979 resultados para 1-lauroyl-2-(12-(S-methyldithio)docecanoyl)-sn-glycero-3-phosphocholine
Resumo:
Bibliograph. Nachweis: Paas P-308; Straus (1600/1700), Nr. 135
Resumo:
zusammengestellt von W. Voigt, O. le Roi (Zoologie) und A. Hahne (Botanik)
Resumo:
arr. par Stumpf
Resumo:
Vorbesitzer: Johann Maximilian Zum Jungen
Resumo:
von Telemann. [Text von Gottfried Simonis]
Resumo:
Signatur des Originals: S 36/F10826
Resumo:
Signatur des Originals: S 36/F11233
Resumo:
Signatur des Originals: S 36/G11012
Resumo:
Vorlesung: "Einführung in die Philosophie der Gegenwart", SS 1926, Typoskript mit eigenhändigen Korrekturen, 185 Blatt; Vortrag: "Über Sinn und Grenze einer soziologischen Behandlungen der Philosophie", 1928 (?), Typsokript mit eigenhändigen Korrekturen, 10 Blatt (GS 11, S. 209-220); Vortrag, gehalten zu Beginn der Vorlesung: "Max Scheler (1874-1928)", "Einführung in die Geschichtsphilosophie", SS 1928, Typoskript mit eigenhändigen Korrekturen, 13 Blatt (GS 11, 145-157); Vortrag: "Über Kantische und moderne Ethik" Typsokript mit eigenhändigen Korrekturen, 6 Blatt (GS 11, S. 138-144);
Resumo:
Entwürfe für ein Mögliches Forschungsprojekt über Liberlaismus des 19. Jahrhunderts; 1953; 1. Typoskript mit eigenhändigen Korrekturen von Theodor W. Adorno; 7 Blatt; 2. Typoskript mit eigenhändigen Korrekturen von Theodor W. Adorno; 3 Blatt; "Untersuchungn des sozialen Klimas in Stadt- und Landkreisen Hessens"; Entwürfe für ein "Handbuch der Methoden zur Messung des sozialen Klimas", nicht veröffentlicht; 1953; 1. Pollock, Friedrich: "Einführung" zum "Handbuch" a) Typoskript mit eigenhändigen Korrekturen; 8 Blatt; b) Typoskript mit eigenhändigen Korrekturen, 5 Blatt; c) Manuskript, "Vorwort"; 5 Blatt; d) Baumert, Gerhard: Entwurf des "Vorworts"; Typoskript mit handschriftlichen Korrekturen, 2 Blatt; e) Baumert, Gerhard: "Notizen zu Vorwort und Einführung des Handbuchs"; Typoskript, 1 Blatt; 2. Inhaltsverzeichnis zum "Handbuch"; 1 Blatt; 3. Pollock, Friedrich: eigenhändige Notizen zur Einführung; 7 Blatt; 4. Pollock, Friedrich: 1 eigenhändiger Brief mit Unterschrift an Theodor W. Adorno, Santa Monica, 21.09.1953; 1 Blatt; "Betriebsklime. Eine industrie-soziologische Untersuchung aus dem Ruhrgebiet" 1954-1956 veröffentlicht als Band 3 der Frankfurter Beiträge zur Soziologie, Frankfurt 1955; 1. Druckfahnen, mit handschriftlichen Korrekturen; 38 Blatt; 2. Korrektur-Notizen zu den Druckfahnen; 4 Blatt; 3. Adorno, Theodor W. [Mitarbeit]: "Grundreiz [Betriebsumfrage)" a) Typoskript mit handschriftlichen Korrekturen, 4 Blatt; b) Typoskript, 5 Blatt; 4. Adorno, Theodor W.: 1 Brief an Max Horkheimer, ohne Ort, 30.06.1954; 1 Blatt; 5. Fragebogen- Entwurf; Typsokript, 2 Blatt; 6. Fragebogen- Entwurf; Typoskript, 2 Blatt; 7. Adorno, Theodor W.: 1 Brief an Max Horkheimer, ohne Ort, ohne Datum [1954]; 1 Blatt; 8. Dirks, Walter: "Notiz über meine Reise nach Köln, Düsseldorf und Essen", 22.02.1955. Typoskript, 2 Blatt; 9. Becker, Hellmut: "Aktennotiz, Betreff: Ersetzung der Pressekonferenz über die Mannesmann-Studie durch in den nächsten Wochen und Monaten aufeinanderfolgende Artikel qualifizierter Korrespondenten", 15.02.1955. Typoskript, 1 Blatt; 10. Adorno, Theodor W.: 1 Brief an Hermann Winkhaus, Mannesmann AG, ohne Ort, 05.03.1956; 2 Blatt; 11. Winkhaus, Hermann, Mannesmann AG: 1 Breifabschrift an das Institut für Sozialforschung, Düsseldorf, 18.07.1955; 12. Presseveröffentlichungen zur Betriebsklima-Untersuchung; 1 Ordner, 13 Blatt; 13. Zeitschriftenartikel und Abschriften von Artikeln zur Betriebsklima- Untersuchung; mit: Becker, Egon: 2 Briefe mit Unterschrift an Max Horkheimer, Frankfurt, 1955; 1 Brief von Max Horkheimer, Zürich, 25.10.1955; Sardemann, Karl: Interview mit einem Juden über sein Leben 1933 bis circa 1953, insbesondere seine Erlebnisse im Konzentrationslager; 1955; 1. Interview; Typsokript, 38 Blatt; 2. Sardemann, Karl: 1 Brief mit Unterschrift an Max Horkheimer, ohne Ort, 15.12.1955; 1 Blatt; "Altersbild und Altersvorsorge der Arbeiter und Angestellten" veröffentlicht als Sonderheft 1 der Frankfurter Beiträge zur Soziologie, Frankfurt 1958.; Zwischenbericht zum Projekt und Material, 1955; 1. Becker, Egon, u.a.: "Zwischenbericht" 10.03.1953; Typoskript, 9 Blatt; mit einem Brief mit Unterschrift von Egon Becker an Max Horkheimer, ohne Ort, 11.03.1955; 1 Blatt; 2. Fragebogen; als Typoskript vervielfältigt, 16 Blatt; 3. Fragebogen; als Typoskript vervielfältigt, 11 Blatt;
Resumo:
von I. N. Mannheimer. Aus dessen schriftl. Nachlasse hrsg. [von S. Hammerschlag]
Resumo:
A growing number of studies show strong associations between stress and altered immune function. In vivo studies of chronic and acute stress have demonstrated that cognitive stressors are strongly correlated with high circulating levels of catecholamines (CT) and corticosteroids (CS) that are associated with changes in type-1/type-2 cytokine expression. Although individual pharmacologic doses of CS and CT can inhibit the expression of T-helper 1 (Th1, type-1 like) and promote the production of T-helper 2 (Th2, type-2 like) cytokines in antigen-specific and mitogen stimulated human leukocyte cultures in vitro, little attention has been focused on the effects of combination physiologic-stress doses of CT and CS that may be more physiologically relevant. In addition, both in-vivo and in-vitro studies suggest that the differential expression of the B7 family of costimulatory molecules CD80 and CD86 may promote the expression of type-1 or type-2 cytokines, respectively. Furthermore, corticosteroids can influence the expression of β2-adrenergic receptors in various human tissues. We therefore investigated the combined effects of physiologic-stress doses of in vitro CT and CS upon the type-1/type-2 cytokine balance and expression of B7 costimulatory molecules of human peripheral blood mononuclear cells (PBMC) as a model to study the immunomodulatory effects of physiologic stress. Results demonstrated a significant decrease in type-1 cytokine expression and a significant increase in type-2 cytokine production in our CS+CT incubated cultures when compared to either CT or CS agents alone. In addition, we demonstrated the differential expression of CD80/CD86 in favor of CD86 at the cellular and population level as determined by flow cytometry in lipopolysaccharide stimulated human Monocytes. Furthermore, we developed flow cytometry based assays to detect total β2AR in human CD4+ T-lymphocytes that demonstrated decreased expression of β2AR in mitogen stimulated CD4+ T-lymphocytes in the presence of physiologic stress levels of CS and CT as single in vitro agents, however, when both CS and CT were combined, significantly higher expression of β2AR was observed. In summary, our in vitro data suggest that both CS and CT work cooperatively to shift immunity towards type-2 responses. ^
Resumo:
Several immune pathologies are the result of aberrant regulation of T lymphocytes. Pronounced T cell proliferation can result in autoimmunity or hematologic malignancy, whereas loss of T cell activity can manifest as immunodeficiency. Thus, there is a critical need to characterize the signal transduction pathways that mediate T cell activation so that novel and rational strategies to detect and effectively control T cell mediated disease can be achieved. ^ The first objective of this dissertation was to identify and characterize novel T cell regulatory proteins that are differentially expressed upon antigen induced activation. Using a functional proteomics approach, two members of the prohibitin (Phb) family of proteins, Phb1 and Phb2, were determined to be upregulated upon activation of primary human T cells. Furthermore, their regulated expression was dependent upon CD3 and CD28 signaling pathways which synergistically increased their expression. In contrast to previous reports of Phb nuclear localization, both proteins were determined to localize to the mitochondrial inner membrane of human T cells. Additionally, novel Phb phosphorylation sites were identified and characterized using mass spectrometry, phosphospecific antibodies and site directed mutagenesis. ^ Prohibitins have been proposed to play important roles in cancer development however the mechanism of action has not been elucidated. The second objective of this dissertation was to define the functional role of Phbs in T cell activity, survival and disease. Compared to levels in normal human T cells, Phb expression was higher in the human tumor T cell line Kit225 and subcellularly localized to the mitochondrion. Ablation of Phb expression by siRNA treatment of Kit225 cells resulted in disruption of mitochondrial membrane potential and significantly enhanced their sensitivity to cell death, suggesting they serve a protective function in T cells. Furthermore, Q-RT-PCR analysis of human oncology cDNA expression libraries indicated the Phbs may represent hematological cancer biomarkers. Indeed, Phb1 and Phb2 protein levels were 6-10 fold higher in peripheral blood mononuclear cells isolated from malignant lymphoma and multiple myeloma patients compared to healthy individuals. ^ Taken together, Phb1 and Phb2 are novel phosphoproteins upregulated during T cell activation and transformation to function in the maintenance of mitochondrial integrity and perhaps energy metabolism, thus representing previously unrecognized intracellular biomarkers and therapeutic targets for regulating T cell activation and hematologic malignancies. ^
Resumo:
Vitamin C (ascorbic acid--AA) can have a substantial impact on human health by reducing the incidence and/or severity of coryza. Studies also suggest it has immunomodulatory functions in humans. Immune function is controlled by cytokines, such as type-1 cytokines (IFNγ) that promote antiviral immunity and type-2 cytokines (IL-4, IL-10) that promote humoral immunity. Knowing the mechanisms responsible for both antiviral immunity and type-1/type-2 cytokine balance, we sought to identify AA-induced alterations of human peripheral blood mononuclear cells (PBMC) in vivo and in vitro . We hypothesized that AA modulates the immune system, altering both number and function of PBMC. We first described the effect of 14 days of oral (1 gram) AA in healthy subjects. AA increased circulating natural killer (NK) cells, CD25+ and HLA-DR+ T cells, and PMA/ionomycin-stimulated intracellular IFNγ. We subsequently developed models for in vitro use. We determined that AA was toxic in vitro to T cells when used at doses found intracellularly but doses found in plasma from individuals taking 1gm/day AA were nontoxic. The model that most fully reproduced our in vivo intracellular cytokine findings used dehydroascorbic acid and buffers to deliver AA intracellularly. This model generated the largest increase in IFNγ at physiologic plasma concentrations. Previous studies demonstrate that chronic psychological stress is associated with a type-2 cytokine response. We hypothesized that vitamin C could prevent the type-2 cytokine shift associated with stress. In a study of medical students taking 1 g AA or placebo, a significant increase in IFNγ was seen intracellularly in CD4+ and CD8+ cells and in tetanus-stimulated cultures in the AA group only. We also observed increases in IFNγ/IL-4 and IFNγ/IL-10 ratios with AA supplementation, indicating a type-1 shift. Furthermore, we noted increased numbers of NK cells and activated T cells in the peripheral blood in the AA treated group only. Lastly, we investigated the role of the CD40L/CD40 and CD28/B7 costimulatory pathway in these cytokine alterations. AA did not have any effect on either pathway studied. Thus costimulatory pathways are not contributing to AA induced modulation of the type-1/type-2 immune balance. ^
