Your search keyword '"Adam Goeken"' showing total 36 results

1. Keratoacanthoma Pathobiology in Mouse Models

Author

Katherine N. Gibson-Corley, Laura M. Rogers, Adam Goeken, Adam J. Dupuy, and David K. Meyerholz

Subjects

keratoacanthoma, mouse models, histopathology, regression, Medicine

Abstract

Recently we described skin tumors driven by skin-specific expression of Zmiz1 and here we define keratoacanthoma pathobiology in this mouse model. Similar to human keratoacanthoma development, we were able to segregate murine keratoacanthomas into three developmental phases: growth, maturation, and regression. These tumors had areas with cellular atypia, high mitotic rate, and minor local invasion in the growth phase, but with development they transitioned to maturation and regression phases with evidence of resolution. The early aggressive appearance could easily be misdiagnosed as a malignant change if the natural pathobiology was not well-defined in the model. To corroborate these findings in the Zmiz1 model, we examined squamous skin tumors from another tumor study in aging mice, and these tumors followed a similar biological progression. Lastly, we were able to evaluate the utility of the model to assess immune cell infiltration (F4/80, B220 Granzyme B, CD3 cells, arginase-1) in the regression phase; however, because inflammation was present at all phases of development, a more comprehensive approach will be needed in future investigations. Our study of keratoacanthomas in selected murine models suggests that these squamous tumors can appear histologically aggressive during early development, but with time will enter a regression phase indicating a benign biology. Importantly, studies of squamous skin tumor models should be cautious in tumor diagnosis as the early growth distinction between malignant versus benign based solely on histopathology may not be easily discerned without longitudinal studies to confirm the tumor pathobiology.

Published

2014

2. Immunohistochemical detection of MUC5AC and MUC5B mucins in ferrets

Author

Meyerholz, David K., Leidinger, Mariah R., Adam Goeken, J., Businga, Thomas R., Vizuett, Sebastian, Akers, Allison, Evans, Idil, Zhang, Yan, and Engelhardt, John F.

Published

2023

3. Immunohistochemical detection of MUC5AC and MUC5B mucins in ferrets

Author

David K. Meyerholz, Mariah R. Leidinger, J. Adam Goeken, Thomas R. Businga, Sebastian Vizuett, Allison Akers, Idil Evans, Yan Zhang, and John F. Engelhardt

Subjects

Cystic fibrosis, Ferret, Immunohistochemistry, Lung, Mucin, Mucus, Medicine, Biology (General), QH301-705.5, Science (General), Q1-390

Abstract

Abstract Objective Cystic fibrosis (CF) is a genetic condition that causes abnormal mucus secretions in affected organs. MUC5AC and MUC5B are gel-forming mucins and frequent targets for investigations in CF tissues. Our objective was to qualify MUC5AC and MUC5B immunohistochemical techniques to provide a useful tool to identify, localize and interpret mucin expression in ferret tissues. Results MUC5AC and MUC5B mucins were detected most commonly in large airways and least in small airways, consistent with reported goblet cell density in airway surface epithelia. We evaluated whether staining method affected the detection of goblet cell mucins in serial sections of bronchial surface epithelia. Significant differences between stains were not observed suggesting common co-expression MUC5AC and MUC5B proteins in goblet cells of airway surface epithelia. Gallbladder and stomach tissues are reported to have differential mucin enrichment, so we tested these tissues in wildtype ferrets. Stomach tissues were enriched in MUC5AC and gallbladder tissues enriched in MUC5B, mucin enrichment similar to human tissues. Mucin immunostaining techniques were further qualified for specificity using lung tissue from recently generated MUC5AC −/− and MUC5B −/− ferrets. Qualified techniques for MUC5AC and MUC5B immunohistochemistry will be useful tools for mucin tissue studies in CF and other ferret models.

Published

2023

4. Utility of CD138/syndecan-1 immunohistochemistry for localization of plasmacytes is tissue-dependent in B6 mice

Author

David K. Meyerholz, Mariah R. Leidinger, J. Adam Goeken, Thomas R. Businga, Allison Akers, Sebastian Vizuett, Courtney A. Kaemmer, Jordan L. Kohlmeyer, Rebecca D. Dodd, and Dawn E. Quelle

Subjects

B-cells, CD138/syndecan-1, Immunohistochemistry, Kappa light chain, Plasmacytes, Medicine, Biology (General), QH301-705.5, Science (General), Q1-390

Abstract

Abstract Objective Inflammation is present in many diseases and identification of immune cell infiltration is a common assessment. CD138 (syndecan-1) is a recommended immunohistochemical marker for human plasmacytes although it is also expressed in various epithelia and tumors. Similarly, CD138 is a marker for murine plasmacytes, but its tissue immunostaining is not well-defined. Endogenous CD138 expression is an important confounding factor when evaluating plasmacyte infiltration. We studied two plasmacyte markers (CD138 and Kappa light chains) for endogenous immunostaining in five organs and one tumor from B6 mice. Results Plasmacytes in Peyer’s patches were positive for CD138 and Kappa markers without endogenous immunostaining. Endogenous CD138 immunostaining was widespread in liver, kidney, lung and a malignant peripheral nerve sheath tumor (MPNST) versus regionalized immunostaining in skin and small intestine wall. Endogenous Kappa immunostaining was absent in all tissues except for plasmacytes. Tissues with widespread endogenous CD138 immunostaining were contrasted by absence of endogenous Kappa immunostaining. Here, plasmacytes would not be distinguished by CD138, but would be obvious by Kappa immunostaining. Our study suggests that utility of immunostaining for plasmacytes by CD138 is tissue dependent in mice. Additionally, Kappa immunostaining may be a useful alternative in mouse tissues with confounding endogenous CD138 immunostaining.

Published

2022

5. Glycogen depletion can increase the specificity of mucin detection in airway tissues

Author

David K. Meyerholz, Amanda P. Beck, J. Adam Goeken, Mariah R. Leidinger, Georgina K. Ofori-Amanfo, Hannah C. Brown, Thomas R. Businga, David A. Stoltz, Leah R. Reznikov, and Heather A. Flaherty

Subjects

Mucus, Mucin, Periodic acid Schiff (PAS), Diastase-periodic acid Schiff (dPAS), Alcian blue, Glycogen, Medicine, Biology (General), QH301-705.5, Science (General), Q1-390

Abstract

Abstract Objective Mucin is an important parameter for detection and assessment in studies of airway disease including asthma and cystic fibrosis. Histochemical techniques are often used to evaluate mucin in tissues sections. Periodic acid Schiff (PAS) is a common technique to detect neutral mucins in tissue, but this technique also detects other tissue components including cellular glycogen. We tested whether depletion of glycogen, a common cellular constituent, could impact the detection of mucin in the surface epithelium of the trachea. Results Normal tissues stained by PAS had significantly more staining than serial sections of glycogen-depleted tissue with PAS staining (i.e. dPAS technique) based on both quantitative analysis and semiquantitative scores. Most of the excess stain by the PAS technique was detected in ciliated cells adjacent to goblet cells. We also compared normal tissues using the Alcian blue technique, which does not have reported glycogen staining, with the dPAS technique. These groups had similar amounts of staining consistent with a high degree of mucin specificity. Our results suggest that when using PAS techniques to stain airways, the dPAS approach is preferred as it enhances the specificity for airway mucin.

Published

2018

6. ISG15-modification of the Arp2/3 complex restricts pathogen spread

Author

Yifeng Zhang, Brittany Ripley, Wei Ouyang, Miranda Sturtz, Ellen Upton, Emma Luhmann, Madeleine Vessely, Rocio Coloma, Nathan Schwery, Scott M. Anthony, Adam Goeken, Thomas O. Moninger, John T. Harty, Aloysius Klingelhutz, Emma Lundberg, David K. Meyerholz, Balaji Manicassamy, Christopher Stipp, Susana Guerra, and Lilliana Radoshevich

Abstract

SummaryThe ubiquitin-like protein, ISG15, can act as a cytokine or can covalently modify host and pathogen-derived proteins. The consequences of ISG15 modification on substrate fate remain unknown. Here we reveal that ISGylation of the Arp2/3 complex slows actin filament formation and stabilizes Arp2/3 dependent structures including cortical actin and lamella. When properly controlled, this serves as an antibacterial and antiviral host defense strategy to directly restrict actin-mediated pathogen spread. However,Listeria monocytogenestakes advantage in models of dysregulated ISGylation, leading to increased mortality due to augmented spread. The underlying molecular mechanism responsible for the ISG15-dependent impact on actin-based motility is due to failed bacterial separation after division. This promotes spread by enabling the formation of multi-headed bacterial “bazookas” with stabilized comet tails that can disseminate deeper into tissues. A bacterial mutant that cannot recruit Arp2/3 or a non-ISGylatable mutant of Arp3 is sufficient to rescue slowed comet tail speed and restrict spread. Importantly, ISG15-deficient neonatal mice have aberrant epidermal epithelia characterized by keratinocytes with diffuse cortical actin, which could underlie observed defects in wound healing in human patients who lack ISG15. Ultimately, our discovery links host innate immune responses to cytoskeletal dynamics with therapeutic implications for viral infection and metastasis.

Published

2022

7. A method for histopathological study of the multifocal nature of spinal cord lesions in murine experimental autoimmune encephalomyelitis

Author

Katherine N. Gibson-Corley, Alexander W. Boyden, Mariah R. Leidinger, Allyn M. Lambertz, Georgina Ofori-Amanfo, Paul W. Naumann, J. Adam Goeken, and Nitin J. Karandikar

Subjects

Mice, Histopathology, Spinal cord, EAE, Medicine, Biology (General), QH301-705.5

Abstract

Experimental autoimmune encephalomyelitis (EAE) is a well-established mouse model for multiple sclerosis and is characterized by infiltration of mononuclear cells and demyelination within the central nervous system along with the clinical symptoms of paralysis. EAE is a multifocal and random disease, which sometimes makes histopathologic analysis of lesions difficult as it may not be possible to predict where lesions will occur, especially when evaluating cross sections of spinal cord. Consequently, lesions may be easily missed due to limited sampling in traditional approaches. To evaluate the entire length of the spinal cord while maintaining anatomic integrity, we have developed a method to section the cord within the decalcified spinal column, which allows for the study of the multifocal nature of this disease and also minimizes handling artifact. HE and Luxol fast blue staining of these spinal cord sections revealed a paucity of lesions in some areas, while others showed marked inflammation and demyelination. The percentage of spinal cord affected by EAE was evaluated at four separate areas of longitudinally sectioned cord and it varied greatly within each animal. Immunohistochemical staining of in situ spinal cords which had undergone decalcification was successful for key immuno-markers used in EAE research including CD3 for T cells, B220 for B cells and F4/80 for murine macrophages. This method will allow investigators to look at the entire spinal cord on a single slide and evaluate the spinal cord with and without classic EAE lesions.

Published

2016

8. Perfusion with 10% neutral-buffered formalin is equivalent to 4% paraformaldehyde for histopathology and immunohistochemistry in a mouse model of experimental autoimmune encephalomyelitis

Author

Jessica M. Snyder, Enrico Radaelli, Adam Goeken, Thomas Businga, Alexander W. Boyden, Nitin J. Karandikar, and Katherine N. Gibson-Corley

Subjects

Perfusion, Rodent Diseases, Disease Models, Animal, Fixatives, Mice, Encephalomyelitis, Autoimmune, Experimental, Tissue Fixation, General Veterinary, Polymers, Formaldehyde, Animals, Immunohistochemistry, Article

Abstract

Intravascular (IV) perfusion of tissue fixative is commonly used in the field of neuroscience as the central nervous system tissues are exquisitely sensitive to handling and fixation artifacts which can affect downstream microscopic analysis. Both 10% neutral-buffered formalin (NBF) and 4% paraformaldehyde (PFA) are used, although IV perfusion with PFA is most commonly referenced. The study objective was to compare the severity of handling and fixation artifacts, semiquantitative scores of inflammatory and neurodegenerative changes, and quantitative immunohistochemistry following terminal IV perfusion of mice with either 10% NBF or 4% PFA in a model of experimental autoimmune encephalitis (EAE). The study included 24 mice; 12 were control animals not immunized and an additional 12 were immunized with PLP139–151subcutaneously, harvested at day 20, and fixed in the same fashion. Equal numbers (4 per group) were perfused with 10% NBF or 4% PFA, and 4 were immersion-fixed in 10% NBF. NBF-perfused mice had less severe dark neuron artifact than PFA-perfused mice ( P < .001). Immersion-fixed animals had significantly higher scores for oligodendrocyte halos, dark neuron artifact, and perivascular clefts than perfusion-fixed animals. Histopathology scores in EAE mice for inflammation, demyelination, and necrosis did not differ among fixation methods. Also, no significant differences in quantitative immunohistochemistry for CD3 and Iba-1 were observed in immunized animals regardless of the method of fixation. These findings indicate that IV perfusion of mice with 10% NBF and 4% PFA are similar and adequate fixation techniques in this model.

Published

2022

9. Lack of airway submucosal glands impairs respiratory host defenses

Author

Eric A. Hoffman, Randall S. Prather, Thomas R. Businga, Margaret P. Price, Lynda S. Ostedgaard, Guillermo S Romano Ibarra, Brian J Goodell, Patrick D Allen, Mallory R. Stroik, Melissa Samuel, Miguel E Ortiz Bezara, David K. Meyerholz, Camilla E Hippee, Steven E Mather, Linda S. Powers, Michael J. Welsh, Lee D. Spate, Nicholas D. Gansemer, Mahmoud H. Abou Alaiwa, Brieanna M Hilkin, Akshaya Warrier, Kristin M. Whitworth, David A. Stoltz, J. Adam Goeken, Anthony J. Fischer, and Keyan Zarei

Subjects

0301 basic medicine, Male, Staphylococcus aureus, QH301-705.5, Science, Sus scrofa, Respiratory Mucosa, Biology, General Biochemistry, Genetics and Molecular Biology, lung, 03 medical and health sciences, Gene Knockout Techniques, 0302 clinical medicine, Exocrine Glands, In vivo, medicine, Animals, Secretion, Respiratory system, Biology (General), Submucosal glands, Lung, General Immunology and Microbiology, General Neuroscience, General Medicine, respiratory system, Ectodysplasins, Mucus, Cell biology, 030104 developmental biology, medicine.anatomical_structure, 030228 respiratory system, host defense, Medicine, Female, Other, Airway, Ex vivo, Research Article

Abstract

Submucosal glands (SMGs) are a prominent structure that lines human cartilaginous airways. Although it has been assumed that SMGs contribute to respiratory defense, that hypothesis has gone without a direct test. Therefore, we studied pigs, which have lungs like humans, and disrupted the gene for ectodysplasin (EDA-KO), which initiates SMG development.EDA-KOpigs lacked SMGs throughout the airways. Their airway surface liquid had a reduced ability to kill bacteria, consistent with SMG production of antimicrobials. In wild-type pigs, SMGs secrete mucus that emerges onto the airway surface as strands. Lack of SMGs and mucus strands disrupted mucociliary transport inEDA-KOpigs. Consequently,EDA-KOpigs failed to eradicate a bacterial challenge in lung regions normally populated by SMGs. These in vivo and ex vivo results indicate that SMGs are required for normal antimicrobial activity and mucociliary transport, two key host defenses that protect the lung.

Published

2020

10. Author response: Lack of airway submucosal glands impairs respiratory host defenses

Author

Akshaya Warrier, Lynda S. Ostedgaard, Michael J. Welsh, Randall S. Prather, Thomas R. Businga, Margaret P. Price, Brieanna M Hilkin, Lee D. Spate, Miguel E Ortiz Bezara, Camilla E Hippee, Guillermo S Romano Ibarra, Keyan Zarei, Patrick D Allen, Steven E Mather, J. Adam Goeken, Mahmoud H. Abou Alaiwa, Linda S. Powers, Anthony J. Fischer, Kristin M. Whitworth, David A. Stoltz, Melissa Samuel, David K. Meyerholz, Mallory R. Stroik, Eric A. Hoffman, Nicholas D. Gansemer, and Brian J Goodell

Subjects

Submucosal glands, business.industry, Host (biology), Immunology, Medicine, Respiratory system, business, Airway

Published

2020

11. Glycogen depletion can increase the specificity of mucin detection in airway tissues

Author

Amanda P. Beck, Heather A. Flaherty, Thomas R. Businga, Mariah R. Leidinger, David K. Meyerholz, David A. Stoltz, J. Adam Goeken, Hannah C. Brown, Leah R. Reznikov, and Georgina K. Ofori-Amanfo

Subjects

Male, 0301 basic medicine, Swine, lcsh:Medicine, Respiratory Mucosa, Periodic acid–Schiff stain, Alcian blue, Sensitivity and Specificity, Cystic fibrosis, Stain, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, chemistry.chemical_compound, Nonspecific staining, medicine, Animals, lcsh:Science (General), lcsh:QH301-705.5, Staining, Staining and Labeling, Glycogen, Chemistry, Periodic acid Schiff (PAS), Mucin, lcsh:R, Mucins, General Medicine, Periodic Acid-Schiff Reaction, medicine.disease, Molecular biology, Mucus, Epithelium, Diastase-periodic acid Schiff (dPAS), Trachea, Research Note, 030104 developmental biology, medicine.anatomical_structure, Liver, lcsh:Biology (General), Specificity, Female, Scoring, lcsh:Q1-390

Abstract

Objective Mucin is an important parameter for detection and assessment in studies of airway disease including asthma and cystic fibrosis. Histochemical techniques are often used to evaluate mucin in tissues sections. Periodic acid Schiff (PAS) is a common technique to detect neutral mucins in tissue, but this technique also detects other tissue components including cellular glycogen. We tested whether depletion of glycogen, a common cellular constituent, could impact the detection of mucin in the surface epithelium of the trachea. Results Normal tissues stained by PAS had significantly more staining than serial sections of glycogen-depleted tissue with PAS staining (i.e. dPAS technique) based on both quantitative analysis and semiquantitative scores. Most of the excess stain by the PAS technique was detected in ciliated cells adjacent to goblet cells. We also compared normal tissues using the Alcian blue technique, which does not have reported glycogen staining, with the dPAS technique. These groups had similar amounts of staining consistent with a high degree of mucin specificity. Our results suggest that when using PAS techniques to stain airways, the dPAS approach is preferred as it enhances the specificity for airway mucin.

Published

2018

12. Allograft Inflammatory Factor 1 as an Immunohistochemical Marker for Macrophages in Multiple Tissues and Laboratory Animal Species

Author

Heather A. Flaherty, Logan P McQuillen, Mariah R. Leidinger, Christine M Hogan, Sailesh C. Harwani, David K. Meyerholz, Kathleen M Donovan, and J. Adam Goeken

Subjects

0301 basic medicine, White pulp, Pathology, medicine.medical_specialty, Swine, Overview, Spleen, Biology, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, Species Specificity, medicine, Animals, Humans, Macrophage, education, education.field_of_study, General Veterinary, Microglia, Macrophages, Calcium-Binding Proteins, Microfilament Proteins, Ferrets, Immunohistochemistry, Rats, DNA-Binding Proteins, 030104 developmental biology, medicine.anatomical_structure, Lymphatic system, Red pulp, Allograft inflammatory factor 1, Biomarkers, Immunostaining

Abstract

Allograft inflammatory factor 1 (AIF1) is a commonly used marker for microglia in the brains of humans and some animal models but has had limited applications elsewhere. We sought to determine whether AIF1 can be used as a macrophage marker across common laboratory animal species and tissues. We studied tissues (that is, spleen, liver, and lung) with defined macrophage populations by using an AIF1 immunostaining technique previously validated in human tissue. Tissues were collected from various mouse strains (n = 20), rat strains (n = 15), pigs (n = 4), ferrets (n = 4), and humans (n = 4, lung only). All samples of liver had scattered immunostaining in interstitial cells, consistent with resident tissue macrophages (Kupffer cells). Spleen samples had cellular immunostaining of macrophages in both the red and white pulp compartments, but the red pulp had more immunostained cellular aggregates and, in some species, increased immunostaining intensity compared with white pulp. In lung, alveolar macrophages had weak to moderate staining, whereas interstitial and perivascular macrophages demonstrated moderate to robust staining. Incidental lesions and tissue changes were detected in some sections, including a tumor, inducible bronchus-associated lymphoid tissue, and inflammatory lesions that demonstrated AIF1 immunostaining of macrophages. Finally, we compared AIF1 immunostaining of alveolar macrophages between a hypertensive rat model (SHR strain) and a normotensive model (WKY strain). SHR lungs had altered intensity and distribution of immunostaining in activated macrophages compared with macrophages of WKY lungs. Overall, AIF1 immunostaining demonstrated reproducible macrophage staining across multiple species and tissue types. Given the increasing breadth of model species used to study human disease, the use of cross-species markers and techniques can reduce some of the inherent variability within translational research.

Published

2018

13. Development of gene augmentation strategy for the treatment of MAK associated Retinitis Pigmentosa

Author

Thomas R. Businga, Edwin M. Stone, Robert F. Mullins, Cathryn M. Cranston, Emily E. Kaalberg, Ian C. Han, Kristin R. Anfinson, Adam Goeken, Diane C. Slusarski, Katherine N. Gibson-Corley, Budd A. Tucker, and Hannah K. Brown

Subjects

business.industry, Immunology, Retinitis pigmentosa, Genetics, Medicine, business, medicine.disease, Molecular Biology, Biochemistry, Gene, Biotechnology

Published

2019

14. A porcine model of neurofibromatosis type 1 that mimics the human disease

Author

Dawn E. Quelle, Adam Goeken, Chun Hung Chan, Rebecca D. Dodd, Frank Rohret, Jessica C. Sieren, Johanna Uthoff, Song Cai, Katherine A. White, Aubin Moutal, Emily Hammond, Margaret R. Wallace, Benjamin W. Darbro, Jill M. Weimer, Shreya S. Bellampalli, Amy H. Tang, Vicki J. Swier, Hua Li, Munir R. Tanas, Jacob T. Cain, Shaikamjad Umesalma, Wennan Li, Jordan L. Kohlmeyer, Christopher S. Rogers, David K. Meyerholz, Mariah R. Leidinger, Karin Panzer, and Rajesh Khanna

Subjects

Male, 0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Neurofibromatosis 1, Tumor suppressor gene, Swine, Mutant, medicine.disease_cause, Ion Channels, Gene Knockout Techniques, 03 medical and health sciences, Exon, 0302 clinical medicine, Memory, Ganglia, Spinal, Café au lait spot, medicine, Animals, Humans, Learning, Neurofibromatosis, neoplasms, Phenocopy, Mutation, Neurofibroma, Neurofibromin 1, biology, Cafe-au-Lait Spots, GTPase-Activating Proteins, Exons, General Medicine, Fibroblasts, medicine.disease, eye diseases, nervous system diseases, Disease Models, Animal, 030104 developmental biology, Technical Advance, Gene Expression Regulation, biology.protein, Cancer research, medicine.symptom, Gene Deletion, 030217 neurology & neurosurgery, Signal Transduction

Abstract

Loss of the NF1 tumor suppressor gene causes the autosomal dominant condition, neurofibromatosis type 1 (NF1). Children and adults with NF1 suffer from pathologies including benign and malignant tumors to cognitive deficits, seizures, growth abnormalities, and peripheral neuropathies. NF1 encodes neurofibromin, a Ras-GTPase activating protein, and NF1 mutations result in hyperactivated Ras signaling in patients. Existing NF1 mutant mice mimic individual aspects of NF1, but none comprehensively models the disease. We describe a potentially novel Yucatan miniswine model bearing a heterozygotic mutation in NF1 (exon 42 deletion) orthologous to a mutation found in NF1 patients. NF1+/ex42del miniswine phenocopy the wide range of manifestations seen in NF1 patients, including café au lait spots, neurofibromas, axillary freckling, and neurological defects in learning and memory. Molecular analyses verified reduced neurofibromin expression in swine NF1+/ex42del fibroblasts, as well as hyperactivation of Ras, as measured by increased expression of its downstream effectors, phosphorylated ERK1/2, SIAH, and the checkpoint regulators p53 and p21. Consistent with altered pain signaling in NF1, dysregulation of calcium and sodium channels was observed in dorsal root ganglia expressing mutant NF1. Thus, these NF1+/ex42del miniswine recapitulate the disease and provide a unique, much-needed tool to advance the study and treatment of NF1.

Published

2018

15. Immunohistochemical Markers for Prospective Studies in Neurofibromatosis-1 Porcine Models

Author

Rajesh Khanna, Dawn E. Quelle, J. Adam Goeken, Georgina K. Ofori-Amanfo, Jessica C. Sieren, Mariah R. Leidinger, David K. Meyerholz, Jill M. Weimer, and Benjamin W. Darbro

Subjects

0301 basic medicine, Male, Pathology, medicine.medical_specialty, Histology, Neurofibromatosis 1, Swine, Vimentin, 03 medical and health sciences, Laminin, Medicine, Animals, Humans, Neurofibromatosis, Rhabdomyosarcoma, Glial fibrillary acidic protein, biology, business.industry, Articles, medicine.disease, Immunohistochemistry, Myelin basic protein, Disease Models, Animal, 030104 developmental biology, biology.protein, Desmin, Female, Anatomy, business, Biomarkers

Abstract

Neurofibromatosis type 1 (NF1) is a common, cancer-predisposing disease caused by mutations in the NF1 tumor gene. Patients with NF1 have an increased risk for benign and malignant tumors of the nervous system (e.g., neurofibromas, malignant peripheral nerve sheath tumors, gliomas) and other tissues (e.g., leukemias, rhabdomyosarcoma, etc.) as well as increased susceptibility to learning disabilities, chronic pain/migraines, hypertension, pigmentary changes, and developmental lesions (e.g., tibial pseudoarthrosis). Pigs are an attractive and upcoming animal model for future NF1 studies, but a potential limitation to porcine model research has been the lack of validated reagents for direct translational study to humans. To address that issue, we used formalin-fixed tissues (human and pigs) to evaluate select immunohistochemical markers (activated caspase-3, allograft inflammatory factor-1, beta-tubulin III, calbindin D, CD13, CD20, desmin, epithelial membrane antigen, glial fibrillary acidic protein, glucose transporter-1, laminin, myelin basic protein, myoglobin, proliferating cell nuclear antigen, S100, vimentin, and von Willebrand factor). The markers were validated by comparing known expression and localization in human and pig tissues. Validation of these markers on fixed tissues will facilitate prospective immunohistochemical studies of NF1 pigs, as well as other pig models, in a more efficient, reproducible, and translationally relevant manner.

Published

2017

16. Development and translational imaging of a TP53 porcine tumorigenesis model

Author

Christopher S. Rogers, Paul W. Naumann, Emily Hammond, Xiao-Jun Wang, Jussara Hagen, J. Adam Goeken, David K. Meyerholz, Richard Van Rheeden, Agshin F. Taghiyev, Frank Rohret, Mariah R. Leidinger, John D. Newell, Jason T. Struzynski, Bryan T. Davis, Judy A. Rohret, Dawn E. Quelle, Benjamin W. Darbro, and Jessica C. Sieren

Subjects

Male, Pathology, medicine.medical_specialty, Carcinogenesis, Swine, Disease, Biology, medicine.disease_cause, Neoplasms, Chromosome instability, medicine, Animals, Humans, Allele, Mutation, medicine.diagnostic_test, Cancer, Magnetic resonance imaging, General Medicine, medicine.disease, Magnetic Resonance Imaging, Genetically modified organism, Disease Models, Animal, Genes, ras, Technical Advance, Cancer research, Female, Tumor Suppressor Protein p53, Tomography, X-Ray Computed

Abstract

Cancer is the second deadliest disease in the United States, necessitating improvements in tumor diagnosis and treatment. Current model systems of cancer are informative, but translating promising imaging approaches and therapies to clinical practice has been challenging. In particular, the lack of a large-animal model that accurately mimics human cancer has been a major barrier to the development of effective diagnostic tools along with surgical and therapeutic interventions. Here, we developed a genetically modified porcine model of cancer in which animals express a mutation in TP53 (which encodes p53) that is orthologous to one commonly found in humans (R175H in people, R167H in pigs). TP53(R167H/R167H) mutant pigs primarily developed lymphomas and osteogenic tumors, recapitulating the tumor types observed in mice and humans expressing orthologous TP53 mutant alleles. CT and MRI imaging data effectively detected developing tumors, which were validated by histopathological evaluation after necropsy. Molecular genetic analyses confirmed that these animals expressed the R167H mutant p53, and evaluation of tumors revealed characteristic chromosomal instability. Together, these results demonstrated that TP53(R167H/R167H) pigs represent a large-animal tumor model that replicates the human condition. Our data further suggest that this model will be uniquely suited for developing clinically relevant, noninvasive imaging approaches to facilitate earlier detection, diagnosis, and treatment of human cancers.

Published

2014

17. Keratoacanthoma Pathobiology in Mouse Models

Author

David K. Meyerholz, Adam J. Dupuy, Katherine N. Gibson-Corley, Laura M. Rogers, and Adam Goeken

Subjects

Keratoacanthoma, Pathology, medicine.medical_specialty, CD3, Skin tumor, lcsh:Medicine, Inflammation, Article, 030207 dermatology & venereal diseases, 03 medical and health sciences, 0302 clinical medicine, medicine, mouse models, Immune cell infiltration, Cellular atypia, biology, business.industry, lcsh:R, medicine.disease, Granzyme B, 030220 oncology & carcinogenesis, biology.protein, histopathology, Histopathology, regression, medicine.symptom, business, keratoacanthoma

Abstract

Recently we described skin tumors driven by skin-specific expression of Zmiz1 and here we define keratoacanthoma pathobiology in this mouse model. Similar to human keratoacanthoma development, we were able to segregate murine keratoacanthomas into three developmental phases: growth, maturation, and regression. These tumors had areas with cellular atypia, high mitotic rate, and minor local invasion in the growth phase, but with development they transitioned to maturation and regression phases with evidence of resolution. The early aggressive appearance could easily be misdiagnosed as a malignant change if the natural pathobiology was not well-defined in the model. To corroborate these findings in the Zmiz1 model, we examined squamous skin tumors from another tumor study in aging mice, and these tumors followed a similar biological progression. Lastly, we were able to evaluate the utility of the model to assess immune cell infiltration (F4/80, B220 Granzyme B, CD3 cells, arginase-1) in the regression phase, however, because inflammation was present at all phases of development, a more comprehensive approach will be needed in future investigations. Our study of keratoacanthomas in selected murine models suggests that these squamous tumors can appear histologically aggressive during early development, but with time will enter a regression phase indicating a benign biology. Importantly, studies of squamous skin tumor models should be cautious in tumor diagnosis as the early growth distinction between malignant versus benign based solely on histopathology may not be easily discerned without longitudinal studies to confirm the tumor pathobiology.

Published

2014

18. Gastrointestinal Pathology in Juvenile and Adult CFTR-Knockout Ferrets

Author

Nicholas W. Keiser, Joann M. Kinyon, Thomas J. Lynch, Weihong Zhou, John F. Engelhardt, Xingshen Sun, Yaling Yi, Scott R. Tyler, J. Adam Goeken, Yulong Zhang, Yi Song, Timothy S. Frana, Xiaoming Liu, Lucas R. Hoffman, Kalpaj R. Parekh, Mitchell J. Brittnacher, Weiliang Xie, Alicia K. Olivier, Hongshu Sui, Bo Liang, David K. Meyerholz, Xiaoyan Wang, Samuel I. Miller, Danielle Fligg, Kyle R. Hager, John T. Fisher, Zoe A. Stewart, Paul M. Kaminsky, Ziying Yan, Christopher E. Pope, Hillary S. Hayden, and Matthew C. Radey

Subjects

Aging, medicine.medical_specialty, Pathology, Cystic Fibrosis, Cystic Fibrosis Transmembrane Conductance Regulator, Gastroenterology, Cystic fibrosis, Pathology and Forensic Medicine, Gene Knockout Techniques, Atrophy, Fibrosis, Internal medicine, medicine, Animals, Humans, Gastrointestinal tract, Bacteria, biology, Biliary hyperplasia, Gallbladder, Ferrets, Regular Article, Gastrointestinal pathology, medicine.disease, Cystic fibrosis transmembrane conductance regulator, 3. Good health, Gastrointestinal Tract, Mucus, medicine.anatomical_structure, Organ Specificity, biology.protein

Abstract

Cystic fibrosis (CF) is a multiorgan disease caused by loss of a functional cystic fibrosis transmembrane conductance regulator (CFTR) chloride channel in many epithelia of the body. Here we report the pathology observed in the gastrointestinal organs of juvenile to adult CFTR-knockout ferrets. CF gastrointestinal manifestations included gastric ulceration, intestinal bacterial overgrowth with villous atrophy, and rectal prolapse. Metagenomic phylogenetic analysis of fecal microbiota by deep sequencing revealed considerable genotype-independent microbial diversity between animals, with the majority of taxa overlapping between CF and non-CF pairs. CF hepatic manifestations were variable, but included steatosis, necrosis, biliary hyperplasia, and biliary fibrosis. Gallbladder cystic mucosal hyperplasia was commonly found in 67% of CF animals. The majority of CF animals (85%) had pancreatic abnormalities, including extensive fibrosis, loss of exocrine pancreas, and islet disorganization. Interestingly, 2 of 13 CF animals retained predominantly normal pancreatic histology (84% to 94%) at time of death. Fecal elastase-1 levels from these CF animals were similar to non-CF controls, whereas all other CF animals evaluated were pancreatic insufficient (

Published

2014

19. Lung Phenotype of Juvenile and Adult Cystic Fibrosis Transmembrane Conductance Regulator–Knockout Ferrets

Author

Paul M. Kaminsky, Zoe A. Stewart, Ziying Yan, R. Marshall Pope, Nicholas W. Keiser, Xingshen Sun, Yaling Yi, John F. Engelhardt, J. Adam Goeken, Kalpaj R. Parekh, Danielle Fligg, Bo Liang, Hongshu Sui, Yi Song, Scott R. Tyler, Weihong Zhou, Thomas J. Lynch, Xiaoyan Wang, David K. Meyerholz, Xiaoming Liu, Joann M. Kinyon, Yulong Zhang, John T. Fisher, Weiliang Xie, Turan I.A. Evans, Alicia K. Olivier, and Timothy S. Frana

Subjects

Pulmonary and Respiratory Medicine, Pathology, medicine.medical_specialty, Cystic Fibrosis, Mucociliary clearance, Clinical Biochemistry, Cystic Fibrosis Transmembrane Conductance Regulator, Atelectasis, Biology, Air trapping, Cystic fibrosis, Animals, Genetically Modified, medicine, Animals, Genetic Predisposition to Disease, Lung, Respiratory Tract Infections, Molecular Biology, Original Research, Submucosal glands, Age Factors, Ferrets, Cell Biology, respiratory system, medicine.disease, Mucus, Cystic fibrosis transmembrane conductance regulator, Anti-Bacterial Agents, respiratory tract diseases, Intestines, Disease Models, Animal, Phenotype, medicine.anatomical_structure, Mucociliary Clearance, Bacterial Translocation, Disease Progression, biology.protein, medicine.symptom

Abstract

Chronic bacterial lung infections in cystic fibrosis (CF) are caused by defects in the CF transmembrane conductance regulator chloride channel. Previously, we described that newborn CF transmembrane conductance regulator–knockout ferrets rapidly develop lung infections within the first week of life. Here, we report a more slowly progressing lung bacterial colonization phenotype observed in juvenile to adult CF ferrets reared on a layered antibiotic regimen. Even on antibiotics, CF ferrets were still very susceptible to bacterial lung infection. The severity of lung histopathology ranged from mild to severe, and variably included mucus obstruction of the airways and submucosal glands, air trapping, atelectasis, bronchopneumonia, and interstitial pneumonia. In all CF lungs, significant numbers of bacteria were detected and impaired tracheal mucociliary clearance was observed. Although Streptococcus, Staphylococcus, and Enterococcus were observed most frequently in the lungs of CF animals, each animal displayed a predominant bacterial species that accounted for over 50% of the culturable bacteria, with no one bacterial taxon predominating in all animals. Matrix-assisted laser desorption–ionization time-of-flight mass spectrometry fingerprinting was used to quantify lung bacteria in 10 CF animals and demonstrated Streptococcus, Staphylococcus, Enterococcus, or Escherichia as the most abundant genera. Interestingly, there was significant overlap in the types of bacteria observed in the lung and intestine of a given CF animal, including bacterial taxa unique to the lung and gut of each CF animal analyzed. These findings demonstrate that CF ferrets develop lung disease during the juvenile and adult stages that is similar to patients with CF, and suggest that enteric bacterial flora may seed the lung of CF ferrets.

Published

2014

20. A method for histopathological study of the multifocal nature of spinal cord lesions in murine experimental autoimmune encephalomyelitis

Author

J. Adam Goeken, Allyn M. Lambertz, Paul W. Naumann, Nitin J. Karandikar, Mariah R. Leidinger, Katherine N. Gibson-Corley, Georgina K. Ofori-Amanfo, and Alexander W. Boyden

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Cord, Histology, Central nervous system, lcsh:Medicine, Histopathology, General Biochemistry, Genetics and Molecular Biology, Luxol fast blue stain, 03 medical and health sciences, Mice, 0302 clinical medicine, Paralysis, medicine, Spinal cord, business.industry, EAE, General Neuroscience, Multiple sclerosis, Experimental autoimmune encephalomyelitis, lcsh:R, General Medicine, medicine.disease, Spinal column, 030104 developmental biology, medicine.anatomical_structure, Neurology, medicine.symptom, General Agricultural and Biological Sciences, business, 030217 neurology & neurosurgery

Abstract

Experimental autoimmune encephalomyelitis (EAE) is a well-established mouse model for multiple sclerosis and is characterized by infiltration of mononuclear cells and demyelination within the central nervous system along with the clinical symptoms of paralysis. EAE is a multifocal and random disease, which sometimes makes histopathologic analysis of lesions difficult as it may not be possible to predict where lesions will occur, especially when evaluating cross sections of spinal cord. Consequently, lesions may be easily missed due to limited sampling in traditional approaches. To evaluate the entire length of the spinal cord while maintaining anatomic integrity, we have developed a method to section the cord within the decalcified spinal column, which allows for the study of the multifocal nature of this disease and also minimizes handling artifact. HE and Luxol fast blue staining of these spinal cord sections revealed a paucity of lesions in some areas, while others showed marked inflammation and demyelination. The percentage of spinal cord affected by EAE was evaluated at four separate areas of longitudinally sectioned cord and it varied greatly within each animal. Immunohistochemical staining of in situ spinal cords which had undergone decalcification was successful for key immuno-markers used in EAE research including CD3 for T cells, B220 for B cells and F4/80 for murine macrophages. This method will allow investigators to look at the entire spinal cord on a single slide and evaluate the spinal cord with and without classic EAE lesions.

Published

2016

21. Optimal oligonucleotide sequences for TLR9 inhibitory activity in human cells: lack of correlation with TLR9 binding

Author

Petar Lenert, J. Adam Goeken, Eicke Latz, and Robert F. Ashman

Subjects

Molecular Sequence Data, Immunology, Anti-Inflammatory Agents, Phosphorothioate Oligonucleotides, Cell Line, Mice, Animals, Humans, Immunology and Allergy, B-Lymphocytes, Base Sequence, biology, Oligonucleotide, HEK 293 cells, TLR9, hemic and immune systems, General Medicine, Transfection, respiratory system, Flow Cytometry, Molecular biology, Fusion protein, DNA-Binding Proteins, Oligodeoxyribonucleotides, Ectodomain, Cell culture, Toll-Like Receptor 9, biology.protein, Antibody, Original Research Papers, Protein Binding

Abstract

Toll-like receptor (TLR)9 performs our innate response to bacterial DNA, warning us of the presence of infection. Inhibitory oligodeoxyribonucleotides (INH-ODN) have been developed that selectively block activation of mouse TLR9. Their inhibitory motif consisting of CCx(not-C)(not-C)xxGGG (x = any base) also reduces anti-DNA antibodies in lupus mice. The current study demonstrates that this motif also provides the sequences required to block TLR9 in human B cells and human embryonic kidney (HEK) cells transfected with human TLR9. However, extending the sequence by four to five bases at the 5' end enhanced activity and this enhancement was greater when a phosphorothioate (pS) backbone replaced the native phosphodiester (pO) backbone. A series of pO-backbone INH-ODN representing a 500-fold range of activity in biologic assays was shown to cover less than a 2.5-fold range of avidity for binding human TLR9-Ig fusion protein, eliminating TLR9 ectodomain binding as the explanation for sequence-specific differences in biologic activity. With few exceptions, the relative activity of INH-ODN in Namalwa cells and HEK/human TLR9 cells was similar to that seen in mouse B cells. INH-ODN activity in human peripheral blood B cells correlated significantly with the cell line data. These results favor the conclusion that although the backbone determines strength of TLR9 binding, critical recognition of the INH-ODN sequence necessary for biologic activity is performed by a molecule that is not TLR9. These studies also identify the strongest INH-ODN for human B cells, helping to guide the selection of INH-ODN sequences for therapeutics in any situation where inflammation is enhanced by TLR9.

Published

2011

22. Extended sequence preferences for oligodeoxyribonucleotide activity

Author

Robert F. Ashman, Adam Goeken, and Petar Lenert

Subjects

Immunology, Dose-Response Relationship, Immunologic, Apoptosis, Mice, Inbred Strains, Biology, DNA-binding protein, Mice, Structure-Activity Relationship, Animals, Immunology and Allergy, Structure–activity relationship, Receptor, Cells, Cultured, Genetics, B-Lymphocytes, Base Sequence, Interleukin-6, HEK 293 cells, G1 Phase, NF-kappa B, TLR9, hemic and immune systems, Original Articles, Transfection, respiratory system, Molecular biology, Toll-Like Receptor 9, DNA-Binding Proteins, Oligodeoxyribonucleotides, CpG site, CpG Islands, Female

Abstract

Synthetic type B phosphorothioate oligodeoxyribonucleotides (ODN) activate mouse B cells via Toll-like receptor 9 (TLR9). Starting with closely related 15-mer prototype ODN, the sequence requirements for stimulatory (ST-) and inhibitory (IN-) activity were contrasted, by measuring apoptosis protection, G(1) entry and interleukin-6 secretion. ST-ODN and IN-ODN differ in that (1) ST-ODN require a 5' T, (2) the central CG is obligatory, (3) CG must be flanked 3' specifically by TT at the position where IN-ODN have GG, and (4) IN-ODN tolerate truncation of the 3' end better than ST-ODN. Features shared by ST-ODN and IN-ODN include (1) requiring CC adjacent to the 5' end, and (2) avoiding CC immediately 5' to the CG. This pattern is used to create a model of how ST-ODN binding might function to aggregate TLR9 so as to initiate the signal, and how the 5' ends of ST-ODN and IN-ODN compete for binding. Further justification for considering TLR9 to be the ODN receptor was provided by a demonstration that in HEK293 cells transfected with TLR9, the potency of a panel of ODN for activating NF-kappaB roughly parallels that seen in the biological assays in mouse B cells.

Published

2006

23. [Untitled]

Author

Robert F. Ashman, Petar Lenert, Barry S. Handwerger, and Adam Goeken

Subjects

Innate immune system, Lipopolysaccharide, medicine.medical_treatment, Immunology, TLR9, Biology, Toll-Like Receptor 9, chemistry.chemical_compound, Cytokine, Immune system, chemistry, medicine, Immunology and Allergy, Cytokine secretion, Secretion

Abstract

Inadequate immune response to infectious danger may contribute to the pathogenesis of systemic autoimmune diseases, e.g., systemic lupus erythematosus. To test this hypothesis, we studied innate responses of prediseased lupus-prone Palmerston North (PN) mice to lipopolysaccharide (LPS), bacterial DNA, and synthetic CpG oligonucleotides. LPS and bacterial DNA/CpG oligodeoxyribonucleotides (ODNs) drove PN splenocytes into the cell cycle and protected B cells against spontaneous apoptosis, as in control lupus-free DBA-1 mice. LPS induced significantly higher IL-6 production in PN than in control splenocytes. In contrast, in PN splenocytes bacterial DNA and CpG ODNs induced approximately four- to sixfold lower IL-12p40 and approximately twofold lower IL-6 secretion than controls. This reduction in cytokine secretion in PN mice was not due to delayed kinetics but was related to significantly higher constitutive and CpG-inducible IL-10 secretion. Neutralizing anti-IL-10 antibodies almost completely restored PN IL-6 and IL-12p40 secretion to DBA-1 levels, whereas exogenous IL-10 inhibited in vitro IL-6 and IL-12p40 production in DBA-1 mice. Importantly, treatment with either IL-10 or anti-IL-10 antibody did not modulate CpG-induced cell cycle entry and apoptosis protection in either strain. In conclusion, lupus-prone PN mice show abnormal innate responses through their pattern-recognition TLR9 receptors, characterized by higher inducible IL-10 and lower IL-12p40 and IL-6 secretion, thus implying that response to infectious danger in PN mice is inappropriate and may be linked to lupus pathogenesis.

Published

2003

24. Genetically modified species in research: Opportunities and challenges for the histology core laboratory

Author

Mary Sturm, David K. Meyerholz, Alicia K. Olivier, Katherine N. Gibson-Corley, Paul W. Naumann, Christine Hochstedler, Janis R Rodgers, and Adam Goeken

Subjects

Protocol (science), Histology, Genetically engineered, media_common.quotation_subject, Physiology, Translational research, Research needs, Research opportunities, Biology, Data science, Article, Genetically modified organism, Medical Laboratory Technology, Quality (business), Anatomy, Core laboratory, media_common

Abstract

Translational research using animal models has traditionally involved genetically modified rodents; however, there is increasing use of other novel genetically engineered species. As histology laboratories interface with researchers studying these novel species there will be many situations in which protocols will need to be adapted to the species, model and research goals. This paper gives examples of protocol adaptations to meet research needs and addresses common considerations that should be addressed for all research tissues submitted to the histotechnology laboratory. Positioning the histotechnologist, as well as the investigator, to meet the challenges associated with novel research models will help maximize research efficacy and quality.

Published

2012

25. Deletion of the Antioxidant Enzyme Methionine Sulfoxide Reductase‐A Impairs Autonomic Regulation and Exacerbates Angiotensin‐induced Hypertension and End‐Organ Damage

Author

Mark W. Chapleau, Ramzi El Accaoui, Francois M. Abboud, J. Adam Goeken, Robert M. Weiss, David K. Meyerholz, Rasna Sabharwal, and Melissa K Davis

Subjects

chemistry.chemical_classification, Antioxidant, End organ damage, medicine.medical_treatment, Pharmacology, medicine.disease, Biochemistry, Autonomic regulation, Enzyme, chemistry, Renin–angiotensin system, Genetics, medicine, Methionine sulfoxide reductase A, Molecular Biology, Biotechnology

Published

2012

26. Aggregation and Secondary Loop Structure of Oligonucleotides do not Determine Their Ability to Inhibit TLR9

Author

Robert F. Ashman, Petar Lenert, and J. Adam Goeken

Subjects

Endosome, Immunology, Oligonucleotides, Plasma protein binding, Biology, Article, Cell Line, Polymerization, Mice, Structure-Activity Relationship, Immunology and Allergy, Structure–activity relationship, Animals, Humans, Binding site, Pharmacology, B-Lymphocytes, Binding Sites, Base Sequence, Oligonucleotide, TLR9, hemic and immune systems, respiratory system, Molecular biology, Cell biology, Toll-Like Receptor 9, Oligodeoxyribonucleotides, Cell culture, Protein Binding

Abstract

Toll-like receptor 9 (TLR9) is an endosomal DNA sensor that warns us of the presence of infectious danger and triggers a rapid pro-inflammatory response in dendritic cells, macrophages, and B cells. The consequences of uncontrolled TLR9 activation can be detrimental for the host, contributing to the pathogenesis of bacterial septic shock or autoimmune diseases, such as systemic lupus erythematosus. Therefore, we need to develop TLR9 antagonists. We and others have created inhibitory oligonucleotides (INH-ODN) that are capable of sequence-dependent inhibition of TLR9-induced activation in both human and mouse cells. However, it is not clear whether marked differences in INH-ODN activity related to base sequence derived from polymerization of INH-ODNs or their ability to complex with stimulatory CpG-oligonucleotides (ST-ODN). Furthermore, the 5' end of INH-ODNs may assume a particular loop configuration that may be needed for binding to a critical site on TLR9. Here, we show that 1) G-tetrads required for ODN stacking were compatible with INH-ODN activity but were not necessary; 2) there was no relationship between activity and self-association at endosomal pH; 3) there was no evidence for direct binding between ST-ODNs and INH-ODNs; 4) when a 3G sequence was disrupted, despite a preserved stem-loop formation, INH-ODN activity was abolished. These results support the conclusion that certain features of the primary linear sequence are critical for TLR9 inhibition, but changes in secondary structure or in ODN aggregation are irrelevant.

Published

2011

27. Sequence requirements for oligodeoxyribonucleotide inhibitory activity

Author

J. Adam Goeken, Robert F. Ashman, Petar Lenert, and Jennifer Drahos

Subjects

CpG Oligodeoxynucleotide, Immunology, Apoptosis, Biology, chemistry.chemical_compound, Mice, Structure-Activity Relationship, medicine, Splenocyte, Immunology and Allergy, Animals, Point Mutation, Secretion, B cell, Sequence (medicine), Cell Proliferation, Genetics, B-Lymphocytes, Oligonucleotide, Interleukin-6, hemic and immune systems, General Medicine, respiratory system, Molecular biology, medicine.anatomical_structure, chemistry, Oligodeoxyribonucleotides, DNA

Abstract

Inhibitory oligonucleotides (IN-ODN) differing from stimulatory CpG ODN (ST-ODN) by as few as two bases can block ST-ODN-induced proliferation, apoptosis protection and IL-6 secretion in B lymphocytes and the production of IL-12p40 by non-B cells. The main objective of this study was to determine the ODN sequence requirements for inhibition in mice. Starting with a strongly inhibitory 15-mer prototype phosphorothioate sequence, we tested the 60 sequences that differed from the prototype by one base, revealing the three areas that are critical for activity. Between these areas were the spacer sequences where base composition mattered little, but the number of bases was important. Truncation of three bases at the 39 end of the 15-mer and one at the 59 end was tolerated with minimal loss of activity. This approach yielded an ‘optimal’ sequence of 59 CC x notC notC xxGGGx or CC x notC notC xGGGxx 39, where x is any base. The sequence requirements for optimal inhibition of B cell responses to Type B (K) ODN and mixed splenocyte IL-12p40 responses to Type A (D) ODN were strikingly similar. Inhibition of ST-ODN by IN-ODN was competitive. A hypothetical model of the ODN-binding site is proposed. Synthetic IN-ODN with the sequence characteristics defined here should provide antidotes for excessive innate reactions to DNA.

Published

2005

28. Innate immune responses in lupus-prone Palmerston North mice: differential responses to LPS and bacterial DNA/CpG oligonucleotides

Author

Petar, Lenert, Adam, Goeken, Barry S, Handwerger, and Robert F, Ashman

Subjects

DNA, Bacterial, Lipopolysaccharides, Interleukin-12 Subunit p40, Interleukin-6, Enzyme-Linked Immunosorbent Assay, Receptors, Cell Surface, Flow Cytometry, Interleukin-12, Interleukin-10, DNA-Binding Proteins, Disease Models, Animal, Mice, Protein Subunits, Oligodeoxyribonucleotides, Toll-Like Receptor 9, Animals, Cytokines, Lupus Erythematosus, Systemic, CpG Islands, Female, Lymphocytes, Cells, Cultured

Abstract

Inadequate immune response to infectious danger may contribute to the pathogenesis of systemic autoimmune diseases, e.g., systemic lupus erythematosus. To test this hypothesis, we studied innate responses of prediseased lupus-prone Palmerston North (PN) mice to lipopolysaccharide (LPS), bacterial DNA, and synthetic CpG oligonucleotides. LPS and bacterial DNA/CpG oligodeoxyribonucleotides (ODNs) drove PN splenocytes into the cell cycle and protected B cells against spontaneous apoptosis, as in control lupus-free DBA-1 mice. LPS induced significantly higher IL-6 production in PN than in control splenocytes. In contrast, in PN splenocytes bacterial DNA and CpG ODNs induced approximately four- to sixfold lower IL-12p40 and approximately twofold lower IL-6 secretion than controls. This reduction in cytokine secretion in PN mice was not due to delayed kinetics but was related to significantly higher constitutive and CpG-inducible IL-10 secretion. Neutralizing anti-IL-10 antibodies almost completely restored PN IL-6 and IL-12p40 secretion to DBA-1 levels, whereas exogenous IL-10 inhibited in vitro IL-6 and IL-12p40 production in DBA-1 mice. Importantly, treatment with either IL-10 or anti-IL-10 antibody did not modulate CpG-induced cell cycle entry and apoptosis protection in either strain. In conclusion, lupus-prone PN mice show abnormal innate responses through their pattern-recognition TLR9 receptors, characterized by higher inducible IL-10 and lower IL-12p40 and IL-6 secretion, thus implying that response to infectious danger in PN mice is inappropriate and may be linked to lupus pathogenesis.

Published

2003

29. NIAM-Deficient Mice Are Predisposed to the Development of Proliferative Lesions including B-Cell Lymphomas

Author

Jussara Hagen, Dawn E. Quelle, Van S. Tompkins, Paul W. Naumann, Timothy R. Rosean, Viviane P. Muniz, Sara M. Reed, J. Adam Goeken, Weizhou Zhang, Siegfried Janz, David K. Meyerholz, Nicholas Borcherding, and Sebastian Sciegienka

Subjects

Male, Pathology, lcsh:Medicine, medicine.disease_cause, Suppressor Genes, Lymphoid hyperplasia, Hematologic Cancers and Related Disorders, Mice, 0302 clinical medicine, Basic Cancer Research, Medicine and Health Sciences, lcsh:Science, 0303 health sciences, Multidisciplinary, Hematology, Animal Models, Hyperplasia, Marginal zone, 3. Good health, DNA-Binding Proteins, Cell Transformation, Neoplastic, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Female, medicine.symptom, Hemangioma, Signal Transduction, Research Article, Adenoma, White pulp, medicine.medical_specialty, Lymphoma, B-Cell, Tumor Suppressor Genes, Down-Regulation, Mice, Transgenic, Mouse Models, Spleen, Biology, Research and Analysis Methods, 03 medical and health sciences, Model Organisms, Gene Types, Genetics, medicine, Animals, Humans, Genetic Predisposition to Disease, B cell, Cell Proliferation, 030304 developmental biology, lcsh:R, Biology and Life Sciences, Cancers and Neoplasms, Cell Biology, medicine.disease, Lymphoma, Cancer research, lcsh:Q, Tumor Suppressor Protein p53, Carcinogenesis

Abstract

Nuclear Interactor of ARF and Mdm2 (NIAM, gene designation Tbrg1) is a largely unstudied inhibitor of cell proliferation that helps maintain chromosomal stability. It is a novel activator of the ARF-Mdm2-Tip60-p53 tumor suppressor pathway as well as other undefined pathways important for genome maintenance. To examine its predicted role as a tumor suppressor, we generated NIAM mutant (NIAM(m/m)) mice homozygous for a β-galactosidase expressing gene-trap cassette in the endogenous gene. The mutant mice expressed significantly lower levels of NIAM protein in tissues compared to wild-type animals. Fifty percent of aged NIAM deficient mice (14 to 21 months) developed proliferative lesions, including a uterine hemangioma, pulmonary papillary adenoma, and a Harderian gland adenoma. No age-matched wild-type or NIAM(+/m) heterozygous animals developed lesions. In the spleen, NIAM(m/m) mice had prominent white pulp expansion which correlated with enhanced increased reactive lymphoid hyperplasia and evidence of systemic inflammation. Notably, 17% of NIAM mutant mice had splenic white pulp features indicating early B-cell lymphoma. This correlated with selective expansion of marginal zone B cells in the spleens of younger, tumor-free NIAM-deficient mice. Unexpectedly, basal p53 expression and activity was largely unaffected by NIAM loss in isolated splenic B cells. In sum, NIAM down-regulation in vivo results in a significant predisposition to developing benign tumors or early stage cancers. These mice represent an outstanding platform for dissecting NIAM's role in tumorigenesis and various anti-cancer pathways, including p53 signaling.

Published

2014

30. Abstract LB-162: Translational imaging of tumorigenesis in a TP53 porcine cancer model

Author

Benjamin W. Darbro, Paul W. Naumann, Christopher S. Rogers, David K. Meyerholz, Adam Goeken, Xiao-Jun Wang, Frank Rohret, John D. Newell, Jason T. Struzynski, Judy A. Rohret, Bryan T. Davis, Jessica C. Sieren, Mariah R. Leidinger, Dawn E. Quelle, Jussara Hagen, Richard Van Rheeden, and Emily Hammond

Subjects

Cancer Research, medicine.medical_specialty, Pathology, business.industry, Cancer Model, Cancer, Disease, medicine.disease_cause, medicine.disease, Oncology, Chromosome instability, medicine, Medical imaging, Cancer research, Histopathology, business, Carcinogenesis, P53 expression

Abstract

Cancer remains the second deadliest disease in the United States, necessitating improvements in tumor diagnosis and treatment. Current model systems of cancer have been informative but also present challenges to translating promising imaging approaches and therapies to the clinic. The lack of a large animal model that accurately mimics human cancer has been a major barrier to the development of effective diagnostic tools and interventions (surgical and therapeutic). This study sought to 1) develop a genetically-modified porcine model of cancer expressing a TP53 mutation commonly found in humans (R175H in people, R167H in pigs), 2) validate the cellular p53 mutation and 3) evaluate tumor development in the animals using medical imaging, histopathology and molecular approaches. TP53R167H/R167H mutant pigs primarily developed lymphomas and osteogenic tumors, mimicking the tumor types observed in mice and humans expressing the orthologous TP53 mutant allele. CT and MRI imaging data effectively detected developing tumors, which were validated by histopathologic evaluation following necropsy. Molecular genetic analyses confirmed mutant p53 expression and characteristic chromosomal instability within the tumors. In conclusion, TP53R167H/R167H pigs provide a novel large animal tumor model that replicates the human condition and is uniquely suited to developing clinically-relevant, non-invasive imaging approaches to facilitate earlier detection, diagnosis and treatment of human cancers. Citation Format: Jessica C. Sieren, Xiao-Jun Wang, Bryan Davis, John D. Newell, Emily Hammond, Judy Rohret, Frank Rohret, Jason Struzynski, Adam Goeken, Paul Naumann, Mariah Leidinger, Jussara Hagen, Richard Van Rheeden, Benjamin W. Darbro, Dawn E. Quelle, David K. Meyerholz, Christopher S. Rogers. Translational imaging of tumorigenesis in a TP53 porcine cancer model. [abstract]. In: Proceedings of the 105th Annual Meeting of the American Association for Cancer Research; 2014 Apr 5-9; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2014;74(19 Suppl):Abstract nr LB-162. doi:10.1158/1538-7445.AM2014-LB-162

Published

2014

31. Sa.50. Inhibitory Oligodeoxynucleotide (ODN) Activity in Human B Cells

Author

Adam Goeken, Petar Lenert, and Robert F. Ashman

Subjects

Immunology, Immunology and Allergy, Inhibitory postsynaptic potential, Molecular biology

Published

2008

32. Inhibitory oligonucleotide (IN-ODN) structure-function relationships: species and backbone differences (131.19)

Author

Robert F. Ashman, Adam Goeken, and Petar Lenert

Subjects

Immunology, Immunology and Allergy

Abstract

The recognition of CpG motifs in bacterial DNA by Toll-like Receptor (TLR9) is a key function of the innate immune system, announcing the presence of an infection. We have previously developed synthetic oligonucleotide (ODN) inhibitory of TLR9 function with phosphorothioate (S) backbones conforming to the sequence n CC n not C not C nn GGG nnnn where n is any base. Here we show that these sequence requirements generate IN-ODN when the backbone is phosphodiester (O) also. In general, whereas stimulatory O-ODN are 2 logs less potent than their S-backbone congeners IN-ODN are 3 logs less potent. Changes in the critical bases diminish activity with either backbone; however, when the backbone is S, such changes diminish activity of stimulators much less, and inhibitors much more, than if the backbone is O. Certain end truncations enhance activity and even the minimal sequence CCTGGAGGG retains substantial inhibitory activity. Human-mouse relative activity comparisons tend to be similar between critical base variants, but may differ substantially between end truncation variants. HEK cells transfected with mouse or human TLR9 and an NFkB binding luciferase promoter respond to much lower concentrations of IN-ODN than do primary cells of either species. The neutral sequences with S backbones developed for mouse cells are also neutral with O backbones and with human cells. Supported by AI04737405 from NIH

Published

2007

33. Su.77. Relevance of Backbone, Species and TLR9-Expressing Cell Type for Cpg Oligonucleotide Action

Author

Robert F. Ashman, Adam Goeken, and Petar Lenert

Subjects

Genetics, Cell type, CPG-oligonucleotide, Action (philosophy), Immunology, Immunology and Allergy, TLR9, Relevance (information retrieval), Biology

Published

2006

34. Sequence requirements for oligodeoxyribonucleotide inhibitory activity.

Author

Robert F. Ashman, J. Adam Goeken, Jennifer Drahos, and Petar Lenert

Subjects

DENDRITIC cells, ANTIGEN presenting cells, APOPTOSIS, CELL death

Abstract

Inhibitory oligonucleotides (IN-ODN) differing from stimulatory CpG ODN (ST-ODN) by as few as two bases can block ST-ODN-induced proliferation, apoptosis protection and IL-6 secretion in B lymphocytes and the production of IL-12p40 by non-B cells. The main objective of this study was to determine the ODN sequence requirements for inhibition in mice. Starting with a strongly inhibitory 15-mer prototype phosphorothioate sequence, we tested the 60 sequences that differed from the prototype by one base, revealing the three areas that are critical for activity. Between these areas were the spacer sequences where base composition mattered little, but the number of bases was important. Truncation of three bases at the 3' end of the 15-mer and one at the 5' end was tolerated with minimal loss of activity. This approach yielded an optimal sequence of 5' CC x notC notC xxGGGx or CC x notC notC xGGGxx 3', where x is any base. The sequence requirements for optimal inhibition of B cell responses to Type B (K) ODN and mixed splenocyte IL-12p40 responses to Type A (D) ODN were strikingly similar. Inhibition of ST-ODN by IN-ODN was competitive. A hypothetical model of the ODN-binding site is proposed. Synthetic IN-ODN with the sequence characteristics defined here should provide antidotes for excessive innate reactions to DNA. [ABSTRACT FROM AUTHOR]

Published

2005

35. Lack of airway submucosal glands impairs respiratory host defenses

Author

Lynda S Ostedgaard, Margaret P Price, Kristin M Whitworth, Mahmoud H Abou Alaiwa, Anthony J Fischer, Akshaya Warrier, Melissa Samuel, Lee D Spate, Patrick D Allen, Brieanna M Hilkin, Guillermo S Romano Ibarra, Miguel E Ortiz Bezara, Brian J Goodell, Steven E Mather, Linda S Powers, Mallory R Stroik, Nicholas D Gansemer, Camilla E Hippee, Keyan Zarei, J Adam Goeken, Thomas R Businga, Eric A Hoffman, David K Meyerholz, Randall S Prather, David A Stoltz, and Michael J Welsh

Subjects

sus scrofa, host defense, lung, Medicine, Science, Biology (General), QH301-705.5

Abstract

Submucosal glands (SMGs) are a prominent structure that lines human cartilaginous airways. Although it has been assumed that SMGs contribute to respiratory defense, that hypothesis has gone without a direct test. Therefore, we studied pigs, which have lungs like humans, and disrupted the gene for ectodysplasin (EDA-KO), which initiates SMG development. EDA-KO pigs lacked SMGs throughout the airways. Their airway surface liquid had a reduced ability to kill bacteria, consistent with SMG production of antimicrobials. In wild-type pigs, SMGs secrete mucus that emerges onto the airway surface as strands. Lack of SMGs and mucus strands disrupted mucociliary transport in EDA-KO pigs. Consequently, EDA-KO pigs failed to eradicate a bacterial challenge in lung regions normally populated by SMGs. These in vivo and ex vivo results indicate that SMGs are required for normal antimicrobial activity and mucociliary transport, two key host defenses that protect the lung.

Published

2020

36. NIAM-deficient mice are predisposed to the development of proliferative lesions including B-cell lymphomas.

Author

Sara M Reed, Jussara Hagen, Viviane P Muniz, Timothy R Rosean, Nick Borcherding, Sebastian Sciegienka, J Adam Goeken, Paul W Naumann, Weizhou Zhang, Van S Tompkins, Siegfried Janz, David K Meyerholz, and Dawn E Quelle

Subjects

Medicine, Science

Abstract

Nuclear Interactor of ARF and Mdm2 (NIAM, gene designation Tbrg1) is a largely unstudied inhibitor of cell proliferation that helps maintain chromosomal stability. It is a novel activator of the ARF-Mdm2-Tip60-p53 tumor suppressor pathway as well as other undefined pathways important for genome maintenance. To examine its predicted role as a tumor suppressor, we generated NIAM mutant (NIAM(m/m)) mice homozygous for a β-galactosidase expressing gene-trap cassette in the endogenous gene. The mutant mice expressed significantly lower levels of NIAM protein in tissues compared to wild-type animals. Fifty percent of aged NIAM deficient mice (14 to 21 months) developed proliferative lesions, including a uterine hemangioma, pulmonary papillary adenoma, and a Harderian gland adenoma. No age-matched wild-type or NIAM(+/m) heterozygous animals developed lesions. In the spleen, NIAM(m/m) mice had prominent white pulp expansion which correlated with enhanced increased reactive lymphoid hyperplasia and evidence of systemic inflammation. Notably, 17% of NIAM mutant mice had splenic white pulp features indicating early B-cell lymphoma. This correlated with selective expansion of marginal zone B cells in the spleens of younger, tumor-free NIAM-deficient mice. Unexpectedly, basal p53 expression and activity was largely unaffected by NIAM loss in isolated splenic B cells. In sum, NIAM down-regulation in vivo results in a significant predisposition to developing benign tumors or early stage cancers. These mice represent an outstanding platform for dissecting NIAM's role in tumorigenesis and various anti-cancer pathways, including p53 signaling.

Published

2014