TY  - THES
A1  - Kipp, Anna Patricia
T1  - Selen, Selenoproteine und der Wnt-Signalweg : Regulation der gastrointestinalen Glutathionperoxidase durch β-Catenin und Beeinflussung des Wnt-Signalwegs durch den Selenstatus
T1  - Selenium, selenoproteins, and the Wnt pathway : regulation of the gastrointestinal glutathione peroxidase via the Wnt pathway and influence of the selenium status on the activity of the Wnt pathway
N2  - Das seit 1957 als essentiell klassifizierte Spurenelement Selen vermittelt seine Funktion hauptsächlich durch seinen Einbau in Selenoproteine in Form der 21. proteinogenen Aminosäure Selenocystein. Insgesamt wurden 25 humane Gene für Selenoproteine identifiziert, deren genaue Funktion häufig noch nicht bekannt ist. Selen ist das einzige Mitglied aus der Gruppe der Mikronährstoffe, für das nach wie vor eine antikanzerogene Funktion vor allem in Bezug auf Darmkrebs postuliert wird. Die Grundlage dafür liefert eine Interventionsstudie, bei der 1.312 Probanden für 4,5 Jahre mit 200 μg Selen/Tag supplementiert wurden. Dies resultierte in einer Senkung der Gesamtkrebsmortalität um 50 %. Die Fragen einer optimalen Selenzufuhr, die nicht nur den Bedarf deckt, sondern auch die Entfaltung der antikanzerogenen Wirkung von Selen gewährleistet und die zugrunde liegenden molekularen Mechanismen sind noch ungeklärt. Zudem liegt die Selenzufuhr bei einem Großteil der europäischen Bevölkerung unter den Empfehlungen. Deshalb wurden in der vorliegenden Arbeit vier Wochen alte Mäuse für sechs Wochen marginal defizient (0,086 mg/kg Futter) bzw. selenadäquat (0,15 mg/kg Futter) gefüttert. Dieser geringe Unterschied im Selengehalt resultierte in einer Senkung des Plasmaselenspiegels der selenarmen Tiere auf 13 % und der GPx-Aktivität in der Leber auf 35 %. Zunächst wurde der Einfluss von Selen auf die globale Genexpression im murinen Colon mittels Microarray untersucht. Von den im Colon exprimierten Selenoproteinen reagierte die mRNA von SelW, SelH, GPx1 und SelM im Selenmangel besonders deutlich mit Expressionsverlust. Da diese Selenoproteine nicht nur im Colon, sondern auch in Leukozyten reguliert waren, sind sie auch als humane Biomarker für die in dieser Studie gewählte Schwankung des Selengehalts geeignet. Des Weiteren wurde auf Basis der Microarraydaten eine Signalweganalyse durchgeführt, die der Identifizierung krebsrelevanter Signalwege diente, um mögliche molekularbiologische Erklärungsansätze für die Rolle von Selen im Krebsgeschehen zu finden. Es zeigte sich, dass die mRNA von Schlüsselgenen des Wnt-Signalwegs wie β-Catenin, Gsk3β, Dvl2, Tle2, Lef1 und c-Myc auf Schwankungen des Selengehalts reagiert. Vor allem die Induktion von c-Myc, einem Zielgen des Wnt-Signalwegs, deutet darauf hin, dass dieser im Selenmangel tatsächlich aktiver ist als bei selenadäquater Versorgung. Ein weiterer möglicher Erklärungsansatz für die postulierte präventive Funktion von Selen gegenüber Darmkrebs ist die gastrointestinale Glutathionperoxidase (GPx2), die physiologisch in den proliferierenden Zellen des Kryptengrunds exprimiert wird. Die Regulation dieses Enzyms durch den Wnt-Signalweg, der ebenfalls in proliferierenden Zellen aktiv ist, konnte mittels Reportergenanalyse und endogen auf mRNA- und Proteinebene in Zellkultur gezeigt werden. Die Aktivierung verkürzter Promotorkonstrukte und die Mutation eines potentiellen Bindeelements identifizierten den für die Bindung von TCF und β-Catenin verantwortlichen Bereich. Als Zielgen des Wnt-Signalwegs scheint GPx2 zu den an Proliferationsprozessen beteiligten Genen zu gehören, was unter physiologischen Bedingungen die Aufrechterhaltung des intestinalen Epithels gewährleistet. Bei der Entstehung intestinaler Tumore, die in der Initiationsphase zu über 90 % mit einer konstitutiven Aktivierung des Wnt-Signalwegs einhergeht, wirkt GPx2 möglicherweise prokanzerogen. Die genaue Funktion von GPx2 während der Kanzerogenese bleibt weiter zu untersuchen.
N2  - Suboptimal selenium (Se) status has been suggested to be associated with a higher risk of developing various cancers, especially colon cancer. In mammals, Se exerts its functions through selenoproteins into which it is incorporated as selenocysteine. Since the function of many selenoproteins has not been identified the underlying mechanisms of the anti-carcinogenic function of Se remains unclear. Therefore, mice were fed either a marginal Se-deficient diet (0.086 mg Se/kg) or a Se-adequate diet (0.15 mg Se/kg) for six weeks. The plasma Se level was reduced to 13 % in the Se-deficient group while GPx activity in the liver was reduced to 35 %. The influence of Se on the global gene expression pattern was analysed using microarray technology. Among selenoproteins SelW, GPx1, SelH and SelM were consistently lower expressed in animals fed with the Se-deficient diet. As the mRNA of these genes was regulated in leucocytes as well, they are possible new biomarkers for the Se status in human studies. In addition, pathway analysis revealed that the cancer-relevant Wnt pathway was affected by the Se status, indicated by changes in the mRNA expression of key proteins like β-catenin, Gsk3β, Dvl2, Tle2, Lef1 and the Wnt target gene c-Myc. The regulation of these genes by Se points to a slightly increased basal activity level of the Wnt pathway in the Se poor state and may therefore contribute to the higher cancer risk in a marginal Se deficiency. Another possible explanation for anti-carcinogenic effects of Se is the gastrointestinal glutathione peroxidase GPx2, a selenoprotein predominantly expressed in proliferating cells at the crypt grounds of the intestine. The regulation of GPx2 via the Wnt pathway was confirmed by reporter gene experiments and by analysing endogenous GPx2 expression on the mRNA as well as on the protein level in different cell culture systems. Shortened promoter constructs and the mutation of a potential TCF binding element identified the area responsible for β-catenin/TCF binding. GPx2 is the first selenoprotein identified as a target of the Wnt pathway. This finding suggests a function of GPx2 in the maintenance of normal renewal of the intestinal epithelium as well as in cancer development.
KW  - Selen
KW  - Biomarker
KW  - Wnt-Signalweg
KW  - GPx2
KW  - Selenium
KW  - biomarker
KW  - Wnt pathway
KW  - GPx2
Y1  - 2008
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:kobv:517-opus-30484
ER  - 
TY  - THES
A1  - Kipp, Anna Patricia
T1  - Physiologische und Tumor-Assoziierte Funktionen von Selen und Selenoproteinen
Y1  - 2014
ER  - 
TY  - JOUR
A1  - Manowsky, Julia
A1  - Camargo, Rodolfo Gonzalez
A1  - Kipp, Anna Patricia
A1  - Henkel, Janin
A1  - Püschel, Gerhard Paul
T1  - Insulin-induced cytokine production in macrophages causes insulin resistance in hepatocytes
JF  - American journal of physiology : Endocrinology and metabolism
N2  - Overweight and obesity are associated with hyperinsulinemia, insulin resistance, and a low-grade inflammation. Although hyperinsulinemia is generally thought to result from an attempt of the beta-cell to compensate for insulin resistance, there is evidence that hyperinsulinaemia itself may contribute to the development of insulin resistance and possibly the low-grade inflammation. To test this hypothesis, U937 macrophages were exposed to insulin. In these cells, insulin induced expression of the proinflammatory cytokines IL-1 beta, IL-8, CCL2, and OSM. The insulin-elicited induction of IL-1 beta was independent of the presence of endotoxin and most likely mediated by an insulin-dependent activation of NF-kappa B. Supernatants of the insulin-treated U937 macrophages rendered primary cultures of rat hepatocytes insulin resistant; they attenuated the insulin-dependent induction of glucokinase by 50%. The cytokines contained in the supernatants of insulin-treated U937 macrophages activated ERK1/2 and IKK beta, resulting in an inhibitory serine phosphorylation of the insulin receptor substrate. In addition, STAT3 was activated and SOCS3 induced, further contributing to the interruption of the insulin receptor signal chain in hepatocytes. These results indicate that hyperinsulinemia per se might contribute to the low-grade inflammation prevailing in overweight and obese patients and thereby promote the development of insulin resistance particularly in the liver, because the insulin concentration in the portal circulation is much higher than in all other tissues.
KW  - metabolic syndrome
KW  - type 2 diabetes
KW  - inflammation
KW  - macrophage
KW  - insulin
KW  - cytokines
Y1  - 2016
U6  - https://doi.org/10.1152/ajpendo.00427.2015
SN  - 0193-1849
SN  - 1522-1555
VL  - 310
SP  - E938
EP  - E946
PB  - American Chemical Society
CY  - Bethesda
ER  - 
TY  - JOUR
A1  - Frede, Katja
A1  - Ebert, Franziska
A1  - Kipp, Anna Patricia
A1  - Schwerdtle, Tanja
A1  - Baldermann, Susanne
T1  - Lutein Activates the Transcription Factor Nrf2 in Human Retinal Pigment Epithelial Cells
JF  - Journal of agricultural and food chemistry : a publication of the American Chemical Society
N2  - The degeneration of the retinal pigment epithelium caused by oxidative damage is a stage of development in age related macular degeneration (AMD). The carotenoid lutein is a major macular pigment that may reduce the incidence and progression of AMD, but the underlying mechanism is currently not fully understood. Carotenoids are known to be direct antioxidants. However, carotenoids can also activate cellular pathways resulting in indirect antioxidant effects. Here, we investigate the influence of lutein on the activation of nuclear factor erythroid 2-related factor 2 (Nrf2) target genes in human retinal pigment epithelial cells (ARPE-19 cells) using lutein-loaded Tween40 micelles. The micelles were identified as a suitable delivery system since they were nontoxic in APRE-19 cells up to 0.04% Tween40 and led to a cellular lutein accumulation of 62 mu M +/- 14 mu M after 24 h. Lutein significantly enhanced Nrf2 translocation to the nucleus 1.5 +/- 0.4-fold compared to that of unloaded micelles after 4 h. Furthermore, lutein treatment for 24 h significantly increased the transcripts of NAD(P)H:quinone oxidoreductase 1 (NQO1) by 1.7 +/- 0.1-fold, glutamate-cysteine ligase regulatory subunit (GCLm) by 1.4 +/- 0.1-fold, and heme oxygenase-1 (HO-1) by 1.8 +/- 0.3-fold. Moreover, we observed a significant enhancement of NQO1 activity by 1.2 +/- 0.1-fold. Collectively, this study indicates that lutein not only serves as a direct antioxidant but also activates Nrf 2 in ARPE-19 cells.
KW  - lutein
KW  - Nif2
KW  - ARPE-19 cells
KW  - AMD
KW  - Tween40 micelles
Y1  - 2017
U6  - https://doi.org/10.1021/acs.jafc.7b01929
SN  - 0021-8561
SN  - 1520-5118
VL  - 65
SP  - 5944
EP  - 5952
PB  - American Chemical Society
CY  - Washington
ER  - 
TY  - JOUR
A1  - Wiesner-Reinhold, Melanie
A1  - Schreiner, Monika
A1  - Baldermann, Susanne
A1  - Schwarz, Dietmar
A1  - Hanschen, Franziska S.
A1  - Kipp, Anna Patricia
A1  - Rowan, Daryl D.
A1  - Bentley-Hewitt, Kerry L.
A1  - McKenzie, Marian J.
T1  - Mechanisms of Selenium Enrichment and Measurement in Brassicaceous Vegetables, and Their Application to Human Health
JF  - Frontiers in plant science
N2  - Selenium (Se) is an essential micronutrient for human health. Se deficiency affects hundreds of millions of people worldwide, particularly in developing countries, and there is increasing awareness that suboptimal supply of Se can also negatively affect human health. Selenium enters the diet primarily through the ingestion of plant and animal products. Although, plants are not dependent on Se they take it up from the soil through the sulphur (S) uptake and assimilation pathways. Therefore, geographic differences in the availability of soil Se and agricultural practices have a profound influence on the Se content of many foods, and there are increasing efforts to biofortify crop plants with Se. Plants from the Brassicales are of particular interest as they accumulate and synthesize Se into forms with additional health benefits, such as methylselenocysteine (MeSeCys). The Brassicaceae are also well-known to produce the glucosinolates; S-containing compounds with demonstrated human health value. Furthermore, the recent discovery of the selenoglucosinolates in the Brassicaceae raises questions regarding their potential bioefficacy. In this review we focus on Se uptake and metabolism in the Brassicaceae in the context of human health, particularly cancer prevention and immunity. We investigate the close relationship between Se and S metabolism in this plant family, with particular emphasis on the selenoglucosinolates, and consider the methodologies available for identifying and quantifying further novel Se-containing compounds in plants. Finally, we summarize the research of multiple groups investigating biofortification of the Brassicaceae and discuss which approaches might be most successful for supplying Se deficient populations in the future.
KW  - Brassica vegetables
KW  - selenium
KW  - biofortification
KW  - glucosinolates
KW  - human health
KW  - immune system
KW  - cancer
KW  - analytical methods
Y1  - 2017
U6  - https://doi.org/10.3389/fpls.2017.01365
SN  - 1664-462X
VL  - 8
PB  - Frontiers Research Foundation
CY  - Lausanne
ER  - 
TY  - JOUR
A1  - Speckmann, Bodo
A1  - Schulz, Sarah
A1  - Hiller, Franziska
A1  - Hesse, Deike
A1  - Schumacher, Fabian
A1  - Kleuser, Burkhard
A1  - Geisel, Juergen
A1  - Obeid, Rima
A1  - Grune, Tilman
A1  - Kipp, Anna Patricia
T1  - Selenium increases hepatic DNA methylation and modulates one-carbon metabolism in the liver of mice
JF  - The journal of nutritional biochemistry
N2  - The average intake of the essential trace element selenium (Se) is below the recommendation in most European countries, possibly causing sub-optimal expression of selenoproteins. It is still unclear how a suboptimal Se status may affect health. To mimic this situation, mice were fed one of three physiologically relevant amounts of Se. We focused on the liver, the organ most sensitive to changes in the Se supply indicated by hepatic glutathione peroxidase activity. In addition, liver is the main organ for synthesis of methyl groups and glutathione via one-carbon metabolism. Accordingly, the impact of Se on global DNA methylation, methylation capacity, and gene expression was assessed. We observed higher global DNA methylation indicated by LINE1 methylation, and an increase of the methylation potential as indicated by higher S-adenosylmethionine (SAM)/S-adenosylhomocysteine (SAH) ratio and by elevated mRNA expression of serine hydroxymethyltransferase in both or either of the Se groups. Furthermore, increasing the Se supply resulted in higher plasma concentrations of triglycerides. Hepatic expression of glycolytic and lipogenic genes revealed consistent Se dependent up-regulation of glucokinase. The sterol regulatory element-binding transcription factor 1 (Srebf1) was also up-regulated by Se. Both effects were confirmed in primary hepatocytes. In contrast to the overall Se-dependent increase of methylation capacity, the up-regulation of Srebf1 expression was paralleled by reduced local methylation of a specific CpG site within the Srebf1 gene. Thus, we provided evidence that Se-dependent effects on lipogenesis involve epigenetic mechanisms. (C) 2017 The Authors. Published by Elsevier Inc.
KW  - Selenium
KW  - DNA methylation
KW  - Liver
KW  - Lipogenesis
KW  - Srebf1
Y1  - 2017
U6  - https://doi.org/10.1016/j.jnutbio.2017.07.002
SN  - 0955-2863
SN  - 1873-4847
VL  - 48
SP  - 112
EP  - 119
PB  - Elsevier
CY  - New York
ER  - 
TY  - JOUR
A1  - Bornhorst, Julia
A1  - Kipp, Anna Patricia
A1  - Haase, Hajo
A1  - Meyer, Soeren
A1  - Schwerdtle, Tanja
T1  - The crux of inept biomarkers for risks and benefits of trace elements
JF  - Trends in Analytical Chemistry
N2  - Nowadays, the role of trace elements (TE) is of growing interest because dyshomeostasis of selenium (Se), manganese (Mn), zinc (Zn), and copper (Cu) is supposed to be a risk factor for several diseases. Thereby, research focuses on identifying new biomarkers for the TE status to allow for a more reliable description of the individual TE and health status. This review mirrors a lack of well-defined, sensitive, and selective biomarkers and summarizes technical limitations to measure them. Thus, the capacity to assess the relationship between dietary TE intake, homeostasis, and health is restricted, which would otherwise provide the basis to define adequate intake levels of single TE in both healthy and diseased humans. Besides that, our knowledge is even more limited with respect to the real life situation of combined TE intake and putative interactions between single TE.
KW  - Trace elements
KW  - Copper
KW  - Zinc
KW  - Manganese
KW  - Selenium
KW  - Biomarker
KW  - Inductively coupled plasma mass spectrometry
KW  - Hyphenated techniques
KW  - Isotope ratios
Y1  - 2018
U6  - https://doi.org/10.1016/j.trac.2017.11.007
SN  - 0165-9936
SN  - 1879-3142
VL  - 104
SP  - 183
EP  - 190
PB  - Elsevier
CY  - Oxford
ER  - 
TY  - JOUR
A1  - Lossow, Kristina
A1  - Schwerdtle, Tanja
A1  - Kipp, Anna Patricia
T1  - Selen und Jod: essenzielle Spurenelemente für die Schilddrüse
T1  - Selenium and iodine - essential trace elements for the thyroid
JF  - Ernährungs-Umschau : Forschung & Praxis
N2  - Selen und Jod sind essenzielle Spurenelemente, die gemeinsam für eine optimale Funktionstüchtigkeit der Schilddrüse erforderlich sind. Der Mangel eines oder beider Elemente führt zu Verschiebungen auf Ebene der Schilddrüsenhormonproduktion mit weitreichenden Konsequenzen für Stoffwechselprozesse, neurologische Entwicklung und Erkrankungen. Auch bei Autoimmunerkrankungen der Schilddrüse spielt die Versorgung mit Jod und Selen eine wichtige Rolle. Als Biomarker für den Selenstatus eignet sich der Gehalt des Gesamtselens oder der des Selenoproteins P im Serum. Zur Bestimmung des Jodstatus wird in der Regel der Jodgehalt im Urin herangezogen. Um den Versorgungszustand an diesen und vier weiteren essenziellen Spurenelementen besser zu erfassen, charakterisiert die Forschungsgruppe TraceAge alters- und geschlechtsspezifische Spurenelementprofile und neue funktionelle Biomarker der einzelnen Spurenelemente. Außerdem sollen Interaktionen weiterer Spurenelemente genauer untersucht werden.
N2  - Selenium and iodine are essential trace elements that work together to ensure that the thyroid functions optimally. A deficiency in one or both of these elements leads to fluctuations in thyroid hormone production, which have far-reaching consequences in terms of metabolic processes, neurological development, and disease. Iodine and selenium supply also play an important role in autoimmune diseases of the thyroid. Both the total selenium concentration in the serum and the concentration of selenoprotein P are suitable biomarkers for determining selenium status. Iodine concentration in the urine is the most commonly used method of determining iodine status. In order to improve assessment of supply status for these two essential trace elements plus an additional four, the TraceAge research group is identifying age- and sex-specific trace element profiles as well as new functional biomarkers for the individual trace elements. In addition, the research group will investigate interactions with other trace elements in more detail.
KW  - Selen
KW  - Jod
KW  - Schilddrüse
KW  - Schilddrüsenautoimmunerkrankungen
KW  - Selenoproteine
KW  - TraceAge
Y1  - 2019
U6  - https://doi.org/10.4455/eu.2019.032
SN  - 0174-0008
VL  - 66
IS  - 9
SP  - M531
EP  - M536
PB  - Umschau-Zeitschriftenverl.
CY  - Frankfurt, Main
ER  - 
TY  - GEN
A1  - Schwarz, Maria
A1  - Lossow, Kristina
A1  - Kopp, Johannes F.
A1  - Schwerdtle, Tanja
A1  - Kipp, Anna Patricia
T1  - Crosstalk of Nrf2 with the Trace Elements Selenium, Iron, Zinc, and Copper
T2  - Postprints der Universität Potsdam : Mathematisch-Naturwissenschaftliche Reihe
N2  - Trace elements, like Cu, Zn, Fe, or Se, are important for the proper functioning of antioxidant enzymes. However, in excessive amounts, they can also act as pro-oxidants. Accordingly, trace elements influence redox-modulated signaling pathways, such as the Nrf2 pathway. Vice versa, Nrf2 target genes belong to the group of transport and metal binding proteins. In order to investigate whether Nrf2 directly regulates the systemic trace element status, we used mice to study the effect of a constitutive, whole-body Nrf2 knockout on the systemic status of Cu, Zn, Fe, and Se. As the loss of selenoproteins under Se-deprived conditions has been described to further enhance Nrf2 activity, we additionally analyzed the combination of Nrf2 knockout with feeding diets that provide either suboptimal, adequate, or supplemented amounts of Se. Experiments revealed that the Nrf2 knockout partially affected the trace element concentrations of Cu, Zn, Fe, or Se in the intestine, liver, and/or plasma. However, aside from Fe, the other three trace elements were only marginally modulated in an Nrf2-dependent manner. Selenium deficiency mainly resulted in increased plasma Zn levels. One putative mediator could be the metal regulatory transcription factor 1, which was up-regulated with an increasing Se supply and downregulated in Se-supplemented Nrf2 knockout mice.
T3  - Zweitveröffentlichungen der Universität Potsdam : Mathematisch-Naturwissenschaftliche Reihe - 1081 
KW  - Nrf2
KW  - selenium
KW  - iron
KW  - copper
KW  - zinc
KW  - homeostasis
Y1  - 2021
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:kobv:517-opus4-472873
SN  - 1866-8372
IS  - 1081
ER  - 
TY  - JOUR
A1  - Kopp, Johannes Florian
A1  - Müller, Sandra Marie
A1  - Pohl, Gabriele
A1  - Lossow, Kristina
A1  - Kipp, Anna Patricia
A1  - Schwerdtle, Tanja
T1  - A quick and simple method for the determination of six trace elements in mammalian serum samples using ICP-MS/MS
JF  - Journal of trace elements in medicine and biology
N2  - In order to assess the individual trace element status of humans for either medical or scientific purposes, amongst others, blood serum levels are determined. Furthermore, animal models are used to study interactions of trace elements. Most published methods require larger amounts (500-1000 mu L) of serum to achieve a reliable determination of multiple trace elements. However, oftentimes, these amounts of serum cannot be dedicated to a single analysis and the amount available for TE-determination is much lower. Therefore, a published ICP-MS/MS method for trace element determination in serum was miniaturized, optimized and validated for the measurement of Mn, Fe, Cu Zn, I and Se in as little as 50 mu L of human and murine serum and is presented in this work. For validation, recoveries of multiple LOTs and levels from commercially available human reference serum samples were determined, infra- and inter-day variations were assessed and limits of detection and quantification determined. It is shown, that the method is capable of giving accurate and reproducible results for all six elements within the relevant concentration ranges for samples from humans living in central Europe as well as from laboratory mice. As a highlight, the achieved limits of detection and quantification for Mn were found to be at 0.02 mu g/L serum and 0.05 mu g/L serum, respectively, while using an alkaline diluent for the parallel determination of iodine.
Y1  - 2019
U6  - https://doi.org/10.1016/j.jtemb.2019.04.015
SN  - 0946-672X
VL  - 54
SP  - 221
EP  - 225
PB  - Elsevier
CY  - München
ER  -