TY - JOUR A1 - Ascierto, Maria Libera A1 - Worschech, Andrea A1 - Yu, Zhiya A1 - Adams, Sharon A1 - Reinboth, Jennifer A1 - Chen, Nanhai G A1 - Pos, Zoltan A1 - Roychoudhuri, Rahul A1 - Di Pasquale, Giovanni A1 - Bedognetti, Davide A1 - Uccellini, Lorenzo A1 - Rossano, Fabio A1 - Ascierto, Paolo A A1 - Stroncek, David F A1 - Restifo, Nicholas P A1 - Wang, Ena A1 - Szalay, Aladar A A1 - Marincola, Francesco M T1 - Permissivity of the NCI-60 cancer cell lines to oncolytic Vaccinia Virus GLV-1h68 JF - BMC Cancer N2 - Background: Oncolytic viral therapy represents an alternative therapeutic strategy for the treatment of cancer. We previously described GLV-1h68, a modified Vaccinia Virus with exclusive tropism for tumor cells, and we observed a cell line-specific relationship between the ability of GLV-1h68 to replicate in vitro and its ability to colonize and eliminate tumor in vivo. Methods: In the current study we surveyed the in vitro permissivity to GLV-1h68 replication of the NCI-60 panel of cell lines. Selected cell lines were also tested for permissivity to another Vaccinia Virus and a vesicular stomatitis virus (VSV) strain. In order to identify correlates of permissity to viral infection, we measured transcriptional profiles of the cell lines prior infection. Results: We observed highly heterogeneous permissivity to VACV infection amongst the cell lines. The heterogeneity of permissivity was independent of tissue with the exception of B cell derivation. Cell lines were also tested for permissivity to another Vaccinia Virus and a vesicular stomatitis virus (VSV) strain and a significant correlation was found suggesting a common permissive phenotype. While no clear transcriptional pattern could be identified as predictor of permissivity to infection, some associations were observed suggesting multifactorial basis permissivity to viral infection. Conclusions: Our findings have implications for the design of oncolytic therapies for cancer and offer insights into the nature of permissivity of tumor cells to viral infection. KW - gene-therapy KW - adenovirus KW - receptor KW - identification KW - infection KW - CD9 KW - panel Y1 - 2011 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-141503 VL - 11 IS - 451 ER - TY - THES A1 - Plochmann, Kathrin T1 - Bioassays zur Untersuchung der biologischen Aktivität von Flavonoiden und Ermittlung eines zellulären Rezeptormoleküls von foamyviralen Vektoren T1 - Bioassay to investigate the biological activity of flavonoids and research to discover the foamyviral receptor N2 - Aufgrund ihrer gut dokumentierten, umfangreichen gesundheitsfördernden biologischen Aktivitäten wird den Flavonoiden eine große Bedeutung zugeordnet. Die Ergebnisse von in vitro- und Tierstudien deuten zudem darauf hin, dass diese Verbindungen bei der Prävention und Therapie von Erkrankungen wie Krebs oder Alzheimer Krankheit (AD) positive Effekte zeigen. Zur besseren Charakterisierung der Interaktion von Flavonoiden mit Krebszellen wurden von uns die Cytotoxizität verschiedener Flavonoide auf T-Lymphoblastomzellen untersucht und Strukturelemente identifiziert, welche für einen Flavonoid-induzierten Zelltod relevant sind. Weitere Studien waren der potentiell neuroprotektiven Wirkung von Flavonoiden gewidmet. Die sowohl in neuronalen Zellkulturen als auch in transgenen Alzheimer-Mäusen (TgAPPsw) festgestellte Erhöhung der sAPPα Produktion und Reduktion von Aβ-Bildung wurden mit Aktivitäts- und Expressionssteigerung der α-Sekretase ADAM-10 assoziiert. Um herauszufinden, ob Flavonoide eine neuroprotektive Wirkung zeigen, wurden erste Vorbereitungen für ein Flavonoid-Screening mit einer sowohl hAPP alsauch ADAM-10 stabil transfizierten HT1080 Zellen getroffen. Dies beinhaltete die Suche nach einer potenten siRNA/shRNA und einem effektiven Flavonoid. Im zweiten Teil der Arbeit wurden Experimente durchgeführt, um die Rolle von Heparansulfat (HS) bei der foamyviralen Anbindung an die Wirtszelle zu untersuchen. Foamyviren (FV) sind Spumaviren und gehören zur Familie der Retroviren. Bei unseren Studien wurde die Bindung von FV an Heparin, die Korrelation der Suszeptibilität verschiedener Zellen mit zellulärem HS und die Reduktion der Infektion durch lösliches Heparin sowie durch enzymatischen HS-Abbau festgestellt. N2 - Flavonoids have well-documented, beneficial biological effects. Furthermore different in vitro- and animal-experiments indicate that these compounds demonstrate positive effects in prevention and therapy of diseases, like cancer or neurodegenerative diseases. In order to characterize the interactionsbetween flavonoids and cancer cells, we examined the cytotoxicity of different flavonoids on a human leukemia cell line and identified structure elements that could be associated to flavonoid-induced cell death. Our further studies were dedicated to the potentially neuroprotective activity of flavonoids. It has been described that in neuronal cells as well as in transgenic AD mice EGCG increases levels of sAPPα- and reduces Aβ-production. This influence of EGCG was associated with enhanced activity and expression of the α-secretase, ADAM-10. To find out, if flavonoids showed neuroprotective activity, preliminary work for a later flavonoid screening on hAPP and ADAM-10 wit stably-transfected HT1080 cells was done. This includes the determination of flavonoid candidates and research of effective siRNAs towards ADAM-10. Furtherrmore we investigated the role of heparansulfat (HS) in attachment of FV to host cell. Foamyviruses (FV) are retroviruses and belong to the subfamily of spumaretroviruses. In our studies we discovered the binding of FV on heparin, the correlation between susceptibility of different cells and cellular HS and the reduction of infectivity through soluble heparin and through enzymatic HS-degradation. KW - Flavonoide KW - Biologische Aktivität KW - Bioassay KW - Virusrezeptor KW - Spumaviren KW - T-Lymphoblastomzellen KW - ADAM-10 KW - alpha-Sekretase KW - Cytotoxizität KW - T-Zell-Leukämie KW - Alzheimer-Krankheit KW - Spumaviren KW - Virusrezeptor KW - Heparansulfat KW - flavonoids KW - cytotoxicity KW - alzheimer's disease KW - foamy virus KW - receptor Y1 - 2011 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-65183 ER -