Your search keyword '"Heather Tillman"' showing total 67 results

1. A Novel Orthotopic Implantation Technique for Osteosarcoma Produces Spontaneous Metastases and Illustrates Dose-Dependent Efficacy of B7-H3-CAR T Cells

Author

Lindsay Jones Talbot, Ashley Chabot, Amy Funk, Phuong Nguyen, Jessica Wagner, Aaron Ross, Heather Tillman, Andrew Davidoff, Stephen Gottschalk, and Christopher DeRenzo

Subjects

osteosarcoma, orthotopic, model, CAR, T cell therapy, B7-H3, Immunologic diseases. Allergy, RC581-607

Abstract

The outcome for metastatic pediatric osteosarcoma (OS) remains poor. Thus, there is an urgent need to develop novel therapies, and immunotherapy with CAR T cells has the potential to meet this challenge. However, there is a lack of preclinical models that mimic salient features of human disease including reliable development of metastatic disease post orthotopic OS cell injection. To overcome this roadblock, and also enable real-time imaging of metastatic disease, we took advantage of LM7 OS cells expressing firefly luciferase (LM7.ffLuc). LM7.ffLuc were implanted in a collagen mesh into the tibia of mice, and mice reliably developed orthotopic tumors and lung metastases as judged by bioluminescence imaging and histopathological analysis. Intratibial implantation also enabled surgical removal by lower leg amputation and monitoring for metastases development post-surgery. We then used this model to evaluate the antitumor activity of CAR T cells targeting B7-H3, an antigen that is expressed in a broad range of solid tumors including OS. B7-H3-CAR T cells had potent antitumor activity in a dose-dependent manner and inhibited the development of pulmonary metastases resulting in a significant survival advantage. In contrast T cells expressing an inactive B7-H3-CAR had no antitumor activity. Using unmodified LM7 cells also enabled us to demonstrate that B7-H3-CAR T cells traffic to orthotopic tumor sites. Hence, we have developed an orthotopic, spontaneously metastasizing OS model. This model may improve our ability not only to predict the safety and efficacy of current and next generation CAR T cell therapies but also other treatment modalities for metastatic OS.

Published

2021

2. MYC competes with MiT/TFE in regulating lysosomal biogenesis and autophagy through an epigenetic rheostat

Author

Ida Annunziata, Diantha van de Vlekkert, Elmar Wolf, David Finkelstein, Geoffrey Neale, Eda Machado, Rosario Mosca, Yvan Campos, Heather Tillman, Martine F. Roussel, Jason Andrew Weesner, Leigh Ellen Fremuth, Xiaohui Qiu, Min-Joon Han, Gerard C. Grosveld, and Alessandra d’Azzo

Subjects

Science

Abstract

Genes related to lysosomal and autophagic systems are transcriptionally regulated by the Mit/TFE family of transcription factors. Here the authors show that MYC, in association with HDACs, suppresses the expression of lysosomal and autophagy genes by competing with the Mit/TFE transcription factors for occupancy of their target gene promoters.

Published

2019

3. 17-DMAG dually inhibits Hsp90 and histone lysine demethylases in alveolar rhabdomyosarcoma

Author

Shivendra Singh, Ahmed Abu-Zaid, Wenwei Lin, Jonathan Low, Alireza Abdolvahabi, Hongjian Jin, Qiong Wu, Bailey Cooke, Jie Fang, John Bowling, Sivaraja Vaithiyalingam, Duane Currier, Mi-Kyung Yun, Dinesh M. Fernando, Julie Maier, Heather Tillman, Purva Bulsara, Zhaohua Lu, Sourav Das, Anang Shelat, Zhenmei Li, Brandon Young, Richard Lee, Zoran Rankovic, Andrew J. Murphy, Stephen W. White, Andrew M. Davidoff, Taosheng Chen, and Jun Yang

Subjects

Molecular Biology, Cancer, Omics, Science

Abstract

Summary: Histone lysine demethylases (KDMs) play critical roles in oncogenesis and therefore may be effective targets for anticancer therapy. Using a time-resolved fluorescence resonance energy transfer demethylation screen assay, in combination with multiple orthogonal validation approaches, we identified geldanamycin and its analog 17-DMAG as KDM inhibitors. In addition, we found that these Hsp90 inhibitors increase degradation of the alveolar rhabdomyosarcoma (aRMS) driver oncoprotein PAX3-FOXO1 and induce the repressive epigenetic mark H3K9me3 and H3K36me3 at genomic loci of PAX3-FOXO1 targets. We found that as monotherapy 17-DMAG significantly inhibits expression of PAX3-FOXO1 target genes and multiple oncogenic pathways, induces a muscle differentiation signature, delays tumor growth and extends survival in aRMS xenograft mouse models. The combination of 17-DMAG with conventional chemotherapy significantly enhances therapeutic efficacy, indicating that targeting KDM in combination with chemotherapy may serve as a therapeutic approach to PAX3-FOXO1-positive aRMS.

Published

2021

4. Redox-Regulation of α-Globin in Vascular Physiology

Author

Laurent Kiger, Julia Keith, Abdullah Freiwan, Alfonso G. Fernandez, Heather Tillman, Brant E. Isakson, Mitchell J. Weiss, and Christophe Lechauve

Subjects

α-globin, endothelial nitric oxide synthase (eNOS), cytochrome, redox system, arteries, blood pressure, Therapeutics. Pharmacology, RM1-950

Abstract

Interest in the structure, function, and evolutionary relations of circulating and intracellular globins dates back more than 60 years to the first determination of the three-dimensional structure of these proteins. Non-erythrocytic globins have been implicated in circulatory control through reactions that couple nitric oxide (NO) signaling with cellular oxygen availability and redox status. Small artery endothelial cells (ECs) express free α-globin, which causes vasoconstriction by degrading NO. This reaction converts reduced (Fe2+) α-globin to the oxidized (Fe3+) form, which is unstable, cytotoxic, and unable to degrade NO. Therefore, (Fe3+) α-globin must be stabilized and recycled to (Fe2+) α-globin to reinitiate the catalytic cycle. The molecular chaperone α-hemoglobin-stabilizing protein (AHSP) binds (Fe3+) α-globin to inhibit its degradation and facilitate its reduction. The mechanisms that reduce (Fe3+) α-globin in ECs are unknown, although endothelial nitric oxide synthase (eNOS) and cytochrome b5 reductase (CyB5R3) with cytochrome b5 type A (CyB5a) can reduce (Fe3+) α-globin in solution. Here, we examine the expression and cellular localization of eNOS, CyB5a, and CyB5R3 in mouse arterial ECs and show that α-globin can be reduced by either of two independent redox systems, CyB5R3/CyB5a and eNOS. Together, our findings provide new insights into the regulation of blood vessel contractility.

Published

2022

5. Platelets Promote Metastasis via Binding Tumor CD97 Leading to Bidirectional Signaling that Coordinates Transendothelial Migration

Author

Yvona Ward, Ross Lake, Farhoud Faraji, Jamie Sperger, Philip Martin, Cameron Gilliard, Kimberly P. Ku, Tamara Rodems, David Niles, Heather Tillman, JuanJuan Yin, Kent Hunter, Adam G. Sowalsky, Joshua Lang, and Kathleen Kelly

Subjects

Biology (General), QH301-705.5

Abstract

Summary: Tumor cells initiate platelet activation leading to the secretion of bioactive molecules, which promote metastasis. Platelet receptors on tumors have not been well-characterized, resulting in a critical gap in knowledge concerning platelet-promoted metastasis. We identify a direct interaction between platelets and tumor CD97 that stimulates rapid bidirectional signaling. CD97, an adhesion G protein-coupled receptor (GPCR), is an overexpressed tumor antigen in several cancer types. Purified CD97 extracellular domain or tumor cell-associated CD97 stimulated platelet activation. CD97-initiated platelet activation led to granule secretion, including the release of ATP, a mediator of endothelial junction disruption. Lysophosphatidic acid (LPA) derived from platelets induced tumor invasiveness via proximal CD97-LPAR heterodimer signaling, coupling coincident tumor cell migration and vascular permeability to promote transendothelial migration. Consistent with this, CD97 was necessary for tumor cell-induced vascular permeability in vivo and metastasis formation in preclinical models. These findings support targeted blockade of tumor CD97 as an approach to ameliorate metastatic spread. : Tumor-initiated platelet activation promotes tissue invasion of cancer cells and metastasis. Ward et al. demonstrate that a common tumor-associated antigen, CD97, accounts for platelet activation and participates directly in LPA-mediated signal transduction leading to tumor cell invasion. CD97 promotes vascular extravasation and metastasis in pre-clinical models. Keywords: platelets, metastasis, transendothelial migration, circulating tumor cells, CD97, adhesion GPCR, LPA

Published

2018

6. Supplementary Figures 11-18 from Antitumor Effects of CAR T Cells Redirected to the EDB Splice Variant of Fibronectin

Author

Stephen Gottschalk, Giedre Krenciute, Heather Tillman, Shondra M. Pruett-Miller, Shaina N. Porter, Jinghui Zhang, Deanna Langfitt, Alejandro Allo Anido, Timothy I. Shaw, Elizabeth Wickman, and Jessica Wagner

Abstract

Supplementary Figures 11-18

Published

2023

7. Data from Antitumor Effects of CAR T Cells Redirected to the EDB Splice Variant of Fibronectin

Author

Stephen Gottschalk, Giedre Krenciute, Heather Tillman, Shondra M. Pruett-Miller, Shaina N. Porter, Jinghui Zhang, Deanna Langfitt, Alejandro Allo Anido, Timothy I. Shaw, Elizabeth Wickman, and Jessica Wagner

Abstract

Chimeric antigen receptor (CAR) T-cell therapy has had limited success in early-phase clinical studies for solid tumors. Lack of efficacy is most likely multifactorial, including a limited array of targetable antigens. We reasoned that targeting the cancer-specific extra domain B (EDB) splice variant of fibronectin might overcome this limitation because it is abundantly secreted by cancer cells and adheres to their cell surface. In vitro, EDB-CAR T cells recognized and killed EDB-positive tumor cells. In vivo, 1 × 106 EDB-CAR T cells had potent antitumor activity in both subcutaneous and systemic tumor xenograft models, resulting in a significant survival advantage in comparison with control mice. EDB-CAR T cells also targeted the tumor vasculature, as judged by IHC and imaging, and their antivascular activity was dependent on the secretion of EDB by tumor cells. Thus, targeting tumor-specific splice variants such as EDB with CAR T cells is feasible and has the potential to improve the efficacy of CAR T-cell therapy.

Published

2023

8. Data from Positron Emission Tomography Detects In Vivo Expression of Disialoganglioside GD2 in Mouse Models of Primary and Metastatic Osteosarcoma

Author

Scott E. Snyder, Barry L. Shulkin, Yuanyuan Han, Amy L. Vāvere, Shana V. Stoddard, Alan B. Packard, Jason L.J. Dearling, Armita Bahrami, Jieun Kim, Jitendra K. Mishra, Elizabeth Stewart, Heather Tillman, Victor Amador Diaz, Paul E. Mead, and Elizabeth R. Butch

Abstract

The cell membrane glycolipid GD2 is expressed by multiple solid tumors, including 88% of osteosarcomas and 98% of neuroblastomas. However, osteosarcomas are highly heterogeneous, with many tumors exhibiting GD2 expression on 64Cu]Cu-Bn-NOTA-hu14.18K322A to detect GD2 expression in osteosarcomas (six patient-derived xenografts and one cell line) in vivo using positron emission tomography (PET). Tumor uptake of the radiolabeled, humanized anti-GD2 antibody [64Cu]Cu-Bn-NOTA-hu14.18K322A was 7-fold higher in modestly GD2-expressing osteosarcomas (32% GD2-positive cells) than in a GD2-negative tumor (9.8% vs. 1.3% of the injected dose per cc, respectively). This radiotracer also identified lesions as small as 29 mm3 in a 34% GD2-positive model of metastatic osteosarcoma of the lung. Radiolabeled antibody accumulation in patient-derived xenografts correlated with GD2 expression as measured by flow cytometry (Pearson r = 0.88, P = 0.01), distinguishing moderately GD2-expressing osteosarcomas (32%–69% GD2-positive cells) from high GD2 expressors (>99%, P < 0.05). These results support the utility of GD2 imaging with PET to measure GD2 expression in osteosarcoma and thus maximize the clinical impact of anti-GD2 immunotherapy.Significance:In situ assessment of all GD2-positive osteosarcoma sites with a novel PET radiotracer could significantly impact anti-GD2 immunotherapy patient selection and enable noninvasive probing of correlations between target expression and therapeutic response.

Published

2023

9. Supplementary Data from Positron Emission Tomography Detects In Vivo Expression of Disialoganglioside GD2 in Mouse Models of Primary and Metastatic Osteosarcoma

Author

Scott E. Snyder, Barry L. Shulkin, Yuanyuan Han, Amy L. Vāvere, Shana V. Stoddard, Alan B. Packard, Jason L.J. Dearling, Armita Bahrami, Jieun Kim, Jitendra K. Mishra, Elizabeth Stewart, Heather Tillman, Victor Amador Diaz, Paul E. Mead, and Elizabeth R. Butch

Abstract

Combined Supplementary Data file containing: Figure S1-Detailed ex vivo biodistribution data for three additional PDX tumors. Only summary data included in the manuscript Table 1. Figure S2-Multimodality imaging protocol. Figure S3-Ex vivo biodistribution of 64Cu-Bn-NOTA-hu14.18K322A in mice with and without co-injection of a therapeutic dose of unmodified hu14.18K322A to verify non-target binding. Table S1-Summary of multi-modality imaging results for all 8 animals in the osteosarcoma lung metastasis model.

Published

2023

10. Data Supplement from AR-Regulated TWEAK-FN14 Pathway Promotes Prostate Cancer Bone Metastasis

Author

Kathleen Kelly, Robert Vessella, Colm Morrissey, Eva Corey, Ross Lake, Lei Fang, Kris Ylaya, Stephen Hewitt, Ben Barrett, Heather Tillman, Yen-Nien Liu, and JuanJuan Yin

Abstract

Supplemental Figure 1.(A) In vitro growth assay for DU145/RasB1 and DU145/RasB1Fn14shRNA cell lines. (B) Average body weight of mice bearing DU145/RasB1 tumors (n= 9mice) or DU145/RasB1Fn14shRNA tumors over time after tumor cell inoculation (shRNA1, n=10 mice; shRNA2, n=10 mice). * p

Published

2023

11. Data from AR-Regulated TWEAK-FN14 Pathway Promotes Prostate Cancer Bone Metastasis

Author

Kathleen Kelly, Robert Vessella, Colm Morrissey, Eva Corey, Ross Lake, Lei Fang, Kris Ylaya, Stephen Hewitt, Ben Barrett, Heather Tillman, Yen-Nien Liu, and JuanJuan Yin

Abstract

The recurrence of prostate cancer metastases to bone after androgen deprivation therapy is a major clinical challenge. We identified FN14 (TNFRSF12A), a TNF receptor family member, as a factor that promotes prostate cancer bone metastasis. In experimental models, depletion of FN14 inhibited bone metastasis, and FN14 could be functionally reconstituted with IKKβ-dependent, NFκB signaling activation. In human prostate cancer, upregulated FN14 expression was observed in more than half of metastatic samples. In addition, FN14 expression was correlated inversely with androgen receptor (AR) signaling output in clinical samples. Consistent with this, AR binding to the FN14 enhancer decreased expression. We show here that FN14 may be a survival factor in low AR output prostate cancer cells. Our results define one upstream mechanism, via FN14 signaling, through which the NFκB pathway contributes to prostate cancer metastasis and suggest FN14 as a candidate therapeutic and imaging target for castrate-resistant prostate cancers. Cancer Res; 74(16); 4306–17. ©2014 AACR.

Published

2023

12. Antitumor Effects of CAR T Cells Redirected to the EDB Splice Variant of Fibronectin

Author

Elizabeth Wickman, Alejandro Allo Anido, Giedre Krenciute, Timothy I. Shaw, Shaina N. Porter, Shondra M. Pruett-Miller, Stephen Gottschalk, Heather Tillman, Deanna Langfitt, Jessica Wagner, and Jinghui Zhang

Subjects

0301 basic medicine, Cancer Research, RNA Splicing, T-Lymphocytes, medicine.medical_treatment, Primary Cell Culture, Immunology, Cell, Biology, Immunotherapy, Adoptive, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, Antigen, Antigens, Neoplasm, In vivo, Cell Line, Tumor, Neoplasms, Human Umbilical Vein Endothelial Cells, medicine, Animals, Humans, Protein Isoforms, Receptors, Chimeric Antigen, Immunotherapy, Xenograft Model Antitumor Assays, Coculture Techniques, Healthy Volunteers, In vitro, Chimeric antigen receptor, Fibronectins, Neoplasm Proteins, 030104 developmental biology, medicine.anatomical_structure, Cell culture, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Feasibility Studies

Abstract

Chimeric antigen receptor (CAR) T-cell therapy has had limited success in early-phase clinical studies for solid tumors. Lack of efficacy is most likely multifactorial, including a limited array of targetable antigens. We reasoned that targeting the cancer-specific extra domain B (EDB) splice variant of fibronectin might overcome this limitation because it is abundantly secreted by cancer cells and adheres to their cell surface. In vitro, EDB-CAR T cells recognized and killed EDB-positive tumor cells. In vivo, 1 × 106 EDB-CAR T cells had potent antitumor activity in both subcutaneous and systemic tumor xenograft models, resulting in a significant survival advantage in comparison with control mice. EDB-CAR T cells also targeted the tumor vasculature, as judged by IHC and imaging, and their antivascular activity was dependent on the secretion of EDB by tumor cells. Thus, targeting tumor-specific splice variants such as EDB with CAR T cells is feasible and has the potential to improve the efficacy of CAR T-cell therapy.

Published

2021

13. A Murine Model Harboring Cooperating DNMT3A and SF3B1 Mutations Phenocopies SF3B1 Driven Myelodysplastic Syndrome

Author

Lashanale Wallace, Ana Leal-Cervantes, Amina Metidji, Jacquelyn Myers, Chandra Rolle, Heather Tillman, and Esther A. Obeng

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Published

2022

14. Impact of Immunoproteasome Inhibition in Preclinical Studies of Hemophagocytic Lymphohistiocytosis

Author

Camille Keenan, Sabrin Albeituni, Alexa Stroh, Heather Tillman, Janet Anderl, Christopher J. Kirk, and Kim E. Nichols

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Published

2022

15. Genome-wide mapping of oncogenic pathways and genetic modifiers of chemotherapy using a high-risk hepatoblastoma genetic model

Author

Jie Fang, Shivendra Singh, Sivaraman Natarajan, Heather Tillman, Ahmed Abuzaid, Adam Durbin, HaWon Lee, Qiong Wu, Jacob Steele, Jon Connelly, Changde Cheng, Hongjian Jin, Wenan Chen, Yiping Fan, Shondra Pruett-Miller, Jerold Rehg, Joseph Emmons, Stefano Cairo, Ruoning Wang, Evan Glazer, Andrew Murphy, Taosheng Chen, Andrew Davidoff, John Easton, Xiang Chen, and Jun Yang

Subjects

digestive system diseases

Abstract

A lack of relevant genetic models and cell lines hampers our understanding of hepatoblastoma pathogenesis and the development of new therapies for this neoplasm. We report a liver-specific MYC-driven hepatoblastoma murine model that faithfully recapitulates the pathological features of mixed fetal and embryonal hepatoblastoma, with transcriptomics resembling the high-risk gene signatures of the human disease. Single-cell RNA-sequencing and spatial transcriptomics identified distinct subpopulations of hepatoblastoma cells. After deriving cell lines from the mouse model, we mapped the cancer dependency genes using CRISPR-Cas9 screening and identified druggable targets shared with human hepatoblastoma (i.e., CDK7, CDK9, PRMT1, PRMT5). Our screen also revealed oncogenes and tumor suppressor genes in hepatoblastoma that engage multiple, druggable cancer signaling pathways. Chemotherapy is critical for human hepatoblastoma treatment. A genetic mapping of doxorubicin response by CRISPR-Cas9 screening identified modifiers whose loss-of-function synergizes with (e.g., PRKDC) or antagonizes (e.g., apoptosis genes) with the effect of chemotherapy. The combination of PRKDC inhibition and doxorubicin-based chemotherapy greatly enhances therapeutic efficacy. These studies have provided a useful set of resources including disease models suitable to identify and validate potential therapeutic targets in human high-risk hepatoblastoma.

Published

2022

16. A murine model of hnRNPH2-related neurodevelopmental disorder recapitulates clinical features of human disease and reveals a mechanism for genetic compensation ofHNRNPH2

Author

Ane Korff, Xiaojing Yang, Kevin O’Donovan, Abner Gonzalez, Brett J. W. Teubner, Haruko Nakamura, James Messing, Fen Yang, Alex Carisey, Yong-Dong Wang, Tushar Patni, Heather Tillman, Stanislav S. Zakharenko, Yuh Min Chook, J. Paul Taylor, and Hong Joo Kim

Abstract

Mutations inHNRNPH2cause an X-linked neurodevelopmental disorder with a phenotypic spectrum that includes developmental delay, intellectual disability, language impairment, motor function deficits, and seizures. More than 90% of patients with this disorder have a missense mutation within or adjacent to the nuclear localization signal (NLS) of hnRNPH2, although the specific pathogenic consequences of these mutations have not been examined. Here we found that hnRNPH2 NLS mutations result in reduced interaction with the nuclear transport receptor Kapβ2 in vitro and in cultured human cells. These mutations also cause modest accumulation of hnRNPH2 in the cytoplasm, suggesting that mislocalization of the protein might contribute to pathogenesis. We generated two knock-in mouse models with human-equivalent mutations in the endogenous mouse geneHnrnph2, as well asHnrnph2knockout (KO) mice, and subjected them to extensive phenotyping. Mutant knock-in mice displayed a spectrum of phenotypes that recapitulated aspects of the human disorder, including reduced survival in males, craniofacial abnormalities, impaired motor and cognitive functions, and increased susceptibility to audiogenic seizures. Mutant knock-in male mice developed more severe phenotypes than female mice, likely due to differences in X-chromosome gene dosage. In contrast, two independent lines ofHnrnph2KO mice showed no detectable phenotypes. Notably, KO mice had upregulated expression ofHnrnph1, a close paralog ofHnrnph2, whereas mutantHnrnph2knock-in mice failed to upregulateHnrnph1.Thus, genetic compensation byHnrnph1might be sufficient to counteract the loss of hnRNPH2. These findings suggest that the pathogenesis ofHNRNPH2-related disorder in humans may be driven by a toxic gain of function or a complex loss ofHNRNPH2function with impaired compensation byHNRNPH1.The mutant knock-in mice described here are an important resource for preclinical studies to assess the potential benefit of either gene replacement or therapeutic knockdown of mutant hnRNPH2.

Published

2022

17. JAK/STAT pathway inhibition sensitizes CD8 T cells to dexamethasone-induced apoptosis in hyperinflammation

Author

Heather Tillman, Brooks Scull, Katherine Verbist, Carl E. Allen, Lauren K. Meyer, Michelle L. Hermiston, Rachel Bassett, Alexa N. Stroh, Kim E. Nichols, and Sabrin Albeituni

Subjects

endocrine system, medicine.medical_treatment, T cell, Immunology, Drug Resistance, Apoptosis, CD8-Positive T-Lymphocytes, Lymphocytic Choriomeningitis, Biochemistry, Dexamethasone, Lymphohistiocytosis, Hemophagocytic, Mice, Immune system, hemic and lymphatic diseases, Nitriles, STAT5 Transcription Factor, Animals, Humans, Janus Kinase Inhibitors, Cytotoxic T cell, Medicine, Janus Kinases, Perforin, business.industry, JAK-STAT signaling pathway, Cell Biology, Hematology, medicine.disease, Specific Pathogen-Free Organisms, Mice, Inbred C57BL, Disease Models, Animal, Pyrimidines, Cytokine, medicine.anatomical_structure, Cancer research, Cytokines, Interleukin-2, Pyrazoles, Drug Therapy, Combination, Cytokine Release Syndrome, business, Janus kinase, Cytokine storm, hormones, hormone substitutes, and hormone antagonists, Signal Transduction

Abstract

Cytokine storm syndromes (CSS) are severe hyperinflammatory conditions characterized by excessive immune system activation leading to organ damage and death. Hemophagocytic lymphohistiocytosis (HLH), a disease often associated with inherited defects in cell-mediated cytotoxicity, serves as a prototypical CSS for which the 5-year survival is only 60%. Frontline therapy for HLH consists of the glucocorticoid dexamethasone (DEX) and the chemotherapeutic agent etoposide. Many patients, however, are refractory to this treatment or relapse after an initial response. Notably, many cytokines that are elevated in HLH activate the JAK/STAT pathway, and the JAK1/2 inhibitor ruxolitinib (RUX) has shown efficacy in murine HLH models and humans with refractory disease. We recently reported that cytokine-induced JAK/STAT signaling mediates DEX resistance in T cell acute lymphoblastic leukemia (T-ALL) cells, and that this could be effectively reversed by RUX. On the basis of these findings, we hypothesized that cytokine-mediated JAK/STAT signaling might similarly contribute to DEX resistance in HLH, and that RUX treatment would overcome this phenomenon. Using ex vivo assays, a murine model of HLH, and primary patient samples, we demonstrate that the hypercytokinemia of HLH reduces the apoptotic potential of CD8 T cells leading to relative DEX resistance. Upon exposure to RUX, this apoptotic potential is restored, thereby sensitizing CD8 T cells to DEX-induced apoptosis in vitro and significantly reducing tissue immunopathology and HLH disease manifestations in vivo. Our findings provide rationale for combining DEX and RUX to enhance the lymphotoxic effects of DEX and thus improve the outcomes for patients with HLH and related CSS.

Published

2020

18. IL-1β Promotes Expansion of IL-33

Author

Diego R. Hijano, Stephania A. Cormier, Heather Tillman, David Siefker, Anh T Q Phan, and Luan D. Vu

Subjects

Pulmonary and Respiratory Medicine, Clinical Biochemistry, Interleukin-1beta, Respiratory Syncytial Virus Infections, Virus, Mice, Disease severity, medicine, Animals, Humans, Respiratory system, Progenitor cell, Molecular Biology, Lung, Original Research, Mice, Inbred BALB C, business.industry, Stem Cells, Infant, Neonatal mouse, Cell Biology, Interleukin-33, Hospitalization, Interleukin 33, medicine.anatomical_structure, Respiratory Syncytial Virus, Human, Immunology, Stem cell, business

Abstract

Respiratory syncytial virus (RSV)-induced immunopathogenesis and disease severity in neonatal mice and human infants have been related to elevated pulmonary IL-33. Thus, targeting IL-33 has been suggested as a potential therapy for respiratory viral infections. Yet, the regulatory mechanisms on IL-33 during early life remain unclear. Here, using a neonatal mouse model of RSV, we demonstrate that IL-1β positively regulates but is not required for RSV-induced expression of pulmonary IL-33 in neonatal mice early after the initial infection. Exogenous IL-1β upregulates RSV-induced IL-33 expression by promoting the proliferation of IL-33(+) lung epithelial stem/progenitor cells. These cells are exclusively detected in RSV-infected neonatal rather than adult mice, partially explaining the IL-1β–independent IL-33 expression in RSV-infected adult mice. Furthermore, IL-1β aggravates IL-33–mediated T-helper cell type 2–biased immunopathogenesis upon reinfection. Collectively, our study demonstrates that IL-1β exacerbates IL-33–mediated RSV immunopathogenesis by promoting the proliferation of IL-33(+) epithelial stem/progenitor cells in early life.

Published

2021

19. Cell type identification in spatial transcriptomics data can be improved by leveraging cell-type-informative paired tissue images using a Bayesian probabilistic model

Author

Paul Geeleher, Heather Tillman, William C. Wright, John Easton, Richard H. Chapple, Hyeong-Min Lee, Sivaraman Natarajan, Asif Zubair, and Min Pan

Subjects

Cell type, Pathology, medicine.medical_specialty, Models, Statistical, Computer science, business.industry, Deep learning, Spatially resolved, Fluorescent Antibody Technique, Bayes Theorem, Transcriptome, Mice, Identification (information), Automatic image annotation, Genetics, medicine, Animals, Tissue cell, Artificial intelligence, business, Immune cell infiltration

Abstract

Spatial transcriptomics technologies have recently emerged as a powerful tool for measuring spatially resolved gene expression directly in tissues sections, revealing cell types and their dysfunction in unprecedented detail. However, spatial transcriptomics technologies are limited in their ability to separate transcriptionally similar cell types and can suffer further difficulties identifying cell types in slide regions where transcript capture is low. Here, we describe a conceptually novel methodology that can computationally integrate spatial transcriptomics data with cell-type-informative paired tissue images, obtained from, for example, the reverse side of the same tissue section, to improve inferences of tissue cell type composition in spatial transcriptomics data. The underlying statistical approach is generalizable to any spatial transcriptomics protocol where informative paired tissue images can be obtained. We demonstrate a use case leveraging cell-type-specific immunofluorescence markers obtained on mouse brain tissue sections and a use case for leveraging the output of AI annotated H&E tissue images, which we used to markedly improve the identification of clinically relevant immune cell infiltration in breast cancer tissue. Thus, combining spatial transcriptomics data with paired tissue images has the potential to improve the identification of cell types and hence to improve the applications of spatial transcriptomics that rely on accurate cell type identification.

Published

2021

20. The Myogenesis Program Drives Clonal Selection and Drug Resistance in Rhabdomyosarcoma

Author

Heather Tillman, Kaley Blankenship, Dominik Wodarz, Matthew J. Krasin, Michael A. Dyer, Natalia L. Komarova, Colleen Reilly, Xin Zhou, Alberto S. Pappo, Brent A. Orr, Jiyang Yu, Anand G. Patel, Jackie L. Norrie, Elizabeth Stewart, Xiang Chen, Clay Mr, Brittney Gordon, Justina McEvoy, Huang X, and Asa Karlstrom

Subjects

Population, Cell, Drug Resistance, Biology, Muscle Development, Article, General Biochemistry, Genetics and Molecular Biology, Rhabdomyosarcoma, medicine, Paraxial mesoderm, Humans, Myocyte, Rhabdomyosarcoma, Embryonal, Child, education, Molecular Biology, EGFR inhibitors, education.field_of_study, Myogenesis, Cell Biology, medicine.disease, Pediatric cancer, ErbB Receptors, medicine.anatomical_structure, Cancer research, Neoplasm Recurrence, Local, Developmental Biology

Abstract

Rhabdomyosarcoma (RMS) is a pediatric cancer with features of skeletal muscle; patients with unresectable or metastatic RMS fare poorly due to high rates of disease recurrence. Here, we use single cell and single nucleus RNA-sequencing to show that RMS tumors recapitulate the spectrum of embryonal myogenesis. Using matched patient samples from a clinical trial and orthotopic patient-derived xenografts (O-PDXs), we show chemotherapy eliminates the most proliferative component with features of myoblasts; after treatment, the quiescent immature population with features of paraxial mesoderm expands to reconstitute the developmental hierarchy of the original tumor. We discovered that this paraxial mesoderm population is dependent on EGFR signaling and is sensitive to EGFR inhibitors. Taken together, this data serves as a proof-of-concept that targeting each developmental state in RMS is an effective strategy for improving outcomes by preventing disease recurrence.

Published

2021

21. A Novel Orthotopic Implantation Technique for Osteosarcoma Produces Spontaneous Metastases and Illustrates Dose-Dependent Efficacy of B7-H3-CAR T Cells

Author

Christopher DeRenzo, Lindsay J. Talbot, Stephen Gottschalk, Amy J. Funk, Aaron Ross, Heather Tillman, Ashley Chabot, Jessica Wagner, Phuong Nguyen, and Andrew M. Davidoff

Subjects

0301 basic medicine, B7 Antigens, Lung Neoplasms, medicine.medical_treatment, Immunology, Dose dependence, Bone Neoplasms, Immunotherapy, Adoptive, 03 medical and health sciences, Mice, 0302 clinical medicine, Antigen, Cell Line, Tumor, medicine, Immunology and Allergy, Bioluminescence imaging, Animals, Humans, Luciferase, orthotopic, Original Research, Osteosarcoma, Lung, model, Receptors, Chimeric Antigen, Tibia, business.industry, Immunotherapy, RC581-607, medicine.disease, Xenograft Model Antitumor Assays, CAR, 030104 developmental biology, medicine.anatomical_structure, Treatment Outcome, B7-H3, 030220 oncology & carcinogenesis, T cell therapy, Cancer research, Female, Car t cells, Immunologic diseases. Allergy, business

Abstract

The outcome for metastatic pediatric osteosarcoma (OS) remains poor. Thus, there is an urgent need to develop novel therapies, and immunotherapy with CAR T cells has the potential to meet this challenge. However, there is a lack of preclinical models that mimic salient features of human disease including reliable development of metastatic disease post orthotopic OS cell injection. To overcome this roadblock, and also enable real-time imaging of metastatic disease, we took advantage of LM7 OS cells expressing firefly luciferase (LM7.ffLuc). LM7.ffLuc were implanted in a collagen mesh into the tibia of mice, and mice reliably developed orthotopic tumors and lung metastases as judged by bioluminescence imaging and histopathological analysis. Intratibial implantation also enabled surgical removal by lower leg amputation and monitoring for metastases development post-surgery. We then used this model to evaluate the antitumor activity of CAR T cells targeting B7-H3, an antigen that is expressed in a broad range of solid tumors including OS. B7-H3-CAR T cells had potent antitumor activity in a dose-dependent manner and inhibited the development of pulmonary metastases resulting in a significant survival advantage. In contrast T cells expressing an inactive B7-H3-CAR had no antitumor activity. Using unmodified LM7 cells also enabled us to demonstrate that B7-H3-CAR T cells traffic to orthotopic tumor sites. Hence, we have developed an orthotopic, spontaneously metastasizing OS model. This model may improve our ability not only to predict the safety and efficacy of current and next generation CAR T cell therapies but also other treatment modalities for metastatic OS.

Published

2021

22. 3220 – SF3B1/DNMT3A CO-MUTATION MIMICS FEATURES OF SOLE SF3B1 OR DNMT3A MUTATION DEPENDING ON STRESS CONDITIONS

Author

LaShanale Wallace, Ana Leal Cervantes, Amina Metidji, Jacquelyn Myers, Koral Campbell, Jordan Skorupa, Henry Fields, Chandra Rolle, Heather Tillman, and Esther Obeng

Subjects

Cancer Research, Genetics, Cell Biology, Hematology, Molecular Biology

Published

2022

23. 3112 – IMPACT OF IMMUNOPROTEASOME INHIBITION IN MOUSE MODEL OF HEMOPHAGOCYTIC LYMPHOHISTIOCYTOSIS

Author

Camille Keenan, Sabrin Albeituni, Alexa Stroh, Heather Tillman, Janet Anderl, Christopher Kirk, and Kim Nichols

Subjects

Cancer Research, Genetics, Cell Biology, Hematology, Molecular Biology

Published

2022

24. Morphologic and Immunohistochemical Characterization of Spontaneous Lymphoma/Leukemia in NSG Mice

Author

Jerold E. Rehg, Heather Tillman, Peter Vogel, Laura J. Janke, and Amy J. Funk

Subjects

Male, Lymphoma, CD3, Mice, SCID, Article, Immunophenotyping, Rodent Diseases, Mice, Mice, Inbred NOD, hemic and lymphatic diseases, Biomarkers, Tumor, medicine, Animals, Severe combined immunodeficiency, Leukemia, General Veterinary, biology, business.industry, Lymphoblastic lymphoma, medicine.disease, Immunohistochemistry, medicine.anatomical_structure, Cancer research, biology.protein, Female, Bone marrow, business, CD8

Abstract

The NOD.Cg- Prkdcscid Il2rgtm1Wjl/SzJ strain (NOD scid gamma, NSG) is a severely immunodeficient inbred laboratory mouse used for preclinical studies because it is amenable to engraftment with human cells. Combining scid and Il2rgnull mutations results in severe immunodeficiency by impairing the maturation, survival, and functionality of interleukin 2–dependent immune cells, including T, B, and natural killer lymphocytes. While NSG mice are reportedly resistant to developing spontaneous lymphomas/leukemias, there are reports of hematopoietic cancers developing. In this study, we characterized the immunophenotype of spontaneous lymphoma/leukemia in 12 NSG mice (20 to 38 weeks old). The mice had a combination of grossly enlarged thymus, spleen, or lymph nodes and variable histologic involvement of the bone marrow and other tissues. All 12 lymphomas were diffusely CD3, TDT, and CD4 positive, and 11 of 12 were also positive for CD8, which together was consistent with precursor T-cell lymphoblastic lymphoma/leukemia (pre-T-LBL). A subset of NSG tissues from all mice and neoplastic lymphocytes from 8 of 12 cases had strong immunoreactivity for retroviral p30 core protein, suggesting an association with a viral infection. These data highlight that NSG mice may develop T-cell lymphoma at low frequency, necessitating the recognition of this spontaneously arising disease when interpreting studies.

Published

2019

25. Positron Emission Tomography Detects In Vivo Expression of Disialoganglioside GD2 in Mouse Models of Primary and Metastatic Osteosarcoma

Author

Amy L. Vāvere, Scott E. Snyder, Armita Bahrami, Jitendra K. Mishra, Yuanyuan Han, Jason L. J. Dearling, Victor Amador Diaz, Alan B. Packard, Shana V. Stoddard, Heather Tillman, Jieun Kim, Elizabeth R. Butch, Paul E. Mead, Elizabeth Stewart, and Barry L. Shulkin

Subjects

musculoskeletal diseases, 0301 basic medicine, Cancer Research, medicine.diagnostic_test, Cell growth, business.industry, medicine.medical_treatment, Immunotherapy, medicine.disease, Target expression, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, In vivo, Apoptosis, Positron emission tomography, 030220 oncology & carcinogenesis, Metastatic osteosarcoma, medicine, Cancer research, Osteosarcoma, business, neoplasms

Abstract

The cell membrane glycolipid GD2 is expressed by multiple solid tumors, including 88% of osteosarcomas and 98% of neuroblastomas. However, osteosarcomas are highly heterogeneous, with many tumors exhibiting GD2 expression on 99%, P < 0.05). These results support the utility of GD2 imaging with PET to measure GD2 expression in osteosarcoma and thus maximize the clinical impact of anti-GD2 immunotherapy. Significance: In situ assessment of all GD2-positive osteosarcoma sites with a novel PET radiotracer could significantly impact anti-GD2 immunotherapy patient selection and enable noninvasive probing of correlations between target expression and therapeutic response.

Published

2019

26. Patrolling monocytes promote the pathogenesis of early lupus-like glomerulonephritis

Author

Peter Vogel, Cliff Guy, Heather Tillman, Patrick D. Walker, Hans Häcker, Jeeba Kuriakose, Sirish K. Ippagunta, Vanessa Redecke, Jingran Zhou, and Ruiqiong Wu

Subjects

0301 basic medicine, Inflammation, Monocytes, Pathogenesis, Mice, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine, Animals, Humans, Adaptor Proteins, Signal Transducing, Mice, Knockout, Autoimmune disease, Kidney, Systemic lupus erythematosus, business.industry, Toll-Like Receptors, Glomerulonephritis, General Medicine, medicine.disease, Lupus Nephritis, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Immunology, medicine.symptom, business, Kidney disease

Abstract

Systemic lupus erythematosus (SLE) is a complex autoimmune disease with genetic and environmental contributions. Hallmarks of the disease are the appearance of immune complexes (IC) containing autoreactive Abs and TLR-activating nucleic acids, whose deposition in kidney glomeruli is suspected to promote tissue injury and glomerulonephritis (GN). Here, using a mouse model based on the human SLE susceptibility locus TNFAIP3-interacting protein 1 (TNIP1, also known as ABIN1), we investigated the pathogenesis of GN. We found that GN was driven by TLRs but, remarkably, proceeded independently of ICs. Rather, disease in 3 different mouse models and patients with SLE was characterized by glomerular accumulation of patrolling monocytes (PMos), a cell type with an emerging key function in vascular inflammation. Consistent with such function in GN, monocyte-specific deletion of ABIN1 promoted kidney disease, whereas selective elimination of PMos provided protection. In contrast to GN, PMo elimination did not protect from reduced survival or disease symptoms such as IC generation and splenomegaly, suggesting that GN and other inflammatory processes are governed by distinct pathogenic mechanisms. These data identify TLR-activated PMos as the principal component of an intravascular process that contributes to glomerular inflammation and kidney injury.

Published

2019

27. Abstract 456: Jointly leveraging spatial transcriptomics and deep learning models for image annotation achieves better-than-pathologist performance in cell type identification in tumors

Author

Asif Zubair, Rich Chapple, Sivaraman Natarajan, William C. Wright, Min Pan, Hyeong-Min Lee, Heather Tillman, John Easton, and Paul Geeleher

Subjects

Cancer Research, Oncology

Abstract

For over 100 years, the traditional tools of pathology, such as tissue-marking dyes (e.g. the H&E stain) have been used to study the disorganization and dysfunction of cells within tissues. This has represented a principal diagnostic and prognostic tool in cancer. However, in the last 5 years, new technologies have promised to revolutionize histopathology, with Spatial Transcriptomics technologies allowing us to measure gene expression directly in pathology-stained tissue sections. In parallel with these developments, Artificial Intelligence (AI) applied to histopathology tissue images now approaches pathologist level performance in cell type identification. However, these new technologies still have severe limitations, with Spatial Transcriptomics suffering difficulties distinguishing transcriptionally similar cell types, and AI-based pathology tools often performing poorly on real world out-of-batch test datasets. Thus, century-old techniques still represent standard-of-care in most areas of clinical cancer diagnostics and prognostics. Here, we present a new frontier in digital pathology: describing a conceptually novel computational methodology, based on Bayesian probabilistic modelling, that allows Spatial Transcriptomics data to be leveraged together with the output of deep learning-based AI used to computationally annotate H&E-stained sections of the same tumor. By leveraging cell-type annotations from multiple independent pathologists, we show that this integrated methodology achieves better performance than any given pathologist’s manual tissue annotation in the task of identifying regions of immune cell infiltration in breast cancer, and easily outperforms either technology alone. We also show that on a subset of histopathology slides examined, the methodology can identify regions of clinically relevant immune cell infiltration that were missed entirely by an initial pathologist’s manual annotation. While this use case has clear diagnostic and prognostic value in cancer (e.g. predicting response to immunotherapy), our methodology is generalizable to any type of pathology images and also has broad applications in spatial transcriptomics data analytics, where most applications (such as identifying cell-cell interactions) rely on correct cell type annotations having been established a priori. We anticipate that this work will spur many follow-up studies, including new computational innovations building on the approach. The work sets the stage for better-than-pathologist performance in other cell-type annotation tasks, with relevant applications in diagnostics and prognostics across almost all cancers. Citation Format: Asif Zubair, Rich Chapple, Sivaraman Natarajan, William C. Wright, Min Pan, Hyeong-Min Lee, Heather Tillman, John Easton, Paul Geeleher. Jointly leveraging spatial transcriptomics and deep learning models for image annotation achieves better-than-pathologist performance in cell type identification in tumors [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2022; 2022 Apr 8-13. Philadelphia (PA): AACR; Cancer Res 2022;82(12_Suppl):Abstract nr 456.

Published

2022

28. 17-DMAG dually inhibits Hsp90 and histone lysine demethylases in alveolar rhabdomyosarcoma

Author

Ahmed Abu-Zaid, Sivaraja Vaithiyalingam, Brandon Young, Sourav Das, Heather Tillman, Bailey Cooke, Alireza Abdolvahabi, Julie Maier, Jonathan Low, Taosheng Chen, Jun J. Yang, Andrew M. Davidoff, Zhenmei Li, John J. Bowling, Hongjian Jin, Shivendra V. Singh, Jie Fang, Purva Bulsara, Wenwei Lin, Zoran Rankovic, Duane G. Currier, Andrew J. Murphy, Zhaohua Lu, Richard E. Lee, Anang A. Shelat, Dinesh M. Fernando, Qiong Wu, Stephen W. White, and Mi-Kyung Yun

Subjects

0301 basic medicine, Omics, 02 engineering and technology, medicine.disease_cause, Article, 03 medical and health sciences, chemistry.chemical_compound, medicine, Epigenetics, lcsh:Science, Gene, Molecular Biology, Demethylation, Cancer, Multidisciplinary, biology, Chemistry, Geldanamycin, 021001 nanoscience & nanotechnology, medicine.disease, Hsp90, 030104 developmental biology, Cancer research, Alveolar rhabdomyosarcoma, biology.protein, lcsh:Q, 0210 nano-technology, Carcinogenesis

Abstract

Summary Histone lysine demethylases (KDMs) play critical roles in oncogenesis and therefore may be effective targets for anticancer therapy. Using a time-resolved fluorescence resonance energy transfer demethylation screen assay, in combination with multiple orthogonal validation approaches, we identified geldanamycin and its analog 17-DMAG as KDM inhibitors. In addition, we found that these Hsp90 inhibitors increase degradation of the alveolar rhabdomyosarcoma (aRMS) driver oncoprotein PAX3-FOXO1 and induce the repressive epigenetic mark H3K9me3 and H3K36me3 at genomic loci of PAX3-FOXO1 targets. We found that as monotherapy 17-DMAG significantly inhibits expression of PAX3-FOXO1 target genes and multiple oncogenic pathways, induces a muscle differentiation signature, delays tumor growth and extends survival in aRMS xenograft mouse models. The combination of 17-DMAG with conventional chemotherapy significantly enhances therapeutic efficacy, indicating that targeting KDM in combination with chemotherapy may serve as a therapeutic approach to PAX3-FOXO1-positive aRMS., Graphical Abstract, Highlights • Identification of geldanamycin/17-DMAG as histone lysine demethylase inhibitors • Geldanamycin/17-DMAG causes degradation of PAX3-FOXO1, an Hsp90 client • Geldanamycin/17-DMAG induces epigenetic changes and targets PAX3-FOXO1 pathway • 17-DMAG alone or combined with chemotherapy show potency to PAX3-FOXO1 xenografts, Molecular Biology; Cancer; Omics

Published

2020

29. Development of mast cell and eosinophil hyperplasia and HLH/MAS-like disease in NSG-SGM3 mice receiving human CD34+ hematopoietic stem cells or patient-derived leukemia xenografts

Author

Zachary T. Freeman, Rosalinda A. Doty, Jerold E. Rehg, Mark J. Hoenerhoff, Portia S Allen, Natalie W. Fowlkes, Ilaria Iacobucci, Kirsten Dickerson, Jiajie J Xu, Charles G. Mullighan, Denise M. Imai, Heather Tillman, Peter Vogel, and Laura J. Janke

Subjects

CD34, Stem cell factor, Mice, SCID, Biology, Article, Lymphohistiocytosis, Hemophagocytic, Rodent Diseases, 03 medical and health sciences, Mice, 0302 clinical medicine, Mice, Inbred NOD, medicine, Animals, Humans, Mast Cells, 030304 developmental biology, Interleukin 3, 0303 health sciences, Hyperplasia, Leukemia, General Veterinary, Macrophage Activation Syndrome, Hematopoietic Stem Cell Transplantation, Eosinophil, medicine.disease, Mast cell, Hematopoietic Stem Cells, Eosinophils, Haematopoiesis, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Cancer research, Heterografts, Stem cell

Abstract

Immunocompromised mouse strains expressing human transgenes are being increasingly used in biomedical research. The genetic modifications in these mice cause various cellular responses, resulting in histologic features unique to each strain. The NSG-SGM3 mouse strain is similar to the commonly used NSG (NOD scid gamma) strain but expresses human transgenes encoding stem cell factor (also known as KIT ligand), granulocyte-macrophage colony-stimulating factor, and interleukin 3. This report describes 3 histopathologic features seen in these mice when they are unmanipulated or after transplantation with human CD34+ hematopoietic stem cells (HSCs), virally transduced hCD34+ HSCs, or a leukemia patient-derived xenograft. The first feature is mast cell hyperplasia: unmanipulated, naïve mice develop periductular pancreatic aggregates of murine mast cells, whereas mice given the aforementioned human cells develop a proliferative infiltrative interstitial pancreatic mast cell hyperplasia but with human mast cells. The second feature is the predisposition of NSG-SGM3 mice given these human cells to develop eosinophil hyperplasia. The third feature, secondary hemophagocytic lymphohistiocytosis/macrophage activation syndrome (HLH/MAS)–like disease, is the most pronounced in both its clinical and histopathologic presentations. As part of this disease, a small number of mice also have histiocytic infiltration of the brain and spinal cord with subsequent neurologic or vestibular signs. The presence of any of these features can confound accurate histopathologic interpretation; therefore, it is important to recognize them as strain characteristics and to differentiate them from what may be experimentally induced in the model being studied.

Published

2020

30. Loss of MAGEL2 in Prader-Willi syndrome leads to decreased secretory granule and neuropeptide production

Author

Patrick Ryan Potts, Li Ding, Heather Tillman, Derek J. C. Tai, Klementina Fon Tacer, Lisa Cole Burnett, Helen Chen, Michael E. Talkowski, John R. Yates, Daniel D. Billadeau, Yiying Zhang, Lawrence T. Reiter, James J. Moresco, Celine E. F. De Esch, Jolene K. Diedrich, A. Kaitlyn Victor, Jonathon Klein, Rudolph L. Leibel, Jamshid Temirov, Michael Rosenbaum, and Alexander Nuttle

Subjects

0301 basic medicine, Male, congenital, hereditary, and neonatal diseases and abnormalities, Proteome, Endosome, Cell, Neurodevelopment, Hypothalamus, Neuropeptide, Protein traffic, Biology, 03 medical and health sciences, Mice, 0302 clinical medicine, Antigens, Neoplasm, medicine, Gene family, Animals, Humans, Induced pluripotent stem cell, Mice, Knockout, Neurons, Secretory Vesicles, Neuropeptides, Proteins, General Medicine, Cell Biology, Phenotype, Cell biology, Mice, Inbred C57BL, Protein Transport, iPS cells, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Medicine, Female, Genomic imprinting, Prader-Willi Syndrome, Research Article, Neuroscience

Abstract

Prader-Willi syndrome (PWS) is a developmental disorder caused by loss of maternally imprinted genes on 15q11-q13, including melanoma antigen gene family member L2 (MAGEL2). The clinical phenotypes of PWS suggest impaired hypothalamic neuroendocrine function; however, the exact cellular defects are unknown. Here, we report deficits in secretory granule (SG) abundance and bioactive neuropeptide production upon loss of MAGEL2 in humans and mice. Unbiased proteomic analysis of Magel2pΔ/m+ mice revealed a reduction in components of SG in the hypothalamus that was confirmed in 2 PWS patient–derived neuronal cell models. Mechanistically, we show that proper endosomal trafficking by the MAGEL2-regulated WASH complex is required to prevent aberrant lysosomal degradation of SG proteins and reduction of mature SG abundance. Importantly, loss of MAGEL2 in mice, NGN2-induced neurons, and human patients led to reduced neuropeptide production. Thus, MAGEL2 plays an important role in hypothalamic neuroendocrine function, and cellular defects in this pathway may contribute to PWS disease etiology. Moreover, these findings suggest unanticipated approaches for therapeutic intervention., Prader-Willi Syndrome arises in part through loss of MAGEL2-regulated secretory granule biogenesis and neuropeptide production in the hypothalamus.

Published

2020

31. Endothelial cell α-globin and its molecular chaperone α-hemoglobin–stabilizing protein regulate arteriolar contractility

Author

Heather Tillman, Abdullah Freiwan, Mitchell J. Weiss, Laurent Kiger, Miranda E. Good, Christophe Lechauve, Joshua T. Butcher, Julia Keith, Lauren A Biwer, Brant E. Isakson, and Hans Ackerman

Subjects

0301 basic medicine, Vascular smooth muscle, Nitric Oxide Synthase Type III, Vasodilation, Nitric Oxide, Endothelial NOS, Mice, 03 medical and health sciences, alpha-Globins, Enos, hemic and lymphatic diseases, Cytochrome b5, medicine, Animals, Mice, Knockout, biology, Chemistry, Dioxygenase activity, Models, Cardiovascular, Endothelial Cells, General Medicine, biology.organism_classification, Cell biology, Endothelial stem cell, Arterioles, 030104 developmental biology, Commentary, medicine.symptom, Vasoconstriction, Molecular Chaperones, Muscle Contraction, Signal Transduction

Abstract

Arteriolar endothelial cell-expressed (EC-expressed) α-globin binds endothelial NOS (eNOS) and degrades its enzymatic product, NO, via dioxygenation, thereby lessening the vasodilatory effects of NO on nearby vascular smooth muscle. Although this reaction potentially affects vascular physiology, the mechanisms that regulate α-globin expression and dioxygenase activity in ECs are unknown. Without β-globin, α-globin is unstable and cytotoxic, particularly in its oxidized form, which is generated by dioxygenation and recycled via endogenous reductases. We show that the molecular chaperone α-hemoglobin-stabilizing protein (AHSP) promotes arteriolar α-globin expression in vivo and facilitates its reduction by eNOS. In Ahsp-/- mice, EC α-globin was decreased by 70%. Ahsp-/- and Hba1-/- mice exhibited similar evidence of increased vascular NO signaling, including arteriolar dilation, blunted α1-adrenergic vasoconstriction, and reduced blood pressure. Purified α-globin bound eNOS or AHSP, but not both together. In ECs in culture, eNOS or AHSP enhanced α-globin expression posttranscriptionally. However, only AHSP prevented oxidized α-globin precipitation in solution. Finally, eNOS reduced AHSP-bound α-globin approximately 6-fold faster than did the major erythrocyte hemoglobin reductases (cytochrome B5 reductase plus cytochrome B5). Our data support a model whereby redox-sensitive shuttling of EC α-globin between AHSP and eNOS regulates EC NO degradation and vascular tone.

Published

2018

32. Geldanamycin inhibits Jumonji histone lysine demethylase KDM4 and targets chimeric transcription factor PAX3-FOXO1

Author

Jonathan Low, Brandon Young, Jun J. Yang, John J. Bowling, Zoran Rankovic, Dinesh M. Fernando, Andrew M. Davidoff, Zhenmei Li, Bailey Cooke, Duane G. Currier, Stephen W. White, Jie Fang, Ahmed Abu-Zaid, Julie Maier, Heather Tillman, Zhaohua Lu, Sourav Das, Shivendra V. Singh, Taosheng Chen, Sivaraja Vaithiyalingam, Purva Bulsara, Wenwei Lin, Richard E. Lee, Alaa Altahan, Mi-Kyung Yun, and Alireza Abdolvahabi

Subjects

0303 health sciences, biology, Phenotypic screening, Geldanamycin, medicine.disease, Hsp90, 3. Good health, Bromodomain, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Histone, chemistry, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Alveolar rhabdomyosarcoma, medicine, Demethylase, Transcription factor, 030304 developmental biology

Abstract

Histone lysine demethylases (KDMs) are emerging as therapeutic targets in cancer. Development of potent KDM inhibitors may provide additional options for epigenomics-oriented therapies. Using a Time-Resolved Fluorescence Resonance Energy Transfer (TR-FRET) functional demethylation assay, in combination with a high-content immunofluorescence imaging phenotypic screen, Matrix-Assisted Laser Desorption/Ionization-Fourier Transform Ion Cyclotron Resonance mass spectrometry (MALDI-FTICR MS) and Amplified Luminescent Proximity Homogeneous Assay (ALPHA), we identified geldanamycin, an inhibitor of heat shock protein 90 (Hsp90), as a novel inhibitor of JmjC-domain containing demethylases such as KDM4B. We further found that geldanamycin can destabilize the PAX3-FOXO1 fusion oncoprotein, an Hsp90 client, which is a driver of clinically unfavorable alveolar rhabdomyosarcoma (aRMS). We then hypothesized that dual inhibition of PAX3-FOXO1 and epigenetic modifiers of aRMS would have synergistic antitumor activity. We repurposed the geldanamycin analog 17-DMAG to target aRMS and found that 17-DMAG significantly delays tumor growth, extends survival in xenograft mouse models, and inhibits expression of PAX3-FOXO1 targets and multiple oncogenic pathways including MYC, E2F and NOTCH. In addition, the combination of 17-DMAG with conventional chemotherapy or the bromodomain inhibitor JQ1 significantly enhances therapeutic efficacy. In summary, we have identified geldanamycin and 17-DMAG as dual KDM/Hsp90 inhibitors and 17-DMAG is efficacious against PAX3-FOXO1-driven rhabdomyosarcoma.

Published

2019

33. GSDMD is critical for autoinflammatory pathology in a mouse model of Familial Mediterranean Fever

Author

Hanne Van Gorp, Apurva Kanneganti, Hiroto Kambara, Heather Tillman, R. K. Subbarao Malireddi, Lieselotte Vande Walle, Hongbo R. Luo, Mohamed Lamkanfi, Pedro Henrique Viana Saavedra, Hongbo Chi, Peter Vogel, and Ramnik J. Xavier

Subjects

0301 basic medicine, PYROPTOTIC CELL-DEATH, Neutrophils, Interleukin-1beta, Familial Mediterranean fever, Disease, PYRIN INFLAMMASOME ACTIVATION, Pyrin domain, Mice, 0302 clinical medicine, Medicine and Health Sciences, Immunology and Allergy, Research Articles, Intracellular Signaling Peptides and Proteins, Pyroptosis, Inflammasome, MEFV, Familial Mediterranean Fever, 3. Good health, DISEASES, 030220 oncology & carcinogenesis, SECRETION, Cytokines, CASPASE-11, Inflammation Mediators, medicine.symptom, medicine.drug, Immunology, Caspase-11, 03 medical and health sciences, medicine, Animals, RELEASE, Inflammation, Clostridioides difficile, Wasting Syndrome, business.industry, Macrophages, Brief Definitive Report, Biology and Life Sciences, Phosphate-Binding Proteins, Pyrin, medicine.disease, Neutrophilia, GASDERMIN D, Disease Models, Animal, IL-1-BETA, 030104 developmental biology, INTERLEUKIN-1-BETA, Apoptosis Regulatory Proteins, business, Spleen

Abstract

Inflammasomes promote interleukin (IL)-1β secretion and pyroptosis. Kanneganti et al. now show that the pyroptosis effector gasdermin D (GSDMD) is required for systemic IL-1β secretion and autoinflammatory pathology in a mouse model of Familial Mediterranean Fever (FMF), suggesting GSDMD inhibitors as potential antiinflammatory treatments., Pyroptosis is an inflammasome-induced lytic cell death mode, the physiological role of which in chronic inflammatory diseases is unknown. Familial Mediterranean Fever (FMF) is the most common monogenic autoinflammatory disease worldwide, affecting an estimated 150,000 patients. The disease is caused by missense mutations in Mefv that activate the Pyrin inflammasome, but the pathophysiologic mechanisms driving autoinflammation in FMF are incompletely understood. Here, we show that Clostridium difficile infection of FMF knock-in macrophages that express a chimeric FMF-associated MefvV726A Pyrin elicited pyroptosis and gasdermin D (GSDMD)–mediated interleukin (IL)-1β secretion. Importantly, in vivo GSDMD deletion abolished spontaneous autoinflammatory disease. GSDMD-deficient FMF knock-in mice were fully protected from the runted growth, anemia, systemic inflammatory cytokine production, neutrophilia, and tissue damage that characterize this autoinflammatory disease model. Overall, this work identifies pyroptosis as a critical mechanism of IL-1β–dependent autoinflammation in FMF and highlights GSDMD inhibition as a potential antiinflammatory strategy in inflammasome-driven diseases.

Published

2018

34. Platelets Promote Metastasis via Binding Tumor CD97 Leading to Bidirectional Signaling that Coordinates Transendothelial Migration

Author

Adam G. Sowalsky, Kathleen Kelly, Philip Martin, Juan Juan Yin, Joshua M. Lang, Heather Tillman, Farhoud Faraji, Ross Lake, Kent W. Hunter, Cameron Gilliard, Tamara S. Rodems, Yvona Ward, David W. Niles, Jamie M. Sperger, and Kimberly P. Ku

Subjects

Blood Platelets, 0301 basic medicine, Epithelial-Mesenchymal Transition, Vascular permeability, Article, General Biochemistry, Genetics and Molecular Biology, Receptors, G-Protein-Coupled, Tight Junctions, Metastasis, 03 medical and health sciences, chemistry.chemical_compound, Circulating tumor cell, Antigens, CD, Cell Movement, Transforming Growth Factor beta, Cell Line, Tumor, Lysophosphatidic acid, Cell Adhesion, medicine, Humans, Secretion, Platelet, Platelet activation, RNA, Small Interfering, Receptors, Lysophosphatidic Acid, lcsh:QH301-705.5, Epidermal Growth Factor, Platelet Activation, medicine.disease, Tumor antigen, 030104 developmental biology, lcsh:Biology (General), chemistry, Cancer research, RNA Interference, Lysophospholipids, Colorectal Neoplasms, Dimerization, Signal Transduction

Abstract

Summary: Tumor cells initiate platelet activation leading to the secretion of bioactive molecules, which promote metastasis. Platelet receptors on tumors have not been well-characterized, resulting in a critical gap in knowledge concerning platelet-promoted metastasis. We identify a direct interaction between platelets and tumor CD97 that stimulates rapid bidirectional signaling. CD97, an adhesion G protein-coupled receptor (GPCR), is an overexpressed tumor antigen in several cancer types. Purified CD97 extracellular domain or tumor cell-associated CD97 stimulated platelet activation. CD97-initiated platelet activation led to granule secretion, including the release of ATP, a mediator of endothelial junction disruption. Lysophosphatidic acid (LPA) derived from platelets induced tumor invasiveness via proximal CD97-LPAR heterodimer signaling, coupling coincident tumor cell migration and vascular permeability to promote transendothelial migration. Consistent with this, CD97 was necessary for tumor cell-induced vascular permeability in vivo and metastasis formation in preclinical models. These findings support targeted blockade of tumor CD97 as an approach to ameliorate metastatic spread. : Tumor-initiated platelet activation promotes tissue invasion of cancer cells and metastasis. Ward et al. demonstrate that a common tumor-associated antigen, CD97, accounts for platelet activation and participates directly in LPA-mediated signal transduction leading to tumor cell invasion. CD97 promotes vascular extravasation and metastasis in pre-clinical models. Keywords: platelets, metastasis, transendothelial migration, circulating tumor cells, CD97, adhesion GPCR, LPA

Published

2018

35. Selective modulation of the androgen receptor AF2 domain rescues degeneration in spinal bulbar muscular atrophy

Author

Baochang Fan, Yimei Li, Brett J. Winborn, J. Paul Taylor, Emmanuelle R. Quemin, Jennifer Moore, Rebecca B. Smith, Helen C. Miranda, Burgess B. Freeman, Jennifer Dearman, Ane Korff, Hong Joo Kim, Pradeep K. Vuppala, Heather Tillman, James Messing, Brian D. Freibaum, Ping-Chung Chen, Albert R. La Spada, Nam Chul Kim, Anderson P. Kanagaraj, Bryce L. Sopher, Yingzhe Wang, and Nisha M. Badders

Subjects

0301 basic medicine, medicine.medical_specialty, Testicular atrophy, business.industry, General Medicine, Motor neuron, medicine.disease, Spinal cord, General Biochemistry, Genetics and Molecular Biology, Neuromuscular junction, 3. Good health, Androgen receptor, Pathogenesis, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Atrophy, Endocrinology, Internal medicine, medicine, business, Receptor, 030217 neurology & neurosurgery

Abstract

Spinal bulbar muscular atrophy (SBMA) is a motor neuron disease caused by toxic gain of function of the androgen receptor (AR). Previously, we found that co-regulator binding through the activation function-2 (AF2) domain of AR is essential for pathogenesis, suggesting that AF2 may be a potential drug target for selective modulation of toxic AR activity. We screened previously identified AF2 modulators for their ability to rescue toxicity in a Drosophila model of SBMA. We identified two compounds, tolfenamic acid (TA) and 1-[2-(4-methylphenoxy)ethyl]-2-[(2-phenoxyethyl)sulfanyl]-1H-benzimidazole (MEPB), as top candidates for rescuing lethality, locomotor function and neuromuscular junction defects in SBMA flies. Pharmacokinetic analyses in mice revealed a more favorable bioavailability and tissue retention of MEPB compared with TA in muscle, brain and spinal cord. In a preclinical trial in a new mouse model of SBMA, MEPB treatment yielded a dose-dependent rescue from loss of body weight, rotarod activity and grip strength. In addition, MEPB ameliorated neuronal loss, neurogenic atrophy and testicular atrophy, validating AF2 modulation as a potent androgen-sparing strategy for SBMA therapy.

Published

2018

36. Sexually dimorphic tumor suppression by small mitochondrial Arf

Author

Heather Tillman, Charles J. Sherr, and Jolieke G. van Oosterwijk

Subjects

0301 basic medicine, Messenger RNA, biology, smArf sexual dimorphism, small mitochondrial Arf (smArf), Cell biology, law.invention, Sexual dimorphism, 03 medical and health sciences, Priority Research Perspective, Arf tumor suppressor, 030104 developmental biology, 0302 clinical medicine, Oncology, law, 030220 oncology & carcinogenesis, biology.protein, Mdm2, Suppressor, Amino acid residue

Abstract

Internal translational initiation of the mRNA encoding the Arf tumor suppressor yields an N-terminally truncated small Arf protein (smArf) that lacks amino acid residues required for Mdm2 binding and p53 activation. Here, we report that female, but not male, mice engineered to produce only smArf in lieu of the full-length Arf protein retain residual, sexually dimorphic tumor suppressive activity.

Published

2019

37. 3025 – GPRASPS SUPPRESSION PROMOTES B-CELL LYMPHOMAGENESIS BY STALLING NORMAL B-CELL MATURATION

Author

Antonio Morales-Hernández, Emilia Kooienga, Heather Tillman, Claire Caprio, Ashley Chabot, Laura Pasqualucci, and Shannon McKinney-Freeman

Subjects

Cancer Research, Genetics, Cell Biology, Hematology, Molecular Biology

Published

2021

38. A Cancer-Specific Ubiquitin Ligase Drives mRNA Alternative Polyadenylation by Ubiquitinating the mRNA 3' End Processing Complex

Author

Kiran Kodali, Klementina Fon Tacer, Heather Tillman, Wei Li, Jung Mi Park, Junmin Peng, Haiyun Gan, Shaina N. Porter, Jon P. Connelly, Shondra M. Pruett-Miller, Lei Li, Patrick Ryan Potts, and Seung Wook Yang

Subjects

Untranslated region, Male, Lung Neoplasms, Polyadenylation, Carcinogenesis, Apoptosis, Mice, SCID, medicine.disease_cause, Mice, 0302 clinical medicine, Ubiquitin, Mice, Inbred NOD, Tumor Cells, Cultured, 3' Untranslated Regions, Ovarian Neoplasms, 0303 health sciences, Cleavage And Polyadenylation Specificity Factor, Ubiquitin ligase, Cell biology, Neoplasm Proteins, Gene Expression Regulation, Neoplastic, Carcinoma, Squamous Cell, Female, RNA Splicing, Ubiquitin-Protein Ligases, Biology, 03 medical and health sciences, Cyclin D2, Antigens, Neoplasm, medicine, Biomarkers, Tumor, PTEN, Animals, Humans, RNA, Messenger, Molecular Biology, 030304 developmental biology, Cell Proliferation, mRNA Cleavage and Polyadenylation Factors, Tumor Suppressor Proteins, Ubiquitination, Cancer, Cell Biology, medicine.disease, Xenograft Model Antitumor Assays, biology.protein, 030217 neurology & neurosurgery

Abstract

Summary Alternative polyadenylation (APA) contributes to transcriptome complexity by generating mRNA isoforms with varying 3′ UTR lengths. APA leading to 3′ UTR shortening (3′ US) is a common feature of most cancer cells; however, the molecular mechanisms are not understood. Here, we describe a widespread mechanism promoting 3′ US in cancer through ubiquitination of the mRNA 3′ end processing complex protein, PCF11, by the cancer-specific MAGE-A11–HUWE1 ubiquitin ligase. MAGE-A11 is normally expressed only in the male germline but is frequently re-activated in cancers. MAGE-A11 is necessary for cancer cell viability and is sufficient to drive tumorigenesis. Screening for targets of MAGE-A11 revealed that it ubiquitinates PCF11, resulting in loss of CFIm25 from the mRNA 3′ end processing complex. This leads to APA of many transcripts affecting core oncogenic and tumor suppressors, including cyclin D2 and PTEN. These findings provide insights into the molecular mechanisms driving APA in cancer and suggest therapeutic strategies.

Published

2019

39. The autophagy-activating kinase ULK1 mediates clearance of free α-globin in β-thalassemia

Author

Jingjing Zhang, Stephanie Fowler, Christophe Lechauve, Mondira Kundu, Heather Tillman, Abdullah Freiwan, Irene Motta, Paola Delbini, Eugene Khandros, Kalin Mayberry, M. Domenica Cappellini, Christopher S. Thom, Mitchell J. Weiss, Emilio Boada Romero, and Julia Keith

Subjects

Reticulocytes, ATG5, Antigens, CD34, mTORC1, Article, Autophagy-Related Protein 5, Mice, alpha-Globins, hemic and lymphatic diseases, Autophagy, medicine, Animals, Autophagy-Related Protein-1 Homolog, Humans, Sirolimus, Kinase, Chemistry, beta-Thalassemia, General Medicine, ULK1, Hematopoietic Stem Cells, Phenotype, Hematopoiesis, Cell biology, Enzyme Activation, Red blood cell, medicine.anatomical_structure, Disease Progression, Lysosomes, Gene Deletion, Intracellular

Abstract

In β-thalassemia, accumulated free α-globin forms intracellular precipitates that impair erythroid cell maturation and viability. Protein quality control systems mitigate β-thalassemia pathophysiology by degrading toxic free α-globin, although the associated mechanisms are poorly understood. We show that loss of the autophagy-activating Unc-51–like kinase 1 (Ulk1) gene in β-thalassemic mice reduces autophagic clearance of α-globin in red blood cell precursors and exacerbates disease phenotypes, whereas inactivation of the canonical autophagy-related 5 (Atg5) gene has relatively minor effects. Systemic treatment with the mTORC1 inhibitor rapamycin reduces α-globin precipitates and lessens pathologies in β-thalassemic mice via an ULK1-dependent pathway. Similarly, rapamycin reduces free α-globin accumulation in erythroblasts derived from CD34(+) cells of β-thalassemic individuals. Our findings define a drug-regulatable pathway for ameliorating β-thalassemia.

Published

2019

40. MYC competes with MiT/TFE in regulating lysosomal biogenesis and autophagy through an epigenetic rheostat

Author

Heather Tillman, Geoffrey Neale, Yvan Campos, Eda Machado, Martine F. Roussel, Rosario Mosca, Leigh E. Fremuth, Elmar Wolf, Gerard Grosveld, Ida Annunziata, Diantha van de Vlekkert, David Finkelstein, Alessandra d'Azzo, Xiaohui Qiu, Min-Joon Han, and Jason A. Weesner

Subjects

0301 basic medicine, Transcription, Genetic, General Physics and Astronomy, Histone Deacetylase 2, 02 engineering and technology, Epigenesis, Genetic, Induced pluripotent stem cell, lcsh:Science, Promoter Regions, Genetic, Polytetrafluoroethylene, Cancer, Regulation of gene expression, Multidisciplinary, Organelle Biogenesis, biology, Chemistry, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors, Stem Cells, Forkhead Transcription Factors, 021001 nanoscience & nanotechnology, Cancer metabolism, 3. Good health, Cell biology, Gene Expression Regulation, Neoplastic, Histone, Mechanisms of disease, Colonic Neoplasms, 0210 nano-technology, Science, General Biochemistry, Genetics and Molecular Biology, Article, Histone Deacetylases, Proto-Oncogene Proteins c-myc, 03 medical and health sciences, Cell Line, Tumor, Autophagy, Humans, Epigenetics, Transcription factor, Binding Sites, General Chemistry, 030104 developmental biology, biology.protein, TFEB, lcsh:Q, Organelle biogenesis, Lysosomes

Abstract

Coordinated regulation of the lysosomal and autophagic systems ensures basal catabolism and normal cell physiology, and failure of either system causes disease. Here we describe an epigenetic rheostat orchestrated by c-MYC and histone deacetylases that inhibits lysosomal and autophagic biogenesis by concomitantly repressing the expression of the transcription factors MiT/TFE and FOXH1, and that of lysosomal and autophagy genes. Inhibition of histone deacetylases abates c-MYC binding to the promoters of lysosomal and autophagy genes, granting promoter occupancy to the MiT/TFE members, TFEB and TFE3, and/or the autophagy regulator FOXH1. In pluripotent stem cells and cancer, suppression of lysosomal and autophagic function is directly downstream of c-MYC overexpression and may represent a hallmark of malignant transformation. We propose that, by determining the fate of these catabolic systems, this hierarchical switch regulates the adaptive response of cells to pathological and physiological cues that could be exploited therapeutically., Genes related to lysosomal and autophagic systems are transcriptionally regulated by the Mit/TFE family of transcription factors. Here the authors show that MYC, in association with HDACs, suppresses the expression of lysosomal and autophagy genes by competing with the Mit/TFE transcription factors for occupancy of their target gene promoters.

Published

2019

41. Deep multiomics profiling of brain tumors identifies signaling networks downstream of cancer driver genes

Author

Junmin Peng, Xusheng Wang, Chunliang Li, Bing Bai, Yang Zhang, Suiping Zhou, Haiyan Tan, Jeffrey M. Sifford, Ji-Hoon Cho, Mingming Niu, Yuxin Li, Anthony A. High, Suzanne J. Baker, Hong Wang, Vishwajeeth Pagala, Suresh Thiagarajan, Alexander K. Diaz, Laura D. Hover, Zhiping Wu, Barbara S. Paugh, Abbas Shirinifard, Andras Sablauer, Heather Tillman, and Timothy I. Shaw

Subjects

0301 basic medicine, Phosphopeptides, Proteomics, Cellular signalling networks, Receptor, Platelet-Derived Growth Factor alpha, Systems biology, Science, Oncogene Protein p65(gag-jun), General Physics and Astronomy, Proteomic analysis, 02 engineering and technology, PDGFRA, Computational biology, Biology, AMP-Activated Protein Kinases, General Biochemistry, Genetics and Molecular Biology, Receptor tyrosine kinase, Article, Transcriptome, Proto-Oncogene Proteins c-myc, 03 medical and health sciences, Mice, Animals, Receptor, trkA, lcsh:Science, Transcription factor, Feedback, Physiological, Multidisciplinary, Brain Neoplasms, Gene Expression Profiling, Systems Biology, General Chemistry, Oncogenes, Glioma, 021001 nanoscience & nanotechnology, Phosphoproteins, Up-Regulation, Gene expression profiling, Disease Models, Animal, 030104 developmental biology, Proteome, Mutation, biology.protein, lcsh:Q, 0210 nano-technology, Proto-Oncogene Proteins c-akt, Signal Transduction

Abstract

High throughput omics approaches provide an unprecedented opportunity for dissecting molecular mechanisms in cancer biology. Here we present deep profiling of whole proteome, phosphoproteome and transcriptome in two high-grade glioma (HGG) mouse models driven by mutated RTK oncogenes, PDGFRA and NTRK1, analyzing 13,860 proteins and 30,431 phosphosites by mass spectrometry. Systems biology approaches identify numerous master regulators, including 41 kinases and 23 transcription factors. Pathway activity computation and mouse survival indicate the NTRK1 mutation induces a higher activation of AKT downstream targets including MYC and JUN, drives a positive feedback loop to up-regulate multiple other RTKs, and confers higher oncogenic potency than the PDGFRA mutation. A mini-gRNA library CRISPR-Cas9 validation screening shows 56% of tested master regulators are important for the viability of NTRK-driven HGG cells, including TFs (Myc and Jun) and metabolic kinases (AMPKa1 and AMPKa2), confirming the validity of the multiomics integrative approaches, and providing novel tumor vulnerabilities., Multi-omic profiling is a powerful approach to dissecting molecular mechanisms in disease. Here the authors generate whole proteome, phosphoproteome and transcriptome profiles from two mouse models of high-grade glioma driven by different oncogenes, and validate identified master regulators with a CRISPR screen.

Published

2019

42. Mechanisms of action of ruxolitinib in murine models of hemophagocytic lymphohistiocytosis

Author

Katherine Verbist, Heather Tillman, Jennifer Picarsic, Sabrin Albeituni, Rachel Bassett, Kim E. Nichols, and Paige Tedrick

Subjects

0301 basic medicine, Ruxolitinib, Immunobiology and Immunotherapy, Neutrophils, T-Lymphocytes, medicine.medical_treatment, Immunology, Inflammation, Lymphocyte Activation, Lymphocytic choriomeningitis, Biochemistry, Lymphohistiocytosis, Hemophagocytic, Proinflammatory cytokine, 03 medical and health sciences, Mice, 0302 clinical medicine, Interferon, Nitriles, Medicine, Animals, Hemophagocytic lymphohistiocytosis, biology, business.industry, Cell Biology, Hematology, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Cytokine, Pyrimidines, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Pyrazoles, medicine.symptom, Antibody, business, medicine.drug

Abstract

Hemophagocytic lymphohistiocytosis (HLH) is an often-fatal disorder characterized by the overactivation of T cells and macrophages that excessively produce proinflammatory cytokines, including interferon-γ (IFN-γ). Previously, we reported that the JAK inhibitor ruxolitinib dampens T-cell activation and lessens inflammation in a model of HLH in which perforin-deficient (Prf1−/−) mice are infected with lymphocytic choriomeningitis virus (LCMV). Ruxolitinib inhibits signaling downstream of IFN-γ, as well as several other JAK-dependent cytokines. As a consequence, it remained unclear whether ruxolitinib was exerting its beneficial effects in HLH by inhibiting IFN-γ signaling or by targeting signaling initiated by other proinflammatory cytokines. To address this question, we compared the effects of ruxolitinib with those obtained using an IFN-γ–neutralizing antibody (αIFN-γ) in 2 murine HLH models. In both models, ruxolitinib and αIFN-γ reduced inflammation-associated anemia, indicating that ruxolitinib operates in an IFN-γ–dependent manner to reverse this HLH manifestation. In contrast, the number and activation status of T cells and neutrophils, as well as their infiltration into tissues, were significantly reduced following treatment with ruxolitinib, but they remained unchanged or were increased following treatment with αIFN-γ. Notably, despite discontinuation of ruxolitinib, LCMV-infected Prf1−/− mice exhibited enhanced survival compared with mice in which αIFN-γ was discontinued. This protective effect could be mimicked by transient treatment with αIFN-γ and a neutrophil-depleting antibody. Thus, ruxolitinib operates through IFN-γ–dependent and -independent mechanisms to dampen HLH by targeting the deleterious effects of T cells and neutrophils, with the latter representing an unappreciated and understudied cell type that contributes to HLH pathogenesis.

Published

2019

43. MAGE cancer-testis antigens protect the mammalian germline under environmental stress

Author

Jon P. Connelly, Marhiah C. Montoya, Heather Tillman, Min Soo Kim, Tessa Lord, Marcin Kamiński, Shondra M. Pruett-Miller, Ramya Ravichandran, Jon M. Oatley, Jonathon Klein, Emily Binshtock, Melissa J. Oatley, Klementina Fon Tacer, Angie L. Bookout, and Patrick Ryan Potts

Subjects

Male, endocrine system, Biology, Deoxyglucose, Germline, Evolution, Molecular, 03 medical and health sciences, 0302 clinical medicine, Stress, Physiological, Neoplasms, parasitic diseases, Testis, medicine, Animals, Humans, Spermatogenesis, neoplasms, Research Articles, 030304 developmental biology, Regulation of gene expression, Mice, Knockout, 0303 health sciences, Melanoma-associated antigen, Evolutionary Biology, Mice, Inbred BALB C, Multidisciplinary, Cancer, SciAdv r-articles, medicine.disease, Spermatogonia, 3. Good health, Cell biology, Gene Expression Regulation, Neoplastic, Mice, Inbred C57BL, Germ Cells, Starvation, 030220 oncology & carcinogenesis, Cancer cell, Knockout mouse, Cancer/testis antigens, Female, Stem cell, Melanoma-Specific Antigens, Research Article, DNA Damage

Abstract

Mammals evolved testis-specific Mage-a genes to protect the male germline under starvation stress and are co-opted in cancer., Ensuring robust gamete production even in the face of environmental stress is of utmost importance for species survival, especially in mammals that have low reproductive rates. Here, we describe a family of genes called melanoma antigens (MAGEs) that evolved in eutherian mammals and are normally restricted to expression in the testis (http://MAGE.stjude.org) but are often aberrantly activated in cancer. Depletion of Mage-a genes disrupts spermatogonial stem cell maintenance and impairs repopulation efficiency in vivo. Exposure of Mage-a knockout mice to genotoxic stress or long-term starvation that mimics famine in nature causes defects in spermatogenesis, decreased testis weights, diminished sperm production, and reduced fertility. Last, human MAGE-As are activated in many cancers where they promote fuel switching and growth of cells. These results suggest that mammalian-specific MAGE genes have evolved to protect the male germline against environmental stress, ensure reproductive success under non-optimal conditions, and are hijacked by cancer cells.

Published

2019

44. 3116 – GPRASP FAMILY MEMBERS AS NOVEL REGULATORS OF B-CELL DEVELOPMENT DURING NORMAL AND MALIGNANT HEMATOPOIESIS

Author

Antonio Morales-Hernandez, Heather Tillman, Ashley Chabot, Claire Caprio, Emilia Kooienga, and Shannon McKinney-Freeman

Subjects

Cancer Research, medicine.medical_treatment, Germinal center, Cell Biology, Hematology, Hematopoietic stem cell transplantation, Biology, CXCR4, Haematopoiesis, Immunophenotyping, medicine.anatomical_structure, Genetics, medicine, Cancer research, Bone marrow, Progenitor cell, Molecular Biology, B cell

Abstract

In our search for novel regulators of hematopoietic stem cell transplantation (HSCT), we recently reported Gprasp1 and Gprasp2 as negative regulators of HSCT. These genes encode proteins that are necessary for the stability, cellular trafficking and the proper degradation of CXCR4, a master regulator of hematopoiesis. Consequently, the absence of either Gprasp1 or Gprasp2 causes increased sensitivity to SDF-1 chemoattractant effect, enhancing HSCs repopulating activity after transplant. Strikingly, although Gprasp gene knockdown enhanced the repopulating activity of HSC at early time-points post-transplant, we observed that a significant number of mice transplanted with Gprasp-deficient hematopoietic progenitors developed an immature B-cell hematologic malignancy, typically at >20 weeks post-transplant. Since CXCR4 plays a crucial role in B-cell differentiation and, more specifically, in the movement of immature B-cells between the light and dark zones of the germinal center, we hypothesize that GPRASP family members are key regulators of CXCR4 during B-cell development during normal and malignant hematopoiesis. Thus, we followed mice transplanted with hematopoietic progenitors treated with control, Gprasp1 or Gprasp2-shRNAs for up to one year post-transplant. The onset of B-cell malignancy coincided with an accumulation of bone marrow common lymphoid progenitors, a complete disruption of the immunophenotype of B-cell progenitors and a loss of mature B-cells in the peripheral blood. Transformed cells invaded bone marrow, spleen, and lymph nodes in primary recipients. 100% of secondary recipients of leukemic cells developed a phenotypically identical malignancy

Published

2020

45. Unc 51–like autophagy-activating kinase (ULK1) mediates clearance of free α-globin in β-thalassemia

Author

Jingjing Zhang, Mondira Kundu, Julia Keith, Christopher S. Thom, Eugene Khandros, Kalin Mayberry, Paola Delbini, Christophe Lechauve, Heather Tillman, Emilio Boada Romero, Stephanie Fowler, M. Domenica Cappellini, Irene Motta, Mitchell J. Weiss, and Abdullah Freiwan

Subjects

0303 health sciences, Chemistry, Kinase, Autophagy, ATG5, mTORC1, ULK1, 3. Good health, Cell biology, 03 medical and health sciences, Haematopoiesis, 0302 clinical medicine, hemic and lymphatic diseases, 030220 oncology & carcinogenesis, Progenitor cell, Intracellular, 030304 developmental biology

Abstract

Erythroid maturation is coordinated to maximize the production of hemoglobin A heterotetramers (α2β2) and minimize the accumulation of potentially toxic free α- or β-globin subunits. In β-thalassemia, mutations in the β-globin gene cause a build-up of free α-globin, which forms intracellular precipitates that impair erythroid cell maturation and viability. Protein quality-control systems mitigate β-thalassemia pathophysiology by degrading toxic free α-globin. We show that loss of the Unc 51–like autophagy-activating kinase geneUlk1in β-thalassemic mice reduces autophagic clearance of α-globin in red cell precursors and exacerbates disease phenotypes, whereas inactivation of the canonical autophagy geneAtg5has minimal effects. Systemic treatment with rapamycin to inhibit the ULK1 inhibitor mTORC1 reduces α-globin precipitates and lessens pathologies in β-thalassemic mice, but not in those lackingUlk1. Similarly, rapamycin reduces free α-globin accumulation in erythroblasts derived from β-thalassemic patient CD34+hematopoietic progenitors. Our findings identify a new, drug-regulatable pathway for ameliorating β-thalassemia.One Sentence SummaryRapamycin alleviates β-thalassemia by stimulating ULK1-dependent autophagy of toxic free α-globin.

Published

2018

46. Positron Emission Tomography Detects

Author

Elizabeth R, Butch, Paul E, Mead, Victor, Amador Diaz, Heather, Tillman, Elizabeth, Stewart, Jitendra K, Mishra, Jieun, Kim, Armita, Bahrami, Jason L J, Dearling, Alan B, Packard, Shana V, Stoddard, Amy L, Vāvere, Yuanyuan, Han, Barry L, Shulkin, and Scott E, Snyder

Subjects

Osteosarcoma, Lung Neoplasms, Antibodies, Monoclonal, Mice, Nude, Apoptosis, Bone Neoplasms, Xenograft Model Antitumor Assays, Article, Mice, Gangliosides, Positron-Emission Tomography, Tumor Cells, Cultured, Animals, Humans, Immunotherapy, Neoplasm Recurrence, Local, Cell Proliferation

Abstract

The cell membrane glycolipid GD2 is expressed by multiple solid tumors, including 88% of osteosarcomas and 98% of neuroblastomas. However, osteosarcomas are highly heterogeneous with many tumors exhibiting GD2 expression on 99%, p

Published

2018

47. Frequent epigenetic alterations in polycomb repressive complex 2 in osteosarcoma cell lines

Author

Jun J. Yang, Helin Feng, Andrew M. Davidoff, Heather Tillman, and Gang Wu

Subjects

0301 basic medicine, biology, EZH2, Cancer, macromolecular substances, medicine.disease, 03 medical and health sciences, 030104 developmental biology, Oncology, Cell culture, Cancer research, biology.protein, medicine, Osteosarcoma, Epigenetics, PRC2, Functional genomics, Loss function

Abstract

Osteosarcoma (OS) cell lines are widely used in understanding the biological functions of cancer, identification and validation of therapeutic targets, as well as in vitro or in vivo preclinical drug screening. Here we report there is a frequent loss-of-function of polycomb repressive complex 2 (PRC2) in OS cell lines but it is rare in tumor samples based on genomic sequencing data, western blotting and immunohistochemistry analysis of H3K27me3. U2OS and 143B cell lines have a complete loss of function of PRC2 and several others have partial loss. In OS tumor tissues, only 1 out of 14 has low expression of H3K27me3. Kaplan-Meier analysis indicates that high EZH2, the component of PRC2, is associated with poor metastasis-free survival. Our observations are to raise the alarm that particular caution should be taken when using OS cell line models to study the disease, functional genomics, therapeutic target validation, drug screening, and epigenetic studies. Nevertheless, these cell lines will become useful biological tools to dissect the functions of PRC2.

Published

2018

48. ASSESSING THE IMPACT OF A B-ALL-ASSOCIATED GERMLINE ETV6 VARIANT ON MURINE HEMATOPOIESIS AND STEM CELL FUNCTION

Author

Rebekah Baskin-Doerfler, Katherine Verbist, Mackenzie Bloom, Kim E. Nichols, Chunliang Li, Heather Tillman, Gang Wu, Rachel Bassett, Ninad Oak, Wentao Yang, Paige Tedrick, Rina Nishii, and Jun J. Yang

Subjects

Cancer Research, medicine.diagnostic_test, Cell Biology, Hematology, Biology, Germline, Flow cytometry, Chromatin, Cell biology, ETV6, Haematopoiesis, medicine.anatomical_structure, Genetics, medicine, Bone marrow, Progenitor cell, Stem cell, Molecular Biology

Abstract

The transcription factor ETV6 is required for bone marrow (BM) hematopoiesis and survival of adult hematopoietic stem cells (HSCs), but the mechanisms by which ETV6 regulates these processes remain unclear. We and others reported that germline variants in ETV6 are associated with autosomal dominant thrombocytopenia and occurrence of B-ALL. We identified likely pathogenic variants in 0.8% of 4,405 childhood ALL cases, and functional evaluation of these variants revealed impairment of transcriptional repression activity of ETV6. To investigate the impact of ETV6 variants on hematopoiesis, we generated a CRISPR-Cas9-derived mouse model (Etv6R355X/+) that mirrors an ETV6 R359X variant observed in multiple ALL cases. Flow cytometry of the BM revealed progressive changes in stem and progenitor cells, with 12-month-old ETV6R355X/+ mice showing ∼40% reductions in HSPCs and ∼40% increases in pro-B cells. Lineage-negative, cKit+, Sca1+ (LSK) cells from 3-month-old ETV6R355X/+ mice showed impaired engraftment in a competitive transplant model, as demonstrated by significantly reduced chimerism in primary, secondary, and tertiary recipients. To determine how the ETV6 R355X variant influences the hematopoietic transcriptional landscape, we performed RNA-seq and ATAC-seq from LSK and pro-B cells of 3-month-old WT or Etv6R355X/+ mice. We found 90 and 125 differentially expressed genes in LSK and pro-B cells, respectively. GSEA revealed enrichment of genes associated with hypoxia response and stem cell maintenance. ATAC-seq revealed a preferential shift toward an increase in open chromatin in Etv6R355X/+ cells within regions highly enriched for ETS DNA consensus motifs, indicating a potential loss of ETV6-mediated repression. These findings demonstrate that a pathogenic ETV6 variant can disrupt normal hematopoiesis and alter the transcriptional profile of stem and progenitor cells.

Published

2019

49. Allogeneic<scp>CD</scp>27‐depleted cells in adoptive cell therapy

Author

Wing Leung, Heather Tillman, Ying Li, Barbara Rooney, Ardiana Moustaki, Robert E. Throm, Aimee C Talleur, and Jean-Yves Metais

Subjects

biology, business.industry, General Engineering, medicine.disease, CD19, Cell therapy, Leukemia, Antigen, Immunology, medicine, biology.protein, General Earth and Planetary Sciences, business, General Environmental Science, Lymphocyte subsets

Published

2019

50. Mitogen-activated protein kinase signaling causes malignant melanoma cells to differentially alter extracellular matrix biosynthesis to promote cell survival

Author

Kandice Tanner, Anna Afasizheva, King Leung Fung, Benjamin H. Blehm, Emily I. Chen, Heather Tillman, Wilfred D. Vieira, Yorihisa Kotobuki, Ben Busby, and Alexus Devine

Subjects

0301 basic medicine, MAPK/ERK pathway, Cancer Research, Cell Survival, Integrin, Cell, Antineoplastic Agents, Tenascin-C, Extracellular matrix, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Cell Line, Tumor, Tumor Microenvironment, Genetics, medicine, Animals, Humans, Neoplasm Metastasis, Melanoma, Protein Kinase Inhibitors, Fibronectin, Extracellular Matrix Proteins, Tumor microenvironment, biology, Dabrafenib, Tenascin, MAPK, Fibronectins, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Vemurafenib, Oncology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Mitogen-activated protein kinase, biology.protein, Cancer research, Heterografts, Female, Mitogen-Activated Protein Kinases, Signal transduction, Signal Transduction, Research Article

Abstract

Background Intrinsic and acquired resistance to drug therapies remains a challenge for malignant melanoma patients. Intratumoral heterogeneities within the tumor microenvironment contribute additional complexity to the determinants of drug efficacy and acquired resistance. Methods We use 3D biomimetic platforms to understand dynamics in extracellular matrix (ECM) biogenesis following pharmaceutical intervention against mitogen-activated protein kinases (MAPK) signaling. We further determined temporal evolution of secreted ECM components by isogenic melanoma cell clones. Results We found that the cell clones differentially secrete and assemble a myriad of ECM molecules into dense fibrillar and globular networks. We show that cells can modulate their ECM biosynthesis in response to external insults. Fibronectin (FN) is one of the key architectural components, modulating the efficacy of a broad spectrum of drug therapies. Stable cell lines engineered to secrete minimal levels of FN showed a concomitant increase in secretion of Tenascin-C and became sensitive to BRAFV600E and ERK inhibition as clonally- derived 3D tumor aggregates. These cells failed to assemble exogenous FN despite maintaining the integrin machinery to facilitate cell- ECM cross-talk. We determined that only clones that increased FN production via p38 MAPK and β1 integrin survived drug treatment. Conclusions These data suggest that tumor cells engineer drug resistance by altering their ECM biosynthesis. Therefore, drug treatment may induce ECM biosynthesis, contributing to de novo resistance. Electronic supplementary material The online version of this article (doi:10.1186/s12885-016-2211-7) contains supplementary material, which is available to authorized users.

Published

2016