Your search keyword '"Samuel W. Brady"' showing total 113 results

1. Convergent evolution and multi-wave clonal invasion in H3 K27-altered diffuse midline gliomas treated with a PDGFR inhibitor

Author

Sasi Arunachalam, Karol Szlachta, Samuel W. Brady, Xiaotu Ma, Bensheng Ju, Bridget Shaner, Heather L. Mulder, John Easton, Benjamin J. Raphael, Matthew Myers, Christopher Tinkle, Sariah J. Allen, Brent A. Orr, Cynthia J. Wetmore, Suzanne J. Baker, and Jinghui Zhang

Subjects

Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract The majority of diffuse midline gliomas, H3 K27-altered (DMG-H3 K27-a), are infiltrating pediatric brain tumors that arise in the pons with no effective treatment. To understand how clonal evolution contributes to the tumor’s invasive spread, we performed exome sequencing and SNP array profiling on 49 multi-region autopsy samples from 11 patients with pontine DMG-H3 K27-a enrolled in a phase I clinical trial of PDGFR inhibitor crenolanib. For each patient, a phylogenetic tree was constructed by testing multiple possible clonal evolution models to select the one consistent with somatic mutations and copy number variations across all tumor regions. The tree was then used to deconvolute subclonal composition and prevalence at each tumor region to study convergent evolution and invasion patterns. Somatic variants in the PI3K pathway, a late event, are enriched in our cohort, affecting 70% of patients. Convergent evolution of PI3K at distinct phylogenetic branches was detected in 40% of the patients. 24 (~ 50%) of tumor regions were occupied by subclones of mixed lineages with varying molecular ages, indicating multiple waves of invasion across the pons and extrapontine. Subclones harboring a PDGFRA amplicon, including one that amplified a PDGRFA Y849C mutant allele, were detected in four patients; their presence in extrapontine tumor and normal brain samples imply their involvement in extrapontine invasion. Our study expands the current knowledge on tumor invasion patterns in DMG-H3 K27-a, which may inform the design of future clinical trials.

Published

2022

2. The chemotherapeutic CX-5461 primarily targets TOP2B and exhibits selective activity in high-risk neuroblastoma

Author

Min Pan, William C. Wright, Richard H. Chapple, Asif Zubair, Manbir Sandhu, Jake E. Batchelder, Brandt C. Huddle, Jonathan Low, Kaley B. Blankenship, Yingzhe Wang, Brittney Gordon, Payton Archer, Samuel W. Brady, Sivaraman Natarajan, Matthew J. Posgai, John Schuetz, Darcie Miller, Ravi Kalathur, Siquan Chen, Jon Patrick Connelly, M. Madan Babu, Michael A. Dyer, Shondra M. Pruett-Miller, Burgess B. Freeman, Taosheng Chen, Lucy A. Godley, Scott C. Blanchard, Elizabeth Stewart, John Easton, and Paul Geeleher

Subjects

Science

Abstract

CX-5461 recently progressed through phase I clinical trial as a first-inhuman inhibitor of RNA-POL I. Here, the authors demonstrate that CX-5461 synergizes with topoisomerase I inhibitors to inhibit neuroblastoma cells and that its primary target in this disease is topoisomerase II beta and not RNA-POL I.

Published

2021

3. The landscape of coding RNA editing events in pediatric cancer

Author

Ji Wen, Michael Rusch, Samuel W. Brady, Ying Shao, Michael N. Edmonson, Timothy I. Shaw, Brent B. Powers, Liqing Tian, John Easton, Charles G. Mullighan, Tanja Gruber, David Ellison, and Jinghui Zhang

Subjects

RNA editing, Pediatric cancer, Genomics, Immunotherapy, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background RNA editing leads to post-transcriptional variation in protein sequences and has important biological implications. We sought to elucidate the landscape of RNA editing events across pediatric cancers. Methods Using RNA-Seq data mapped by a pipeline designed to minimize mapping ambiguity, we investigated RNA editing in 711 pediatric cancers from the St. Jude/Washington University Pediatric Cancer Genome Project focusing on coding variants which can potentially increase protein sequence diversity. We combined de novo detection using paired tumor DNA-RNA data with analysis of known RNA editing sites. Results We identified 722 unique RNA editing sites in coding regions across pediatric cancers, 70% of which were nonsynonymous recoding variants. Nearly all editing sites represented the canonical A-to-I (n = 706) or C-to-U sites (n = 14). RNA editing was enriched in brain tumors compared to other cancers, including editing of glutamate receptors and ion channels involved in neurotransmitter signaling. RNA editing profiles of each pediatric cancer subtype resembled those of the corresponding normal tissue profiled by the Genotype-Tissue Expression (GTEx) project. Conclusions In this first comprehensive analysis of RNA editing events in pediatric cancer, we found that the RNA editing profile of each cancer subtype is similar to its normal tissue of origin. Tumor-specific RNA editing events were not identified indicating that successful immunotherapeutic targeting of RNA-edited peptides in pediatric cancer should rely on increased antigen presentation on tumor cells compared to normal but not on tumor-specific RNA editing per se.

Published

2021

4. Novel temporal and spatial patterns of metastatic colonization from breast cancer rapid-autopsy tumor biopsies

Author

Xiaomeng Huang, Yi Qiao, Samuel W. Brady, Rachel E. Factor, Erinn Downs-Kelly, Andrew Farrell, Jasmine A. McQuerry, Gajendra Shrestha, David Jenkins, W. Evan Johnson, Adam L. Cohen, Andrea H. Bild, and Gabor T. Marth

Subjects

Tumor evolution, Subclone, Metastatic breast cancer, Medicine, Genetics, QH426-470

Abstract

Abstract Background Metastatic breast cancer is a deadly disease with a low 5-year survival rate. Tracking metastatic spread in living patients is difficult and thus poorly understood. Methods Via rapid autopsy, we have collected 30 tumor samples over 3 timepoints and across 8 organs from a triple-negative metastatic breast cancer patient. The large number of sites sampled, together with deep whole-genome sequencing and advanced computational analysis, allowed us to comprehensively reconstruct the tumor’s evolution at subclonal resolution. Results The most unique, previously unreported aspect of the tumor’s evolution that we observed in this patient was the presence of “subclone incubators,” defined as metastatic sites where substantial tumor evolution occurs before colonization of additional sites and organs by subclones that initially evolved at the incubator site. Overall, we identified four discrete waves of metastatic expansions, each of which resulted in a number of new, genetically similar metastasis sites that also enriched for particular organs (e.g., abdominal vs bone and brain). The lung played a critical role in facilitating metastatic spread in this patient: the lung was the first site of metastatic escape from the primary breast lesion, subclones at this site were likely the source of all four subsequent metastatic waves, and multiple sites in the lung acted as subclone incubators. Finally, functional annotation revealed that many known drivers or metastasis-promoting tumor mutations in this patient were shared by some, but not all metastatic sites, highlighting the need for more comprehensive surveys of a patient’s metastases for effective clinical intervention. Conclusions Our analysis revealed the presence of substantial tumor evolution at metastatic incubator sites in a patient, with potentially important clinical implications. Our study demonstrated that sampling of a large number of metastatic sites affords unprecedented detail for studying metastatic evolution.

Published

2021

5. The acquisition of molecular drivers in pediatric therapy-related myeloid neoplasms

Author

Jason R. Schwartz, Jing Ma, Jennifer Kamens, Tamara Westover, Michael P. Walsh, Samuel W. Brady, J. Robert Michael, Xiaolong Chen, Lindsey Montefiori, Guangchun Song, Gang Wu, Huiyun Wu, Cristyn Branstetter, Ryan Hiltenbrand, Michael F. Walsh, Kim E. Nichols, Jamie L. Maciaszek, Yanling Liu, Priyadarshini Kumar, John Easton, Scott Newman, Jeffrey E. Rubnitz, Charles G. Mullighan, Stanley Pounds, Jinghui Zhang, Tanja Gruber, Xiaotu Ma, and Jeffery M. Klco

Subjects

Science

Abstract

Paediatric therapy-related myeloid neoplasms (tMN) have a dismal prognosis and have not been comprehensively profiled. Here the authors characterise the molecular landscape of 84 paediatric tMN patients, and find that, unlike adult tMNs, these do not emerge from pre-existing clones and that MECOM dysregulation is frequent.

Published

2021

6. Pan-neuroblastoma analysis reveals age- and signature-associated driver alterations

Author

Samuel W. Brady, Yanling Liu, Xiaotu Ma, Alexander M. Gout, Kohei Hagiwara, Xin Zhou, Jian Wang, Michael Macias, Xiaolong Chen, John Easton, Heather L. Mulder, Michael Rusch, Lu Wang, Joy Nakitandwe, Shaohua Lei, Eric M. Davis, Arlene Naranjo, Cheng Cheng, John M. Maris, James R. Downing, Nai-Kong V. Cheung, Michael D. Hogarty, Michael A. Dyer, and Jinghui Zhang

Subjects

Science

Abstract

Genomic analysis of neuroblastoma has revealed important disease etiology. In this study, the authors assembled whole genome, exome and transcriptome data from over 700 neuroblastomas and identified molecular signatures correlated with age, and rare, potentially targetable variants overlooked in smaller cohorts.

Published

2020

7. A `one-two punch' therapy strategy to target chemoresistance in estrogen receptor positive breast cancer

Author

Feng Chi, Jiayi Liu, Samuel W. Brady, Patrick A. Cosgrove, Aritro Nath, Jasmine A. McQuerry, Sumana Majumdar, Philip J. Moos, Jeffrey T. Chang, Michael Kahn, and Andrea H. Bild

Subjects

CSL, Chemotherapy, HDAC, Single-cell RNA-Seq, MYC, Chemoresistance, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Cancer cell phenotypes evolve during a tumor's treatment. In some cases, tumor cells acquire cancer stem cell-like (CSL) traits such as resistance to chemotherapy and diminished differentiation; therefore, targeting these cells may be therapeutically beneficial. In this study we show that in progressive estrogen receptor positive (ER+) metastatic breast cancer tumors, resistant subclones that emerge following chemotherapy have increased CSL abundance. Further, in vitro organoid growth of ER+ patient cancer cells also shows that chemotherapy treatment leads to increased abundance of ALDH+/CD44+ CSL cells. Chemotherapy induced CSL abundance is blocked by treatment with a pan-HDAC inhibitor, belinostat. Belinostat treatment diminished both mammosphere formation and size following chemotherapy, indicating a decrease in progenitor CSL traits. HDAC inhibitors specific to class IIa (HDAC4, HDAC5) and IIb (HDAC6) were shown to primarily reverse the chemo-resistant CSL state. Single-cell RNA sequencing analysis with patient samples showed that HDAC targets and MYC signaling were promoted by chemotherapy and inhibited upon HDAC inhibitor treatment. In summary, HDAC inhibition can block chemotherapy-induced drug resistant phenotypes with ‘one-two punch’ strategy in refractory breast cancer cells.

Published

2021

8. Combating subclonal evolution of resistant cancer phenotypes

Author

Samuel W. Brady, Jasmine A. McQuerry, Yi Qiao, Stephen R. Piccolo, Gajendra Shrestha, David F. Jenkins, Ryan M. Layer, Brent S. Pedersen, Ryan H. Miller, Amanda Esch, Sara R. Selitsky, Joel S. Parker, Layla A. Anderson, Brian K. Dalley, Rachel E. Factor, Chakravarthy B. Reddy, Jonathan P. Boltax, Dean Y. Li, Philip J. Moos, Joe W. Gray, Laura M. Heiser, Saundra S. Buys, Adam L. Cohen, W. Evan Johnson, Aaron R. Quinlan, Gabor Marth, Theresa L. Werner, and Andrea H. Bild

Subjects

Science

Abstract

In metastatic breast cancer, subclonal evolution can drive drug resistance. Here, the authors genetically and transcriptionally follow the evolution of four breast cancers over time and treatment, and suggest a phenotype-targeted treatment strategy to adapt to cancer as it evolves.

Published

2017

9. Publisher Correction: Combating subclonal evolution of resistant cancer phenotypes

Author

Samuel W. Brady, Jasmine A. McQuerry, Yi Qiao, Stephen R. Piccolo, Gajendra Shrestha, David F. Jenkins, Ryan M. Layer, Brent S. Pedersen, Ryan H. Miller, Amanda Esch, Sara R. Selitsky, Joel S. Parker, Layla A. Anderson, Brian K. Dalley, Rachel E. Factor, Chakravarthy B. Reddy, Jonathan P. Boltax, Dean Y. Li, Philip J. Moos, Joe W. Gray, Laura M. Heiser, Saundra S. Buys, Adam L. Cohen, W. Evan Johnson, Aaron R. Quinlan, Gabor Marth, Theresa L. Werner, and Andrea H. Bild

Subjects

Science

Abstract

The originally published version of this Article contained an error in Figure 4. In panel a, grey boxes surrounding the subclones associated with patients #2 and #4 obscured adjacent portions of the heatmap. This error has now been corrected in both the PDF and HTML versions of the Article.

Published

2018

10. Supplementary Data-1 from Clinical Significance of Novel Subtypes of Acute Lymphoblastic Leukemia in the Context of Minimal Residual Disease–Directed Therapy

Author

Ching-Hon Pui, Charles G. Mullighan, Dario Campana, Mary V. Relling, Williams E. Evans, James R. Downing, Cheng Cheng, Jun J. Yang, Zhaohui Gu, Samuel W. Brady, Chunxu Qu, Seth E. Karol, Susana C. Raimondi, Tanja A. Gruber, Raul C. Ribeiro, Jeffrey E. Rubnitz, Hiroto Inaba, Elaine Coustan-Smith, Deqing Pei, Kathryn G. Roberts, John Choi, and Sima Jeha

Abstract

Supplementary Data Legend, Supplementary Table (S7) and Supplementary Figures (S1-S6)

Published

2023

11. Data from Clinical Significance of Novel Subtypes of Acute Lymphoblastic Leukemia in the Context of Minimal Residual Disease–Directed Therapy

Author

Ching-Hon Pui, Charles G. Mullighan, Dario Campana, Mary V. Relling, Williams E. Evans, James R. Downing, Cheng Cheng, Jun J. Yang, Zhaohui Gu, Samuel W. Brady, Chunxu Qu, Seth E. Karol, Susana C. Raimondi, Tanja A. Gruber, Raul C. Ribeiro, Jeffrey E. Rubnitz, Hiroto Inaba, Elaine Coustan-Smith, Deqing Pei, Kathryn G. Roberts, John Choi, and Sima Jeha

Abstract

We evaluated clinical significance of recently identified subtypes of acute lymphoblastic leukemia (ALL) in 598 children treated with minimal residual disease (MRD)–directed therapy. Among the 16 B-cell ALL (B-ALL) and 8 T-cell ALL subtypes identified by next-generation sequencing, ETV6–RUNX1, high-hyperdiploid, and DUX4-rearranged B-ALL had the best 5-year event-free survival rates (95.0%–98.4%); TCF3–PBX1, PAX5-altered (PAX5alt), T-cell, early T-cell precursor (ETP), intrachromosomal amplification of chromosome 21 (iAMP21), and hypodiploid ALL intermediate rates (80.0%–88.2%); and BCR–ABL1, BCR–ABL1-like, ETV6–RUNX1-like, and KMT2A-rearranged ALL the worst rates (64.1%–76.2%). All but 3 of the 142 patients with day 8 blood MRD DUX4-rearranged, BCR–ABL1-like, and ZNF384-rearranged ALL, and achievement of day 42 MRD MEF2D-rearranged, and ETV6–RUNX1-like ALL. Thus, new subtypes including DUX4-rearranged, PAX5alt, BCR–ABL1-like, ETV6–RUNX1-like, MEF2D-rearranged, and ZNF384-rearranged ALL have important prognostic and therapeutic implications.Significance:Genomic analyses and MRD should be used together for risk-directed treatment of childhood ALL. Six recently described subtypes—DUX4-rearranged, PAX5alt, BCR–ABL1-like, ETV6–RUNX1-like, MEF2D-rearranged, and ZNF384-rearranged ALL—had prognostic and therapeutic significance with contemporary risk-directed treatment.See related commentary by Segers and Cools, p. 294.See related video from the AACR Annual Meeting 2021: https://vimeo.com/558556916

Published

2023

12. Tables S1-S5 from Clinical Significance of Novel Subtypes of Acute Lymphoblastic Leukemia in the Context of Minimal Residual Disease–Directed Therapy

Author

Ching-Hon Pui, Charles G. Mullighan, Dario Campana, Mary V. Relling, Williams E. Evans, James R. Downing, Cheng Cheng, Jun J. Yang, Zhaohui Gu, Samuel W. Brady, Chunxu Qu, Seth E. Karol, Susana C. Raimondi, Tanja A. Gruber, Raul C. Ribeiro, Jeffrey E. Rubnitz, Hiroto Inaba, Elaine Coustan-Smith, Deqing Pei, Kathryn G. Roberts, John Choi, and Sima Jeha

Abstract

Supplementary Table S1-S5

Published

2023

13. Table S6 from Clinical Significance of Novel Subtypes of Acute Lymphoblastic Leukemia in the Context of Minimal Residual Disease–Directed Therapy

Author

Ching-Hon Pui, Charles G. Mullighan, Dario Campana, Mary V. Relling, Williams E. Evans, James R. Downing, Cheng Cheng, Jun J. Yang, Zhaohui Gu, Samuel W. Brady, Chunxu Qu, Seth E. Karol, Susana C. Raimondi, Tanja A. Gruber, Raul C. Ribeiro, Jeffrey E. Rubnitz, Hiroto Inaba, Elaine Coustan-Smith, Deqing Pei, Kathryn G. Roberts, John Choi, and Sima Jeha

Abstract

Supplementary Table S6

Published

2023

14. Supplementary Figure S4 from Genomes for Kids: The Scope of Pathogenic Mutations in Pediatric Cancer Revealed by Comprehensive DNA and RNA Sequencing

Author

Kim E. Nichols, Jinghui Zhang, James R. Downing, David W. Ellison, Ching-Hon Pui, Liza-Marie Johnson, Giles Robinson, Alberto S. Pappo, Stacy J. Hines-Dowell, Jessica M. Valdez, Leslie M. Taylor, Elsie L. Gerhardt, Roya Mostafavi, Regina Nuccio, Emily A. Quinn, Rose B. McGee, Charles G. Mullighan, Zhaohui Gu, Jian Wang, Alexander M. Gout, Jay Knight, Victor Pastor, Jamie L. Maciaszek, Manish Kubal, Delaram Rahbarinia, Mark R. Wilkinson, Aman Patel, Jared Becksfort, Eric Davis, Manjusha Pande, Ti-Cheng Chang, Xin Zhou, Samuel W. Brady, Yu Liu, Zhaojie Zhang, Yanling Liu, Antonina Silkov, Annastasia Ouma, Michael R. Clay, Lu Wang, Lynn W. Harrison, Jiali Gu, Jeffery M. Klco, Brent A. Orr, Armita Bahrami, Andrew Thrasher, Michael N. Edmonson, Scott G. Foy, Kayla V. Hamilton, Dale J. Hedges, Sheila Shurtleff, Michael Rusch, David A. Wheeler, Elizabeth M. Azzato, Chimene A. Kesserwan, Joy Nakitandwe, and Scott Newman

Abstract

Supplementary Figure S4

Published

2023

15. Data from Genomes for Kids: The Scope of Pathogenic Mutations in Pediatric Cancer Revealed by Comprehensive DNA and RNA Sequencing

Author

Kim E. Nichols, Jinghui Zhang, James R. Downing, David W. Ellison, Ching-Hon Pui, Liza-Marie Johnson, Giles Robinson, Alberto S. Pappo, Stacy J. Hines-Dowell, Jessica M. Valdez, Leslie M. Taylor, Elsie L. Gerhardt, Roya Mostafavi, Regina Nuccio, Emily A. Quinn, Rose B. McGee, Charles G. Mullighan, Zhaohui Gu, Jian Wang, Alexander M. Gout, Jay Knight, Victor Pastor, Jamie L. Maciaszek, Manish Kubal, Delaram Rahbarinia, Mark R. Wilkinson, Aman Patel, Jared Becksfort, Eric Davis, Manjusha Pande, Ti-Cheng Chang, Xin Zhou, Samuel W. Brady, Yu Liu, Zhaojie Zhang, Yanling Liu, Antonina Silkov, Annastasia Ouma, Michael R. Clay, Lu Wang, Lynn W. Harrison, Jiali Gu, Jeffery M. Klco, Brent A. Orr, Armita Bahrami, Andrew Thrasher, Michael N. Edmonson, Scott G. Foy, Kayla V. Hamilton, Dale J. Hedges, Sheila Shurtleff, Michael Rusch, David A. Wheeler, Elizabeth M. Azzato, Chimene A. Kesserwan, Joy Nakitandwe, and Scott Newman

Abstract

Genomic studies of pediatric cancer have primarily focused on specific tumor types or high-risk disease. Here, we used a three-platform sequencing approach, including whole-genome sequencing (WGS), whole-exome sequencing (WES), and RNA sequencing (RNA-seq), to examine tumor and germline genomes from 309 prospectively identified children with newly diagnosed (85%) or relapsed/refractory (15%) cancers, unselected for tumor type. Eighty-six percent of patients harbored diagnostic (53%), prognostic (57%), therapeutically relevant (25%), and/or cancer-predisposing (18%) variants. Inclusion of WGS enabled detection of activating gene fusions and enhancer hijacks (36% and 8% of tumors, respectively), small intragenic deletions (15% of tumors), and mutational signatures revealing of pathogenic variant effects. Evaluation of paired tumor–normal data revealed relevance to tumor development for 55% of pathogenic germline variants. This study demonstrates the power of a three-platform approach that incorporates WGS to interrogate and interpret the full range of genomic variants across newly diagnosed as well as relapsed/refractory pediatric cancers.Significance:Pediatric cancers are driven by diverse genomic lesions, and sequencing has proven useful in evaluating high-risk and relapsed/refractory cases. We show that combined WGS, WES, and RNA-seq of tumor and paired normal tissues enables identification and characterization of genetic drivers across the full spectrum of pediatric cancers.This article is highlighted in the In This Issue feature, p. 2945

Published

2023

16. Supplementary Figure Legend from Enhanced PI3K p110α Signaling Confers Acquired Lapatinib Resistance That Can Be Effectively Reversed by a p110α-Selective PI3K Inhibitor

Author

Dihua Yu, Hai Wang, Daniel Seok, Jian Zhang, and Samuel W. Brady

Abstract

PDF - 76K, Legends for Supplementary Figures 1-9.

Published

2023

17. Supplementary Data from St. Jude Cloud: A Pediatric Cancer Genomic Data-Sharing Ecosystem

Author

Jinghui Zhang, James R. Downing, Keith Perry, Richard Daly, Michael Rusch, Scott Newman, Geralyn Miller, Michael A. Dyer, Suzanne J. Baker, Charles G. Mullighan, Chaitanya Bangur, David W. Ellison, Kim E. Nichols, Yutaka Yasui, Leslie L. Robison, Gregory T. Armstrong, Mitchell J. Weiss, Ludmil B. Alexandrov, Soheil Meshinchi, Yong Cheng, Carmen L. Wilson, Zhaoming Wang, Alberto S. Pappo, Matthew Lear, James McMurry, Leigh Tanner, Ed Suh, Gang Wu, Lance E. Palmer, Xing Tang, Darrell Gentry, Nedra Robison, Irina McGuire, Omar Serang, Tuan Nguyen, Singer Ma, Vijay Kandali, Pamella Tater, Naina Thangaraj, Christopher Meyer, S.M. Ashiqul Islam, Shaohua Lei, Liqing Tian, Ti-Cheng Chang, Andrew M. Frantz, Mark R. Wilkinson, Michael N. Edmonson, Aman Patel, Xiaotu Ma, Yu Liu, J. Robert Michael, Shuoguo Wang, Edgar Sioson, Jian Wang, Scott Foy, Stephanie Wiggins, Andrew Swistak, Arthur Chiao, Tracy K. Ard, Bob Davidson, Madison Treadway, Brent A. Orr, Rahul Mudunuri, Jobin Sunny, David Finkelstein, Kirby Birch, Michael Macias, Samuel W. Brady, Delaram Rahbarinia, Andrew Thrasher, Xin Zhou, Alexander M. Gout, and Clay McLeod

Abstract

Involves Supplementary Table Legends and Supplementary Figures and associated legends

Published

2023

18. Data from St. Jude Cloud: A Pediatric Cancer Genomic Data-Sharing Ecosystem

Author

Jinghui Zhang, James R. Downing, Keith Perry, Richard Daly, Michael Rusch, Scott Newman, Geralyn Miller, Michael A. Dyer, Suzanne J. Baker, Charles G. Mullighan, Chaitanya Bangur, David W. Ellison, Kim E. Nichols, Yutaka Yasui, Leslie L. Robison, Gregory T. Armstrong, Mitchell J. Weiss, Ludmil B. Alexandrov, Soheil Meshinchi, Yong Cheng, Carmen L. Wilson, Zhaoming Wang, Alberto S. Pappo, Matthew Lear, James McMurry, Leigh Tanner, Ed Suh, Gang Wu, Lance E. Palmer, Xing Tang, Darrell Gentry, Nedra Robison, Irina McGuire, Omar Serang, Tuan Nguyen, Singer Ma, Vijay Kandali, Pamella Tater, Naina Thangaraj, Christopher Meyer, S.M. Ashiqul Islam, Shaohua Lei, Liqing Tian, Ti-Cheng Chang, Andrew M. Frantz, Mark R. Wilkinson, Michael N. Edmonson, Aman Patel, Xiaotu Ma, Yu Liu, J. Robert Michael, Shuoguo Wang, Edgar Sioson, Jian Wang, Scott Foy, Stephanie Wiggins, Andrew Swistak, Arthur Chiao, Tracy K. Ard, Bob Davidson, Madison Treadway, Brent A. Orr, Rahul Mudunuri, Jobin Sunny, David Finkelstein, Kirby Birch, Michael Macias, Samuel W. Brady, Delaram Rahbarinia, Andrew Thrasher, Xin Zhou, Alexander M. Gout, and Clay McLeod

Abstract

Effective data sharing is key to accelerating research to improve diagnostic precision, treatment efficacy, and long-term survival in pediatric cancer and other childhood catastrophic diseases. We present St. Jude Cloud (https://www.stjude.cloud), a cloud-based data-sharing ecosystem for accessing, analyzing, and visualizing genomic data from >10,000 pediatric patients with cancer and long-term survivors, and >800 pediatric sickle cell patients. Harmonized genomic data totaling 1.25 petabytes are freely available, including 12,104 whole genomes, 7,697 whole exomes, and 2,202 transcriptomes. The resource is expanding rapidly, with regular data uploads from St. Jude's prospective clinical genomics programs. Three interconnected apps within the ecosystem—Genomics Platform, Pediatric Cancer Knowledgebase, and Visualization Community—enable simultaneously performing advanced data analysis in the cloud and enhancing the Pediatric Cancer knowledgebase. We demonstrate the value of the ecosystem through use cases that classify 135 pediatric cancer subtypes by gene expression profiling and map mutational signatures across 35 pediatric cancer subtypes.Significance:To advance research and treatment of pediatric cancer, we developed St. Jude Cloud, a data-sharing ecosystem for accessing >1.2 petabytes of raw genomic data from >10,000 pediatric patients and survivors, innovative analysis workflows, integrative multiomics visualizations, and a knowledgebase of published data contributed by the global pediatric cancer community.This article is highlighted in the In This Issue feature, p. 995

Published

2023

19. Supplementary Figure 9 from Enhanced PI3K p110α Signaling Confers Acquired Lapatinib Resistance That Can Be Effectively Reversed by a p110α-Selective PI3K Inhibitor

Author

Dihua Yu, Hai Wang, Daniel Seok, Jian Zhang, and Samuel W. Brady

Abstract

PDF - 308K, Supplementary Figure 9. Inhibition of Akt and Erk phosphorylation in vivo by combination treatment.

Published

2023

20. Supplementary Figures 1 through 8 from Enhanced PI3K p110α Signaling Confers Acquired Lapatinib Resistance That Can Be Effectively Reversed by a p110α-Selective PI3K Inhibitor

Author

Dihua Yu, Hai Wang, Daniel Seok, Jian Zhang, and Samuel W. Brady

Abstract

PDF - 299K, Supplementary Figure 1. HER3 activation is not increased in LapR cells. Supplementary Figure 2. Time-independent maintenance of phospho-Akt during lapatinib treatment in BT474 LapR cells. Supplementary Figure 3. p110α knockdown sensitizes lapatinib-resistant cells to lapatinib. Supplementary Figure 4. p110α knockdown is more effective in BT474 LapR cells than UACC893 LapR cells. Supplementary Figure 5. Wild-type and mutant p110α promote basal proliferation. BT474 cells stably infected with indicated p110α constructs were grown for 4 days. Supplementary Figure 6. Analysis of combination treatment synergy. Supplementary Figure 7. Lapatinib plus BYL719 inhibits HER3. Supplementary Figure 8. Lapatinib plus BYL719 does not induce weight loss.

Published

2023

21. Data from The Clonal Evolution of Metastatic Osteosarcoma as Shaped by Cisplatin Treatment

Author

Jinghui Zhang, Michael A. Dyer, Benjamin J. Raphael, Alberto S. Pappo, James R. Downing, Richard K. Wilson, Elaine R. Mardis, Xiang Chen, Ludmil B. Alexandrov, John Easton, Michael N. Edmonson, Donald A. Yergeau, Heather L. Mulder, Daniel K. Putnam, Michael Rusch, Scott Newman, Gang Wu, Gryte Satas, Armita Bahrami, Xiaotu Ma, and Samuel W. Brady

Abstract

To investigate the genomic evolution of metastatic pediatric osteosarcoma, we performed whole-genome and targeted deep sequencing on 14 osteosarcoma metastases and two primary tumors from four patients (two to eight samples per patient). All four patients harbored ancestral (truncal) somatic variants resulting in TP53 inactivation and cell-cycle aberrations, followed by divergence into relapse-specific lineages exhibiting a cisplatin-induced mutation signature. In three of the four patients, the cisplatin signature accounted for >40% of mutations detected in the metastatic samples. Mutations potentially acquired during cisplatin treatment included NF1 missense mutations of uncertain significance in two patients and a KIT G565R activating mutation in one patient. Three of four patients demonstrated widespread ploidy differences between samples from the sample patient. Single-cell seeding of metastasis was detected in most metastatic samples. Cross-seeding between metastatic sites was observed in one patient, whereas in another patient a minor clone from the primary tumor seeded both metastases analyzed. These results reveal extensive clonal heterogeneity in metastatic osteosarcoma, much of which is likely cisplatin-induced.Implications:The extent and consequences of chemotherapy-induced damage in pediatric cancers is unknown. We found that cisplatin treatment can potentially double the mutational burden in osteosarcoma, which has implications for optimizing therapy for recurrent, chemotherapy-resistant disease.

Published

2023

22. Supplementary Tables S1-S5 from The Clonal Evolution of Metastatic Osteosarcoma as Shaped by Cisplatin Treatment

Author

Jinghui Zhang, Michael A. Dyer, Benjamin J. Raphael, Alberto S. Pappo, James R. Downing, Richard K. Wilson, Elaine R. Mardis, Xiang Chen, Ludmil B. Alexandrov, John Easton, Michael N. Edmonson, Donald A. Yergeau, Heather L. Mulder, Daniel K. Putnam, Michael Rusch, Scott Newman, Gang Wu, Gryte Satas, Armita Bahrami, Xiaotu Ma, and Samuel W. Brady

Abstract

Osteosarcoma clinical history and capture validation sequencing data. Supplementary Table S1. Sample and treatment information for relapsed osteosarcoma patients. Supplementary Table S2. SJOS0011101 SNVs detected by capture validation and tumor purity. Supplementary Table S3. SJOS0011105 SNVs detected by capture validation and tumor purity. Supplementary Table S4. SJOS0011107 SNVs detected by capture validation and tumor purity. Supplementary Table S5. SJOS010 SNVs detected by capture validation and tumor purity.

Published

2023

23. Supplementary Figure S5 from Src Inhibition Blocks c-Myc Translation and Glucose Metabolism to Prevent the Development of Breast Cancer

Author

Dihua Yu, Victoria L. Seewaldt, Wei Jia, Rebecca Richards-Kortum, Banu K. Arun, Christopher Sistrunk, Adrian Ambrose, Tomasz S. Tkaczyk, Matt Kyrish, Jessica Dobbs, Hong Zhao, Ping Li, Samuel W. Brady, Qingling Zhang, Hai Wang, Catherine Ibarra-Drendall, Chia-Chi Chang, Xiao Wang, and Shalini Jain

Abstract

Saracatinib inhibits proliferation and c-Myc, and GLUT1 in MFPs of ER- MMTV-neu* mouse model.

Published

2023

24. Data from Src Inhibition Blocks c-Myc Translation and Glucose Metabolism to Prevent the Development of Breast Cancer

Author

Dihua Yu, Victoria L. Seewaldt, Wei Jia, Rebecca Richards-Kortum, Banu K. Arun, Christopher Sistrunk, Adrian Ambrose, Tomasz S. Tkaczyk, Matt Kyrish, Jessica Dobbs, Hong Zhao, Ping Li, Samuel W. Brady, Qingling Zhang, Hai Wang, Catherine Ibarra-Drendall, Chia-Chi Chang, Xiao Wang, and Shalini Jain

Abstract

Preventing breast cancer will require the development of targeted strategies that can effectively block disease progression. Tamoxifen and aromatase inhibitors are effective in addressing estrogen receptor–positive (ER+) breast cancer development, but estrogen receptor–negative (ER−) breast cancer remains an unmet challenge due to gaps in pathobiologic understanding. In this study, we used reverse-phase protein array to identify activation of Src kinase as an early signaling alteration in premalignant breast lesions of women who did not respond to tamoxifen, a widely used ER antagonist for hormonal therapy of breast cancer. Src kinase blockade with the small-molecule inhibitor saracatinib prevented the disorganized three-dimensional growth of ER− mammary epithelial cells in vitro and delayed the development of premalignant lesions and tumors in vivo in mouse models developing HER2+ and ER− mammary tumors, extending tumor-free and overall survival. Mechanistic investigations revealed that Src blockade reduced glucose metabolism as a result of an inhibition in ERK1/2–MNK1–eIF4E–mediated cap-dependent translation of c-Myc and transcription of the glucose transporter GLUT1, thereby limiting energy available for cell growth. Taken together, our results provide a sound rationale to target Src pathways in premalignant breast lesions to limit the development of breast cancers. Cancer Res; 75(22); 4863–75. ©2015 AACR.

Published

2023

25. Supplementary Table S1 from Src Inhibition Blocks c-Myc Translation and Glucose Metabolism to Prevent the Development of Breast Cancer

Author

Dihua Yu, Victoria L. Seewaldt, Wei Jia, Rebecca Richards-Kortum, Banu K. Arun, Christopher Sistrunk, Adrian Ambrose, Tomasz S. Tkaczyk, Matt Kyrish, Jessica Dobbs, Hong Zhao, Ping Li, Samuel W. Brady, Qingling Zhang, Hai Wang, Catherine Ibarra-Drendall, Chia-Chi Chang, Xiao Wang, and Shalini Jain

Abstract

RPPA data showing fold changes in transcriptional regulator expressions in saracatinib treated 10A.B2 cells over vehicle control.

Published

2023

26. Supplementary Methods and References from Src Inhibition Blocks c-Myc Translation and Glucose Metabolism to Prevent the Development of Breast Cancer

Author

Dihua Yu, Victoria L. Seewaldt, Wei Jia, Rebecca Richards-Kortum, Banu K. Arun, Christopher Sistrunk, Adrian Ambrose, Tomasz S. Tkaczyk, Matt Kyrish, Jessica Dobbs, Hong Zhao, Ping Li, Samuel W. Brady, Qingling Zhang, Hai Wang, Catherine Ibarra-Drendall, Chia-Chi Chang, Xiao Wang, and Shalini Jain

Abstract

Description of additional methods and procedures used in the study. Also includes Supplementary References.

Published

2023

27. Figure S4 from The Small GTPase ARF6 Activates PI3K in Melanoma to Induce a Prometastatic State

Author

Allie H. Grossmann, Sheri L. Holmen, Dean Y. Li, Shannon J. Odelberg, Andrea Bild, David A. Kircher, Coulson P. Rich, Donghan Shin, Tara Mleynek, Roger K. Wolff, Lise K. Sorensen, Jingfu Peng, Aaron Rogers, Lehi Acosta-Alvarez, Samuel W. Brady, and Jae Hyuk Yoo

Abstract

Figure S4. Primary tumor incidence, growth, survival and metastasis in Ptenf/f vs. Arf6Q67L mice. (a) Increased tumor incidence (% = # of mice that developed a tumor / # TVA positive, injected mice) in Ptenf/f vs. Arf6Q67L cohorts. Fisher's exact test, two-tailed, α

Published

2023

28. Data from The Small GTPase ARF6 Activates PI3K in Melanoma to Induce a Prometastatic State

Author

Allie H. Grossmann, Sheri L. Holmen, Dean Y. Li, Shannon J. Odelberg, Andrea Bild, David A. Kircher, Coulson P. Rich, Donghan Shin, Tara Mleynek, Roger K. Wolff, Lise K. Sorensen, Jingfu Peng, Aaron Rogers, Lehi Acosta-Alvarez, Samuel W. Brady, and Jae Hyuk Yoo

Abstract

Melanoma has an unusual capacity to spread in early-stage disease, prompting aggressive clinical intervention in very thin primary tumors. Despite these proactive efforts, patients with low-risk, low-stage disease can still develop metastasis, indicating the presence of permissive cues for distant spread. Here, we show that constitutive activation of the small GTPase ARF6 (ARF6Q67L) is sufficient to accelerate metastasis in mice with BRAFV600E/Cdkn2aNULL melanoma at a similar incidence and severity to Pten loss, a major driver of PI3K activation and melanoma metastasis. ARF6Q67L promoted spontaneous metastasis from significantly smaller primary tumors than PTENNULL, implying an enhanced ability of ARF6-GTP to drive distant spread. ARF6 activation increased lung colonization from circulating melanoma cells, suggesting that the prometastatic function of ARF6 extends to late steps in metastasis. Unexpectedly, ARF6Q67L tumors showed upregulation of Pik3r1 expression, which encodes the p85 regulatory subunit of PI3K. Tumor cells expressing ARF6Q67L displayed increased PI3K protein levels and activity, enhanced PI3K distribution to cellular protrusions, and increased AKT activation in invadopodia. ARF6 is necessary and sufficient for activation of both PI3K and AKT, and PI3K and AKT are necessary for ARF6-mediated invasion. We provide evidence for aberrant ARF6 activation in human melanoma samples, which is associated with reduced survival. Our work reveals a previously unknown ARF6-PI3K-AKT proinvasive pathway, it demonstrates a critical role for ARF6 in multiple steps of the metastatic cascade, and it illuminates how melanoma cells can acquire an early metastatic phenotype in patients.Significance:These findings reveal a prometastatic role for ARF6 independent of tumor growth, which may help explain how melanoma spreads distantly from thin, early-stage primary tumors.

Published

2023

29. Table S1 from The Small GTPase ARF6 Activates PI3K in Melanoma to Induce a Prometastatic State

Author

Allie H. Grossmann, Sheri L. Holmen, Dean Y. Li, Shannon J. Odelberg, Andrea Bild, David A. Kircher, Coulson P. Rich, Donghan Shin, Tara Mleynek, Roger K. Wolff, Lise K. Sorensen, Jingfu Peng, Aaron Rogers, Lehi Acosta-Alvarez, Samuel W. Brady, and Jae Hyuk Yoo

Abstract

Table S1: ARF6 pathways and related genes.

Published

2023

30. Supplementary Table and Figure Legends from Src Inhibition Blocks c-Myc Translation and Glucose Metabolism to Prevent the Development of Breast Cancer

Author

Dihua Yu, Victoria L. Seewaldt, Wei Jia, Rebecca Richards-Kortum, Banu K. Arun, Christopher Sistrunk, Adrian Ambrose, Tomasz S. Tkaczyk, Matt Kyrish, Jessica Dobbs, Hong Zhao, Ping Li, Samuel W. Brady, Qingling Zhang, Hai Wang, Catherine Ibarra-Drendall, Chia-Chi Chang, Xiao Wang, and Shalini Jain

Abstract

Legend for Supplementary Table S1 and Supplementary Figures S1-S5.

Published

2023

31. Supplementary Figure 4 from Concomitant Targeting of Tumor Cells and Induction of T-cell Response Synergizes to Effectively Inhibit Trastuzumab-Resistant Breast Cancer

Author

Dihua Yu, Gabriel N. Hortobagyi, William J. Muller, Elizabeth M. Jaffee, Hailiang Ge, Ping Li, Samuel W. Brady, Ozgur Sahin, Yi Xiao, Hai Wang, Shau-Hsuan Li, and Qingfei Wang

Abstract

PDF file - 255K, The observation of more lymphocytes/leukocytes infiltration after HER2/Neu antibody and Akt inhibitor TCN combination treatment

Published

2023

32. Supplementary Figure 8 from Concomitant Targeting of Tumor Cells and Induction of T-cell Response Synergizes to Effectively Inhibit Trastuzumab-Resistant Breast Cancer

Author

Dihua Yu, Gabriel N. Hortobagyi, William J. Muller, Elizabeth M. Jaffee, Hailiang Ge, Ping Li, Samuel W. Brady, Ozgur Sahin, Yi Xiao, Hai Wang, Shau-Hsuan Li, and Qingfei Wang

Abstract

PDF file - 206K, No significant changes in the number of tumor infiltrating T cells (including CD8+ and CD4+ ) upon the addition of anti-CTLA-4 mAb to HER2/Neu antibody and triciribine combination treatment

Published

2023

33. Supplementary Figure 2 from Concomitant Targeting of Tumor Cells and Induction of T-cell Response Synergizes to Effectively Inhibit Trastuzumab-Resistant Breast Cancer

Author

Dihua Yu, Gabriel N. Hortobagyi, William J. Muller, Elizabeth M. Jaffee, Hailiang Ge, Ping Li, Samuel W. Brady, Ozgur Sahin, Yi Xiao, Hai Wang, Shau-Hsuan Li, and Qingfei Wang

Abstract

PDF file - 25K, HER2/Neu antibody 7.16.4 and Akt inhibitor TCN combination treatment reduced tumor multiplicity and lung metastasis in PTEN-/-/NIC mice

Published

2023

34. Supplementary Figure 3 from Concomitant Targeting of Tumor Cells and Induction of T-cell Response Synergizes to Effectively Inhibit Trastuzumab-Resistant Breast Cancer

Author

Dihua Yu, Gabriel N. Hortobagyi, William J. Muller, Elizabeth M. Jaffee, Hailiang Ge, Ping Li, Samuel W. Brady, Ozgur Sahin, Yi Xiao, Hai Wang, Shau-Hsuan Li, and Qingfei Wang

Abstract

PDF file - 410K, Histological and immunohistochemical analysis of tumors derived from PTEN-/-/ErbB2KI mice receiving single or combination treatment

Published

2023

35. Supplementary Figure 6 from Concomitant Targeting of Tumor Cells and Induction of T-cell Response Synergizes to Effectively Inhibit Trastuzumab-Resistant Breast Cancer

Author

Dihua Yu, Gabriel N. Hortobagyi, William J. Muller, Elizabeth M. Jaffee, Hailiang Ge, Ping Li, Samuel W. Brady, Ozgur Sahin, Yi Xiao, Hai Wang, Shau-Hsuan Li, and Qingfei Wang

Abstract

PDF file - 137K, Depletion of CD8+ cells, CD4+ cells or both during HER2/Neu antibody and triciribine combination treatment

Published

2023

36. Data from Concomitant Targeting of Tumor Cells and Induction of T-cell Response Synergizes to Effectively Inhibit Trastuzumab-Resistant Breast Cancer

Author

Dihua Yu, Gabriel N. Hortobagyi, William J. Muller, Elizabeth M. Jaffee, Hailiang Ge, Ping Li, Samuel W. Brady, Ozgur Sahin, Yi Xiao, Hai Wang, Shau-Hsuan Li, and Qingfei Wang

Abstract

Trastuzumab is an iconic rationally designed targeted therapy for HER2-positive breast cancers. However, the low response rate and development of resistance call for novel approaches for the treatment of patients. Here, we report that concurrent targeting of tumor cells and activation of T cells in the tumor microenvironment results in a synergistic inhibitory effect on tumor growth and overcomes resistance in two distinct PTEN loss–mediated trastuzumab-resistant mammary tumor mouse models. In vivo combination treatment with HER2/Neu antibody and Akt inhibitor triciribine effectively inhibited tumor growth in both models via inhibiting PI3K/AKT and mitogen-activated protein kinase signaling accompanied by increased T-cell infiltration in the tumor microenvironment. We showed that both CD8+ and CD4+ T cells were essential to the optimal antitumor effect of this combination treatment in an IFN-γ–dependent manner. Importantly, the antitumor activities of HER2/Neu antibody and triciribine combination treatment were further improved when coinhibitory receptor cytotoxic T-lymphocyte–associated antigen 4 was blocked to enhance the T-cell response. Our data indicate that multitargeted combinatorial therapies targeting tumor cells and concomitantly enhancing T-cell response in the tumor microenvironment could cooperate to exert maximal therapeutic activity, suggesting a promising clinical strategy for treating trastuzumab-resistant breast cancers and other advanced malignancies. Cancer Res; 72(17); 4417–28. ©2012 AACR.

Published

2023

37. Supplementary Figure 9 from Concomitant Targeting of Tumor Cells and Induction of T-cell Response Synergizes to Effectively Inhibit Trastuzumab-Resistant Breast Cancer

Author

Dihua Yu, Gabriel N. Hortobagyi, William J. Muller, Elizabeth M. Jaffee, Hailiang Ge, Ping Li, Samuel W. Brady, Ozgur Sahin, Yi Xiao, Hai Wang, Shau-Hsuan Li, and Qingfei Wang

Abstract

PDF file - 24K, HER2/Neu antibody and TCN plus anti-CTLA-4 mAb triple combination treatment increased serum IFN-gamma level

Published

2023

38. Supplementary Figure 7 from Concomitant Targeting of Tumor Cells and Induction of T-cell Response Synergizes to Effectively Inhibit Trastuzumab-Resistant Breast Cancer

Author

Dihua Yu, Gabriel N. Hortobagyi, William J. Muller, Elizabeth M. Jaffee, Hailiang Ge, Ping Li, Samuel W. Brady, Ozgur Sahin, Yi Xiao, Hai Wang, Shau-Hsuan Li, and Qingfei Wang

Abstract

PDF file - 37K, Anti-CTLA-4 mAb alone, anti-CTLA-4 mAb combined with HER2/Neu antibody only, or with TCN only showed no significant enhancement of antitumor effect

Published

2023

39. Supplementary Table 1 from Concomitant Targeting of Tumor Cells and Induction of T-cell Response Synergizes to Effectively Inhibit Trastuzumab-Resistant Breast Cancer

Author

Dihua Yu, Gabriel N. Hortobagyi, William J. Muller, Elizabeth M. Jaffee, Hailiang Ge, Ping Li, Samuel W. Brady, Ozgur Sahin, Yi Xiao, Hai Wang, Shau-Hsuan Li, and Qingfei Wang

Abstract

PDF file - 82K, Primer sequences for quantitative real-time reverse transcription-PCR

Published

2023

40. Supplementary Figure 1 from Concomitant Targeting of Tumor Cells and Induction of T-cell Response Synergizes to Effectively Inhibit Trastuzumab-Resistant Breast Cancer

Author

Dihua Yu, Gabriel N. Hortobagyi, William J. Muller, Elizabeth M. Jaffee, Hailiang Ge, Ping Li, Samuel W. Brady, Ozgur Sahin, Yi Xiao, Hai Wang, Shau-Hsuan Li, and Qingfei Wang

Abstract

PDF file - 85K, Characterization of PTEN-/-/NIC mouse model

Published

2023

41. Supplementary Figure Legends 1-9 from Concomitant Targeting of Tumor Cells and Induction of T-cell Response Synergizes to Effectively Inhibit Trastuzumab-Resistant Breast Cancer

Author

Dihua Yu, Gabriel N. Hortobagyi, William J. Muller, Elizabeth M. Jaffee, Hailiang Ge, Ping Li, Samuel W. Brady, Ozgur Sahin, Yi Xiao, Hai Wang, Shau-Hsuan Li, and Qingfei Wang

Abstract

PDF file - 126K

Published

2023

42. Supplementary Figure 5 from Concomitant Targeting of Tumor Cells and Induction of T-cell Response Synergizes to Effectively Inhibit Trastuzumab-Resistant Breast Cancer

Author

Dihua Yu, Gabriel N. Hortobagyi, William J. Muller, Elizabeth M. Jaffee, Hailiang Ge, Ping Li, Samuel W. Brady, Ozgur Sahin, Yi Xiao, Hai Wang, Shau-Hsuan Li, and Qingfei Wang

Abstract

PDF file - 36K, Evaluation of markers of other tumor-infiltrating immune cells

Published

2023

43. Opposing Effects of KDM6A and JDP2 on Glucocorticoid Sensitivity in T-ALL

Author

Anya Levinson, Karensa Tjoa, Benjamin J. Huang, Lauren K. Meyer, Mi-Ok Kim, Samuel W Brady, Jinghui Zhang, Kevin M Shannon, and Anica Wandler

Subjects

Hematology

Abstract

Glucocorticoids (GCs) are a cornerstone of acute lymphoblastic leukemia (ALL) therapy. While mutations in NR3C1, which encodes the GC receptor (GR), and other genes involved in GC signaling occur at relapse, additional mechanisms of adaptive GC resistance are uncertain. We transplanted and treated ten primary mouse T-lineage acute lymphoblastic leukemias (T-ALLs) initiated by retroviral insertional mutagenesis with the GC dexamethasone (DEX). Multiple, distinct relapsed clones from one such leukemia (T-ALL 8633) exhibited discrete retroviral integrations that up-regulated Jdp2 expression. This leukemia harbored a Kdm6a mutation. In the human T-ALL cell line CCRF-CEM, enforced JDP2 over-expression conferred GC resistance, while KDM6A inactivation unexpectedly enhanced GC sensitivity. In the context of KDM6A knock-out, JDP2 over-expression induced profound GC resistance, counteracting the sensitization conferred by KDM6A loss. These resistant "double mutant" cells with combined KDM6A loss and JDP2 over-expression exhibited decreased NR3C1 mRNA and GR protein up-regulation upon DEX exposure. Analysis of paired samples from two KDM6A-mutant T-ALL patients in a relapsed pediatric ALL cohort revealed a somatic NR3C1 mutation at relapse in one and markedly elevated JDP2 expression in another. Together, these data implicate JDP2 over-expression as a mechanism of adaptive GC resistance in T-ALL that functionally interacts with KDM6A inactivation.

Published

2023

44. Uncovering novel mutational signatures by de novo extraction with SigProfilerExtractor

Author

S.M. Ashiqul Islam, Marcos Díaz-Gay, Yang Wu, Mark Barnes, Raviteja Vangara, Erik N. Bergstrom, Yudou He, Mike Vella, Jingwei Wang, Jon W. Teague, Peter Clapham, Sarah Moody, Sergey Senkin, Yun Rose Li, Laura Riva, Tongwu Zhang, Andreas J. Gruber, Christopher D. Steele, Burçak Otlu, Azhar Khandekar, Ammal Abbasi, Laura Humphreys, Natalia Syulyukina, Samuel W. Brady, Boian S. Alexandrov, Nischalan Pillay, Jinghui Zhang, David J. Adams, Iñigo Martincorena, David C. Wedge, Maria Teresa Landi, Paul Brennan, Michael R. Stratton, Steven G. Rozen, and Ludmil B. Alexandrov

Subjects

cancer genomics, Tobacco Smoke and Health, Prevention, Human Genome, mutational signatures, Biochemistry, Genetics and Molecular Biology (miscellaneous), Good Health and Well Being, ddc:570, Tobacco, genomics, Genetics, mutagenesis, Cancer, Biotechnology

Abstract

Mutational signature analysis is commonly performed in cancer genomic studies. Here, we present SigProfilerExtractor, an automated tool for de novo extraction of mutational signatures, and benchmark it against another 13 bioinformatics tools by using 34 scenarios encompassing 2,500 simulated signatures found in 60,000 synthetic genomes and 20,000 synthetic exomes. For simulations with 5% noise, reflecting high-quality datasets, SigProfilerExtractor outperforms other approaches by elucidating between 20% and 50% more true-positive signatures while yielding 5-fold less false-positive signatures. Applying SigProfilerExtractor to 4,643 whole-genome- and 19,184 whole-exome-sequenced cancers reveals four novel signatures. Two of the signatures are confirmed in independent cohorts, and one of these signatures is associated with tobacco smoking. In summary, this report provides a reference tool for analysis of mutational signatures, a comprehensive benchmarking of bioinformatics tools for extracting signatures, and several novel mutational signatures, including one putatively attributed to direct tobacco smoking mutagenesis in bladder tissues. published

Published

2022

45. Chemotherapy and mismatch repair deficiency cooperate to fuel TP53 mutagenesis and ALL relapse

Author

Lijuan Du, Pandurang Kolekar, Jiaoyang Cai, Jeffery M. Klco, Houshun Fang, Xiaotu Ma, Bin-Bing S. Zhou, Omkar Pathak, Huiying Sun, Samuel W. Brady, Hong-Zhuan Chen, Yu Liu, Benshang Li, Hui Li, Xiaomeng Li, Lixia Ding, Cornelia Eckert, Renate Kirschner-Schwabe, Malwine J. Barz, Shuhong Shen, Jinghui Zhang, Cai-Wen Duan, Fan Yang, Chao Tang, Arend von Stackelberg, Yao Chen, and Tianyi Wang

Subjects

Cancer Research, Chemotherapy, Thiopurine methyltransferase, biology, Mechanism (biology), business.industry, medicine.medical_treatment, Standard treatment, Mutagenesis (molecular biology technique), Somatic evolution in cancer, Oncology, medicine, biology.protein, Cancer research, MISMATCH REPAIR DEFICIENCY, DNA mismatch repair, business

Abstract

Chemotherapy is a standard treatment for pediatric acute lymphoblastic leukemia (ALL), which sometimes relapses with chemoresistant features. However, whether acquired drug-resistance mutations in relapsed ALL pre-exist or are induced by treatment remains unknown. Here we provide direct evidence of a specific mechanism by which chemotherapy induces drug-resistance-associated mutations leading to relapse. Using genomic and functional analysis of relapsed ALL we show that thiopurine treatment in mismatch repair (MMR)-deficient leukemias induces hotspot TP53 R248Q mutations through a specific mutational signature (thio-dMMR). Clonal evolution analysis reveals sequential MMR inactivation followed by TP53 mutation in some patients with ALL. Acquired TP53 R248Q mutations are associated with on-treatment relapse, poor treatment response and resistance to multiple chemotherapeutic agents, which could be reversed by pharmacological p53 reactivation. Our findings indicate that TP53 R248Q in relapsed ALL originates through synergistic mutagenesis from thiopurine treatment and MMR deficiency and suggest strategies to prevent or treat TP53-mutant relapse. Zhou and colleagues demonstrate that thiopurine chemotherapy in mismatch repair-deficient ALL cells leads to R248Q TP53 mutations and clonal selection that favors on-treatment ALL relapse and chemoresistance.

Published

2021

46. The acquisition of molecular drivers in pediatric therapy-related myeloid neoplasms

Author

Stanley Pounds, Lindsey E. Montefiori, Charles G. Mullighan, Jamie L. Maciaszek, Yanling Liu, Jing Ma, Jennifer Kamens, Tanja A. Gruber, Michael P. Walsh, Samuel W. Brady, Kim E. Nichols, Jinghui Zhang, Ryan Hiltenbrand, Jeffrey E. Rubnitz, Xiao-Long Chen, Scott Newman, Priyadarshini Kumar, J. Robert Michael, Huiyun Wu, John Easton, Cristyn Branstetter, Michael Walsh, Jeffery M. Klco, Xiaotu Ma, Jason R. Schwartz, Gang Wu, Tamara Westover, and Guangchun Song

Subjects

0301 basic medicine, Lineage (genetic), Myeloid, MECOM, Science, General Physics and Astronomy, Bioinformatics, Article, Acute myeloid leukaemia, General Biochemistry, Genetics and Molecular Biology, Germline, 03 medical and health sciences, 0302 clinical medicine, Exome Sequencing, Cancer genomics, medicine, Humans, Child, Exome, Exome sequencing, Multidisciplinary, biology, business.industry, Neoplasms, Second Primary, Genomics, Histone-Lysine N-Methyltransferase, General Chemistry, Prognosis, medicine.disease, Gene Expression Regulation, Neoplastic, Leukemia, Myeloid, Acute, Leukemia, 030104 developmental biology, medicine.anatomical_structure, KMT2A, Myelodysplastic Syndromes, 030220 oncology & carcinogenesis, Mutation, biology.protein, Gene expression, business, Myelodysplastic syndrome, Myeloid-Lymphoid Leukemia Protein

Abstract

Pediatric therapy-related myeloid neoplasms (tMN) occur in children after exposure to cytotoxic therapy and have a dismal prognosis. The somatic and germline genomic alterations that drive these myeloid neoplasms in children and how they arise have yet to be comprehensively described. We use whole exome, whole genome, and/or RNA sequencing to characterize the genomic profile of 84 pediatric tMN cases (tMDS: n = 28, tAML: n = 56). Our data show that Ras/MAPK pathway mutations, alterations in RUNX1 or TP53, and KMT2A rearrangements are frequent somatic drivers, and we identify cases with aberrant MECOM expression secondary to enhancer hijacking. Unlike adults with tMN, we find no evidence of pre-existing minor tMN clones (including those with TP53 mutations), but rather the majority of cases are unrelated clones arising as a consequence of cytotoxic therapy. These studies also uncover rare cases of lineage switch disease rather than true secondary neoplasms., Paediatric therapy-related myeloid neoplasms (tMN) have a dismal prognosis and have not been comprehensively profiled. Here the authors characterise the molecular landscape of 84 paediatric tMN patients, and find that, unlike adult tMNs, these do not emerge from pre-existing clones and that MECOM dysregulation is frequent.

Published

2021

47. St. Jude Cloud: A Pediatric Cancer Genomic Data-Sharing Ecosystem

Author

Zhaoming Wang, J. Robert Michael, Darrell Gentry, Suzanne J. Baker, Jobin Sunny, S M Ashiqul Islam, Clay McLeod, David W. Ellison, Michael A. Dyer, Mark R. Wilkinson, Jinghui Zhang, Ludmil B. Alexandrov, Chaitanya Bangur, Bob Davidson, Singer Ma, Geralyn Miller, Pamella Tater, Yong Cheng, Arthur Chiao, Alexander M. Gout, Tuan Nguyen, James R. Downing, Edgar Sioson, Gang Wu, Delaram Rahbarinia, Ed Suh, Xiaotu Ma, Shaohua Lei, Yutaka Yasui, Andrew Frantz, Kirby Birch, Scott G. Foy, Nedra Robison, Kim E. Nichols, Aman Patel, Richard Daly, Alberto S. Pappo, Naina Thangaraj, Xin Zhou, Leslie L. Robison, Matthew Lear, Vijay Kandali, Christopher P. Meyer, David Finkelstein, Stephanie Wiggins, Tracy Ard, Irina McGuire, Yu Liu, Samuel W. Brady, Gregory T. Armstrong, Liqing Tian, Charles G. Mullighan, Brent A. Orr, Ti-Cheng Chang, Keith Perry, Michael Macias, Shuoguo Wang, Lance E. Palmer, Soheil Meshinchi, Carmen L. Wilson, James McMurry, Andrew Swistak, Michael Rusch, Scott Newman, Leigh Tanner, Madison Treadway, Xing Tang, Omar Serang, Jian Wang, Andrew Thrasher, Rahul Mudunuri, Mitchell J. Weiss, and Michael N. Edmonson

Subjects

0301 basic medicine, Genomic data, MEDLINE, Cloud computing, Anemia, Sickle Cell, Article, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, Humans, Medicine, Child, Ecosystem, Information Dissemination, business.industry, Cancer, Genomics, Cloud Computing, Hospitals, Pediatric, medicine.disease, Pediatric cancer, Data science, Treatment efficacy, Data sharing, 030104 developmental biology, Workflow, Oncology, 030220 oncology & carcinogenesis, business

Abstract

Effective data sharing is key to accelerating research to improve diagnostic precision, treatment efficacy, and long-term survival in pediatric cancer and other childhood catastrophic diseases. We present St. Jude Cloud (https://www.stjude.cloud), a cloud-based data-sharing ecosystem for accessing, analyzing, and visualizing genomic data from >10,000 pediatric patients with cancer and long-term survivors, and >800 pediatric sickle cell patients. Harmonized genomic data totaling 1.25 petabytes are freely available, including 12,104 whole genomes, 7,697 whole exomes, and 2,202 transcriptomes. The resource is expanding rapidly, with regular data uploads from St. Jude's prospective clinical genomics programs. Three interconnected apps within the ecosystem—Genomics Platform, Pediatric Cancer Knowledgebase, and Visualization Community—enable simultaneously performing advanced data analysis in the cloud and enhancing the Pediatric Cancer knowledgebase. We demonstrate the value of the ecosystem through use cases that classify 135 pediatric cancer subtypes by gene expression profiling and map mutational signatures across 35 pediatric cancer subtypes. Significance: To advance research and treatment of pediatric cancer, we developed St. Jude Cloud, a data-sharing ecosystem for accessing >1.2 petabytes of raw genomic data from >10,000 pediatric patients and survivors, innovative analysis workflows, integrative multiomics visualizations, and a knowledgebase of published data contributed by the global pediatric cancer community. This article is highlighted in the In This Issue feature, p. 995

Published

2021

48. Opposing Effects of KDM6A and JDP2 on Glucocorticoid Sensitivity in T-ALL

Author

Anya Levinson, Karensa Tjoa, Benjamin J. Huang, Lauren K. Meyer, Samuel W Brady, Jinghui Zhang, Kevin M. Shannon, and Anica Wandler

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Published

2022

49. Therapy-induced mutations drive the genomic landscape of relapsed acute lymphoblastic leukemia

Author

Jie Zhao, Ke Xu, Fan Yang, Ludmil B. Alexandrov, Edgar Sioson, Cheng Cheng, Samuel W. Brady, Shuhong Shen, Lele Sun, Liqing Tian, Benshang Li, Heather L. Mulder, Tianyi Wang, Yu Liu, Diane Flasch, James R. Downing, Ting Nien Lin, Xiaofan Zhu, Hui Zhang, Lijuan Du, Ching-Hon Pui, Matthew A. Myers, Yongjin Li, Ningling Wang, Michael Rusch, Karol Szlachta, Xiaotu Ma, Liu Yang, Jingyan Tang, Bin-Bing S. Zhou, Xin Zhou, Benjamin J. Raphael, Jinghui Zhang, Hui Li, Hui Ying Sun, Lixia Ding, Li Dong, Ying Shao, Jiaoyang Cai, Jingliao Zhang, Yingchi Zhang, Hongye Sun, Michael N. Edmonson, Kohei Hagiwara, John Easton, Yanling Liu, and Jun J. Yang

Subjects

0301 basic medicine, Immunology, Clone (cell biology), Drug resistance, medicine.disease_cause, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Recurrence, Acute lymphocytic leukemia, DNA Mutational Analysis, medicine, Humans, Mutation, Lymphoid Neoplasia, Thiopurine methyltransferase, biology, business.industry, Cancer, Genomics, Cell Biology, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, 030104 developmental biology, MSH2, 030220 oncology & carcinogenesis, biology.protein, Cancer research, business

Abstract

To study the mechanisms of relapse in acute lymphoblastic leukemia (ALL), we performed whole-genome sequencing of 103 diagnosis-relapse-germline trios and ultra-deep sequencing of 208 serial samples in 16 patients. Relapse-specific somatic alterations were enriched in 12 genes (NR3C1, NR3C2, TP53, NT5C2, FPGS, CREBBP, MSH2, MSH6, PMS2, WHSC1, PRPS1, and PRPS2) involved in drug response. Their prevalence was 17% in very early relapse (36 months) groups. Convergent evolution, in which multiple subclones harbor mutations in the same drug resistance gene, was observed in 6 relapses and confirmed by single-cell sequencing in 1 case. Mathematical modeling and mutational signature analysis indicated that early relapse resistance acquisition was frequently a 2-step process in which a persistent clone survived initial therapy and later acquired bona fide resistance mutations during therapy. In contrast, very early relapses arose from preexisting resistant clone(s). Two novel relapse-specific mutational signatures, one of which was caused by thiopurine treatment based on in vitro drug exposure experiments, were identified in early and late relapses but were absent from 2540 pan-cancer diagnosis samples and 129 non-ALL relapses. The novel signatures were detected in 27% of relapsed ALLs and were responsible for 46% of acquired resistance mutations in NT5C2, PRPS1, NR3C1, and TP53. These results suggest that chemotherapy-induced drug resistance mutations facilitate a subset of pediatric ALL relapses.

Published

2020

50. The landscape of coding RNA editing events in pediatric cancer

Author

Samuel W. Brady, David W. Ellison, Ji Wen, Charles G. Mullighan, Tanja A. Gruber, John Easton, Timothy I. Shaw, Brent B Powers, Michael Rusch, Michael N. Edmonson, Liqing Tian, Jinghui Zhang, and Ying Shao

Subjects

Nonsynonymous substitution, RNA editing, Cancer Research, Pediatric cancer, Genomics, Computational biology, Biology, Open Reading Frames, Protein sequencing, Neoplasms, Genetics, medicine, Humans, Coding region, RNA, Neoplasm, Child, RC254-282, Whole Genome Sequencing, Brain Neoplasms, Sequence Analysis, RNA, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Cancer, DNA, Neoplasm, Genome project, medicine.disease, Oncology, Organ Specificity, Immunotherapy, Research Article

Abstract

Background RNA editing leads to post-transcriptional variation in protein sequences and has important biological implications. We sought to elucidate the landscape of RNA editing events across pediatric cancers. Methods Using RNA-Seq data mapped by a pipeline designed to minimize mapping ambiguity, we investigated RNA editing in 711 pediatric cancers from the St. Jude/Washington University Pediatric Cancer Genome Project focusing on coding variants which can potentially increase protein sequence diversity. We combined de novo detection using paired tumor DNA-RNA data with analysis of known RNA editing sites. Results We identified 722 unique RNA editing sites in coding regions across pediatric cancers, 70% of which were nonsynonymous recoding variants. Nearly all editing sites represented the canonical A-to-I (n = 706) or C-to-U sites (n = 14). RNA editing was enriched in brain tumors compared to other cancers, including editing of glutamate receptors and ion channels involved in neurotransmitter signaling. RNA editing profiles of each pediatric cancer subtype resembled those of the corresponding normal tissue profiled by the Genotype-Tissue Expression (GTEx) project. Conclusions In this first comprehensive analysis of RNA editing events in pediatric cancer, we found that the RNA editing profile of each cancer subtype is similar to its normal tissue of origin. Tumor-specific RNA editing events were not identified indicating that successful immunotherapeutic targeting of RNA-edited peptides in pediatric cancer should rely on increased antigen presentation on tumor cells compared to normal but not on tumor-specific RNA editing per se.

Published

2021