spectrum of the MAPK pathway activating alterations associated with PLNTY and demonstrates recurrent chromosomal copy number changes consistent with chromosomal instability.

Published

2021

2. Frequent POLE-driven hypermutation in ovarian endometrioid cancer revealed by mutational signatures in RNA sequencing

Author

Jaime I. Davila, Vivekananda Sarangi, Ellen L. Goode, Pritha Chanana, S. John Weroha, Yajue Huang, Chen Wang, Zachary C. Fogarty, and Ruifeng Guo

Subjects

COSMIC cancer database, Colorectal cancer, Research, Hypermutation, DNA polymerase epsilon, Mutational signatures, Cancer, Somatic hypermutation, Biology, QH426-470, medicine.disease, RC31-1245, Human genetics, Ovarian endometrioid cancer, POLE, medicine, Cancer research, Genetics, RNA-seq, Ovarian cancer, Carcinoma, Endometrioid, Gene, Internal medicine, Genetics (clinical)

Abstract

Background DNA polymerase epsilon (POLE) is encoded by the POLE gene, and POLE-driven tumors are characterized by high mutational rates. POLE-driven tumors are relatively common in endometrial and colorectal cancer, and their presence is increasingly recognized in ovarian cancer (OC) of endometrioid type. POLE-driven cases possess an abundance of TCT > TAT and TCG > TTG somatic mutations characterized by mutational signature 10 from the Catalog of Somatic Mutations in Cancer (COSMIC). By quantifying the contribution of COSMIC mutational signature 10 in RNA sequencing (RNA-seq) we set out to identify POLE-driven tumors in a set of unselected Mayo Clinic OC. Methods Mutational profiles were calculated using expressed single-nucleotide variants (eSNV) in the Mayo Clinic OC tumors (n = 195), The Cancer Genome Atlas (TCGA) OC tumors (n = 419), and the Genotype-Tissue Expression (GTEx) normal ovarian tissues (n = 84). Non-negative Matrix Factorization (NMF) of the mutational profiles inferred the contribution per sample of four distinct mutational signatures, one of which corresponds to COSMIC mutational signature 10. Results In the Mayo Clinic OC cohort we identified six tumors with a predicted contribution from COSMIC mutational signature 10 of over five mutations per megabase. These six cases harbored known POLE hotspot mutations (P286R, S297F, V411L, and A456P) and were of endometrioid histotype (P = 5e−04). These six tumors had an early onset (average age of patients at onset, 48.33 years) when compared to non-POLE endometrioid OC cohort (average age at onset, 60.13 years; P = .008). Samples from TCGA and GTEx had a low COSMIC signature 10 contribution (median 0.16 mutations per megabase; maximum 1.78 mutations per megabase) and carried no POLE hotspot mutations. Conclusions From the largest cohort of RNA-seq from endometrioid OC to date (n = 53), we identified six hypermutated samples likely driven by POLE (frequency, 11%). Our result suggests the clinical need to screen for POLE driver mutations in endometrioid OC, which can guide enrollment in immunotherapy clinical trials.

Published

2021

3. RNA-Seq Reveals Differences in Expressed Tumor Mutation Burden in Colorectal and Endometrial Cancers with and without Defective DNA-Mismatch Repair

Author

Bruce W. Eckloff, Rory A. Jackson, Mazen A. Atiq, Sarah E. Kerr, Margaret A. DiGuardo, Asha Nair, Kevin C. Halling, Jin Jen, Kandelaria M. Rumilla, Jesse S. Voss, Rondell P. Graham, Jaime I. Davila, Andrew M. Bellizzi, Benjamin R. Kipp, Numrah Fadra, Kay Minn, Dora Lam-Himlin, Shannon M. Knight, Shabnam Zarei, Joseph H. Blommel, and Robert B. Jenkins

Subjects

Adult, Male, 0301 basic medicine, Biology, medicine.disease_cause, MLH1, DNA Mismatch Repair, Pathology and Forensic Medicine, 03 medical and health sciences, 0302 clinical medicine, Biomarkers, Tumor, medicine, Humans, RNA-Seq, Aged, Retrospective Studies, Aged, 80 and over, Mutation, Endometrial cancer, RNA, Middle Aged, Prognosis, medicine.disease, digestive system diseases, Endometrial Neoplasms, 030104 developmental biology, 030220 oncology & carcinogenesis, DNA methylation, Cancer research, Molecular Medicine, Biomarker (medicine), Microsatellite, Female, DNA mismatch repair, Colorectal Neoplasms, Follow-Up Studies

Abstract

Tumor mutation burden (TMB) is an emerging biomarker of immunotherapy response. RNA sequencing in FFPE tissue samples was used for determining TMB in microsatellite-stable (MSS) and microsatellite instability–high (MSI-H) tumors in patients with colorectal or endometrial cancer. Tissue from tumors and paired normal tissue from 46 MSI-H and 12 MSS cases were included. Of the MSI-H tumors, 29 had defective DNA mismatch–repair mutations, and 17 had MLH1 promoter hypermethylation. TMB was measured using the expressed somatic nucleotide variants (eTMB). A method of accurate measurement of eTMB was developed that removes FFPE-derived artifacts by leveraging mutation signatures. There was a significant difference in the median eTMB values observed between MSI-H and MSS cases: 27.3 versus 6.7 mutations/megabase (mut/Mb) (P = 3.5 × 10−9). Among tumors with defective DNA-mismatch repair, those with mismatch-repair mutations had a significantly higher median eTMB than those with hypermethylation: 28.1 versus 17.5 mut/Mb (P = 0.037). Multivariate analysis showed that MSI status, tumor type (endometrial or colorectal), and age were significantly associated with eTMB. Additionally, using whole-exome sequencing in a subset of these patients, it was determined that DNA TMB correlated well with eTMB (Spearman correlation coefficient, 0.83). These results demonstrate that RNA sequencing can be used for measuring eTMB in FFPE tumor specimens.

Published

2021

4. Transcriptomic and Proteomic Analysis of Steatohepatitic Hepatocellular Carcinoma Reveals Novel Distinct Biologic Features

Author

Jaime I. Davila, Andrew M. Bellizzi, Daniela S. Allende, Rondell P. Graham, Roger K. Moreira, Erik Jessen, Benjamin J. Van Treeck, Taofic Mounajjed, Mushfig Orujov, and Stephen M. Lagana

Subjects

Adult, Male, Proteomics, 0301 basic medicine, Carcinoma, Hepatocellular, Proteome, Biology, medicine.disease_cause, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, GLI1, Gene expression, Biomarkers, Tumor, medicine, Humans, Aged, Gene Expression Profiling, Liver Neoplasms, General Medicine, Middle Aged, medicine.disease, Immunohistochemistry, Phenotype, Hedgehog signaling pathway, Fatty Liver, Gene expression profiling, 030104 developmental biology, Liver, Hepatocellular carcinoma, biology.protein, Cancer research, Female, 030211 gastroenterology & hepatology, Carcinogenesis

Abstract

ObjectivesSteatohepatitic hepatocellular carcinoma is a distinct variant of hepatocellular carcinoma strongly associated with underlying nonalcoholic steatohepatitis. The molecular biology of steatohepatitic hepatocellular carcinoma is not fully elucidated, and thus we aimed to investigate the molecular underpinnings of this entity.MethodsTranscriptomic analysis using RNAseq was performed on eight tumor-nonneoplastic pairs of steatohepatitic hepatocellular carcinoma with comparison to conventional hepatocellular carcinoma transcriptomes curated in The Cancer Genome Atlas. Immunohistochemistry was used to validate key RNA-level findings.ResultsSteatohepatitic hepatocellular carcinoma demonstrated a distinctive differential gene expression profile compared with The Cancer Genome Atlas curated conventional hepatocellular carcinomas (n = 360 cases), indicating the distinctive steatohepatitic hepatocellular carcinoma morphology is associated with a unique gene expression profile. Pathway analysis comparing tumor-nonneoplastic pairs revealed significant upregulation of the hedgehog pathway based on GLI1 overexpression and significant downregulation of carnitine palmitoyltransferase 2 transcript. Glutamine synthetase transcript was significantly upregulated, and fatty acid binding protein 1 transcript was significantly downregulated and immunohistochemically confirmed, indicating steatohepatitic hepatocellular carcinoma tumor cells display a zone 3 phenotype.ConclusionsSteatohepatitic hepatocellular carcinoma demonstrates a distinctive morphology and gene expression profile, phenotype of zone 3 hepatocytes, and activation of the hedgehog pathway and repression of carnitine palmitoyltransferase 2, which may be important in tumorigenesis.

Published

2020

5. Desmoplastic Infantile Ganglioglioma: A MAPK Pathway-Driven and Microglia/Macrophage-Rich Neuroepithelial Tumor

Author

Melissa M. Blessing, Rory A. Jackson, Chandra Krishnan, Dragana Milosevic, Benjamin R. Kipp, Emily G. Barr Fritcher, Christopher D. Zysk, Amulya A. Nageswara Rao, Asha Nair, Kevin C. Halling, Jaime I. Davila, Patrick R. Blackburn, William R. Macon, Jessica R. Balcom, David J. Daniels, Robert B. Jenkins, Cristiane M. Ida, Virginia L. Harrod, and Nadia N. Laack

Subjects

Male, MAPK/ERK pathway, MAP Kinase Signaling System, medicine.medical_treatment, Biology, Pathology and Forensic Medicine, Targeted therapy, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Dig, Glioma, medicine, Humans, Allele frequency, Ganglioglioma, Brain Neoplasms, Macrophages, Brain, Infant, General Medicine, medicine.disease, Neoplasms, Neuroepithelial, Neuroepithelial cell, Neurology, 030220 oncology & carcinogenesis, Cancer research, Female, Microglia, Neurology (clinical), CD163, 030217 neurology & neurosurgery, V600E

Abstract

MAPK pathway activation has been recurrently observed in desmoplastic infantile ganglioglioma/astrocytoma (DIG/DIA) with reported disproportionally low mutation allele frequencies relative to the apparent high tumor content, suggesting that MAPK pathway alterations may be subclonal. We sought to expand the number of molecularly profiled cases and investigate if tumor cell composition could account for the observed low mutation allele frequencies. Molecular (targeted neuro-oncology next-generation sequencing/RNA sequencing and OncoScan microarray) and immunohistochemical (CD68-PGM1/CD163/CD14/CD11c/lysozyme/CD3/CD20/CD34/PD-L1) studies were performed in 7 DIG. Activating MAPK pathway alterations were identified in 4 (57%) cases: 3 had a BRAF mutation (V600E/V600D/V600_W604delinsDQTDG, at 8%–27% variant allele frequency) and 1 showed a TPM3-NTRK1 fusion. Copy number changes were infrequent and nonrecurrent. All tumors had at least 30% of cells morphologically and immunophenotypically consistent with microglial/macrophage lineage. Two subtotally resected tumors regrew; 1 was re-excised and received adjuvant treatment (chemotherapy/targeted therapy), with clinical response to targeted therapy only. Even with residual tumor, all patients are alive (median follow-up, 83 months; 19–139). This study further supports DIG as another MAPK pathway-driven neuroepithelial tumor, thus expanding potential treatment options for tumors not amenable to surgical cure, and suggests that DIG is a microglia/macrophage-rich neuroepithelial tumor with frequent low driver mutation allele frequencies.

Published

2019

6. Gene expression differences between matched pairs of ovarian cancer patient tumors and patient-derived xenografts

Author

Paul Haluska, Cordelia D. McGehee, Ellen L. Goode, Jaime I. Davila, Valentina Zanfagnin, S. John Weroha, Yuanhang Liu, Xiaonan Hou, Pritha Chanana, Chen Wang, and Eric C. Polley

Subjects

0301 basic medicine, endocrine system, Stromal cell, endocrine system diseases, lcsh:Medicine, PDGFRB, PDGFRA, Biology, digestive system, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, Stroma, Ovarian cancer, Gene expression, Cancer genomics, medicine, Animals, Humans, lcsh:Science, Gene, Ovarian Neoplasms, Regulation of gene expression, Multidisciplinary, lcsh:R, nutritional and metabolic diseases, medicine.disease, Computational biology and bioinformatics, Neoplasm Proteins, 3. Good health, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Cancer research, Heterografts, Female, lcsh:Q, Neoplasm Transplantation, 030217 neurology & neurosurgery, hormones, hormone substitutes, and hormone antagonists

Abstract

As patient derived xenograft (PDX) models are increasingly used for preclinical drug development, strategies to account for the nonhuman component of PDX RNA expression data are critical to its interpretation. A bioinformatics pipeline to separate donor tumor and mouse stroma transcriptome profiles was devised and tested. To examine the molecular fidelity of PDX versus donor tumors, we compared mRNA differences between paired PDX-donor tumors from nine ovarian cancer patients. 1,935 differentially expressed genes were identified between PDX and donor tumors. Over 90% (n = 1767) of these genes were down-regulated in PDX models and enriched in stroma-specific functions. Several protein kinases were also differentially expressed in PDX tumors, e.g. PDGFRA, PDGFRB and CSF1R. Upon in silico removal of these PDX-donor tumor differentially expressed genes, a stronger transcriptional resemblance between PDX-donor tumor pairs was seen (average correlation coefficient increases from 0.91 to 0.95). We devised and validated an effective bioinformatics strategy to separate mouse stroma expression from human tumor expression for PDX RNAseq. In addition, we showed most of the PDX-donor differentially expressed genes were implicated in stromal components. The molecular similarities and differences between PDX and donor tumors have implications in future therapeutic trial designs and treatment response evaluations using PDX models.

Published

2019

7. RNA sequencing identifies a novel USP9X‐USP6 promoter swap gene fusion in a primary aneurysmal bone cyst

Author

Kevin C. Halling, Patrick R. Blackburn, Rory A. Jackson, Mark G. Hessler, Rebecca N. Wehrs, Beth A. Pitel, Mazen A. Atiq, Asha Nair, Robert B. Jenkins, Todd J. VanDeWalker, Katherine B. Geiersbach, Karen J. Fritchie, Sara K. Hovel, Jaime I. Davila, and Numrah Fadra

Subjects

Male, Cancer Research, Adolescent, Oncogene Proteins, Fusion, Biopsy, Chromosomal translocation, Computational biology, Biology, Fusion gene, 03 medical and health sciences, Exon, 0302 clinical medicine, Proto-Oncogene Proteins, Biomarkers, Tumor, Genetics, medicine, Humans, Coding region, Genetic Predisposition to Disease, Promoter Regions, Genetic, Gene, Genetic Association Studies, In Situ Hybridization, Fluorescence, medicine.diagnostic_test, Computational Biology, High-Throughput Nucleotide Sequencing, RNA, Aneurysmal bone cyst, medicine.disease, Magnetic Resonance Imaging, Chromosome Banding, Bone Cysts, Aneurysmal, 030220 oncology & carcinogenesis, Tomography, X-Ray Computed, Ubiquitin Thiolesterase, Fluorescence in situ hybridization

Abstract

Primary aneurysmal bone cyst (ABC) is a benign multiloculated cystic lesion of bone that is defined cytogenetically by USP6 gene rearrangements. Rearrangements involving USP6 are promoter swaps, usually generated by fusion of the noncoding upstream exons of different partner genes with exon 1 or 2 of USP6, thus leading to transcriptional upregulation of full-length USP6 coding sequence. Testing for USP6 rearrangements is used diagnostically to distinguish it from secondary ABC and other giant cell-rich primary bone tumors. In this report, we present a case of a 16-year-old male with a primary ABC of the left distal femur. USP6 break apart fluorescence in situ hybridization was positive for a rearrangement and conventional chromosome analysis identified a reciprocal X;17 translocation. In order to identify the putative USP6 fusion partner, we performed RNA sequencing and uncovered a novel USP9X-USP6 promoter swap fusion. This result was confirmed by reverse transcription-polymerase chain reaction (RT-PCR) and by mate pair sequencing thus showing the utility of these alternative methodologies in identifying novel fusion candidates. Ubiquitin-specific protease 9X (USP9X), like USP6, encodes a highly conserved substrate-specific deubiquitylating enzyme. USP9X is highly expressed in a number of tissue types and acts as both an oncogene and tumor suppressor in several human cancers. We conclude that oncogenic activation of USP6 via USP9X promoter exchange represents a novel driver of primary ABC formation.

Published

2019

8. Identification and Development of a Lung Adenocarcinoma PDX Model With STRN-ALK Fusion

Author

Joanne E. Yi, Helena Kovarikova, Jaime I. Davila, Patrick W. Eiken, Aaron S. Mansfield, Karlyn E. Pierson, Jin Jen, Jin Sung Jang, Asha Nair, Xiaonan Hou, Julian R. Molina, Sarah H. Johnson, Hongzheng Ren, Jin Zhang, Ping Yang, and Randolph S. Marks

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, Cancer Research, Lung Neoplasms, Oncogene Proteins, Fusion, medicine.medical_treatment, Adenocarcinoma of Lung, Nerve Tissue Proteins, Mice, SCID, Targeted therapy, Fusion gene, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, hemic and lymphatic diseases, medicine, Animals, Humans, Anaplastic lymphoma kinase, Anaplastic Lymphoma Kinase, Lung cancer, Gene, Neoplasm Staging, Lung, business.industry, Membrane Proteins, Middle Aged, medicine.disease, Xenograft Model Antitumor Assays, 030104 developmental biology, medicine.anatomical_structure, Oncology, Protein kinase domain, 030220 oncology & carcinogenesis, Cancer research, Adenocarcinoma, Calmodulin-Binding Proteins, Female, business

Abstract

Gene fusions involving the anaplastic lymphoma kinase ( ALK) gene occurs in approximately 3-5% of lung adenocarcinomas. The most common fusion partner is EML4 but several other fusion partners to the ALK kinase domain have been identified. Herein we report a lung adenocarcinoma case harboring a fusion between ALK and Striatin ( STRN ), with extended responses to targeted therapy. Using CT-guided needle biopsy approach, we successfully generated a patient-derived xenograft model from this tumor and molecularly characterized the STRN-ALK gene fusion.

Published

2019

9. Abstract P3-08-10: A unique coding and non-coding benign breast transcriptome in post-menopausal ER+ breast cancer

Author

AA Nair, Amy C. Degnim, Derek C. Radisky, Jaime I. Davila, Tanya L. Hoskin, Jodi M. Carter, DW Visscher, SJ Winham, and Ethan P. Heinzen

Subjects

Cancer Research, Messenger RNA, RNA, Cancer, Biology, medicine.disease, medicine.disease_cause, Antisense RNA, Transcriptome, Breast cancer, Oncology, medicine, Cancer research, Carcinogenesis, Gene

Abstract

Background: Differences in ER+ and ER- breast cancer tumor biology are well-documented, but little is known about the field of background benign breast in which those cancers arise. We evaluated the transcriptome of benign breast tissues from women with concurrent ipsilateral ER+ and ER- breast cancers (BC) to characterize coding and non-coding RNA profiles. This pilot study provides insight into the transcriptomic landscapes of benign breast tissues in patients with BC, and the microenvironment of the at-risk benign tissue. Methods: With institutional approval, cryobanked breast tissues from patients with concurrent ipsilateral ER+ BC (benign ER+BC, N=14) or ER- BC (benign ER-BC, N=10), were selected for benign tissues with similar epithelial:stromal ratios and grouped into pre (preM) and post-menopausal (PM) groups. Following RNA sequencing (Illumina TruSeq Stranded mRNA kit & Illumina HiSeq 4000), reads were processed (MAP-RSeq v3.0.0) and aligned (STAR aligner; hg38). Differential expression (DE) analysis (edgeR 2.6.2) identified DE genes from normalized RPKM reads (absolute log2 fold change (FC) > 1 and false discovery rate (FDR) < 0.10), corrected for intra-group biases. Over-representation analysis [Ingenuity pathway analysis (IPA), Ingenuity® Systems] and gene set enrichment analysis [(GSEA), GeneTrail 2.0] identified significantly-enriched pathways. Results: In the PM group, there were 144 DE transcripts between benign ER+BC and benign ER-BC, including coding RNAs (40%), antisense RNAs (35%) and lncRNAs (7%). In contrast, the preM group had no significantly DE genes between benign ER+BC and benign ER-BC. In the PM DE coding gene set, the top DE transcripts in benign ER+BC included many genes implicated in BC development# or ER+ BC progression (*) (e.g. up-regulated: KAAG1*, DNAJB7/HSP40*, TMEM151B, ZBTB32# p < 0.001 ; down-regulated: CPB1*, FOS, TPPP3#, CLEC3B#p < 0.001). Top canonical pathways altered in benign ER+BC included MAPK, PI3K, and acute phase response pathways (p 0.4) functionally grouped as immune function-related (T cell function and antigen presentation). Depleted pathways with NES > 0.4, (N=6) functionally grouped into proteasome-related, fatty acid biosynthesis and mitochondrial energy metabolism. Among the non-coding DE gene set, notably, the entire DE antisense RNA gene set (N=51 transcripts) was up-regulated in benign ER+ BC compared to benign ER-BC (P< 0.001) with a subset (N=11) showing marked up-regulation (> 4 log2FC). Among the DE antisense RNAs, 70% have reported roles in carcinogenesis or BC progression (e.g. KRT7-AS, NAV2-AS2, CCDC144NL-AS1, RP11-66B24.4, HSA-MIR4454). Conclusion: The benign breast transcriptome differs between postmenopausal women with ER+ vs ER- BC, with distinctive coding and non-coding RNA signatures. In postmenopausal women with ER+ BC, benign breast expresses a unique antisense RNA set and is enriched in genes implicated in BC development or progression. These data provide insight into at-risk benign breast and facilitate identification of potential biomarkers of carcinogenesis. Citation Format: Carter JM, Nair AA, Davila JI, Heinzen EP, Hoskin TL, Winham SJ, Radisky DC, Visscher DW, Degnim AC. A unique coding and non-coding benign breast transcriptome in post-menopausal ER+ breast cancer [abstract]. In: Proceedings of the 2018 San Antonio Breast Cancer Symposium; 2018 Dec 4-8; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2019;79(4 Suppl):Abstract nr P3-08-10.

Published

2019

10. ST3GAL1 is a target of the SOX2-GLI1 transcriptional complex and promotes melanoma metastasis through AXL

Author

Brooke D. Paradise, Lorenzo Tofani, Li Ying, Jaime I. Davila, Giulia Anichini, Silvia Pietrobono, Jann N. Sarkaria, Fabrizio Manetti, Martin E. Fernandez-Zapico, Ryan M. Carr, Barbara Stecca, Hu Li, Alexander Meves, Sara Pepe, Cheng Zhang, Cesare Sala, Luciana L. Almada, Ilaria Battisti, and Giorgio Arrigoni

Subjects

0301 basic medicine, Glycosylation, Skin Neoplasms, Transcription, Genetic, Nude, General Physics and Astronomy, Receptor tyrosine kinase, Metastasis, Mice, 0302 clinical medicine, lcsh:Science, Animals, Gene Expression Regulation, Neoplastic, Humans, Melanoma, Mice, Nude, Multiprotein Complexes, Proto-Oncogene Proteins, Receptor Protein-Tyrosine Kinases, SOXB1 Transcription Factors, Sialyltransferases, Xenograft Model Antitumor Assays, Zinc Finger Protein GLI1, Cancer, Multidisciplinary, Molecular medicine, biology, 030220 oncology & carcinogenesis, Transcription, beta-Galactoside alpha-2,3-Sialyltransferase, Science, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Genetic, SOX2, GLI1, medicine, Gene silencing, neoplasms, Neoplastic, General Chemistry, medicine.disease, Axl Receptor Tyrosine Kinase, 030104 developmental biology, Gene Expression Regulation, biology.protein, Cancer research, lcsh:Q

Abstract

Understanding the molecular events controlling melanoma progression is of paramount importance for the development of alternative treatment options for this devastating disease. Here we report a mechanism regulated by the oncogenic SOX2-GLI1 transcriptional complex driving melanoma invasion through the induction of the sialyltransferase ST3GAL1. Using in vitro and in vivo studies, we demonstrate that ST3GAL1 drives melanoma metastasis. Silencing of this enzyme suppresses melanoma invasion and significantly reduces the ability of aggressive melanoma cells to enter the blood stream, colonize distal organs, seed and survive in the metastatic environment. Analysis of glycosylated proteins reveals that the receptor tyrosine kinase AXL is a major effector of ST3GAL1 pro-invasive function. ST3GAL1 induces AXL dimerization and activation that, in turn, promotes melanoma invasion. Our data support a key role of the ST3GAL1-AXL axis as driver of melanoma metastasis, and highlight the therapeutic potential of targeting this axis to treat metastatic melanoma., Understanding the molecular events controlling melanoma progression are necessary to find improved therapeutics. Here, the authors report oncogenic SOX2-GLI1 transcriptional complex to drive melanoma invasion through the induction of the sialyltransferase ST3GAL1, and report ST3GAL1-AXL axis as driver of melanoma metastasis.

Published

2020

11. Molecular Genetic Landscape of Sclerosing Pneumocytomas

Author

Hee Eun Lee, Joseph J. Maleszewski, Jennifer M. Boland, Benjamin R. Kipp, Erik Jessen, Rondell P. Graham, Jaime I. Davila, Emily G. Barr Fritcher, Eunhee S. Yi, and Jesse S. Voss

Subjects

0301 basic medicine, Oncology, Adult, medicine.medical_specialty, Adolescent, AKT1, medicine.disease_cause, Translocation, Genetic, Fusion gene, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Pulmonary Sclerosing Hemangioma, Internal medicine, medicine, Biomarkers, Tumor, PTEN, Humans, PI3K/AKT/mTOR pathway, Aged, Retrospective Studies, Mutation, Everolimus, biology, business.industry, Sequence Analysis, RNA, TOR Serine-Threonine Kinases, Cancer, High-Throughput Nucleotide Sequencing, General Medicine, Middle Aged, medicine.disease, 030104 developmental biology, 030220 oncology & carcinogenesis, biology.protein, Female, business, Progressive disease, medicine.drug, Signal Transduction

Abstract

Objectives Sclerosing pneumocytomas are rare pulmonary neoplasms that are typically benign. However, rare patients experience progressive disease, and therapy targeting specific genetic underpinnings could be an attractive therapeutic option. Recent studies have found recurrent AKT 1 mutations in sclerosing pneumocytoma, but little is known about whether oncogenic fusion genes may also be present. Methods To better understand the genetic background, 10 sclerosing pneumocytomas were subjected to next-generation sequencing cancer mutation panel testing (n = 9) and/or RNA sequencing (n = 3). The patients were all women (average age, 47 years; range, 17-74 years). Results Eight patients had solitary sclerosing pneumocytomas, while one had two tumors, and one had many bilateral tumors. Recurrent mutations were noted in genes involved in the mTOR pathway, including AKT1, PIK3R1, and PTEN. AKT1 alterations were particularly common, present in 78%. No recurrent genetic fusions were identified. The patient in our study with multiple bilateral lesions was treated with the mammalian target of rapamycin (mTOR) inhibitor everolimus, with no objective radiographic evidence of treatment response after 4 months. Conclusions Our data further support that abnormal activation of the mTOR pathway is a consistent genetic event in sclerosing pneumocytoma. This warrants further exploration to determine if mTOR pathway inhibitors may be effective in patients with metastatic or recurrent disease.

Published

2020

12. Multiple isodicentric Y chromosomes in myeloid malignancies: a unique cytogenetic entity and potential therapeutic target

Author

Mrinal M. Patnaik, Gavin R. Oliver, Daniel L. Van Dyke, Kevin C. Halling, Kathleen Kaiser-Rogers, Patricia T. Greipp, Jaime I. Davila, Michelle A. Elliott, Abhishek A. Mangaonkar, Numrah Fadra, Kathleen W. Rao, and Rebecca N. Wehrs

Subjects

Cancer Research, Myeloid, Treatment outcome, Chromosome, macromolecular substances, Hematology, Biology, medicine.disease, Y chromosome, Isodicentric y, 03 medical and health sciences, Leukemia, 0302 clinical medicine, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Cytogenetic Abnormality, Gene duplication, medicine, Cancer research, 030215 immunology

Abstract

Multiple isodicentric Y chromosome [idic(Y)] is a cytogenetic abnormality consisting of duplicative copies of the short-arm of Y chromosome. Several mechanisms have been postulated to explain the f...

Published

2018

13. Spindle cell rhabdomyosarcoma of bone withFUS-TFCP2fusion: confirmation of a very recently described rhabdomyosarcoma subtype

Author

Kevin C. Halling, Asha Nair, Nooshi K. Dashti, William R. Sukov, Jan C. Buckner, Jaime I. Davila, Rebecca N. Wehrs, Andrew L. Folpe, Benjamin M. Howe, Brittany C. Thomas, and Anthony P. Martinez

Subjects

Male, musculoskeletal diseases, 0301 basic medicine, Pathology, medicine.medical_specialty, Histology, Oncogene Proteins, Fusion, Sclerosing rhabdomyosarcoma, urologic and male genital diseases, Pathology and Forensic Medicine, Lesion, 03 medical and health sciences, 0302 clinical medicine, hemic and lymphatic diseases, Rhabdomyosarcoma, medicine, Humans, Spindle cell rhabdomyosarcoma, neoplasms, Aged, business.industry, Mandible, Soft tissue, General Medicine, medicine.disease, female genital diseases and pregnancy complications, DNA-Binding Proteins, Mandibular Neoplasms, 030104 developmental biology, 030220 oncology & carcinogenesis, RNA-Binding Protein FUS, Immunohistochemistry, Differential diagnosis, medicine.symptom, business, Transcription Factors

Abstract

Aims Rhabdomyosarcomas of bone are extremely rare, with fewer than 10 reported cases. A very rare subtype of spindle cell/sclerosing rhabdomyosarcoma harbouring a FUS-TFCP2 fusion and involving both soft tissue and bone locations has been reported very recently. We report only the fourth case of this unusual, clinically aggressive rhabdomyosarcoma. Material and results A previously well 72-year-old male presented with a destructive lesion of the mandible. Morphological and immunohistochemical study of a needle biopsy and the subsequent resection showed a spindle cell rhabdomyosarcoma. RNA-seq, RT-PCR and FISH confirmed the presence of the FUS-TFCP2 fusion. Conclusions Spindle cell rhabdomyosarcomas carrying the FUS-TFCP2 fusion are very rare rhabdomyosarcoma variants with osseous predilection. The classification and differential diagnosis of this unusual molecular variant of spindle cell/sclerosing rhabdomyosarcoma are discussed.

Published

2018

14. Composite hemangioendothelioma with neuroendocrine marker expression: an aggressive variant

Author

Andrew L. Folpe, Hongzheng Ren, Kyle D. Perry, William R. Sukov, Henry D. Tazelaar, Stefan E. Pambuccian, Andrew E. Horvai, Brian P. Rubin, Asha Nair, Alyaa Al-Lbraheemi, Jaime I. Davila, Jin Sung Jang, and Jin Jen

Subjects

Adult, Male, Composite Hemangioendothelioma, Pathology, medicine.medical_specialty, Adolescent, Conventional Angiosarcoma, Neuroendocrine differentiation, Pathology and Forensic Medicine, Hemangioendothelioma, Young Adult, 030207 dermatology & venereal diseases, 03 medical and health sciences, 0302 clinical medicine, Biomarkers, Tumor, medicine, Humans, Child, Epithelioid hemangioendothelioma, biology, Chromogranin A, Middle Aged, medicine.disease, 030220 oncology & carcinogenesis, Synaptophysin, biology.protein, Female, Epithelioid cell

Abstract

Aberrant expression of neuroendocrine markers is extremely rare in endothelial neoplasms, with only a single report describing three cases. Although originally classified as conventional angiosarcoma, further assessment of these tumors revealed a strikingly composite morphology composed of retiform and epithelioid elements reminiscent of composite hemangioendothelioma, a rare subtype of hemangioendothelioma. To further investigate these findings, available materials from 11 morphologically distinctive endothelial tumors showing neuroendocrine marker expression were retrieved from our archives. Immunohistochemistry for CD31, CD34, FLI-1, synaptophysin, chromogranin, D2-40, ERG, keratin (OSCAR), and CAMTA1 was performed. Total RNA from five cases were extracted and subjected to whole transcriptome sequencing. Clinical follow-up was obtained. These tumors were found to arise in five males and six females in patients from 9 to 55 years in age (median 47 years). They arose both in superficial (wrist, ankle, scalp, hip, and foot) and deep (periaortic tissues, C5 vertebra, pulmonary vein, and liver) locations. All contained elongated, retiform vascular channels lined by hyperchromatic 'hobnail' endothelial cells and a solid growth of uniform epithelioid cells reminiscent of epithelioid hemangioendothelioma. Hemangioma-like foci also lined by hobnail endothelial cells were frequently present. Mitotic activity was typically

Published

2017

15. Gastroblastoma harbors a recurrent somatic MALAT1–GLI1 fusion gene

Author

Asha Nair, Jaime I. Davila, Andrew L. Folpe, Rondell P. Graham, Sara M. Kloft-Nelson, Henry D. Appelman, Ryan A. Knudson, Long Jin, William R. Sukov, Jorge Torres-Mora, Kyle D. Perry, Patricia T. Greipp, Lizhi Zhang, Jin Jen, and Tsung Teh Wu

Subjects

Adult, Male, 0301 basic medicine, Pathology, medicine.medical_specialty, Oncogene Proteins, Fusion, Biphasic Synovial Sarcoma, Biology, Zinc Finger Protein GLI1, Pathology and Forensic Medicine, Fusion gene, 03 medical and health sciences, 0302 clinical medicine, Stomach Neoplasms, GLI1, medicine, Humans, Stromal tumor, Child, MALAT1, integumentary system, Middle Aged, medicine.disease, Neoplasms, Complex and Mixed, Hedgehog signaling pathway, Gene expression profiling, 030104 developmental biology, 030220 oncology & carcinogenesis, biology.protein, Female, RNA, Long Noncoding, Sarcoma

Abstract

Gastroblastoma is a rare distinctive biphasic tumor of the stomach. The molecular biology of gastroblastoma has not been studied, and no affirmative diagnostic markers have been developed. We retrieved two gastroblastomas from the consultation practices of the authors and performed transcriptome sequencing on formalin-fixed paraffin-embedded tissue. Recurrent predicted fusion genes were validated at genomic and RNA levels. The presence of the fusion gene was confirmed on two additional paraffin-embedded cases of gastroblastoma. Control cases of histologic mimics (biphasic synovial sarcoma, leiomyoma, leiomyosarcoma, desmoid-type fibromatosis, EWSR1-FLI1-positive Ewing sarcoma, Wilms' tumor, gastrointestinal stromal tumor, plexiform fibromyxoma, Sonic hedgehog-type medulloblastomas, and normal gastric mucosa and muscularis propria were also analyzed. The gastroblastomas affected two males and two females aged 9-56 years. Transcriptome sequencing identified recurrent somatic MALAT1-GLI1 fusion genes, which were predicted to retain the key domains of GLI1. The MALAT1-GLI1 fusion gene was validated by break-apart and dual-fusion FISH and RT-PCR. The additional two gastroblastomas were also positive for the MALAT1-GLI1 fusion gene. None of the other control cases harbored MALAT1-GLI1. Overexpression of GLI1 in the cases of gastroblastomas was confirmed at RNA and protein levels. Pathway analysis revealed activation of the Sonic hedgehog pathway in gastroblastoma and gene expression profiling showed that gastroblastomas grouped together and were most similar to Sonic hedgehog-type medulloblastomas. In summary, we have identified an oncogenic MALAT1-GLI1 fusion gene in all cases of gastroblastoma that may serve as a diagnostic biomarker. The fusion gene is predicted to encode a protein that includes the zinc finger domains of GLI1 and results in overexpression of GLI1 protein and activation of the Sonic hedgehog pathway.

Published

2017

16. Network-directed cis-mediator analysis of normal prostate tissue expression profiles reveals downstream regulatory associations of prostate cancer susceptibility loci

Author

Melissa C. Larson, Jaime I. Davila, Saurabh Baheti, John C. Cheville, Asha Nair, Shannon K. McDonnell, Shaun M. Riska, Liang Wang, Stephen N. Thibodeau, Daniel J. Schaid, Alexandra M Weber, Daniel R. O'Brien, Nicholas B. Larson, and Zach Fogarty

Subjects

0301 basic medicine, medicine.medical_specialty, Locus (genetics), genetic risk, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, medicine, MSMB, mediation, Gene, Genetic association, Genetics, business.industry, expression quantitative trait loci, Anatomical pathology, medicine.disease, HNF1B, prostate cancer, 3. Good health, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Expression quantitative trait loci, business, Research Paper

Abstract

// Nicholas B. Larson 1 , Shannon K. McDonnell 1 , Zach Fogarty 1 , Melissa C. Larson 1 , John Cheville 2 , Shaun Riska 1 , Saurabh Baheti 1 , Alexandra M. Weber 3 , Asha A. Nair 1 , Liang Wang 4 , Daniel O’Brien 1 , Jaime Davila 1 , Daniel J. Schaid 1 and Stephen N. Thibodeau 5 1 Division of Biomedical Statistics and Informatics, Department of Health Sciences Research, Mayo Clinic, Rochester, MN, USA 2 Division of Anatomic Pathology, Department of Laboratory Medicine and Pathology, Mayo Clinic, Rochester, MN, USA 3 Department of Computational Medicine and Bioinformatics, University of Michigan, Ann Arbor, MI, USA 4 Department of Pathology, Medical College of Wisconsin, Milwaukee, WI, USA 5 Division of Laboratory Genetics, Department of Laboratory Medicine and Pathology, Mayo Clinic, Rochester, MN, USA Correspondence to: Nicholas B. Larson, email: Larson.nicholas@mayo.edu Keywords: prostate cancer, genetic risk, expression quantitative trait loci, mediation Received: April 26, 2017 Accepted: July 29, 2017 Published: September 08, 2017 ABSTRACT Large-scale genome-wide association studies have identified multiple single-nucleotide polymorphisms associated with risk of prostate cancer. Many of these genetic variants are presumed to be regulatory in nature; however, follow-up expression quantitative trait loci (eQTL) association studies have to-date been restricted largely to cis -acting associations due to study limitations. While trans -eQTL scans suffer from high testing dimensionality, recent evidence indicates most trans -eQTL associations are mediated by cis -regulated genes, such as transcription factors. Leveraging a data-driven gene co-expression network, we conducted a comprehensive cis -mediator analysis using RNA-Seq data from 471 normal prostate tissue samples to identify downstream regulatory associations of previously identified prostate cancer risk variants. We discovered multiple trans -eQTL associations that were significantly mediated by cis -regulated transcripts, four of which involved risk locus 17q12, proximal transcription factor HNF1B , and target trans -genes with known HNF response elements ( MIA2 , SRC , SEMA6A , KIF12 ). We additionally identified evidence of cis -acting down-regulation of MSMB via rs10993994 corresponding to reduced co-expression of NDRG1 . The majority of these cis -mediator relationships demonstrated trans -eQTL replicability in 87 prostate tissue samples from the Gene-Tissue Expression Project. These findings provide further biological context to known risk loci and outline new hypotheses for investigation into the etiology of prostate cancer.

Published

2017

17. Leiomyoma with KAT6B-KANSL1 fusion: case report of a rapidly enlarging uterine mass in a postmenopausal woman

Author

Jaime I. Davila, Nooshin K. Dashti, Rohini Mopuri, Kevin C. Halling, Rory A. Jackson, Taofic Mounajjed, Karen J. Fritchie, Alessandra J. Ainsworth, J. Kenneth Schoolmeester, and Jamie N. Bakkum-Gamez

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Histology, Uterus, Asymptomatic, Pathology and Forensic Medicine, MED12, 03 medical and health sciences, 0302 clinical medicine, HMGA2, lcsh:Pathology, medicine, Humans, neoplasms, KAT6B-KANSL1, Aged, Histone Acetyltransferases, Uterine leiomyoma, Leiomyoma, biology, business.industry, Nuclear Proteins, General Medicine, medicine.disease, female genital diseases and pregnancy complications, Menopause, surgical procedures, operative, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Uterine Neoplasms, biology.protein, Female, Sarcoma, Gene Fusion, medicine.symptom, business, lcsh:RB1-214

Abstract

Background Uterine leiomyomas, in contrast to sarcomas, tend to cease growth following menopause. In the setting of a rapidly enlarging uterine mass in a postmenopausal patient, clinical distinction of uterine leiomyoma from sarcoma is difficult and requires pathologic examination. Case presentation A 74-year-old woman presented with postmenopausal bleeding and acute blood loss requiring transfusion. She was found to have a rapidly enlarging uterine mass clinically suspicious for sarcoma. An abdominal hysterectomy and bilateral salpingo-oophorectomy were performed. A 15.5 cm partially necrotic intramural mass was identified in the uterine corpus. The tumor was classified as a cellular leiomyoma. RNA sequencing identified a KAT6B-KANSL1 fusion that was confirmed by RT-PCR and Sanger sequencing. After 6 months of follow-up, the patient remains asymptomatic without evidence of disease. Conclusion Prior studies of uterine leiomyomas have identified KAT6B (previously MORF) rearrangements in uterine leiomyomas, but this case is the first to identify a KAT6B-KANSL1 gene fusion in a uterine leiomyoma. While alterations of MED12 and HMGA2 are most common in uterine leiomyomas, a range of other genetic pathways have been described. Our case contributes to the evolving molecular landscape of uterine leiomyomas.

Published

2019

18. Abstract B18: Transcriptional profiling of tumor stroma using ovarian cancer PDX models with induced platinum-resistance

Author

Yuanhang Liu, Beverly Long, Pritha Chanana, Jaime I. Davila, Joe Pathoulas, Brad Evans, Valentina Zanfagnin, Saravut J. Weroha, Xiaonan Pritha, and Chen Wang

Subjects

Cancer Research, Tumor microenvironment, Stromal cell, Biology, medicine.disease, Carboplatin, chemistry.chemical_compound, Oncology, Stroma, SOX2, Downregulation and upregulation, Paclitaxel, chemistry, medicine, Cancer research, Ovarian cancer

Abstract

Introduction: Acquired resistance to platinum remains a major clinical problem in ovarian cancer since systemic therapies have limited efficacy in this setting. There is growing evidence that the tumor microenvironment (TME) contributes to such resistance, as well as the pathogenesis of the disease. The study of the TME is limited by technical challenges of separating the epithelial from the stromal component. To overcome this limitation, we performed RNA sequencing (RNA-Seq) for three pairs of sensitive and induced resistant patient-derived xenograft models since the epithelial transcripts originate from human tissue and the stroma component is murine. Methods: To determine which TME genes might be contributing to chemotherapy resistance, three platinum-sensitive ovarian cancer PDX lines were treated repeatedly with carboplatin/paclitaxel until resistance occurred. Primary platinum-sensitive and induced platinum resistant tumors were characterized histologically by H&E and Masson Trichrome staining. The three pairs of sensitive and resistant PDX models were then subjected to RNA-Seq. Raw sequencing data were processed through Xenome to classify the reads into epithelial carcinoma (human) or TME (mouse) through Mayo Clinic’s internal RNA-Seq pipeline for transcriptome quantification. Differential expression analysis between induced resistant and sensitive models was carried out for both carcinoma and TME components using edgeR paired analysis. Gene set enrichment analysis was used to identify overrepresented biologic functions for differentially expressed genes between the pairs. Top significantly varied, differentially expressed genes between the pairs were validated using species-specific qPCR. Results: Histologic analysis of the matched sensitive/resistant pairs revealed a marked increase of the stromal component in the resistant tumors evident by H&E and Masson trichrome staining. A total number of 95 and 312 genes were differentially expressed in the epithelial and TME component, respectively (FDR1.5). The stemness marker SOX2 was significantly upregulated in the human component of the resistant tumors as confirmed by qPCR. Genes involved in stroma remodeling were upregulated in the “murine” component of the resistant tumors, and upregulation was confirmed by qPCR (normalized to a murine housekeeper gene). Gene set enrichment analysis showed that the upregulated genes in TME of resistant models were enriched for cytoskeleton related functions, while the downregulated genes were enriched for extracellular matrix-related functions. Conclusion: A bioinformatics strategy able to map human and murine reads separately may identify resistance mechanisms attributed to the two tumor subcompartments and could lead to strategies to potentially target each separately or concurrently. Citation Format: Valentina Zanfagnin, Yuanhang Liu, Pritha Chanana, Xiaonan Pritha, Beverly Long, Joe Pathoulas, Brad Evans, Jaime Davila, Chen Wang, Saravut John Weroha. Transcriptional profiling of tumor stroma using ovarian cancer PDX models with induced platinum-resistance [abstract]. In: Proceedings of the AACR Special Conference on Advances in Ovarian Cancer Research; 2019 Sep 13-16, 2019; Atlanta, GA. Philadelphia (PA): AACR; Clin Cancer Res 2020;26(13_Suppl):Abstract nr B18.

Published

2020

19. TP53mutations, tetraploidy and homologous recombination repair defects in early stage high-grade serous ovarian cancer

Author

Jeremy Chien, R. Keira Cheetham, Yan W. Asmann, Ellen L. Goode, Jean Pierre A. Kocher, Lynn C. Hartmann, Scott H. Kaufmann, Russell J. Grocock, Julie M. Cunningham, Yaman Tarabishy, Steven N. Hart, John F. Peden, Ann L. Oberg, Ying Li, Kimberly R. Kalli, Rui Kuang, Marina Bibikova, David Bentley, Jaime I. Davila, Elizabeth J. Atkinson, Saurabh Baheti, Sabine Dietmann, Viji Shridhar, Chen Wang, Debra A. Bell, Takayo Ota, Elizabeth M. Swisher, Jian-Bing Fan, Hugues Sicotte, and Sean Humphray

Subjects

p53, Mutation rate, endocrine system diseases, Somatic cell, Loss of Heterozygosity, DNA Primase, Biology, Loss of heterozygosity, 03 medical and health sciences, Rare Diseases, 0302 clinical medicine, Mutation Rate, Information and Computing Sciences, Genetics, Carcinoma, medicine, Humans, 2.1 Biological and endogenous factors, neoplasms, Cancer, 030304 developmental biology, Ovarian Neoplasms, 0303 health sciences, Prevention, Human Genome, Recombinational DNA Repair, Genomics, Biological Sciences, Genes, p53, medicine.disease, BRCA2 Protein, Molecular biology, Ovarian Cancer, 3. Good health, Tetraploidy, Genes, 030220 oncology & carcinogenesis, Mutation, Cancer research, Female, Ploidy, Homologous recombination, Ovarian cancer, Environmental Sciences, Biotechnology, Developmental Biology

Abstract

To determine early somatic changes in high-grade serous ovarian cancer (HGSOC), we performed whole genome sequencing on a rare collection of 16 low stage HGSOCs. The majority showed extensive structural alterations (one had an ultramutated profile), exhibited high levels of p53 immunoreactivity, and harboured a TP53 mutation, deletion or inactivation. BRCA1 and BRCA2 mutations were observed in two tumors, with nine showing evidence of a homologous recombination (HR) defect. Combined Analysis with The Cancer Genome Atlas (TCGA) indicated that low and late stage HGSOCs have similar mutation and copy number profiles. We also found evidence that deleterious TP53 mutations are the earliest events, followed by deletions or loss of heterozygosity (LOH) of chromosomes carrying TP53, BRCA1 or BRCA2. Inactivation of HR appears to be an early event, as 62.5% of tumours showed a LOH pattern suggestive of HR defects. Three tumours with the highest ploidy had little genome-wide LOH, yet one of these had a homozygous somatic frame-shift BRCA2 mutation, suggesting that some carcinomas begin as tetraploid then descend into diploidy accompanied by genome-wide LOH. Lastly, we found evidence that structural variants (SV) cluster in HGSOC, but are absent in one ultramutated tumor, providing insights into the pathogenesis of low stage HGSOC.

Published

2015

20. Inherited Mutations in 17 Breast Cancer Susceptibility Genes Among a Large Triple-Negative Breast Cancer Cohort Unselected for Family History of Breast Cancer

Author

Angela Cox, Heli Nevanlinna, Judy Garber, Liisa M. Pelttari, Florentia Fostira, Arif B. Ekici, Xianshu Wang, Susan L. Slager, Lorraine Durcan, Penelope Miron, Drakoulis Yannoukakos, Seth W. Slettedahl, William J. Tapper, Curtis Olswold, Brigitte Rack, Wolfgang Janni, Celine M. Vachon, Jaime I. Davila, Irene Konstantopoulou, Charles L. Shapiro, Robert Pilarski, Fergus J. Couch, Lucia Guidugli, Hiltrud Brauch, Peter A. Fasching, V. Shane Pankratz, Athanassios Vratimos, Priyanka Sharma, Diana Eccles, Matthias W. Beckmann, George Fountzilas, Simon S. Cross, Christine B. Ambrosone, Emily Hallberg, Song Yao, Janet E. Olson, Jennifer R. Klemp, Andrew K. Godwin, Dennis J. Slamon, Steven N. Hart, and Amanda E. Toland

Subjects

Adult, Oncology, Cancer Research, medicine.medical_specialty, PALB2, DNA Mutational Analysis, Triple Negative Breast Neoplasms, Cohort Studies, Young Adult, Germline mutation, Breast cancer, Internal medicine, medicine, Humans, Genetic Predisposition to Disease, Genetic Testing, Family history, Germ-Line Mutation, Triple-negative breast cancer, Aged, Genetic testing, Aged, 80 and over, BRCA2 Protein, Family Health, Ovarian Neoplasms, Genetics, medicine.diagnostic_test, BRCA1 Protein, business.industry, Cancer, Middle Aged, medicine.disease, 3. Good health, Female, business

Abstract

Purpose Recent advances in DNA sequencing have led to the development of breast cancer susceptibility gene panels for germline genetic testing of patients. We assessed the frequency of mutations in 17 predisposition genes, including BRCA1 and BRCA2, in a large cohort of patients with triple-negative breast cancer (TNBC) unselected for family history of breast or ovarian cancer to determine the utility of germline genetic testing for those with TNBC. Patients and Methods Patients with TNBC (N = 1,824) unselected for family history of breast or ovarian cancer were recruited through 12 studies, and germline DNA was sequenced to identify mutations. Results Deleterious mutations were identified in 14.6% of all patients. Of these, 11.2% had mutations in the BRCA1 (8.5%) and BRCA2 (2.7%) genes. Deleterious mutations in 15 other predisposition genes were detected in 3.7% of patients, with the majority observed in genes involved in homologous recombination, including PALB2 (1.2%) and BARD1, RAD51D, RAD51C, and BRIP1 (0.3% to 0.5%). Patients with TNBC with mutations were diagnosed at an earlier age (P < .001) and had higher-grade tumors (P = .01) than those without mutations. Conclusion Deleterious mutations in predisposition genes are present at high frequency in patients with TNBC unselected for family history of cancer. Mutation prevalence estimates suggest that patients with TNBC, regardless of age at diagnosis or family history of cancer, should be considered for germline genetic testing of BRCA1 and BRCA2. Although mutations in other predisposition genes are observed among patients with TNBC, better cancer risk estimates are needed before these mutations are used for clinical risk assessment in relatives.

Published

2015

21. Development and Verification of an RNA Sequencing (RNA-Seq) Assay for the Detection of Gene Fusions in Tumors

Author

Eric W. Klee, Amber McDonald, Jadee L. Neff, Benjamin R. Kipp, Jessica R. Balcom, Gavin R. Oliver, Brittany C. Thomas, Jin Jen, Robert B. Jenkins, Jesse S. Voss, Kevin C. Halling, Umut Aypar, Numrah Fadra, Long Jin, Jaime I. Davila, Xianglin Wu, Kandelaria M. Rumilla, Asha Nair, Rebecca N. Wehrs, Rondell P. Graham, and Jennifer L. Winters

Subjects

0301 basic medicine, Sequence analysis, RNA Stability, RNA-Seq, Biology, Sensitivity and Specificity, Pathology and Forensic Medicine, 03 medical and health sciences, Limit of Detection, Complementary DNA, Neoplasms, medicine, Humans, Oncogene Fusion, RNA, Neoplasm, Gene, Regulation of gene expression, medicine.diagnostic_test, Sequence Analysis, RNA, RNA, Cancer, Reproducibility of Results, medicine.disease, Molecular biology, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Molecular Medicine, Fluorescence in situ hybridization

Abstract

We assessed the performance characteristics of an RNA sequencing (RNA-Seq) assay designed to detect gene fusions in 571 genes to help manage patients with cancer. Polyadenylated RNA was converted to cDNA, which was then used to prepare next-generation sequencing libraries that were sequenced on an Illumina HiSeq 2500 instrument and analyzed with an in-house developed bioinformatic pipeline. The assay identified 38 of 41 gene fusions detected by another method, such as fluorescence in situ hybridization or RT-PCR, for a sensitivity of 93%. No false-positive gene fusions were identified in 15 normal tissue specimens and 10 tumor specimens that were negative for fusions by RNA sequencing or Mate Pair NGS (100% specificity). The assay also identified 22 fusions in 17 tumor specimens that had not been detected by other methods. Eighteen of the 22 fusions had not previously been described. Good intra-assay and interassay reproducibility was observed with complete concordance for the presence or absence of gene fusions in replicates. The analytical sensitivity of the assay was tested by diluting RNA isolated from gene fusion–positive cases with fusion-negative RNA. Gene fusions were generally detectable down to 12.5% dilutions for most fusions and as little as 3% for some fusions. This assay can help identify fusions in patients with cancer; these patients may in turn benefit from both US Food and Drug Administration–approved and investigational targeted therapies.

Published

2017

22. Comprehensive Genomic Profiling of a Rare Thyroid Follicular Dendritic Cell Sarcoma

Author

Jaime I. Davila, Gavin R. Oliver, John D. Casler, Yan W. Asmann, Alexander S. Parker, Jason S. Starr, Brian M. Necela, Jean Pierre A. Kocher, David M. Menke, E. Aubrey Thompson, Steven Attia, Robert C. Smallridge, Ryan A. Knudson, Vivekananda Sarangi, Yingxue Ren, Zhifu Sun, Richard W. Joseph, John A. Copland, and Chen Wang

Subjects

0301 basic medicine, fusion, Histology, Case Report, Biology, medicine.disease_cause, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, medicine, Missense mutation, PTEN, thyroid FDCS, Mutation, Chromothripsis, Point mutation, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 030104 developmental biology, Oncology, genomic rearrangement, 030220 oncology & carcinogenesis, Follicular dendritic cell sarcoma, genomic sequencing, Cancer research, biology.protein, Sarcoma, genomic sequencing, thyroid FDCS, genomic rearrangement, fusion, Carcinogenesis

Abstract

We previously reported an extremely rare case of follicular dendritic cell sarcoma (FDCS) presented as a thyroid mass. Given the rarity of this disease, there are no personalized and molecularly targeted treatment options due to the lack of knowledge in the genomic makeup of the tumor. A 44-year-old white woman was diagnosed with an extranodal FDCS in thyroid. The patient underwent a total thyroidectomy, central compartment dissection, parathyroid re-implantation, and adjuvant radiation therapy. Tumor DNA sequencing of 236 genes by FoundationOne panel found truncating mutations in PTEN and missense mutations in RET and TP53. However, patient-matched germline DNA was not sequenced which is critical for identification of true somatic mutations. Furthermore, the FoundationOne panel doesn't measure genomic rearrangements which have been shown to be abundant in sarcomas and are associated with sarcoma tumorigenesis and progression. In the current study, we carried out comprehensive genomic sequencing of the tumor, adjacent normal tissues, and patient-matched blood, in an effort to understand the genomic makeup of this rare extranodal FDCS and to identify potential therapeutic targets. Eighty-one somatic point mutations were identified in tumor but not in adjacent normal tissues or blood. A clonal truncating mutation in the CLTCL1 gene, which stabilizes the mitotic spindle, was likely a driver mutation of tumorigenesis and could explain the extensive copy number aberrations (CNAs) and genomic rearrangements in the tumor including a chr15/chr17 local chromothripsis resulted in 6 expressed fusion genes. The fusion gene HDGFRP3→SHC4 led to a 200-fold increase in the expression of oncogene SHC4 which is a potential target of the commercial drug Dasatinib. Missense mutations in ATM and splice-site mutation in VEGFR1 were also detected in addition to the TP53 missense mutation reported by FoundationOne.

Published

2017

23. NovelTRAF1-ALKfusion identified by deep RNA sequencing of anaplastic large cell lymphoma

Author

George Vasmatzis, Yan W. Asmann, Ariel J. Caride, Jaime I. Davila, Andrew L. Feldman, Julie C. Porcher, Stephen M. Ansell, Sarah H. Johnson, Bruce W. Eckloff, and Sumit Middha

Subjects

Sanger sequencing, Cancer Research, Biology, medicine.disease, Fusion protein, Molecular biology, Deep sequencing, Fusion gene, symbols.namesake, Fusion transcript, Chimeric RNA, hemic and lymphatic diseases, Genetics, symbols, medicine, Anaplastic lymphoma kinase, Anaplastic large-cell lymphoma

Abstract

Chromosomal translocations leading to expression of abnormal fusion proteins play a major role in the pathogenesis of various hematologic malignancies. The recent development of high-throughput, "deep" sequencing has allowed discovery of novel translocations leading to a rapid increase in understanding these diseases. Translocations involving the anaplastic lymphoma kinase (ALK) gene leading to ALK fusion proteins originally were discovered in anaplastic large cell lymphomas (ALCLs). Among ALCLs, NPM1-ALK fusions are most common and lead to nuclear localization of the fusion protein. Here, we present a 50-year-old male with ALCL demonstrating cytoplasmic ALK immunoreactivity only, suggesting the presence of a non-NPM1 fusion partner. We performed deep RNA sequencing of tumor tissue from this patient and identified a novel transcript fusing Exon 6 of TRAF1 to Exon 20 of ALK. The TRAF1-ALK fusion transcript was confirmed at the mRNA level by Sanger sequencing and the fusion protein was visualized by Western blot. The discovery of this TRAF1-ALK fusion expands the diversity of known ALK fusion partners and highlights the power of deep sequencing for fusion transcript discovery. © 2013 Wiley Periodicals, Inc.

Published

2013

24. Integrated mate-pair and RNA sequencing identifies novel, targetable gene fusions in peripheral T-cell lymphoma

Author

George Vasmatzis, Yan W. Asmann, Brian K. Link, Yu Zeng, Julie C. Porcher, Sarah H. Johnson, Ryan A. Knudson, Guangzhen Hu, Surendra Dasari, Jaime I. Davila, Mark A. McNiven, Bruce W. Eckloff, Patricia T. Greipp, James B. Smadbeck, Paul J. Kurtin, Andrew L. Feldman, James R. Cerhan, Daniel D. Billadeau, Gina L. Razidlo, Rebecca L. Boddicker, and Stephen M. Ansell

Subjects

0301 basic medicine, Male, VAV1, Oncogene Proteins, Fusion, Immunology, Biology, Biochemistry, Fusion gene, 03 medical and health sciences, Jurkat Cells, Mice, 0302 clinical medicine, medicine, Animals, Humans, Anaplastic large-cell lymphoma, Gene, Aged, Genetics, medicine.diagnostic_test, High-Throughput Nucleotide Sequencing, Lymphoma, T-Cell, Peripheral, Cell Biology, Hematology, Middle Aged, medicine.disease, Peripheral T-cell lymphoma, Lymphoma, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer research, NIH 3T3 Cells, Ectopic expression, Female, Fluorescence in situ hybridization

Abstract

Peripheral T-cell lymphomas (PTCLs) represent a heterogeneous group of T-cell malignancies that generally demonstrate aggressive clinical behavior, often are refractory to standard therapy, and remain significantly understudied. The most common World Health Organization subtype is PTCL, not otherwise specified (NOS), essentially a “wastebasket” category because of inadequate understanding to assign cases to a more specific diagnostic entity. Identification of novel fusion genes has contributed significantly to improving the classification, biologic understanding, and therapeutic targeting of PTCLs. Here, we integrated mate-pair DNA and RNA next-generation sequencing to identify chromosomal rearrangements encoding expressed fusion transcripts in PTCL, NOS. Two of 11 cases had novel fusions involving VAV1, encoding a truncated form of the VAV1 guanine nucleotide exchange factor important in T-cell receptor signaling. Fluorescence in situ hybridization studies identified VAV1 rearrangements in 10 of 148 PTCLs (7%). These were observed exclusively in PTCL, NOS (11%) and anaplastic large cell lymphoma (11%). In vitro, ectopic expression of a VAV1 fusion promoted cell growth and migration in a RAC1-dependent manner. This growth was inhibited by azathioprine, a clinically available RAC1 inhibitor. We also identified novel kinase gene fusions, ITK-FER and IKZF2-ERBB4, as candidate therapeutic targets that show similarities to known recurrent oncogenic ITK-SYK fusions and ERBB4 transcript variants in PTCLs, respectively. Additional novel and potentially clinically relevant fusions also were discovered. Together, these findings identify VAV1 fusions as recurrent and targetable events in PTCLs and highlight the potential for clinical sequencing to guide individualized therapy approaches for this group of aggressive malignancies.

Published

2016

25. Proteomic detection of immunoglobulin light chain variable region peptides from amyloidosis patient biopsies

Author

Julie A. Vrana, Ahmet Dogan, Paul J. Kurtin, Vivekananda Sarangi, Roman M. Zenka, Renee C. Tschumper, Diane F. Jelinek, Surendra Dasari, Patrick Quint, Prasuna Muppa, Jaime I. Davila, Oana M. Meureta, and Jason D. Theis

Subjects

Proteomics, Amyloid, biology, Amyloidosis, Immunoglobulin Variable Region, Computational Biology, General Chemistry, Plasma cell neoplasm, Immunoglobulin light chain, Proteogenomics, medicine.disease, Biochemistry, Molecular biology, Subtyping, Cohort Studies, AL amyloidosis, medicine, biology.protein, Humans, Immunoglobulin Light Chains, Antibody, Clone (B-cell biology), Peptides

Abstract

Immunoglobulin light chain (LC) amyloidosis (AL) is caused by deposition of clonal LCs produced by an underlying plasma cell neoplasm. The clonotypic LC sequences are unique to each patient, and they cannot be reliably detected by either immunoassays or standard proteomic workflows that target the constant regions of LCs. We addressed this issue by developing a novel sequence template-based workflow to detect LC variable (LCV) region peptides directly from AL amyloid deposits. The workflow was implemented in a CAP/CLIA compliant clinical laboratory dedicated to proteomic subtyping of amyloid deposits extracted from either formalin-fixed paraffin-embedded tissues or subcutaneous fat aspirates. We evaluated the performance of the workflow on a validation cohort of 30 AL patients, whose amyloidogenic clone was identified using a novel proteogenomics method, and 30 controls. The recall and negative predictive values of the workflow, when identifying the gene family of the AL clone, were 93 and 98%, respectively. Application of the workflow on a clinical cohort of 500 AL amyloidosis samples highlighted a bias in the LCV gene families used by the AL clones. We also detected similarity between AL clones deposited in multiple organs of systemic AL patients. In summary, AL proteomic data sets are rich in LCV region peptides of potential clinical significance that are recoverable with advanced bioinformatics.

Published

2015

26. RNA toxicity and missplicing in the common eye disease fuchs endothelial corneal dystrophy

Author

Jaime I. Davila, Eric D. Wieben, Sanjay V. Patel, Joel M. Gottesfeld, Xiaojia Tang, Elisabetta Soragni, Jean-Pierre A. Kocher, Ross A. Aleff, Keith H. Baratz, Jinfu Nie, Jintang Du, and Krishna R. Kalari

Subjects

Fuchs Endothelial Dystrophy, RNA Splicing, Context (language use), RNA-binding protein, Biology, Eye, Biochemistry, Myotonic dystrophy, Cornea, chemistry.chemical_compound, Transcription Factor 4, RNA Foci, medicine, MBNL1, Humans, Fuchs Corneal Dystrophy, RNA, Messenger, Molecular Biology, Trinucleotide Repeat Disease, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors, Fuchs' Endothelial Dystrophy, RNA, RNA-Binding Proteins, Molecular Bases of Disease, Cell Biology, medicine.disease, Molecular biology, Alternative Splicing, chemistry, RNA splicing, RNA Toxicity, Cancer research, Trinucleotide repeat expansion, Trinucleotide Repeat Expansion, Transcription Factors

Abstract

Background: Expansion of intronic (CTG·CAG)n repeats in TCF4 is found in most Fuchs endothelial corneal dystrophy (FECD) patients. Results: RNA foci co-localizing with the splicing factor MBNL1 are found in FECD cells, and changes in mRNA splicing occur. Conclusion: Trinucleotide repeat expansion in FECD is associated with RNA focus formation and missplicing. Significance: RNA toxicity occurs in a disease affecting millions of patients., Fuchs endothelial corneal dystrophy (FECD) is an inherited degenerative disease that affects the internal endothelial cell monolayer of the cornea and can result in corneal edema and vision loss in severe cases. FECD affects ∼5% of middle-aged Caucasians in the United States and accounts for >14,000 corneal transplantations annually. Among the several genes and loci associated with FECD, the strongest association is with an intronic (CTG·CAG)n trinucleotide repeat expansion in the TCF4 gene, which is found in the majority of affected patients. Corneal endothelial cells from FECD patients harbor a poly(CUG)n RNA that can be visualized as RNA foci containing this condensed RNA and associated proteins. Similar to myotonic dystrophy type 1, the poly(CUG)n RNA co-localizes with and sequesters the mRNA-splicing factor MBNL1, leading to missplicing of essential MBNL1-regulated mRNAs. Such foci and missplicing are not observed in similar cells from FECD patients who lack the repeat expansion. RNA-Seq splicing data from the corneal endothelia of FECD patients and controls reveal hundreds of differential alternative splicing events. These include events previously characterized in the context of myotonic dystrophy type 1 and epithelial-to-mesenchymal transition, as well as splicing changes in genes related to proposed mechanisms of FECD pathogenesis. We report the first instance of RNA toxicity and missplicing in a common non-neurological/neuromuscular disease associated with a repeat expansion. The FECD patient population with this (CTG·CAG)n trinucleotide repeat expansion exceeds that of the combined number of patients in all other microsatellite expansion disorders.

Published

2015

27. IL-33 facilitates oncogene-induced cholangiocarcinoma in mice by an interleukin-6-sensitive mechanism

Author

Gregory J. Gores, Steven F. Bronk, Jorge A. Bezerra, Mitesh J. Borad, Mia D. Champion, Xin Chen, Jaime I. Davila, Sumera Rizvi, Daisaku Yamada, and Nataliya Razumilava

Subjects

Male, Pathology, Cell Cycle Proteins, Medical Biochemistry and Metabolomics, medicine.disease_cause, Inbred C57BL, Cholangiocarcinoma, Mice, Fibrosis, Models, Tumor Cells, Cultured, 2.1 Biological and endogenous factors, Aetiology, Cancer, Intrahepatic, Cultured, Liver Disease, Interleukin, Adaptor Proteins, Tumor Cells, Biliary tract, Liver Cancer, medicine.medical_specialty, Clinical Sciences, Immunology, Biology, Proinflammatory cytokine, Rare Diseases, Genetic, medicine, Genetics, Animals, Humans, Protein kinase B, Digestive Diseases - (Gallbladder), Adaptor Proteins, Signal Transducing, Hepatology, Oncogene, Gastroenterology & Hepatology, Models, Genetic, Interleukin-6, Interleukins, Signal Transducing, YAP-Signaling Proteins, Oncogenes, medicine.disease, Interleukin-33, Phosphoproteins, Interleukin 33, Mice, Inbred C57BL, Bile Ducts, Intrahepatic, Bile Duct Neoplasms, Bile Ducts, Carcinogenesis, Digestive Diseases, Proto-Oncogene Proteins c-akt

Abstract

Cholangiocarcinoma (CCA) is a lethal hepatobiliary neoplasm originating from the biliary apparatus. In humans, CCA risk factors include hepatobiliary inflammation and fibrosis. The recently identified interleukin (IL)−1 family member, IL-33, has been shown to be a biliary mitogen which also promotes liver inflammation and fibrosis. Our aim was to generate a mouse model of CCA mimicking the human disease. Ectopic oncogene expression in the biliary tract was accomplished by the Sleeping Beauty transposon transfection system with transduction of constitutively active AKT (myr-AKT) and Yes-associated protein. Intrabiliary instillation of the transposon–transposase complex was coupled with lobar bile duct ligation in C57BL/6 mice, followed by administration of IL-33 for 3 consecutive days. Tumors developed in 72% of the male mice receiving both oncogenes plus IL-33 by 10 weeks but in only 20% of the male mice transduced with the oncogenes alone. Tumors expressed SOX9 and pancytokeratin (features of CCA) but were negative for HepPar1 (a marker of hepatocellular carcinoma). Substantive overlap with human CCA specimens was revealed by RNA profiling. Not only did IL-33 induce IL-6 expression by human cholangiocytes but it likely facilitated tumor development in vivo by an IL-6–sensitive process as tumor development was significantly attenuated in Il-6–/– male animals. Furthermore, tumor formation occurred at a similar rate when IL-6 was substituted for IL-33 in this model. Conclusion: The transposase-mediated transduction of constitutively active AKT and Yes-associated protein in the biliary epithelium coupled with lobar obstruction and IL-33 administration results in the development of CCA with morphological and biochemical features of the human disease; this model highlights the role of inflammatory cytokines in CCA oncogenesis. (Hepatology 2015;61:1627–1642)

Published

2014

28. Clinical characteristics of ovarian cancer classified by BRCA1, BRCA2, and RAD51C status

Author

Melissa C. Larson, P Pharoah, Jian-Bing Fan, Jeremy Chien, Boris Winterhoff, Brooke L. Fridley, Ellen L. Goode, Ed Dicks, Jaime I. Davila, Honglin Song, Patricia Harrington, Noralane M. Lindor, Julie M. Cunningham, Chen Wang, Kimberly R. Kalli, Myra J. Wick, Mine S. Cicek, Nicholas B. Larson, Marina Bibikova, Gottfried E. Konecny, Habib Hamidi, Song, Honglin [0000-0001-5076-7371], Dicks, Ed [0000-0002-0617-0401], Pharoah, Paul [0000-0001-8494-732X], and Apollo - University of Cambridge Repository

Subjects

endocrine system diseases, Biology, Carcinoma, Ovarian Epithelial, medicine.disease_cause, Germline, Article, Rare Diseases, Germline mutation, Neoplasms, Ovarian Epithelial, Breast Cancer, Genetics, Carcinoma, medicine, 2.1 Biological and endogenous factors, Humans, Neoplasms, Glandular and Epithelial, Aetiology, Homologous Recombination, skin and connective tissue diseases, Cancer, BRCA2 Protein, Ovarian Neoplasms, Mutation, Multidisciplinary, Base Sequence, BRCA1 Protein, Human Genome, Glandular and Epithelial, DNA, Sequence Analysis, DNA, DNA Methylation, Middle Aged, medicine.disease, female genital diseases and pregnancy complications, Ovarian Cancer, 3. Good health, DNA-Binding Proteins, Serous fluid, Cancer research, RAD51C, Female, Ovarian cancer, Sequence Analysis

Abstract

We evaluated homologous recombination deficient (HRD) phenotypes in epithelial ovarian cancer (EOC) considering BRCA1, BRCA2, and RAD51C in a large well-annotated patient set. We evaluated EOC patients for germline deleterious mutations (n = 899), somatic mutations (n = 279) and epigenetic alterations (n = 482) in these genes using NGS and genome-wide methylation arrays. Deleterious germline mutations were identified in 32 (3.6%) patients for BRCA1, in 28 (3.1%) for BRCA2 and in 26 (2.9%) for RAD51C. Ten somatically sequenced patients had deleterious alterations, six (2.1%) in BRCA1 and four (1.4%) in BRCA2. Fifty two patients (10.8%) had methylated BRCA1 or RAD51C. HRD patients with germline or somatic alterations in any gene were more likely to be high grade serous, have an earlier diagnosis age and have ovarian and/or breast cancer family history. The HRD phenotype was most common in high grade serous EOC. Identification of EOC patients with an HRD phenotype may help tailor specific therapies.

Published

2014

29. Gene Expression Profiling Identifies Distinct Signatures for Dysplastic and Proliferative Chronic Myelomonocytic Leukemia

Author

Luciana L. Almada, Jaime I. Davila, Ayalew Tefferi, Daniela Barraco, Rhett P. Ketterling, Naseema Gangat, Terra L. Lasho, Curtis A. Hanson, Ezequiel J. Tolosa, Nathalie Droin, Aref Al-Kali, Mrinal M. Patnaik, Martin E. Fernandez-Zapico, Christy Finke, and Eric Solary

Subjects

Chromosome 7 (human), medicine.medical_specialty, Monosomy, Myeloid, Immunology, Cytogenetics, Chronic myelomonocytic leukemia, Cell Biology, Hematology, Biology, medicine.disease, Trisomy 8, Biochemistry, Molecular biology, Fold change, Leukemia, medicine.anatomical_structure, hemic and lymphatic diseases, medicine

Abstract

Background : The 2016 revision to the World Health Organization classification of myeloid neoplasms has recommended distinction between "proliferative" (WBC ≥ 13 x 10(9)/L) and "dysplastic" (WBC < 13 X 10(9)/L) subtypes of chronic myelomonocytic leukemia (CMML). In addition, CMML is characterized by a spectrum of cytogenetic and molecular abnormalities (Patnaik Leukemia 2014). In the current study, we looked for correlations between gene expression profiles (GEP) and morphologic or molecular categories of previously untreated patients with CMML. Methods : 35 patients with CMML were included in the study. Targeted capture assays were carried out on BM DNA specimens obtained at diagnosis for 28 myeloid-relevant genes (Patnaik Blood C. J.). RNA sequencing (Stranded Total RNA- Illumina, San Diego, CA), was performed on 9 normal BM controls, and 35 CMML samples (25 peripheral blood (PB) and 10 BM). The RNA-Seq data was analyzed using MAPRSeq v.2.0. Normalization and differential expression analysis was performed using edgeR 2.6.2. We selected genes that were differentially expressed with a False Discovery Rate (FDR) Results: Among the 35 study patients, 75% were males and median age was 71 years (range, 55-87). 21 (60%), 9 (25%) and 5 (15%) patients were classified as CMML-0, 1 and 2, respectively. 16 (45%) had a dysplastic while 19 (55%) had a proliferative phenotype. At a median follow-up of 16 months, 5 (14%) deaths and 4 (14%) leukemic transformations were documented. Mutational frequencies included; TET2 45%, ASXL1 45%, SRSF2 40%, NRAS 14%, SETBP1 13%, CBL 10%, JAK2 7%, RUNX1 6%, DNMT3A 6%, U2AF1 6%, SF3B1 5%, ZRSR2 4%, Tp53 4%, and IDH2 4%. Abnormal cytogenetics (n=9, 35%) included; -Y 8%, trisomy 8 6%, monosomy 7 3%, del(13q) 3% and monosomal karyotype 3%. i) Differential GEP in PB samples: 25 PB CMML samples were analyzed. Unsupervised GEP demonstrated two unique clusters (figure one); cluster one was enriched with dysplastic CMML (90%) and cluster two with proliferative CMML (64%). Consistent with the difference in the distribution of morphologic categories, in comparison to cluster one, patients in cluster two had a higher white blood count (p=0.003), higher monocyte count (p=0.02) and higher risk prognostication by the Mayo Model (p=0.016); there was no significant difference between the two clusters in terms of age and gender distribution, hemoglobin level, neutrophil and platelet counts, PB or BM blast content, cytogenetic risk stratification, ASXL1, TET2, RAS, CBL and SETBP1 mutational status. Genes significantly upregulated (FDR ii) Differential GEP in BM samples: 10 BM CMML samples were analyzed along with 10 normal controls. Samples and controls clustered separately and within the CMML samples two clusters were identified (figure two). These clusters had equal representations of dysplastic (n=5) and proliferative (n=5) CMML sub-types. Additional samples are being processed. Conclusions: Differential gene expression profiling in patients with CMML identifies two unique clusters, clinically demarcated, at least in PB samples, by "proliferative" and "dysplastic" CMML subtypes. The proliferative cluster is enriched in genes involved in cell cycle regulation and DNA damage response; whereas the dysplastic cluster is enriched in T-cell receptor and STAT3 signalling. The prognostic and therapeutic impact of these gene clusters remains to be assessed in a larger group of informative patients. Figure 1. Figure 1. Figure 2. Figure 2. Disclosures Al-Kali: Novartis: Research Funding; Celgene: Research Funding.

Published

2016

30. Abstract 1894: Extensive genomic profiling of a rare extranodal-follicular dendritic cell sarcoma: Implications for future individualized therapy

Author

John A. Copland, Gavin R. Oliver, Richard W. Joseph, Xue Wang, Steven Attia, Casler John, Chen Wang, David M. Menke, Brian M. Necela, Yan W. Asmann, E. Aubrey Thompson, Alexander S. Parker, Robert C. Smallridge, Vivek Sarangi, Jaime I. Davila, and Jason S. Starr

Subjects

Genetics, Cancer Research, Mitotic spindle organization, Biology, medicine.disease, medicine.disease_cause, Fusion gene, MRNA Sequencing, Oncology, Fusion transcript, Follicular dendritic cell sarcoma, medicine, Copy-number variation, Carcinogenesis, Exome

Abstract

Background: Extranodal follicular dendritic cell sarcoma (FDCS) is an exceedingly rare tumor type that is limited to few cases in the literature. Given the rarity of this tumor, there is a lack of genetic understanding of this disease resulting in a non-individualized plan of care for patients with this disease. Herein, we are the first to describe extensively molecularly the DNA and RNA of this tumor. Methods: Under an IRB approved protocol, the patient's tumor and whole blood was freshly frozen for molecular analysis. We performed Next Generation Sequencing (NGS) genomic profiling including exome capture, mate pair and mRNA sequencing on this tumor. Exome and mRNA data were processed through Mayo's Bioinformatics Core standard pipelines, GENOME GPS 1.2.1 and MAPRSeq v1.2.1. Mutations and indels were prioritized depending on whether or not they belonged to known cancer associated genes. Copy number variations (CNVs) in Exome and Mate Pair data was found through PatternCNV v 1.0.1 and fusion transcripts were found using SNOWSHOES-FTD and Tophat-Fusion 2.0.6. Results: At the genomic level large scale genomic rearrangements were detected, including chr19 and chr20 trisomy, chr15q and chr17q segmental duplications result in two intra-chromosomal fusion genes, and translocations leading to four inter-chromosomal fusion genes between chr15 and chr17. Of particular interest is a stop codon gain in the CLTC1 (chr22) gene, which is involved in the mitotic spindle organization which has been associated with meningiomas and breast tumorigenesis. The new stop codon is before the site required for the recruitment of the proteins to the spindle. The large scale genomic rearrangement described above is consistent with this defective spindle assembly hypothesis. Another intriguing mutation detected in the VEGFR1 (chr13) gene leads to a 45% mis-spliced transcript. VEGFR1 is thought to modulate VEGFR2 which plays an essential role in angiogenesis, by acting as a decoy receptor. Therefore the loss of function of VEGFR1 might lead to hyper-activity of VEGFR2 pathway and a potential therapeutic strategy is to directly inhibit the VEGFR2 pathway. Furthermore missense mutations in the ATM (chr11) and TP53 (chr17) genes were found. PARP inhibitors have been used with success for cancer with defects in the ATM gene. Finally a novel fusion transcript of HDGRFP3 (chr15) and SHC4 (chr15) was identified. Such fusion results in an overexpressed SHC4 gene which has been associated with metastatic melanomas. Conclusions: In summary, genomic profiling of a rare thyroid FDCS identified drug targetable genes as well as changes related to tumor etiology. Future work is necessary to determine the functional significance of these molecular findings and whether they will predict benefit to targeted therapies. Citation Format: Jaime I. Davila, Jason Starr, Steven Attia, Chen Wang, Xue Wang, Brian Necela, Casler John, David Menke, Vivek Sarangi, Gavin Oliver, Richard Joseph, John Copland, Alexander Parker, E. Aubrey Thompson, Robert Smallridge, Yan W. Asmann. Extensive genomic profiling of a rare extranodal-follicular dendritic cell sarcoma: Implications for future individualized therapy. [abstract]. In: Proceedings of the 105th Annual Meeting of the American Association for Cancer Research; 2014 Apr 5-9; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2014;74(19 Suppl):Abstract nr 1894. doi:10.1158/1538-7445.AM2014-1894

Published

2014

31. Abstract 3462: Comparative RNA-Seq analysis of MIS signaling: Potential relevance as therapeutic strategy in ovarian cancer treatment

Author

Jaime I. Davila, Qing Zhang, Xueqian Yin, Eati Basal, William A. Cliby, and Edward B. Leof

Subjects

Cancer Research, DNA repair, Cell growth, Cancer, Biology, Bioinformatics, medicine.disease, Oncology, Downregulation and upregulation, Apoptosis, medicine, Cancer research, Signal transduction, Receptor, Gene

Abstract

Ovarian cancer (OC) is the fifth leading cause of cancer death in women in the US. Müllerian inhibiting substance (MIS) is a glycoprotein hormone that causes Müllerian duct regression through a complex of TGF- β family homologous receptors: a type II ligand-binding receptor (T2R) and a tissue-specific type I receptor (T1R) that initiates downstream signaling. MIS has been proposed as potential therapeutic agent in OC. We have previously shown that specific combination of T2R/T1R receptors are expressed on OC cells, however data is lacking on the MIS-dependent pathways activated in OC cells in a T1R-specific manner. These limitations hinder further development of MIS as a therapy. We sought to determine the downstream signaling pathways activated by MIS in a T1R specific manner. We designed a chimeric OC cell model system in which GM-CSF can function as the ligand to specifically activate candidate T2R/T1R combinations (MISRII with either ALK2, ALK3, or ALK6). RNA-Seq technology was used to identify differentially expressed early and late response genes. Over 15,032 genes were analyzed, restricted to genes in which there were > 32 counts for duplicate samples. Pathway analysis was performed using Ingenuity's Integrative Pathway Analysis Tool (IPA) for genes which were expressed over 2 fold, with an False Discovery Rate (FDR)-0.001. We observed 56, 37, and 51 early response (1hr) genes which were up- or down-regulated after stimulation in OC cells engineered to express either ALK2, ALK3, and ALK6, respectively. We identified a subset of 18 of genes (e.g., ID1, SMAD7, FOSB) which were upregulated after treatment in all MISRII/T1R combinations, suggesting redundancy amongst the three T1R partner receptors. These observations will be confirmed by RT-qPCR and immunoblotting. A majority of these redundant genes are known to play roles in TGF-β signaling and cell proliferation pathways. Importantly, as we have previously shown that not all T1R candidates are expressed in OC, we report subsets of genes (e.g., RASSF6, C/EBPBβ, CSMD3) which were uniquely altered after stimulation only in the presence of a specific T1R. This indicates specific pathway activation is dependent upon T1R expression pattern in OC and likely determines response. In addition to previously known TGF- β signaling pathway, we found gene signatures (e.g. FOSB, RASSF6, LRP1B, ID1) suggesting pathways which affect cell proliferation, apoptosis, chemotherapy resistance, and DNA repair in response to MIS. This is the first study to begin to define the specific roles candidate T1R's play in signaling in response to MIS in an OC model. An understanding of these pathways is a necessary prerequisite to examining MIS as a therapy. These preliminary data suggest a role for MIS in apoptosis, cytotoxic drug resistance and DNA repair. This can be used to test combination therapy with currently available drugs and MIS in OC treatment. Citation Format: Qing Zhang, Eati Basal, Jaime I. Davila, Xueqian Yin, Edward B. Leof, William A. Cliby. Comparative RNA-Seq analysis of MIS signaling: Potential relevance as therapeutic strategy in ovarian cancer treatment. [abstract]. In: Proceedings of the 105th Annual Meeting of the American Association for Cancer Research; 2014 Apr 5-9; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2014;74(19 Suppl):Abstract nr 3462. doi:10.1158/1538-7445.AM2014-3462

Published

2014

32. A tool to predict post-transcriptional instability related to the dysregulation of the SETD2 histone methyltransferase in renal cell carcinoma (RCC)

Author

Jean-Pierre A. Kocher, Huihuang Yan, A. Keith Stewart, Richard W. Joseph, Jared M. Evans, Mia D. Champion, Thai H. Ho, Raymond Moore, Jeong Heon Lee, Zhiguo Zhang, Jeff Nie, Jaime I. Davila, Eric Jonasch, and Tamas Ordog

Subjects

Cancer Research, biology, business.industry, Lysine, medicine.disease, Histone, Oncology, Renal cell carcinoma, SETD2, Histone methyltransferase, Cancer research, medicine, biology.protein, lipids (amino acids, peptides, and proteins), business

Abstract

11072 Background: Recent studies report that dysregulation of the SETD2 histone methyltransferase in (RCC) decreases global histone 3 lysine 36 trimethylation (H3K36me3), resulting in mis-regulatio...

Published

2014