Your search keyword '"Ganser, Arnold"' showing total 125 results

1. The graft-versus-leukemia effect of prophylactic donor lymphocyte infusions after allogeneic stem cell transplantation is equally effective in relapse prevention but safer compared to spontaneous graft-versus-host disease.

Author

Stadler, Michael, Hambach, Lothar, Dammann, Elke, Diedrich, Helmut, Kamal, Haytham, Hamwi, Iyas, Schultze-Florey, Christian, Varvenne, Michael, Ehrlich, Steve, Buchholz, Stefanie, Koenecke, Christian, Beutel, Gernot, Weissinger, Eva M., Krauter, Jürgen, Eder, Matthias, Hertenstein, Bernd, and Ganser, Arnold

Subjects

STEM cell transplantation, HEMATOPOIETIC stem cell transplantation, GRAFT versus host disease, PROGRESSION-free survival, ACUTE diseases, LYMPHOCYTES, DISEASE relapse, ACUTE leukemia

Abstract

Therapeutic donor lymphocyte infusions (tDLI) are used to reinforce the graft-versus-leukemia (GvL) effect in relapse after allogeneic stem cell transplantation (alloSCT). In contrast, the role of prophylactic DLI (proDLI) in preventing leukemia relapse has been less clearly established, although supported by retrospective, case-control, and registry analyses. We report a prospective, monocentric, ten year cohort of patients with high risk acute leukemias (AL) or myelodysplasia (MDS) in whom proDLI were applied beyond day +120 post alloSCT to compensate for lack of GvL. 272 consecutive allotransplanted AL or MDS patients in complete remission and off immunosuppression at day +120 were stratified according to the prior appearance of relevant GvHD (acute GvHD °II-IV or extensive chronic GvHD) as a clinical indicator for GvL. Escalating doses of unmodified proDLI were applied to 72/272 patients without prior relevant GvHD. Conversely, 157/272 patients with prior spontaneous GvHD did not receive proDLI, nor did 43/272 patients with contraindications (uncontrolled infections, patient refusal, DLI unavailability). By day 160-landmark analysis (median day of first DLI application), proDLI recipients had significantly higher five-year overall (OS) and disease free survival (DFS) (77% and 67%) than patients with spontaneous GvHD (54% and 53%) or with contraindications (46% and 45%) (p=0.003). Relapse incidence for patients with proDLI (30%) or spontaneous GvHD (29%) was significantly lower than in patients with contraindications (39%; p=0.021). With similar GvHD incidence beyond day +160, non-relapse mortality (NRM) was less with proDLI (5%) than without proDLI (18%; p=0.036). In conclusion, proDLI may be able to compensate for lack of GvL in alloSCT recipients with high risk AL or MDS. [ABSTRACT FROM AUTHOR]

Published

2023

2. Improving survival in metastatic renal cell carcinoma (mRCC) patients: do elderly patients benefit from expanded targeted therapeutic options?

Author

Eggers, Hendrik, Schünemann, Christoph, Grünwald, Viktor, Rudolph, Linda, Tiemann, Maria-Luisa, Reuter, Christoph, Anders-Meyn, Merle Freya, Ganser, Arnold, and Ivanyi, Philipp

Subjects

OLDER patients, RENAL cell carcinoma, AGE groups, METASTASIS, SURVIVAL rate

Abstract

Introduction: Treatment advances in metastatic renal cell carcinoma (mRCC) have improved overall survival (OS) in mRCC patients over the last two decades. This single center retrospective analysis assesses if the purported survival benefits are also applicable in elderly mRCC patients. Methods: 401 patients with mRCC treated at Hannover Medical School from 01/2003–05/2016 were identified and evaluated by chart review. Treatment periods were defined as 01.01.2003–31.12.2009 (P1) and 01.01.2010–31.05.2016 (P2). Age groups were defined according to WHO classes (≤ 60 years: younger, > 60–75 years: elderly and > 75 years: old). Descriptive statistics, Kaplan–Meier analysis and logistic regression were performed. Results: Median OS improved from 35.1 months in P1 to 59.1 months in P2. Sub-division into the respective age groups revealed median survival of 38.1 (95%-CI: 28.6–47.6) months in younger patients, 42.9 (95%-CI: 29.5–56.3) months among elderly patients and 27.3 (95%-CI: 12.8–41.8) months among old patients. Risk reduction for death between periods was most evident among old patients (young: HR 0.71 (95%-CI: 0.45–1.13, p = 0.2); elderly: HR 0.62 (95%-CI: 0.40–0.97, p = 0.04); old: HR 0.43 (95%-CI: 0.18–1.05, p = 0.06)). Age ≥ 75 years was an independent risk factor for death in P1 but not in P2. Conclusion: Improved OS in the targeted treatment period was confirmed. Surprisingly elderly and old patients seem to profit the most form expansion of therapeutic armamentarium, within the TKI-dominated observation period. [ABSTRACT FROM AUTHOR]

Published

2022

3. Unified classification and risk-stratification in Acute Myeloid Leukemia.

Author

Tazi, Yanis, Arango-Ossa, Juan E., Zhou, Yangyu, Bernard, Elsa, Thomas, Ian, Gilkes, Amanda, Freeman, Sylvie, Pradat, Yoann, Johnson, Sean J., Hills, Robert, Dillon, Richard, Levine, Max F., Leongamornlert, Daniel, Butler, Adam, Ganser, Arnold, Bullinger, Lars, Döhner, Konstanze, Ottmann, Oliver, Adams, Richard, and Döhner, Hartmut

Subjects

ACUTE myeloid leukemia, CLINICAL decision support systems, INDUCTION chemotherapy, NOSOLOGY, SYMPTOMS

Abstract

Clinical recommendations for Acute Myeloid Leukemia (AML) classification and risk-stratification remain heavily reliant on cytogenetic findings at diagnosis, which are present in <50% of patients. Using comprehensive molecular profiling data from 3,653 patients we characterize and validate 16 molecular classes describing 100% of AML patients. Each class represents diverse biological AML subgroups, and is associated with distinct clinical presentation, likelihood of response to induction chemotherapy, risk of relapse and death over time. Secondary AML-2, emerges as the second largest class (24%), associates with high-risk disease, poor prognosis irrespective of flow Minimal Residual Disease (MRD) negativity, and derives significant benefit from transplantation. Guided by class membership we derive a 3-tier risk-stratification score that re-stratifies 26% of patients as compared to standard of care. This results in a unified framework for disease classification and risk-stratification in AML that relies on information from cytogenetics and 32 genes. Last, we develop an open-access patient-tailored clinical decision support tool. Classification and risk-stratification for Acute Myeloid Leukemia (AML) at diagnosis are primarily based on cytogenetics and only a few gene mutations. Here, the authors study the genomic landscape of 3653 AML patients and characterize 16 non-overlapping molecular subgroups of clinical relevance for disease classification and risk prognostication. [ABSTRACT FROM AUTHOR]

Published

2022

4. Haploidentical transplantation and posttransplant cyclophosphamide for treating aplastic anemia patients: a report from the EBMT Severe Aplastic Anemia Working Party

Author

Prata, Pedro H., Eikema, Dirk-Jan, Afansyev, Boris, Bosman, Paul, Smiers, Frans, Diez-Martin, José L., Arrais Rodrigues, Celso, Koc, Yener, Poire, Xavier, Sirvent, Anne, Kroger, Nicolaus, Porta, Fulvio, Holter, Wolfgang, Bloor, Adrian, Jubert, Charlotte, Ganser, Arnold, Tanase, Alina, Menard, Anne-Lise, Pioltelli, Pietro, Pérez-Simón, José A., Ho, Aloysius, Aljurf, Mahmoud, Russell, Nigel, Labussiere-Wallet, Helene, Kerre, Tessa, Rocha, Vanderson, Socie, Gerard, Risitano, Antonio, Dufour, Carlo, Peffault de Latour, Regis, Prata, Pedro H., Eikema, Dirk-Jan, Afansyev, Boris, Bosman, Paul, Smiers, Frans, Diez-Martin, José L., Arrais Rodrigues, Celso, Koc, Yener, Poire, Xavier, Sirvent, Anne, Kroger, Nicolaus, Porta, Fulvio, Holter, Wolfgang, Bloor, Adrian, Jubert, Charlotte, Ganser, Arnold, Tanase, Alina, Menard, Anne-Lise, Pioltelli, Pietro, Pérez-Simón, José A., Ho, Aloysius, Aljurf, Mahmoud, Russell, Nigel, Labussiere-Wallet, Helene, Kerre, Tessa, Rocha, Vanderson, Socie, Gerard, Risitano, Antonio, Dufour, Carlo, and Peffault de Latour, Regis

Abstract

In the absence of an HLA-matched donor, the best treatment for acquired aplastic anemia patients refractory to immunosuppression is unclear. We collected and analyzed data from all acquired aplastic anemia patients who underwent a haploidentical transplantation with posttransplant cyclophosphamide in Europe from 2011 to 2017 (n = 33). The cumulative incidence of neutrophil engraftment was 67% (CI95%: 51–83%) at D +28 and was unaffected by age group, stem cell source, ATG use, or Baltimore conditioning regimen. The cumulative incidence of grades II–III acute GvHD was 23% at D +100, and limited chronic GvHD was 10% (0–20) at 2 years, without cases of grade IV acute or extensive chronic GvHD. Two-year overall survival was 78% (64–93), and 2-year graft-versus-host disease-free survival was 63% (46–81). In univariate analysis, the 2-year OS was higher among patients who received the Baltimore conditioning regimen (93% (81–100) versus 64% (41–87), p = 0.03), whereas age group, stem cell source, and ATG use had no effect. Our results using unmanipulated haploidentical transplantation and posttransplant cyclophosphamide for treating refractory AA patients are encouraging, but warrant confirmation in a prospective study with a larger number of patients and longer follow-up.

Published

2019

5. Impact of sarcopenia in advanced and metastatic soft tissue sarcoma.

Author

Strassmann, Dennis, Hensen, Bennet, Grünwald, Viktor, Stange, Katharina, Eggers, Hendrik, Länger, Florian, Omar, Mohamed, Zardo, Patrick, Christiansen, Hans, Reuter, Christoph W., Wacker, Frank K., Ganser, Arnold, and Ivanyi, Philipp

Subjects

SARCOMA, SARCOPENIA, PROGRESSION-free survival, OVERALL survival, BODY composition

Abstract

Introduction: Advanced or metastatic soft tissue sarcoma (a/mSTS) is associated with a dismal prognosis. Patient counseling on treatment aggressiveness is pivotal to avoid over- or undertreatment. Recently, evaluation of body composition markers like the skeletal muscle index (SMI) became focus of interest in a variety of cancers. This study focuses on the prognostic impact of SMI in a/mSTS, retrospectively. Methods: 181 a/mSTS patients were identified, 89 were eligible due to prespecified criteria for SMI assessment. Baseline CT-Scans were analyzed using an institutional software solution. Sarcopenia defining cut-off values for the SMI were established by optimal fitting method. Primary end point was overall survival (OS) and secondary endpoints were progression free survival (PFS), disease control rate (DCR), overall response rate (ORR). Descriptive statistics as well as Kaplan Meier- and Cox regression analyses were administered. Results: 28/89 a/mSTS patients showed sarcopenia. Sarcopenic patients were significantly older, generally tended to receive less multimodal therapies (62 vs. 57 years, P = 0.025; respectively median 2.5 vs. 4, P = 0.132) and showed a significantly lower median OS (4 months [95%CI 1.9–6.0] vs. 16 months [95%CI 8.8–23.2], Log-rank P = 0.002). Sarcopenia was identified as independent prognostic parameter of impaired OS (HR 2.40 [95%-CI 1.4–4.0], P < 0.001). Moreover, DCR of first palliative medical treatment was superior in non-sarcopenic patients (49.2% vs. 25%, P = 0.032). Conclusion: This study identifies sarcopenia as a prognostic parameter in a/mSTS. Further on, the data suggest that sarcopenia shows a trend of being associated with first line therapy response. SMI is a promising prognostic parameter, which needs further validation. [ABSTRACT FROM AUTHOR]

Published

2021

6. Prognostic role of docetaxel-induced suppression of free testosterone serum levels in metastatic prostate cancer patients.

Author

Kappler, Paula, Morgan, Michael A., Ivanyi, Philipp, Brunotte, Stefan J., Ganser, Arnold, and Reuter, Christoph W. M.

Subjects

DOCETAXEL, PROSTATE cancer patients, TESTOSTERONE, OVERALL survival, DISEASE progression

Abstract

To date, only few data concerning the biologically active, free form of testosterone (FT) are available in metastatic prostate cancer (mPC) and the impact of FT on disease, therapy and outcome is largely unknown. We retrospectively studied the effect of docetaxel on FT and total testosterone (TT) serum levels in 67 mPC patients monitored between April 2008 and November 2020. FT and TT levels were measured before and weekly during therapy. The primary endpoint was overall survival (OS). Secondary endpoints were prostate-specific antigen response and radiographic response (PSAR, RR), progression-free survival (PFS), FT/TT levels and safety. Median FT and TT serum levels were completely suppressed to below the detection limit during docetaxel treatment (FT: from 0.32 to < 0.18 pg/mL and TT: from 0.12 to < 0.05 ng/mL, respectively). Multivariate Cox regression analyses identified requirement of non-narcotics, PSAR, complete FT suppression and FT nadir values < 0.18 pg/mL as independent parameters for PFS. Prior androgen-receptor targeted therapy (ART), soft tissue metastasis and complete FT suppression were independent prognostic factors for OS. FT was not predictive for treatment outcome in mPC patients with a history of ART. [ABSTRACT FROM AUTHOR]

Published

2021

7. Phase I/II trial of lenalidomide, methotrexate, leucovorin, cytarabine, and rituximab (LeMLAR) in relapsed or refractory diffuse large B cell lymphoma.

Author

Dührsen, Ulrich, Tometten, Mareike, Kroschinsky, Frank, Ganser, Arnold, Ibach, Stefan, Bertram, Stefanie, and Hüttmann, Andreas

Subjects

METHOTREXATE, RITUXIMAB, B cell lymphoma

Published

2021

8. Measurable residual disease status and outcome of transplant in acute myeloid leukemia in second complete remission: a study by the acute leukemia working party of the EBMT.

Author

Gilleece, Maria H., Shimoni, Avichai, Labopin, Myriam, Robinson, Stephen, Beelen, Dietrich, Socié, Gerard, Unal, Ali, Ganser, Arnold, Vitek, Antonin, Sengeloev, Henrik, Yakoub-Agha, Ibrahim, Tholouli, Eleni, Polge, Emmanuelle, Mohty, Mohamad, and Nagler, Arnon

Subjects

ACUTE myeloid leukemia, DISEASE remission, HEMATOPOIETIC stem cell transplantation, HLA histocompatibility antigens, CANCER relapse

Abstract

Measurable residual disease (MRD) prior to hematopoietic cell transplant (HCT) for acute myeloid leukemia (AML) in first complete morphological remission (CR1) is an independent predictor of outcome, but few studies address CR2. This analysis by the Acute Leukemia Working Party of the European Society for Blood and Marrow Transplantation registry assessed HCT outcomes by declared MRD status in a cohort of 1042 adult patients with AML CR2 at HCT. Patients were transplanted 2006–2016 from human leukocyte antigen (HLA) matched siblings (n = 719) or HLA 10/10 matched unrelated donors (n = 293). Conditioning was myeloablative (n = 610) or reduced-intensity (n = 432) and 566 patients (54%) had in-vivo T cell depletion. At HCT, 749 patients (72%) were MRD negative (MRD NEG) and 293 (28%) were MRD positive (MRD POS). Time from diagnosis to HCT was longer in MRD NEG than MRD POS patients (18 vs. 16 months (P < 0.001). Two-year relapse rates were 24% (95% CI, 21–28) and 40% (95% CI, 34–46) in MRD NEG and MRD POS groups (P < 0.001), respectively. Leukemia-free survival (LFS) was 57% (53–61) and 46% (40–52%), respectively (P = 0.001), but there was no difference in terms of overall survival. Prognostic factors for relapse and LFS were MRD NEG status, good risk cytogenetics, and longer time from diagnosis to HCT. In-vivo T cell depletion predicted relapse. [ABSTRACT FROM AUTHOR]

Published

2021

9. Severe allo-immune antibody-associated peripheral and central nervous system diseases after allogeneic hematopoietic stem cell transplantation.

Author

Hümmert, Martin W., Stadler, Michael, Hambach, Lothar, Gingele, Stefan, Bredt, Martin, Wattjes, Mike P., Göhring, Gudrun, Venturini, Letizia, Möhn, Nora, Stangel, Martin, Trebst, Corinna, Ganser, Arnold, Wegner, Florian, and Skripuletz, Thomas

Subjects

HEMATOPOIETIC stem cell transplantation, GRAFT versus host disease, ENCEPHALOMYELITIS, IMMUNOTHERAPY, MYELODYSPLASTIC syndromes

Abstract

Allogeneic hematopoietic stem cell transplantation (alloHSCT) is a curative treatment for hematologic malignancies. Acute and chronic graft-versus-host disease (GvHD) are the major immune-mediated complications after alloHSCT. However, there is controversy whether neurologic complications after alloHSCT might represent manifestations of GvHD. We report three patients who acquired distinct, severe immune-mediated peripheral or central nervous system diseases after alloHSCT without other, concomitant GvHD manifestations. One patient had been diagnosed with B-cell chronic lymphocytic leukemia and two patients with high risk myelodysplastic syndrome. Patient #1 presented as LGI1- and GAD-IgG positive immune-mediated encephalitis, patient #2 was diagnosed with MOG-IgG positive encephalomyelitis, and patient #3 had chronic inflammatory polyneuropathy associated with SSA(Ro)-IgG positive Sjögren's syndrome. 100% donor chimerism was detectable in the peripheral blood in all three. The specific antibodies were undetectable in donors' and patients' blood before alloHSCT suggesting that the antibodies had arisen from the transplanted donor immune system. Early intensive immunotherapy led to improvement of clinical symptoms and stability of the neurological disease, however, at the cost of losing the graft-versus-malignancy effect in one patient. In conclusion, we provide evidence of isolated, severe allo-immune diseases of the peripheral and central nervous system as complications of alloHSCT ("neuro-GvHD"). Interdisciplinary surveillance and thorough diagnostic work-up are needed for early diagnosis and treatment of neuro-immunologic complications after alloHSCT to improve the otherwise poor outcome. [ABSTRACT FROM AUTHOR]

Published

2021

10. The transplant cohort of the German center for infection research (DZIF Tx-Cohort): study design and baseline characteristics.

Author

Karch, André, Schindler, Daniela, Kühn-Steven, Andrea, Blaser, Rainer, Kuhn, Klaus A., Sandmann, Lisa, Sommerer, Claudia, Guba, Markus, Heemann, Uwe, Strohäker, Jens, Glöckner, Stephan, Mikolajczyk, Rafael, Busch, Dirk H., Schulz, Thomas F., for the Transplant Cohort of the German Center for Infection Research (DZIF Transplant Cohort) Consortium, Lehmann, Andreas, Ganser, Arnold, Lange, Berit, Maecker-Kolhoff, Britta, and Tönshoff, Burkhard

Subjects

STEM cell transplantation, TRANSPLANTATION of organs, tissues, etc., RESEARCH institutes, EXPERIMENTAL design, STANDARD operating procedure, ARTIFICIAL pancreases, ARTIFICIAL hearts

Abstract

Infectious complications are the major cause of morbidity and mortality after solid organ and stem cell transplantation. To better understand host and environmental factors associated with an increased risk of infection as well as the effect of infections on function and survival of transplanted organs, we established the DZIF Transplant Cohort, a multicentre prospective cohort study within the organizational structure of the German Center for Infection Research. At time of transplantation, heart-, kidney-, lung-, liver-, pancreas- and hematopoetic stem cell- transplanted patients are enrolled into the study. Follow-up visits are scheduled at 3, 6, 9, 12 months after transplantation, and annually thereafter; extracurricular visits are conducted in case of infectious complications. Comprehensive standard operating procedures, web-based data collection and monitoring tools as well as a state of the art biobanking concept for blood, purified PBMCs, urine, and faeces samples ensure high quality of data and biosample collection. By collecting detailed information on immunosuppressive medication, infectious complications, type of infectious agent and therapy, as well as by providing corresponding biosamples, the cohort will establish the foundation for a broad spectrum of studies in the field of infectious diseases and transplant medicine. By January 2020, baseline data and biosamples of about 1400 patients have been collected. We plan to recruit 3500 patients by 2023, and continue follow-up visits and the documentation of infectious events at least until 2025. Information about the DZIF Transplant Cohort is available at https://www.dzif.de/en/working-group/transplant-cohort. [ABSTRACT FROM AUTHOR]

Published

2021

11. 18F-FDG PET/CT of off-target lymphoid organs in CD19-targeting chimeric antigen receptor T-cell therapy for relapsed or refractory diffuse large B-cell lymphoma.

Author

Derlin, Thorsten, Schultze-Florey, Christian, Werner, Rudolf A., Möhn, Nora, Skripuletz, Thomas, David, Sascha, Beutel, Gernot, Eder, Matthias, Ross, Tobias L., Bengel, Frank M., Ganser, Arnold, and Koenecke, Christian

Abstract

Objective: The interplay between systemic inflammation, activity of lymphoid organs and lymphoma activity in CD19-targeting chimeric antigen receptor (CAR)-T-cell immunotherapy, and its significance for response and toxicity, is not well defined.Methods: Using serial 18F-fluorodeoxyglucose (FDG) positron emission tomography/computed tomography (PET/CT), metabolic parameters of lymphoma and lymphoid organs were analyzed in ten patients receiving Tisagenlecleucel (an autologous CD19 CAR-T cell product) for relapsed or refractory diffuse large B-cell lymphoma. The prevalence and severity of toxicity (e.g., neurotoxicity) were noted.Results: Achieving remission required early metabolic response (P = 0.0476). Early suppression of metabolic activity of lymphoid organs (spleen, P = 0.0368; lymph nodes, P = 0.0470) was associated with poor outcome. Lymphoma metabolic activity was significantly higher in patients with neurotoxicity (P = 0.0489).Conclusions: Early metabolic changes in lymphoma lesions and off-target lymphoid organs parallel medium-term response to CAR-T-cell therapy. PET can identify patients at risk for severe toxicity. [ABSTRACT FROM AUTHOR]

Published

2021

12. Treatment of Relapsed Acute Myeloid Leukemia.

Author

Thol, Felicitas and Ganser, Arnold

Abstract

Opinion Statement: Relapse is still a common scenario in acute myeloid leukemia (AML) treatment and occurs in 40-50% of younger and the great majority of elderly patients. The prognosis in relapsed AML patients is generally poor but depends largely on the timing of relapse (early versus late) and the possibility of allogeneic hematopoietic stem cell transplantation (HSCT). At the time of relapse, we again perform a mutational screening and cytogenetic analysis in all AML patients as clonal evolution of disease is frequent. Clinical trials should be first priority in all relapsed patients. In fit patients without prior transplant, we aim to perform HSCT after salvage therapy. In AML patients relapsing after HSCT and good performance status, intensive therapy can be considered with subsequent cellular therapy such as donor lymphocyte infusion (DLI) or a second HSCT. However, less than 20% of these patients are alive after 5 years. For those patients that are unfit, the therapeutic aim is to prolong life with acceptable quality of life. Here, hypomethylating agents (HMA), low-dose AraC (LDAC), and solely cytoreductive therapy with hydroxurea are options depending on first-line therapy. For those patients that have not been treated with venetoclax in first line, the combination therapy of venetoclax with demethylating agents achieves encouraging response rates. Venetoclax is currently also studied in combination with intensive salvage therapy. Importantly, for patients with isocitrate dehydrogenase (IDH) 1/2-mutated AML, ivosidenib, an IDH1 inhibitor, and enasidenib, an IDH2 inhibitor, present well-tolerated options in the setting of refractory or relapsed (r/r) disease even in elderly and heavily pre-treated patients with response rates of 30-40%. Both substances have been approved by the U.S. Food and Drug Administration (FDA) for r/r AML patients with IDH1/2 mutations (but not yet by the European Medicines Agency (EMA)). For patients with FMS-like tyrosine kinase 3 (FLT3) mutations, treatment with the selective FLT3 inhibitor gilteritinib is well tolerated and leads to improved outcome compared with standard salvage therapy. The approval has been granted by the FDA and the EMA. Generally, we would recommend targeted therapy for IDH1/2- and FLT3-mutated AML if available. In order to improve outcome in relapsed AML, it will be important to intelligently combine novel substances with each other as well as chemotherapy in prospective clinical trials. The development of therapies with bispecific antibodies or chimeric antigen receptor T cells (CAR-T) are still in early development. [ABSTRACT FROM AUTHOR]

Published

2020

13. Monosomal karyotype and chromosome 17p loss or TP53 mutations in decitabine-treated patients with acute myeloid leukemia.

Author

Becker, Heiko, Pfeifer, Dietmar, Ihorst, Gabriele, Pantic, Milena, Wehrle, Julius, Rüter, Björn H., Bullinger, Lars, Hackanson, Björn, Germing, Ulrich, Kuendgen, Andrea, Platzbecker, Uwe, Döhner, Konstanze, Ganser, Arnold, Hagemeijer, Anne, Wijermans, Pierre W., Döhner, Hartmut, Duyster, Justus, and Lübbert, Michael

Subjects

ACUTE myeloid leukemia, GENETIC mutation, CHROMOSOMES, IMPACT response, CHROMOSOME duplication, PRELEUKEMIA, ALLOIMMUNITY

Abstract

TP53 aberrations reportedly predict favorable responses to decitabine (DAC) in acute myeloid leukemia (AML). We evaluated clinical features and outcomes associated with chromosome 17p loss or TP53 gene mutations in older, unfit DAC-treated AML patients in a phase II trial. Of 178 patients, 25 had loss of 17p in metaphase cytogenetics; 24 of these had a complex (CK+) and 21 a monosomal karyotype (MK+). In analyses in all patients and restricted to CK+ and MK+ patients, 17p loss tended to associate with higher rates of complete remission (CR), partial remission (PR), or antileukemic effect (ALE). Despite favorable response rates, there was no significant OS difference between patients with or without loss of 17p in the entire cohort or in the CK+ and MK+ cohort. TP53 mutations were identified in eight of 45 patients with material available. Five of the eight TP53-mutated patients had 17p loss. TP53-mutated patients had similar rates of CR/PR/ALE but shorter OS than those with TP53 wild type (P = 0.036). Moreover, patients with a subclone based on mutation data had shorter OS than those without (P = 0.05); only one patient with TP53-mutated AML had a subclone. In conclusion, 17p loss conferred a favorable impact on response rates, even among CK+ and MK+ patients that however could not be maintained. The effect of TP53 mutations appeared to be different; however, patient numbers were low. Future research needs to further dissect the impact of the various TP53 aberrations in HMA-based combination therapies. The limited duration of favorable responses to HMA treatment in adverse-risk genetics AML should prompt physicians to advance allografting for eligible patients in a timely fashion. [ABSTRACT FROM AUTHOR]

Published

2020

14. Adenosine stress perfusion cardiac magnetic resonance imaging in patients undergoing intracoronary bone marrow cell transfer after ST-elevation myocardial infarction: the BOOST-2 perfusion substudy.

Author

Seitz, Andreas, Wollert, Kai C., Meyer, Gerd P., Müller-Ehmsen, Jochen, Tschöpe, Carsten, May, Andreas E., Empen, Klaus, Chorianopoulos, Emmanuel, Ritter, Benedikta, Pirr, Jens, Arseniev, Lubomir, Heuft, Hans-Gert, Ganser, Arnold, Abu-Zaid, Eed, Katus, Hugo A., Felix, Stephan B., Gawaz, Meinrad P., Schultheiss, Heinz-Peter, Ladage, Dennis, and Bauersachs, Johann

Abstract

Aims: In the placebo-controlled, double-blind BOne marrOw transfer to enhance ST-elevation infarct regeneration (BOOST) 2 trial, intracoronary autologous bone marrow cell (BMC) transfer did not improve recovery of left ventricular ejection fraction (LVEF) at 6 months in patients with ST-elevation myocardial infarction (STEMI) and moderately reduced LVEF. Regional myocardial perfusion as determined by adenosine stress perfusion cardiac magnetic resonance imaging (S-CMR) may be more sensitive than global LVEF in detecting BMC treatment effects. Here, we sought to evaluate (i) the changes of myocardial perfusion in the infarct area over time (ii) the effects of BMC therapy on infarct perfusion, and (iii) the relation of infarct perfusion to LVEF recovery at 6 months. Methods and results: In 51 patients from BOOST-2 (placebo, n = 10; BMC, n = 41), S-CMR was performed 5.1 ± 2.9 days after PCI (before placebo/BMC treatment) and after 6 months. Infarct perfusion improved from baseline to 6 months in the overall patient cohort as reflected by the semi-quantitative parameters, perfusion defect–infarct size ratio (change from 0.54 ± 0.20 to 0.43 ± 0.22; P = 0.006) and perfusion defect–upslope ratio (0.54 ± 0.23 to 0.68 ± 0.22; P < 0.001), irrespective of randomised treatment. Perfusion defect–upslope ratio at baseline correlated with LVEF recovery (r = 0.62; P < 0.001) after 6 months, with a threshold of 0.54 providing the best sensitivity (79%) and specificity (74%) (area under the curve, 0.79; 95% confidence interval, 0.67–0.92). Conclusion: Infarct perfusion improves from baseline to 6 months and predicts LVEF recovery in STEMI patients undergoing early PCI. Intracoronary BMC therapy did not enhance infarct perfusion in the BOOST-2 trial. [ABSTRACT FROM AUTHOR]

Published

2020

15. Inferior outcome of allogeneic stem cell transplantation for secondary acute myeloid leukemia in first complete remission as compared to de novo acute myeloid leukemia.

Author

Schmaelter, Ann-Kristin, Labopin, Myriam, Socié, Gerard, Itälä-Remes, Maija, Blaise, Didier, Yakoub-Agha, Ibrahim, Forcade, Edouard, Cornelissen, Jan, Ganser, Arnold, Beelen, Dietrich, Labussière-Wallet, Hélène, Passweg, Jakob, Savani, Bipin N., Schmid, Christoph, Nagler, Arnon, and Mohty, Mohamad

Subjects

CANCER chemotherapy, BLOOD diseases, ACUTE myeloid leukemia, GRAFT versus host disease, STEM cell transplantation

Abstract

Following chemotherapy, secondary acute myeloid leukemia (sAML), occurring after antecedent hematologic diseases, previous chemotherapy or radiation, has an inferior prognosis compared with de novo AML. To define the outcome of sAML in the context of allogeneic stem cell transplantation (alloSCT), a retrospective, registry-based comparison was performed, including 11,439 patients with de novo and 1325 with sAML. Among transplants in first complete remission (CR1) (n = 8,600), the 3-year cumulative incidence of relapse (RI) and non-relapse mortality (NRM) was 28.5% and 16.4% for de novo, and 35% and 23.4% for sAML. Three-year overall survival (OS), leukemia-free survival (LFS) and Graft-versus-Host Disease/relapse-free survival (GRFS) was 60.8%, 55.1%, and 38.6% for de novo, and 46.7%, 41.6%, and 28.4% for sAML, respectively. In multivariate analysis, sAML was associated with a lower OS (HR = 1.33 [95% CI = 1.21–1.48]; p < 10−5), LFS (HR = 1.32 [95% CI = 1.19–1.45]; p < 10−5) and GRFS (HR = 1.2 [95% CI = 1.1–1.31]; p < 10−4) and higher NRM (HR = 1.37 [95% CI = 1.17–1.59]; p < 10−4) and RI (HR = 1.27 [95% CI = 1.12–1.44]; p < 10−3). Results of the Cox model were confirmed in a matched-pair analysis. In contrast, results did not differ between de novo and sAML after alloSCT in induction failure or relapse. Hence, this analysis identified sAML as an independent risk factor for outcome after alloSCT in CR1. [ABSTRACT FROM AUTHOR]

Published

2020

16. Monocytes reprogrammed with lentiviral vectors co-expressing GM-CSF, IFN-α2 and antigens for personalized immune therapy of acute leukemia pre- or post-stem cell transplantation.

Author

Bialek-Waldmann, Julia K., Heuser, Michael, Ganser, Arnold, and Stripecke, Renata

Subjects

ACUTE leukemia, CELL transplantation, MONOCYTES, STEM cell transplantation, ACUTE myeloid leukemia

Abstract

Acute myeloid leukemia (AML) is the most common acute leukemia in adults and overall survival remains poor. Chemotherapy is the standard of care for intensive induction therapy. Patients who achieve a complete remission require post-remission therapies to prevent relapse. There is no standard of care for patients with minimal residual disease (MRD), and stem cell transplantation is a salvage therapy. Considering the AML genetic heterogeneity and the leukemia immune-suppressive properties, novel cellular immune therapies to effectively harness immunological responses to prevent relapse are needed. We developed a novel modality of immune therapy consisting of monocytes reprogrammed with lentiviral vectors expressing GM-CSF, IFN-α and antigens. Preclinical studies in humanized mice showed that the reprogrammed monocytes self-differentiated into highly viable induced dendritic cells (iDCs) in vivo which migrated effectively to lymph nodes, producing remarkable effects in the de novo regeneration of T and B cell responses. For the first-in-man clinical trial, the patient's monocytes will be transduced with an integrase-defective tricistronic lentiviral vector expressing GM-CSF, IFN-α and a truncated WT1 antigen. For transplanted patients, pre-clinical development of iDCs co-expressing cytomegalovirus antigens is ongoing. To simplify the product chain for a de-centralized supply model, we are currently exploring a closed automated system for a short two-day manufacturing of iDCs. A phase I clinical trial study is in preparation for immune therapy of AML patients with MRD. The proposed cell therapy can fill an important gap in the current and foreseeable future immunotherapies of AML. [ABSTRACT FROM AUTHOR]

Published

2019

17. Diagnostik und Management des myelodysplastischen Syndroms.

Author

Nolte, Florian, Hofmann, Wolf-Karsten, Ganser, Arnold, and Heuser, Michael

Abstract

Copyright of Der Onkologe is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2019

18. Lipid nanoparticle-mediated siRNA delivery for safe targeting of human CML in vivo.

Author

Jyotsana, Nidhi, Sharma, Amit, Chaturvedi, Anuhar, Budida, Ramachandramouli, Scherr, Michaela, Kuchenbauer, Florian, Lindner, Robert, Noyan, Fatih, Sühs, Kurt-Wolfram, Stangel, Martin, Grote-Koska, Denis, Brand, Korbinian, Vornlocher, Hans-Peter, Eder, Matthias, Thol, Felicitas, Ganser, Arnold, Humphries, R. Keith, Ramsay, Euan, Cullis, Pieter, and Heuser, Michael

Subjects

BIODEGRADABLE nanoparticles, SMALL interfering RNA, CHRONIC myeloid leukemia, MYELOID leukemia, LIPIDS, RNA interference

Abstract

Efficient and safe delivery of siRNA in vivo is the biggest roadblock to clinical translation of RNA interference (RNAi)-based therapeutics. To date, lipid nanoparticles (LNPs) have shown efficient delivery of siRNA to the liver; however, delivery to other organs, especially hematopoietic tissues still remains a challenge. We developed DLin-MC3-DMA lipid-based LNP-siRNA formulations for systemic delivery against a driver oncogene to target human chronic myeloid leukemia (CML) cells in vivo. A microfluidic mixing technology was used to obtain reproducible ionizable cationic LNPs loaded with siRNA molecules targeting the BCR-ABL fusion oncogene found in CML. We show a highly efficient and non-toxic delivery of siRNA in vitro and in vivo with nearly 100% uptake of LNP-siRNA formulations in bone marrow of a leukemic model. By targeting the BCR-ABL fusion oncogene, we show a reduction of leukemic burden in our myeloid leukemia mouse model and demonstrate reduced disease burden in mice treated with LNP-BCR-ABL siRNA as compared with LNP-CTRL siRNA. Our study provides proof-of-principle that fusion oncogene specific RNAi therapeutics can be exploited against leukemic cells and promise novel treatment options for leukemia patients. [ABSTRACT FROM AUTHOR]

Published

2019

19. Six versus eight doses of rituximab in patients with aggressive B cell lymphoma receiving six cycles of CHOP: results from the "Positron Emission Tomography-Guided Therapy of Aggressive Non-Hodgkin Lymphomas" (PETAL) trial.

Author

Hüttmann, Andreas, Rekowski, Jan, Müller, Stefan P., Hertenstein, Bernd, Franzius, Christiane, Mesters, Rolf, Weckesser, Matthias, Kroschinsky, Frank, Kotzerke, Jörg, Ganser, Arnold, Bengel, Frank M., La Rosée, Paul, Freesmeyer, Martin, Höffkes, Heinz-Gert, Hertel, Andreas, Behringer, Dirk, Prange-Krex, Gabriele, Griesshammer, Martin, Holzinger, Jens, and Wilop, Stefan

Subjects

B cells, ANTINEOPLASTIC agents, B cell lymphoma, COMPARATIVE studies, DEOXY sugars, DOXORUBICIN, LONGITUDINAL method, RESEARCH methodology, MEDICAL cooperation, PREDNISONE, PROGNOSIS, RADIOPHARMACEUTICALS, RESEARCH, RESEARCH funding, POSITRON emission tomography, VINCRISTINE, EVALUATION research, RANDOMIZED controlled trials, CYCLOPHOSPHAMIDE

Abstract

Standard first-line treatment of aggressive B cell lymphoma comprises six or eight cycles of cyclophosphamide, doxorubicin, vincristine, and prednisone (CHOP) plus eight doses of rituximab (R). Whether adding two doses of rituximab to six cycles of R-CHOP is of therapeutic benefit has not been systematically investigated. The Positron Emission Tomography-Guided Therapy of Aggressive Non-Hodgkin Lymphomas (PETAL) trial investigated the ability of [18F]-fluorodesoxyglucose PET scanning to guide treatment in aggressive non-Hodgkin lymphomas. Patients with B cell lymphomas and a negative interim scan received six cycles of R-CHOP with or without two extra doses of rituximab. For reasons related to trial design, only about a third underwent randomization between the two options. Combining randomized and non-randomized patients enabled subgroup analyses for diffuse large B cell lymphoma (DLBCL; n = 544), primary mediastinal B cell lymphoma (PMBCL; n = 37), and follicular lymphoma (FL) grade 3 (n = 35). With a median follow-up of 52 months, increasing the number of rituximab administrations failed to improve outcome. A non-significant trend for improved event-free survival was seen in DLBCL high-risk patients, as defined by the International Prognostic Index, while inferior survival was observed in female patients below the age of 60 years. Long-term outcome in PMBCL was excellent. Differences between FL grade 3a and FL grade 3b were not apparent. The results were confirmed in a Cox proportional hazard regression model and a propensity score matching analysis. In conclusion, adding two doses of rituximab to six cycles of R-CHOP did not improve outcome in patients with aggressive B cell lymphomas and a fast metabolic treatment response. [ABSTRACT FROM AUTHOR]

Published

2019

20. Histiocytic sarcoma progressing from follicular lymphoma and mimicking acquired hemophagocytic lymphohistiocytosis.

Author

Schünemann, Christoph, Göhring, Gudrun, Behrens, Yvonne Lisa, Kreipe, Hans-Heinrich, Ganser, Arnold, and Thol, Felicitas

Subjects

RETICULUM cell sarcoma, ERDHEIM-Chester disease, LYMPHOMAS, BONE marrow, IMMUNOGLOBULIN heavy chains

Published

2020

21. Improved short- and long-term outcome of allogeneic stem cell recipients admitted to the intensive care unit: a retrospective longitudinal analysis of 942 patients.

Author

Lueck, Catherina, Stadler, Michael, Koenecke, Christian, Hoeper, Marius M., Dammann, Elke, Schneider, Andrea, Kielstein, Jan T., Ganser, Arnold, Eder, Matthias, and Beutel, Gernot

Subjects

STEM cell transplantation, CRITICAL care medicine, INTENSIVE care units, CRITICALLY ill, SEPSIS, SEPTIC shock, RESPIRATORY insufficiency, PATIENTS

Abstract

Purpose: Intensive care unit (ICU) admission of allogeneic hematopoietic stem cell transplant (HSCT) recipients is associated with relatively poor outcome. Since longitudinal data on this topic remains scarce, we analyzed reasons for ICU admission as well as short- and long-term outcome of critically ill HSCT recipients.Methods: A total of 942 consecutive adult patients were transplanted at Hannover Medical School from 2000 to 2013. Of those, 330 patients were at least admitted once to the ICU and included in this retrospective study. To analyze time-dependent improvements, we separately compared patient characteristics as well as reasons and outcome of ICU admission for the periods 2000-2006 and 2007-2013.Results: The main reasons for ICU admission were acute respiratory failure (ARF) in 35%, severe sepsis/septic shock in 23%, and cardiac problems in 18%. ICU admission was clearly associated with shortened survival (p < 0.001), but survival of ICU patients after hospital discharge reached 44% up to 5 years and was comparable to that of non-ICU HSCT patients. When ICU admission periods were compared, patients were older (48 vs. 52 years; p < 0.005) and the percentage of ARF as leading cause for ICU admission decreased from 43% in the first to 30% in the second period. Over time ICU and hospital survival improved from 44 to 60% (p < 0.01) and from 26 to 43% (p < 0.01), respectively. The 1- and 3-year survival rate after ICU admission increased significantly from 14 to 32% and from 11 to 23% (p < 0.01).Conclusions: Besides ARF and septic shock, cardiac events were especially a major reason for ICU admission. Both short- and long-term survival of critically ill HSCT patients has improved significantly in recent years, and survival of HSCT recipients discharged from hospital is not significantly affected by a former ICU stay. [ABSTRACT FROM AUTHOR]

Published

2018

22. The hypomorphic TERT A1062T variant is associated with increased treatment-related toxicity in acute myeloid leukemia.

Author

Both, Anna, Krauter, Jürgen, Damm, Frederik, Thol, Felicitas, Göhring, Gudrun, Heuser, Michael, Ottmann, Oliver, Lübbert, Michael, Wattad, Mohammed, Kanz, Lothar, Schlimok, Günter, Raghavachar, Aruna, Fiedler, Walter, Kirchner, Hartmut, Brugger, Wolfram, Schlegelberger, Brigitte, Heil, Gerhard, Ganser, Arnold, and Wagner, Katharina

Subjects

ACUTE myeloid leukemia, ACUTE myeloid leukemia treatment, KARYOTYPES, TELOMERASE reverse transcriptase, GENETIC mutation, PATIENTS

Abstract

Hypomorphic germline variants in TERT, the gene encoding the reverse transcriptase component of the human telomerase complex, occur with a frequency of 3-5% in acute myeloid leukemia. We analyzed the clinical and prognostic impact of the most common TERT A1062T variant in younger patients with acute myeloid leukemia intensively treated within two prospective multicenter trials. Four hundred and twenty patients (age 17-60 years) were analyzed for the TERT A1062T variant by direct sequencing. Fifteen patients (3.6%) carried the TERT A1062T variant. Patients with the TERT A1062T variant had a trend towards less favorable and more intermediate 2/adverse karyotypes/genotypes according to the European Leukemia Net classification. In univariate and multivariate analysis, patients with the TERT A1062T variant had a significantly inferior overall survival compared to wild-type patients (6-year overall survival 20 vs. 41%, p = 0.005). Patients with the TERT A1062T variant showed a high rate of treatment-related mortality: 5/15 (33%) died during induction therapy or in complete remission as compared to 62/405 (15%) of the wild-type patients. In patients with the TERT variant, 14/15 (93%) suffered from non-hematological/non-infectious grade 3/4 adverse events (mostly hepatic and/or mucosal) as compared to 216/405 (53%) wild-type patients (p = 0.006). In multivariate analysis, the TERT A1062T variant was an independent risk factor predicting for adverse events during induction chemotherapy. In conclusion, the TERT A1062T variant is an independent negative prognostic factor in younger patients with acute myeloid leukemia and seems to predispose those patients to treatment-related toxicity. [ABSTRACT FROM AUTHOR]

Published

2017

23. Peripheral blood cytogenetics allows treatment monitoring and early identification of treatment failure to lenalidomide in MDS patients: results of the LE-MON-5 trial.

Author

Braulke, Friederike, Schulz, Xenia, Germing, Ulrich, Schuler, Esther, Platzbecker, Uwe, Nolte, Florian, Hofmann, Wolf-Karsten, Giagounidis, Aristoteles, Götze, Katharina, Lübbert, Michael, Schlenk, Richard, Schanz, Julie, Bacher, Ulrike, Ganser, Arnold, Büsche, Guntram, Letsch, Anne, Schafhausen, Philippe, Bug, Gesine, Brümmendorf, Tim, and Haas, Rainer

Subjects

MYELODYSPLASTIC syndromes, CYTOGENETICS, BLOOD transfusion, CHROMOSOME banding, FLUORESCENCE in situ hybridization, PATIENTS, NEOVASCULARIZATION inhibitors, ANTIGENS, CHROMOSOMES, CLINICAL trials, COMPARATIVE studies, KARYOTYPES, RESEARCH methodology, MEDICAL cooperation, GENETIC mutation, PROGNOSIS, RESEARCH, EVALUATION research, THALIDOMIDE, MYELOID leukemia, TREATMENT effectiveness, ACUTE diseases, MONONUCLEAR leukocytes, DIAGNOSIS, THERAPEUTICS

Abstract

Transfusion-dependent patients with low- or intermediate-1-risk myelodysplastic syndrome, <5% bone marrow (BM) blasts and isolated 5q-deletion received lenalidomide within the German MDS study group phase-II clinical trial LE-MON-5 (EudraCT:2008-001866-10) of the University of Duesseldorf, Germany. Cytogenetic monitoring was performed by chromosome banding analyses (CBA) of BM cells and fluorescence in situ hybridization (FISH) analyses of peripheral blood (PB) mononuclear CD34+ cells using extended probe panels. Out of 144 patients screened for study enrollment, 24% failed to meet inclusion criteria due to cytogenetic findings. Eighty-seven patients were followed with a median observation time of 30 months. Cytogenetic response detected by FISH and CBA in 74 and 66% of patients, respectively, was predictive for hematologic response as well as of high prognostic relevance. After 2 years, AML rate was 8% for all patients. Karyotype evolution was detected in 21 (FISH)-34% (CBA) of patients associated with significantly shorter AML-free survival. Disease progression was first detectable on the cytogenetic level on average 5-6 months before recurrence of transfusion dependence. Our data show for the first time in a prospective setting that a cytogenetic monitoring from the PB helps to early identify treatment failure and progressive disease in lenalidomide-treated patients to improve clinical management.Trial Registration: EudraCT:2008-001866-10. [ABSTRACT FROM AUTHOR]

Published

2017

24. Entstehung, Entwicklung und Erfolge des Kompetenznetzes Akute und Chronische Leukämien (KNL).

Author

Kossak-Roth, Ute, Saußele, Susanne, Aul, Carlo, Büchner, Thomas, Döhner, Hartmut, Dugas, Martin, Ehninger, Gerhard, Ganser, Arnold, Giagounidis, Aristoteles, Gökbuget, Nicola, Griesshammer, Martin, Hasford, Jörg, Heuser, Michael, Hiddemann, Wolfgang, Hochhaus, Andreas, Hoelzer, Dieter, Niederwieser, Dietger, Reiter, Andreas, Röllig, Christoph, and Hehlmann, Rüdiger

Abstract

Copyright of Bundesgesundheitsblatt - Gesundheitsforschung - Gesundheitsschutz is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2016

25. Leukemogenic potency of the novel FLT3-N676K mutant.

Author

Huang, Kezhi, Yang, Min, Pan, Zengkai, Heidel, Florian, Scherr, Michaela, Eder, Matthias, Fischer, Thomas, Büsche, Guntram, Welte, Karl, Neuhoff, Nils, Ganser, Arnold, Li, Zhixiong, Heidel, Florian H, and von Neuhoff, Nils

Subjects

PROTEIN-tyrosine kinases, GENETIC mutation, MYELOID leukemia, CANCER cells, LEUKEMIA etiology, PHYSIOLOGY, GENETICS, ANTINEOPLASTIC agents, CANCER chemotherapy, HETEROCYCLIC compounds, STEM cell transplantation, THIAZOLES, PIPERIDINE, UREA, PROTEIN kinase inhibitors, AMINO acids, ANIMAL experimentation, BONE marrow transplantation, COMPARATIVE studies, DISEASE susceptibility, GENES, GENOMES, LEUKEMIA, RESEARCH methodology, MEDICAL cooperation, MICE, PROTEINS, RESEARCH, RETROVIRUSES, TRANSFERASES, EVALUATION research, IMMUNOCOMPROMISED patients, NEOPLASTIC cell transformation, COLONY-forming units assay, THERAPEUTICS

Abstract

The novel FMS-like tyrosine kinase 3 (FLT3)-N676K point mutation within the FLT3 kinase domain-1 was recently identified in 6 % of de novo acute myeloid leukemia (AML) patients with inv(16). Because FLT3-N676K was encountered almost exclusively in inv(16) AML, we investigated the transforming potential of FLT3-N676K, the cooperation between FLT3-N676K and core binding factor ß-smooth muscle myosin heavy chain (CBFß-SMMHC) (encoded by the inv(16) chimeric gene CBFB-MYH11) in inducing acute leukemia, and tested the sensitivity of FLT3-N676K-positive leukemic cells to FLT3 inhibitors. Retroviral expression of FLT3-N676K in myeloid 32D cells induced AML in syngeneic C3H/HeJ mice (n = 11/13, median latency 58 days), with a transforming activity similar to FLT3-internal tandem duplication (ITD) (n = 8/8), FLT3-TKD D835Y (n = 8/9), and FLT3-ITD-N676K (n = 9/9) mutations. Three out of 14 (21.4 %) C57BL/6J mice transplanted with FLT3-N676K-transduced primary hematopoietic progenitor cells developed acute leukemia (latency of 68, 77, and 273 days), while no hematological malignancy was observed in the control groups including FLT3-ITD. Moreover, co-expression of FLT3-N676K/CBFß-SMMHC did not promote acute leukemia in three independent experiments (n = 16). In comparison with FLT3-ITD, FLT3-N676K induced much higher activation of FLT3 and tended to trigger stronger phosphorylation of MAPK and AKT. Importantly, leukemic cells carrying the FLT3-N676K mutant in the absence of an ITD mutation were highly sensitive to FLT3 inhibitors AC220 and crenolanib, and crenolanib even retained activity against the AC220-resistant FLT3-ITD-N676K mutant. Taken together, the FLT3-N676K mutant is potent to transform murine hematopoietic stem/progenitor cells in vivo. This is the first report of acute leukemia induced by an activating FLT3 mutation in C57BL/6J mice. Moreover, further experiments investigating molecular mechanisms for leukemogenesis induced by FLT3-N676K mutation and clinical evaluation of FLT3 inhibitors in FLT3-N676K-positive AML seem warranted. [ABSTRACT FROM AUTHOR]

Published

2016

26. Decitabine improves progression-free survival in older high-risk MDS patients with multiple autosomal monosomies: results of a subgroup analysis of the randomized phase III study 06011 of the EORTC Leukemia Cooperative Group and German MDS Study Group.

Author

Lübbert, Michael, Suciu, Stefan, Hagemeijer, Anne, Rüter, Björn, Platzbecker, Uwe, Giagounidis, Aristoteles, Selleslag, Dominik, Labar, Boris, Germing, Ulrich, Salih, Helmut, Muus, Petra, Pflüger, Karl-Heinz, Schaefer, Hans-Eckart, Bogatyreva, Lioudmila, Aul, Carlo, Witte, Theo, Ganser, Arnold, Becker, Heiko, Huls, Gerwin, and Helm, Lieke

Subjects

MYELODYSPLASTIC syndromes, DECITABINE, DISEASE progression, CYTOGENETICS, KARYOTYPES, PATIENTS, THERAPEUTICS, ANTINEOPLASTIC agents, CANCER chemotherapy, LEUKEMIA diagnosis, THERAPEUTIC use of antimetabolites, CHROMOSOME abnormalities, COMPARATIVE studies, LEUKEMIA, RESEARCH methodology, MEDICAL cooperation, PROGNOSIS, RESEARCH, EVALUATION research, RANDOMIZED controlled trials, AZACITIDINE, DIAGNOSIS

Abstract

In a study of elderly AML patients treated with the hypomethylating agent decitabine (DAC), we noted a surprisingly favorable outcome in the (usually very unfavorable) subgroup with two or more autosomal monosomies (MK2+) within a complex karyotype (Lübbert et al., Haematologica 97:393-401, 2012). We now analyzed 206 myelodysplastic syndrome (MDS) patients (88 % of 233 patients randomized in the EORTC/GMDSSG phase III trial 06011, 61 of them with RAEBt, i.e. AML by WHO) with cytogenetics informative for MK status.. Endpoints are the following: complete/partial (CR/PR) and overall response rate (ORR) and progression-free (PFS) and overall survival (OS). Cytogenetic subgroups are the following: 63 cytogenetically normal (CN) patients, 143 with cytogenetic abnormalities, 73 of them MK-negative (MK-), and 70 MK-positive (MK+). These MK+ patients could be divided into 17 with a single autosomal monosomy (MK1) and 53 with at least two monosomies (MK2+). ORR with DAC in CN patients: 36.1 %, in MK- patients: 16.7 %, in MK+ patients: 43.6 % (MK1: 44.4 %, MK2+ 43.3 %). PFS was prolonged by DAC compared to best supportive care (BSC) in the CN (hazard ratio (HR) 0.55, 99 % confidence interval (CI), 0.26; 1.15, p = 0.03) and MK2+ (HR 0.50; 99 % CI, 0.23; 1.06, p = 0.016) but not in the MK-, MK+, and MK1 subgroups. OS was not improved by DAC in any subgroup. In conclusion, we demonstrate for the first time in a randomized phase III trial that high-risk MDS patients with complex karyotypes harboring two or more autosomal monosomies attain encouraging responses and have improved PFS with DAC treatment compared to BSC. [ABSTRACT FROM AUTHOR]

Published

2016

27. Decitabine versus best supportive care in older patients with refractory anemia with excess blasts in transformation (RAEBt) - results of a subgroup analysis of the randomized phase III study 06011 of the EORTC Leukemia Cooperative Group and German MDS Study Group (GMDSSG).

Author

Becker, Heiko, Suciu, Stefan, Rüter, Björn, Platzbecker, Uwe, Giagounidis, Aristoteles, Selleslag, Dominik, Labar, Boris, Germing, Ulrich, Salih, Helmut, Muus, Petra, Pflüger, Karl-Heinz, Hagemeijer, Anne, Schaefer, Hans-Eckart, Fiaccadori, Valeria, Baron, Frédéric, Ganser, Arnold, Aul, Carlo, Witte, Theo, Wijermans, Pierre, and Lübbert, Michael

Subjects

ANEMIA treatment, TREATMENT of chronic myeloid leukemia, ANEMIA, ANTIMETABOLITES, ANTINEOPLASTIC agents, PROGNOSIS, STATISTICAL sampling, SURVIVAL, CHRONIC myeloid leukemia, RANDOMIZED controlled trials, AZACITIDINE

Abstract

In the European Organisation for Research and Treatment of Cancer (EORTC)/GMDSSG phase III trial 06011, we compared decitabine (15 mg/m(2) every 8 h for 3 days) with best supportive care (BSC) in patients ≥60 years with myelodysplastic syndromes (MDS) by French-American-British (FAB) criteria. Here, we reinvestigate trial 06011 for the activity and efficacy specifically in patients with refractory anemia with excess blasts in transformation (RAEBt). Response rates in the decitabine arm (N = 40) were as follows: complete or partial remission, 15 %; hematologic improvement, 15 %; resistant disease, 30 %. RAEBt patients in the decitabine arm had longer progression-free survival (PFS; hazard ratio (HR) 0.30, 95 % confidence interval (CI) 0.18-0.51; median, 6.2 vs 2.8 months) and overall survival (OS; HR 0.68, 95 % CI 0.42-1.11; median, 8.0 vs 6.0 months) than in the BSC arm (N = 35). Censoring at allogeneic hematopoietic stem cell transplantation, the OS difference between the treatment groups increased, particularly among patients aged 60-74 years (HR 0.48, 95 % CI 0.26-0.89). After regrouping the study cohort according to World Health Organization (WHO) criteria, patients with acute myeloid leukemia (AML) (i.e., ≥20 % blasts) in the decitabine arm (N = 27) also had longer PFS than in the BSC arm (N = 23) (HR 0.46, 95 % CI 0.26-0.83; median, 6.2 vs 2.8 months). In conclusion, 3-day decitabine displays clinical activity and efficacy in MDS and/or AML with 5-30 % blood or 20-30 % marrow blasts. [ABSTRACT FROM AUTHOR]

Published

2015

28. Myeloid-derived growth factor (C19orf10) mediates cardiac repair following myocardial infarction.

Author

Korf-Klingebiel, Mortimer, Reboll, Marc R, Klede, Stefanie, Brod, Torben, Pich, Andreas, Polten, Felix, Napp, L Christian, Bauersachs, Johann, Ganser, Arnold, Brinkmann, Eva, Reimann, Ines, Kempf, Tibor, Niessen, Hans W, Mizrahi, Jacques, Schönfeld, Hans-Joachim, Iglesias, Antonio, Bobadilla, Maria, Wang, Yong, and Wollert, Kai C

Subjects

MYOCARDIAL infarction, GROWTH factors, BONE marrow cells, OPEN reading frames (Genetics), CHROMOSOMES, NEOVASCULARIZATION, MACROPHAGES

Abstract

Paracrine-acting proteins are emerging as a central mechanism by which bone marrow cell-based therapies improve tissue repair and heart function after myocardial infarction (MI). We carried out a bioinformatic secretome analysis in bone marrow cells from patients with acute MI to identify novel secreted proteins with therapeutic potential. Functional screens revealed a secreted protein encoded by an open reading frame on chromosome 19 (C19orf10) that promotes cardiac myocyte survival and angiogenesis. We show that bone marrow-derived monocytes and macrophages produce this protein endogenously to protect and repair the heart after MI, and we named it myeloid-derived growth factor (MYDGF). Whereas Mydgf-deficient mice develop larger infarct scars and more severe contractile dysfunction compared to wild-type mice, treatment with recombinant Mydgf reduces scar size and contractile dysfunction after MI. This study is the first to assign a biological function to MYDGF, and it may serve as a prototypical example for the development of protein-based therapies for ischemic tissue repair. [ABSTRACT FROM AUTHOR]

Published

2015

29. The Hematopoietic Growth Factors in Acute Leukemia: A European Perspective.

Author

Heuser, Michael, Ganser, Arnold, and Hoelzer, Dieter

Abstract

Acute myeloid leukemia (AML) and acute lymphoblastic leukemia (ALL) are malignant clonal disorders of the blood system requiring intensive and long-term cytotoxic treatment. Current chemotherapy protocols not only target the malignant cell, but are also highly toxic to normal hematopoietic cells as well. Leukemia patients thus experience prolonged times of neutropenia, thrombocytopenia, and anemia, which increase the risk for secondary complications like infections and bleeding. Twenty years ago leukemia patients were considered the ideal candidates to benefit from accelerated recovery of cytopenias by treatment with recombinant cytokines. Moreover, based on in vitro data, it was hypothesized that myeloid growth factors may sensitize AML cells to cytotoxic agents. Numerous clinical trials have documented the biologic activity of granulocyte and granulocyte–macrophage growth factors to accelerate neutrophil recovery after chemotherapy. However, there is high-level evidence that these myeloid growth factors neither reduce the incidence of severe infections nor improve the outcome of AML patients. Evidence from ALL trials is mixed with some studies suggesting a reduction of severe infections by myeloid growth factors whereas others report no effect. Most studies of acute leukemia patients suggested that myeloid growth factors are safe to use, however, a negative impact on event-free survival was found in one trial and an increased risk for secondary AML was reported in pediatric ALL patients. Thrombopoietins have not led so far to a significant increase in platelet numbers in leukemia patients. Chemokine receptor antagonists are now being evaluated in clinical trials for synergistic effects with chemotherapy and will be discussed briefly. Cytokine development mirrors the great advances that have been achieved in the understanding of regulatory mechanisms in hematopoiesis. As this understanding grows, new drugs and new applications will emerge. [ABSTRACT FROM AUTHOR]

Published

2011

30. Proteomics Studies After Hematopoietic Stem Cell Transplantation.

Author

Weissinger, Eva M., Zürbig, Petra, and Ganser, Arnold

Published

2009

31. Treatment of Adult ALL According to Protocols of the German Multicenter Study Group for Adult ALL (GMALL).

Author

Estey, E. H., Faderl, S. H., Kantarjian, H. M., Gökbuget, Nicola, Arnold, Renate, Böhme, Angelika, Fietkau, Rainer, Freund, Matthias, Ganser, Arnold, Kneba, Michael, Lipp, Thomas, Ludwig, Wolf-Dieter, Maschmeyer, Georg, Messerer, Dorle, Rieder, Harald, Thiel, Eckhard, and Hoelzer, Dieter

Abstract

Since 1978 more than 4500 adult ALL patients have been treated according to the protocols of the German Multicenter Study Group for Adult Acute Lymphoblastic Leukemia (GMALL). GMALL protocols are administered in hospitals all over Germany and the number of participating centers in Germany increased from 25 in 1981 to 120 in the most recent trial. Up to now seven consecutive trials for adult de novo ALL have been conducted. The major aim of all trials was the improvement of remission duration and survival of adult ALL patients, detailed diagnostic characterization, the development of prognostic models and the evaluation of risk-adapted, individualized and targeted treatment strategies. The time-periods and further aims of these studies are briefly summarized in Table 13.1. [ABSTRACT FROM AUTHOR]

Published

2008

32. Interstitial lung disease during targeted therapy in metastatic renal cell carcinoma: a case series from three centres.

Author

Ivanyi, Philipp, Fuehner, Thomas, Adam, Meike, Eichelberg, Christian, Herrmann, Edwin, Merseburger, Axel, Ganser, Arnold, and Grünwald, Viktor

Abstract

Interstitial lung disease (ILD) is an adverse event which occurs also during targeted treatment of patients with metastatic renal cell carcinoma (mRCC). Experiences on ILD-management in mRCC remain limited. mRCC patients treated with everolimus, temsirolimus, or sunitinib at three centres from January 2006 until December 2009 were analysed, retrospectively. Medical records and imaging studies, as well as clinical course, the incidence, diagnostic measures, treatment, and outcome of ILD were assessed. Twenty-six ILD patients (11 %) were identified out of 237 mRCC patients. Median treatment until ILD-diagnosis was 3.8 (range: 1-21.5) months. The ILD-frequency was 2.7 % (n = 6/226) during sunitinib therapy and 19.8 % (n = 20/101) during m-TOR-inhibitor treatment. Cough was the prevailing symptom (69.2 %, n = 18). Bronchoalveolar lavage reviled often lymphocytic (42.9 %, n = 6/14) or eosinophilic cellularity (28.6 %, n = 4/14). Dose reduction (42.3 %, n = 11), treatment interruption (46.2 %, n = 12) or termination (23.1 %, n = 6), and steroid application (34.6 %, n = 9) were common measures in ILD. Interestingly, eosinophilic ILD required pulsed steroids. Improvement occurred in 73.7 % of symptomatic patients. Continuation of targeted therapies was warranted in 65.4 % of ILD patients. No patient died from ILD. ILD during targeted mRCC treatment is common, and supportive measures should be adapted to the clinical course, and potentially in dependence of BAL findings. Re-exposure to targeted therapies appears feasible. [ABSTRACT FROM AUTHOR]

Published

2014

33. Explaining survival differences between two consecutive studies with allogeneic stem cell transplantation in patients with chronic myeloid leukemia.

Author

Pfirrmann, Markus, Saussele, Susanne, Hochhaus, Andreas, Reiter, Andreas, Berger, Ute, Hossfeld, Dieter, Nerl, Christoph, Scheid, Christof, Spiekermann, Karsten, Mayer, Jiri, Hellmann, Andrzej, Lechner, Klaus, Falge, Christiane, Sayer, Herbert, Bunjes, Donald, Ganser, Arnold, Beelen, Dietrich, Baldomero, Helen, Schanz, Urs, and Heimpel, Hermann

Subjects

CHRONIC myeloid leukemia, HEMATOPOIETIC stem cell transplantation, HLA histocompatibility antigens, DISEASE incidence, HEALTH outcome assessment, RANDOMIZED controlled trials, PROGNOSIS

Abstract

Purpose: In the two consecutive German studies III and IIIA on chronic myeloid leukemia, between 1995 and 2004, 781 patients were randomized to receive either allogeneic hematopoietic stem cell transplantation with a related donor or continued drug treatment. Despite comparable transplantation protocols and most centers participating in both studies, the post-transplant survival probabilities for patients transplanted in first chronic phase were significantly higher in study IIIA (144 patients) than in study III (113 patients). Prior to the decision on a combined analysis of both studies, reasons for this discrepancy had to be investigated. Methods: The Cox proportional hazard cure model was used to identify prognostic factors for post-transplant survival. Results: Donor-recipient matching for human leukocyte antigen, patient age, time between diagnosis and transplantation, and calendar time showed a significant influence on survival and/or the incidence of cure. Added as a further factor, affiliation to study IIIA had no significant impact any longer. Conclusions: Discrepancies in influential prognostic factors explained the different post-transplant survival probabilities between the studies. The significance of calendar time suggests a lack of consistency of transplantation practice over time. Accordingly, the prerequisite for a common assessment of overall survival in the two randomized transplantation arms was not met. Moreover, our analyses provide an independent validation of established prognostic factors and their cutoffs. The statistical approach in investigating and modeling potential prognostic factors for survival sets an example for the examination of studies with unexpected outcome differences in concurrent treatment arms. [ABSTRACT FROM AUTHOR]

Published

2014

34. Lack of noncanonical RAS mutations in cytogenetically normal acute myeloid leukemia.

Author

Reuter, Christoph, Krauter, Jürgen, Onono, Fredrick, Bunke, Tania, Damm, Frederik, Thol, Felicitas, Wagner, Katharina, Göhring, Gudrun, Schlegelberger, Brigitte, Heuser, Michael, Ganser, Arnold, and Morgan, Michael

Subjects

ACUTE myeloid leukemia treatment, GENETIC mutation, ACUTE myeloid leukemia, RAS oncogenes, NUCLEOPHOSMIN, CYTOGENETICS, PATIENTS

Abstract

Transforming mutations in RAS genes are commonly found in human malignancies, including myeloid leukemias. To investigate the incidence, spectrum, and distribution of activating K- and N- RAS mutations in cytogenetically normal acute myeloid leukemia (CN-AML) patients, 204 CN-AML patients were screened. Activating K- and N- RAS mutations were detected in 3 of 204 (1.5 %) and 22 of 204 (10.8 %) CN-AML samples, respectively. RAS mutated patients presented with a lower percentage of bone marrow blasts (65 vs 80 %, P = 0.022). RAS mutations tended to occur with nucleophosmin-1 ( NPM1) mutations ( P = 0.079), and all three samples containing K- RAS mutations had concomitant NPM1 mutations. There was no significant overlap between K- RAS mutations and N- RAS, FLT3, CEBPA, IDH1/ 2, WT1 or MLL mutations. RAS mutation status did not impact relapse-free or overall survival of CN-AML patients. In contrast to reports of noncanonical RAS mutations in other cancers, including some leukemia subtypes, we only observed K- and N- RAS mutations in codons 12, 13, or 61 in CN-AML samples. Our findings suggest that while K- RAS mutations are infrequent in CN-AML, activating K- RAS mutations may cooperate with mutated NPM1 to induce leukemia. [ABSTRACT FROM AUTHOR]

Published

2014

35. Long-term results of a prospective randomized trial evaluating G-CSF priming in intensive induction chemotherapy followed by autologous stem cell transplantation in elderly patients with acute myeloid leukemia.

Author

Bug, Gesine, Koschmieder, Steffen, Krauter, Juergen, Heuser, Michael, Thol, Felicitas, Wiebe, Stefanie, Hofmann, Wolf-Karsten, Klein, Stefan, Wegener, Gerd, Göhring, Gudrun, Heit, Wolfgang, Hoelzer, Dieter, Ganser, Arnold, and Ottmann, Oliver

Subjects

ACUTE myeloid leukemia, GRANULOCYTE-colony stimulating factor, CANCER chemotherapy, CANCER treatment, STEM cell transplantation research

Abstract

Few studies have evaluated granulocyte colony-stimulating factor (G-CSF) priming in elderly patients with intensively treated acute myeloid leukemia (AML), and no data are available for genetically defined AML subgroups. We provide long-term results (median follow-up 7.6 years) of a randomized trial in which 183 patients (median age 67 years) received G-CSF prior to (G-CSF priming) or after two cycles of induction chemotherapy. CR rates with G-CSF priming and G-CSF post-chemotherapy were comparable (57 vs. 67 %, p = 0.153), with overall survival (OS) probabilities of 14 vs. 17 % at 10 years. Induction mortality was significantly higher with G-CSF priming (23 vs. 10 %, p = 0.015), primarily in normal karyotype (NK) AML. In this subgroup, a trend for better relapse-free survival (RFS) was observed with G-CSF priming (44 vs. 22 % at 10 years, p = 0.074) but did not translate into an OS benefit. G-CSF priming had no impact on AML with FLT3-ITD and NPM mutations and did not improve outcome in patients with adverse cytogenetics. In a landmark analysis, late consolidation with autologous stem cell transplantation or a second consolidation cycle significantly improved RFS compared with one consolidation cycle (21.0 vs. 12.8 months, p = 0.046). Future studies on G-CSF priming should be restricted to NK AML and used only in post-remission therapy. [ABSTRACT FROM AUTHOR]

Published

2014

36. Individualisierte Medizin in der Diagnostik und prognostischen Einschätzung in der akuten myeloischen Leukämie mit normalem Karyotyp bei Erwachsenen unter 65 Jahren: eine systematische Literaturrecherche und Metaanalyse zu FLT3-ITD.

Author

Port, Matthias, Böttcher, Miriam, Thol, Felicitas, Trachte, Nicole, Wasem, Jürgen, Ganser, Arnold, Pouryamout, Laura, and Neumann, Anja

Abstract

Copyright of Ethik in der Medizin is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2013

37. Monitoring dendritic cell and cytokine biomarkers during remission prior to relapse in patients with FLT3-ITD acute myeloid leukemia.

Author

Rickmann, Mareike, Macke, Laura, Sundarasetty, Bala, Stamer, Kathrin, Figueiredo, Constanca, Blasczyk, Rainer, Heuser, Michael, Krauter, Juergen, Ganser, Arnold, and Stripecke, Renata

Subjects

DENDRITIC cells, CYTOKINES, BIOMARKERS, DISEASE remission, ACUTE myeloid leukemia treatment, CANCER relapse, GENETIC mutation

Abstract

Relapse occurs frequently after treatment of acute myeloid leukemia (AML) patients with the FMS-like tyrosine kinase 3-internal tandem duplication (ITD) mutation. The availability of immunologic biomarkers to predict patients at high risk could allow clinicians to accelerate alternative treatments such as stem cell transplantation, immunotherapy, or novel drugs. We have previously reported that first diagnostic (FD) ITD AML showed immunophenotypic and functional characteristics of arrested dendritic cell (DC) precursors. In this study, we show that the high frequency of precursor DCs in 16 FD ITD AML samples (Lin/HLA-DR/CD11c/CD123) was associated with a lack of terminal DCs (myeloid DCs: BDCA-1 or BDCA-3; plasmacytoid DC: BDCA-2). We further evaluated prospectively the peripheral blood complete remission (CR) samples obtained from 11 ITD AML patients after chemotherapy regarding the frequency of DCs and their pattern of cytokine production. Whereas the aberrant frequencies of precursor and terminal plasmacytoid DCs resolved during remission, the myeloid DC compartment did not fully recover. For an available cohort of patients ( n = 4) who could be monitored over a period of >15 months after FD, we identified IL-10, TNF-α, IL-6, and IL-1β as cytokines produced by the CR samples at high levels a few months prior to relapse. Cell-free supernatant of an FD ITD AML sample stimulated monocytes obtained from two healthy donors to secrete IL-10, TNF-α, IL-6, and IL-1β. Thus, we hypothesize that ITD AML minimal residual disease can act directly as dysfunctional antigen-presenting cells or indirectly by production of factors that convert monocytes into myeloid-derived suppressor cells secreting cytokines that promote immune evasion. Monitoring these immunologic biomarkers could improve prediction of relapse. [ABSTRACT FROM AUTHOR]

Published

2013

38. Acute leukemias of ambiguous lineage in adults: molecular and clinical characterization.

Author

Heesch, Sandra, Neumann, Martin, Schwartz, Stefan, Bartram, Isabelle, Schlee, Cornelia, Burmeister, Thomas, Hänel, Matthias, Ganser, Arnold, Heuser, Michael, Wendtner, Clemens-Martin, Berdel, Wolfgang, Gökbuget, Nicola, Hoelzer, Dieter, Hofmann, Wolf-Karsten, Thiel, Eckhard, and Baldus, Claudia

Subjects

ACUTE leukemia, MOLECULAR biology, PHENOTYPES, FLOW cytometry, GENE expression, GENETIC mutation

Abstract

Acute leukemias of ambiguous lineage represent a heterogeneous group of rare, poorly characterized leukemias with adverse outcome. No larger studies have yet performed a combined approach of molecular and clinical characterization of acute undifferentiated leukemia (AUL) and biphenotypic acute leukemia (BAL) in adults. Here we describe 16 adults with AUL and 26 with BAL and performed mutational as well as expression studies of genes with prognostic impact in acute leukemia ( BAALC, ERG, MN1, WT1, and IGFBP7). AUL showed overexpression of these genes compared to T-lymphoblastic leukemia (T-ALL), B-precursor ALL, and to acute myeloid leukemia (AML). Genotype alterations were not detectable in AUL. BAL samples were characterized by frequent WT1 mutations (18 %) and BCR-ABL translocations (30 %). ALL-based treatment protocols induced complete remissions in 40 % and AML-like therapies in 22 % of AUL/BAL patients. The outcome in both groups was very poor; a long-term survival was only observed in patients undergoing allogeneic stem cell transplantation (SCT). Our findings indicate that AUL and BAL share important molecular and high-risk features of both myeloid and lymphoid leukemias. BAL patients exhibited genetic alterations, which can be targeted therapeutically. Importantly, ALL therapy might be more effective than AML protocols and AUL/BAL patients should be considered for allogeneic SCT. [ABSTRACT FROM AUTHOR]

Published

2013

39. Morphology and quantitative composition of hematopoietic cells in murine bone marrow and spleen of healthy subjects.

Author

Yang, Min, Büsche, Guntram, Ganser, Arnold, and Li, Zhixiong

Subjects

LEUKEMIA, HEMATOPOIETIC system, BONE marrow, MICE, IMMUNE system

Abstract

Laboratory mice play an outstanding role in modeling human development and disease. In contrast to human leukemia, the spleen is involved in almost all cases, and the bone marrow is only variably involved in murine models. Although mice have been used for medical research for over 100 years, there are only few reports with a small number of cases looking at morphology and quantitative composition of murine hematopoietic cells in the bone marrow of non-transplanted animals of most strains. To our knowledge, there is not even a single report describing the splenogram in C57BL/6J mice, one of the most commonly used strains for medical research. The present study illustrates the morphology of the hematopoietic cells in the bone marrow and spleen of non-treated C57BL/6J mice and establishes the murine myelogram from the largest healthy C57BL/6J cohort reported to date. Furthermore, we present the first murine splenogram described for C57BL/6J mice. Our study supports the acceptance of the presence of >5 % blast cells as providing clear evidence of abnormality in bone marrow like in humans. In addition, we are the first to show <1 % blast cells in the normal spleen. Interestingly, classical dysplastic changes were rare in normal healthy mice. Our study of the bone marrow and spleen of healthy non-transplanted animals provides reference ranges of each cell type and for the myeloid/erythroid ratio, which can be used to interpret preclinical gene therapy data, leukemogenesis, and hematopoiesis studies, and may improve the quality of such analyses. [ABSTRACT FROM AUTHOR]

Published

2013

40. Cytological characterization of murine bone marrow and spleen hematopoietic compartments for improved assessment of toxicity in preclinical gene marking models.

Author

Yang, Min, Büsche, Guntram, Ganser, Arnold, and Li, Zhixiong

Subjects

BONE marrow, GENE therapy, HEMATOPOIETIC system, MUTAGENESIS, IMMUNE system

Abstract

Gene therapy has proven its potential to cure diseases of the hematopoietic system, but potential adverse reactions related to insertional mutagenesis by integrating gene vectors and chromosomal instability in long-lived repopulating cells have emerged as a major limitation. Preclinical gene therapy in murine models is a powerful model for assessment of gene marking efficiency and adverse reactions. However, changes in the hematologic composition after transplantation with retrovirally modified hematopoietic stem cells have not been well investigated in large cohorts of animals by systematic cytological analyses. In the present study, cytological analyses of bone marrow and spleen were performed in a large cohort ( n = 58) of C57BL/6J mice over an extended observation period after gene marking. Interestingly, we observed hematological malignancies in four out of 30 animals transplanted with dLNGFR (truncated form of the human p75 low-affinity nerve growth factor receptor) and tCD34 modified stem/progenitor cells. Our data demonstrate that cytological analysis provides important information for diagnosis of hematological disorders and thus should be included in preclinical studies and performed in each investigated animal. Together with histological analysis, flow cytometric analysis, and other analyses, the quality and predictive value of preclinical gene therapy studies will be improved. [ABSTRACT FROM AUTHOR]

Published

2013

41. Prognostic significance of expression levels of stem cell regulators MSI2 and NUMB in acute myeloid leukemia.

Author

Thol, Felicitas, Winschel, Claudia, Sonntag, Ann-Kathrin, Damm, Frederik, Wagner, Katharina, Chaturvedi, Anuhar, Göhring, Gudrun, Schlegelberger, Brigitte, Lübbert, Michael, Fiedler, Walter, Kirchner, Hartmut, Krauter, Jürgen, Ganser, Arnold, and Heuser, Michael

Subjects

ACUTE myeloid leukemia, GENE expression, HEMATOPOIETIC stem cells, CLINICAL trials, BIOMARKERS, TRANSCRIPTION factors, MULTIVARIATE analysis, REVERSE transcriptase polymerase chain reaction, PROGNOSIS

Abstract

Deregulation of the hematopoietic stem cell (HSC) compartment represents a hallmark of acute myeloid leukemia (AML). Recently, in vivo screening for genes that are involved in the regulation of HSCs has led to the discovery of Musashi-2 ( MSI2) as a key regulator of HSCs and as a suppressor of NUMB. In order to analyze the prognostic importance of MSI2 and NUMB expression in AML, MSI2 and NUMB transcript levels from 454 AML patients treated in multicenter trials AML SHG 0199 (ClinicalTrials Identifier NCT00209833) and 0295, and 38 healthy volunteers were analyzed by reverse transcriptase PCR in the context of other molecular markers ( NPM1, FLT3, CEBPA, IDH1/IDH2, DNMT3A, NRAS, WT1, KIT, MN1, BAALC, ERG, and WT1). In AML, patients with high MSI2 expression were more likely to be FLT3-ITD positive ( P < .001), NPM1 ( P < .001), and DNMT3A ( P = .003) mutated. Overall survival (OS) was shorter in AML patients with high MSI2 expression (hazard ratio, 1.48; 95 % confidence interval, 1.13-1.95, P = .005). However, relapse-free survival (RFS, P = .15) and complete remission (CR, P = .39) rates were not influenced by MSI2 expression. In multivariate analysis, MSI2 expression remained an independent prognostic factor for OS ( P = .03). NUMB expression had no impact on survival (OS, P = .47; RFS, P = .59) and CR rate ( P = .39). MSI2 but not NUMB is associated with shorter OS in AML patients and may indicate a more aggressive form of AML. [ABSTRACT FROM AUTHOR]

Published

2013

42. Interactions among HCLS1, HAX1 and LEF-1 proteins are essential for G-CSF-triggered granulopoiesis.

Author

Skokowa, Julia, Klimiankou, Maxim, Klimenkova, Olga, Lan, Dan, Gupta, Kshama, Hussein, Kais, Carrizosa, Esteban, Kusnetsova, Inna, Li, Zhixiong, Sustmann, Claudio, Ganser, Arnold, Zeidler, Cornelia, Kreipe, Hans-Heinrich, Burkhardt, Janis, Grosschedl, Rudolf, and Welte, Karl

Subjects

PROTEIN-protein interactions, HEMATOPOIETIC stem cells, GRANULOCYTE-colony stimulating factor, PHOSPHORYLATION, MYELOID leukemia, CANCER cells, GENE expression

Abstract

We found that hematopoietic cell-specific Lyn substrate 1 (HCLS1 or HS1) is highly expressed in human myeloid cells and that stimulation with granulocyte colony-stimulating factor (G-CSF) leads to HCLS1 phosphorylation. HCLS1 binds the transcription factor lymphoid-enhancer binding factor 1 (LEF-1), transporting LEF-1 into the nucleus upon G-CSF stimulation and inducing LEF-1 autoregulation. In patients with severe congenital neutropenia, inherited mutations in the gene encoding HCLS1-associated protein X-1 (HAX1) lead to profound defects in G-CSF-triggered phosphorylation of HCLS1 and subsequently to reduced autoregulation and expression of LEF-1. Consistent with these results, HCLS1-deficient mice are neutropenic. In bone marrow biopsies of the majority of tested patients with acute myeloid leukemia, HCLS1 protein expression is substantially elevated, associated with high levels of G-CSF synthesis and, in some individuals, a four-residue insertion in a proline-rich region of HCLS1 protein known to accelerate intracellular signaling. These data demonstrate the importance of HCLS1 in myelopoiesis in vitro and in vivo. [ABSTRACT FROM AUTHOR]

Published

2012

43. Prognostic significance of combined MN1, ERG, BAALC, and EVI1 (MEBE) expression in patients with myelodysplastic syndromes.

Author

Thol, Felicitas, Yun, Haiyang, Sonntag, Ann-Kathrin, Damm, Frederik, Weissinger, Eva, Krauter, Jürgen, Wagner, Katharina, Morgan, Michael, Wichmann, Martin, Göhring, Gudrun, Bug, Gesine, Ottmann, Oliver, Hofmann, Wolf-Karsten, Schambach, Axel, Schlegelberger, Brigitte, Haferlach, Torsten, Bowen, David, Mills, Ken, Ganser, Arnold, and Heuser, Michael

Subjects

GENE expression, MYELODYSPLASTIC syndromes, CYTOGENETICS, ACUTE myeloid leukemia, MULTIVARIATE analysis, BONE marrow

Abstract

Overexpression of MN1, ERG, BAALC, and EVI1 (MEBE) genes in cytogenetically normal acute myeloid leukemia (AML) patients is associated with poor prognosis, but their prognostic effect in patients with myelodysplastic syndromes (MDS) has not been studied systematically. Expression data of the four genes from 140 MDS patients were combined in an additive score, which was validated in an independent patient cohort of 110 MDS patients. A high MEBE score, defined as high expression of at least two of the four genes, predicted a significantly shorter overall survival (OS) (HR 2.29, 95 % CI 1.3-4.09, P = .005) and time to AML progression (HR 4.83, 95 % CI 2.01-11.57, P < .001) compared to a low MEBE score in multivariate analysis independent of karyotype, percentage of bone marrow blasts, transfusion dependence, ASXL1, and IDH1 mutation status. In a validation cohort of 110 MDS patients, a high MEBE score predicted shorter OS (HR 1.77; 95 % CI 1.04-3.0, P = .034) and time to AML progression (HR 3.0, 95 % CI 1.17-7.65, P = .022). A high MEBE expression score is an unfavorable prognostic marker in MDS and is associated with an increased risk for progression to AML. Expression of the MEBE genes is regulated by FLI1 and c-MYC, which are potential upstream targets of the MEBE signature. [ABSTRACT FROM AUTHOR]

Published

2012

44. Modulation of anthracycline-induced cytotoxicity by targeting the prenylated proteome in myeloid leukemia cells.

Author

Morgan, Michael, Onono, Fredrick, Spielmann, H., Subramanian, Thangaiah, Scherr, Michaela, Venturini, Letizia, Dallmann, Iris, Ganser, Arnold, and Reuter, Christoph

Subjects

MYELOID leukemia, DRUG development, IDARUBICIN, APOPTOSIS, DUAL specificity phosphatase 1, PROTEINS, ANTHRACYCLINES, CELL growth

Abstract

Deregulation of Ras/ERK signaling in myeloid leukemias makes this pathway an interesting target for drug development. Myeloid leukemia cell lines were screened for idarubicin-induced apoptosis, cell-cycle progression, cell-cycle-dependent MAP kinase kinase (MEK-1/2) activation, and Top2 expression. Cell-cycle-dependent activation of MEK/ERK signaling was blocked using farnesyltransferase inhibitor (FTI) BMS-214,662 and dual prenyltransferase inhibitor (DPI) L-778,123 to disrupt Ras signaling. Idarubicin caused a G2/M cell-cycle arrest characterized by elevated diphosphorylated MEK-1/2 and Top2α expression levels. The FTI/DPIs elicited distinct effects on Ras signaling, protein prenylation, cell cycling and apoptosis. Combining these FTI/DPIs with idarubicin synergistically inhibited proliferation of leukemia cell lines, but the L-778,123+idarubicin combination exhibited synergistic growth inhibition over a greater range of drug concentrations. Interestingly, combined FTI/DPI treatment synergistically inhibited cell proliferation, induced apoptosis and nearly completely blocked protein prenylation. Inhibition of K-Ras expression by RNA interference or blockade of its post-translational prenylation led to increased BMS-214,662-induced apoptosis. Our results suggest that nearly complete inhibition of protein prenylation using an FTI + DPI combination is the most effective method to induce apoptosis and to block anthracycline-induced activation of ERK signaling. [ABSTRACT FROM AUTHOR]

Published

2012

45. Elevated frequencies of leukemic myeloid and plasmacytoid dendritic cells in acute myeloid leukemia with the FLT3 internal tandem duplication.

Author

Rickmann, Mareike, Krauter, Juergen, Stamer, Kathrin, Heuser, Michael, Salguero, Gustavo, Mischak-Weissinger, Eva, Ganser, Arnold, and Stripecke, Renata

Subjects

ACUTE myeloid leukemia, DENDRITIC cells, PROTEIN-tyrosine kinases, GENE expression, PROTEIN precursors, CELL metabolism, DISEASE progression, BIOCHEMISTRY, GENETIC mutation, CYTOMETRY, PHENOMENOLOGY, TRANSFERASES, CELLS, GENOMES, IMMUNOPHENOTYPING, GENES

Abstract

Some 30% of acute myeloid leukemia (AML) patients display an internal tandem duplication (ITD) mutation in the FMS-like tyrosine kinase 3 (FLT3) gene. FLT3-ITDs are known to drive hematopoietic stem cells towards FLT3 ligand independent growth, but the effects on dendritic cell (DC) differentiation during leukemogenesis are not clear. We compared the frequency of cells with immunophenotype of myeloid DC (mDC: Lin(-), HLA-DR(+), CD11c(+), CD86(+)) and plasmacytoid DC (pDC: Lin(-), HLA-DR(+), CD123(+), CD86(+)) in diagnostic samples of 47 FLT3-ITD(-) and 40 FLT3-ITD(+) AML patients. The majority of ITD(+) AML samples showed high frequencies of mDCs or pDCs, with significantly decreased HLA-DR expression compared with DCs detectable in ITD(-) AML samples. Interestingly, mDCs and pDCs sorted out from ITD(+) AML samples contained the ITD insert revealing their leukemic origin and, upon ex vivo culture with cytokines, they acquired DC morphology. Notably, mDC/pDCs were detectable concurrently with single lineage mDCs and pDCs in all ITD(+) AML (n = 11) and ITD(-) AML (n = 12) samples analyzed for mixed lineage DCs (Lin(-), HLA-DR(+), CD11c(+), CD123(+)). ITD(+) AML mDCs/pDCs could be only partially activated with CD40L and CpG for production of IFN-α, TNF-α, and IL-1α, which may affect the anti-leukemia immune surveillance in the course of disease progression. [ABSTRACT FROM AUTHOR]

Published

2011

46. Myeloid growth factors in acute myeloid leukemia: systematic review of randomized controlled trials.

Author

Heuser, Michael, Zapf, Antonia, Morgan, Michael, Krauter, Jürgen, and Ganser, Arnold

Subjects

ACUTE myeloid leukemia, RANDOMIZED controlled trials, NEUTROPHILS, FEBRILE neutropenia, COLONY-stimulating factors (Physiology), HOSPITAL care

Abstract

Randomized controlled trials (RCT) investigating administration of colony-stimulating factors (CSF) during or after chemotherapy in acute myeloid leukemia (AML) patients have not been systematically reviewed. We performed a meta-analysis of all reported RCTs comparing prophylactic or concurrent use of CSFs in adult AML patients. Two reviewers extracted data independently. Summary estimates with 95% confidence intervals (CIs) were calculated using a fixed effects model. Fourteen RCTs ( n = 4,069 patients) were identified investigating prophylactic CSF administration. Time to neutrophil recovery (>500/μl) was significantly reduced in the CSF group (−4.13 days; 95% CI, −4.23 to −4.04) as was the length of hospitalization (−2.06 days; 95% CI, −2.36 to −1.76). However, no significant reduction in infection-related mortality was observed in CSF-treated compared with control patients (odds ratio (OR) 0.94; 95% CI, 0.8 to 1.1). Prophylactic CSF administration did not impact complete remission (CR) rate or survival. Fourteen RCTs ( n = 4,518 patients) were identified investigating administration of CSFs during chemotherapy. Summary estimates of CR, disease/event-free, or overall survival were not significantly different for CSF versus control patients. Prophylactic CSF administration reduces the time to neutrophil recovery and length of hospitalization, but has no impact on documented infections or outcome. Economic analyses of prophylactic CSF administration in AML patients are warranted. [ABSTRACT FROM AUTHOR]

Published

2011

47. Leukemias induced by altered TRK-signaling are sensitive to mTOR inhibitors in preclinical models.

Author

Rhein, Mathias, Schwarzer, Adrian, Min Yang, Kaever, Volkhard, Brugman, Martijn, Meyer, Johann, Ganser, Arnold, Baum, Christopher, and Zhixiong Li

Subjects

LEUKEMIA treatment, RAPAMYCIN, TROPOMYOSINS, PROTEIN-tyrosine kinases, BIOMARKERS, DRUG efficacy, PHOSPHORYLATION, LABORATORY mice

Abstract

Rapamycin is a potent allosteric mTORC1 inhibitor with clinical applications as an anticancer agent. However, only a fraction of cancer patients responds to the drug, and no biomarkers are available to predict tumor sensitivity. Recently, we and others have obtained evidence for potential involvement of tropomyosin-related kinase (TRK) receptor protein tyrosine kinases (TRKA, TRKB, TRKC) in leukemia. In the present study, we tested the therapeutic effect of Rapamycin and its analog RAD001 on altered TRK-induced leukemia in a murine model. Daily treatment with Rapamycin (2 mg/kg) or RAD001 (1 mg/kg) significantly prolonged the survival of treated animals ( n = 40) compared with the placebo group. Consistently, both mTOR and S6 proteins were strongly dephosphorylated in vitro and in vivo after treatment with Rapamycin or RAD001. However, Rapamycin did not completely inhibit mTORC1-dependent phosphorylation of 4E-BP1. With exception of one mouse showing slight reactivation of Akt after treatment, no reactivation of MAPK or Akt pathways was observed in other resistant tumors. Interestingly, leukemic cells isolated from a Rapamycin-resistant mouse were still highly sensitive to Rapamycin in vitro. Our findings suggest that altered TRK signaling may be a good predictor of tumor sensitivity to mTOR inhibition and that pathways other than MAPK and Akt exist that may trigger resistance of leukemic cells to Rapamycin in vivo. [ABSTRACT FROM AUTHOR]

Published

2011

48. Acute but not chronic graft-versus-host disease is associated with a reduction of circulating CD4CD25CD127 regulatory T cells.

Author

Ukena, Sya N., Grosse, Jens, Mischak-Weissinger, Eva, Buchholz, Stefanie, Stadler, Michael, Ganser, Arnold, and Franzke, Anke

Subjects

T cells, GRAFT versus host disease, STEM cell transplantation, IMMUNE response, INFLAMMATION

Abstract

Defects in central and peripheral tolerance are thought to contribute to life-threatening graft-versus-host disease (GvHD), a severe complication following allogeneic stem cell transplantation (SCT). Recent investigations have demonstrated regulatory T cells (Tregs) to suppress allogeneic immune reactions. Therefore, SCT patients with no or critically low numbers of Tregs may have an increased risk of GvHD. To address this hypothesis, we analyzed the recovery of CD4CD25CD127 Tregs in the peripheral blood of patients who have never developed GvHD ( n = 6), patients who developed acute/chronic GvHD ( n = 18), and patients who developed chronic GvHD without an earlier acute manifestation ( n = 5) every 30 days for the first 6 months after peripheral blood SCT (PBSCT). The number of Tregs continuously improved in acute/chronic GvHD patients, but always remained lower than Tregs quantified in patients who never developed a GvHD. In contrast, chronic GvHD patients who did not develop acute GvHD earlier displayed significantly increased Treg cell numbers at the timepoint of chronic inflammation. These results indicate that numerically deficient Tregs following PBSCT are associated with the development of acute but not chronic GvHD. [ABSTRACT FROM AUTHOR]

Published

2011

49. Molecular pathogenesis of acute myeloid leukemia: A diverse disease with new perspectives.

Author

Thol, Felicitas and Ganser, Arnold

Abstract

ute myeloid leukemia (AML) is a very heterogeneous neoplasm of the hematopoietic stem cell. Despite important achievements in the treatment of AML, the long term survival of patients with the disease remains poor. Understanding the pathogenesis of AML better is crucial for finding new treatment approaches. During AML development, hematopoietic precursor cells undergo clonal transformation in a multistep process through acquisition of chromosomal rearrangements and/or different gene mutations. Over recent years, novel gene mutations have been found in patients with AML. These mutations can be divided into two important categories, class I mutations that confer a proliferation advantage and class II mutations that inhibit myeloid differentiation. Screening for some of these mutations is now part of the initial diagnostic workup in newly diagnosed AML patients. Information about the mutation status of specific genes is useful for risk-stratification, minimal residual disease (MRD) monitoring and increasingly also for targeted therapy, especially for patients with cytogenetically normal AML (CN-AML). Besides chromosomal rearrangements and gene mutations, epigenetic regulation of genes - meaning changes in gene expression by mechanisms other than changes in the underlying DNA sequence - also represents an important mechanism of leukemogenesis. This article reviews some of the most common mutations in CN-AML and gives a perspective of the translation of these discoveries from bench to bedside. [ABSTRACT FROM AUTHOR]

Published

2010

50. Azacitidine for treatment of patients with myelodysplastic syndromes (MDS): practical recommendations of the German MDS Study Group.

Author

Götze, Katharina, Platzbecker, Uwe, Giagounidis, Aristoteles, Haase, Detlef, Lübbert, Michael, Aul, Carlo, Ganser, Arnold, Germing, Ulrich, and Hofmann, Wolf-Karsten

Subjects

MYELODYSPLASTIC syndromes, BONE marrow diseases, MYELOID leukemia, HEMATOPOIESIS, QUALITY of life

Abstract

Myelodysplastic syndromes (MDS) are a group of common bone marrow disorders characterized by ineffective hematopoiesis, peripheral cytopenias, and a substantial risk of progression to acute myeloid leukemia (AML). For many years, the main treatment option for MDS was best supportive care which alleviates symptoms, but has no effect on the natural course of the disease. Recently, demethylating agents have become available as a promising new treatment for patients with MDS. In two randomized clinical trials, the demethylating agent azacitidine has demonstrated a reduced risk of transformation to AML, improvement of peripheral blood values, an improved quality of life, and a definite survival advantage compared to conventional care regimens for patients with International Prognostic Scoring System score of intermediate-2 or high-risk MDS. This review aims to provide practical recommendations for the use of azacitidine and the management of its side effects in patients with MDS, assuring safe administration and best efficacy of treatment. [ABSTRACT FROM AUTHOR]

Published

2010