Your search keyword '"J. von Seggern"' showing total 15 results

1. Investigate-Design-Practice-Reflect: An Iterative Community-Engaged Action Process to Improve Population Health

Author

Rosen, Marisa S., Rogers, Ann E., J. Von Seggern, Mary, Grimm, Brandon L., Ramos, Athena K., Schenkelberg, Michaela A., Idoate, Regina E., and Dzewaltowski, David A.

Published

2024

2. Sociodemographic influences on youth sport participation and physical activity among children living within concentrated Hispanic/Latino rural communities

Author

Mary J. Von Seggern, Ann E. Rogers, Michaela A. Schenkelberg, Debra K. Kellstedt, Gregory J. Welk, Robin High, and David A. Dzewaltowski

Subjects

child/children, physical activity, rural, youth sport, Hispanic/Latino, health disparities, Public aspects of medicine, RA1-1270

Abstract

IntroductionLack of physical activity (PA) among children living in rural communities is a documented public health problem. Although studies have examined community conditions defined by a rural–urban dichotomy, few have investigated rural community conditions with a concentration of Hispanic/Latino people. This cross-sectional study examined sociodemographic characteristics associated with youth sport (YS) participation and daily PA among children living within concentrated Hispanic/Latino rural U.S. Midwest communities.MethodsDuring spring 2022, 97% of 3rd–6th grade children (n = 281, aged approximately 8–12 years) attending school in rural Midwestern communities (n = 2) with >50% concentration of Hispanic students participated in the Wellscapes Project, a community randomized trial. Participants completed the Youth Activity Profile and supplemental National Survey of Children’s Health questions assessing PA behaviors and YS participation. Caregivers of a subsample of children (n = 215; males, n = 93; females, n = 122) consented to pair their child’s survey results with school enrollment records (e.g., free/reduced lunch status and race and ethnicity). Mixed models with community as a random effect examined main and interaction effects of grade, sex, ethnoracial status, and family income on YS participation and these sociodemographic characteristics and YS participation on daily moderate-to-vigorous PA (MVPA).ResultsApproximately half of children participated in YS. Non-Hispanic White children (n = 82) were over five times more likely to participate in YS than Hispanic peers (n = 133) (OR = 5.54, 95% CI = 2.64–11.61, p

Published

2024

3. COVID-19 pandemic and changes in children’s physical activity in a rural US community: a mixed methods study

Author

Richard R Rosenkranz, Gregory J Welk, Debra K Kellstedt, Ann M Essay, Michaela A Schenkelberg, Marisa S Rosen, Mary J Von Seggern, Regina Idoate, and David A Dzewaltowski

Subjects

Medicine

Abstract

Objectives To examine differences in rural community children’s moderate-to-vigorous physical activity (MVPA) and participation in out-of-school activities from fall 2019 to fall 2020 and explore enacted PA opportunity modifications post initial COVID-19 disruption.Design Mixed methods study using the validated Youth Activity Profile (YAP), administrator reports and stakeholder surveys and semistructured interviews.Setting Children and community stakeholders from one rural US Great Plains community in the state of Nebraska were recruited.Participants Third through fifth graders in fall 2019 (n=144) and fall 2020 (n=174) reported MVPA and participation in out-of-school activities using the YAP. School administrators reported weekly physical education (PE) and recess minutes. Community stakeholders reported pandemic-related changes in community social structures in semistructured interviews (n=4) and surveys (n=19).Results Average daily MVPA minutes increased from 2019 to 2020 (75.0 vs 81.3, SE=1.6, p

Published

2022

4. Youth sport participation and physical activity in rural communities

Author

Debra K. Kellstedt, Michaela A. Schenkelberg, Ann M. Essay, Mary J. Von Seggern, Richard R. Rosenkranz, Gregory J. Welk, Robin High, and David A. Dzewaltowski

Subjects

Physical activity, Rural, Youth sport, Health equity, Public aspects of medicine, RA1-1270

Abstract

Abstract Background Physical activity, a high-frequency health behavior, varies by where children live, learn, and play. Children accumulate physical activity in adult-led in-school and out-of-school settings. Youth sport is a potential setting for physical activity, but there are differences in youth sport participation based on age, sex, and socioeconomic status. There is a gap in understanding demographic influences on youth sport participation and how these factors interact to influence physical activity. This study examines influences of grade, sex, and family income on youth sport participation and these factors and youth sport participation on moderate-to-vigorous physical activity of children in rural communities. Methods Children (n = 418 3rd–6th graders) living in two rural communities completed the online Youth Activity Profile as part of Wellscapes, a type 3 hybrid implementation-effectiveness community randomized trial. Mixed models with community as a random effect examined main effects and interactions of grade, sex, and family income on youth sport participation and these factors and youth sport participation on moderate-to-vigorous physical activity. Results About 80% of children engaged in youth sport, and full-pay lunch students were almost four times more likely to have youth sport participation than students with free/reduced lunch (OR = 3.91, 95% CI = 1.95, 7.8). Females and 6th graders (p

Published

2021

5. Development of Renal-targeted Vectors Through Combined In Vivo Phage Display and Capsid Engineering of Adenoviral Fibers From Serotype 19p

Author

Eugene Wu, Stuart A. Nicklin, Lorraine M. Work, Andrew H. Baker, John H. McVey, Laura Denby, and Dan J. Von Seggern

Subjects

Male, Phage display, Genetic Vectors, Molecular Sequence Data, Gene delivery, Biology, Kidney, medicine.disease_cause, Virus, Adenoviridae, Mice, Transduction (genetics), Peptide Library, Drug Discovery, Genetics, medicine, Animals, Amino Acid Sequence, Serotyping, Molecular Biology, Tropism, Pharmacology, Sequence Homology, Amino Acid, Gene Transfer Techniques, Immunohistochemistry, Virology, Capsid, Pseudotyping, Molecular Medicine, Capsid Proteins

Abstract

The potential efficacy of gene delivery is dictated by the infectivity profile of existing vectors, which is often restrictive. In order to target cells and organs for which no efficient vector is currently available, a promising approach would be to engineer vectors with novel transduction profiles. Applications that involve injecting adenovirus (Ad) vectors into the bloodstream require that native tropism for the liver be removed, and that targeting moieties be engineered into the capsid. We previously reported that pseudotyping the Ad serotype 5 fiber for that of Ad19p results in reduced hepatic transduction. In this study we show that this may be caused, at least in part, by a reduction in the capacity of the Ad19p-based virus to bind blood coagulation factors. It is therefore a potential candidate for vector retargeting, focusing on the kidney as a therapeutic target. We used in vivo phage display in rats, and identified peptides HTTHREP and HITSLLS that homed to the kidneys following intravenous injection. We engineered the HI loop of Ad19p to accommodate peptide insertions and clones. Intravenous delivery of each peptide-modified virus resulted in selective renal targeting, with HTTHREP and HITSLLS-targeted viruses selectively transducing tubular epithelium and glomeruli, respectively. Our study has important implications for the use of genetic engineering of Ad fibers to produce targeted gene delivery vectors.

Published

2007

6. In vitro dendritic cell infection by pseudotyped adenoviral vectors does not correlate with their in vivo immunogenicity

Author

Dan J. Von Seggern, Glen R. Nemerow, P. Frosst, Catherine Hsu, Megan M. Boysen, and Lance D. Gritton

Subjects

Antigen Presentation, Mice, Inbred BALB C, Immunogenicity, Genetic enhancement, T cell, Genetic Vectors, Gene Transfer Techniques, Bone Marrow Cells, Dendritic cell, Dendritic Cells, Gene delivery, Biology, Virology, Adenoviridae, Mice, Immune system, medicine.anatomical_structure, Antigen, In vivo, medicine, Animals

Abstract

Expression of antigens in dendritic cells (DC) can stimulate protective immunity against both viral infection and tumor growth, making them important targets for gene therapy. In-vitro-generated DC are commonly used in gene delivery studies with the assumption that the results will correlate with in vivo activity. Adenovirus Type 5 (Ad5) vectors have been widely used with DC, but these cells lack the primary receptor (CAR) used by Ad5 and are poorly infected. We investigated the use of Ad5 vector particles pseudotyped with fibers from other Ad serotypes in DC targeting. Several fiber proteins, including those from Ad16 (Subgroup B) and Ad37 (Subgroup D), conferred dramatically increased in vitro infection. Surprisingly, neither dendritic cell infection nor the immune response to an Ad-delivered antigen was improved when the modified viruses were tested in vivo. These results underscore the importance of using appropriate animal models in gene delivery studies.

Published

2005

7. Adenoviral Serotype 5 Vectors Pseudotyped with Fibers from Subgroup D Show Modified Tropism In Vitro and In Vivo

Author

Laura Denby, Lorraine M. Work, Delyth Graham, Catherine Hsu, Dan J. von Seggern, Stuart A. Nicklin, and Andrew H. Baker

Subjects

Genetics, Molecular Medicine, Molecular Biology

Published

2004

8. Development of Efficient Viral Vectors Selective for Vascular Smooth Muscle Cells

Author

Dan J. Von Seggern, Nick J.R. Brain, Hildegard Büning, Lorraine M. Work, Stuart A. Nicklin, Michael Hallek, Kate L. Dishart, and Andrew H. Baker

Subjects

Proteasome Endopeptidase Complex, Phage display, Vascular smooth muscle, viruses, Transgene, Genetic Vectors, Cell, Gene delivery, Biology, Protein Engineering, medicine.disease_cause, Muscle, Smooth, Vascular, Adenoviridae, Viral vector, Transduction (genetics), Multienzyme Complexes, Peptide Library, Drug Discovery, Genetics, medicine, Humans, Saphenous Vein, Molecular Biology, Adeno-associated virus, Cells, Cultured, Pharmacology, Heparin, Dependovirus, Virology, Cell biology, Cysteine Endopeptidases, Protein Transport, medicine.anatomical_structure, Organ Specificity, cardiovascular system, Molecular Medicine, Capsid Proteins, Peptides

Abstract

The vascular smooth muscle cell (SMC) is integral to the pathogenesis of neointimal formation associated with late vein graft failure, in-stent restenosis, and transplant arteriopathy. Viral vectors transduce SMC with low efficiency and hence, there is a need for improvement. We aimed to enhance the efficiency and selectivity of gene delivery to human SMC. Targeting ligands were identified using phage display on primary human saphenous vein SMC with linear and cyclic libraries. Two linear peptides, EYHHYNK (EYH) and GETRAPL (GET), were incorporated into the HI loop of adenovirus (Ad) fibers and the capsid protein of adeno-associated virus-2 (AAV-2). Exposure of human venous SMC to EYH-modified (but not the GET-modified) Ad vector resulted in a significant increase in transgene expression levels at short, clinically relevant exposure times. Similarly, the EYH-modified AAV vector resulted in enhanced gene transfer to human venous SMC but not endothelial cells in a time- and dose-dependent manner. The EYH-modified AAV vector also enhanced (up to 70-fold) gene delivery to primary human arterial SMC. Hence, incorporation of EYH into Ad and AAV capsids resulted in a significant and selective enhancement in transduction of SMC and has implications for improving local gene delivery to the vasculature.

Published

2004

9. In vivo transduction of photoreceptors or ciliary body by intravitreal injection of pseudotyped adenoviral vectors

Author

Glen R. Nemerow, Susan C. Stevenson, Shonna Kaye Fleck, Edith Aguilar, Dan J. Von Seggern, J.C Gonzalez Armas, Martin Friedlander, Karen Kinder, and Peter Ghazal

Subjects

Cell type, genetic structures, Transgene, Genetic Vectors, Biology, Gene delivery, medicine.disease_cause, Adenoviridae, Mice, Transduction (genetics), Ciliary body, Transduction, Genetic, In vivo, Drug Discovery, Genetics, medicine, Animals, Molecular Biology, Pharmacology, Mice, Inbred BALB C, Retina, Ciliary Body, Virology, eye diseases, Cell biology, Vitreous Body, medicine.anatomical_structure, Molecular Medicine, Female, Photoreceptor Cells, Vertebrate

Abstract

Strategies for retargeting adenoviral (Ad) vectors have been developed, but their in vivo efficacy remains to be demonstrated. Gene delivery to specific ocular cell types represents an approach to treating many diseases that cause irreversible blindness. One of these cell types, the photoreceptor (PR), is not infected by standard Ad5-based vectors. We evaluated gene delivery after intraocular injection of Ads pseudotyped with three different fiber proteins and found three distinct patterns of infection. An intravitreally injected Ad5 vector readily infected the iris, corneal endothelium, and ciliary body, while few cells in the retina expressed transgene product. In contrast, an Ad3-pseudotyped virus selectively transduced ciliary body, of interest for treating diseases such as glaucoma. A vector pseudotyped with the fiber protein of Ad37 transduced PRs as well as ciliary body. This finding has potential application to the treatment of retinal degenerative or neovascular diseases. These studies demonstrate cell type-selective gene delivery in vivo with retargeted Ads, provide information about the cellular tropisms of several Ad serotypes, and should lead to improved strategies for preserving vision.

Published

2003

10. Signaling antibodies complexed with adenovirus circumvent CAR and integrin interactions and improve gene delivery

Author

G B Brown, Swati L. Brown, D J Von Seggern, Erguang Li, and Glen R. Nemerow

Subjects

Insecta, Recombinant Fusion Proteins, media_common.quotation_subject, Genetic Vectors, Integrin, Gene Expression, Gene delivery, Transfection, medicine.disease_cause, Adenoviridae, Growth factor receptor, Antigens, CD, Neoplasms, Tumor Cells, Cultured, Genetics, medicine, Animals, Humans, Enzyme Inhibitors, Insulin-Like Growth Factor I, Internalization, Melanoma, Molecular Biology, Phosphoinositide-3 Kinase Inhibitors, media_common, Epidermal Growth Factor, biology, Tumor Necrosis Factor-alpha, Genetic Therapy, Integrin alphaV, beta-Galactosidase, Molecular biology, Cell biology, Recombinant Growth Factor, Androstadienes, Enzyme Activation, biology.protein, Receptors, Virus, Molecular Medicine, Signal transduction, Colorectal Neoplasms, Genetic Engineering, Wortmannin, Signal Transduction

Abstract

Current adenoviral (Ad) vectors cannot be targeted to specific cell types due to the widespread distribution of the Ad receptor (CAR). Moreover, CAR and/or internalization receptors (alphav integrins) are absent or present at low levels on some cell types, rendering them resistant to Ad-mediated gene delivery. To address these problems, we have developed a novel vector targeting approach that takes advantage of the common cell signaling pathways initiated by ligation of alphav integrins and growth factor receptors. Recombinant growth factor/cytokines (TNF-alpha, IGF-1, EGF) which trigger phosphatidylinositol-3-OH kinase (PI3K) activation, a signaling molecule involved in adenovirus internalization, were fused to a monoclonal antibody specific for the viral penton base. Ad vectors complexed with these bifunctional mAbs increased gene delivery 10 to 50-fold to human melanoma cells lacking alphav integrins. The bifunctional mAbs also enhanced gene delivery by fiberless adenovirus particles which cannot bind to CAR. Improved gene delivery correlated with increased virus internalization and attachment as well as PI3K activity. The use of bifunctional mAbs to trigger specific cell signaling pathways offers a widely applicable method for bypassing the normal Ad receptors in gene delivery and potentially increasing the selectivity of gene transfer.

Published

2000

11. In vitro and in vivo characterisation of endothelial cell selective adenoviral vectors.

Author

Stuart A. Nicklin, Steve J. White, Campbell G. Nicol, Dan J. Von Seggern, and Andrew H. Baker

Abstract

Both viral and non-viral gene transfer vectors transduce vascular endothelial cells (EC) with low efficiency compared with other cell types such as hepatocytes. Generation of EC-selective vectors would enhance the clinical utility of gene therapy for diverse vascular-targeted applications. 12mer peptides derived by in vitro phage display with EC binding specificity [MTPFPTSNEANL (MTP) and MSLTTPPAVARP (MSL)] were inserted at position T542 in the exposed HI loop of the adenovirus (Ad) serotype 5 fiber using overlapping oligonucleotides; in combination with a double point mutation (KO1) to ablate virus : cell binding via the coxsackie-adenovirus receptor (CAR). The resulting modified viruses were tested in vitro and in vivo for their ability to direct endothelial-specific gene transfer. Peptide insertion was not deleterious to fiber trimerisation or virion maturation. In vitro gene transfer studies using a panel of cell types demonstrated that both peptide-targeted Ad vectors mediated efficient CAR-independent gene transfer to vascular EC compared with non-modified Ads. Neither peptide supported gene delivery to non-EC. Upon systemic injection into mice and subsequent evaluation of transgene expression we failed to observe a reduction in hepatic Ad accumulation but observed a significant elevation in β-galactosidase in blood vessels with the MSLTTPPAVARP-targeted Ad vector. We have genetically engineered two novel Ads that transduce human EC selectively in vitro, one of which leads to altered Ad biodistribution in vivo. The successful generation of genetically engineered tropism for EC has broad implications for cardiovascular gene therapy. Further modifications to the Ad capsid will be required to improve in vivo biodistribution profiles. Copyright © 2004 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2004

12. A residual gas analyzer compatible with reactive and radioactive gases

Author

J. von Seggern, W. O. Hofer, M. Erdweg, and S. Berger

Subjects

Residual gas analyzer, Spectrometer, Chemistry, Nuclear engineering, Analytical chemistry, food and beverages, Surfaces and Interfaces, Partial pressure, equipment and supplies, Condensed Matter Physics, humanities, Particle detector, Gas analyzer, Surfaces, Coatings and Films, Gas analysis, High dynamic range

Abstract

A conventional residual gas analyzer was equipped with an ion‐electron converter as particle detector and tested in tritium‐containing environments. Substantial advantages can be asserted for this setup: high dynamic range, easy regenerability by baking without detrimental effects on the multiplier, insensitivity to exposure to reactive gases, and inexpensive replacement.

Published

1984

13. The beryllium limiter experiment in ISX-B

Author

Alan J Wootton, P.H. Edmonds, A.C. England, P.K. Mioduszewski, P.E. Stott, G.H. Neilson, W.A. Gabbard, C.E. Bush, R. A. Langley, P.D. Morgan, James B. Roberto, K.H. Behringer, C. H. Ma, C. E. Thomas, A. Carnevali, R. E. Clausing, D.H.J. Goodall, R. B. Clayton, J. von Seggern, E. A. Lazarus, N. J. Peacock, M. Murakami, J. G. Dietz, R.A. Zuhr, R. D. Watson, L.C. Emerson, J. E. Simpkins, R.R. Kindsfather, K.G. Tschersich, A. Tanga, P. J. Lomas, R.C. Isler, T.B. Cook, K. Yokoyama, J.B. Whitley, L. Heatherly, J.G. Watkins, K.H. Sonnenberg, E. Källne, P.W. King, D. P. Hutchinson, and M.F. Smith

Subjects

Nuclear and High Energy Physics, Tokamak, Materials science, Hydrogen, Nuclear engineering, Evaporation, chemistry.chemical_element, Plasma, Condensed Matter Physics, respiratory tract diseases, law.invention, chemistry, Getter, law, Impurity, Limiter, Beryllium

Abstract

An experiment to test beryllium as a limiter material has been performed in the ISX-B tokamak. The effect of the plasma on the limiter and the effect of the limiter on the plasma were studied in detail. Heat and particle fluxes to the limiter were measured, and limiter damage by melting was documented as a function of power flux. Strong melting and evaporation of the limiter caused beryllium gettering of the vacuum vessel. Postmortem analysis of the limiter was performed to document the amount of retained hydrogen and the erosion and impurity deposition on the limiter. The effect of the limiter on the plasma performance was studied in terms of parameter space, impurity content, and confinement for the ungettered and gettered cases. Operational experience with beryllium in a fusion experiment is discussed.

Published

1986

14. Cleanup and gettering during the Beryllium Limiter Experiment in Impurity Study Experiment‐B

Author

K.G. Tschersich, R.C. Isler, R. E. Clausing, P.K. Mioduszewski, J. von Seggern, J. E. Simpkins, L. Heatherly, and R.A. Zuhr

Subjects

Alkaline earth metal, Tokamak, Materials science, Radiochemistry, Metallurgy, chemistry.chemical_element, Surfaces and Interfaces, Condensed Matter Physics, respiratory tract diseases, Surfaces, Coatings and Films, law.invention, chemistry, law, Impurity, Getter, Limiter, Beryllium, Surface finishing, Titanium

Abstract

Changes in plasma impurities and radiated power due to cleanup and gettering during the Beryllium Limiter Experiment are related to changes of the surface composition of the torus walls and residual gases in the torus. Pulse discharge cleaning was very effective in cleaning the ISX‐B vacuum vessel after installation of the beryllium limiter. As a result of discharge cleaning, areas near the limiter were soon covered with a beryllium rich deposit containing some iron, nickel, chromium, and titanium as well as oxygen, carbon, sulfur, and nitrogen. Oxygen levels on the wall were reduced to below 10 at. %. Materials transport during discharge cleaning was apparently due to sputtered neutrals. Evaporation of beryllium from the limiter and subsequent deposition on the torus walls caused by high power tokamak shots produced gettering of the machine equal or better than that previously obtained with titanium or chromium. This gettering by beryllium eliminated the need for further discharge cleaning or other gette...

Published

1986

15. Summary Abstract: Cleanup and gettering during the Beryllium Limiter Experiment in the Impurity Study Experiment‐B

Author

J. E. Simpkins, J. von Seggern, R. E. Clausing, R.C. Isler, L. Heatherly, R.A. Zuhr, P.K. Mioduszewski, and K.G. Tschersich

Subjects

Materials science, chemistry, Getter, Impurity, Metallurgy, Radiochemistry, Limiter, chemistry.chemical_element, Surfaces and Interfaces, Beryllium, Condensed Matter Physics, Surfaces, Coatings and Films

Published

1986