Your search keyword '"Joanna H Maltbaek"' showing total 7 results

1. ABCC1 transporter exports the immunostimulatory cyclic dinucleotide cGAMP

Author

Joanna H. Maltbaek, Stephanie Cambier, Jessica M. Snyder, and Daniel B. Stetson

Subjects

Mice, Infectious Diseases, Adenosine Triphosphate, Immunology, Immunology and Allergy, Animals, Humans, Membrane Transport Proteins, DNA, Interferons, Multidrug Resistance-Associated Proteins, Nucleotides, Cyclic, Nucleotidyltransferases

Abstract

The DNA sensor cyclic GMP-AMP synthase (cGAS) is important for antiviral and anti-tumor immunity. cGAS generates cyclic GMP-AMP (cGAMP), a diffusible cyclic dinucleotide that activates the antiviral response through the adaptor protein stimulator of interferon genes (STING). cGAMP cannot passively cross cell membranes, but recent advances have established a role for extracellular cGAMP as an "immunotransmitter" that can be imported into cells. However, the mechanism by which cGAMP exits cells remains unknown. Here, we identifed ABCC1 as a direct, ATP-dependent cGAMP exporter in mouse and human cells. We show that ABCC1 overexpression enhanced cGAMP export and limited STING signaling and that loss of ABCC1 reduced cGAMP export and potentiated STING signaling. We demonstrate that ABCC1 deficiency exacerbated cGAS-dependent autoimmunity in the Trex1

Published

2022

2. The V654A second-site KIT mutation increases tumor oncogenesis and STAT activation in a mouse model of gastrointestinal stromal tumor

Author

Benjamin D. Medina, Jennifer K. Loo, Ferdinand Rossi, Joanna H. Maltbaek, Adrian M. Seifert, Peter Besmer, Cristina R. Antonescu, Shan Zeng, Jennifer Q. Zhang, Benedikt Bosbach, Nesteene J. Param, Ronald P. DeMatteo, and Gerardo A. Vitiello

Subjects

0301 basic medicine, Cancer Research, Carcinogenesis, Gastrointestinal Stromal Tumors, Kit mutation, Biology, medicine.disease_cause, Article, STAT activation, 03 medical and health sciences, symbols.namesake, Mice, 0302 clinical medicine, Genetics, medicine, Tumor Microenvironment, Animals, Humans, Stromal tumor, Molecular Biology, neoplasms, Gastrointestinal Neoplasms, GiST, Sunitinib, Imatinib, medicine.disease, digestive system diseases, Interstitial cell of Cajal, Disease Models, Animal, Proto-Oncogene Proteins c-kit, STAT Transcription Factors, 030104 developmental biology, 030220 oncology & carcinogenesis, Mutation (genetic algorithm), Mutation, Cancer research, symbols, imatinib resistance, Sarcoma, V654A, Gastrointestinal stromal tumor, medicine.drug, Signal Transduction

Abstract

Gastrointestinal stromal tumor (GIST) is the most common human sarcoma and arises in the gastrointestinal tract. Most GISTs are caused by activating mutations in the KIT receptor tyrosine kinase, such as the exon 11 KIT V559Δ mutation. The small molecule imatinib inhibits KIT and has been a mainstay of therapy in GIST. Unfortunately, imatinib-treated patients typically relapse, most often due to clonal emergence of the resistance-associated KIT V654A mutation. To determine the biologic impact of this second-site mutation in vivo, we created a mouse model with the corresponding V558Δ;V653A Kit double mutation restricted (a) spatially to ETV1+ cells, which include the interstitial cells of Cajal (ICCs) from which GISTs presumably originate, and (b) temporally through tamoxifen treatment after birth. This resulted in the first in vivo model of the most common second-site mutation associated with imatinib resistance in GIST and the first in vivo demonstration that cell-autonomous expression of mutant KIT in the ICC lineage leads to GIST. GISTs driven by the V558Δ;V653A Kit double mutation were resistant to imatinib, while cabozantinib was more effective in overcoming resistance than sunitinib. Compared to control mice with a single V558Δ Kit mutation, mice with a double V558Δ; V653A Kit mutation had increased tumor oncogenesis and associated KIT-dependent STAT activation. Our findings demonstrate that the biologic consequences of a second-site mutation in an oncogenic driver may include not only a mechanism for drug resistance, but changes in tumor oncogenic potential and differential activation of signaling pathways.

Published

2020

3. Human DNA-PK activates a STING-independent DNA sensing pathway

Author

Daniel B. Stetson, Richard C. James, Joanna H. Maltbaek, Richard Green, Michael Gale, Stephanie Cambier, and Katelyn Burleigh

Subjects

0301 basic medicine, DNA damage, Ubiquitin-Protein Ligases, Immunology, Viral Oncogene, DNA-Activated Protein Kinase, Herpesvirus 1, Human, Biology, medicine.disease_cause, Virus, Adenoviridae, Cell Line, Immediate-Early Proteins, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Heat shock protein, medicine, Animals, Humans, Kinase activity, Protein kinase A, HSPA8, 030304 developmental biology, 0303 health sciences, Innate immune system, Membrane Proteins, Herpes Simplex, General Medicine, 3. Good health, Cell biology, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, Phosphorylation, Adenovirus E1A Proteins, DNA

Abstract

Detection of intracellular DNA by the cGAS-STING pathway activates a type I interferon-mediated innate immune response that protects from virus infection. Whether there are additional DNA sensing pathways, and how such pathways might function, remains controversial. We show here that humans-but not laboratory mice-have a second, potent, STING-independent DNA sensing pathway (SIDSP). We identify human DNA-dependent protein kinase (DNA-PK) as the sensor of this pathway and demonstrate that DNA-PK activity drives a robust and broad antiviral response. We show that the E1A oncoprotein of human adenovirus 5 and the ICP0 protein of herpes simplex virus 1 block this response. We found heat shock protein HSPA8/HSC70 as a target for inducible phosphorylation in the DNA-PK antiviral pathway. Last, we demonstrate that DNA damage and detection of foreign DNA trigger distinct modalities of DNA-PK activity. These findings reveal the existence, sensor, a specific downstream target, and viral antagonists of a SIDSP in human cells.

Published

2019

4. Csf1r or Mer inhibition delays liver regeneration via suppression of Kupffer cells

Author

Jennifer K. Loo, Ronald P. DeMatteo, Megan H. Crawley, Jennifer Q. Zhang, Joanna H. Maltbaek, Juan A. Santamaria-Barria, Noah A. Cohen, Adrian M. Seifert, Shan Zeng, Jonathan B. Greer, Michael J. Beckman, and Benjamin L. Green

Subjects

0301 basic medicine, Physiology, medicine.medical_treatment, Pathology and Laboratory Medicine, Biochemistry, Receptor tyrosine kinase, Monocytes, Tyrosine Kinases, Mice, White Blood Cells, 0302 clinical medicine, Spectrum Analysis Techniques, Animal Cells, Immune Physiology, Medicine and Health Sciences, Receptors, Immunologic, Receptor, Immune Response, Liver injury, Innate Immune System, Multidisciplinary, medicine.diagnostic_test, biology, Chemistry, Liver cell, Flow Cytometry, Liver regeneration, Enzymes, Cytokine, Receptors, Granulocyte-Macrophage Colony-Stimulating Factor, Spectrophotometry, 030220 oncology & carcinogenesis, Medicine, Cytokines, Cytophotometry, Cellular Types, Cellular Structures and Organelles, Tyrosine kinase, Research Article, Kupffer Cells, Science, Immune Cells, Immunology, Research and Analysis Methods, Flow cytometry, 03 medical and health sciences, Signs and Symptoms, Diagnostic Medicine, medicine, Animals, Hepatectomy, Vesicles, Molecular Biology Techniques, Protein Kinase Inhibitors, Molecular Biology, Inflammation, Blood Cells, Macrophages, Receptor Protein-Tyrosine Kinases, Biology and Life Sciences, Proteins, Cell Biology, Molecular Development, medicine.disease, Molecular biology, Antigens, Differentiation, eye diseases, Liver Regeneration, Antigens, Differentiation, B-Lymphocyte, 030104 developmental biology, Immune System, Liposomes, biology.protein, Enzymology, Protein Kinases, Cloning, Developmental Biology

Abstract

IntroductionMurine Kupffer cells (KCs) comprise CD11bhi and F4/80hi subsets. Tissue-resident macrophages are known to express the tyrosine kinase receptors colony-stimulating factor 1 receptor (Csf1r) and Mer. However, the expression of Csf1r and Mer on KC subsets and the importance of these tyrosine kinases during liver regeneration (LR) are unknown.MethodsKCs from wild-type and Csf1r-GFP mice were characterized by flow cytometry. Partial hepatectomy (PH) was performed in mice treated with clodronate liposomes, a Csf1r small molecule inhibitor or depleting antibody, or a small molecule Mer inhibitor. Sera and livers were analyzed. The function of sorted KC subsets was tested in vitro.ResultsMer was specifically expressed on tissue-resident F4/80hi KCs, 55% of which also expressed Csf1r. Mer+Csf1r+ and Mer+Csf1r- KCs had distinct expression of macrophage markers. Csf1r inhibition in mice reduced F4/80hi KCs by approximately 50%, but did not affect CD11bhi KCs. Clodronate liposomes depleted F4/80hi KCs, but also altered levels of other intrahepatic leukocytes. Csf1r inhibition delayed LR, as demonstrated by a 20% reduction in liver-to-body weight ratios 7 days after PH. At 36h after PH, Csf1r inhibition increased serum ALT and histological liver injury, and decreased liver cell proliferation. A small molecule inhibitor of Mer did not alter the percentage of KCs or their proliferation and just modestly delayed LR. In vitro, Csf1r or Mer inhibition did not decrease KC viability, but did attenuate their cytokine response to stimulation.ConclusionsF4/80hi KCs are Mer+ and can be subdivided based on Csf1r expression. Csf1r or Mer inhibition each reduces KC cytokine production and delays LR.

Published

2019

5. Oncogenic kinase inhibition limits Batf3-dependent dendritic cell development and antitumor immunity

Author

Adrian M. Seifert, Timothy G. Bowler, Vinod P. Balachandran, Shan Zeng, Jennifer Q. Zhang, Jennifer K. Loo, Mengyuan Liu, Joanna H. Maltbaek, Gerardo A. Vitiello, Michael J. Cavnar, Benjamin D. Medina, Ferdinand Rossi, Ronald P. DeMatteo, and Nesteene J. Param

Subjects

Carcinogenesis, Gastrointestinal Stromal Tumors, T cell, Immunology, chemical and pharmacologic phenomena, CD8-Positive T-Lymphocytes, Proto-Oncogene Mas, Article, 03 medical and health sciences, 0302 clinical medicine, Antigens, CD, Monitoring, Immunologic, medicine, Immunology and Allergy, Animals, Progenitor cell, Protein Kinase Inhibitors, Research Articles, 030304 developmental biology, 0303 health sciences, Chemotactic Factors, Chemistry, Macrophages, Immunity, Granulocyte-Macrophage Colony-Stimulating Factor, Imatinib, hemic and immune systems, Cell Differentiation, Receptors, Antigen, T-Cell, gamma-delta, Dendritic cell, Dendritic Cells, Oncogenes, 3. Good health, Mice, Inbred C57BL, Repressor Proteins, Granulocyte macrophage colony-stimulating factor, Imatinib mesylate, medicine.anatomical_structure, Basic-Leucine Zipper Transcription Factors, 030220 oncology & carcinogenesis, Cancer research, Imatinib Mesylate, Tyrosine kinase, Immunologic Memory, CD8, medicine.drug

Abstract

Medina et al. demonstrate that Kit oncogene activity in gastrointestinal stromal tumor modulates the CD103+CD11b− dendritic cell (DC) lineage. The antitumor efficacy of oncogene inhibition initially depends on preexisting immunity orchestrated by CD103+CD11b− DCs, but subsequently is limited by a decrease in DC lineage maturation., Gastrointestinal stromal tumor (GIST) is driven by an activating mutation in the KIT proto-oncogene. Using a mouse model of GIST and human specimens, we show that intratumoral murine CD103+CD11b− dendritic cells (DCs) and human CD141+ DCs are associated with CD8+ T cell infiltration and differentiation. In mice, the antitumor effect of the Kit inhibitor imatinib is partially mediated by CD103+CD11b− DCs, and effector CD8+ T cells initially proliferate. However, in both mice and humans, chronic imatinib therapy decreases intratumoral DCs and effector CD8+ T cells. The mechanism in our mouse model depends on Kit inhibition, which reduces intratumoral GM-CSF, leading to the accumulation of Batf3-lineage DC progenitors. GM-CSF is produced by γδ T cells via macrophage IL-1β. Stimulants that expand and mature DCs during imatinib treatment improve antitumor immunity. Our findings identify the importance of tumor cell oncogene activity in modulating the Batf3-dependent DC lineage and reveal therapeutic limitations for combined checkpoint blockade and tyrosine kinase inhibition.

Published

2018

6. Macrophages and CD8

Author

Jennifer Q, Zhang, Shan, Zeng, Gerardo A, Vitiello, Adrian M, Seifert, Benjamin D, Medina, Michael J, Beckman, Jennifer K, Loo, Juan, Santamaria-Barria, Joanna H, Maltbaek, Nesteene J, Param, John A, Moral, Julia N, Zhao, Vinod, Balachandran, Ferdinand, Rossi, Cristina R, Antonescu, and Ronald P, DeMatteo

Subjects

Gastrointestinal Stromal Tumors, Macrophages, Gene Expression, Drug Synergism, CD8-Positive T-Lymphocytes, Xenograft Model Antitumor Assays, digestive system diseases, Monocytes, Article, Immunophenotyping, Tumor Burden, Chemotaxis, Leukocyte, Disease Models, Animal, Mice, Proto-Oncogene Proteins c-kit, Cell Line, Tumor, Imatinib Mesylate, Animals, Humans, Immunotherapy, CD40 Antigens, neoplasms, Protein Kinase Inhibitors, Biomarkers

Abstract

Tyrosine kinase inhibition of gastrointestinal stromal tumors (GIST) is effective but typically culminates in resistance and is rarely curative. Immunotherapy has potential application to GIST, as we previously showed that T-cell checkpoint blockade increases the antitumor effects of imatinib. Here, we showed that ligation of CD40 using an agonistic antibody (anti-CD40) activated tumor-associated macrophages (TAMs) in vivo in a knock-in mouse model of GIST harboring a germline mutation in Kit exon 11. Activated TAMs had greater TNF production and NFκB signaling and directly inhibited tumor cells in vitro. Anti-CD40 required concomitant therapy with imatinib for efficacy and depended on TAMs, and to a lesser extent CD8+ T cells, but not on CD4+ T cells or B cells. In an analysis of 50 human GIST specimens by flow cytometry, we found that CD40 was expressed on human TAMs and tumor cells yet was downregulated after response to imatinib. CD40 ligation did not have a direct inhibitory effect on human GIST cells. Our findings provide the rationale for combining anti-CD40 and tyrosine kinase inhibition to treat human GIST.

Published

2017

7. Wnt/β-catenin Signaling Contributes to Tumor Malignancy and Is Targetable in Gastrointestinal Stromal Tumor

Author

Jennifer Q. Zhang, Adrian M. Seifert, Megan H. Crawley, Juan A. Santamaria-Barria, Ferdinand Rossi, Vinod P. Balachandran, Noah A. Cohen, Ronald P. DeMatteo, Joanna H. Maltbaek, Cristina R. Antonescu, Peter Besmer, Benjamin D. Medina, Shan Zeng, Jennifer K. Loo, Michael J. Beckman, Michael J. Cavnar, and Teresa S. Kim

Subjects

0301 basic medicine, Cancer Research, Beta-catenin, Gastrointestinal Stromal Tumors, Ubiquitin-Protein Ligases, Antineoplastic Agents, Mice, Transgenic, 03 medical and health sciences, Mice, 0302 clinical medicine, Cell Line, Tumor, Wnt3A Protein, AXIN2, Animals, Humans, Molecular Targeted Therapy, Stromal tumor, neoplasms, Wnt Signaling Pathway, beta Catenin, Neoplasm Staging, biology, GiST, Wnt signaling pathway, LRP5, Xenograft Model Antitumor Assays, digestive system diseases, Disease Models, Animal, 030104 developmental biology, Imatinib mesylate, Oncology, 030220 oncology & carcinogenesis, Immunology, biology.protein, Cancer research, Imatinib Mesylate, Intercellular Signaling Peptides and Proteins, Neoplasm Grading

Abstract

Gastrointestinal stromal tumor (GIST) is the most common type of sarcoma and usually harbors either a KIT or PDGFRA mutation. However, the molecular basis for tumor malignancy is not well defined. Although the Wnt/β-catenin signaling pathway is important in a variety of cancers, its role in GIST is uncertain. Through analysis of nearly 150 human GIST specimens, we found that some human GISTs expressed β-catenin and contained active, dephosphorylated nuclear β-catenin. Furthermore, advanced human GISTs expressed reduced levels of the Wnt antagonist DKK4. Accordingly, in human GIST T1 cells, Wnt stimulation increased β-catenin–mediated transcriptional activity in a reporter assay as well as transcription of the downstream target genes Axin2 and CCND1. In contrast, DKK4 overexpression in GIST T1 cells reduced Wnt/β-catenin signaling. In addition, we showed that nuclear β-catenin stability was partially regulated by the E3 ligase COP1, as demonstrated with coimmunoprecipitation and COP1 knockdown. Three molecular inhibitors of the Wnt/β-catenin pathway demonstrated antitumor efficacy in various GIST models, both in vitro and in vivo. Notably, the tankyrase inhibitor G007-LK alone had substantial activity against tumors of genetically engineered KitV558Δ/+ mice, and the effect was increased by the addition of the Kit inhibitor imatinib mesylate. Collectively, our findings demonstrate that Wnt/β-catenin signaling is a novel therapeutic target for selected untreated or imatinib-resistant GISTs. Mol Cancer Ther; 16(9); 1954–66. ©2017 AACR.

Published

2017