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    Publication Date: 2013-11-15
    Description: Introduction Enhanced progenitor proliferation, bone marrow (BM) hypervascularization and disturbed immune regulation contribute to the pathogenesis of myelodysplastic syndromes (MDS). Inhibition of mammalian-target of rapamycin (mTor) by temsirolimus (TEM) might be a promising strategy to target these disease-specific cellular alterations. We report on the effects of single agent TEM on the clinical course as well as on immune composition and BM vascularization of MDS patients treated within the prospective, multicenter “TEMDS”-trial (NCT01111448). Patients, Materials and Methods Twenty patients being either IPSS low/int-1 MDS (n = 9) or IPSS int-2/high after azacitidine failure were treated with TEM at a dose of 25 mg/week in the absence of toxicity or disease progression. BM was reevaluated after 4 months of treatment with the option of TEM continuation for a maximum of 12 months in responding patients. Translational research within this study included flowcytometry-based measurement of changes in T-cell composition as well as determination of cytokine levels and BM-vascularization prior to and after TEM. Results Of 20 patients treated, 15 discontinued TEM treatment prematurely due to intolerable side effects (n = 11), infectious complications (n = 3), or progression to AML (n = 1). Fatigue, stomatitis and profound leukopenia were the most frequent adverse events. A total of 13 severe adverse events were encountered in 10 patients and 1 patient died of infectious complications during TEM treatment. Of the 5 patients who were treated for at least 4 months and underwent regular BM reevaluation, none showed signs of response according to IWG criteria. TEM treatment resulted in a remarkable, although non-significant, decrease in total number of lymphocytes in the pB (pre: 74.6%, post: 48.4%, p = 0,083) and BM (pre: 23.5% post: 20.1%, p = 0.123). Within the T-helper cell compartment a trend towards an increase in regulatory T-cell (Treg) frequency was observed (pB: pre: 6.0 %, post: 6.4 %, p = 0.083). Moreover, the balance between naive (CD45RA+/CD45RO-) and activated/memory (CD45RA-/CD45RO+) Treg shifted significantly in favor of the latter (p = 0.004). Plasma analysis in BM and pB revealed, that these changes were obviously not mediated by alterations in TGFβ plasma levels. In a total of 12 assessable patients, a significant (p = 0.006) decrease of BM vascularization was observed after treatment with TEM for a median of 5 weeks (Fig. 1). There were, however, no changes in the medullary or peripheral blood VEGF concentration (data not shown). Conclusions Selective inhibition of the mTOR signaling cascade in MDS patients results in specific alterations of the composition of T-cell subsets as well as BM vascularization. Given the absence of any hematological response we suggest that these drug-induced modifications cannot alter the natural course of the disease. Disclosures: Wermke: Pfizer: Research Funding. Off Label Use: Temsirolimus is licensend for the treatment of MCL and RCC but not MDS. Platzbecker:Pfizer: Research Funding.
    Print ISSN: 0006-4971
    Electronic ISSN: 1528-0020
    Topics: Biology , Medicine
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  • 3
    Publication Date: 2014-12-06
    Description: Background Lenalidomide (LEN) results in hematopoietic improvement in the majority of treated patients with myelodysplastic syndrome and isolated deletion of the long arm of chromosome 5 (MDS-del5q). The drug is believed to exert antiangiogenetic, antiproliferative, proerythropoietic and immunomodulatory effects. The precise nature especially of the latter mode of action is incompletely understood. While some reports in multiple myeloma argue for an immunosuppressive effect, others proposed immunostimulatory properties. This prompted us to study the effects of LEN on the adaptive immune system in a cohort of patients with MDS-del5q. Patients, Material and Methods The composition of the T-cell compartment in peripheral blood (pB) and bone marrow (BM) of 11 patients with MDS-del5q treated within a multicenter, single-arm, phase II study of the German MDS study group (LEMON-5 trial) was studied by flow cytometry. Patients received LEN 10 mg per day for 21 days of each 28 day cycle. The median age was 71 years and 9 patients were female. Regulatory T-cells (Treg) were defined as CD3+CD4+CD25++CD127dimFoxP3+ while Th17 cells had to be CD3+CD4+ with positive intracellular staining for IL17 and negative intracellular staining for IFNgamma. Peripheral blood samples were taken prior to initiation of each new LEN cycle and BM specimens were obtained prior to treatment initiation and after 5 to 7 cycles of LEN. The results obtained in MDS patients were compared to a cohort of 27 healthy volunteer donors. Results After a median of 6 cycles all but one patient had responded with a hematologic improvement of erythrocytes, while 6 individuals achieved a complete morphologic and 5 a complete cytogenetic remission. In comparison to healthy donors, MDS patients had significantly lower frequencies of Treg in pB (5.0 vs. 7.4 %, p = 0.008) and BM (3.4 vs. 7.4 %, p = 0.006). After initiation of LEN treatment we observed a rapid increase in Treg frequencies in pB (Figure 1A) and after a median of 6 cycles the Treg were significantly more abundant in pB (9.6 % p = 0.001, Figure 1B) and BM (8.1 %, p = 0.016, Figure 1C) compared to baseline. The median Treg frequency reached the level observed in normal donors in BM and surpassed it in pB (Figure 1B+C). Fluorescence-in-situ hybridization demonstrated that the expanded Treg were not part of the malignant clone. Interestingly, although the median absolute lymphocyte count increased during LEN treatment (pre: 1.10 Gpt/l vs. post: 1.43 Gpt/l p = 0.013) there were no significant changes with respect to relative lymphocyte frequency (pre: 68.3 %, post: 75.61 %, p=0.499) or the percentage of T-effector cells (pre: 48.0 %, post: 51.5 %, p=0.520). Moreover, the expansion of Treg was not accompanied by a counter-regulatory increase of pro-inflammatory Th17-cells (pre: 2.3 % vs. post: 1.33 %, p = 0.328). To address a possible mechanism of the observed Treg expansion we analyzed the concentration of transforming growth factor beta (TGFbeta), a key factor contributing to the development of Treg, in pB and BM plasma. However, LEN treatment was not associated with an increase of TGFbeta levels in these two compartments. On the contrary, the TGFbeta levels after 6 cycles of LEN were significantly lower than pre-treatment values in pB and BM (pB 4.9 vs. 2.3 ng/ml, p = 0.039; BM 4.5 vs. 0.8 ng/ml, p = 0.023). Discussion Our results show that LEN treatment corrects an MDS-del5q-inherent Treg deficit. This Treg expansion is not accompanied by a counter-regulatory increase in pro-inflammatory Th17 or other T-effector cells and therefore possibly results in an immunosuppressive milieu, which might contribute to the beneficial effects of the drug on myelodysplastic hematopoiesis but may also facilitate leukemic progression. Figure 1 Figure 1. Disclosures Platzbecker: Celgene: Research Funding.
    Print ISSN: 0006-4971
    Electronic ISSN: 1528-0020
    Topics: Biology , Medicine
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  • 4
    Publication Date: 2021-03-29
    Description: In der vorliegenden Arbeit werden die Auswirkungen elektromagnetischer, sowie elektrostatischer Turbulenz speziell im Hinblick auf die Anwendung auf Jets aktiver galaktische Kerne untersucht. Dazu werden analytische Lösungen für ein Modell erstellt, dass bisher ausschließlich in numerischer Form vorlag. Mit Hilfe der analytischen Lösungen ist es nunmehr möglich, das Wechselspiel der unterschiedlichen, im Modell beschriebenen Prozesse zu analysieren. Ferner wird die Anwendbarkeit des Modelles durch Vergleich mit Datenmaterial bestätigt.
    Description: thesis
    Keywords: 523 ; TFG 000 ; TBK 000 ; Magnetohydrodynamik und Plasma-Astrophysik ; Hochenergieastronomie
    Language: German
    Type: monograph , publishedVersion
    Format: 110 S.
    Format: application/pdf
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