Your search keyword '"Bennett A. Caughey"' showing total 12 results

1. Clinical impact of MAPK pathway alterations in advanced biliary tract cancer (BTC): SCRUM-Japan GOZILA and COLOMATE international collaboration

Author

Hideaki Takahashi, Bennett Adam Caughey, Kumiko Umemoto, Michelle Green, Yoshiaki Nakamura, Michael Datto, Makoto Ueno, Daniel Walden, Taito Esaki, Thomas Oliver, Yoshito Komatsu, Nobumasa Mizuno, Eiji Oki, Hiroya Taniguchi, Hideaki Bando, Chigusa Morizane, Takayuki Yoshino, John H Strickler, Masafumi Ikeda, and Tanios S. Bekaii-Saab

Subjects

Cancer Research, Oncology

Abstract

4086 Background: Abnormalities in the MAPK pathway are potential therapeutic targets in various cancers. However, the clinical impact of alterations in the MAPK pathway in BTC have not been elucidated, especially outside of canonical mutations in KRAS and BRAF. We investigated the clinical outcomes of advanced BTC with MAPK pathway alterations treated with chemotherapy in Japan and the United States. Methods: Patients with advanced BTC who received gemcitabine plus cisplatin as first-line therapy were included from the GOZILA study in Japan and Duke Molecular Registry of Tumors in the US. Genetic abnormalities were detected by Guardant360, a cell-free DNA assay, in Japan and by blood or tissue-based next-generation sequencing (NGS) at Duke University. Two hundred and seven patients with BTC from Japan were included in an exploratory cohort to evaluate the association of MAPK alterations with overall survival (OS) according to MAPK alteration status. One hundred and ten patients with BTC from both Japan and the US harboring oncogenic alterations in the MAPK pathway were included in a biomarker selected cohort to assess the association of specific MAPK alterations with OS. Multivariate analysis was performed using a Cox regression model based on a univariate p-value < 0.2. Results: MAPK pathway-related oncogenic alterations detected in each cohort are shown in the table below. In the exploratory cohort, median OS was shorter for patients with MAPK alterations vs. no MAPK alteration (15.9 m vs. 24.9 m, log-rank p = 0.001). Based on univariate analysis, the following covariates were selected for multivariate analyses: age, prior resection, and MAPK pathway alteration in the exploratory cohort; country, the timing of NGS, distant metastasis, KRAS amplification, and BRAF class 2 mutation in the biomarker selected cohort. In the exploratory cohort, multivariate analysis identified MAPK pathway alterations as an independent predictor of shorter OS with a HR of 1.92 (95% CI = 1.28-2.87, p = 0.001). In the biomarker selected cohort, multivariate analysis identified BRAF class 2 mutations and KRAS amplification as independent predictors of shorter OS with a HR of 16.2 (95% CI = 3.26-80.8, p = 0.001) and 5.97 (95% CI = 1.74-19.3, p = 0.002) respectively. Conclusions: MAPK pathway alterations, especially BRAF class 2 mutation and KRAS amplification, had a significant negative impact on clinical outcomes in BTC receiving first-line chemotherapy. These results are newly confirmed in BTC. [Table: see text]

Published

2022

2. Frequency of practice-changing findings identified by comprehensive genomic profiling in non-myeloid hematologic malignancies

Author

Katherine I. Zhou, Chenyu Lin, Michelle Green, Bennett Adam Caughey, Michael Datto, John H Strickler, and Matthew McKinney

Subjects

Cancer Research, Oncology

Abstract

3060 Background: Comprehensive genomic profiling (CGP) is increasingly used to guide management of myeloid and advanced solid malignancies, but its role in non-myeloid hematologic malignancies is less clear. Studies have found a high rate of potentially actionable variants by CGP in this population, but these do not always translate into clinical practice changes. We aimed to determine the rate at which variants found on CGP changed clinical practice. Methods: We retrospectively reviewed a cohort of 101 consecutive patients with non-myeloid hematologic malignancies at Duke, comprising a total of 105 samples that were sent for CGP by FoundationOne Heme (104) or HemeComplete (1) in 2014–2021. We identified variants of clinical significance and classified them by evidence level according to the AMP/ASCO/CAP 2017 guidelines (e.g., for therapies, level A: FDA-approved / in guidelines; B: expert consensus; C: clinical trial / FDA-approved in different tumor type; D: preclinical data). We further identified documented changes in clinical practice that occurred in direct response to CGP results. Results: Commonly cited reasons for CGP included guiding therapy selection (27), identifying resistance mutations (19), refining prognosis (14), and clarifying diagnosis (11). Of the 105 samples sent for sequencing, 92 (88%) yielded at least one pathogenic or likely pathogenic variant. CGP resulted after death in 12 patients and within 1 month of death in another 11 patients. Seventy-three out of 101 patients (72%) had at least one variant with therapy sensitizing, diagnostic, or prognostic significance (levels A–C) or associated with therapy resistance (levels A/D). While 61 patients (60%) had a therapy sensitizing variant, only 6 patients (10%) were offered a biomarker-directed therapy. In contrast, the presence of a resistance mutation led to discontinuation of current therapy or influenced future therapy selection in 9 of 13 patients (69%). The absence of a resistance mutation influenced choice of therapy in another 4 patients. Sequencing results also helped clarify a previously uncertain diagnosis in 4 patients and led to medical genetics referrals in 3 patients. Conclusions: Comprehensive genomic profiling of non-myeloid hematologic malignancies identified variants of clinical significance in 72% of patients and led to changes in practice in 22% of patients. CGP was often sent late in the clinical course. [Table: see text]

Published

2022

3. Identification of an optimal circulating tumor DNA (ctDNA) shedding threshold to detect actionable driver mutations in colorectal and pancreatic adenocarcinoma

Author

Bennett Adam Caughey, Kumiko Umemoto, Michelle Green, Masafumi Ikeda, Rachel D'Anna, Makoto Ueno, Donna Niedzwiecki, Hiroya Taniguchi, Daniel Walden, Yoshito Komatsu, Katherine I. Zhou, Taito Esaki, Ryne Ramaker, Tadamichi Denda, Michael Datto, Hideaki Bando, Tanios S. Bekaii-Saab, Takayuki Yoshino, John H Strickler, and Yoshiaki Nakamura

Subjects

Cancer Research, Oncology

Abstract

3571 Background: In colorectal cancer (CRC), mutations in KRAS, NRAS, and BRAF predict resistance to anti-EGFR therapies. In pancreatic ductal adenocarcinoma (PDAC), ~90% of patients harbor KRAS mutations, while KRAS wild-type tumors often have clinically actionable fusion alterations. Thus, in both cancers, the accurate ascertainment of RAS and BRAF driver status is essential. Sequencing of cell-free DNA (cfDNA) from plasma allows convenient assessment of a tumor’s molecular profile, but sensitivity can be limited by low ctDNA shedding. We sought to establish a ctDNA shedding threshold at which actionable driver mutations can be reliably detected. Methods: Molecular reports and matched clinical data were obtained from the Duke Molecular Registry of Tumors and the SCRUM-Japan GOZILA and GI-SCREEN. CRC or PDAC patients with a pathogenic KRAS, NRAS, or BRAF activating point mutation (“driver”) present on tissue next-generation sequencing (NGS) assays and who also had cfDNA assay available were included. Tissue NGS included Foundation One CDx and Oncomine Comprehensive Assay. Guardant 360 (G360) was the sole plasma cfDNA assay. 131 CRC and 24 PDAC cases with 189 total G360 assays met criteria and were included. Samples were analyzed according to detection of the driver mutation and the maximum mutant allele frequency (MAF) of non-driver mutations on G360. An optimal cut-point for max MAF was explored among the CRC and PDAC patients using a maximally selected Wilcoxon rank statistic method. Results: 76.8% of driver mutations were in KRAS, 22.6% in BRAF, and 1.9% in NRAS with an overlap of 1 BRAF and 1 NRAS mutation with a KRAS mutation. Overall sensitivity of G360 for drivers was 83.0% for CRC and 54.2% for PDAC. No variants were detected on G360 in 9.1% of CRC and 37.5% of PDAC. Sensitivity for driver mutations increased with higher maximum non-driver MAF, with MAF > 1% predicting sensitivity > 98% (Table). Optimal cut-point analysis identified MAF of > 0.34% (p < 0.0001), above which the driver was identified in 97% of patients and below which only 27%. Conclusions: In our study, non-driver MAF > 1% on cfDNA NGS predicts high sensitivity for RAS and BRAF mutations and thus is adequate to guide clinical decisions such as anti-EGFR therapy in CRC, evaluation for fusions in PDAC, and validity in clinical trials. MAF ≤0.34% is a clear threshold to consider an assay inadequate and thus seek alternative testing. Sensitivity rises for MAF between 0.35 and 1% but will require greater patient numbers to establish clinically relevant sensitivity thresholds. These results will be updated with additional data for final presentation. [Table: see text]

Published

2022

4. DNA methylation markers for diagnosis and prognosis of common cancers

Author

Liang Zhao, Xiaoke Hao, Maryam Jafari, Heng Zhang, Debanjan Dhar, Ken Flagg, Lianghong Zheng, Jian-Kang Zhu, William Shi, Rui Hou, Wei Wei, Wenqiu Wang, Edward Zhang, Michal Krawczyk, Xin Fu, Michael Karin, Jiayi Hou, Danni Lin, Christopher Chung, Shaohua Yi, Bennett A. Caughey, Juan Wang, Jie Zhu, Huiyan Luo, Gen Li, Rui-Hua Xu, Kang Zhang, and Charlotte Zhang

Subjects

Male, 0301 basic medicine, Oncology, Lung Neoplasms, Time Factors, Colorectal cancer, Kaplan-Meier Estimate, survival analysis, Cohort Studies, cancer diagnosis, Neoplasms, Neoplasm Metastasis, Cancer, screening and diagnosis, DNA methylation, Multidisciplinary, medicine.diagnostic_test, Liver Disease, Liver Neoplasms, Methylation, Biological Sciences, Prognosis, Colo-Rectal Cancer, Detection, CpG site, Hepatocellular carcinoma, Colonic Neoplasms, Female, 4.2 Evaluation of markers and technologies, Liver Cancer, Risk, medicine.medical_specialty, Breast Neoplasms, Biology, cancer prognosis, 03 medical and health sciences, Rare Diseases, Clinical Research, Internal medicine, Breast Cancer, Biopsy, Genetics, medicine, Humans, Genetic Testing, Alleles, Survival analysis, Human Genome, Case-control study, DNA Methylation, medicine.disease, 4.1 Discovery and preclinical testing of markers and technologies, 030104 developmental biology, Case-Control Studies, gene expression, CpG Islands, Digestive Diseases

Abstract

The ability to identify a specific cancer using minimally invasive biopsy holds great promise for improving the diagnosis, treatment selection, and prediction of prognosis in cancer. Using whole-genome methylation data from The Cancer Genome Atlas (TCGA) and machine learning methods, we evaluated the utility of DNA methylation for differentiating tumor tissue and normal tissue for four common cancers (breast, colon, liver, and lung). We identified cancer markers in a training cohort of 1,619 tumor samples and 173 matched adjacent normal tissue samples. We replicated our findings in a separate TCGA cohort of 791 tumor samples and 93 matched adjacent normal tissue samples, as well as an independent Chinese cohort of 394 tumor samples and 324 matched adjacent normal tissue samples. The DNA methylation analysis could predict cancer versus normal tissue with more than 95% accuracy in these three cohorts, demonstrating accuracy comparable to typical diagnostic methods. This analysis also correctly identified 29 of 30 colorectal cancer metastases to the liver and 32 of 34 colorectal cancer metastases to the lung. We also found that methylation patterns can predict prognosis and survival. We correlated differential methylation of CpG sites predictive of cancer with expression of associated genes known to be important in cancer biology, showing decreased expression with increased methylation, as expected. We verified gene expression profiles in a mouse model of hepatocellular carcinoma. Taken together, these findings demonstrate the utility of methylation biomarkers for the molecular characterization of cancer, with implications for diagnosis and prognosis.

Published

2017

5. MicroRNA Expression Profile on Solid Subtype of Invasive Lung Adenocarcinoma Reveals a Panel of Four miRNAs to Be Associated with Poor Prognosis in Chinese Patients

Author

Yan Xu, Xun Hu, Guiqun Cao, You Lu, Wei-Ya Wang, Kang Zhang, Ping Fan, Jian-Xin Xue, Li-Li Jiang, Yong-Qiang Zhang, Wei-Wei Tan, and Bennett A. Caughey

Subjects

Lung adenocarcinoma, 0301 basic medicine, Poor prognosis, Biology, Malignancy, Bioinformatics, stage I-III, 03 medical and health sciences, 0302 clinical medicine, microRNA, Solid subtype, medicine, Stage (cooking), Lung, microRNA (miRNA), MicroRNA Expression Profile, Prognosis, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, Oncology, Cell culture, 030220 oncology & carcinogenesis, Cancer research, bacteria, Adenocarcinoma, Research Paper

Abstract

According to the reclassification of lung adenocarcinoma (LAC) proposed in 2011, solid predominant lung adenocarcinoma (SPA) has been associated with poor outcomes for LAC patients. However, the prognostic value of the presence of solid subtype remains unclear. Besides, there is little data about the roles of microRNA (miRNA) in solid subtype of LAC. In this study, 243 LAC patients were classified into solid subtype positive and negative groups (S+ LAC, n=134 and S- LAC, n=109) according to whether the solid subtype was more than 5% of the tumor component or not. We analyzed the relationship between solid subtype and patients' outcome by univariate and multivariate analyses. Solid subtype was proved to be significantly associated with the 5-year overall survival and played as an independent prognostic factor for stage I-III invasive LAC patients. Then miRNA microarray was used to identify differentially expressed miRNAs in solid subtype, resulting in 31 differential miRNAs. Quantitative reverse transcription-PCR (QRT-PCR) was used to validate 4 key miRNAs (miR-133b, miR-155-5p, miR-124-3p, miR-145-5p). Further, CCK-8 and transwell assays were performed to validate the impact of one dysregulated miRNA (miR-133b) on LAC cell function. Interestingly, while miR-133b could significantly inhibit the proliferation of A549 and SPC-A1, it showed no effect on the migration or invasion of LAC cell lines. These results suggest that solid subtype can exert independent prognostic impact on LAC patients, and 4 important dysregulated miRNAs in solid subtype of LAC may be involved in the malignancy of S+LAC, thus may further have clinical perspective for S+ LAC in the future.

Published

2016

6. Noninvasive detection of fetal subchromosomal abnormalities by semiconductor sequencing of maternal plasma DNA

Author

Rachel Q. Xue, Huang Quanfei, Daniel Zhang, Yangyi Chen, Mindy Zhang, Jiexia Yang, Kang Zhang, Rui Hou, Chang Liu, Dong-hong Luo, Yiming Qi, Michael Ai, Ai-hua Yin, Jian Liu, Mingqin Mai, Lianghong Zheng, Hailiang Liu, Dongmei Wang, Michal Krawczyk, Bennett A. Caughey, Chun-fang Peng, Fangfang Guo, Michael Karin, Yunan Wang, Wei-wei Huang, Xin Zhao, and Jing Wu

Subjects

Pathology, medicine.medical_specialty, Aneuploidy, Prenatal diagnosis, Biology, DNA sequencing, Deep sequencing, Fetus, Pregnancy, Prenatal Diagnosis, Chromosome Duplication, Gene duplication, medicine, Humans, Chromosome Aberrations, Comparative Genomic Hybridization, Multidisciplinary, Cell-Free System, DNA, Sequence Analysis, DNA, Ion semiconductor sequencing, Biological Sciences, medicine.disease, Molecular biology, Molecular Weight, Semiconductors, Cell-free fetal DNA, Female, Chromosome Deletion, Comparative genomic hybridization

Abstract

Noninvasive prenatal testing (NIPT) using sequencing of fetal cell-free DNA from maternal plasma has enabled accurate prenatal diagnosis of aneuploidy and become increasingly accepted in clinical practice. We investigated whether NIPT using semiconductor sequencing platform (SSP) could reliably detect subchromosomal deletions/duplications in women carrying high-risk fetuses. We first showed that increasing concentration of abnormal DNA and sequencing depth improved detection. Subsequently, we analyzed plasma from 1,456 pregnant women to develop a method for estimating fetal DNA concentration based on the size distribution of DNA fragments. Finally, we collected plasma from 1,476 pregnant women with fetal structural abnormalities detected on ultrasound who also underwent an invasive diagnostic procedure. We used SSP of maternal plasma DNA to detect subchromosomal abnormalities and validated our results with array comparative genomic hybridization (aCGH). With 3.5 million reads, SSP detected 56 of 78 (71.8%) subchromosomal abnormalities detected by aCGH. With increased sequencing depth up to 10 million reads and restriction of the size of abnormalities to more than 1 Mb, sensitivity improved to 69 of 73 (94.5%). Of 55 false-positive samples, 35 were caused by deletions/duplications present in maternal DNA, indicating the necessity of a validation test to exclude maternal karyotype abnormalities. This study shows that detection of fetal subchromosomal abnormalities is a viable extension of NIPT based on SSP. Although we focused on the application of cell-free DNA sequencing for NIPT, we believe that this method has broader applications for genetic diagnosis, such as analysis of circulating tumor DNA for detection of cancer.

Published

2015

7. Circulating tumour DNA methylation markers for diagnosis and prognosis of hepatocellular carcinoma

Author

Wei Wei, Charlotte Zhang, Rui Hou, Shaohua Yi, Wenqiu Wang, Huimin Cai, Kang Zhang, William Shi, Gen Li, Huiyan Luo, Binwu Ying, Edward Zhang, Heng Zhang, Xiaoke Hao, Zheng Zhong, Qi Zhao, Ken Flagg, Yaou Duan, Jian-Kang Zhu, Qingli Quan, Jiayi Hou, Yanxin Xu, Rongping Guo, Danni Lin, Wengeng Zhang, Juan Wang, Xin Fu, Rui-Hua Xu, Oulan Li, Runze Zhang, Jie Zhu, Bennett A. Caughey, Lianghong Zheng, Hannah Carter, Meixing Yu, Kang Li, and Michal Krawczyk

Subjects

0301 basic medicine, Oncology, Male, medicine.medical_specialty, Carcinoma, Hepatocellular, Models, Biological, Circulating Tumor DNA, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Carcinoma, Biomarkers, Tumor, Humans, General Materials Science, Epigenetics, Liquid biopsy, Stage (cooking), business.industry, Mechanical Engineering, Liver Neoplasms, Cancer, General Chemistry, Methylation, DNA Methylation, Condensed Matter Physics, medicine.disease, Prognosis, digestive system diseases, 030104 developmental biology, Mechanics of Materials, 030220 oncology & carcinogenesis, Hepatocellular carcinoma, DNA methylation, Female, business

Abstract

An effective blood-based method for the diagnosis and prognosis of hepatocellular carcinoma (HCC) has not yet been developed. Circulating tumour DNA (ctDNA) carrying cancer-specific genetic and epigenetic aberrations may enable a noninvasive 'liquid biopsy' for diagnosis and monitoring of cancer. Here, we identified an HCC-specific methylation marker panel by comparing HCC tissue and normal blood leukocytes and showed that methylation profiles of HCC tumour DNA and matched plasma ctDNA are highly correlated. Using cfDNA samples from a large cohort of 1,098 HCC patients and 835 normal controls, we constructed a diagnostic prediction model that showed high diagnostic specificity and sensitivity (P < 0.001) and was highly correlated with tumour burden, treatment response, and stage. Additionally, we constructed a prognostic prediction model that effectively predicted prognosis and survival (P < 0.001). Together, these findings demonstrate in a large clinical cohort the utility of ctDNA methylation markers in the diagnosis, surveillance, and prognosis of HCC.

Published

2016

8. Validation of a Prognostic Model and the Impact of Mutations in Patients With Lower-Risk Myelodysplastic Syndromes

Author

Hagop M. Kantarjian, Donna Neuberg, Guillermo Garcia-Manero, Ross L. Levine, Naomi Galili, Omar Abdel-Wahab, Kristen E. Stevenson, Benjamin L. Ebert, David P. Steensma, Rafael Bejar, Bennett A. Caughey, and Azra Raza

Subjects

Male, Oncology, Cancer Research, medicine.medical_specialty, Pathology, DNA Mutational Analysis, Disease, Lower risk, Predictive Value of Tests, Internal medicine, medicine, Humans, Enhancer of Zeste Homolog 2 Protein, Survival analysis, business.industry, Myelodysplastic syndromes, Hazard ratio, Polycomb Repressive Complex 2, Reproducibility of Results, ORIGINAL REPORTS, Middle Aged, Prognosis, medicine.disease, Survival Analysis, International Prognostic Scoring System, Myelodysplastic Syndromes, Predictive value of tests, Multivariate Analysis, Mutation, Cohort, Female, business, Follow-Up Studies

Abstract

Purpose A subset of patients with myelodysplastic syndromes (MDS) who are predicted to have lower-risk disease as defined by the International Prognostic Scoring System (IPSS) demonstrate more aggressive disease and shorter overall survival than expected. The identification of patients with greater-than-predicted prognostic risk could influence the selection of therapy and improve the care of patients with lower-risk MDS. Patients and Methods We performed an independent validation of the MD Anderson Lower-Risk Prognostic Scoring System (LR-PSS) in a cohort of 288 patients with low- or intermediate-1 IPSS risk MDS and examined bone marrow samples from these patients for mutations in 22 genes, including SF3B1, SRSF2, U2AF1, and DNMT3A. Results The LR-PSS successfully stratified patients with lower-risk MDS into three risk categories with significant differences in overall survival (20% in category 1 with median of 5.19 years [95% CI, 3.01 to 10.34 years], 56% in category 2 with median of 2.65 years [95% CI, 2.18 to 3.30 years], and 25% in category 3 with median of 1.11 years [95% CI, 0.82 to 1.51 years]), thus validating this prognostic model. Mutations were identified in 71% of all samples, and mutations associated with a poor prognosis were enriched in the highest-risk LR-PSS category. Mutations of EZH2, RUNX1, TP53, and ASXL1 were associated with shorter overall survival independent of the LR-PSS. Only EZH2 mutations retained prognostic significance in a multivariable model that included LR-PSS and other mutations (hazard ratio, 2.90; 95% CI, 1.85 to 4.52). Conclusion Combining the LR-PSS and EZH2 mutation status identifies 29% of patients with lower-risk MDS with a worse-than-expected prognosis. These patients may benefit from earlier initiation of disease-modifying therapy.

Published

2012

9. TET2 mutations predict response to hypomethylating agents in myelodysplastic syndrome patients

Author

Albert Perez-Ladaga, Allegra M. Lord, Benjamin L. Ebert, Kristen E. Stevenson, Rui Chen, Rafael Bejar, Bennett A. Caughey, Jacques Zaneveld, Gad Getz, Richard Stone, Michal Bar-Natan, David P. Steensma, Guillermo Garcia-Manero, Petar Stojanov, Hagop M. Kantarjian, Hui Wang, and Donna Neuberg

Subjects

Male, Genotype, Immunology, Azacitidine, Decitabine, Kaplan-Meier Estimate, Biology, medicine.disease_cause, Biochemistry, Dioxygenases, Gene Frequency, Proto-Oncogene Proteins, medicine, Biomarkers, Tumor, Animals, Humans, Enzyme Inhibitors, DNA Modification Methylases, Aged, Bone Marrow Transplantation, Mice, Knockout, Mutation, Transplantation Chimera, Myelodysplastic syndromes, Hazard ratio, Cell Biology, Hematology, DNA Methylation, medicine.disease, PTPN11, DNA-Binding Proteins, Repressor Proteins, Logistic Models, Treatment Outcome, Myelodysplastic Syndromes, DNA methylation, Cancer research, Female, Tumor Suppressor Protein p53, medicine.drug

Abstract

Only a minority of myelodysplastic syndrome (MDS) patients respond to hypomethylating agents (HMAs), but strong predictors of response are unknown. We sequenced 40 recurrently mutated myeloid malignancy genes in tumor DNA from 213 MDS patients collected before treatment with azacitidine (AZA) or decitabine (DEC). Mutations were examined for association with response and overall survival. The overall response rate of 47% was not different between agents. Clonal TET2 mutations predicted response (odds ratio [OR] 1.99, P = .036) when subclones unlikely to be detected by Sanger sequencing (allele fraction

Published

2014

10. Somatic Mutations Predict Poor Outcome in Patients With Myelodysplastic Syndrome After Hematopoietic Stem-Cell Transplantation

Author

Donna Neuberg, Benjamin L. Ebert, Kristen E. Stevenson, Robert J. Soiffer, R. Coleman Lindsley, Brenton G. Mar, David P. Steensma, Philippe Armand, Corey Cutler, Gad Getz, Joseph H. Antin, Petar Stojanov, Jerome Ritz, Vincent T. Ho, Edwin P. Alyea, Rafael Bejar, John Koreth, and Bennett A. Caughey

Subjects

Oncology, Adult, Male, Cancer Research, Candidate gene, medicine.medical_specialty, Transplantation Conditioning, medicine.medical_treatment, Hematopoietic stem cell transplantation, medicine.disease_cause, Transplantation, Autologous, Disease-Free Survival, Young Adult, Internal medicine, medicine, Humans, Young adult, Aged, Mutation, business.industry, Myelodysplastic syndromes, Hazard ratio, Hematopoietic Stem Cell Transplantation, ORIGINAL REPORTS, Middle Aged, medicine.disease, Prognosis, Transplantation, Haematopoiesis, Treatment Outcome, Myelodysplastic Syndromes, Immunology, Female, business

Abstract

Purpose Recurrently mutated genes in myelodysplastic syndrome (MDS) are pathogenic drivers and powerfully associated with clinical phenotype and prognosis. Whether these types of mutations predict outcome after allogeneic hematopoietic stem-cell transplantation (HSCT) in patients with MDS is not known. Patients and Methods We used massively parallel sequencing to examine tumor samples collected from 87 patients with MDS before HSCT for coding mutations in 40 recurrently mutated MDS genes. Results Mutations were identified in 92% of patients, most frequently in the ASXL1 (29%), TP53 (21%), DNMT3A (18%), and RUNX1 (16%) genes. In univariable analyses, only TP53 mutations were associated with shorter overall (OS; hazard ratio [HR], 3.74; P < .001) and progression-free survival (HR, 3.97; P < .001). After adjustment for clinical variables associated with these end points, mutations in TP53 (HR, 2.30; P = .027), TET2 (HR, 2.40; P = .033), and DNMT3A (HR, 2.08; P = .049) were associated with decreased OS. In multivariable analysis including clinical variables, complex karyotype status, and candidate genes, mutations in TP53 (HR, 4.22; P ≤ .001) and TET2 (HR, 1.68; P = .037) were each independently associated with shorter OS. Nearly one half of patients (46%) carried a mutation in TP53, DNMT3A, or TET2 and accounted for 64% of deaths. Three-year OS in patients without these mutations was 59% (95% CI, 43% to 72%), versus 19% (95% CI, 9% to 33%) in patients with these mutations. Conclusion Mutations in TP53, TET2, or DNMT3A identify patients with MDS with shorter OS after HSCT.

Published

2014

11. O-024 Next-generation sequencing of 213 MDS patient samples identifies mutation profiles associated with response to hypomethylating agents and overall survival

Author

Kristen E. Stevenson, Gad Getz, R. Chen, David P. Steensma, Michal Bar-Natan, Bennett A. Caughey, Rafael Bejar, Richard Stone, Jacques Zaneveld, G. Garcia-Manero, Hagop M. Kantarjian, H. Wang, K. Cibulskis, Petar Stojanov, Donna Neuberg, and Benjamin L. Ebert

Subjects

Genetics, Cancer Research, Oncology, business.industry, Mutation (genetic algorithm), Overall survival, Medicine, Hematology, business, DNA sequencing

Published

2013

12. Functional Defects In Neutrophils Derived From Ezh2 Null Mice

Author

Benjamin L. Ebert, Rafael Bejar, Huafeng Xie, Albert Perez-Ladaga, Stuart H. Orkin, David B. Sykes, and Bennett A. Caughey

Subjects

medicine.diagnostic_test, Cellular differentiation, Immunology, Zymosan, macromolecular substances, Cell Biology, Hematology, Cell cycle, Biochemistry, Molecular biology, Flow cytometry, chemistry.chemical_compound, TLR2, medicine.anatomical_structure, chemistry, Cell culture, medicine, Bone marrow, Progenitor cell

Abstract

Introduction We investigate the role of Ezh2 in neutrophil function using murine progenitor cells differentiated into neutrophils lacking the Ezh2 gene. Ezh2 is the catalytic component of the polycomb repressive complex 2, which methylates lysine 27 of histone H3. It is frequently disrupted in myelodysplastic syndromes (MDS) leading to loss of function (Ernst et al., 2010). Mutations in EZH2 are found in 6% of MDS patients and while not strongly linked to cytopenias or blast proportion, they are independently associated with worse overall survival compared to patients with wildtype EZH2 (Bejar R. et al., 2011 and 2012). We hypothesize that Ezh2 mutations may cause qualitative defects in myeloid cells that impact their function and could contribute to the adverse prognosis observed in EZH2 mutant MDS. Methods Bone marrow from Ezh2 null (Ezh2-/-) and littermate control mice (WT) were transduced with HOXB8 fused to the estrogen receptor ligand-binding domain to produce immortalized myeloid progenitor cells. Removal of estrogen from the media allows these cells differentiate into mature neutrophils (Wang G.G., 2006). Differentiated cells were characterized for surface markers by flow cytometry and for gene expression by PCR of mRNA. Spontaneous cell death was measured by annexin/PI staining. Cell cycle patterns were determined by measuring the red emission of PI. Chemotactic function was assessed by counting cells that migrated across a transwell in presence/absence of the attractant zymosan. For phagocytosis experiments, cells were incubated with Fluoresbrite YG carboxylate beads at 37°C or 4°C. Reactive oxygen species (ROS) generation was measured by the oxidation of dihydrorhodamine 123 into fluorescent rhodamine 123. Results Estrogen withdrawal caused differentiation of both WT and Ezh2-/- lines into cells with mature neutrophil morphology after six days (Figure 1a). Both differentiated lines expressed the neutrophil surface markers CD11b and CD62L and the neutrophil-specific genes lactoferrin and Itgb2l. Ezh2 -/- cells had an increased rate of spontaneous cell death compared to WT in undifferentiated (32.81% vs. 20.33%) and mature cells (32.82% vs. 14.23%). Nevertheless, both progenitor cell lines showed similar cell cycle patterns, demonstrating that Ezh2 absence had no other effect on cell cycle progression. Ezh2 -/- neutrophils failed to migrate towards zymosan (Figure 1b). Expression of Tlr2, which binds zymosan, and other Toll-like receptors (Tlr4/5/9) were similar between the differentiated cell lines. Cells incubated with FITC-zymosan at 37°C showed no fluorescence differences between cell lines, indicating similar adherence. Experiments with neutrophils from an MDS patient with homozygous EZH2 mutations demonstrated a similar migration defect. Additional studies in MDS patient samples are ongoing and will be presented. Phagocytosis was reduced in Ezh2-/-cells. Unstimulated, the number of cells ingesting and adhering YG-beads was significantly greater with WT cells than with Ezh2-/-cells. When activated with fMLP, both lines showed increased adherence of YG-beads but the number of phagocytosing Ezh2-/- cells was reduced. The average number of beads ingested by each cell was lower for Ezh2-/- cells compared to WT (5.95 vs 2.94, p < 0.001) in resting cells, and 9.47 vs. 3.73 in fMLP-activated cells, p < 0.01. The fraction of Ezh2-/- neutrophils generating ROS when stimulated with PMA is 2.4-fold higher than for WT cells. ROS production was greatly reduced in the presence of diphenyleneiodonium (DPI), confirming the role of NADPH oxidase in the generation of ROS. Conclusion Our results indicate impaired function of neutrophils derived from Ezh2-/- mice, demonstrating increased spontaneous cell death, impaired migration, decreased phagocytosis, and overproduction of ROS. Qualitative defects observed in neutrophils deficient for EZH2 may help explain the adverse prognosis associated with these mutations in MDS patients. Disclosures: Bejar: Genoptix: Consultancy, Honoraria, Membership on an entity’s Board of Directors or advisory committees; Celgene: Consultancy, Membership on an entity’s Board of Directors or advisory committees.

Published

2013