Your search keyword '"Paul A. Meyers"' showing total 337 results

1. Clinical sequencing of soft tissue and bone sarcomas delineates diverse genomic landscapes and potential therapeutic targets

Author

Benjamin A. Nacev, Francisco Sanchez-Vega, Shaleigh A. Smith, Cristina R. Antonescu, Evan Rosenbaum, Hongyu Shi, Cerise Tang, Nicholas D. Socci, Satshil Rana, Rodrigo Gularte-Mérida, Ahmet Zehir, Mrinal M. Gounder, Timothy G. Bowler, Anisha Luthra, Bhumika Jadeja, Azusa Okada, Jonathan A. Strong, Jake Stoller, Jason E. Chan, Ping Chi, Sandra P. D’Angelo, Mark A. Dickson, Ciara M. Kelly, Mary Louise Keohan, Sujana Movva, Katherine Thornton, Paul A. Meyers, Leonard H. Wexler, Emily K. Slotkin, Julia L. Glade Bender, Neerav N. Shukla, Martee L. Hensley, John H. Healey, Michael P. La Quaglia, Kaled M. Alektiar, Aimee M. Crago, Sam S. Yoon, Brian R. Untch, Sarah Chiang, Narasimhan P. Agaram, Meera R. Hameed, Michael F. Berger, David B. Solit, Nikolaus Schultz, Marc Ladanyi, Samuel Singer, and William D. Tap

Subjects

Science

Abstract

Sarcomas are rare tumours with many different subtypes and clinical outcomes; a broader knowledge of their genetic features is required. Here, the authors analyse 2138 soft tissue and bone sarcomas across 45 subtypes using MSK-IMPACT targeted sequencing and find genomic groups that are distinct from histological subgroups.

Published

2022

2. Effects of dexrazoxane on doxorubicin-related cardiotoxicity and second malignant neoplasms in children with osteosarcoma: a report from the Children’s Oncology Group

Author

Lisa M. Kopp, Richard B. Womer, Cindy L. Schwartz, David H. Ebb, Vivian I. Franco, David Hall, Donald A. Barkauskas, Mark D. Krailo, Holcombe E. Grier, Paul A. Meyers, Leonard H. Wexler, Neyssa M. Marina, Katherine A. Janeway, Richard Gorlick, Mark L. Bernstein, Steven E. Lipshultz, and for the Children’s Oncology Group

Subjects

Osteosarcoma, Pediatrics, Cardiotoxicity, Doxorubicin, Diseases of the circulatory (Cardiovascular) system, RC666-701, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Dexrazoxane protects from lower-cumulative-dose doxorubicin cardiotoxicity, but the effect of dexrazoxane in children with sarcoma treated with higher-cumulative-dose doxorubicin is unknown. Methods We evaluated children with osteosarcoma (OS) on two Children’s Oncology Group trials with higher dose doxorubicin (375–600 mg/m2) preceded by dexrazoxane (10:1 dexrazoxane:doxorubicin dosing). They were evaluated after the minimum expected treatment time (METT), defined as 28 weeks. Cardiotoxicity was identified by echocardiography and serum N-terminal pro-brain natriuretic peptide (NT-proBNP). Second malignant neoplasm (SMN) data was collected. Results All children had normal left ventricular (LV) systolic function as measured by LV fractional shortening and no heart failure. The end-diastolic septal thickness Z-scores (P

Published

2019

3. Unusual abdominal metastases in osteosarcoma

Author

Simon Berhe, Enrico Danzer, Paul A. Meyers, Gerald Behr, Michael P. LaQuaglia, and Anita P. Price

Subjects

Pediatrics, RJ1-570, Surgery, RD1-811

Abstract

Intraabdominal metastases in the setting of osteosarcoma are very rare. We describe a case of a 17-year-old boy with high-grade right distal femur osteosarcoma who, two years after diagnosis, developed extensive intra abdominal metastases involving the omentum, peritoneum, bowel serosa, psoas muscles and abdominal soft tissue. Awareness of and surveillance for unusual patterns of metastasis may allow for earlier detection, intervention, and palliative care decision-making, which may affect survival and quality of life. This report underlines the need for prospective studies evaluating surveillance guidelines for patients after medical and surgical management of osteosarcoma, especially in cases complicated by pulmonary metastases. Keywords: Pediatric osteosarcoma, Extrapulmonary metastases, Extrapulmonary recurrence, Surveillance imaging

Published

2018

4. Prognostic Factors and Survival in Pediatric and Adolescent Liposarcoma

Author

Eric J. Stanelle, Emily R. Christison-Lagay, Emma L. Sidebotham, Samuel Singer, Cristina R. Antonescu, Paul A. Meyers, and Michael P. La Quaglia

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Purpose. Liposarcoma is extremely rare in the pediatric population. To identify prognostic factors and determine treatment outcomes, we reviewed our institutional experience with pediatric liposarcoma. Methods. We retrospectively reviewed all pediatric patients (age

Published

2012

5. Impairment of Methotrexate Transport Is Common in Osteosarcoma Tumor Samples

Author

Rebecca Sowers, Bethanne D. Wenzel, Condon Richardson, Paul A. Meyers, John H. Healey, Adam S. Levy, and Richard Gorlick

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Osteosarcoma does not respond well to conventional dose methotrexate but does respond to high-dose methotrexate. Previous work has indicated that this resistance may be due to impaired transport of methotrexate across the cell membrane. In this study, the PT430 competitive displacement assay was adapted to evaluate methotrexate transport in 69 high-grade osteosarcoma tumor samples. All samples studied were shown to have relatively impaired methotrexate transport by PT430 assay. Ninety-nine percent of the samples had less than 20% PT430 displacement by methotrexate. Eighty-eight percent exhibited displacement by methotrexate at less than 50% of the displacement by trimetrexate. The high frequency of impaired transport suggests the presence of decreased functionality of the reduced folate carrier protein. The overwhelming presence of impaired transport may explain why methotrexate needs to be given in high doses to be effective in osteosarcoma therapy and suggests that reduced folate carrier-independent antifolates should be explored.

Published

2011

6. Tandem LC-MS Identification of Antitubercular Compounds in Zones of Growth Inhibition Produced by South African Filamentous Actinobacteria

Author

Daniel J. Watson, Lubbe Wiesner, Tlhalefo Matimela, Denzil Beukes, and Paul R. Meyers

Subjects

antitubercular, filamentous actinobacteria, HPLC-MS/MS, natural products, zone of inhibition, Organic chemistry, QD241-441

Abstract

Novel antitubercular compounds are urgently needed to combat drug-resistant Mycobacterium tuberculosis (Mtb). Filamentous actinobacteria have historically been an excellent source of antitubercular drugs. Despite this, drug discovery from these microorganisms has fallen out of favour due to the continual rediscovery of known compounds. To increase the chance of discovering novel antibiotics, biodiverse and rare strains should be prioritised. Subsequently, active samples need to be dereplicated as early as possible to focus efforts on truly novel compounds. In this study, 42 South African filamentous actinobacteria were screened for antimycobacterial activity using the agar overlay method against the Mtb indicator Mycolicibacterium aurum under six different nutrient growth conditions. Known compounds were subsequently identified through extraction and high-resolution mass spectrometric analysis of the zones of growth inhibition produced by active strains. This allowed the dereplication of 15 hits from six strains that were found to be producing puromycin, actinomycin D and valinomycin. The remaining active strains were grown in liquid cultures, extracted and submitted for screening against Mtb in vitro. Actinomadura napierensis B60T was the most active sample and was selected for bioassay-guided purification. This resulted in the identification of tetromadurin, a known compound, but which we show for the first time to have potent antitubercular activity, with the MIC90s within the range of 73.7–151.6 nM against M. tuberculosis H37RvT in vitro under different test conditions. This shows that South African actinobacteria are a good source of novel antitubercular compounds and warrant further screening. It is also revealed that active hits can be dereplicated by HPLC-MS/MS analysis of the zones of growth inhibition produced by the agar overlay technique.

Published

2023

7. Rare BRAF mutations in pancreatic neuroendocrine tumors may predict response to RAF and MEK inhibition.

Author

Amy Allen, Alice Can Ran Qin, Nitya Raj, Jiawan Wang, Sharmeen Uddin, Zhan Yao, Laura Tang, Paul A Meyers, Barry S Taylor, Michael F Berger, Rona Yaeger, Diane Reidy-Lagunes, and Christine A Pratilas

Subjects

Medicine, Science

Abstract

The clinical significance of BRAF alterations in well-differentiated (WD) metastatic pancreatic neuroendocrine tumor (panNET) is unknown, but BRAF-mutated panNET could represent a subset characterized by an identifiable and clinically actionable driver. Following the identification of two patients with WD metastatic panNET whose tumors harbored BRAF mutations, we queried the MSK-IMPACT series of 80 patients with WD metastatic panNET for additional mutations in BRAF, and in other genes involved in RAS/ RTK/ PI3K signaling pathways. BRAF mutations were identified in six samples (7.5%): two tumors harbored V600E mutations, one tumor each expressed K601E, T599K, and T310I mutations, and one tumor expressed both G596D and E451K BRAF. Few additional actionable driver alterations were identified. To determine the ERK activating capability of four BRAF mutations not previously characterized, mutant constructs were tested in model systems. Biochemical characterization of BRAF mutations revealed both high and low activity mutants. Engineered cells expressing BRAF K601E and V600E were used for in vitro drug testing of RAF and MEK inhibitors currently in clinical use. BRAF K601E demonstrated reduced sensitivity to dabrafenib compared to BRAF V600E, but the combination of RAF plus MEK inhibition was effective in cells expressing this mutation. Herein, we describe the clinical course of a patient with BRAF K601E and a patient with BRAF V600E WD metastatic panNET, and the identification of four mutations in BRAF not previously characterized. The combined clinical and biochemical data support a potential role for RAF and MEK inhibitors, or a combination of these, in a selected panNET population.

Published

2019

8. Supplementary Figure 1 from Comprehensive Molecular Profiling of Desmoplastic Small Round Cell Tumor

Author

Neerav Shukla, Marc Ladanyi, Ahmet Zehir, Elli Papaemmanuil, Andrew L. Kung, Paul A. Meyers, Leonard H. Wexler, Michael P. LaQuaglia, Todd E. Heaton, Justin T. Gerstle, Gunes Gundem, Daoqi You, Nancy Bouvier, Katherine A. Thornton, Mrinal M. Gounder, William D. Tap, Shakeel Modak, Nestor Rosales, Glorymar I. Sanchez, Diego F. Coutinho, Filemon Dela Cruz, Max F. Levine, Anita S. Bowman, and Emily K. Slotkin

Abstract

Supplementary Figure 1 depicts copy number alterations in the described cohort

Published

2023

9. Supplementary Table 1 from Comprehensive Molecular Profiling of Desmoplastic Small Round Cell Tumor

Author

Neerav Shukla, Marc Ladanyi, Ahmet Zehir, Elli Papaemmanuil, Andrew L. Kung, Paul A. Meyers, Leonard H. Wexler, Michael P. LaQuaglia, Todd E. Heaton, Justin T. Gerstle, Gunes Gundem, Daoqi You, Nancy Bouvier, Katherine A. Thornton, Mrinal M. Gounder, William D. Tap, Shakeel Modak, Nestor Rosales, Glorymar I. Sanchez, Diego F. Coutinho, Filemon Dela Cruz, Max F. Levine, Anita S. Bowman, and Emily K. Slotkin

Abstract

Supplementary Table 1 shows point mutations found in DSRCT samples

Published

2023

10. Supplementary Figure 3 from Comprehensive Molecular Profiling of Desmoplastic Small Round Cell Tumor

Author

Neerav Shukla, Marc Ladanyi, Ahmet Zehir, Elli Papaemmanuil, Andrew L. Kung, Paul A. Meyers, Leonard H. Wexler, Michael P. LaQuaglia, Todd E. Heaton, Justin T. Gerstle, Gunes Gundem, Daoqi You, Nancy Bouvier, Katherine A. Thornton, Mrinal M. Gounder, William D. Tap, Shakeel Modak, Nestor Rosales, Glorymar I. Sanchez, Diego F. Coutinho, Filemon Dela Cruz, Max F. Levine, Anita S. Bowman, and Emily K. Slotkin

Abstract

Supplementary Figure 3 provides a breakdown of the structural variant types found via whole genome sequencing in DSRCT samples

Published

2023

11. Supplementary Figure 2 from Comprehensive Molecular Profiling of Desmoplastic Small Round Cell Tumor

Author

Neerav Shukla, Marc Ladanyi, Ahmet Zehir, Elli Papaemmanuil, Andrew L. Kung, Paul A. Meyers, Leonard H. Wexler, Michael P. LaQuaglia, Todd E. Heaton, Justin T. Gerstle, Gunes Gundem, Daoqi You, Nancy Bouvier, Katherine A. Thornton, Mrinal M. Gounder, William D. Tap, Shakeel Modak, Nestor Rosales, Glorymar I. Sanchez, Diego F. Coutinho, Filemon Dela Cruz, Max F. Levine, Anita S. Bowman, and Emily K. Slotkin

Abstract

Supplementary Figure 2 depicts whole genome sequencing findings

Published

2023

12. Data from Comprehensive Molecular Profiling of Desmoplastic Small Round Cell Tumor

Author

Neerav Shukla, Marc Ladanyi, Ahmet Zehir, Elli Papaemmanuil, Andrew L. Kung, Paul A. Meyers, Leonard H. Wexler, Michael P. LaQuaglia, Todd E. Heaton, Justin T. Gerstle, Gunes Gundem, Daoqi You, Nancy Bouvier, Katherine A. Thornton, Mrinal M. Gounder, William D. Tap, Shakeel Modak, Nestor Rosales, Glorymar I. Sanchez, Diego F. Coutinho, Filemon Dela Cruz, Max F. Levine, Anita S. Bowman, and Emily K. Slotkin

Abstract

Desmoplastic small round cell tumor (DSRCT) is characterized by the EWSR1–WT1 t(11;22) (p13:q12) translocation. Few additional putative drivers have been identified, and research has suffered from a lack of model systems. Next-generation sequencing (NGS) data from 68 matched tumor-normal samples, whole-genome sequencing data from 10 samples, transcriptomic and affymetrix array data, and a bank of DSRCT patient-derived xenograft (PDX) are presented. EWSR1–WT1 fusions were noted to be simple, balanced events. Recurrent mutations were uncommon, but were noted in TERT (3%), ARID1A (6%), HRAS (5%), and TP53 (3%), and recurrent loss of heterozygosity (LOH) at 11p, 11q, and 16q was identified in 18%, 22%, and 34% of samples, respectively. Comparison of tumor-normal matched versus unmatched analysis suggests overcalling of somatic mutations in prior publications of DSRCT NGS data. Alterations in fibroblast growth factor receptor 4 (FGFR4) were identified in 5 of 68 (7%) of tumor samples, whereas differential overexpression of FGFR4 was confirmed orthogonally using 2 platforms. PDX models harbored the pathognomic EWSR1–WT1 fusion and were highly representative of corresponding tumors. Our analyses confirm DSRCT as a genomically quiet cancer defined by the balanced translocation, t(11;22)(p13:q12), characterized by a paucity of secondary mutations but a significant number of copy number alterations. Against this genomically quiet background, recurrent activating alterations of FGFR4 stood out, and suggest that this receptor tyrosine kinase, also noted to be highly expressed in DSRCT, should be further investigated. Future studies of DSRCT biology and preclinical therapeutic strategies should benefit from the PDX models characterized in this study.Implications:These data describe the general quiescence of the desmoplastic small round cell tumor (DSRCT) genome, present the first available bank of DSRCT model systems, and nominate FGFR4 as a key receptor tyrosine kinase in DSRCT, based on high expression, recurrent amplification, and recurrent activating mutations.

Published

2023

13. Supplementary Figure 4 from Comprehensive Molecular Profiling of Desmoplastic Small Round Cell Tumor

Author

Neerav Shukla, Marc Ladanyi, Ahmet Zehir, Elli Papaemmanuil, Andrew L. Kung, Paul A. Meyers, Leonard H. Wexler, Michael P. LaQuaglia, Todd E. Heaton, Justin T. Gerstle, Gunes Gundem, Daoqi You, Nancy Bouvier, Katherine A. Thornton, Mrinal M. Gounder, William D. Tap, Shakeel Modak, Nestor Rosales, Glorymar I. Sanchez, Diego F. Coutinho, Filemon Dela Cruz, Max F. Levine, Anita S. Bowman, and Emily K. Slotkin

Abstract

Supplementary Figure 4 shows data related to FGFR4 inhibition in DSRCT and control models

Published

2023

14. Supplementary Table 2 from Comprehensive Molecular Profiling of Desmoplastic Small Round Cell Tumor

Author

Neerav Shukla, Marc Ladanyi, Ahmet Zehir, Elli Papaemmanuil, Andrew L. Kung, Paul A. Meyers, Leonard H. Wexler, Michael P. LaQuaglia, Todd E. Heaton, Justin T. Gerstle, Gunes Gundem, Daoqi You, Nancy Bouvier, Katherine A. Thornton, Mrinal M. Gounder, William D. Tap, Shakeel Modak, Nestor Rosales, Glorymar I. Sanchez, Diego F. Coutinho, Filemon Dela Cruz, Max F. Levine, Anita S. Bowman, and Emily K. Slotkin

Abstract

Supplementary Table 2 shows the raw data further described in Figure 3

Published

2023

15. Subclonal somatic copy number alterations emerge and dominate in recurrent osteosarcoma

Author

Michael D. Kinnaman, Simone Zaccaria, Alvin Makohon-Moore, Brian Arnold, Max Levine, Gunes Gundem, Juan E. Arango Ossa, Dominik Glodzik, M. Irene Rodríguez-Sánchez, Nancy Bouvier, Shanita Li, Emily Stockfisch, Marisa Dunigan, Cassidy Cobbs, Umesh Bhanot, Daoqi You, Katelyn Mullen, Jerry Melchor, Michael V. Ortiz, Tara O’Donohue, Emily Slotkin, Leonard H. Wexler, Filemon S. Dela Cruz, Meera Hameed, Julia L. Glade Bender, William D. Tap, Paul A. Meyers, Elli Papaemmanuil, Andrew L. Kung, and Christine A Iacobuzio-Donahue

Subjects

Article

Abstract

Multiple large-scale tumor genomic profiling efforts have been undertaken in osteosarcoma, however, little is known about the spatial and temporal intratumor heterogeneity and how it may drive treatment resistance. We performed whole-genome sequencing of 37 tumor samples from eight patients with relapsed or refractory osteosarcoma. Each patient had at least one sample from a primary site and a metastatic or relapse site. We identified subclonal copy number alterations in all but one patient. We observed that in five patients, a subclonal copy number clone from the primary tumor emerged and dominated at subsequent relapses.MYCgain/amplification was enriched in the treatment-resistant clone in 6 out of 7 patients with more than one clone. Amplifications in other potential driver genes, such asCCNE1,RAD21,VEGFA, andIGF1R, were also observed in the resistant copy number clones. Our study sheds light on intratumor heterogeneity and the potential drivers of treatment resistance in osteosarcoma.SignificanceSubclonal copy number clones emerged and dominated in relapsed osteosarcoma, withMYCgain/amplification being the defining characteristic in our cohort. Selective pressure from neoadjuvant chemotherapy revealed this clone at the time of primary resection, highlighting that genomic profiling at this time may identify clones that are selected for, or determine innate resistance to primary chemotherapy.

Published

2023

16. Irinotecan dose schedule for the treatment of Ewing sarcoma

Author

Emily K. Slotkin and Paul A. Meyers

Subjects

Dacarbazine, Oncology, Pediatrics, Perinatology and Child Health, Antineoplastic Combined Chemotherapy Protocols, Temozolomide, Humans, Camptothecin, Hematology, Sarcoma, Ewing, Neuroectodermal Tumors, Primitive, Peripheral, Neoplasm Recurrence, Local, Irinotecan

Abstract

Irinotecan and temozolomide achieve objective responses in patients with Ewing sarcoma that recurs after initial therapy. Optimal dose schedules have not been defined. We reviewed published series of patients treated with irinotecan and temozolomide for Ewing sarcoma that recurred after initial therapy. We compared objective response rates for patients who received 5-day irinotecan treatment schedules to response rates for patients who achieved 10-day irinotecan treatment schedules. Among 89 patients treated with a 10-day irinotecan schedule, there were 47 objective responses (53%). Among 180 patients treated with a 5-day irinotecan schedule, there were 52 responses (29%). In the treatment of recurrent Ewing sarcoma, investigators should consider the use of a 10-day schedule for administration of irinotecan.

Published

2022

17. Prospective Clinical Genomic Profiling of Ewing Sarcoma

Author

Koichi, Ogura, Arielle, Elkrief, Anita S, Bowman, Richard P, Koche, Elisa, de Stanchina, Ryma, Benayed, Audrey, Mauguen, Marissa S, Mattar, Inna, Khodos, Paul A, Meyers, John H, Healey, William D, Tap, Meera, Hameed, Ahmet, Zehir, Neerav, Shukla, Charles, Sawyers, Rohit, Bose, Emily, Slotkin, and Marc, Ladanyi

Subjects

Adult, Repressor Proteins, Biological Products, Mutation, Humans, Genomics, Neuroectodermal Tumors, Primitive, Peripheral, Prospective Studies, Receptor, Fibroblast Growth Factor, Type 1, Sarcoma, Ewing, United States

Abstract

Ewing sarcoma (ES) is a primitive sarcoma defined by EWSR1-ETS fusions as the primary driver alteration. To better define the landscape of cooperating secondary genetic alterations in ES, we analyzed clinical genomic profiling data of 113 patients with ES, a cohort including more adult patients (18 years) and more patients with advanced stage at presentation than previous genomic cohorts.The data set consisted of patients with ES prospectively tested with the US Food and Drug Administration-cleared Memorial Sloan Kettering-Integrated Mutation Profiling of Actionable Cancer Targets large panel, hybrid capture-based next-generation sequencing assay. To assess the functional significance ofNovel subsets were defined by recurrent secondary alterations inOur findings open avenues to new insights into ES pathobiology and to novel therapeutic approaches in a subset of patients with ES.

Published

2022

18. Oxalate utilisation is widespread in the actinobacterial genus Kribbella

Author

Caroline F.M. Robertson and Paul R. Meyers

Subjects

DNA, Bacterial, Oxalates, Bacteria, Formates, RNA, Ribosomal, 16S, Actinomycetales, Applied Microbiology and Biotechnology, Microbiology, Ecology, Evolution, Behavior and Systematics, Soil Microbiology, Phylogeny, Carbon, Antiporters

Abstract

The type strains of all 33 species in the genus Kribbella were tested for growth on oxalate (

Published

2022

19. Comprehensive Molecular Profiling of Desmoplastic Small Round Cell Tumor

Author

Marc Ladanyi, Nancy Bouvier, Nestor Rosales, Emily K. Slotkin, Filemon S. Dela Cruz, Todd E. Heaton, Max Levine, Mrinal M. Gounder, Paul A. Meyers, Andrew L. Kung, Anita S. Bowman, Katherine Anne Thornton, Neerav Shukla, Michael P. LaQuaglia, Shakeel Modak, Diego F. Coutinho, Leonard H. Wexler, Elli Papaemmanuil, Justin T. Gerstle, Ahmet Zehir, Glorymar Ibanez Sanchez, Gunes Gundem, William D. Tap, and Daoqi You

Subjects

Adult, Male, 0301 basic medicine, Cancer Research, Adolescent, DNA Copy Number Variations, Oncogene Proteins, Fusion, Desmoplastic small-round-cell tumor, ARID1A, Chromosomal translocation, Desmoplastic Small Round Cell Tumor, Article, Receptor tyrosine kinase, Loss of heterozygosity, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, medicine, Humans, Receptor, Fibroblast Growth Factor, Type 4, HRAS, Child, WT1 Proteins, Molecular Biology, biology, Gene Expression Profiling, High-Throughput Nucleotide Sequencing, Cancer, Fibroblast growth factor receptor 4, Middle Aged, medicine.disease, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Female, RNA-Binding Protein EWS, Multiplex Polymerase Chain Reaction

Abstract

Desmoplastic small round cell tumor (DSRCT) is characterized by the EWSR1–WT1 t(11;22) (p13:q12) translocation. Few additional putative drivers have been identified, and research has suffered from a lack of model systems. Next-generation sequencing (NGS) data from 68 matched tumor-normal samples, whole-genome sequencing data from 10 samples, transcriptomic and affymetrix array data, and a bank of DSRCT patient-derived xenograft (PDX) are presented. EWSR1–WT1 fusions were noted to be simple, balanced events. Recurrent mutations were uncommon, but were noted in TERT (3%), ARID1A (6%), HRAS (5%), and TP53 (3%), and recurrent loss of heterozygosity (LOH) at 11p, 11q, and 16q was identified in 18%, 22%, and 34% of samples, respectively. Comparison of tumor-normal matched versus unmatched analysis suggests overcalling of somatic mutations in prior publications of DSRCT NGS data. Alterations in fibroblast growth factor receptor 4 (FGFR4) were identified in 5 of 68 (7%) of tumor samples, whereas differential overexpression of FGFR4 was confirmed orthogonally using 2 platforms. PDX models harbored the pathognomic EWSR1–WT1 fusion and were highly representative of corresponding tumors. Our analyses confirm DSRCT as a genomically quiet cancer defined by the balanced translocation, t(11;22)(p13:q12), characterized by a paucity of secondary mutations but a significant number of copy number alterations. Against this genomically quiet background, recurrent activating alterations of FGFR4 stood out, and suggest that this receptor tyrosine kinase, also noted to be highly expressed in DSRCT, should be further investigated. Future studies of DSRCT biology and preclinical therapeutic strategies should benefit from the PDX models characterized in this study.Implications:These data describe the general quiescence of the desmoplastic small round cell tumor (DSRCT) genome, present the first available bank of DSRCT model systems, and nominate FGFR4 as a key receptor tyrosine kinase in DSRCT, based on high expression, recurrent amplification, and recurrent activating mutations.

Published

2021

20. Abstract 3556: Assessing patterns of genomic instability in recurrent osteosarcoma

Author

Michael David Kinnaman, Simone Zaccaria, Alvin Makohon-Moore, Gunes Gundem, Juan E. Arango Ossa, Filemon S. Dela Cruz, Paul A. Meyers, Meera Hameed, William D. Tap, Julia Lynne Glade Bender, Elli Papaemmanuil, Andrew Kung, and Christine Iacobuzio Donahue

Subjects

Cancer Research, Oncology

Abstract

Objective: The osteosarcoma genome is characterized by high levels of genomic instability, however whether there is pervasive ongoing genomic instability, or instability introduced by an early catastrophic event, is still unsettled. Methods: We performed 30-80x whole genome sequencing (WGS) of 37 tumor samples from 8 patients with relapsed or refractory osteosarcoma. Each patient had at least one sample from a primary site and one sample from a metastatic or relapse site. A set of high confidence single nucleotide variants (SNV), copy number alterations (CNA), structural variations (SV) were called for each sample using our pediatric expanded genomics pipeline and an analysis focused on markers of genomic instability was performed using a custom pipeline of computational tools. Results: Of the 8 patients in our cohort, 4 had localized disease at diagnosis (OSCE4, OSCE5, OSCE6, OSCE9) and 4 had metastatic disease at diagnosis (OSCE1, OSCE2, OSCE3, OSCE10). There were 17 samples from primary sites, 7 pretreatment biopsies, 10 on therapy primary resections, 20 metastatic sites, 15 of which were from lung metastases. We have previously reported on the clonal evolution regarding SNVs and CNAs within this cohort. TP53 structural variants involving intron 1/2 were seen in 6/8 patients (OSCE2, OSCE3, OSCE4, OSCE6, OSCE9, OSCE10). No new structural variants in consensus driver genes emerged in metastatic or relapse samples. Comparing the earliest sample to most recent sample in each patient, only OSCE1, OSCE9, and OSCE10 demonstrated an increase of ≥100 structural variants at the final timepoint. In OSCE2, OSCE5, and OSCE6, there were less structural variants identified at the final timepoint when compared to the earliest timepoint. Homologous recombination deficiency (HRD) scores were calculated for each sample. Only 4/8 patients (OSCE3, OSCE4, OSCE9, OSCE10) had an HRD score in the most recently acquired sample higher than the score from the primary site. Regions of hypermutation consistent with kataegis were identified for each sample, with the number of kataegis events remaining unchanged or decreasing in some instances. Kataegis events co-localized with rearrangement events a majority of the time (range 50-100%, Avg= 72.6%). Complex rearrangements such as chromothripsis and chromoplexy were assesed. In 6 patients there were > 9 chromosomal arms involved in complex rearrangements that were shared between primary sites and metastatic/recurrent sites, while ≤ 4 chromosomal arms were involved with new complex rearrangements unique to the metastatic sites. Conclusion: The patterns observed in our cohort reveal that osteosarcoma is relatively stable from diagnosis through subsequent relapses, supporting the model that an early catastrophic event accounts for the genomic instability observed in osteosarcoma. Citation Format: Michael David Kinnaman, Simone Zaccaria, Alvin Makohon-Moore, Gunes Gundem, Juan E. Arango Ossa, Filemon S. Dela Cruz, Paul A. Meyers, Meera Hameed, William D. Tap, Julia Lynne Glade Bender, Elli Papaemmanuil, Andrew Kung, Christine Iacobuzio Donahue. Assessing patterns of genomic instability in recurrent osteosarcoma. [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 1 (Regular and Invited Abstracts); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(7_Suppl):Abstract nr 3556.

Published

2023

21. DICER1-associated central nervous system sarcoma in children: comprehensive clinicopathologic and genetic analysis of a newly described rare tumor

Author

Abigail Ward, Katherine A. Janeway, Junne Kamihara, Kris Ann P. Schultz, Catherine Clinton, Jonathan A. Nowak, Elizabeth Mullen, Steven G. DuBois, Deirdre Reidy, Sara O. Vargas, David S. Shulman, William D. Foulkes, Dinesh Rakheja, Micheál Breen, Vera A. Paulson, Alanna J. Church, Michelle Schoettler, Jaclyn Schienda, Theodore W. Laetsch, Paul A. Meyers, Daniel A. Weiser, and R. Seth Pinches

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Chemotherapy, business.industry, Cartilage, medicine.medical_treatment, Disease, medicine.disease, Malignancy, Germline, Pathology and Forensic Medicine, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Eosinophilic, medicine, Desmin, Sarcoma, business

Abstract

The spectrum of neoplasms associated with DICER1 variants continues to expand, with the recent addition of primary “DICER1-associated central nervous system sarcoma” (DCS). DCS is a high-grade malignancy predominantly affecting pediatric patients. Six pediatric DCS were identified through a combination of clinical diagnostic studies, archival inquiry, and interinstitutional collaboration. Clinical, histologic, immunohistologic, and molecular features were examined. Genomic findings in the 6 DCS were compared with those in 14 additional DICER1-associated tumors sequenced with the same assay. The six patients presented at ages 3–15 years with CNS tumors located in the temporal (n = 2), parietal (n = 1), fronto-parietal (n = 1), and frontal (n = 2) lobes. All underwent surgical resection. Histologic examination demonstrated high-grade malignant spindle cell tumors with pleuropulmonary blastoma-like embryonic “organoid” features and focal rhabdomyoblastic differentiation; immature cartilage was seen in one case. Immunohistochemically, there was patchy desmin and myogenin staining, and patchy loss of H3K27me3, and within eosinophilic cytoplasmic globules, alfa-fetoprotein staining. Biallelic DICER1 variants were identified in all cases, with germline variants in two of five patients tested. DCS demonstrated genomic alterations enriched for Ras pathway activation and TP53 inactivation. Tumor mutational burden was significantly higher in the 6 DCS tumors than in 14 other DICER1-associated tumors examined (mean 12.9 vs. 6.8 mutations/Mb, p = 0.035). Postoperative care included radiation (n = 5) and chemotherapy (n = 3); at the last follow-up, three patients were alive without DCS, and three had died of disease. Our analysis expands the clinical, histologic, immunohistological, and molecular spectrum of DCS, identifying distinctive features that can aid in the diagnosis, multidisciplinary evaluation, and treatment of DCS.

Published

2020

22. Deep Learning-Based Objective and Reproducible Osteosarcoma Chemotherapy Response Assessment and Outcome Prediction

Author

David J. Ho, Narasimhan P. Agaram, Marc-Henri Jean, Stephanie D. Suser, Cynthia Chu, Chad M. Vanderbilt, Paul A. Meyers, Leonard H. Wexler, John H. Healey, Thomas J. Fuchs, and Meera R. Hameed

Subjects

FOS: Computer and information sciences, Computer Vision and Pattern Recognition (cs.CV), Computer Science - Computer Vision and Pattern Recognition, Pathology and Forensic Medicine

Abstract

Osteosarcoma is the most common primary bone cancer whose standard treatment includes pre-operative chemotherapy followed by resection. Chemotherapy response is used for predicting prognosis and further management of patients. Necrosis is routinely assessed post-chemotherapy from histology slides on resection specimens where necrosis ratio is defined as the ratio of necrotic tumor to overall tumor. Patients with necrosis ratio >=90% are known to have better outcome. Manual microscopic review of necrosis ratio from multiple glass slides is semi-quantitative and can have intra- and inter-observer variability. We propose an objective and reproducible deep learning-based approach to estimate necrosis ratio with outcome prediction from scanned hematoxylin and eosin whole slide images. We collected 103 osteosarcoma cases with 3134 WSIs to train our deep learning model, to validate necrosis ratio assessment, and to evaluate outcome prediction. We trained Deep Multi-Magnification Network to segment multiple tissue subtypes including viable tumor and necrotic tumor in pixel-level and to calculate case-level necrosis ratio from multiple WSIs. We showed necrosis ratio estimated by our segmentation model highly correlates with necrosis ratio from pathology reports manually assessed by experts where mean absolute differences for Grades IV (100%), III (>=90%), and II (>=50% and

Published

2022

23. Development of a Kribbella-specific isolation medium and description of Kribbella capetownensis sp. nov. and Kribbella speibonae sp. nov., isolated from soil

Author

Sarah M. Curtis, James G Pelser, Gareth J. Everest, Paul R. Meyers, Iulia Norton, and Marli C de Kock

Subjects

0106 biological sciences, 0301 basic medicine, Sequence analysis, Biology, 010603 evolutionary biology, 01 natural sciences, Microbiology, Kribbella pittospori, South Africa, 03 medical and health sciences, RNA, Ribosomal, 16S, Actinomycetales, Molecular Biology, Phylogeny, Soil Microbiology, Genetics, Strain (biology), Kribbella, General Medicine, rpoB, 16S ribosomal RNA, Isolation (microbiology), biology.organism_classification, Actinobacteria, 030104 developmental biology, Genus Kribbella, Genes, Bacterial, Multilocus Sequence Typing

Abstract

Two actinobacterial strains were isolated from samples collected from the University of Cape Town, South Africa. A third actinobacterial strain was isolated from soil collected in the town of Stellenbosch, South Africa, using a newly-developed Kribbella-selective medium. Analysis of the 16S rRNA genes showed that the three strains belonged to the genus Kribbella. A multilocus sequence analysis using the concatenated gene sequences of the gyrB, rpoB, relA, recA and atpD genes showed that strains YM55T and SK5 were most closely related to the type strains of Kribbella sindirgiensis and Kribbella soli, while strain YM53T was most closely related to the type strain of Kribbella pittospori. Digital DNA–DNA hybridisation and Average Nucleotide Identity (ANI) analyses showed that strains YM55T and SK5 belong to the same genomic species (OrthoANI value = 98.4%), but are distinct from the genomic species represented by the type strains of K. sindirgiensis (OrthoANI values

Published

2019

24. Ewing sarcoma withFEVgene rearrangements is a rare subset with predilection for extraskeletal locations and aggressive behavior

Author

Cristina R. Antonescu, John H. Healey, Brendan C. Dickson, David Swanson, Yusuke Tsuda, Lei Zhang, Paul A. Meyers, and Yun-Shao Sung

Subjects

Adult, Male, Cancer Research, Pathology, medicine.medical_specialty, Adolescent, Oncogene Proteins, Fusion, Bone Neoplasms, Soft Tissue Neoplasms, Sarcoma, Ewing, Biology, Article, Translocation, Genetic, Metastasis, Young Adult, 03 medical and health sciences, Exon, 0302 clinical medicine, Immunophenotyping, Transcriptional Regulator ERG, Biomarkers, Tumor, Genetics, medicine, Humans, Neoplasm Metastasis, Child, Gene, Transcription factor, Gene Rearrangement, medicine.diagnostic_test, Microfilament Proteins, DNA-binding domain, Middle Aged, Prognosis, medicine.disease, DNA-Binding Proteins, Survival Rate, Child, Preschool, 030220 oncology & carcinogenesis, Trans-Activators, RNA-Binding Protein FUS, Female, Sarcoma, RNA-Binding Protein EWS, Transcription Factors, Fluorescence in situ hybridization

Abstract

The molecular hallmark of Ewing sarcoma (ES) is a fusion involving the EWSR1 gene and a member of the ETS family of transcription factors. EWSR1-FLI1 is the most common variant, occurring in 90% of cases, followed by EWSR1-ERG. In a small subset, the FUS gene can substitute for EWSR1 in these fusions. Only rare case reports have been described to date of ES with FEV gene rearrangements. In this study, we investigate the clinicopathologic and molecular features of 10 ES patients with FEV-rearrangements, either fused to EWSR1 (n = 4) or to FUS (n = 6). The median age at diagnosis was 38 years (range, 5-61 years); occurring in six males and four females. All tumors were located at extraskeletal sites, occurring more often in the axial soft tissues. Tumors had a similar morphologic appearance and immunophenotype as ES with more common EWSR1-ETS fusions. Of six patients with follow-up data, five patients (83%) developed metastasis and two patients (33%) died of their diseases. The diagnosis was confirmed either by fluorescence in situ hybridization and/or targeted RNA sequencing. In the five cases tested by targeted sequencing, the fusion transcripts were composed of EWSR1 or FUS fused to either exon 1 or 2 of FEV, retaining the FEV ETS DNA binding domain. This is the largest study to date investigating the ES subset with EWSR1/FUS-FEV fusions showing a predilection for extraskeletal sites and aggressive behavior.

Published

2019

25. Discovery of Novel Cyclic Ethers with Synergistic Antiplasmodial Activity in Combination with Valinomycin

Author

Daniel J. Watson, Paul R. Meyers, Kojo Sekyi Acquah, Godwin A. Dziwornu, Christopher Bevan Barnett, and Lubbe Wiesner

Subjects

malaria, ionophores, cyclic ethers, polypropylene glycol, valinomycin, synergy, Cell Survival, Plasmodium falciparum, Drug Resistance, Pharmaceutical Science, Organic chemistry, CHO Cells, Article, Analytical Chemistry, Antimalarials, Cricetulus, QD241-441, Parasitic Sensitivity Tests, Ethers, Cyclic, Drug Discovery, Animals, Physical and Theoretical Chemistry, Dose-Response Relationship, Drug, Streptomyces, Chemistry (miscellaneous), Molecular Medicine

Abstract

With drug resistance threatening our first line antimalarial treatments, novel chemotherapeutics need to be developed. Ionophores have garnered interest as novel antimalarials due to their theorized ability to target unique systems found in the Plasmodium-infected erythrocyte. In this study, during the bioassay-guided fractionation of the crude extract of Streptomyces strain PR3, a group of cyclodepsipeptides, including valinomycin, and a novel class of cyclic ethers were identified and elucidated. Further study revealed that the ethers were cyclic polypropylene glycol (cPPG) oligomers that had leached into the bacterial culture from an extraction resin. Molecular dynamics analysis suggests that these ethers are able to bind cations such as K+, NH4+ and Na+. Combination studies using the fixed ratio isobologram method revealed that the cPPGs synergistically improved the antiplasmodial activity of valinomycin and reduced its cytotoxicity in vitro. The IC50 of valinomycin against P. falciparum NF54 improved by 4–5-fold when valinomycin was combined with the cPPGs. Precisely, it was improved from 3.75 ± 0.77 ng/mL to 0.90 ± 0.2 ng/mL and 0.75 ± 0.08 ng/mL when dosed in the fixed ratios of 3:2 and 2:3 of valinomycin to cPPGs, respectively. Each fixed ratio combination displayed cytotoxicity (IC50) against the Chinese Hamster Ovary cell line of 57–65 µg/mL, which was lower than that of valinomycin (12.4 µg/mL). These results indicate that combinations with these novel ethers may be useful in repurposing valinomycin into a suitable and effective antimalarial.

Published

2021

26. Ewing’s Sarcoma

Author

Paul A. Meyers, Joseph A. Ludwig, and Uta Dirksen

Subjects

business.industry, Medizin, MEDLINE, Ewing's sarcoma, Bone Neoplasms, Tumor cells, Sarcoma, Ewing, General Medicine, medicine.disease, Tumor Cells, Cultured, Cancer research, Humans, Medicine, Sarcoma, business

Published

2021

27. Clinical sequencing of soft tissue and bone sarcomas delineates diverse genomic landscapes and potential therapeutic targets

Author

Cerise Tang, Hongyu Shi, Timothy G. Bowler, Jake Stoller, Meera Hameed, Neerav Shukla, John H. Healey, Sandra P. D'Angelo, Aimee M. Crago, Ciara Marie Kelly, Mary Louise Keohan, Emily K. Slotkin, Nicholas D. Socci, Cristina R. Antonescu, Ping Chi, Leonard H. Wexler, Samuel Singer, Azusa Okada, Michael P. La Quaglia, Ahmet Zehir, Julia Glade Bender, Satshil Rana, Evan Rosenbaum, Brian R. Untch, Nikolaus Schultz, Jason E. Chan, Jonathan A. Strong, Sujana Movva, Benjamin A. Nacev, Mrinal M. Gounder, David B. Solit, Kaled M. Alektiar, Paul A. Meyers, Shaleigh A. Smith, Rodrigo Gularte-Mérida, Bhumika Jadeja, Martee L. Hensley, Sarah Chiang, Francisco Sanchez-Vega, Sam S. Yoon, Narasimhan P. Agaram, Mark A. Dickson, Katherine Thornton, Michael F. Berger, William D. Tap, Anisha Luthra, and Marc Ladanyi

Subjects

Clinical research, Somatic cell, biology.protein, medicine, Cancer research, Sarcoma, Epigenetics, Biology, Bone Sarcoma, medicine.disease, Genome, Receptor tyrosine kinase, PI3K/AKT/mTOR pathway

Abstract

The genetic, biologic, and clinical heterogeneity of sarcomas poses a challenge for the identification of therapeutic targets, clinical research, and advancing patient care. Because there are > 100 sarcoma subtypes, in-depth genetic studies have focused on one or a few subtypes. Herein, we report a comparative genetic analyses analysis of 2,138 sarcomas representing 45 pathological entities. This cohort was prospectively analyzed using targeted sequencing to characterize subtype-specific somatic alterations in targetable pathways, rates of whole genome doubling, mutational signatures, and subtype-agnostic genomic clusters. The most common alterations were in cell cycle control andTP53, receptor tyrosine kinases/PI3K/RAS, and epigenetic regulators. Subtype-specific associations includedTERTamplification in intimal sarcoma and SWI/SNF alterations in uterine adenosarcoma. Tumor mutational burden, while low compared to other cancers, varied between and within subtypes. This resource will improve sarcoma models, motivate studies of subtype-specific alterations, and inform investigations of genetic factors and their correlations with treatment response.

Published

2021

28. Abstract B023: Prospective clinical genomic profiling of ewing sarcoma: ERF and FGFR1 mutations as recurrent secondary alterations of potential biological and therapeutic relevance

Author

Arielle Elkrief, Koichi Ogura, Anita S. Bowman, Richard P. Koche, Ryma Benayed, Audrey Mauguen, Marissa S. Mattar, Inna Khodos, Elisa de Stanchina, Paul A. Meyers, John H. Healey, William D. Tap, Neerav Shukla, Meera Hameed, Ahmet Zehir, Charles Sawyers, Rohit Bose, Emily Slotkin, and Marc Ladanyi

Subjects

Cancer Research, Oncology

Abstract

Background: Ewing Sarcoma (ES) is a primitive sarcoma defined by EWSR1–ETS fusions as the primary driver alteration. To expand our understanding of the genetic and molecular characterization of ES, we conducted a comprehensive analysis of clinical genomic profiling data on tumors from 113 patients using the MSK-IMPACT platform (Integrated Mutation Profiling of Actionable Cancer Targets). Methods: The dataset consisted of ES patients prospectively tested with the FDA-cleared MSK-IMPACT large panel, hybrid capture-based NGS assay. To assess the functional significance of ERF loss, we generated ES cell lines with increased expression of ERF as well as lines with knockdown of ERF. We assessed cell viability, clonogenic growth, and motility and performed transcriptomic and epigenetic analyses. Finally, we validated our findings in vivo using cell line xenografts. Results: Unlike previous ES genomic cohorts, ours included more adult patients (>18 years of age) and more patients with advanced stage at presentation. TP53, STAG2, and CDKN2A were the most common alterations and were associated with worse overall survival at 5-years. Notably, 3% had activating FGFR1 alterations (1 amplification and 2 hotspot activating kinase domain mutations). Mining data generated using a targeted RNAseq assay that includes FGFR1 based on the Archer Anchored Multiplex PCR technology, FGFR1 was highly expressed in the ES cohort (N=42). The 2 patients with activating FGFR1 mutations had relatively high expression of FGFR1. The second novel subset of patients in our cohort were defined by recurrent secondary alterations in ERF, which encodes an ETS domain transcriptional repressor, in 7% of patients (5 truncating mutations, 1 deep deletion, 2 missense mutations). ERF alterations were non-overlapping with STAG2 alterations, suggesting a potentially important biologic role in ES. As the functional significance of FGFR1 mutation in ES has been previously studied, we focused our functional studies on the role of ERF status in ES. In vitro, increased expression of ERF decreased tumor cell growth, colony formation, and motility in two ES cell lines, while ERF loss induced cellular proliferation and clonogenic growth. Transcriptomic analysis of cell lines with ERF loss revealed increased expression of genes and pathways associated with aggressive tumor biology, and epigenetic, chromatin-based studies revealed that ERF competes with EWSR1-FLI1 at ETS binding sites. Conclusion: Our study reveals a previously unexplored role of ERF loss-of-function in ES. Older age in our cohort, and a higher proportion of patients with advanced disease at presentation, could potentially explain the finding of ERF alterations which were associated with aggressive tumor biology in our preclinical studies. Our functional analyses of how ERF modulates EWSR1-FLI1 oncogenicity may open a new window into the pathobiology of ES. Moreover, our data suggest that 3% of ES patients harbor activating FGFR1 mutations, the first targetable kinase alteration in this sarcoma. Citation Format: Arielle Elkrief, Koichi Ogura, Anita S. Bowman, Richard P. Koche, Ryma Benayed, Audrey Mauguen, Marissa S. Mattar, Inna Khodos, Elisa de Stanchina, Paul A. Meyers, John H. Healey, William D. Tap, Neerav Shukla, Meera Hameed, Ahmet Zehir, Charles Sawyers, Rohit Bose, Emily Slotkin, Marc Ladanyi. Prospective clinical genomic profiling of ewing sarcoma: ERF and FGFR1 mutations as recurrent secondary alterations of potential biological and therapeutic relevance [abstract]. In: Proceedings of the AACR Special Conference: Sarcomas; 2022 May 9-12; Montreal, QC, Canada. Philadelphia (PA): AACR; Clin Cancer Res 2022;28(18_Suppl):Abstract nr B023.

Published

2022

29. Prospective pan-cancer germline testing using MSK-IMPACT informs clinical translation in 751 patients with pediatric solid tumors

Author

Yasmin Khakoo, Maria I. Carlo, Elise Fiala, Ozge Ceyhan-Birsoy, Leonard H. Wexler, Nancy Bouvier, Diana Mandelker, Jasmine H. Francis, Alicia Latham, Sowmya Jairam, Marc Ladanyi, Gowtham Jayakumaran, Sameer Farouk Sait, Filemon S. Dela Cruz, Ira J. Dunkel, Michael Walsh, Michael F. Berger, Todd E. Heaton, Ellen M. Basu, Matthias A. Karajannis, Ciyu Yang, Christopher J. Forlenza, Neerav Shukla, Emily K. Slotkin, Julia Glade Bender, Tanya M. Trippett, Nai-Kong Cheung, Danielle Novetsky Friedman, Justin T. Gerstle, Semanti Murkherjee, Ahmet Zehir, Zsofia K. Stadler, Erin E. Salo-Mullen, Maria Luisa Sulis, Yelena Kemel, Karen Cadoo, Sabine Topka, Jennifer Kennedy, Megan Harlan Fleischut, Nikolaus Schultz, Richard J. O'Reilly, Anna Maio, Margaret Sheehan, Shakeel Modak, Michael V. Ortiz, Alex Kentsis, Andrew L. Kung, Paul A. Meyers, Stephen S. Roberts, Kenneth Offit, Angela G. Arnold, Mark E. Robson, David H. Abramson, Stephen Gilheeney, Liying Zhang, Audrey Mauguen, and Joseph Vijai

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Cascade testing, Pediatric Cancer, Germline, Article, Rare Diseases, Clinical Research, Internal medicine, Neoplasms, Genetics, medicine, 2.1 Biological and endogenous factors, Humans, Genetic Predisposition to Disease, Genetic Testing, Prospective Studies, Aetiology, Child, Likely pathogenic, Germ-Line Mutation, Cancer, Pediatric, screening and diagnosis, Pan cancer, business.industry, Human Genome, medicine.disease, Penetrance, Pediatric cancer, Detection, Good Health and Well Being, Germ Cells, Medical genetics, business, 4.2 Evaluation of markers and technologies

Abstract

The spectrum of germline predisposition in pediatric cancer continues to be realized. Here we report 751 solid tumor patients who underwent prospective matched tumor-normal DNA sequencing and downstream clinical use (clinicaltrials.gov NCT01775072). Germline pathogenic and likely pathogenic (P/LP) variants were reported. One or more P/LP variants were found in 18% (138/751) of individuals when including variants in low, moderate, and high penetrance dominant or recessive genes, or 13% (99/751) in moderate and high penetrance dominant genes. 34% of high or moderate penetrance variants were unexpected based on the patient's diagnosis and previous history. 76% of patients with positive results completed a clinical genetics visit, and 21% had at least one relative undergo cascade testing as a result of this testing. Clinical actionability additionally included screening, risk reduction in relatives, reproductive use, and use of targeted therapies. Germline testing should be considered for all children with cancer.

Published

2021

30. Clinical Genomic Sequencing of Pediatric and Adult Osteosarcoma Reveals Distinct Molecular Subsets with Potentially Targetable Alterations

Author

Neerav Shukla, Meera Hameed, Achim A. Jungbluth, Debyani Chakravarty, Ahmet Zehir, George Jour, Yoshiyuki Suehara, Anita S. Bowman, Denise Frosina, Takuo Hayashi, Emily K. Slotkin, Marc Ladanyi, Paul A. Meyers, John H. Healey, Deepu Alex, Khedoudja Nafa, Lu Wang, and Sumit Middha

Subjects

Adult, Male, 0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Adolescent, Genomics, PDGFRA, Article, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Humans, Medicine, Molecular Targeted Therapy, Precision Medicine, Young adult, Child, Aged, Aged, 80 and over, Osteosarcoma, business.industry, Gene Amplification, Chromosome Mapping, High-Throughput Nucleotide Sequencing, Middle Aged, Precision medicine, medicine.disease, Neoplasm Proteins, Clinical trial, 030104 developmental biology, PTCH1, 030220 oncology & carcinogenesis, Mutation, Immunohistochemistry, Female, business

Abstract

Purpose: Although multimodal chemotherapy has improved outcomes for patients with osteosarcoma, the prognosis for patients who present with metastatic and/or recurrent disease remains poor. In this study, we sought to define how often clinical genomic sequencing of osteosarcoma samples could identify potentially actionable alterations. Experimental Design: We analyzed genomic data from 71 osteosarcoma samples from 66 pediatric and adult patients sequenced using MSK-IMPACT, a hybridization capture-based large panel next-generation sequencing assay. Potentially actionable genetic events were categorized according to the OncoKB precision oncology knowledge base, of which levels 1 to 3 were considered clinically actionable. Results: We found at least one potentially actionable alteration in 14 of 66 patients (21%), including amplification of CDK4 (n = 9, 14%: level 2B) and/or MDM2 (n = 9, 14%: level 3B), and somatic truncating mutations/deletions in BRCA2 (n = 3, 5%: level 2B) and PTCH1 (n = 1, level 3B). In addition, we observed mutually exclusive patterns of alterations suggesting distinct biological subsets defined by gains at 4q12 and 6p12-21. Specifically, potentially targetable gene amplifications at 4q12 involving KIT, KDR, and PDGFRA were identified in 13 of 66 patients (20%), which showed strong PDGFRA expression by IHC. In another largely nonoverlapping subset of 14 patients (24%) with gains at 6p12-21, VEGFA amplification was identified. Conclusions: We found potentially clinically actionable alterations in approximately 21% of patients with osteosarcoma. In addition, at least 40% of patients have tumors harboring PDGFRA or VEGFA amplification, representing candidate subsets for clinical evaluation of additional therapeutic options. We propose a new genomically based algorithm for directing patients with osteosarcoma to clinical trial options.

Published

2019

31. Effects of dexrazoxane on doxorubicin-related cardiotoxicity and second malignant neoplasms in children with osteosarcoma: a report from the Children’s Oncology Group

Author

Cindy L. Schwartz, Richard Gorlick, David H. Ebb, Donald A. Barkauskas, Paul A. Meyers, Leonard H. Wexler, Lisa M. Kopp, Neyssa Marina, Mark Krailo, Mark L. Bernstein, Vivian I. Franco, Steven E. Lipshultz, David Hall, Holcombe E. Grier, Richard B. Womer, and Katherine A. Janeway

Subjects

Oncology, medicine.medical_specialty, lcsh:Diseases of the circulatory (Cardiovascular) system, medicine.drug_class, Population, Pediatrics, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Natriuretic peptide, Doxorubicin, 030212 general & internal medicine, education, education.field_of_study, Cardiotoxicity, Osteosarcoma, business.industry, Research, General Medicine, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 3. Good health, lcsh:RC666-701, 030220 oncology & carcinogenesis, Heart failure, Dexrazoxane, Sarcoma, business, medicine.drug

Abstract

Background Dexrazoxane protects from lower-cumulative-dose doxorubicin cardiotoxicity, but the effect of dexrazoxane in children with sarcoma treated with higher-cumulative-dose doxorubicin is unknown. Methods We evaluated children with osteosarcoma (OS) on two Children’s Oncology Group trials with higher dose doxorubicin (375–600 mg/m2) preceded by dexrazoxane (10:1 dexrazoxane:doxorubicin dosing). They were evaluated after the minimum expected treatment time (METT), defined as 28 weeks. Cardiotoxicity was identified by echocardiography and serum N-terminal pro-brain natriuretic peptide (NT-proBNP). Second malignant neoplasm (SMN) data was collected. Results All children had normal left ventricular (LV) systolic function as measured by LV fractional shortening and no heart failure. The end-diastolic septal thickness Z-scores (P Z-scores (P Z-scores were significantly smaller for girls (P P = 0.06). Girls had significantly smaller LV end-diastolic dimension Z-scores normalized to BSA (P Conclusions Dexrazoxane prevented LV dysfunction and heart failure in children with OS receiving higher dose doxorubicin. However, LV structural changes were not fully prevented, especially in girls. As a result, hearts become abnormally small for body size, resulting in higher LV stress. Dexrazoxane did not increase the risk of SMN. Dexrazoxane should be used in this population, particularly for girls, to mitigate anthracycline-induced cardiotoxicity. Trial registrations ClinicalTrials.gov: NCT00003937 (P9754) registered 1 Nov 1999, and NCT00023998 (AOST0121) registered 13 Sept 2001.

Published

2019

32. Subclonal somatic copy number alterations emerge and dominate in recurrent osteosarcoma

Author

Michael David Kinnaman, Simone Zaccaria, Alvin Makohon-Moore, Gunes Gundem, Juan E. Arango Ossa, Nancy Bouvier, Filemon S. Dela Cruz, Meera Hameed, Julia Lynne Glade Bender, William D. Tap, Paul A. Meyers, Elli Papaemmanuil, Andrew Kung, and Christine A Iacobuzio-Donahue

Subjects

Cancer Research, Oncology

Abstract

11533 Background: Multiple large-scale tumor genomic profiling efforts have been undertaken in osteosarcoma, however little is known about the spatial and temporal intratumor heterogeneity and how it may drive treatment resistance. Methods: We performed 30-80x whole genome sequencing (WGS) of 37 tumor samples from 8 patients with relapsed or refractory osteosarcoma. A set of high confidence single nucleotide variants (SNV), copy number alterations (CNA), structural variations (SV) were called for each sample using our pediatric expanded genomics pipeline and an evolutionary analysis was performed using a custom pipeline of computational tools. Results: Of the 8 patients in our cohort, 4 had localized disease at diagnosis (OSCE4, OSCE5, OSCE6, OSCE9) and 4 had metastatic disease at diagnosis (OSCE1, OSCE2, OSCE3, OSCE10). There were 17 samples from primary sites, 7 were pretreatment biopsies, 10 from on therapy primary resections. 20 samples came from metastatic sites, 15 of which were from lung metastases. Driver gene SNV’s were identified in 5 of 8 patients, including TP53 (OSCE1), ATRX (OSCE3, OSCE10), RB1 (OSCE4), and CDKN2A (OSCE9). No new driver SNV’s emerged post-therapy in any patient. HATCHet, an algorithm which infers clone specific copy number alterations, identified subclonal CNAs in all but one patient (OSCE2). In the 7 patients with subclonal CNAs, 6 had two copy number clones identified, and 1 patient (OSCE10) had three copy number clones identified. In 5 patients (OSCE1, OSCE4, OSCE5, OSCE6, OSCE10) there is a copy number clone that is subclonal in the primary tumor which emerges and dominates at subsequent relapses. The resistant clone in each of these cases had either MYC gain/amplification. Amplifications in CCNE1 (OSCE1), RAD21 (OSCE4, OSCE5, OSCE10), VEGFA (OSCE1, OSCE9), IGF1R (OSCE6) were also identified as potential drivers in the resistant copy number clones. In two of these patients (OSCE1, OSCE6), the treatment resistant subclone becomes the dominant copy number clone by the time of primary resection. SNV based phylogenies revealed monoclonal and polyclonal seeding of metastases and monophyletic and polyphyletic modes of dissemination. Over half the new mutations acquired in recurrent disease were attributed to HRD or cisplatin mutational signatures. Conclusions: Subclonal copy number clones emerge and dominate in relapsed osteosarcoma, with MYC gain/amplification a defining characteristic in our cohort. Selective pressure from neoadjuvant chemotherapy reveals this clone at the time of primary resection, implying genomic profiling at this timepoint may be more reflective of its metastatic potential. [Table: see text]

Published

2022

33. A phase I/II study of prexasertib in combination with irinotecan in patients with relapsed/refractory desmoplastic small round cell tumor and rhabdomyosarcoma

Author

Emily K Slotkin, Audrey Mauguen, Michael Vincent Ortiz, Filemon S. Dela Cruz, Tara O'Donohue, Michael David Kinnaman, Paul A. Meyers, Leonard H. Wexler, Scarlett Rodriguez, Viswatej Avutu, Ciara Marie Kelly, Sandra P. D'Angelo, Mary Louise Keohan, Mrinal M. Gounder, Benjamin Alexander Nacev, Evan Rosenbaum, Mark Andrew Dickson, Katherine Anne Thornton, Julia Lynne Glade Bender, and William D. Tap

Subjects

Cancer Research, Oncology

Abstract

11503 Background: Prexasertib (PRX) is an inhibitor of CHK1, prevents DNA repair leading to mitotic catastrophe, and can enhance the activity of DNA-damaging chemotherapy. Translocation driven sarcomas exhibit high levels of replication stress and have demonstrated susceptibility to CHK1 inhibition in preclinical models. Desmoplastic small round cell tumor (DSRCT) and rhabdomyosarcoma (RMS) are aggressive sarcomas of children, adolescents and young adults for which novel therapies are urgently required. Methods: We conducted a phase I/II trial of PRX with irinotecan (irino) in patients ≥ 12 months of age with relapsed or refractory DSRCT or RMS. Eligible patients could have any number of prior therapies, including irino. Dose level 1 was PRX 80 mg/m2 on day 1 + irino 20 mg/m2 for 10 days. Dose levels 2 and 2A were PRX 105 or 150 mg/m2 (>21 years or ≤ 21 years) on day 1 and irino 20 mg/m2 for 10 (level 2) or 5 (level 2A) days. All cycles were 21 days. The primary objectives were to determine the RP2D of PRX with irino, and to determine the best overall response rate (ORR) in 6 months at the RP2D (RECIST v1.1) in DSRCT, with 3 or more responses out of 16 considered promising. Results: 21 patients were enrolled (DSRCT: 19; 2 RMS:2). The RP2D was dose level 2A. Treatment was well tolerated with the most common adverse events being neutropenia (48%), nausea (48%), and fatigue (52%). Cytopenias were managed with the aid of growth factor support in all patients once the RP2D was established. The DSRCT expansion enrolled 13 of 16 planned patients due to discontinuation of PRX supply prior to study completion. Four patients remain on therapy at the time of this submission. Responses in DSRCT patients at all dose levels are shown in Table. Sixteen of 21 enrolled patients, and 5 of 6 patients achieving PR had previously received irino. The median (range) number of cycles was 7 (2-26). Both RMS patients treated at the RP2D experienced SD as best response. The estimated ORR at the RP2D was 23%, and lower boundary of the one-sided 90% confidence interval was 9%, exceeding the unpromising rate of 5%. The two-sided 90% confidence interval was 7 to 49%. In addition, 3 patients had a PR at doses lower than the RP2D, bringing the ORR for all dose levels (n = 19) to 32% (90%CI: 15 to 53%). Conclusions: The RP2D of PRX in combination with irino is PRX 105 or 150 mg/m2 (>21 years or ≤ 21 years) on day 1 and irino 20 mg/m2 for 5 days in 21 day cycles with myelosuppression successfully managed with growth factor support. The study met its primary objective to consider PRX + irino promising in DSRCT and should be further investigated. Clinical trial information: NCT04095221. [Table: see text]

Published

2022

34. Osteosarcoma: History of Therapy

Author

Paul A. Meyers

Subjects

Oncology, Cisplatin, medicine.medical_specialty, Ifosfamide, business.industry, Combination chemotherapy, medicine.disease, Primary tumor, Internal medicine, medicine, Osteosarcoma, Methotrexate, Doxorubicin, business, Etoposide, medicine.drug

Abstract

Successful treatment for osteosarcoma (OS) requires the combination of effective systemic chemotherapy and surgical resection of all sites of clinically detectable disease. Prior to the introduction of systemic chemotherapy, patients who presented with OS of the extremity without clinically detectable metastatic disease underwent immediate surgical resection of the primary tumor. Five-year survival rates using this approach ranged from 11 to 25% (Anninga et al. 2011). In the early 1970s, trials evaluated OS response to single agents including high-dose methotrexate (HDMTX) with leucovorin rescue, cisplatin (CDDP), and doxorubicin (DOX) (Table 7.1) (Anninga et al. 2011; Pratt and Shanks 1974). Several studies reported that single agent or combination chemotherapy administered to patients with OS after primary tumor resection resulted in improved survival compared to historical controls (Anninga et al. 2011). Other reports suggested that the apparent improvement in outcome was related to improvement in diagnosis and surgery rather than a benefit from adjuvant chemotherapy (Carter 1984; Taylor et al. 1985). Two randomized prospective trials subsequently confirmed the benefit of adjuvant chemotherapy following resection of primary OS (Eilber et al. 1987; Link et al. 1986). Trials evaluating regimens including doxorubicin and high-dose methotrexate or doxorubicin and cisplatin following resection of the primary tumor reported 3- to 5-year event-free survival ranging from 50 to 60% or more in patients who presented without clinically detectable metastases (Anninga et al. 2011; Ettinger et al. 1981; Goorin et al. 1987; Pratt et al. 1990). In the 1980s, several investigations established the activity of ifosfamide or ifosfamide and etoposide in recurrent and metastatic OS (Harris et al. 1995; Miser et al. 1987).

Published

2020

35. Novel South African Rare Actinomycete Kribbella speibonae Strain SK5: A Prolific Producer of Hydroxamate Siderophores Including New Dehydroxylated Congeners

Author

Digby F. Warner, Hai Deng, Kojo Sekyi Acquah, Paul R. Meyers, Suthananda N. Sunassee, Denzil R. Beukes, Marcel Jaspars, Fleurdeliz Maglangit, and David W. Gammon

Subjects

Siderophore, siderophore, Stereochemistry, Iron, Pharmaceutical Science, Siderophores, Deferoxamine, 010402 general chemistry, Hydroxamic Acids, speibonoxamine, hydroxamate, 01 natural sciences, Article, Analytical Chemistry, lcsh:QD241-441, 03 medical and health sciences, Nocardamine, lcsh:Organic chemistry, Tandem Mass Spectrometry, RNA, Ribosomal, 16S, Drug Discovery, Actinomycetales, Physical and Theoretical Chemistry, 030304 developmental biology, mass spectrometry, 0303 health sciences, molecular networking, biology, Strain (chemistry), Chemistry, Kribbella, Organic Chemistry, biology.organism_classification, 0104 chemical sciences, Actinobacteria, Molecular network, Genus Kribbella, Chemistry (miscellaneous), Genes, Bacterial, Molecular networking, Molecular Medicine

Abstract

In this paper, we report on the chemistry of the rare South African Actinomycete Kribbella speibonae strain SK5, a prolific producer of hydroxamate siderophores and their congeners. Two new analogues, dehydroxylated desferrioxamines, speibonoxamine 1 and desoxy-desferrioxamine D1 2, have been isolated, together with four known hydroxamates, desferrioxamine D1 3, desferrioxamine B 4, desoxy-nocardamine 5 and nocardamine 6, and a diketopiperazine (DKP) 7. The structures of 1&ndash, 7 were characterized by the analysis of HRESIMS and 1D and 2D NMR data, as well as by comparison with the relevant literature. Three new dehydroxy desferrioxamine derivatives 8&ndash, 10 were tentatively identified in the molecular network of K. speibonae strain SK5 extracts, and structures were proposed based on their MS/MS fragmentation patterns. A plausible spb biosynthetic pathway was proposed. To the best of our knowledge, this is the first report of the isolation of desferrioxamines from the actinobacterial genus Kribbella.

Published

2020

36. Muramyl Tripeptide-Phosphatidyl Ethanolamine Encapsulated in Liposomes (L-MTP-PE) in the Treatment of Osteosarcoma

Author

Paul A, Meyers

Subjects

Clinical Trials as Topic, Osteosarcoma, Dogs, Phosphatidylethanolamines, Liposomes, Animals, Humans, Immunologic Factors, Bone Neoplasms, Acetylmuramyl-Alanyl-Isoglutamine

Abstract

The recruitment of autologous macrophages to attack osteosarcoma represents a novel immunotherapy approach to the treatment of osteosarcoma. Muramyl tripeptide-phosphatidyl ethanolamine encapsulated in liposomes (L-MTP-PE) was derived as a compound with the ability to stimulate macrophages to destroy autologous osteosarcoma tumor cells. Preclinical studies including studies in dogs with spontaneously arising osteosarcoma showed the ability of L-MTP-PE to control microscopic metastatic disease in osteosarcoma. A pivotal clinical trial led to the approval of L-MTP-PE for the treatment of newly diagnosed osteosarcoma in over 40 countries.

Published

2020

37. The clinical heterogeneity of round cell sarcomas with EWSR1/FUS gene fusions: Impact of gene fusion type on clinical features and outcome

Author

Paul A. Meyers, Lei Zhang, Cristina R. Antonescu, William D. Tap, John H. Healey, and Yusuke Tsuda

Subjects

Oncology, Adult, Male, Cancer Research, medicine.medical_specialty, NFATC2, Adolescent, Oncogene Proteins, Fusion, Bone Neoplasms, Sarcoma, Ewing, Biology, Article, Fusion gene, 03 medical and health sciences, 0302 clinical medicine, Ewing family of tumors, Internal medicine, Genetics, medicine, Round cell, Biomarkers, Tumor, Humans, Oncogene Fusion, Child, Gene, Cells, Cultured, Aged, ETS transcription factor family, Infant, Middle Aged, medicine.disease, Primary tumor, Survival Analysis, 030220 oncology & carcinogenesis, Child, Preschool, RNA-Binding Protein FUS, Female, Sarcoma, RNA-Binding Protein EWS

Abstract

The genetic hallmark of classic Ewing sarcoma is a recurrent fusion between EWSR1 and FUS gene with a member of the ETS transcription factor family. In contrast, tumors with non-ETS gene partners have been designated until recently "Ewing-like sarcoma," as a provisional molecular entity, as their clinical and pathologic features were still evolving. However, this group was reclassified as "round cell sarcoma with EWSR1-non-ETS fusions" in the latest 2020 WHO classification. Moreover, round cell sarcomas with either CIC or BCOR gene abnormalities, initially classified under Ewing family of tumors, are now regarded as stand-alone pathologic entities based on their distinct features. In this study we investigated the clinical characteristics of 226 confirmed Ewing sarcoma patients (EWSR1-FLI1 [n = 176], EWSR1/FUS-ERG [n = 35], EWSR1/FUS-FEV [n = 12], and EWSR1-ETV1/4 [n = 3]) and 14 round cell sarcoma patients with EWSR1-non-ETS fusion (EWSR1/FUS-NFATC2 [n = 10], EWSR1-PATZ1 [n = 3], and EWSR1-VEZF1 [n = 1]). The impact on overall survival (OS) was assessed in 90 patients with available follow-up, treated between 2011 and 2018. Patients with fusions involving FEV and NFATC2 genes showed an older median age at diagnosis, compared to those with EWSR1-FLI1 (P = .005), while extraskeletal location was more common in tumors with noncanonical EWSR1-FLI1 fusions (P = .001). Axial and pelvic primary sites were more common in patients with EWSR1-FLI1 (72%), while tumors with NFATC2 fusions were more frequent in the limb (78%, P = .006). The 3-year OS in patients with EWSR1-FLI1 was 91%, compared to only 60% in patients with alternative fusions (P = .037); the latter group showing a higher rate of metastases at presentation. However, this OS difference was not significant in patients with localized tumor (P = .585). Our study demonstrates significant correlations between fusion subtype and age at presentation, primary tumor sites, and OS, in both conventional Ewing sarcoma and round cell sarcoma with EWSR1-non ETS fusions patients. Larger studies are needed to determine survival differences in localized tumors.

Published

2020

38. Muramyl Tripeptide-Phosphatidyl Ethanolamine Encapsulated in Liposomes (L-MTP-PE) in the Treatment of Osteosarcoma

Author

Paul A. Meyers

Published

2020

39. Why defaecate on your doorstep? Investigating an unusual behaviour in Africa’s smallest falcon

Author

Claire N. Spottiswoode, Billi A Krochuk, Anthony M. Lowney, Robert L. Thomson, Diana Bolopo, Rajendra Mg Raman, and Paul R. Meyers

Subjects

0106 biological sciences, Nest, Disease exposure, Zoology, Parasite hosting, Biology, Falcon, 010603 evolutionary biology, 01 natural sciences, computer, Ecology, Evolution, Behavior and Systematics, 010605 ornithology, computer.programming_language

Abstract

Depositing faeces at the nest should be expected to carry risks such as increased parasite loads and disease exposure. This perplexing behaviour is unusual in birds but is consistently shown by a h...

Published

2018

40. Management of Patients with Acute Methotrexate Nephrotoxicity with High-Dose Leucovorin

Author

Carlos D. Flombaum, Paul A. Meyers, Ilya G. Glezerman, Sherry Mathew, Shirley Qiong Yan, Amelia Chan, Dazhi Liu, and Thangamani Muthukumar

Subjects

medicine.medical_specialty, business.industry, Glucarpidase, Acute kidney injury, Renal function, Neutropenia, medicine.disease, Gastroenterology, Article, Nephrotoxicity, 03 medical and health sciences, 0302 clinical medicine, Supportive psychotherapy, 030220 oncology & carcinogenesis, Internal medicine, medicine, Mucositis, Pharmacology (medical), Methotrexate, 030212 general & internal medicine, business, medicine.drug

Abstract

BACKGROUND: Acute kidney injury complicating high-dose methotrexate therapy increases the risk for severe mucositis, myelosuppression, and death. It is unclear whether high-dose leucovorin and supportive therapy without the use of glucarpidase can reduce toxicity from high-dose methotrexate. STUDY DESIGN: The charts of all patients at Memorial Sloan Kettering Cancer Center whose methotrexate drug levels at 48 or 72 hours after administration were ≥10 times the toxic level were reviewed between January 2000 and December 2011. RESULTS: Eighty-eight patients (median age 51 years, range 9–90 years) who received 100 courses of high-dose methotrexate were identified. Serum creatinine increased by 2-fold from baseline (median, range 1- to 10-fold), but all patients recovered kidney function. Serum levels of methotrexate were 69 μmol/L (median, range 2.2–400), 6.9 μmol/L (1.3–64), and 2.0 μmol/L (0.05–26) at 24, 48, and 72 hours, respectively, after administration. There was a statistically significant correlation between methotrexate levels at 48, 72, 96, and 120 hours after administration, but not between 24 and 72 hours or subsequent time points. High-dose leucovorin was given in 81% of courses in accordance to institutional protocols in most cases. Myelosuppression was present in 42%; Grade ≥III neutropenia in 29% and thrombocytopenia in 25%. Infectious complications, oral mucositis, and diarrhea occurred in 21%, 17%, and 6% of patients, respectively. There were 5 deaths, none directly attributed to complications from methotrexate administration. Seven additional patients received glucarpidase at the discretion of a treating physician during the study period, and results are reported separately. CONCLUSION: Patients who had 100 episodes of high-dose methotrexate-associated acute kidney injury were treated with a strategy that only included usual supportive measures and high-dose leucovorin. There were no deaths directly attributed to complications related to high-dose methotrexate therapy. Glucarpidase, an expensive drug, may not be necessary for a significant number of patients.

Published

2018

41. Streptosporangium minutum sp. nov., isolated from garden soil exposed to microwave radiation

Author

Kim Durrell, Marilize Le Roes-Hill, Alaric Prins, and Paul R. Meyers

Subjects

0301 basic medicine, Genotype, 030106 microbiology, Microbial Sensitivity Tests, medicine.disease_cause, Enterococcus faecalis, Microbiology, Soil, 03 medical and health sciences, Actinomycetales, Databases, Genetic, Drug Discovery, medicine, DNA, Fungal, Microwaves, Escherichia coli, Soil Microbiology, Mycelium, Pharmacology, biology, Antibiosis, Sequence Analysis, DNA, biology.organism_classification, 16S ribosomal RNA, Anti-Bacterial Agents, Acinetobacter baumannii, Enterobacter cloacae, Soil microbiology

Abstract

The actinobacterium, strain M26T, was isolated from garden soil that was pre-treated with microwave radiation. The soil sample was collected in Roodepoort, Gauteng Province, South Africa as part of an antibiotic-screening programme. The isolate produced branched vegetative mycelium with sporangiophores bearing small sporangia ranging from 3 to 6 μm in diameter. Rapid genus identification revealed that the isolate belongs to the genus Streptosporangium. To confirm this result, the strain was subjected to polyphasic taxonomic characterisation. Chemotaxonomic characteristics were as follows: meso-DAP in the peptidoglycan, the whole-cell hydrolysate yielded madurose, predominant menaquinones were MK9 (21%), MK9(H2) (40%), MK9(H4) (31%) and MK9(H6) (3%); the polar lipid profile included an aminolipid, phosphoglycolipids, phosphatidylethanolamine, and phosphatidylmonomethylethanolamine. In addition, the fatty acid profile showed the presence of C16:0 (12.8%), C17:1ω8c (14.2%), and 10-methyl-C17:0 (15.8%). Furthermore, 16S rRNA gene sequence phylogenetic analysis showed that the strain is closely related to members of the genus Streptosporangium, which supports its classification within the family Streptosporangiaceae. Strain M26T exhibited antibiosis against a range of pathogenic bacteria, including, but not limited to Acinetobacter baumannii ATCC 19606T, Enterobacter cloacae subsp. cloacae ATCC BAA-1143, Enterococcus faecalis ATCC 51299 (vancomycin resistant), Escherichia coli ATCC 25922, Listeria monocytogenes ATCC 19111, Mycobacterium tuberculosis H37RvT, Pseudomonas aeruginosa ATCC 27853, Salmonella enterica subsp. arizonae ATCC 13314T, and the methicillin-resistant Staphylococcus aureus subsp. aureus ATCC 33591 (MRSA). The name Streptosporangium minutum is proposed with the type strain M26T (=LMG 28850T =NRRL B-65295T).

Published

2018

42. Screening of Actinobacteria for Novel Antimalarial Compounds

Author

Daniel J Watson, Lubbe Wiesner, and Paul R Meyers

Subjects

Clinical pharmacology, biology, Traditional medicine, law, Applied Mathematics, General Mathematics, biology.organism_classification, law.invention, Actinobacteria

Published

2018

43. Unusual abdominal metastases in osteosarcoma

Author

Gerald Behr, Anita P. Price, Michael P. LaQuaglia, Paul A. Meyers, Enrico Danzer, and Simon Berhe

Subjects

musculoskeletal diseases, medicine.medical_specialty, Palliative care, lcsh:Surgery, Article, Psoas Muscles, Metastasis, 03 medical and health sciences, 0302 clinical medicine, Quality of life, Peritoneum, 0502 economics and business, medicine, Prospective cohort study, business.industry, 05 social sciences, lcsh:RJ1-570, Soft tissue, lcsh:Pediatrics, lcsh:RD1-811, medicine.disease, 3. Good health, Surgery, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Pediatrics, Perinatology and Child Health, Osteosarcoma, business, 050203 business & management

Abstract

Intraabdominal metastases in the setting of osteosarcoma are very rare. We describe a case of a 17-year-old boy with high-grade right distal femur osteosarcoma who, two years after diagnosis, developed extensive intra abdominal metastases involving the omentum, peritoneum, bowel serosa, psoas muscles and abdominal soft tissue. Awareness of and surveillance for unusual patterns of metastasis may allow for earlier detection, intervention, and palliative care decision-making, which may affect survival and quality of life. This report underlines the need for prospective studies evaluating surveillance guidelines for patients after medical and surgical management of osteosarcoma, especially in cases complicated by pulmonary metastases. Keywords: Pediatric osteosarcoma, Extrapulmonary metastases, Extrapulmonary recurrence, Surveillance imaging

Published

2018

44. DNA Methylation–Based Classifier for Accurate Molecular Diagnosis of Bone Sarcomas

Author

Twana M. Jackson, Matija Snuderl, Daniel Gorovets, Marc Ladanyi, Paul A. Meyers, Fang Bu, Christopher Bowman, J. Keith Killian, David J. Pisapia, Neerav Shukla, Shiyang Wang, Benjamin T. Cooper, Jonathan Serrano, Kristen Thomas, S. Peter Wu, Richard Gorlick, and Matthias A. Karajannis

Subjects

0301 basic medicine, Cancer Research, Pathology, medicine.medical_specialty, Methylation, Bone Sarcoma, Biology, medicine.disease, Article, Synovial sarcoma, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, CpG site, 030220 oncology & carcinogenesis, DNA methylation, Cancer research, medicine, Osteosarcoma, Sarcoma, Classifier (UML)

Abstract

Purpose Pediatric sarcomas provide a unique diagnostic challenge. There is considerable morphologic overlap between entities, increasing the importance of molecular studies in the diagnosis, treatment, and identification of therapeutic targets. We developed and validated a genome-wide DNA methylation–based classifier to differentiate between osteosarcoma, Ewing sarcoma, and synovial sarcoma. Methods DNA methylation status of 482,421 CpG sites in 10 Ewing sarcoma, 11 synovial sarcoma, and 15 osteosarcoma samples were determined using the Illumina Infinium HumanMethylation450 array. We developed a random forest classifier trained from the 400 most differentially methylated CpG sites within the training set of 36 sarcoma samples. This classifier was validated on data drawn from The Cancer Genome Atlas synovial sarcoma, TARGET-Osteosarcoma, and a recently published series of Ewing sarcoma. Results Methylation profiling revealed three distinct patterns, each enriched with a single sarcoma subtype. Within the validation cohorts, all samples from The Cancer Genome Atlas were accurately classified as synovial sarcoma (10 of 10; sensitivity and specificity, 100%), all but one sample from TARGET-Osteosarcoma were classified as osteosarcoma (85 of 86; sensitivity, 98%; specificity, 100%), and 14 of 15 Ewing sarcoma samples were classified correctly (sensitivity, 93%; specificity, 100%). The single misclassified osteosarcoma sample demonstrated high EWSR1 and ETV1 expression on RNA sequencing, although no fusion was found on manual curation of the transcript sequence. Two additional clinical samples that were difficult to classify by morphology and molecular methods were classified as osteosarcoma; one had been suspected of being a synovial sarcoma and the other of being Ewing sarcoma on initial diagnosis. Conclusion Osteosarcoma, synovial sarcoma, and Ewing sarcoma have distinct epigenetic profiles. Our validated methylation-based classifier can be used to provide diagnostic assistance when histologic and standard techniques are inconclusive.

Published

2017

45. Plasma DNA-Based Molecular Diagnosis, Prognostication, and Monitoring of Patients With EWSR1 Fusion-Positive Sarcomas

Author

Marc Ladanyi, Daoqi You, Srikanth R. Ambati, Agnes Viale, Jiabin Tang, Leonard H. Wexler, Ellinor I.B. Peerschke, Fanli Meng, Heather Magnan, Paul A. Meyers, Juber Patel, Ahmet Zehir, Alexander J. Chou, Aliaksandra Samoila, Neerav Shukla, Michael F. Berger, and Emily K. Slotkin

Subjects

0301 basic medicine, Cancer Research, Pathology, medicine.medical_specialty, Plasma dna, Breakpoint, Biology, medicine.disease, Plasma.cfDNA, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, Oncology, chemistry, 030220 oncology & carcinogenesis, Potential biomarkers, medicine, Round cell, Cancer research, Digital polymerase chain reaction, Sarcoma, DNA

Abstract

Purpose Ewing sarcoma (ES) and desmoplastic small round cell tumors (DSRCTs) are aggressive sarcomas molecularly characterized by EWSR1 gene fusions. As pathognomonic genomic events in these respective tumor types, EWSR1 fusions represent robust potential biomarkers for disease monitoring. Methods To investigate the feasibility of identifying EWSR1 fusions in plasma-derived cell-free DNA (cfDNA) from patients with ES and DSRCT, we evaluated two complementary approaches in samples from 17 patients with radiographic evidence of disease. The first approach involved identification of patient-specific genomic EWSR1 fusion breakpoints in formalin-fixed, paraffin-embedded tumor DNA using a broad, hybridization capture-based next-generation sequencing (NGS) panel, followed by design of patient-specific droplet digital polymerase chain reaction (ddPCR) assays for plasma cfDNA interrogation. The second approach used a disease-tailored targeted hybridization capture-based NGS panel applied directly to cfDNA, which included EWSR1 as well as several other genes with potential prognostic use. Results EWSR1 fusions were identified in 11 of 11 (100%) ES and five of six (83%) DSRCT cfDNA samples by ddPCR, whereas 10 of 11 (91%) and four of six (67%) were identified by NGS. The ddPCR approach had higher sensitivity, ranging between 0.009% and 0.018%. However, the hybrid capture–based NGS assay identified the precise fusion breakpoints in the majority of cfDNA samples, as well as mutations in TP53 and STAG2, two other recurrent, clinically significant alterations in ES, all without prior knowledge of the tumor genotype. Conclusion These results provide a compelling rationale for an integrated approach using both NGS and ddPCR for plasma cfDNA-based biomarker evaluations in prospective cooperative group studies.

Published

2017

46. Molecular-signature analyses support the establishment of the actinobacterial genus Sphaerimonospora (Mingma et al. 2016)

Author

Paul R. Meyers

Subjects

DNA, Bacterial, 0106 biological sciences, 0301 basic medicine, food.ingredient, Sequence analysis, 010603 evolutionary biology, 01 natural sciences, Applied Microbiology and Biotechnology, Microbiology, Actinobacteria, 03 medical and health sciences, food, Genus, Phylogenetics, RNA, Ribosomal, 16S, Amino Acid Sequence, Peptide sequence, Phylogeny, Ecology, Evolution, Behavior and Systematics, Genetics, biology, Phylogenetic tree, Fatty Acids, Sequence Analysis, DNA, biology.organism_classification, Rec A Recombinases, 030104 developmental biology, DNA Gyrase, Microbispora, Multilocus sequence typing, Multilocus Sequence Typing

Abstract

The genera Microbispora and Sphaerimonospora were examined for GyrB and RecA amino-acid signatures to determine whether molecular-signature analyses support the recent establishment of the genus Sphaerimonospora. The creation of Sphaerimonospora was based mainly upon morphological differences between Microbispora and Sphaerimonospora and the clustering of the type strains of the two genera in phylogenetic trees based on a multilocus sequence analysis. The molecular-signature analyses showed that all members of Sphaerimonospora can be distinguished from all members of Microbispora at 14 amino acid positions in the GyrB protein and at four positions in the shorter RecA protein. These amino acid differences can be used as signatures to differentiate the members of these genera from each other and thus provide support for the establishment of the genus Sphaerimonospora. This is the first demonstration of the use of molecular signatures to support the establishment of a new genus in the family Streptosporangiaceae. Following the transfer of Microbispora mesophila and Microbispora thailandensis from Microbispora to Sphaerimonospora, all species in the genus Microbispora are characterised by the insertion of a small, hydrophobic amino acid after position 208 in the GyrB protein. This insertion is absent from the GyrB protein of members of the genus Sphaerimonospora.

Published

2017

47. A 20-year retrospective analysis of CT-based pre-operative identification of pulmonary metastases in patients with osteosarcoma: A single-center review

Author

Valerie Pallos, Benjamin A. Farber, Anita P. Price, Todd E. Heaton, William J. Hammond, Michael P. LaQuaglia, Paul A. Meyers, and Alexander J. Chou

Subjects

Adult, Male, medicine.medical_specialty, Lung Neoplasms, Adolescent, medicine.medical_treatment, Bone Neoplasms, Single Center, Palpation, Article, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Pediatric surgery, medicine, Humans, Thoracotomy, Child, Lung, Retrospective Studies, Osteosarcoma, medicine.diagnostic_test, business.industry, Metastasectomy, Retrospective cohort study, General Medicine, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Pediatrics, Perinatology and Child Health, Complete Metastasectomy, Female, 030211 gastroenterology & hepatology, Surgery, Radiology, Tomography, X-Ray Computed, business

Abstract

Purpose Cooperative studies support complete metastasectomy in osteosarcoma (OS). Pre-operative CT is used to identify and quantify metastases and can facilitate minimally invasive techniques. Here we assess the accuracy of pre-operative CT compared to findings at thoracotomy and its change over time. Methods We reviewed OS thoracotomies performed at our institution from 1996 to 2015. The number of metastases identified on pre-operative chest CT was compared to the number of metastases seen on pathology (both metastases with viable cells and non-viable, osteoid-only metastases). Results Eighty-eight patients underwent 161 thoracotomies with a median of 14days (range, 1–85) between CT and surgery, a median of 2 CT-identified lesions (range, 0–15), and a median of 4 resected lesions (range, 1–25). In 56 (34.8%) cases, more metastases were found surgically than were seen on CT, and among these, 34 (21.1%) had a greater number of viable metastases. There was poor overall correlation between CT and pathology findings (Kendall Tau-b=0.506), regardless of CT slice thickness, decade of thoracotomy, or total number of CT-identified lesions. Conclusions CT accuracy in pre-operatively quantifying OS pulmonary metastases has not improved in recent decades. Consequently, we recommend an open technique with direct lung palpation for complete identification and resection of OS pulmonary metastases. Level of evidence Level IV, retrospective study with no comparison group.

Published

2017

48. Rare presentation of Ewing sarcoma metastasis to the sella and suprasellar cistern

Author

Vaios Hatzoglou, Paul A. Meyers, Michael T. Starc, and Marc K. Rosenblum

Subjects

Adult, Pathology, medicine.medical_specialty, Bone Neoplasms, Sellar mass, Sarcoma, Ewing, Article, 030218 nuclear medicine & medical imaging, Metastasis, Diagnosis, Differential, 03 medical and health sciences, 0302 clinical medicine, Pituitary adenoma, Positron Emission Tomography Computed Tomography, Sphenoid Bone, Humans, Medicine, Sella Turcica, Radiology, Nuclear Medicine and imaging, Clinical teaching, Brain Neoplasms, Cistern, business.industry, Chemoradiotherapy, medicine.disease, Magnetic Resonance Imaging, Female, Sarcoma, Presentation (obstetrics), Differential diagnosis, business, 030217 neurology & neurosurgery

Abstract

We present an exceedingly rare case of a Ewing sarcoma metastasis manifesting as a sellar mass mimicking a pituitary adenoma. The differential diagnosis of the young adult with a sellar mass is presented and correlated with a review of available literature, demonstrating this case's unique potential for clinical teaching. More specifically, this case illustrates that in a patient with a clinical history of Ewing sarcoma, a metastasis may involve the sella and suprasellar cistern without apparent osseous involvement.

Published

2017

49. DICER1-associated central nervous system sarcoma in children: comprehensive clinicopathologic and genetic analysis of a newly described rare tumor

Author

Junne, Kamihara, Vera, Paulson, Micheál A, Breen, Theodore W, Laetsch, Dinesh, Rakheja, David S, Shulman, Michelle L, Schoettler, Catherine M, Clinton, Abigail, Ward, Deirdre, Reidy, R Seth, Pinches, Daniel A, Weiser, Elizabeth A, Mullen, Jaclyn, Schienda, Paul A, Meyers, Steven G, DuBois, Jonathan A, Nowak, William D, Foulkes, Kris Ann P, Schultz, Katherine A, Janeway, Sara O, Vargas, and Alanna J, Church

Subjects

Central Nervous System Neoplasms, DEAD-box RNA Helicases, Male, Ribonuclease III, Adolescent, Child, Preschool, Mutation, Humans, Female, Sarcoma, Child

Abstract

The spectrum of neoplasms associated with DICER1 variants continues to expand, with the recent addition of primary "DICER1-associated central nervous system sarcoma" (DCS). DCS is a high-grade malignancy predominantly affecting pediatric patients. Six pediatric DCS were identified through a combination of clinical diagnostic studies, archival inquiry, and interinstitutional collaboration. Clinical, histologic, immunohistologic, and molecular features were examined. Genomic findings in the 6 DCS were compared with those in 14 additional DICER1-associated tumors sequenced with the same assay. The six patients presented at ages 3-15 years with CNS tumors located in the temporal (n = 2), parietal (n = 1), fronto-parietal (n = 1), and frontal (n = 2) lobes. All underwent surgical resection. Histologic examination demonstrated high-grade malignant spindle cell tumors with pleuropulmonary blastoma-like embryonic "organoid" features and focal rhabdomyoblastic differentiation; immature cartilage was seen in one case. Immunohistochemically, there was patchy desmin and myogenin staining, and patchy loss of H3K27me3, and within eosinophilic cytoplasmic globules, alfa-fetoprotein staining. Biallelic DICER1 variants were identified in all cases, with germline variants in two of five patients tested. DCS demonstrated genomic alterations enriched for Ras pathway activation and TP53 inactivation. Tumor mutational burden was significantly higher in the 6 DCS tumors than in 14 other DICER1-associated tumors examined (mean 12.9 vs. 6.8 mutations/Mb, p = 0.035). Postoperative care included radiation (n = 5) and chemotherapy (n = 3); at the last follow-up, three patients were alive without DCS, and three had died of disease. Our analysis expands the clinical, histologic, immunohistological, and molecular spectrum of DCS, identifying distinctive features that can aid in the diagnosis, multidisciplinary evaluation, and treatment of DCS.

Published

2019

50. Phase 1 expansion trial of the LSD1 inhibitor seclidemstat (SP-2577) with and without topotecan and cyclophosphamide (TC) in patients (pts) with relapsed or refractory Ewing sarcoma (ES) and select sarcomas

Author

David D. Stenehjem, Damon R. Reed, Nadeem Q. Mirza, Bhuvana A. Setty, Steven G. DuBois, Daniela Y. Santiesteban, Leo Mascarenhas, Sant P. Chawla, David M. Loeb, Jonathan Metts, Paul A. Meyers, Douglas J. Harrison, Brian D. Crompton, Stephen L. Lessnick, and David S. Wages

Subjects

Cancer Research, Cyclophosphamide, business.industry, Chromosomal translocation, medicine.disease, Oncology, Refractory, Cancer research, Medicine, In patient, Topotecan, Sarcoma, Cancer development, business, TAF15, medicine.drug

Abstract

TPS11577 Background: Several sarcomas possess chromosomal translocations in FET family members ( FUS, EWSR1, and TAF15) responsible for cancer development. Sarcomas caused by FET family gene rearrangements include ES, desmoplastic round cell small tumors (DSRCT), myxoid liposarcoma (ML), and several others. Lysine specific demethylase 1 (LSD1) is a critical protein for sarcoma development and progression through its colocalization and/or association with several FET family oncogenic transcription factors. This suggests that pharmacologic inhibition of LSD1 may be a therapeutic strategy. Seclidemstat (SP-2577, Salarius Pharmaceuticals) is an oral, first-in-class, small molecule with reversible, noncompetitive inhibition of LSD1 (IC50: 25–50 nM). In vitro and in vivo data demonstrate seclidemstat, or analogs, modulate EWS/ETS transcriptional activity, down-regulating oncogene expression and up-regulating tumor-suppressor gene expression, leading to significant tumor growth inhibition in ES mouse xenograft studies. Seclidemstat has shown in in vitro ES cell lines near additivity efficacy when added to TC. In in vitro studies of other FET-translocated sarcomas, including ML (FUS/DDIT3 fusion) and clear cell sarcoma (EWS/ATF1 fusion), seclidemstat showed anti-proliferative activity. In an ongoing Phase 1 trial investigating single agent seclidemstat in advanced solid tumors (NCT03895684), three pts with metastatic FET-translocated sarcomas had a median progression-free survival of 5.7 months (range: 4.3–7.2) with a best response of stable disease despite having a median of 5 (range: 1–7) prior therapies. Methods: This dose expansion Phase 1 study (NCT03600649) assesses seclidemstat at 900 mg PO BID, the recommended Phase 2 dose, in two expansion cohorts: a single agent expansion in select sarcoma pts (n = 30) and a safety lead-in dose escalation and expansion (n = 24) of seclidemstat combined with TC in pts with ES. Pts must be ≥12 years old, have ECOG performance status of 0 or 1, with a life expectancy > 4 months. In the select sarcoma cohort, pts must have ML (n = 15) or other sarcomas with FET family translocations (n = 15) including DSRCT. One to 3 prior lines of therapy are allowed. In the ES combination cohort, up to 2 lines of prior therapy are allowed. Primary objective is safety/tolerability and secondary objective is efficacy. The trial is currently recruiting across 8 locations in the United States. Clinical trial information: NCT03600649.

Published

2021