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3. Predictors of success in establishing orthotopic patient-derived xenograft models of triple negative breast cancer

Author

Echeverria, Gloria V., Cai, Shirong, Tu, Yizheng, Shao, Jiansu, Powell, Emily, Redwood, Abena B., Jiang, Yan, McCoy, Aaron, Rinkenbaugh, Amanda L., Lau, Rosanna, Trevarton, Alexander J., Fu, Chunxiao, Gould, Rebekah, Ravenberg, Elizabeth E., Huo, Lei, Candelaria, Rosalind, Santiago, Lumarie, Adrada, Beatriz E., Lane, Deanna L., Rauch, Gaiane M., Yang, Wei T., White, Jason B., Chang, Jeffrey T., Moulder, Stacy L., Symmans, W. Fraser, Hilsenbeck, Susan G., and Piwnica-Worms, Helen

Published
2023
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4. Activation of the IFN Signaling Pathway is Associated with Resistance to CDK4/6 Inhibitors and Immune Checkpoint Activation in ER-Positive Breast Cancer

Author

De Angelis, Carmine, Fu, Xiaoyong, Cataldo, Maria Letizia, Nardone, Agostina, Pereira, Resel, Veeraraghavan, Jamunarani, Nanda, Sarmistha, Qin, Lanfang, Sethunath, Vidyalakshmi, Wang, Tao, Hilsenbeck, Susan G, Benelli, Matteo, Migliaccio, Ilenia, Guarducci, Cristina, Malorni, Luca, Litchfield, Lacey M, Liu, Jiangang, Donaldson, Joshua, Selenica, Pier, Brown, David N, Weigelt, Britta, Reis-Filho, Jorge S, Park, Ben H, Hurvitz, Sara A, Slamon, Dennis J, Rimawi, Mothaffar F, Jansen, Valerie M, Jeselsohn, Rinath, Osborne, C Kent, and Schiff, Rachel

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Genetics, Breast Cancer, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Good Health and Well Being, Antineoplastic Agents, Breast Neoplasms, Cyclin-Dependent Kinase 4, Cyclin-Dependent Kinase 6, Female, Humans, Piperazines, Pyridines, Receptors, Estrogen, Signal Transduction, Tumor Cells, Cultured, Oncology & Carcinogenesis, Clinical sciences, Oncology and carcinogenesis
Abstract

PurposeCyclin-dependent kinase 4 (CDK4) and CDK6 inhibitors (CDK4/6i) are highly effective against estrogen receptor-positive (ER+)/HER2- breast cancer; however, intrinsic and acquired resistance is common. Elucidating the molecular features of sensitivity and resistance to CDK4/6i may lead to identification of predictive biomarkers and novel therapeutic targets, paving the way toward improving patient outcomes.Experimental designParental breast cancer cells and their endocrine-resistant derivatives (EndoR) were used. Derivatives with acquired resistance to palbociclib (PalboR) were generated from parental and estrogen deprivation-resistant MCF7 and T47D cells. Transcriptomic and proteomic analyses were performed in palbociclib-sensitive and PalboR lines. Gene expression data from CDK4/6i neoadjuvant trials and publicly available datasets were interrogated for correlations of gene signatures and patient outcomes.ResultsParental and EndoR breast cancer lines showed varying degrees of sensitivity to palbociclib. Transcriptomic analysis of these cell lines identified an association between high IFN signaling and reduced CDK4/6i sensitivity; thus an "IFN-related palbociclib-resistance Signature" (IRPS) was derived. In two neoadjuvant trials of CDK4/6i plus endocrine therapy, IRPS and other IFN-related signatures were highly enriched in patients with tumors exhibiting intrinsic resistance to CDK4/6i. PalboR derivatives displayed dramatic activation of IFN/STAT1 signaling compared with their short-term treated or untreated counterparts. In primary ER+/HER2- tumors, the IRPS score was significantly higher in lumB than lumA subtype and correlated with increased gene expression of immune checkpoints, endocrine resistance, and poor prognosis.ConclusionsAberrant IFN signaling is associated with intrinsic resistance to CDK4/6i. Experimentally, acquired resistance to palbociclib is associated with activation of the IFN pathway, warranting additional studies to clarify its involvement in resistance to CDK4/6i.

Published
2021

5. Identifying biomarkers of differential chemotherapy response in TNBC patient-derived xenografts with a CTD/WGCNA approach

Author

Petrosyan, Varduhi, Dobrolecki, Lacey E., Thistlethwaite, Lillian, Lewis, Alaina N., Sallas, Christina, Srinivasan, Ramakrishnan R., Lei, Jonathan T., Kovacevic, Vladimir, Obradovic, Predrag, Ellis, Matthew J., Osborne, C. Kent, Rimawi, Mothaffar F., Pavlick, Anne, Shafaee, Maryam Nemati, Dowst, Heidi, Jain, Antrix, Saltzman, Alexander B., Malovannaya, Anna, Marangoni, Elisabetta, Welm, Alana L., Welm, Bryan E., Li, Shunqiang, Wulf, Gerburg M., Sonzogni, Olmo, Huang, Chen, Vasaikar, Suhas, Hilsenbeck, Susan G., Zhang, Bing, Milosavljevic, Aleksandar, and Lewis, Michael T.

Published
2023
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6. Targeting eIF4A triggers an interferon response to synergize with chemotherapy and suppress triple-negative breast cancer

Author

Zhao, Na, Kabotyanski, Elena B., Saltzman, Alexander B., Malovannaya, Anna, Yuan, Xueying, Reineke, Lucas C., Lieu, Nadia, Gao, Yang, Pedroza, Diego A., Calderon, Sebastian J., Smith, Alex J., Hamor, Clark, Safari, Kazem, Savage, Sara, Zhang, Bing, Zhou, Jianling, Solis, Luisa M., Hilsenbeck, Susan G., Fan, Cheng, Perou, Charles M., and Rosen, Jeffrey M.

Subjects
Interferon -- Analysis, Immunotherapy -- Patient outcomes, Protein biosynthesis -- Analysis, Chemotherapy -- Patient outcomes, Cancer -- Chemotherapy, Health care industry
Abstract

Protein synthesis is frequently dysregulated in cancer and selective inhibition of mRNA translation represents an attractive cancer therapy. Here, we show that therapeutically targeting the RNA helicase eIF4A with zotatifin, the first-in-class eIF4A inhibitor, exerts pleiotropic effects on both tumor cells and the tumor immune microenvironment in a diverse cohort of syngeneic triple-negative breast cancer (TNBC) mouse models. Zotatifin not only suppresses tumor cell proliferation but also directly repolarizes macrophages toward an M1-like phenotype and inhibits neutrophil infiltration, which sensitizes tumors to immune checkpoint blockade. Mechanistic studies revealed that zotatifin reprograms the tumor translational landscape, inhibits the translation of Sox4 and Fgfr1, and induces an interferon (IFN) response uniformly across models. The induction of an IFN response is partially due to the inhibition of Sox4 translation by zotatifin. A similar induction of IFN-stimulated genes was observed in breast cancer patient biopsies following zotatifin treatment. Surprisingly, zotatifin significantly synergizes with carboplatin to trigger DNA damage and an even heightened IFN response, resulting in T cell-dependent tumor suppression. These studies identified a vulnerability of eIF4A in TNBC, potential pharmacodynamic biomarkers for zotatifin, and provide a rationale for new combination regimens consisting of zotatifin and chemotherapy or immunotherapy as treatments for TNBC., Introduction Triple-negative breast cancer (TNBC) is a heterogeneous group of breast cancers defined by the absence of estrogen receptor (ER), progesterone receptor (PR), or human epidermal growth factor receptor 2 [...]

Published
2023
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7. LOAd703, an oncolytic virus-based immunostimulatory gene therapy, combined with chemotherapy for unresectable or metastatic pancreatic cancer (LOKON001) results from arm 1 of a non-randomised, single-centre, phase 1/2 study

Author

Musher, Benjamin L., Rowinsky, Eric K., Smaglo, Brandon G., Abidi, Wasif, Othman, Mohamed, Patel, Kalpesh, Jawaid, Salmaan, Jing, James, Brisco, Amanda, Leen, Ann M., Wu, Mengfen, Sandin, Linda C., Wenthe, Jessica, Eriksson, Emma, Ullenhag, Gustav J., Grilley, Bambi, Leja-Jarblad, Justyna, Hilsenbeck, Susan G., Brenner, Malcolm K., Loskog, Angelica, Musher, Benjamin L., Rowinsky, Eric K., Smaglo, Brandon G., Abidi, Wasif, Othman, Mohamed, Patel, Kalpesh, Jawaid, Salmaan, Jing, James, Brisco, Amanda, Leen, Ann M., Wu, Mengfen, Sandin, Linda C., Wenthe, Jessica, Eriksson, Emma, Ullenhag, Gustav J., Grilley, Bambi, Leja-Jarblad, Justyna, Hilsenbeck, Susan G., Brenner, Malcolm K., and Loskog, Angelica

Abstract

Background Pancreatic ductal adenocarcinoma is characterised by low immunogenicity and an immunosuppressive tumour microenvironment. LOAd703, an oncolytic adenovirus with transgenes encoding TMZ-CD40L and 4-1BBL, lyses cancer cells selectively, activates cytotoxic T cells, and induces tumour regression in preclinical models. The aim of this study was to evaluate the safety and feasibility of combining LOAd703 with chemotherapy for advanced pancreatic ductal adenocarcinoma. Methods LOKON001 was a non-randomised, phase 1/2 study conducted at the Dan L Duncan Comprehensive Cancer Center, Baylor College of Medicine, Houston, TX, USA, and consisted of two arms conducted sequentially; the results of arm 1 are presented here. In arm 1, patients 18 years or older with previously treated or treatment-naive unresectable or metastatic pancreatic ductal adenocarcinoma were treated with standard 28-day cycles of intravenous nab-paclitaxel 125 mg/m 2 plus gemcitabine 1000 mg/m 2 (up to 12 cycles) and intratumoural injections of LOAd703 every 2 weeks. Patients were assigned using Bayesian optimal interval design to receive 500 mu L of LOAd703 at 5 x 10 10 (dose 1), 1 x 10 11 (dose 2), or 5 x 10 11 (dose 3) viral particles per injection, injected endoscopically or percutaneously into the pancreatic tumour or a metastasis for six injections. The primary endpoints were safety and treatment-emergent immune response in patients who received at least one dose of LOAd703, and antitumour activity was a secondary endpoint. This study was registered with ClinicalTrials.gov, NCT02705196, arm 2 is ongoing and open to new participants. Findings Between Dec 2, 2016, and Oct 17, 2019, 23 patients were assessed for eligibility, leading to 22 patients being enrolled. One patient withdrew consent, resulting in 21 patients (13 [62%] men and eight [38%] women) assigned to a dose group (three to dose 1, four to dose 2, and 14 to dose 3). 21 patients were evaluable for safety. Median follow-up time was

Published
2024
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8. Neurofibromin Is an Estrogen Receptor-α Transcriptional Co-repressor in Breast Cancer

Author

Zheng, Ze-Yi, Anurag, Meenakshi, Lei, Jonathan T., Cao, Jin, Singh, Purba, Peng, Jianheng, Kennedy, Hilda, Nguyen, Nhu-Chau, Chen, Yue, Lavere, Philip, Li, Jing, Du, Xin-Hui, Cakar, Burcu, Song, Wei, Kim, Beom-Jun, Shi, Jiejun, Seker, Sinem, Chan, Doug W., Zhao, Guo-Qiang, Chen, Xi, Banks, Kimberly C., Lanman, Richard B., Shafaee, Maryam Nemati, Zhang, Xiang H.-F., Vasaikar, Suhas, Zhang, Bing, Hilsenbeck, Susan G., Li, Wei, Foulds, Charles E., Ellis, Matthew J., and Chang, Eric C.

Published
2020
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9. Analysis of phosphatases in ER-negative breast cancers identifies DUSP4 as a critical regulator of growth and invasion

Author

Mazumdar, Abhijit, Poage, Graham M, Shepherd, Jonathan, Tsimelzon, Anna, Hartman, Zachary C, Den Hollander, Petra, Hill, Jamal, Zhang, Yun, Chang, Jenny, Hilsenbeck, Susan G, Fuqua, Suzanne, Kent Osborne, C, Mills, Gordon B, and Brown, Powel H

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Breast Cancer, Cancer, Aetiology, 2.1 Biological and endogenous factors, Animals, Breast Neoplasms, Cell Line, Tumor, Cell Movement, Cell Proliferation, Down-Regulation, Dual-Specificity Phosphatases, Female, Gene Expression Regulation, Neoplastic, Humans, MCF-7 Cells, Mice, Mitogen-Activated Protein Kinase Phosphatases, Neoplasm Invasiveness, Neoplasm Transplantation, Phosphorylation, Protein Array Analysis, Receptors, Estrogen, Signal Transduction, MAPK pathways, Mouse xenograft, Phosphatase, TNBC, Clinical Sciences, Oncology & Carcinogenesis, Clinical sciences, Oncology and carcinogenesis
Abstract

Estrogen receptor (ER)-negative cancers have a poor prognosis, and few targeted therapies are available for their treatment. Our previous analyses have identified potential kinase targets critical for the growth of ER-negative, progesterone receptor (PR)-negative and HER2-negative, or "triple-negative" breast cancer (TNBC). Because phosphatases regulate the function of kinase signaling pathways, in this study, we investigated whether phosphatases are also differentially expressed in ER-negative compared to those in ER-positive breast cancers. We compared RNA expression in 98 human breast cancers (56 ER-positive and 42 ER-negative) to identify phosphatases differentially expressed in ER-negative compared to those in ER-positive breast cancers. We then examined the effects of one selected phosphatase, dual specificity phosphatase 4 (DUSP4), on proliferation, cell growth, migration and invasion, and on signaling pathways using protein microarray analyses of 172 proteins, including phosphoproteins. We identified 48 phosphatase genes are significantly differentially expressed in ER-negative compared to those in ER-positive breast tumors. We discovered that 31 phosphatases were more highly expressed, while 11 were underexpressed specifically in ER-negative breast cancers. The DUSP4 gene is underexpressed in ER-negative breast cancer and is deleted in approximately 50 % of breast cancers. Induced DUSP4 expression suppresses both in vitro and in vivo growths of breast cancer cells. Our studies show that induced DUSP4 expression blocks the cell cycle at the G1/S checkpoint; inhibits ERK1/2, p38, JNK1, RB, and NFkB p65 phosphorylation; and inhibits invasiveness of TNBC cells. These results suggest that that DUSP4 is a critical regulator of the growth and invasion of triple-negative breast cancer cells.

Published
2016

10. Blockade of AP-1 Potentiates Endocrine Therapy and Overcomes Resistance

Author

Malorni, Luca, Giuliano, Mario, Migliaccio, Ilenia, Wang, Tao, Creighton, Chad J, Lupien, Mathieu, Fu, Xiaoyong, Hilsenbeck, Susan G, Healy, Nuala, De Angelis, Carmine, Mazumdar, Abhijit, Trivedi, Meghana V, Massarweh, Suleiman, Gutierrez, Carolina, De Placido, Sabino, Jeselsohn, Rinath, Brown, Myles, Brown, Powel H, Osborne, C Kent, and Schiff, Rachel

Subjects
Breast Cancer, Genetics, Cancer, Estrogen, Aetiology, 2.1 Biological and endogenous factors, Animals, Breast Neoplasms, Cell Proliferation, Drug Resistance, Neoplasm, Drug Synergism, Estradiol, Female, Humans, MCF-7 Cells, Mice, Promoter Regions, Genetic, Receptors, Estrogen, Tamoxifen, Transcription Factor AP-1, Xenograft Model Antitumor Assays, Oncology and Carcinogenesis, Developmental Biology, Oncology & Carcinogenesis
Abstract

UnlabelledThe transcription factor AP-1 is downstream of growth factor (GF) receptors (GFRs) and stress-related kinases, both of which are implicated in breast cancer endocrine resistance. Previously, we have suggested that acquired endocrine resistance is associated with increased activity of AP-1 in an in vivo model. In this report, we provide direct evidence for the role of AP-1 in endocrine resistance. First, significant overlap was found between genes modulated in tamoxifen resistance and a gene signature associated with GF-induced estrogen receptor (ER) cistrome. Interestingly, these overlapping genes were enriched for key signaling components of GFRs and stress-related kinases and had AP-1 motifs in their promoters/enhancers. Second, to determine a more definitive role of AP-1 in endocrine resistance, AP-1 was inhibited using an inducible dominant-negative (DN) cJun expressed in MCF7 breast cancer cells in vitro and in vivo AP-1 blockade enhanced the antiproliferative effect of endocrine treatments in vitro, accelerated xenograft tumor response to tamoxifen and estrogen deprivation in vivo, promoted complete regression of tumors, and delayed the onset of tamoxifen resistance. Induction of DN-cJun after the development of tamoxifen resistance resulted in dramatic tumor shrinkage, accompanied by reduced proliferation and increased apoptosis. These data suggest that AP-1 is a key determinant of endocrine resistance by mediating a global shift in the ER transcriptional program.ImplicationsAP-1 represents a viable therapeutic target to overcome endocrine resistance. Mol Cancer Res; 14(5); 470-81. ©2016 AACR.

Published
2016

11. Phosphatase PTP4A3 Promotes Triple-Negative Breast Cancer Growth and Predicts Poor Patient Survival

Author

den Hollander, Petra, Rawls, Kathryn, Tsimelzon, Anna, Shepherd, Jonathan, Mazumdar, Abhijit, Hill, Jamal, Fuqua, Suzanne AW, Chang, Jenny C, Osborne, C Kent, Hilsenbeck, Susan G, Mills, Gordon B, and Brown, Powel H

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Breast Cancer, 2.1 Biological and endogenous factors, Aetiology, Cell Line, Tumor, Cell Proliferation, Humans, Neoplasm Proteins, Phosphoric Monoester Hydrolases, Prognosis, Protein Tyrosine Phosphatases, Signal Transduction, Survival Analysis, Triple Negative Breast Neoplasms, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis
Abstract

Triple-negative breast cancer (TNBC) has the worst prognosis of all breast cancers, and women diagnosed with TNBC currently lack targeted treatment options. To identify novel targets for TNBC, we evaluated phosphatase expression in breast tumors and characterized their contributions to in vitro and in vivo growth of TNBC. Using Affymetrix microarray analysis of 102 breast cancers, we identified 146 phosphatases that were significantly differentially expressed in TNBC compared with estrogen receptor (ER)-positive tumors. Of these, 19 phosphatases were upregulated (0.66-fold; FDR = 0.05) in TNBC compared with ER-positive breast cancers. We knocked down 17 overexpressed phosphatases in four triple-negative and four ER-positive breast cancer lines using specific siRNAs and found that depletion of six of these phosphatases significantly reduced growth and anchorage-independent growth of TNBC cells to a greater extent than ER-positive cell lines. Further analysis of the phosphatase PTP4A3 (also known as PRL-3) demonstrated its requirement for G1-S cell-cycle progression in all breast cancer cells, but PTP4A3 regulated apoptosis selectively in TNBC cells. In addition, PTP4A3 inhibition reduced the growth of TNBC tumors in vivo Moreover, in silico analysis revealed the PTP4A3 gene to be amplified in 29% of basal-like breast cancers, and high expression of PTP4A3 could serve as an independent prognostic indicator for worse overall survival. Collectively, these studies define the importance of phosphatase overexpression in TNBC and lay the foundation for the development of new targeted therapies directed against phosphatases or their respective signaling pathways for TNBC patients. Cancer Res; 76(7); 1942-53. ©2016 AACR.

Published
2016

12. The SOX11 transcription factor is a critical regulator of basal-like breast cancer growth, invasion, and basal-like gene expression

Author

Shepherd, Jonathan H, Uray, Ivan P, Mazumdar, Abhijit, Tsimelzon, Anna, Savage, Michelle, Hilsenbeck, Susan G, and Brown, Powel H

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Breast Cancer, Cancer, Genetics, Biotechnology, Aetiology, 2.1 Biological and endogenous factors, Biomarkers, Tumor, Breast Neoplasms, Cell Line, Tumor, Cell Movement, Cell Proliferation, Female, Gene Expression Regulation, Neoplastic, Humans, Neoplasm Invasiveness, SOXC Transcription Factors, SOX11, basal-like breast cancer, growth, migration, transcription factor, Oncology and carcinogenesis
Abstract

Basal-like breast cancers (BLBCs) are aggressive breast cancers associated with poor survival. Defining the key drivers of BLBC growth will allow identification of molecules for targeted therapy. In this study, we performed a primary screen integrating multiple assays that compare transcription factor expression and activity in BLBC and non-BLBC at the RNA, DNA, and protein levels. This integrated screen identified 33 transcription factors that were elevated in BLBC in multiple assays comparing mRNA expression, DNA cis-element sequences, or protein DNA-binding activity. In a secondary screen to identify transcription factors critical for BLBC cell growth, 8 of the 33 candidate transcription factors (TFs) were found to be necessary for growth in at least two of three BLBC cell lines. Of these 8 transcription factors, SOX11 was the only transcription factor required for BLBC growth, but not for growth of non-BLBC cells. Our studies demonstrate that SOX11 is a critical regulator of multiple BLBC phenotypes, including growth, migration, invasion, and expression of signature BLBC genes. High SOX11 expression was also found to be an independent prognostic indicator of poor survival in women with breast cancer. These results identify SOX11 as a potential target for the treatment of BLBC, the most aggressive form of breast cancer.

Published
2016

13. Comprehensive Genomic Analysis Identifies Novel Subtypes and Targets of Triple-Negative Breast Cancer

Author

Burstein, Matthew D, Tsimelzon, Anna, Poage, Graham M, Covington, Kyle R, Contreras, Alejandro, Fuqua, Suzanne AW, Savage, Michelle I, Osborne, C Kent, Hilsenbeck, Susan G, Chang, Jenny C, Mills, Gordon B, Lau, Ching C, and Brown, Powel H

Subjects
Genetics, Breast Cancer, Biotechnology, Human Genome, Cancer, Adult, Aged, Female, Gene Expression Profiling, Humans, Kaplan-Meier Estimate, Middle Aged, Proportional Hazards Models, Transcriptome, Triple Negative Breast Neoplasms, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

PurposeGenomic profiling studies suggest that triple-negative breast cancer (TNBC) is a heterogeneous disease. In this study, we sought to define TNBC subtypes and identify subtype-specific markers and targets.Experimental designRNA and DNA profiling analyses were conducted on 198 TNBC tumors [estrogen receptor (ER) negativity defined as Allred scale value ≤ 2] with >50% cellularity (discovery set: n = 84; validation set: n = 114) collected at Baylor College of Medicine (Houston, TX). An external dataset of seven publically accessible TNBC studies was used to confirm results. DNA copy number, disease-free survival (DFS), and disease-specific survival (DSS) were analyzed independently using these datasets.ResultsWe identified and confirmed four distinct TNBC subtypes: (i) luminal androgen receptor (AR; LAR), (ii) mesenchymal (MES), (iii) basal-like immunosuppressed (BLIS), and (iv) basal-like immune-activated (BLIA). Of these, prognosis is worst for BLIS tumors and best for BLIA tumors for both DFS (log-rank test: P = 0.042 and 0.041, respectively) and DSS (log-rank test: P = 0.039 and 0.029, respectively). DNA copy number analysis produced two major groups (LAR and MES/BLIS/BLIA) and suggested that gene amplification drives gene expression in some cases [FGFR2 (BLIS)]. Putative subtype-specific targets were identified: (i) LAR: androgen receptor and the cell surface mucin MUC1, (ii) MES: growth factor receptors [platelet-derived growth factor (PDGF) receptor A; c-Kit], (iii) BLIS: an immunosuppressing molecule (VTCN1), and (iv) BLIA: Stat signal transduction molecules and cytokines.ConclusionThere are four stable TNBC subtypes characterized by the expression of distinct molecular profiles that have distinct prognoses. These studies identify novel subtype-specific targets that can be targeted in the future for the effective treatment of TNBCs.

Published
2015

14. Neratinib plus trastuzumab is superior to pertuzumab plus trastuzumab in HER2-positive breast cancer xenograft models

Author

Veeraraghavan, Jamunarani, Gutierrez, Carolina, Sethunath, Vidyalakshmi, Mehravaran, Sepideh, Giuliano, Mario, Shea, Martin J., Mitchell, Tamika, Wang, Tao, Nanda, Sarmistha, Pereira, Resel, Davis, Robert, Goutsouliak, Kristina, Qin, Lanfang, De Angelis, Carmine, Diala, Irmina, Lalani, Alshad S., Nagi, Chandandeep, Hilsenbeck, Susan G., Rimawi, Mothaffar F., Osborne, C. Kent, and Schiff, Rachel

Published
2021
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15. Bacteria-to-Human Protein Networks Reveal Origins of Endogenous DNA Damage

Author

Xia, Jun, Chiu, Li-Ya, Nehring, Ralf B., Bravo Núñez, María Angélica, Mei, Qian, Perez, Mercedes, Zhai, Yin, Fitzgerald, Devon M., Pribis, John P., Wang, Yumeng, Hu, Chenyue W., Powell, Reid T., LaBonte, Sandra A., Jalali, Ali, Matadamas Guzmán, Meztli L., Lentzsch, Alfred M., Szafran, Adam T., Joshi, Mohan C., Richters, Megan, Gibson, Janet L., Frisch, Ryan L., Hastings, P.J., Bates, David, Queitsch, Christine, Hilsenbeck, Susan G., Coarfa, Cristian, Hu, James C., Siegele, Deborah A., Scott, Kenneth L., Liang, Han, Mancini, Michael A., Herman, Christophe, Miller, Kyle M., and Rosenberg, Susan M.

Published
2019
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17. Metastasis tumor-associated protein 2 enhances metastatic behavior and is associated with poor outcomes in estrogen receptor-negative breast cancer

Author

Covington, Kyle R, Brusco, Lauren, Barone, Ines, Tsimelzon, Anna, Selever, Jennifer, Corona-Rodriguez, Arnoldo, Brown, Powel, Kumar, Rakesh, Hilsenbeck, Susan G, and Fuqua, Suzanne AW

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Prevention, Cancer, Breast Cancer, 2.1 Biological and endogenous factors, Aetiology, Clinical Sciences, Oncology & Carcinogenesis, Clinical sciences, Oncology and carcinogenesis
Abstract

Metastasis remains a major clinical problem in breast cancer. One family of genes previously linked with metastasis is the metastasis tumor-associated (MTA) family, with members MTA1 enhancing and MTA3 inhibiting cancer metastasis. We have previously found that MTA2 enhances anchorage-independent growth in estrogen receptor α (ERα) breast cancers, and, in combination with other genes, performed as a predictive biomarker in ERα-positive breast cancer. We therefore hypothesized that MTA2 enhances breast cancer progression. To test this, cell growth, soft-agar colony formation, migration, and in vivo metastasis were examined in MTA2-overexpressing and Vector control transfected ERα-negative breast cancer cells. Pathways regulating cell-cell interaction, adhesion, and signaling through the Rho pathway were also investigated. Effects of the inhibition of the Rho pathway using a Rho Kinase inhibitor were assessed in soft-agar colony formation and motility assays in MTA2-overexpressing cells. MTA2 expression was associated with poor prognostic markers, and levels of MTA2 were associated with increased risk of early recurrence in retrospective analyses. MTA2 overexpression was associated with enhanced metastasis, and pathways regulating cell-cell interactions in vitro and in vivo. Most critically, MTA2-enhanced motility could be blocked by inhibiting Rho pathway signaling. We present the novel finding that MTA2 defined a subset of ERα-negative patients with a particularly poor outcome.

Published
2013

18. The oral selective oestrogen receptor degrader (SERD) AZD9496 is comparable to fulvestrant in antagonising ER and circumventing endocrine resistance

Author

Nardone, Agostina, Weir, Hazel, Delpuech, Oona, Brown, Henry, De Angelis, Carmine, Cataldo, Maria Letizia, Fu, Xiaoyong, Shea, Martin J., Mitchell, Tamika, Veeraraghavan, Jamunarani, Nagi, Chandandeep, Pilling, Mark, Rimawi, Mothaffar F., Trivedi, Meghana, Hilsenbeck, Susan G., Chamness, Gary C., Jeselsohn, Rinath, Osborne, C. Kent, and Schiff, Rachel

Published
2019
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19. A moderate elevation of circulating levels of IGF-I does not alter ErbB2 induced mammary tumorigenesis

Author

Dearth, Robert K, Kuiatse, Isere, Wang, Yu-Fen, Liao, Lan, Hilsenbeck, Susan G, Brown, Powel H, Xu, Jianming, and Lee, Adrian V

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Breast Cancer, Aetiology, 2.1 Biological and endogenous factors, Animals, Cell Transformation, Neoplastic, Female, Gene Expression Regulation, Insulin-Like Growth Factor I, Mammary Glands, Animal, Mammary Neoplasms, Experimental, Mice, Mice, Inbred C57BL, Mice, Transgenic, Receptor, ErbB-2, Signal Transduction, Transgenes, Receptor, erbB-2, Public Health and Health Services, Oncology & Carcinogenesis, Oncology and carcinogenesis, Epidemiology
Abstract

BackgroundEpidemiological evidence suggests that moderately elevated levels of circulating insulin-like growth factor-I (IGF-I) are associated with increased risk of breast cancer in women. How circulating IGF-I may promote breast cancer incidence is unknown, however, increased IGF-I signaling is linked to trastuzumab resistance in ErbB2 positive breast cancer. Few models have directly examined the effect of moderately high levels of circulating IGF-I on breast cancer initiation and progression. The purpose of this study was to assess the ability of circulating IGF-I to independently initiate mammary tumorigenesis and/or accelerate the progression of ErbB2 mediated mammary tumor growth.MethodsWe crossed heterozygous TTR-IGF-I mice with heterozygous MMTV-ErbB2 mice to generate 4 different genotypes: TTR-IGF-I/MMTV-ErbB2 (bigenic), TTR-IGF-I only, MMTV-ErbB2 only, and wild type (wt). Virgin females were palpated twice a week and harvested when tumors reached 1000 mm(3). For study of normal development, blood and tissue were harvested at 4, 6 and 9 weeks of age in TTR-IGF-I and wt mice.ResultsTTR-IGF-I and TTR-IGF-I/ErbB2 bigenic mice showed a moderate 35% increase in circulating total IGF-I compared to ErbB2 and wt control mice. Elevation of circulating IGF-I had no effect upon pubertal mammary gland development. The transgenic increase in IGF-I alone wasn't sufficient to initiate mammary tumorigenesis. Elevated circulating IGF-I had no effect upon ErbB2-induced mammary tumorigenesis or metastasis, with median time to tumor formation being 30 wks and 33 wks in TTR-IGF-I/ErbB2 bigenic and ErbB2 mice respectively (p = 0.65). Levels of IGF-I in lysates from ErbB2/TTR-IGF-I tumors compared to ErbB2 was elevated in a similar manner to the circulating IGF-I, however, there was no effect on the rate of tumor growth (p = 0.23). There were no morphological differences in tumor type (solid adenocarcinomas) between bigenic and ErbB2 mammary glands.ConclusionUsing the first transgenic animal model to elevate circulating levels of IGF-I to those comparable to women at increased risk of breast cancer, we showed that moderately high levels of systemic IGF-I have no effect on pubertal mammary gland development, initiating mammary tumorigenesis or promoting ErbB2 driven mammary carcinogenesis. Our work suggests that ErbB2-induced mammary tumorigenesis is independent of the normal variation in circulating levels of IGF-I.

Published
2011

20. beta1 Integrin mediates an alternative survival pathway in breast cancer cells resistant to lapatinib

Author

Huang, Catherine, Park, Catherine C, Hilsenbeck, Susan G, Ward, Robin, Rimawi, Mothaffar F, Wang, Yen-chao, Shou, Jiang, Bissell, Mina J, Osborne, C Kent, and Schiff, Rachel

Abstract

Abstract Introduction The overexpression of human epidermal growth factor receptor (HER)-2 in 20% of human breast cancers and its association with aggressive growth has led to widespread use of HER2-targeted therapies, such as trastuzumab (T) and lapatinib (L). Despite the success of these drugs, their efficacy is limited in patients whose tumors demonstrate de novo or acquired resistance to treatment. The β1 integrin resides on the membrane of the breast cancer cell, activating several elements of breast tumor progression including proliferation and survival. Methods We developed a panel of HER2-overexpressing cell lines resistant to L, T, and the potent LT combination through long-term exposure and validated these models in 3D culture. Parental and L/T/LT-resistant cells were subject to HER2 and β1 integrin inhibitors in 3D and monitored for 12 days, followed by quantification of colony number. Parallel experiments were conducted where cells were either stained for Ki-67 and Terminal deoxynucleotidyl transferase dUTP nick end labeling (TUNEL) or harvested for protein and analyzed by immunoblot. Results were subjected to statistical testing using analysis of variance and linear contrasts, followed by adjustment with the Sidak method. Results Using multiple cell lines including BT474 and HCC1954, we reveal that in L and LT resistance, where phosphorylation of EGFR/HER1, HER2, and HER3 are strongly inhibited, kinases downstream of β1 integrin--including focal adhesion kinase (FAK) and Src--are up-regulated. Blockade of β1 by the antibody AIIB2 abrogates this up-regulation and functionally achieves significant growth inhibition of L and LT resistant cells in 3D, without dramatically affecting the parental cells. SiRNA against β1 as well as pharmacologic inhibition of FAK achieve the same growth inhibitory effect. In contrast, trastuzumab-resistant cells, which retain high levels of phosphorylated EGFR/HER1, HER2, and HER3, are only modestly growth-inhibited by AIIB2. Conclusions Our data suggest that HER2 activity, which is suppressed in resistance involving L but not T alone, dictates whether β1 mediates an alternative pathway driving resistance. Our findings justify clinical studies investigating the inhibition of β1 or its downstream signaling moieties as strategies to overcome acquired L and LT resistance.

Published
2011

21. Proteomic and transcriptomic profiling reveals a link between the PI3K pathway and lower estrogen receptor (ER) levels and activity in ER+ breast cancer

Author

Creighton, Chad J, Fu, Xiaoyong, Hennessy, Bryan T, Casa, Angelo J, Zhang, Yiqun, Gonzalez-Angulo, Ana Maria, Lluch, Ana, Gray, Joe W, Brown, Powell H, Hilsenbeck, Susan G, Osborne, C Kent, Mills, Gordon B, Lee, Adrian V, and Schiff, Rachel

Abstract

Abstract Introduction Accumulating evidence suggests that both levels and activity of the estrogen receptor (ER) and the progesterone receptor (PR) are dramatically influenced by growth-factor receptor (GFR) signaling pathways, and that this crosstalk is a major determinant of both breast cancer progression and response to therapy. The phosphatidylinositol 3-kinase (PI3K) pathway, a key mediator of GFR signaling, is one of the most altered pathways in breast cancer. We thus examined whether deregulated PI3K signaling in luminal ER+ breast tumors is associated with ER level and activity and intrinsic molecular subtype. Methods We defined two independent molecular signatures of the PI3K pathway: a proteomic (reverse-phase proteomic array) PI3K signature, based on protein measurement for PI3K signaling intermediates, and a PI3K transcriptional (mRNA) signature based on the set of genes either induced or repressed by PI3K inhibitors. By using these signatures, we scored each ER+ breast tumor represented in multiple independent expression-profiling datasets (four mRNA, n = 915; one protein, n = 429) for activation of the PI3K pathway. Effects of PI3K inhibitor BEZ-235 on ER expression and activity levels and cell growth were tested by quantitative real-time PCR and cell proliferation assays. Results Within ER+ tumors, ER levels were negatively correlated with the PI3K activation scores, both at the proteomic and transcriptional levels, in all datasets examined. PI3K signature scores were also higher in ER+ tumors and cell lines of the more aggressive luminal B molecular subtype versus those of the less aggressive luminal A subtype. Notably, BEZ-235 treatment in four different ER+ cell lines increased expression of ER and ER target genes including PR, and treatment with IGF-I (which signals via PI3K) decreased expression of ER and target genes, thus further establishing an inverse functional relation between ER and PI3K. BEZ-235 had an additional effect on tamoxifen in inhibiting the growth of a number of ER+ cell lines. Conclusions Our data suggest that luminal B tumors have hyperactive GFR/PI3K signaling associated with lower ER levels, which has been correlated with resistance to endocrine therapy. Targeting PI3K in these tumors might reverse loss of ER expression and signaling and restore hormonal sensitivity.

Published
2010

22. Proteogenomic Approaches for the Identification of NF1/Neurofibromin-depleted Estrogen Receptor–positive Breast Cancers for Targeted Treatment

Author

Kim, Beom-Jun, primary, Zheng, Ze-Yi, additional, Lei, Jonathan T., additional, Holt, Matthew V., additional, Chen, Anran, additional, Peng, Jianheng, additional, Fandino, Diana, additional, Singh, Purba, additional, Kennedy, Hilda, additional, Dou, Yongchao, additional, Chica-Parrado, María del Rosario, additional, Bikorimana, Emmanuel, additional, Ye, Dan, additional, Wang, Yunguan, additional, Hanker, Ariella B., additional, Mohamed, Nada, additional, Hilsenbeck, Susan G., additional, Lim, Bora, additional, Asirvatham, Jaya Ruth, additional, Sreekumar, Arun, additional, Zhang, Bing, additional, Miles, George, additional, Anurag, Meenakshi, additional, Ellis, Matthew J., additional, and Chang, Eric C., additional

Published
2023
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24. BCL9/STAT3 regulation of transcriptional enhancer networks promote DCIS progression

Author

Elsarraj, Hanan S., Hong, Yan, Limback, Darlene, Zhao, Ruonan, Berger, Jenna, Bishop, Stephanie C., Sabbagh, Aria, Oppenheimer, Linzi, Harper, Haleigh E., Tsimelzon, Anna, Huang, Shixia, Hilsenbeck, Susan G., Edwards, Dean P., Fontes, Joseph, Fan, Fang, Madan, Rashna, Fangman, Ben, Ellis, Ashley, Tawfik, Ossama, Persons, Diane L., Fields, Timothy, Godwin, Andrew K., Hagan, Christy R., Swenson-Fields, Katherine, Coarfa, Cristian, Thompson, Jeffrey, and Behbod, Fariba

Published
2020
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26. Combinatorial inhibition of PTPN12-regulated receptors leads to a broadly effective therapeutic strategy in triple-negative breast cancer

Author

Nair, Amritha, Chung, Hsiang-Ching, Sun, Tingting, Tyagi, Siddhartha, Dobrolecki, Lacey E, Dominguez-Vidana, Rocio, Kurley, Sarah J, Orellana, Mayra, Renwick, Alexander, Henke, David M, Katsonis, Panagiotis, Schmitt, Earlene, Chan, Doug W, Li, Hui, Mao, Sufeng, Petrovic, Ivana, Creighton, Chad J, Gutierrez, Carolina, Dubrulle, Julien, Stossi, Fabio, Tyner, Jeffrey W, Lichtarge, Olivier, Lin, Charles Y, Zhang, Bing, Scott, Kenneth L, Hilsenbeck, Susan G, Sun, Jinpeng, Yu, Xiao, Osborne, C Kent, Schiff, Rachel, Christensen, James G, Shields, David J, Rimawi, Mothaffar F, Ellis, Matthew J, Shaw, Chad A, Lewis, Michael T, and Westbrook, Thomas F

Subjects
Cell receptors -- Health aspects, Esterases -- Health aspects, Gene mutation -- Health aspects, Breast cancer -- Genetic aspects -- Development and progression -- Care and treatment, Gene expression -- Health aspects, Biological sciences, Health
Abstract

Author(s): Amritha Nair [1, 2]; Hsiang-Ching Chung [1, 2, 3]; Tingting Sun [1, 2]; Siddhartha Tyagi [1, 2]; Lacey E Dobrolecki [4]; Rocio Dominguez-Vidana [1, 2, 3]; Sarah J Kurley [...]

Published
2018
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28. A Multiparameter Molecular Classifier to Predict Response to Neoadjuvant Lapatinib plus Trastuzumab without Chemotherapy in HER2+ Breast Cancer

Author

Veeraraghavan, Jamunarani, primary, Gutierrez, Carolina, additional, De Angelis, Carmine, additional, Davis, Robert, additional, Wang, Tao, additional, Pascual, Tomas, additional, Selenica, Pier, additional, Sanchez, Katherine, additional, Nitta, Hiroaki, additional, Kapadia, Monesh, additional, Pavlick, Anne C., additional, Galvan, Patricia, additional, Rexer, Brent, additional, Forero-Torres, Andres, additional, Nanda, Rita, additional, Storniolo, Anna M., additional, Krop, Ian E., additional, Goetz, Matthew P., additional, Nangia, Julie R., additional, Wolff, Antonio C., additional, Weigelt, Britta, additional, Reis-Filho, Jorge S., additional, Hilsenbeck, Susan G., additional, Prat, Aleix, additional, Osborne, C. Kent, additional, Schiff, Rachel, additional, and Rimawi, Mothaffar F., additional

Published
2023
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30. FOXA1 overexpression mediates endocrine resistance by altering the ER transcriptome and IL-8 expression in ER-positive breast cancer

Author

Fu, Xiaoyong, Jeselsohn, Rinath, Pereira, Resel, Hollingsworth, Emporia F., Creighton, Chad J., Li, Fugen, Shea, Martin, Nardone, Agostina, De Angelis, Carmine, Heiser, Laura M., Anur, Pavana, Wang, Nicholas, Grasso, Catherine S., Spellman, Paul T., Griffith, Obi L., Tsimelzon, Anna, Gutierrez, Carolina, Huang, Shixia, Edwards, Dean P., Trivedi, Meghana V., Rimawi, Mothaffar F., Lopez-Terrada, Dolores, Hilsenbeck, Susan G., Gray, Joe W., Brown, Myles, Osborne, C. Kent, and Schiff, Rachel

Published
2016

31. The Signaling Pathways Project, an integrated ‘omics knowledgebase for mammalian cellular signaling pathways

Author

Ochsner, Scott A., Abraham, David, Martin, Kirt, Ding, Wei, McOwiti, Apollo, Kankanamge, Wasula, Wang, Zichen, Andreano, Kaitlyn, Hamilton, Ross A., Chen, Yue, Hamilton, Angelica, Gantner, Marin L., Dehart, Michael, Qu, Shijing, Hilsenbeck, Susan G., Becnel, Lauren B., Bridges, Dave, Ma’ayan, Avi, Huss, Janice M., Stossi, Fabio, Foulds, Charles E., Kralli, Anastasia, McDonnell, Donald P., and McKenna, Neil J.

Published
2019
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32. Abstract P2-23-01: Patient-derived xenografts allow deconvolution of single agent and combination chemotherapy responses in triple-negative breast cancer

Author

Lei, Jonathan T., primary, Huang, Chen, additional, Srinivasan, Ramakrishnan R., additional, Vasaikar, Suhas, additional, Dobrolecki, Lacey E., additional, Lewis, Alaina N., additional, Zhao, Na, additional, Cao, Jin, additional, Hilsenbeck, Susan G., additional, Osborne, C. Kent, additional, Rimawi, Mothaffar, additional, Ellis, Matthew J., additional, Petrosyan, Varduhi, additional, Saltzman, Alexander B., additional, Malovannaya, Anna, additional, Landua, John D., additional, Wen, Bo, additional, Jain, Antrix, additional, Wulf, Gerburg M., additional, Li, Shunqiang, additional, Kraushaar, Daniel C., additional, Wang, Tao, additional, Chen, Xi, additional, Echeverria, Gloria V., additional, Anurag, Meenakshi, additional, Zhang, Bing, additional, and Lewis, Michael T., additional

Published
2023
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34. The Oncogenic STP Axis Promotes Triple-Negative Breast Cancer via Degradation of the REST Tumor Suppressor

Author

Karlin, Kristen L., Mondal, Gourish, Hartman, Jessica K., Tyagi, Siddhartha, Kurley, Sarah J., Bland, Chris S., Hsu, Tiffany Y.T., Renwick, Alexander, Fang, Justin E., Migliaccio, Ilenia, Callaway, Celetta, Nair, Amritha, Dominguez-Vidana, Rocio, Nguyen, Don X., Osborne, C. Kent, Schiff, Rachel, Yu-Lee, Li-Yuan, Jung, Sung Y., Edwards, Dean P., Hilsenbeck, Susan G., Rosen, Jeffrey M., Zhang, Xiang H.-F., Shaw, Chad A., Couch, Fergus J., and Westbrook, Thomas F.

Published
2014
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35. GATA2 facilitates steroid receptor coactivator recruitment to the androgen receptor complex

Author

He, Bin, Lanz, Rainer B., Fiskus, Warren, Geng, Chuandong, Yi, Ping, Hartig, Sean M., Rajapakshe, Kimal, Shou, John, Wei, Liping, Shah, Shrijal S., Foley, Christopher, Chew, Sue Anne, Eedunuri, Vijay K., Bedoya, Diego J., Feng, Qin, Minami, Takashi, Mitsiades, Constantine S., Frolov, Anna, Weigel, Nancy L., Hilsenbeck, Susan G., Rosen, Daniel G., Palzkill, Timothy, Ittmann, Michael M., Song, Yongcheng, Coarfa, Cristian, O'Malley, Bert W., and Mitsiades, Nicholas

Published
2014

42. Residual Breast Cancers after Conventional Therapy Display Mesenchymal as Well as Tumor-Initiating Features

Author

Creighton, Chad J., Li, Xiaoxian, Landis, Melissa, Dixon, J. Michael, Neumeister, Veronique M., Sjolund, Ashley, Rimm, David L., Wong, Helen, Rodriguez, Angel, Herschkowitz, Jason I., Fan, Cheng, Zhang, Xiaomei, He, Xiaping, Pavlick, Anne, Gutierrez, M. Carolina, Renshaw, Lorna, Larionov, Alexey A., Faratian, Dana, Hilsenbeck, Susan G., Perou, Charles M., Lewis, Michael T., Rosen, Jeffrey M., Chang, Jenny C., and Weinberg, Robert A.

Published
2009
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44. Activation of Multiple Proto-oncogenic Tyrosine Kinases in Breast Cancer via Loss of the PTPN12 Phosphatase

Author

Sun, Tingting, Aceto, Nicola, Meerbrey, Kristen L., Kessler, Jessica D., Zhou, Chunshui, Migliaccio, Ilenia, Nguyen, Don X., Pavlova, Natalya N., Botero, Maria, Huang, Jian, Bernardi, Ronald J., Schmitt, Earlene, Hu, Guang, Li, Mamie Z., Dephoure, Noah, Gygi, Steven P., Rao, Mitchell, Creighton, Chad J., Hilsenbeck, Susan G., Shaw, Chad A., Muzny, Donna, Gibbs, Richard A., Wheeler, David A., Osborne, C. Kent, Schiff, Rachel, Bentires-Alj, Mohamed, Elledge, Stephen J., and Westbrook, Thomas F.

Published
2011
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45. Abstract P5-07-01: Proteogenomic analysis of differential chemotherapy responses in patient-derived xenografts of triple-negative breast cancer

Author

Lei, Jonathan T, primary, Huang, Chen, additional, Srinivasan, Ramakrishnan R, additional, Vasaikar, Suhas, additional, Dobrolecki, Lacey E, additional, Lewis, Alaina N, additional, Sallas, Christina, additional, Hilsenbeck, Susan G, additional, Osborne, C. Kent, additional, Rimawi, Mothaffar F, additional, Ellis, Matthew J, additional, Petrosyan, Varduhi, additional, Saltzman, Alexander B, additional, Malovannaya, Anna, additional, Wulf, Gerburg, additional, Kraushaar, Daniel C, additional, Wang, Tao, additional, Chen, Xi, additional, Echeverria, Gloria V, additional, Anurag, Meenakshi, additional, Zhang, Bing, additional, and Lewis, Michael T, additional

Published
2022
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49. Tumor Suppressor PLK2 May Serve as a Biomarker in Triple-Negative Breast Cancer for Improved Response to PLK1 Therapeutics

Author

Gao, Yang, primary, Kabotyanski, Elena B., additional, Shepherd, Jonathan H., additional, Villegas, Elizabeth, additional, Acosta, Deanna, additional, Hamor, Clark, additional, Sun, Tingting, additional, Montmeyor-Garcia, Celina, additional, He, Xiaping, additional, Dobrolecki, Lacey E., additional, Westbrook, Thomas F., additional, Lewis, Michael T., additional, Hilsenbeck, Susan G., additional, Zhang, Xiang H.-F., additional, Perou, Charles M., additional, and Rosen, Jeffrey M., additional

Published
2021
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