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2. Assessing the Relative Importance of Satellite-Detected Methane Superemitters in Quantifying Total Emissions for Oil and Gas Production Areas in Algeria

Author

Naus, S., primary, Maasakkers, J. D., additional, Gautam, R., additional, Omara, M., additional, Stikker, R., additional, Veenstra, A. K., additional, Nathan, B., additional, Irakulis-Loitxate, I., additional, Guanter, L., additional, Pandey, S., additional, Girard, M., additional, Lorente, A., additional, Borsdorff, T., additional, and Aben, I., additional

Published
2023
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5. Methyl Chloroform Continues to Constrain the Hydroxyl (OH) Variability in the Troposphere

Author

Patra, P.K., Krol, M.C., Prinn, R.G., Takigawa, M., Mühle, J., Montzka, S.A., Lal, S., Yamashita, Y., Naus, S., Chandra, N., Weiss, R.F., Krummel, P.B., Fraser, P.J., O'Doherty, S., Elkins, J.W., Patra, P.K., Krol, M.C., Prinn, R.G., Takigawa, M., Mühle, J., Montzka, S.A., Lal, S., Yamashita, Y., Naus, S., Chandra, N., Weiss, R.F., Krummel, P.B., Fraser, P.J., O'Doherty, S., and Elkins, J.W.

Abstract

Trends and variability in tropospheric hydroxyl (OH) radicals influence budgets of many greenhouse gases, air pollutant species, and ozone depleting substances. Estimations of tropospheric OH trends and variability based on budget analysis of methyl chloroform (CH3CCl3) and process-based chemistry transport models often produce conflicting results. Here we use a previously tested transport model to simulate atmospheric CH3CCl3 for the period 1985–2018. Based on mismatches between model output and observations, we derive consistent anomalies in the inverse lifetime of CH3CCl3 (KG) using measurements from two independent observational networks (National Oceanic and Atmospheric Administration and Advanced Global Atmospheric Gases Experiment). Our method allows a separation between “physical” (transport, temperature) and “chemical” (i.e., abundance) influences on OH + CH3CCl3 reaction rate in the atmosphere. Small increases in KG due to “physical” influences are mostly driven by increases in the temperature-dependent reaction between OH and CH3CCl3 and resulted in a smoothly varying increase of 0.80% decade−1. Chemical effects on KG, linked to global changes in OH sources and sinks, show larger year-to-year variations (∼2%–3%), and have a negative correlation with the El Niño Southern Oscillation. A significant positive trend in KG can be derived after 2001, but it persists only through 2015 and only if we assume that CH3CCl3 emissions decayed more slowly over time than our best estimate suggests. If global CH3CCl3 emissions dropped below 3 Gg year−1 after 2015, recent CH3CCl3 measurements indicate that the 2015–2018 loss rate of CH3CCl3 due to reaction with OH is comparable to its value 2 decades ago.

Published
2021

6. Methyl Chloroform Continues to Constrain the Hydroxyl (OH) Variability in the Troposphere

Author

Patra, P. K., primary, Krol, M. C., additional, Prinn, R. G., additional, Takigawa, M., additional, Mühle, J., additional, Montzka, S. A., additional, Lal, S., additional, Yamashita, Y., additional, Naus, S., additional, Chandra, N., additional, Weiss, R. F., additional, Krummel, P. B., additional, Fraser, P. J., additional, O'Doherty, S., additional, and Elkins, J. W., additional

Published
2021
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7. The isotopic composition of CO in car exhaust

Author

Naus, S., Röckmann, T. (Thesis Advisor), Popa, E., Naus, S., Röckmann, T. (Thesis Advisor), and Popa, E.

Abstract

In this study, the isotopic composition of CO and of CO$_2$ and the CO:CO$_2$, CH$_4$:CO$_2$ and H$_2$:CO gas ratios in the exhaust of individual cars were investigated. This was done under idling and revving conditions, and for three cars in a full driving cycle on a test bench. The spread in the results, even within a single car, was large: for \delc in CO $\sim$ 0 to -60 \textperthousand, for \delo in CO $\sim$ +20 to +35 \textperthousand, and for all gas ratios several orders of magnitude. The results show an increase in the spread of isotopic values for CO compared to previous studies, suggesting that increasing complexity of emission regulations in cars might be reflected in the isotopic composition. When including all samples, we find a weighted mean for the \delc and \delo in CO of -28.7 $\pm$ 0.5 \perm \ and 24.8 $\pm$ 0.3 \perm \ respectively. This result is dominated by cold petrol cars. Our results suggest that in driving cycles where cold emissions are less important, both \delc and \delo would be expected to increase, which would result in isotopic values more in line with previous studies. For the H$_2$:CO ratio, averaged over all cars, we found a value of 0.71 $\pm$ 0.31 ppb:ppb, in agreement with previous literature. The CO:CO$_2$ ratio, with a mean of 19.4 $\pm$ 6.8 ppb:ppm, and the CH$_4$:CO$_2$ ratio, with a mean of 0.26 $\pm$ 0.05 ppb:ppm, are both higher than is reported in recent literature. This is likely because our sampling distribution was biased towards cold cars, and therefore towards higher emission situations. In many ways the CH$_4$:CO$_2$ ratio was found to behave similarly to the CO:CO$_2$ ratio, suggesting that the processes affecting CO and CH$_4$ are similar. Diesel cars behaved as a distinct group, with CO enriched in $^{13}$C and depleted in $^{18}$O compared to petrol cars. CO emissions from cold diesel cars were found to be significant, but reduced sharply in hot diesel cars. The \delc values in CO$_2$ were close to the \delc

Published
2016

8. Machbarkeitsprüfung und Qualitätsentwicklung zur Gewinnung von Biomaterialien in den Pretest-Studien der Deutschen Nationalen Kohorte

Author

Kühn, A., Nieters, Alexandra, Köttgen, Anna, Goek, Oemer Necmi, Michels, K., Nöthlings, Ute, Jacobs, G., Meisinger, Christa, Pessler, Frank, Akmatov, M. F., Kühnisch, Jan, Moebus, Susanne, Glocker, E., Naus, S., Keimling, M., Leitzmann, Michael Fred, Linseisen, Jakob P., Sarioglu, H., Von Toerne, C., Hauck, S. M., Wallaschofski, Henri, Wichmann, Hans Erich, and Illig, T.

Subjects
Medizin
Abstract

Hintergrund Ein Hauptziel der Nationalen Kohorte ist es, Volkskrankheiten, wie z. B. Krebs, Diabetes, Infektions-, allergische, neurologische oder Herz-Kreislauf-Erkrankungen auf unterschiedlichen Ebenen besser zu verstehen: Es sollen Risikofaktoren für die Entstehungen dieser Erkrankungen identifiziert und Biomarker für ihre Früherkennung sowie präventive Maßnahmen entwickelt werden. Die Sammlung von Biomaterialien in Kombination mit Fragebogendaten und medizinischen Untersuchungen bilden wesentliche Komponenten der Studie. Ziel der Arbeit In 2 Pretest-Studien wurden zwischen 2011 und 2013 Biomaterialien von einer definierten Anzahl an Probanden gesammelt, um die Machbarkeit einer solchen Sammlung und die Probenqualität zu testen. In den Pretest 1 waren 10 und in den Pretest 2 18 Studienzentren involviert. Standardarbeitsanweisungen (SOPs) wurden entwickelt und evaluiert, um präanalytische Artefakte während der Probengewinnung zu minimieren. Während der 2 Pretest-Studien war die Überprüfung der Aspekte Machbarkeit der Probensammlung und -präparation sowie Qualitätskontrolle von Biomarker und Proteom wesentlich. Zudem wurden die Rekrutierung von Studienteilnehmern für spezifische Projekte und die Untersuchungsabläufe in allen teilnehmenden Studienzentren in einer bestimmten Zeit mit Blick auf die gemeinsamen Standards (Teil 2) getestet sowie Tests zum Transport und zur dezentralisierten Lagerung von biologischen Proben durchgeführt. Die Pretest-Studien dienen als Basis für die Biomaterialiensammlung in der Hauptstudie der Nationalen Kohorte, die 2014 startet. Material und Methoden Zufällig aus der Bevölkerung ausgewählte Teilnehmer (im Pretest I n = 1000, in 10 Studienzentren rekrutiert) wurden gebeten, Blut-, Urin-, Speichel- und Stuhlproben zu spenden. Ferner wurden Nasen- und Rachenabstriche im Studienzentrum und von den Teilnehmern zu Hause gesammelt. SOPs für die Probensammlung, Probenverarbeitung, Lagerung und für den Transport der Proben wurden erarbeitet und nach dem Pretest 1 für Pretest 2 angepasst. Im Pretest 2 wurden von n = 599 Teilnehmern in 18 Studienzentren Biomaterialien nahezu identisch zum Vorgehen in Pretest 1 gesammelt. Anschließend wurden an den Proben molekulare Qualitätsanalysen durchgeführt. Ergebnisse In Pretest 1 und 2 konnten alle genannten Biomaterialien von fast allen eingeladenen Probanden gesammelt werden. Die durchschnittliche Teilnahme am Biomaterialienprogramm lag bei 95 %, alle entwickelten SOPs waren umsetzbar und nach kleinen Anpassungen und Modifikationen für die Hauptphase der Studie einsetzbar. Ein wesentliches Ergebnis war z. B., dass die Abtrennung der zellulären Blutfraktion vom Serum und Plasma innerhalb der ersten Stunde nach Blutabnahme erfolgen sollte, um signifikante Variationen bei den hier untersuchten Biomarkern zu vermeiden. Zudem zeigte die Qualitätskontrolle in einem Proteomics-Ansatz keine signifikante Zusammenlagerung von Proteinen bei verschiedenen Lagerungsbedingungen nach Blutentnahme. Zusätzlich wurden elektronische und manuelle (Papier-)Dokumentationsbögen entwickelt und getestet, um Zeitstempel, Volumina, Einfrierzeiten und Anzahl an Aliquoten der gesammelten Biomaterialien zu erfassen. Diskussion Die Sammlung der Biomaterialien war ohne größere Probleme an allen teilnehmenden Studienzentren möglich. In einigen Fällen waren allerdings die Prozesszeiten zu lang. Zur Vermeidung präanalytischer Artefakte bei der Probengewinnung ist eine gute Standardisierung wesentlich. Um dies zu erreichen, werden die Blut- und Urinverarbeitung an speziellen Bedingungen der Nutzung eines Liquid-Handling-Roboters ausgerichtet, der zur Hauptstudie an allen Studienzentren verfügbar sein wird. Die strikte Einhaltung der SOPs, eine intensive Schulung des Personals und eine exakte Dokumentation sind unerlässlich, um eine sehr gute Probenqualität für spätere Analysen zu erreichen. Diese Biomaterialien sind eine wichtige Quelle für die Infektionsforschung und die Erforschung anderer Volkskrankheiten.

Published
2014
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9. The energized monument

Author

Naus, S. (author) and Naus, S. (author)

Abstract

The goal of this graduation project is transforming monuments from +/- 1900 with a non-housing function to monuments with collective, near zero-energy housing. In this design the elements collective housing, near zero-energy and monument are combined at the Binnengasthuis area in Amsterdam. The project focuses on solutions in historic inner city centers that become more dense. Besides that it anticipates on finding a solution for reusing and creating more energy efficient monuments., Heritage & Housing, Heritage & Design, Architecture and The Built Environment

Published
2015

11. letters.

Author

Lake, Jordanna, Naus, S. K., Moore, Barbara, and Beaton, Joyce

Subjects
LETTERS to the editor, JEANS (Clothing), ORGANIC foods, HOUSEWIVES, HOMEMAKERS
Abstract

Several letters to the editor are presented in response to articles in previous issues, including "Blue Heaven," in the October 2006 issue, "Organic Versus Nonorganic Food" and "It's Your Floor, Too," by June Callwood.

Published
2007

12. Aging Alone in a Continuous Traumatic Situation: External Coping Resources.

Author

Hadida-Naus S, Spector-Mersel G, and Shiovitz-Ezra S

Abstract

Exposure to a persistent terrorist threat constitutes a continuous traumatic situation (CTS) that can severely impact one's mental and physical health. For older adults living in CTS, this risk is compounded by the challenges of aging. This vulnerability is significantly heightened for older adults living alone in CTS, who typically experience increased social isolation and loneliness. Past research has explored internal coping resources that help these individuals deal with their stressful circumstances. Nevertheless, external coping resources have been hardly explored, making it difficult to create policies and practices to support older adults living alone in areas affected by terrorism. To address this lacuna, we conducted semi-structured in-depth interviews with 15 older adults living alone in Sderot, an Israeli city that has been under constant terror attacks for over two decades, and analyzed them using thematic analysis. Four external coping resources were identified: family; friendships; communal resources including a sense of belonging to their community and neighbors; and formal resources provided to them by the municipality and the state, comprising instrumental and emotional support. The findings affirm the significance of external coping resources for older adults facing continuous stress and trauma, suggesting ways to strengthen these resources to boost individuals' resilience.

Published
2024
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13. Alone in the shadow of terror: Strategies and internal resources of older adults living alone in a continuous traumatic situation.

Author

Hadida-Naus S, Spector-Mersel G, and Shiovitz-Ezra S

Subjects
Humans, Aged, Aging psychology, Stress, Psychological psychology, Home Environment, Adaptation, Psychological
Abstract

Continuous traumatic situations (CTS) caused by prolonged exposure to terrorist threat can harm individuals' mental and physical health. For older adults living alone in CTS, this risk joins the challenges of aging and loneliness, creating a triple vulnerability. No previous research has explored this particular vulnerability and specifically addressed the coping strategies and internal resources used by older adults to manage these stressful circumstances. The present study aimed to fill this lacuna, by exploring how older adults living alone in CTS cope with these challenges and the internal resources that help them do so. In-depth interviews with 15 persons aged 65 + years living alone in Sderot, an Israeli city exposed to a continuous terror threat, were conducted and analyzed thematically. Participants described various coping strategies. Some are deployed at the psychological level: positive thinking, deliberate disengagement, perception of being alone as an advantage, and social comparison; others have behavioral implications: acknowledging reality and dealing with it and "turning it into an engine." Participants also identified four internal resources that helped them cope: functional independence, faith, character traits, and previous experience with stressful life events. Participants coped with the difficulties of living alone in CTS actively and creatively, relying on various psychological and functional resources. The findings support theories that emphasize older adults' resilience and ability to cope with stress and trauma, suggesting ways to strengthen the resilience of older adults facing CTS, particularly those living alone. (PsycInfo Database Record (c) 2023 APA, all rights reserved).

Published
2023
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14. Deficiency of the metalloproteinase-disintegrin ADAM8 is associated with thymic hyper-cellularity.

Author

Gossens K, Naus S, Holländer GA, and Ziltener HJ

Subjects
ADAM Proteins genetics, ADAM Proteins immunology, Animals, Antigens, CD genetics, Antigens, CD immunology, Cell Differentiation, Cell Movement, Cell Proliferation, Female, Male, Membrane Proteins genetics, Membrane Proteins immunology, Mice, Mice, Inbred C57BL, Mice, Knockout, T-Lymphocytes enzymology, T-Lymphocytes immunology, Thymus Gland immunology, ADAM Proteins deficiency, Membrane Proteins deficiency, T-Lymphocytes cytology, Thymus Gland cytology, Thymus Gland enzymology
Abstract

Background: Thymopoiesis requires thymocyte-stroma interactions and proteases that promote cell migration by degrading extracellular matrix and releasing essential cytokines and chemokines. A role for several members of the A Disintegrin and Metalloprotease (ADAM) family in T cell development has been reported in the past., Methodology/principal Findings: Here, we present data indicating that the family member ADAM8 plays a role in thymic T cell development. We used qrtPCR on FACS sorted thymic subsets together with immunofluorescence to analyze thymic ADAM8 expression. We found that ADAM8 was expressed in murine thymic stromal cells and at lower levels in thymocytes where its expression increased as cell matured, suggesting involvement of ADAM8 in thymopoiesis. Further flow cytometry analysis revealed that ADAM8 deficient mice showed normal development and expansion of immature thymocyte subsets. There was however an intrathymic accumulation of single positive CD4 and CD8 T cells which was most noticeable in the late mature T cell subsets. Accumulation of single positive T cells coincided with changes in the thymic architecture manifest in a decreased cortex/medulla ratio and an increase in medullary epithelial cells as determined by histology and flow cytometry. The increase in single positive T cells was thymus-intrinsic, independent of progenitor homing to the thymus or thymic exit rate of mature T cells. Chemotaxis assays revealed that ADAM8 deficiency was associated with reduced migration of single positive thymocytes towards CCL21., Conclusions/significance: Our results show that ADAM8 is involved in T cell maturation in the medulla and suggest a role for this protease in fine-tuning maturation of thymocytes in the medulla. In contrast to ADAM10 and ADAM17 lack of ADAM8 appears to have a relatively minor impact on T cell development, which was unexpected given that maturation of thymocytes is dependent on proper localization and timing of migration.

Published
2010
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15. Tumor necrosis factor-alpha (TNF-alpha) regulates shedding of TNF-alpha receptor 1 by the metalloprotease-disintegrin ADAM8: evidence for a protease-regulated feedback loop in neuroprotection.

Author

Bartsch JW, Wildeboer D, Koller G, Naus S, Rittger A, Moss ML, Minai Y, and Jockusch H

Subjects
ADAM Proteins deficiency, ADAM Proteins genetics, ADAM Proteins pharmacology, Animals, Animals, Newborn, Antigens, CD genetics, Antigens, CD pharmacology, Cell Count methods, Central Nervous System metabolism, Central Nervous System pathology, Dose-Response Relationship, Drug, Enzyme-Linked Immunosorbent Assay methods, Humans, Kaplan-Meier Estimate, Leukocyte Common Antigens metabolism, Membrane Proteins deficiency, Membrane Proteins genetics, Membrane Proteins pharmacology, Mice, Mice, Inbred C57BL, Mice, Knockout, Muscular Atrophy genetics, Nerve Tissue Proteins metabolism, Neurodegenerative Diseases mortality, Neurodegenerative Diseases pathology, Neuroglia drug effects, Neuroglia metabolism, Neurons drug effects, Neurons metabolism, RNA, Messenger metabolism, Receptors, Tumor Necrosis Factor, Type I drug effects, Receptors, Tumor Necrosis Factor, Type II metabolism, Tumor Necrosis Factor-alpha pharmacology, ADAM Proteins metabolism, Antigens, CD metabolism, Gene Expression Regulation genetics, Membrane Proteins metabolism, Neurodegenerative Diseases genetics, Receptors, Tumor Necrosis Factor, Type I metabolism, Tumor Necrosis Factor-alpha metabolism
Abstract

Tumor necrosis factor alpha (TNF-alpha) is a potent cytokine in neurodegenerative disorders, but its precise role in particular brain disorders is ambiguous. In motor neuron (MN) disease of the mouse, exemplified by the model wobbler (WR), TNF-alpha causes upregulation of the metalloprotease-disintegrin ADAM8 (A8) in affected brain regions, spinal cord, and brainstem. The functional role of A8 during MN degeneration in the wobbler CNS was investigated by crossing WR with A8-deficient mice: a severely aggravated neuropathology was observed for A8-deficient WR compared with WR A8(+/-) mice, judged by drastically reduced survival [7 vs 81% survival at postnatal day 50 (P50)], accelerated force loss in the forelimbs, and terminal akinesis. In vitro protease assays using soluble A8 indicated specific cleavage of a TNF-alpha receptor 1 (p55 TNF-R1) but not a TNF-R2 peptide. Cleavage of TNF-R1 was confirmed in situ, because levels of soluble TNF-R1 were increased in spinal cords of standard WR compared with wild-type mice but not in A8-deficient WR mice. In isolated primary neurons and microglia, TNF-alpha-induced TNF-R1 shedding was dependent on the A8 gene dosage. Furthermore, exogenous TNF-alpha showed higher toxicity for cultured neurons from A8-deficient than for those from wild-type mice, demonstrating that TNF-R1 shedding by A8 is neuroprotective. Our results indicate an essential role for ADAM8 in modulating TNF-alpha signaling in CNS diseases: a feedback loop integrating TNF-alpha, ADAM8, and TNF-R1 shedding as a plausible mechanism for TNF-alpha mediated neuroprotection in situ and a rationale for therapeutic intervention.

Published
2010
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16. The metalloprotease-disintegrin ADAM8 is essential for the development of experimental asthma.

Author

Naus S, Blanchet MR, Gossens K, Zaph C, Bartsch JW, McNagny KM, and Ziltener HJ

Subjects
Animals, Bronchoalveolar Lavage Fluid cytology, Bronchoalveolar Lavage Fluid immunology, Cell Differentiation immunology, Disease Models, Animal, Enzyme-Linked Immunosorbent Assay methods, Flow Cytometry methods, Inflammation immunology, Mice, Mice, Inbred C57BL, Ovalbumin, Reverse Transcriptase Polymerase Chain Reaction methods, ADAM Proteins immunology, Antigens, CD immunology, Asthma genetics, Asthma immunology, Bronchial Hyperreactivity genetics, Bronchial Hyperreactivity immunology, Membrane Proteins immunology
Abstract

Rationale: Expression of the metalloprotease ADAM8 is increased in patients with asthma, but the functional significance of elevated ADAM8 expression in the context of asthma pathogenesis remains elusive., Objectives: To study development of asthma in ADAM8-deficient mice., Methods: Ovalbumin-induced asthma was studied in wild-type, ADAM8-deficient, and ADAM8-chimeric mice. Lung inflammation was assessed by histology, analysis of bronchoalveolar lavage, and airway hyperresponsiveness., Measurements and Main Results: ADAM8-deficient mice are highly resistant to the development of ovalbumin-induced airway inflammation and hyperresponsiveness. ADAM8 expression was induced in both hematopoietic cells and the nonhematopoietic microenvironment after induction of asthma, and ADAM8 expression in both cell populations was required for the full manifestation of asthma. Interestingly, loss of ADAM8 on T cells alone was sufficient to significantly decrease the asthma response. The attenuated response was not due to an intrinsic defect in antigen presentation or cytokine production but reflected an impaired migration of T cells, eosinophils, CD11b(+) CD11c(-), and CD11c(+) cells from blood vessels to the lung and alveolar space, suggesting a general hematopoietic cell deficiency in the absence of ADAM8., Conclusions: The results show that ADAM8 plays a proinflammatory role in airway inflammation. The milder disease outcome in the absence of ADAM8 suggests that this protein might be an interesting new target in treatment of this, and potentially other, inflammatory diseases in which recruitment of inflammatory cells is an essential part of pathogenesis.

Published
2010
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17. PSGL-1 function in immunity and steady state homeostasis.

Author

Carlow DA, Gossens K, Naus S, Veerman KM, Seo W, and Ziltener HJ

Subjects
Animals, Glycosylation, Hematopoietic Stem Cells immunology, Hematopoietic Stem Cells metabolism, Humans, Hyaluronan Receptors immunology, Hyaluronan Receptors metabolism, Membrane Glycoproteins chemistry, Membrane Glycoproteins immunology, Selectins immunology, Signal Transduction immunology, T-Lymphocytes immunology, T-Lymphocytes metabolism, Transferases immunology, Transferases metabolism, Cell Movement immunology, Homeostasis immunology, Leukocyte Rolling immunology, Membrane Glycoproteins metabolism, Selectins metabolism
Abstract

The substantial importance of P-selectin glycoprotein ligand 1 (PSGL-1) in leukocyte trafficking has continued to emerge beyond its initial identification as a selectin ligand. PSGL-1 seemed to be a relatively simple molecule with an extracellular mucin domain extended as a flexible rod, teleologically consistent with its primary role in tethering leukocytes to endothelial selectins. The rolling interaction between leukocyte and endothelium mediated by this selectin-PSGL-1 interaction requires branched O-glycan extensions on specific PSGL-1 amino acid residues. In some cells, such as neutrophils, the glycosyltransferases involved in formation of the O-glycans are constitutively expressed, while in other cells, such as T cells, they are expressed only after appropriate activation. Thus, PSGL-1 supports leukocyte recruitment in both innate and adaptive arms of the immune response. A complex array of amino acids within the selectins engage multiple sugar residues of the branched O-glycans on PSGL-1 and provide the molecular interactions responsible for the velcro-like catch bonds that support leukocyte rolling. Such binding of PSGL-1 can also induce signaling events that influence cell phenotype and function. Scrutiny of PSGL-1 has revealed a better understanding of how it performs as a selectin ligand and yielded unexpected insights that extend its scope from supporting leukocyte rolling in inflammatory settings to homeostasis including stem cell homing to the thymus and mature T-cell homing to secondary lymphoid organs. PSGL-1 has been found to bind homeostatic chemokines CCL19 and CCL21 and to support the chemotactic response to these chemokines. Surprisingly, the O-glycan modifications of PSGL-1 that support rolling mediated by selectins in inflammatory conditions interfere with PSGL-1 binding to homeostatic chemokines and thereby limit responsiveness to the chemotactic cues used in steady state T-cell traffic. The multi-level influence of PSGL-1 on cell traffic in both inflammatory and steady state settings is therefore substantially determined by the orchestrated addition of O-glycans. However, central as specific O-glycosylation is to PSGL-1 function, in vivo regulation of PSGL-1 glycosylation in T cells remains poorly understood. It is our purpose herein to review what is known, and not known, of PSGL-1 glycosylation and to update understanding of PSGL-1 functional scope.

Published
2009
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18. Thymic progenitor homing and lymphocyte homeostasis are linked via S1P-controlled expression of thymic P-selectin/CCL25.

Author

Gossens K, Naus S, Corbel SY, Lin S, Rossi FM, Kast J, and Ziltener HJ

Subjects
Animals, Bone Marrow Cells immunology, Homeostasis, Lymphocytes immunology, Membrane Glycoproteins deficiency, Membrane Glycoproteins genetics, Mice, Mice, Knockout, Proprotein Convertases, RNA genetics, Receptors, Interleukin-7 deficiency, Receptors, Interleukin-7 genetics, Serine Endopeptidases blood, Transcription, Genetic, P-Selectin genetics, Serine Endopeptidases immunology, T-Lymphocytes immunology, Thymus Gland immunology
Abstract

Thymic T cell progenitor (TCP) importation is a periodic, gated event that is dependent on the expression of functional P-selectin ligands on TCPs. Occupancy of intrathymic TCP niches is believed to negatively regulate TCP importation, but the nature of this feedback mechanism is not yet resolved. We show that P-selectin and CCL25 are periodically expressed in the thymus and are essential parts of the thymic gate-keeping mechanism. Periodicity of thymic TCP receptivity and the size of the earliest intrathymic TCP pool were dependent on the presence of functional P-selectin ligand on TCPs. Furthermore, we show that the numbers of peripheral blood lymphocytes directly affected thymic P-selectin expression and TCP receptivity. We identified sphingosine-1-phosphate (S1P) as one feedback signal that could mediate influence of the peripheral lymphocyte pool on thymic TCP receptivity. Our findings suggest a model whereby thymic TCP importation is controlled by both early thymic niche occupancy and the peripheral lymphocyte pool via S1P.

Published
2009
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19. ADAM8/MS2/CD156, an emerging drug target in the treatment of inflammatory and invasive pathologies.

Author

Koller G, Schlomann U, Golfi P, Ferdous T, Naus S, and Bartsch JW

Subjects
Animals, Humans, Inflammation pathology, Mice, ADAM Proteins drug effects, Inflammation drug therapy, Membrane Proteins drug effects
Abstract

While it is highly accepted that ADAM family members with ubiquitous expression patterns, such as ADAM10 and ADAM17 have major roles in homoeostasis and pathology, ADAM8 was initially considered as an immune-specific ADAM with a cell-specific expression pattern. Therefore, ADAM8 had a "sleeping beauty" existence for many years, and has recently come back into focus as it was detected under several pathological conditions. These were found to typically involve inflammation and remodelling of the extracellular matrix, including cancers and serious respiratory diseases such as asthma. In these diseases, induced expression of ADAM8 by different stimuli results in cleavage of various substrates, including cell adhesion molecules, cytokine receptors, and ECM components. Involvement of ADAM8 in individual diseases indicates its usefulness as both a diagnostic and prognostic marker. Even more strikingly, as ADAM8 progressively emerges as a key effector in pathological processes, so does its attractiveness as a therapeutic target rather than being a mere indicator of disease and its progression. This is encouraged by analysis of ADAM8 null mice, identifying no adverse phenotype in the absence of functional ADAM8. Thus, ADAM8 potentially is an attractive drug target in a variety of diseases. In this review, the current knowledge on ADAM8 in diseases and avenues for specific inhibition based on unique biochemical features of ADAM8 will be presented.

Published
2009
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20. Interaction of the selectin ligand PSGL-1 with chemokines CCL21 and CCL19 facilitates efficient homing of T cells to secondary lymphoid organs.

Author

Veerman KM, Williams MJ, Uchimura K, Singer MS, Merzaban JS, Naus S, Carlow DA, Owen P, Rivera-Nieves J, Rosen SD, and Ziltener HJ

Subjects
Animals, Cell Adhesion genetics, Cell Adhesion immunology, Chemokine CCL19, Chemokine CCL21, Chemokines, CC biosynthesis, Chemokines, CC genetics, Lymphoid Tissue immunology, Membrane Glycoproteins immunology, Mice, Chemokines, CC physiology, Homeostasis physiology, Lymphoid Tissue cytology, Membrane Glycoproteins metabolism, T-Lymphocytes physiology
Abstract

P-selectin glycoprotein ligand 1 (PSGL-1) is central to the trafficking of immune effector cells to areas of inflammation through direct interactions with P-selectin, E-selectin and L-selectin. Here we show that PSGL-1 was also required for efficient homing of resting T cells to secondary lymphoid organs but functioned independently of selectin binding. PSGL-1 mediated an enhanced chemotactic T cell response to the secondary lymphoid organ chemokines CCL21 and CCL19 but not to CXCL12 or to inflammatory chemokines. Our data show involvement of PSGL-1 in facilitating the entry of T cells into secondary lymphoid organs, thereby demonstrating the bifunctional nature of this molecule.

Published
2007
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21. Metalloproteinase disintegrins ADAM8 and ADAM19 are highly regulated in human primary brain tumors and their expression levels and activities are associated with invasiveness.

Author

Wildeboer D, Naus S, Amy Sang QX, Bartsch JW, and Pagenstecher A

Subjects
Animals, Blotting, Western methods, Brain Neoplasms enzymology, Brain Neoplasms genetics, Brain Neoplasms pathology, Cell Line, Tumor, Enzyme Activation, Gene Expression Regulation drug effects, Glioma enzymology, Glioma genetics, Glioma pathology, Humans, Immunohistochemistry methods, Metalloproteases physiology, Neoplasm Invasiveness, RNA, Messenger, Rats, Reverse Transcriptase Polymerase Chain Reaction methods, ADAM Proteins metabolism, Brain Neoplasms metabolism, Gene Expression Regulation physiology, Glioma metabolism, Membrane Proteins metabolism
Abstract

Patients with primary brain tumors have bleak prognoses and there is an urgent desire to identify new markers for sensitive diagnosis and new therapeutic targets for effective treatment. A family of proteins, the disintegrin and metalloproteinases (ADAMs or adamalysins), are cell surface and extracellular multidomain proteins implicated in cell-cell signaling, cell adhesion, and cell migration. Their putative biological and pathological roles make them candidates for promoting tumor growth and malignancy. We investigated the expression levels of 12 cerebrally expressed ADAM genes in human primary brain tumors (astrocytoma WHO grade I-III, glioblastoma WHO grade IV, oligoastrocytoma WHO grade II and III, oligodendroglioma WHO grade II and III, ependymoma WHO grade II and III, and primitive neuroectodermal tumor WHO grade IV) using real-time PCR. The mRNAs of the five ADAMs 8, 12, 15, 17, and 19 were significantly upregulated. The ADAM8 and ADAM19 proteins were mainly located in tumor cells and in some tumors in endothelia of blood vessels. In brain tumor tissue, ADAM8 and ADAM19 undergo activation by prodomain removal resulting in active proteases. By using specific peptide substrates for ADAM8 and ADAM19, respectively, we demonstrated that the proteases exert enhanced proteolytic activity in those tumor specimens with the highest expression levels. In addition, expression levels and the protease activities of ADAM8 and ADAM19 correlated with invasive activity of glioma cells, indicating that ADAM8 and ADAM19 may play a significant role in tumor invasion that may be detrimental to patients survival.

Published
2006
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22. Identification of candidate substrates for ectodomain shedding by the metalloprotease-disintegrin ADAM8.

Author

Naus S, Reipschläger S, Wildeboer D, Lichtenthaler SF, Mitterreiter S, Guan Z, Moss ML, and Bartsch JW

Subjects
ADAM Proteins chemistry, ADAM Proteins isolation & purification, ADAM10 Protein, Amino Acid Sequence, Amyloid Precursor Protein Secretases, Amyloid beta-Protein Precursor metabolism, Cells, Cultured, Disintegrins chemistry, Disintegrins isolation & purification, Escherichia coli genetics, Gene Expression Regulation, Humans, Inflammation metabolism, Kidney cytology, Kidney embryology, Membrane Proteins chemistry, Membrane Proteins isolation & purification, Metalloproteases chemistry, Metalloproteases isolation & purification, Molecular Sequence Data, Neurodegenerative Diseases metabolism, Peptide Fragments chemistry, Platelet Aggregation Inhibitors pharmacology, ADAM Proteins metabolism, Disintegrins metabolism, Membrane Proteins metabolism, Metalloproteases metabolism
Abstract

ADAM proteases are type I transmembrane proteins with extracellular metalloprotease domains. As for most ADAM family members, ADAM8 (CD156a, MS2) is involved in ectodomain shedding of membrane proteins and is linked to inflammation and neurodegeneration. To identify potential substrates released under these pathologic conditions, we screened 10-mer peptides representing amino acid sequences from extracellular domains of various membrane proteins using the ProteaseSpot system. A soluble ADAM8 protease containing a pro- and metalloprotease domain was expressed in E. coli and purified as active protease owing to autocatalytic prodomain removal. From 34 peptides tested in the peptide cleavage assay, significant cleavage by soluble ADAM8 was observed for 14 peptides representing membrane proteins with functions in inflammation and neurodegeneration, among them the beta-amyloid precursor protein (APP). The in vivo relevance of the ProteaseSpot method was confirmed by cleavage of full-length APP with ADAM8 in human embryonic kidney 293 cells expressing tagged APP. ADAM8 cleaved APP with similar efficiency as ADAM10, whereas the inactive ADAM8 mutant did not. Exchanging amino acids at defined positions in the cleavage sequence of myelin basic protein (MBP) revealed sequence criteria for ADAM8 cleavage. Taken together, the results allowed us to identify novel candidate substrates that could be cleaved by ADAM8 in vivo under pathologic conditions.

Published
2006
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24. Ectodomain shedding of the neural recognition molecule CHL1 by the metalloprotease-disintegrin ADAM8 promotes neurite outgrowth and suppresses neuronal cell death.

Author

Naus S, Richter M, Wildeboer D, Moss M, Schachner M, and Bartsch JW

Subjects
ADAM Proteins, Animals, Cell Communication physiology, Cell Death physiology, Mice, Mutation, Neurites physiology, Neurites ultrastructure, Neurons cytology, Peptide Fragments, Protein Structure, Tertiary, Antigens, CD physiology, Membrane Proteins physiology, Metalloendopeptidases physiology, Neurons physiology
Abstract

The neural cell adhesion molecule "close homologue of L1," termed CHL1, has functional importance in the nervous system. CHL1 is expressed as a transmembrane protein of 185 kDa, and ectodomain shedding releases soluble fragments relevant for its physiological function. Here we describe that ADAM8, a member of the family of metalloprotease disintegrins cleaves a CHL1-Fc fusion protein in vitro at two sites corresponding to release of the extracellular domain of CHL1 in fibronectin (FN) domains II (125 kDa) and V (165 kDa), inhibited by batimastat (BB-94). Cleavage of CHL1-Fc in the 125-kDa fragment was not detectable under non-reducing conditions arguing that cleavage resulting in the 165-kDa fragment is more relevant in releasing soluble CHL1 in vivo. In cells transfected with full-length ADAM8, membrane proximal cleavage of CHL1 was similar and not stimulated by phorbol ester 12-O-tetradecanoylphorbol-13-acetate and pervanadate. No cleavage of CHL1 was observed in cells expressing either inactive ADAM8 with a Glu330 to Gln exchange (EQ-A8), or active ADAM10 and ADAM17. Consequently, processing of CHL1 was hardly detectable in brain extracts of ADAM8-deficient mice but enhanced in a neurodegenerative mouse mutant. CHL1 processed by ADAM8 in supernatants of COS-7 cells and in co-culture with cerebellar granule neurons was very potent in stimulating neurite outgrowth and suppressing neuronal cell death, not observed in cells co-transfected with CHL1/EQ-A8, CHL1/ADAM10, or CHL1/ADAM17. Taken together, we propose that ADAM8 plays an important role in physiological and pathological cell interactions by a specific release of functional CHL1 from the cell surface.

Published
2004
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