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  • 1995-1999  (3)
  • 1
    Electronic Resource
    Electronic Resource
    New York : Cambridge University Press
    International organization 49 (1995), S. 415-450 
    ISSN: 0020-8183
    Source: Cambridge Journals Digital Archives
    Topics: Political Science
    Notes: Systemic theories of international politics are inadequate for explaining particular states' policies, and some neorealists reach for supplementary foreign-policy-level concepts. Yet these studies almost never provide the empirical evidence required by their motivational constructs. Available psychological studies rely too heavily on notions peculiar to the cold war—such as the image of the enemy. A new theory proposes four additional ideal-type images. Each image is likely to lead to a specified set of strategic behaviors. An application to dyadic relations across the Persian Gulf from 1977 through 1990 suggests that this theory can help account for otherwise puzzling behavior, and it illustrates a promising route toward a more sensitive interactionist international relations theory suited both to the former superpower relationship and to diverse others.
    Type of Medium: Electronic Resource
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  • 2
    ISSN: 1432-0851
    Keywords: Key words Gene therapy ; Cytokine ; NK ; Xenogenic
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Abstract Eleven patients with advanced cancer were treated in a clinical gene therapy trial by repeated intra- tumoral injections with different doses of xenogenic fibroblasts secreting high amounts of human interleukin-2 (Vero-IL2). Treatments in a total of 14 courses were well tolerated and resulted in clinical responses and measurable biological effects. Together with increases in serum interleukin-2 (IL-2), modifications of the V-β T cell receptor repertoire and induction of intratumoral T-cell infiltration were observed. When the intratumoral expression of endogenous cytokine genes and the persistence of the IL-2 transgene at the application site and in peripheral blood were investigated, rapid disappearance of the transgene at the application site appeared to be the most prominent biological effect. Tests detecting a single Vero-IL2 cell against a background of 105 non-transfected cells were not able to demonstrate significant expression of exogenous IL-2 (i.e. the transgene or transgene-carrying cells) in tumor biopsies or blood at different times. Therefore, further studies were performed to evaluate the mechanism(s) involved in the rapid disappearance of xenogenic carrier cells in more detail. We show here that significant in vitro cytotoxicity against transgene-carrying Vero cells can be observed in peripheral blood of all the patients before treatment as well as in healthy controls. “Cold” target inhibition shows that significant killing of Vero-IL2 cells is mediated by natural killer (NK) cells. This was confirmed by showing that established CD3−/CD16 + /CD56 + peripheral blood NK cell clones kill both K562 and Vero-IL2 target cells. The failure of other mechanisms (complement, antibody-dependent cell cytotoxicity or cytotoxic T lymphocytes) to destroy xenogenic, histoincompatible Vero cells in vitro suggests that NK cells also might be responsible for the killing of Vero-IL2 in vivo and for the failure to detect the transgene at the application site. These results might also be of importance for some aspects of the current discussion of xenotransplantation.
    Type of Medium: Electronic Resource
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  • 3
    Electronic Resource
    Electronic Resource
    Springer
    Journal of cancer research and clinical oncology 122 (1996), S. 671-675 
    ISSN: 1432-1335
    Keywords: p53 ; MDR1 ; Colorectal cancer ; Metastasis
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Abstract Overexpression of the multidrug resistanceMDR1 gene is thought to contribute to drug resistance in non-responsive cancers like colorectal carcinoma. Little is known about the mechanisms by which expression ofMDR1 is regulated in human tumours. However, there is growing evidence that regulation primarily takes place at the transcriptional level and that the process of tumour progression is related to activation of theMDR1 gene. Mutations in thep53 tumour-suppression gene occur in approximately 70% of colorectal cancers. As a transcriptional regulator,p53 might be involved in regulation ofMDR1 expression in these tumours. We therefore determinedMDR1 expression using the differential polymerase chain reaction technique in 30 colorectal tumours (4 primaries and 26 metastates) and correlated our results with previously reported data onp53 in the same group of patients. We found a significant positive correlation betweenp53 andMDR1 expression inp53-mutated tumours (P=0.005;r=0.596), but not in tumours without ap53 mutation. In addition, we observed a tendency towards higherMDR1 expression levels in tumours carryingp53 mutations (P=0.14) compound to wild-typep53 tumours. These data indicate that mutantp53 may play a role in the regulation ofMDR1 expression in human cholorectal cancer.
    Type of Medium: Electronic Resource
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