Your search keyword '"Leukemias"' showing total 2,019 results

51. Sleeping Beauty-engineered CAR T cells achieve antileukemic activity without severe toxicities.

Author

Magnani, Chiara F., Gaipa, Giuseppe, Lussana, Federico, Belotti, Daniela, Gritti, Giuseppe, Napolitano, Sara, Matera, Giada, Cabiati, Benedetta, Buracchi, Chiara, Borleri, Gianmaria, Fazio, Grazia, Zaninelli, Silvia, Tettamanti, Sarah, Cesana, Stefania, Colombo, Valentina, Quaroni, Michele, Cazzaniga, Giovanni, Rovelli, Attilio, Biagi, Ettore, and Galimberti, Stefania

Subjects

*T cells, *HEMATOPOIETIC stem cell transplantation, *ANTIGEN receptors, *DISEASE relapse, *GRAFT versus host disease, *LYMPHOBLASTIC leukemia treatment, *RESEARCH, *IMMUNIZATION, *HOMOGRAFTS, *LYMPHOBLASTIC leukemia, *RESEARCH methodology, *EVALUATION research, *MEDICAL cooperation, *COMPARATIVE studies, *RESEARCH funding

Abstract

BACKGROUNDChimeric antigen receptor (CAR) T cell immunotherapy has resulted in complete remission (CR) and durable response in highly refractory patients. However, logistical complexity and high costs of manufacturing autologous viral products limit CAR T cell availability.METHODSWe report the early results of a phase I/II trial in B cell acute lymphoblastic leukemia (B-ALL) patients relapsed after allogeneic hematopoietic stem cell transplantation (HSCT) using donor-derived CD19 CAR T cells generated with the Sleeping Beauty (SB) transposon and differentiated into cytokine-induced killer (CIK) cells.RESULTSThe cellular product was produced successfully for all patients from the donor peripheral blood (PB) and consisted mostly of CD3+ lymphocytes with 43% CAR expression. Four pediatric and 9 adult patients were infused with a single dose of CAR T cells. Toxicities reported were 2 grade I and 1 grade II cytokine-release syndrome (CRS) cases at the highest dose in the absence of graft-versus-host disease (GVHD), neurotoxicity, or dose-limiting toxicities. Six out of 7 patients receiving the highest doses achieved CR and CR with incomplete blood count recovery (CRi) at day 28. Five out of 6 patients in CR were also minimal residual disease negative (MRD-). Robust expansion was achieved in the majority of the patients. CAR T cells were measurable by transgene copy PCR up to 10 months. Integration site analysis showed a positive safety profile and highly polyclonal repertoire in vitro and at early time points after infusion.CONCLUSIONSB-engineered CAR T cells expand and persist in pediatric and adult B-ALL patients relapsed after HSCT. Antileukemic activity was achieved without severe toxicities.TRIAL REGISTRATIONClinicalTrials.gov NCT03389035.FUNDINGThis study was supported by grants from the Fondazione AIRC per la Ricerca sul Cancro (AIRC); Cancer Research UK (CRUK); the Fundación Científica de la Asociación Española Contra el Cáncer (FC AECC); Ministero Della Salute; Fondazione Regionale per la Ricerca Biomedica (FRRB). [ABSTRACT FROM AUTHOR]

Published

2020

52. Descriptive and Analytical Study of Acute Leukemia in Adults in Eastern Algeria.

Author

Tebbani, Fethi, Boudiba, Nassima, Tadjine, Karima, Rouabah, Abdelkader, and Rouabah, Leila

Subjects

*ACUTE leukemia, *LYMPHOBLASTIC leukemia, *DISEASE complications, *SYMPTOMS, *CLONE cells

Abstract

Acute leukemia (AL) is a group of malignant hemopathies characterized by monoclonal intramedullary proliferation of abnormal hematopoietic cells, the maturation process of which is blocked at the "Blast" stage. In these pathologies, an abnormal cell clone proliferates. By its character of anarchy, of nonresponse to normal regulators of cell proliferation, and its invasive character, this clone assumes all the characters of malignancy. The diagnosis of ALL can no longer be based solely on morphological and cytochemical characteristics but must include the elements of the immunological phenotype of leukemic cells. Currently, a classification based on immunophenotypic and cytogenetic data, as well as on molecular biology data, is necessary for the determination of the optimal treatment. The objective of this work is to reach a descriptive approach of acute leukemia in the region of Annaba, in the east of Algeria. Description of the epidemiological, clinical, and cytological characteristics of the cases of acute leukemia collected in the Hematology Laboratory of Dorban Hospital over a period of 6 years. Analysis of the results of our study and their comparison with those published in the literature, with a reminder of the epidemiological and diagnostic data. The retrospective study was conducted in the division of the hematology hospital of Sidi Ammar- Annaba, during the period from January 2018 to July 2019. This study was based on data from 50 patients. During our study period, the results show that 50 cases of acute leukemia confirmed by the myelogram were notified. The annual average is 12.3 cases. The collected data were made in Annaba at the CHU-Dorban. We noted a variety of clinical signs and a variety of symptoms represented mainly by fever (100%), anemia (100%), hemorrhagic syndromes (30, 6%), and splenomegaly (80.6%), for the myelogram. Acute lymphoblastic leukemia (ALL) was predominant with 25 cases. In conclusion, we can say that. Acute leukemia in adults in eastern Algeria can be expressed by a variety of symptoms and hematological disorders, in addition to a series of associated conditions. [ABSTRACT FROM AUTHOR]

Published

2020

53. Perforin-deficient CAR T cells recapitulate late-onset inflammatory toxicities observed in patients.

Author

Ishii, Kazusa, Pouzolles, Marie, Chien, Christopher D, Erwin-Cohen, Rebecca A, Kohler, M Eric, Qin, Haiying, Lei, Haiyan, Kuhn, Skyler, Ombrello, Amanda K, Dulau-Florea, Alina, Eckhaus, Michael A, Shalabi, Haneen, Yates, Bonnie, Lichtenstein, Daniel A, Zimmermann, Valérie S, Kondo, Taisuke, Shern, Jack F, Young, Howard A, Taylor, Naomi, and Shah, Nirali N

Abstract

Late-onset inflammatory toxicities resembling hemophagocytic lymphohistiocytosis (HLH) or macrophage activation syndrome (MAS) occur after chimeric antigen receptor T cell (CAR T cell) infusion and represent a therapeutic challenge. Given the established link between perforin deficiency and primary HLH, we investigated the role of perforin in anti-CD19 CAR T cell efficacy and HLH-like toxicities in a syngeneic murine model. Perforin contributed to both CD8+ and CD4+ CAR T cell cytotoxicity but was not required for in vitro or in vivo leukemia clearance. Upon CAR-mediated in vitro activation, perforin-deficient CAR T cells produced higher amounts of proinflammatory cytokines compared with WT CAR T cells. Following in vivo clearance of leukemia, perforin-deficient CAR T cells reexpanded, resulting in splenomegaly with disruption of normal splenic architecture and the presence of hemophagocytes, which are findings reminiscent of HLH. Notably, a substantial fraction of patients who received anti-CD22 CAR T cells also experienced biphasic inflammation, with the second phase occurring after the resolution of cytokine release syndrome, resembling clinical manifestations of HLH. Elevated inflammatory cytokines such as IL-1β and IL-18 and concurrent late CAR T cell expansion characterized the HLH-like syndromes occurring in the murine model and in humans. Thus, a murine model of perforin-deficient CAR T cells recapitulated late-onset inflammatory toxicities occurring in human CAR T cell recipients, providing therapeutically relevant mechanistic insights. [ABSTRACT FROM AUTHOR]

Published

2020

54. CBFB-MYH11 fusion neoantigen enables T cell recognition and killing of acute myeloid leukemia.

Author

Biernacki, Melinda A, Foster, Kimberly A, Woodward, Kyle B, Coon, Michael E, Cummings, Carrie, Cunningham, Tanya M, Dossa, Robson G, Brault, Michelle, Stokke, Jamie, Olsen, Tayla M, Gardner, Kelda, Estey, Elihu, Meshinchi, Soheil, Rongvaux, Anthony, and Bleakley, Marie

Subjects

*PROTEINS, *HOMICIDE, *IN vivo studies, *GENETIC mutation, *MUSCLE proteins, *CARCINOGENESIS, *LEUCOCYTES, *ACUTE myeloid leukemia

Abstract

Proteins created from recurrent fusion genes like CBFB-MYH11 are prevalent in acute myeloid leukemia (AML), often necessary for leukemogenesis, persistent throughout the disease course, and highly leukemia specific, making them attractive neoantigen targets for immunotherapy. A nonameric peptide derived from a prevalent CBFB-MYH11 fusion protein was found to be immunogenic in HLA-B*40:01+ donors. High-avidity CD8+ T cell clones isolated from healthy donors killed CBFB-MYH11+ HLA-B*40:01+ AML cell lines and primary human AML samples in vitro. CBFB-MYH11-specific T cells also controlled CBFB-MYH11+ HLA-B*40:01+ AML in vivo in a patient-derived murine xenograft model. High-avidity CBFB-MYH11 epitope-specific T cell receptors (TCRs) transduced into CD8+ T cells conferred antileukemic activity in vitro. Our data indicate that the CBFB-MYH11 fusion neoantigen is naturally presented on AML blasts and enables T cell recognition and killing of AML. We provide proof of principle for immunologically targeting AML-initiating fusions and demonstrate that targeting neoantigens has clinical relevance even in low-mutational frequency cancers like fusion-driven AML. This work also represents a first critical step toward the development of TCR T cell immunotherapy targeting fusion gene-driven AML. [ABSTRACT FROM AUTHOR]

Published

2020

55. Oncogene-independent BCR-like signaling adaptation confers drug resistance in Ph-like ALL.

Author

Hurtz, Christian, Wertheim, Gerald B., Loftus, Joseph P., Blumenthal, Daniel, Lehman, Anne, Yong Li,, Bagashev, Asen, Cummins, Katherine D., Burkhardt, Janis K., Perl, Alexander E., Carroll, Martin, Tasian, Sarah K., Li, Yong, and Manning, Bryan

Subjects

*PROTEIN metabolism, *PROTEINS, *RESEARCH, *DEXAMETHASONE, *PROTEIN kinase inhibitors, *LYMPHOBLASTIC leukemia, *ANIMAL experimentation, *RESEARCH methodology, *EVALUATION research, *MEDICAL cooperation, *CELLULAR signal transduction, *COMPARATIVE studies, *RESEARCH funding, *CELL lines, *MICE, *PHARMACODYNAMICS

Abstract

Children and adults with Philadelphia chromosome-like B cell acute lymphoblastic leukemia (Ph-like B-ALL) experience high relapse rates despite best-available conventional chemotherapy. Ph-like ALL is driven by genetic alterations that activate constitutive cytokine receptor and kinase signaling, and early-phase trials are investigating the potential of the addition of tyrosine kinase inhibitors (TKIs) to chemotherapy to improve clinical outcomes. However, preclinical studies have shown that JAK or PI3K pathway inhibition is insufficient to eradicate the most common cytokine receptor-like factor 2-rearranged (CRLF2-rearranged) Ph-like ALL subset. We thus sought to define additional essential signaling pathways required in Ph-like leukemogenesis for improved therapeutic targeting. Herein, we describe an adaptive signaling plasticity of CRLF2-rearranged Ph-like ALL following selective TKI pressure, which occurs in the absence of genetic mutations. Interestingly, we observed that Ph-like ALL cells have activated SRC, ERK, and PI3K signaling consistent with activated B cell receptor (BCR) signaling, although they do not express cell surface μ-heavy chain (μHC). Combinatorial targeting of JAK/STAT, PI3K, and "BCR-like" signaling with multiple TKIs and/or dexamethasone prevented this signaling plasticity and induced complete cell death, demonstrating a more optimal and clinically pragmatic therapeutic strategy for CRLF2-rearranged Ph-like ALL. [ABSTRACT FROM AUTHOR]

Published

2020

56. Mesenchymal niche remodeling impairs hematopoiesis via stanniocalcin 1 in acute myeloid leukemia.

Author

Waclawiczek, Alexander, Hamilton, Ashley, Rouault-Pierre, Kevin, Abarrategi, Ander, Garcia Albornoz, Manuel, Miraki-Moud, Farideh, Bah, Nourdine, Gribben, John, Fitzgibbon, Jude, Taussig, David, Bonnet, Dominique, and Albornoz, Manuel Garcia

Subjects

*ACUTE myeloid leukemia, *HEMATOPOIETIC stem cells, *BLOOD cells, *STROMAL cells, *STEM cell migration, *BIOLOGICAL crosstalk, *BONE marrow, *PROTEIN metabolism, *PROTEINS, *RESEARCH, *ANIMAL experimentation, *RESEARCH methodology, *EVALUATION research, *MEDICAL cooperation, *COMPARATIVE studies, *GLYCOPROTEINS, *RESEARCH funding, *HEMATOPOIESIS, *MICE

Abstract

Acute myeloid leukemia (AML) disrupts the generation of normal blood cells, predisposing patients to hemorrhage, anemia, and infections. Differentiation and proliferation of residual normal hematopoietic stem and progenitor cells (HSPCs) are impeded in AML-infiltrated bone marrow (BM). The underlying mechanisms and interactions of residual hematopoietic stem cells (HSCs) within the leukemic niche are poorly understood, especially in the human context. To mimic AML infiltration and dissect the cellular crosstalk in human BM, we established humanized ex vivo and in vivo niche models comprising AML cells, normal HSPCs, and mesenchymal stromal cells (MSCs). Both models replicated the suppression of phenotypically defined HSPC differentiation without affecting their viability. As occurs in AML patients, the majority of HSPCs were quiescent and showed enrichment of functional HSCs. HSPC suppression was largely dependent on secreted factors produced by transcriptionally remodeled MSCs. Secretome analysis and functional validation revealed MSC-derived stanniocalcin 1 (STC1) and its transcriptional regulator HIF-1α as limiting factors for HSPC proliferation. Abrogation of either STC1 or HIF-1α alleviated HSPC suppression by AML. This study provides a humanized model to study the crosstalk among HSPCs, leukemia, and their MSC niche, and a molecular mechanism whereby AML impairs normal hematopoiesis by remodeling the mesenchymal niche. [ABSTRACT FROM AUTHOR]

Published

2020

57. Enasidenib drives human erythroid differentiation independently of isocitrate dehydrogenase 2.

Author

Dutta, Ritika, Tian Yi Zhang, Köhnke, Thomas, Thomas, Daniel, Linde, Miles, Gars, Eric, Stafford, Melissa, Kaur, Satinder, Nakauchi, Yusuke, Yin, Raymond, Azizi, Armon, Narla, Anupama, Majeti, Ravindra, and Zhang, Tian Yi

Subjects

*CELL differentiation, *PORPHYRINS, *RESEARCH, *HETEROCYCLIC compounds, *RESEARCH methodology, *EVALUATION research, *MEDICAL cooperation, *COMPARATIVE studies, *AMINOPYRIDINES, *CELLS, *RESEARCH funding, *OXIDOREDUCTASES, *HEMATOPOIETIC stem cells, *CHEMICAL inhibitors

Abstract

Cancer-related anemia is present in more than 60% of newly diagnosed cancer patients and is associated with substantial morbidity and high medical costs. Drugs that enhance erythropoiesis are urgently required to decrease transfusion rates and improve quality of life. Clinical studies have observed an unexpected improvement in hemoglobin and RBC transfusion-independence in patients with acute myeloid leukemia (AML) treated with the isocitrate dehydrogenase 2 (IDH2) mutant-specific inhibitor enasidenib, leading to improved quality of life without a reduction in AML disease burden. Here, we demonstrate that enasidenib enhanced human erythroid differentiation of hematopoietic progenitors. The phenomenon was not observed with other IDH1/2 inhibitors and occurred in IDH2-deficient CRISPR-engineered progenitors independently of D-2-hydroxyglutarate. The effect of enasidenib on hematopoietic progenitors was mediated by protoporphyrin accumulation, driving heme production and erythroid differentiation in committed CD71+ progenitors rather than hematopoietic stem cells. Our results position enasidenib as a promising therapeutic agent for improvement of anemia and provide the basis for a clinical trial using enasidenib to decrease transfusion dependence in a wide array of clinical contexts. [ABSTRACT FROM AUTHOR]

Published

2020

58. Targeting AML-associated FLT3 mutations with a type I kinase inhibitor.

Author

Jones, LaQuita M., Melgar, Katelyn, Bolanos, Lyndsey, Hueneman, Kathleen, Walker, Morgan M., Jian-Kang Jiang, Wilson, Kelli M., Xiaohu Zhang, Jian Shen, Fan Jiang, Sutter, Patrick, Wang, Amy, Xin Xu, Tawa, Gregory J., Hoyt, Scott B., Wunderlich, Mark, O’Brien, Eric, Perentesis, John P., Starczynowski, Daniel T., and Thomas, Craig J.

Subjects

*ANIMAL experimentation, *COMPARATIVE studies, *DRUG delivery systems, *RESEARCH methodology, *MEDICAL cooperation, *MICE, *GENETIC mutation, *RESEARCH, *TRANSFERASES, *EVALUATION research, *ACUTE myeloid leukemia, *PROTEIN kinase inhibitors, *PHARMACODYNAMICS

Abstract

Tyrosine kinase domain (TKD) mutations contribute to acquired resistance to FMS-like tyrosine kinase 3 (FLT3) inhibitors used to treat FLT3-mutant acute myeloid leukemia (AML). We report a cocrystal structure of FLT3 with a type I inhibitor, NCGC1481, that retained potent binding and activity against FLT3 TKD and gatekeeper mutations. Relative to the current generation of advanced FLT3 inhibitors, NCGC1481 exhibited superior antileukemic activity against the common, clinically relevant FLT3-mutant AML cells in vitro and in vivo. [ABSTRACT FROM AUTHOR]

Published

2020

59. A stress-responsive enhancer induces dynamic drug resistance in acute myeloid leukemia.

Author

Williams, Mark S., Amaral, Fabio M. R., Simeoni, Fabrizio, Somervaille, Tim C. P., Amaral, Fabio Mr, and Somervaille, Tim Cp

Subjects

*DAUNOMYCIN, *ACUTE myeloid leukemia, *DRUG resistance, *DRUG resistance in cancer cells, *PROTEIN metabolism, *PROTEINS, *BIOCHEMISTRY, *RESEARCH, *GENETICS, *RESEARCH methodology, *ANTINEOPLASTIC agents, *ORGANIC compounds, *EVALUATION research, *MEDICAL cooperation, *PHENOMENOLOGY, *HYDROCARBONS, *COMPARATIVE studies, *CELLS, *GENES, *ACETIC acid, *ALKANES, *RESEARCH funding, *PHARMACODYNAMICS

Abstract

The drug efflux pump ABCB1 is a key driver of chemoresistance, and high expression predicts treatment failure in acute myeloid leukemia (AML). In this study, we identified and functionally validated the network of enhancers that controls expression of ABCB1. We show that exposure of leukemia cells to daunorubicin activated an integrated stress response-like transcriptional program to induce ABCB1 through remodeling and activation of an ATF4-bound, stress-responsive enhancer. Protracted stress primed enhancers for rapid increases in activity following re-exposure of cells to daunorubicin, providing an epigenetic memory of prior drug treatment. In primary human AML, exposure of fresh blast cells to daunorubicin activated the stress-responsive enhancer and led to dose-dependent induction of ABCB1. Dynamic induction of ABCB1 by diverse stressors, including chemotherapy, facilitated escape of leukemia cells from targeted third-generation ABCB1 inhibition, providing an explanation for the failure of ABCB1 inhibitors in clinical trials. Stress-induced upregulation of ABCB1 was mitigated by combined use of the pharmacologic inhibitors U0126 and ISRIB, which inhibit stress signaling and have potential for use as adjuvants to enhance the activity of ABCB1 inhibitors. [ABSTRACT FROM AUTHOR]

Published

2020

60. Menin inhibitor MI-3454 induces remission in MLL1-rearranged and NPM1-mutated models of leukemia.

Author

Klossowski, Szymon, Hongzhi Miao, Kempinska, Katarzyna, Tao Wu, Purohit, Trupta, EunGi Kim, Linhares, Brian M., Dong Chen, Jih, Gloria, Perkey, Eric, Huang Huang, Miao He, Bo Wen, Yi Wang, Ke Yu, Chun-Wei Lee, Stanley, Danet-Desnoyers, Gwenn, Trotman, Winifred, Kandarpa, Malathi, and Cotton, Anitria

Subjects

*LEUKEMIA, *ACUTE leukemia, *NUCLEOPHOSMIN, *PROTEIN-protein interactions, *HEMATOPOIESIS, *PROTEIN metabolism, *PROTEINS, *RESEARCH, *GENETIC mutation, *NUCLEAR proteins, *RESEARCH methodology, *ANTINEOPLASTIC agents, *EVALUATION research, *MEDICAL cooperation, *COMPARATIVE studies, *TRANSFERASES, *CELLS, *RESEARCH funding, *TUMORS, *MOLECULAR structure, *DISEASE remission, *PHARMACODYNAMICS, *CHEMICAL inhibitors

Abstract

The protein-protein interaction between menin and mixed lineage leukemia 1 (MLL1) plays a critical role in acute leukemias with translocations of the MLL1 gene or with mutations in the nucleophosmin 1 (NPM1) gene. As a step toward clinical translation of menin-MLL1 inhibitors, we report development of MI-3454, a highly potent and orally bioavailable inhibitor of the menin-MLL1 interaction. MI-3454 profoundly inhibited proliferation and induced differentiation in acute leukemia cells and primary patient samples with MLL1 translocations or NPM1 mutations. When applied as a single agent, MI-3454 induced complete remission or regression of leukemia in mouse models of MLL1-rearranged or NPM1-mutated leukemia, including patient-derived xenograft models, through downregulation of key genes involved in leukemogenesis. We also identified MEIS1 as a potential pharmacodynamic biomarker of treatment response with MI-3454 in leukemia, and demonstrated that this compound is well tolerated and did not impair normal hematopoiesis in mice. Overall, this study demonstrates, for the first time to our knowledge, profound activity of the menin-MLL1 inhibitor as a single agent in clinically relevant PDX models of leukemia. These data provide a strong rationale for clinical translation of MI-3454 or its analogs for leukemia patients with MLL1 rearrangements or NPM1 mutations. [ABSTRACT FROM AUTHOR]

Published

2020

61. Inhospital exercise benefits in childhood cancer: A prospective cohort study.

Author

Morales, Javier S., Santana‐Sosa, Elena, Santos‐Lozano, Alejandro, Baño‐Rodrigo, Antonio, Valenzuela, Pedro L., Rincón‐Castanedo, Cecilia, Fernández‐Moreno, David, González Vicent, Marta, Pérez‐Somarriba, Marta, Madero, Luis, Lassaletta, Alvaro, Fiuza‐Luces, Carmen, and Lucia, Alejandro

Subjects

*LEUKEMIA treatment, *ANTHROPOMETRY, *CANCER chemotherapy, *CANCER relapse, *CARDIOVASCULAR system physiology, *HOSPITAL care of children, *COMBINED modality therapy, *ECONOMIC aspects of diseases, *ECHOCARDIOGRAPHY, *EXERCISE therapy, *LEFT heart ventricle, *LONGITUDINAL method, *MEDICAL care costs, *METASTASIS, *RISK assessment, *SURVIVAL, *TUMORS in children, *DISEASE risk factors, DIAGNOSIS of tumors in children

Abstract

Childhood cancer patients are at risk of developing important adverse effects, mortality and disease relapse after treatments, which has a substantial economic impact on healthcare systems. The objective of this study was to determine the effects of supervised inhospital exercise on clinical endpoints during childhood cancer treatment. 169 children with a new diagnosis of cancer were divided into an exercise intervention (n = 68, 11 ± 4 years) or a control group (n = 101, 11 ± 3 years). The cohort was followed up from the start of treatment for up to five years. Supervised inhospital exercise intervention was performed during the neoadjuvant (for solid tumors) or intensive chemotherapy treatment period (for leukemias). The median duration of the intervention was 22 (interquartile range, 14‐28) weeks. We assessed survival, risk of disease relapse or metastasis, and days of hospitalization (primary outcomes), and cardiovascular function, anthropometry and blood variables (secondary outcomes). No exercise‐related adverse events were noted. The exercise group had significantly less days of hospitalization than the control group (P = .031), resulting in a lower (~−17%) mean total economic cost of hospitalization in the former. Moreover, echocardiography‐determined left ventricular function (ejection fraction and fractional shortening) was significantly impaired in the control group after treatment compared with baseline, whereas it was maintained in the exercise group (P = .024 and.021 for the between‐group differences, respectively). In conclusion, supervised inhospital exercise intervention is safe and plays a cardioprotective role, at least in the short term, in children with cancer, also reducing hospitalization time, and therefore alleviating the economic burden. [ABSTRACT FROM AUTHOR]

Published

2020

62. SHP2 inhibition reduces leukemogenesis in models of combined genetic and epigenetic mutations.

Author

Pandey, Ruchi, Ramdas, Baskar, Changlin Wan, Sandusky, George, Mohseni, Morvarid, Chi Zhang, Kapur, Reuben, Wan, Changlin, and Zhang, Chi

Subjects

*GENETIC models, *PRELEUKEMIA, *PROTEIN-tyrosine phosphatase, *ACUTE myeloid leukemia, *CYTOKINE receptors, *PHOSPHOPROTEIN phosphatases, *ALLOSTERIC regulation

Abstract

In patients with acute myeloid leukemia (AML), 10% to 30% with the normal karyotype express mutations in regulators of DNA methylation, such as TET2 or DNMT3A, in conjunction with activating mutation in the receptor tyrosine kinase FLT3. These patients have a poor prognosis because they do not respond well to established therapies. Here, utilizing mouse models of AML that recapitulate cardinal features of the human disease and bear a combination of loss-of-function mutations in either Tet2 or Dnmt3a along with expression of Flt3ITD, we show that inhibition of the protein tyrosine phosphatase SHP2, which is essential for cytokine receptor signaling (including FLT3), by the small molecule allosteric inhibitor SHP099 impairs growth and induces differentiation of leukemic cells without impacting normal hematopoietic cells. We also show that SHP099 normalizes the gene expression program associated with increased cell proliferation and self-renewal in leukemic cells by downregulating the Myc signature. Our results provide a new and more effective target for treating a subset of patients with AML who bear a combination of genetic and epigenetic mutations. [ABSTRACT FROM AUTHOR]

Published

2019

63. Chimeric antigen receptor-induced BCL11B suppression propagates NK-like cell development.

Author

Maluski, Marcel, Ghosh, Arnab, Herbst, Jessica, Scholl, Vanessa, Baumann, Rolf, Huehn, Jochen, Geffers, Robert, Meyer, Johann, Maul, Holger, Eiz-Vesper, Britta, Krueger, Andreas, Schambach, Axel, van den Brink, Marcel R. M., Sauer, Martin G., and van den Brink, Marcel Rm

Subjects

*HEMATOPOIETIC stem cells, *TRANSGENE expression, *STEM cell transplantation, *CHIMERIC antigen receptors, *B cells

Abstract

The transcription factor B cell CLL/lymphoma 11B (BCL11B) is indispensable for T lineage development of lymphoid progenitors. Here, we show that chimeric antigen receptor (CAR) expression during early phases of ex vivo generation of lymphoid progenitors suppressed BCL11B, leading to suppression of T cell-associated gene expression and acquisition of NK cell-like properties. Upon adoptive transfer into hematopoietic stem cell transplant recipients, CAR-expressing lymphoid progenitors differentiated into CAR-induced killer (CARiK) cells that mediated potent antigen-directed antileukemic activity even across MHC barriers. CD28 and active immunoreceptor tyrosine-based activation motifs were critical for a functional CARiK phenotype. These results give important insights into differentiation of murine and human lymphoid progenitors driven by synthetic CAR transgene expression and encourage further evaluation of ex vivo-generated CARiK cells for targeted immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2019

64. Tissue Transplantation

Author

Khan, Manzoor M. and Khan, Manzoor M

Published

2016

65. Biallelic TET2 mutations confer sensitivity to 5'-azacitidine in acute myeloid leukemia.

Author

Stölzel, Friedrich, Stölzel, Friedrich, Fordham, Sarah E, Nandana, Devi, Lin, Wei-Yu, Blair, Helen, Elstob, Claire, Bell, Hayden L, Mohr, Brigitte, Ruhnke, Leo, Kunadt, Desiree, Dill, Claudia, Allsop, Daniel, Piddock, Rachel, Soura, Emmanouela-Niki, Park, Catherine, Fadly, Mohd, Rahman, Thahira, Alharbi, Abrar, Wobus, Manja, Altmann, Heidi, Röllig, Christoph, Wagenführ, Lisa, Jones, Gail L, Menne, Tobias, Jackson, Graham H, Marr, Helen J, Fitzgibbon, Jude, Onel, Kenan, Meggendorfer, Manja, Robinson, Amber, Bziuk, Zuzanna, Bowes, Emily, Heidenreich, Olaf, Haferlach, Torsten, Villar, Sara, Ariceta, Beñat, Diaz, Rosa Ayala, Altschuler, Steven J, Wu, Lani F, Prosper, Felipe, Montesinos, Pau, Martinez-Lopez, Joaquin, Bornhäuser, Martin, Allan, James M, Stölzel, Friedrich, Stölzel, Friedrich, Fordham, Sarah E, Nandana, Devi, Lin, Wei-Yu, Blair, Helen, Elstob, Claire, Bell, Hayden L, Mohr, Brigitte, Ruhnke, Leo, Kunadt, Desiree, Dill, Claudia, Allsop, Daniel, Piddock, Rachel, Soura, Emmanouela-Niki, Park, Catherine, Fadly, Mohd, Rahman, Thahira, Alharbi, Abrar, Wobus, Manja, Altmann, Heidi, Röllig, Christoph, Wagenführ, Lisa, Jones, Gail L, Menne, Tobias, Jackson, Graham H, Marr, Helen J, Fitzgibbon, Jude, Onel, Kenan, Meggendorfer, Manja, Robinson, Amber, Bziuk, Zuzanna, Bowes, Emily, Heidenreich, Olaf, Haferlach, Torsten, Villar, Sara, Ariceta, Beñat, Diaz, Rosa Ayala, Altschuler, Steven J, Wu, Lani F, Prosper, Felipe, Montesinos, Pau, Martinez-Lopez, Joaquin, Bornhäuser, Martin, and Allan, James M

Abstract

Precision medicine can significantly improve outcomes for patients with cancer, but implementation requires comprehensive characterization of tumor cells to identify therapeutically exploitable vulnerabilities. Here, we describe somatic biallelic TET2 mutations in an elderly patient with acute myeloid leukemia (AML) that was chemoresistant to anthracycline and cytarabine but acutely sensitive to 5'-azacitidine (5'-Aza) hypomethylating monotherapy, resulting in long-term morphological remission. Given the role of TET2 as a regulator of genomic methylation, we hypothesized that mutant TET2 allele dosage affects response to 5'-Aza. Using an isogenic cell model system and an orthotopic mouse xenograft, we demonstrate that biallelic TET2 mutations confer sensitivity to 5'-Aza compared with cells with monoallelic mutations. Our data argue in favor of using hypomethylating agents for chemoresistant disease or as first-line therapy in patients with biallelic TET2-mutated AML and demonstrate the importance of considering mutant allele dosage in the implementation of precision medicine for patients with cancer.

Published

2023

66. Multiomics of Bohring-Opitz syndrome truncating ASXL1 mutations identify canonical and noncanonical Wnt signaling dysregulation.

Author

Lin, Isabella, Lin, Isabella, Wei, Angela, Awamleh, Zain, Singh, Meghna, Ning, Aileen, Herrera, Analeyla, REACH Biobank and Registry, Russell, Bianca E, Weksberg, Rosanna, Arboleda, Valerie A, Lin, Isabella, Lin, Isabella, Wei, Angela, Awamleh, Zain, Singh, Meghna, Ning, Aileen, Herrera, Analeyla, REACH Biobank and Registry, Russell, Bianca E, Weksberg, Rosanna, and Arboleda, Valerie A

Abstract

ASXL1 (additional sex combs-like 1) plays key roles in epigenetic regulation of early developmental gene expression. De novo protein-truncating mutations in ASXL1 cause Bohring-Opitz syndrome (BOS; OMIM #605039), a rare neurodevelopmental condition characterized by severe intellectual disabilities, distinctive facial features, hypertrichosis, increased risk of Wilms tumor, and variable congenital anomalies, including heart defects and severe skeletal defects giving rise to a typical BOS posture. These BOS-causing ASXL1 variants are also high-prevalence somatic driver mutations in acute myeloid leukemia. We used primary cells from individuals with BOS (n = 18) and controls (n = 49) to dissect gene regulatory changes caused by ASXL1 mutations using comprehensive multiomics assays for chromatin accessibility (ATAC-seq), DNA methylation, histone methylation binding, and transcriptome in peripheral blood and skin fibroblasts. Our data show that regardless of cell type, ASXL1 mutations drive strong cross-tissue effects that disrupt multiple layers of the epigenome. The data showed a broad activation of canonical Wnt signaling at the transcriptional and protein levels and upregulation of VANGL2, which encodes a planar cell polarity pathway protein that acts through noncanonical Wnt signaling to direct tissue patterning and cell migration. This multiomics approach identifies the core impact of ASXL1 mutations and therapeutic targets for BOS and myeloid leukemias.

Published

2023

67. Cancers in Adolescence

Author

Harif, Mhamed, Stefan, Daniela Cristina, Stefan, Daniela Cristina, and Harif, Mhamed

Published

2017

68. Ectonucleotidases in Blood Malignancies: A Tale of Surface Markers and Therapeutic Targets

Author

Tiziana Vaisitti, Francesca Arruga, Giulia Guerra, and Silvia Deaglio

Subjects

CD38, CD39, CD73, leukemias, myeloma, lymphoma, Immunologic diseases. Allergy, RC581-607

Abstract

Leukemia develops as the result of intrinsic features of the transformed cell, such as gene mutations and derived oncogenic signaling, and extrinsic factors, such as a tumor-friendly, immunosuppressed microenvironment, predominantly in the lymph nodes and the bone marrow. There, high extracellular levels of nucleotides, mainly NAD+ and ATP, are catabolized by different ectonucleotidases, which can be divided in two families according to substrate specificity: on one side those that metabolize NAD+, including CD38, CD157, and CD203a; on the other, those that convert ATP, namely CD39 (and other ENTPDases) and CD73. They generate products that modulate intracellular calcium levels and that activate purinergic receptors. They can also converge on adenosine generation with profound effects, both on leukemic cells, enhancing chemoresistance and homing, and on non-malignant immune cells, polarizing them toward tolerance. This review will first provide an overview of ectonucleotidases expression within the immune system, in physiological and pathological conditions. We will then focus on different hematological malignancies, discussing their role as disease markers and possibly pathogenic agents. Lastly, we will describe current efforts aimed at therapeutic targeting of this family of enzymes.

Published

2019

69. Rewiring the Epigenetic Networks in MLL-Rearranged Leukemias: Epigenetic Dysregulation and Pharmacological Interventions

Author

Anthony K. N. Chan and Chun-Wei Chen

Subjects

MLL-rearranged, leukemias, epigenetics, MLL, chromatin, Biology (General), QH301-705.5

Abstract

Leukemias driven by chromosomal translocation of the mixed-lineage leukemia gene (MLL or KMT2A) are highly prevalent in pediatric oncology. The poor survival rate and lack of an effective targeted therapy for patients with MLL-rearranged (MLL-r) leukemias emphasize an urgent need for improved knowledge and novel therapeutic approaches for these malignancies. The resulting chimeric products of MLL gene rearrangements, i.e., MLL-fusion proteins (MLL-FPs), are capable of transforming hematopoietic stem/progenitor cells (HSPCs) into leukemic blasts. The ability of MLL-FPs to reprogram HSPCs toward leukemia requires the involvement of multiple chromatin effectors, including the histone 3 lysine 79 methyltransferase DOT1L, the chromatin epigenetic reader BRD4, and the super elongation complex. These epigenetic regulators constitute a complicated network that dictates maintenance of the leukemia program, and therefore represent an important cluster of therapeutic opportunities. In this review, we will discuss the role of MLL and its fusion partners in normal HSPCs and hematopoiesis, including the links between chromatin effectors, epigenetic landscapes, and leukemia development, and summarize current approaches to therapeutic targeting of MLL-r leukemias.

Published

2019

70. PD-1H/VISTA mediates immune evasion in acute myeloid leukemia.

Author

Kim TK, Han X, Hu Q, Vandsemb EN, Fielder CM, Hong J, Kim KW, Mason EF, Plowman RS, Wang J, Wang Q, Zhang JP, Badri T, Sanmamed MF, Zheng L, Zhang T, Alawa J, Lee SW, Zeidan AM, Halene S, Pillai MM, Chandhok NS, Lu J, Xu ML, Gore SD, and Chen L

Subjects

Animals, Humans, Mice, Bone Marrow, Immunity, Cellular, Immunotherapy, Immune Evasion, Leukemia, Myeloid, Acute drug therapy

Abstract

Acute myeloid leukemia (AML) presents a pressing medical need in that it is largely resistant to standard chemotherapy as well as modern therapeutics, such as targeted therapy and immunotherapy, including anti-programmed cell death protein (anti-PD) therapy. We demonstrate that programmed death-1 homolog (PD-1H), an immune coinhibitory molecule, is highly expressed in blasts from the bone marrow of AML patients, while normal myeloid cell subsets and T cells express PD-1H. In studies employing syngeneic and humanized AML mouse models, overexpression of PD-1H promoted the growth of AML cells, mainly by evading T cell-mediated immune responses. Importantly, ablation of AML cell-surface PD-1H by antibody blockade or genetic knockout significantly inhibited AML progression by promoting T cell activity. In addition, the genetic deletion of PD-1H from host normal myeloid cells inhibited AML progression, and the combination of PD-1H blockade with anti-PD therapy conferred a synergistic antileukemia effect. Our findings provide the basis for PD-1H as a potential therapeutic target for treating human AML.

Published

2024

71. Targeting lysine demethylase 6B ameliorates ASXL1 truncation-mediated myeloid malignancies in preclinical models.

Author

Ge G, Zhang P, Sui P, Chen S, Yang H, Guo Y, Rubalcava IP, Noor A, Delma CR, Agosto-Peña J, Geng H, Medina EA, Liang Y, Nimer SD, Mesa R, Abdel-Wahab O, Xu M, and Yang FC

Subjects

Humans, Mice, Animals, Lysine, Repressor Proteins genetics, Repressor Proteins metabolism, Transcription Factors metabolism, Jumonji Domain-Containing Histone Demethylases metabolism, Histones metabolism, Neoplasms

Abstract

ASXL1 mutation frequently occurs in all forms of myeloid malignancies and is associated with aggressive disease and poor prognosis. ASXL1 recruits Polycomb repressive complex 2 (PRC2) to specific gene loci to repress transcription through trimethylation of histone H3 on lysine 27 (H3K27me3). ASXL1 alterations reduce H3K27me3 levels, which results in leukemogenic gene expression and the development of myeloid malignancies. Standard therapies for myeloid malignancies have limited efficacy when mutated ASXL1 is present. We discovered upregulation of lysine demethylase 6B (KDM6B), a demethylase for H3K27me3, in ASXL1-mutant leukemic cells, which further reduces H3K27me3 levels and facilitates myeloid transformation. Here, we demonstrated that heterozygous deletion of Kdm6b restored H3K27me3 levels and normalized dysregulated gene expression in Asxl1Y588XTg hematopoietic stem/progenitor cells (HSPCs). Furthermore, heterozygous deletion of Kdm6b decreased the HSPC pool, restored their self-renewal capacity, prevented biased myeloid differentiation, and abrogated progression to myeloid malignancies in Asxl1Y588XTg mice. Importantly, administration of GSK-J4, a KDM6B inhibitor, not only restored H3K27me3 levels but also reduced the disease burden in NSG mice xenografted with human ASXL1-mutant leukemic cells in vivo. This preclinical finding provides compelling evidence that targeting KDM6B may be a therapeutic strategy for myeloid malignancies with ASXL1 mutations.

Published

2024

72. Genome editing-induced t(4;11) chromosomal translocations model B cell precursor acute lymphoblastic leukemias with KMT2A-AFF1 fusion.

Author

Pan F, Sarno J, Jeong J, Yang X, Jager A, Gruber TA, Davis KL, and Cleary ML

Subjects

Humans, Gene Editing, Proteomics, Myeloid-Lymphoid Leukemia Protein genetics, DNA-Binding Proteins genetics, Transcriptional Elongation Factors genetics, Translocation, Genetic, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma genetics

Abstract

A t(4;11) leukemia model established from CRISPR-engineered chromosomal translocations between the KMT2A and AFF1 genes recapitulate proteomic, epigenomic, and transcriptomic features of primary patient leukemias.

Published

2024

73. A gain-of-function p53 mutant synergizes with oncogenic NRAS to promote acute myeloid leukemia in mice.

Author

Rajagopalan A, Feng Y, Gayatri MB, Ranheim EA, Klungness T, Matson DR, Lee MH, Jung MM, Zhou Y, Gao X, Nadiminti KV, Yang DT, Tran VL, Padron E, Miyamoto S, Bresnick EH, and Zhang J

Subjects

Animals, Humans, Mice, Gain of Function Mutation, GTP Phosphohydrolases genetics, GTP Phosphohydrolases metabolism, Membrane Proteins genetics, Membrane Proteins metabolism, Mitogen-Activated Protein Kinase Kinases, Mutation, Leukemia, Myeloid, Acute genetics, Leukemia, Myeloid, Acute metabolism, NF-kappa B metabolism, Tumor Suppressor Protein p53 genetics

Abstract

We previously demonstrated that a subset of acute myeloid leukemia (AML) patients with concurrent RAS pathway and TP53 mutations have an extremely poor prognosis and that most of these TP53 mutations are missense mutations. Here, we report that, in contrast to the mixed AML and T cell malignancy that developed in NrasG12D/+ p53-/- (NP-/-) mice, NrasG12D/+ p53R172H/+ (NPmut) mice rapidly developed inflammation-associated AML. Under the inflammatory conditions, NPmut hematopoietic stem and progenitor cells (HSPCs) displayed imbalanced myelopoiesis and lymphopoiesis and mostly normal cell proliferation despite MEK/ERK hyperactivation. RNA-Seq analysis revealed that oncogenic NRAS signaling and mutant p53 synergized to establish an NPmut-AML transcriptome distinct from that of NP-/- cells. The NPmut-AML transcriptome showed GATA2 downregulation and elevated the expression of inflammatory genes, including those linked to NF-κB signaling. NF-κB was also upregulated in human NRAS TP53 AML. Exogenous expression of GATA2 in human NPmut KY821 AML cells downregulated inflammatory gene expression. Mouse and human NPmut AML cells were sensitive to MEK and NF-κB inhibition in vitro. The proteasome inhibitor bortezomib stabilized the NF-κB-inhibitory protein IκBα, reduced inflammatory gene expression, and potentiated the survival benefit of a MEK inhibitor in NPmut mice. Our study demonstrates that a p53 structural mutant synergized with oncogenic NRAS to promote AML through mechanisms distinct from p53 loss.

Published

2023

74. Proteogenomic analysis reveals cytoplasmic sequestration of RUNX1 by the acute myeloid leukemia-initiating CBFB::MYH11 oncofusion protein.

Author

Day RB, Hickman JA, Xu Z, Katerndahl CD, Ferraro F, Ramakrishnan SM, Erdmann-Gilmore P, Sprung RW, Mi Y, Townsend RR, Miller CA, and Ley TJ

Subjects

Humans, Mice, Animals, Core Binding Factor Alpha 2 Subunit genetics, Translocation, Genetic, Oncogene Proteins, Fusion genetics, Oncogene Proteins, Fusion metabolism, Core Binding Factor beta Subunit, Myosin Heavy Chains genetics, Proteogenomics, Leukemia, Myeloid, Acute pathology

Abstract

Several canonical translocations produce oncofusion genes that can initiate acute myeloid leukemia (AML). Although each translocation is associated with unique features, the mechanisms responsible remain unclear. While proteins interacting with each oncofusion are known to be relevant for how they act, these interactions have not yet been systematically defined. To address this issue in an unbiased fashion, we fused a promiscuous biotin ligase (TurboID) in-frame with 3 favorable-risk AML oncofusion cDNAs (PML::RARA, RUNX1::RUNX1T1, and CBFB::MYH11) and identified their interacting proteins in primary murine hematopoietic cells. The PML::RARA- and RUNX1::RUNX1T1-TurboID fusion proteins labeled common and unique nuclear repressor complexes, implying their nuclear localization. However, CBFB::MYH11-TurboID-interacting proteins were largely cytoplasmic, probably because of an interaction of the MYH11 domain with several cytoplasmic myosin-related proteins. Using a variety of methods, we showed that the CBFB domain of CBFB::MYH11 sequesters RUNX1 in cytoplasmic aggregates; these findings were confirmed in primary human AML cells. Paradoxically, CBFB::MYH11 expression was associated with increased RUNX1/2 expression, suggesting the presence of a sensor for reduced functional RUNX1 protein, and a feedback loop that may attempt to compensate by increasing RUNX1/2 transcription. These findings may have broad implications for AML pathogenesis.

Published

2023

75. Stochasticity and Determinism in Models of Hematopoiesis

Author

Kimmel, Marek, Cohen, Irun R., Series editor, Lajtha, N.S. Abel, Series editor, Paoletti, Rodolfo, Series editor, Lambris, John D., Series editor, Corey, Seth Joel, editor, Kimmel, Marek, editor, and Leonard, Joshua N., editor

Published

2014

76. MicroRNAs and Blood Cancers

Author

Lawrie, Charles H. and Babashah, Sadegh, editor

Published

2014

77. DNA methyltransferase inhibition overcomes diphthamide pathway deficiencies underlying CD123-targeted treatment resistance.

Author

Katsuhiro Togami, Pastika, Timothy, Stephansky, Jason, Ghandi, Mahmoud, Christie, Amanda L., Jones, Kristen L., Johnson, Carl A., Lindsay, Ross W., Brooks, Christopher L., Letai, Anthony, Craig, Jeffrey W., Pozdnyakova, Olga, Weinstock, David M., Montero, Joan, Aster, Jon C., Johannessen, Cory M., Lane, Andrew A., and Togami, Katsuhiro

Subjects

*DNA methyltransferases, *AZACITIDINE, *DIPHTHERIA toxin, *ACUTE myeloid leukemia, *O6-Methylguanine-DNA Methyltransferase, *INTERLEUKIN-3, *DNA methylation, *PROTEIN metabolism, *DRUG delivery systems, *DENDRITIC cells, *RESEARCH, *ANIMAL experimentation, *RESEARCH methodology, *CELL receptors, *ANTINEOPLASTIC agents, *EVALUATION research, *COMPARATIVE studies, *HEMATOLOGIC malignancies, *RESEARCH funding, *CELL lines, *MICE, *HISTOCOMPATIBILITY antigens, *RECOMBINANT proteins, *PHARMACODYNAMICS

Abstract

The interleukin-3 receptor α subunit, CD123, is expressed in many hematologic malignancies including acute myeloid leukemia (AML) and blastic plasmacytoid dendritic cell neoplasm (BPDCN). Tagraxofusp (SL-401) is a CD123-targeted therapy consisting of interleukin-3 fused to a truncated diphtheria toxin payload. Factors influencing response to tagraxofusp other than CD123 expression are largely unknown. We interrogated tagraxofusp resistance in patients and experimental models and found that it was not associated with CD123 loss. Rather, resistant AML and BPDCN cells frequently acquired deficiencies in the diphthamide synthesis pathway, impairing tagraxofusp's ability to ADP-ribosylate cellular targets. Expression of DPH1, encoding a diphthamide pathway enzyme, was reduced by DNA CpG methylation in resistant cells. Treatment with the DNA methyltransferase inhibitor azacitidine restored DPH1 expression and tagraxofusp sensitivity. We also developed a drug-dependent ADP-ribosylation assay in primary cells that correlated with tagraxofusp activity and may represent an additional novel biomarker. As predicted by these results and our observation that resistance also increased mitochondrial apoptotic priming, we found that the combination of tagraxofusp and azacitidine was effective in patient-derived xenografts treated in vivo. These data have important implications for clinical use of tagraxofusp and led to a phase 1 study combining tagraxofusp and azacitidine in myeloid malignancies. [ABSTRACT FROM AUTHOR]

Published

2019

78. LRRC33 is a novel binding and potential regulating protein of TGF-β1 function in human acute myeloid leukemia cells.

Author

Ma, Wenjiang, Qin, Yan, Chapuy, Bjoern, and Lu, Chafen

Subjects

*ACUTE myeloid leukemia, *CARRIER proteins, *INTEGRINS, *CELLS, *CELL membranes, *PROTEINS

Abstract

Transforming growth factor‑β1 (TGF-β1) is a versatile cytokine. It has context-dependent pro- and anti-cell proliferation functions. Activation of latent TGF-β1 requires release of the growth factor from pro-complexes and is regulated through TGF-β binding proteins. Two types of TGF-β binding partners, latent TGF-β-binding proteins (LTBPs) and leucine-rich-repeat-containing protein 32 (LRRC32), have been identified and their expression are cell specific. TGF-β1 also plays important roles in acute myeloid leukemia (AML) cells. However, the expression of LTBPs and LRRC32 are lacking in myeloid lineage cells and the binding protein of TGF-β1 in these cells are unknown. Here we show that a novel leucine-rich-repeat-containing protein family member, LRRC33, with high mRNA level in AML cells, to be the binding and regulating protein of TGF-β1 in AML cells. Using two representative cell lines MV4-11 and AML193, we demonstrate that the protein expression of LRRC33 and TGF-β1 are correlated. LRRC33 co-localizes and forms complex with latent TGF-β1 protein on the cell surface and intracellularly in these cells. Similar as in other cell types, the activation of TGF-β1 in MV4-11 and AML193 cells are also integrin dependent. We anticipate our study to be a starting point of more comprehensive research on LRRC33 as novel TGF-β regulating protein and potential non-genomic based drug target for AML and other myeloid malignancy. [ABSTRACT FROM AUTHOR]

Published

2019

79. Vancomycin-resistance gene cluster, vanC, in the gut microbiome of acute leukemia patients undergoing intensive chemotherapy.

Author

Rashidi, Armin, Zhu, Zhigang, Kaiser, Thomas, Manias, Dawn A., Holtan, Shernan G., Rehman, Tauseef Ur, Weisdorf, Daniel J., Khoruts, Alexander, Dunny, Gary M., and Staley, Christopher

Subjects

*ENTEROCOCCAL infections, *ACUTE leukemia, *GENE clusters, *GUT microbiome, *CANCER chemotherapy, *VANCOMYCIN resistance, *DRUG resistance in cancer cells

Abstract

Two recent reports suggested that the less common, less virulent enterococcal species, Enterococcus gallinarum and E. casseliflavus, with low-level vancomycin resistance due to chromosomally encoded vanC1 and vanC2/3, may influence host immunity. We reported that peri-transplant gut colonization with E. gallinarum and E. casseliflavus is associated with lower mortality after allogeneic hematopoietic cell transplantation (HCT). Because most acute leukemia patients undergoing HCT have received intensive chemotherapy (usually requiring prolonged hospitalization) for their underlying disease before HCT, we hypothesized that some may have acquired vanC-positive enterococci during chemotherapy. Therefore, we evaluated the presence of the vanC gene cluster using vanC1 and vanC2/3 qPCR in thrice-weekly collected stool samples from 20 acute leukemia patients undergoing intensive chemotherapy. We found that an unexpectedly large proportion of patients have detectable vanC1 and vanC2/3 (15% and 35%, respectively) in at least one stool sample. Comparing qPCR results with 16S rRNA gene sequencing results suggested that E. gallinarum may reach high abundances, potentially persisting into HCT and influencing transplant outcomes. [ABSTRACT FROM AUTHOR]

Published

2019

80. Ectonucleotidases in Blood Malignancies: A Tale of Surface Markers and Therapeutic Targets.

Author

Vaisitti, Tiziana, Arruga, Francesca, Guerra, Giulia, and Deaglio, Silvia

Subjects

PURINERGIC receptors, INTRACELLULAR calcium, BONE marrow, HEMATOLOGIC malignancies, BLOOD

Abstract

Leukemia develops as the result of intrinsic features of the transformed cell, such as gene mutations and derived oncogenic signaling, and extrinsic factors, such as a tumor-friendly, immunosuppressed microenvironment, predominantly in the lymph nodes and the bone marrow. There, high extracellular levels of nucleotides, mainly NAD+ and ATP, are catabolized by different ectonucleotidases, which can be divided in two families according to substrate specificity: on one side those that metabolize NAD+, including CD38, CD157, and CD203a; on the other, those that convert ATP, namely CD39 (and other ENTPDases) and CD73. They generate products that modulate intracellular calcium levels and that activate purinergic receptors. They can also converge on adenosine generation with profound effects, both on leukemic cells, enhancing chemoresistance and homing, and on non-malignant immune cells, polarizing them toward tolerance. This review will first provide an overview of ectonucleotidases expression within the immune system, in physiological and pathological conditions. We will then focus on different hematological malignancies, discussing their role as disease markers and possibly pathogenic agents. Lastly, we will describe current efforts aimed at therapeutic targeting of this family of enzymes. [ABSTRACT FROM AUTHOR]

Published

2019

81. Blast vacuolization in AML patients indicates adverse-risk AML and is associated with impaired survival after intensive induction chemotherapy.

Author

Ballo, Olivier, Stratmann, Jan, Serve, Hubert, Steffen, Björn, Finkelmeier, Fabian, and Brandts, Christian

Subjects

*ACUTE myeloid leukemia, *MYELOID leukemia, *BIOLOGICAL tags, *BLASTING, *CANCER chemotherapy, *BONE marrow, *BOMBINGS

Abstract

Introduction: Vacuolization is a frequently found morphological feature in acute myeloid leukemia (AML) blasts. Subcellular origin and biological function as well as prognostic impact are currently unknown. The aim of this study was to evaluate whether vacuolization correlates with clinically relevant AML features. Materials & methods: Bone marrow smears of patients diagnosed with AML at the University Hospital Frankfurt between January 2011 and August 2013 were analyzed for blast vacuolization and correlated with clinically relevant AML features. Patients undergoing standard induction chemotherapy were further analyzed for molecular and cytogenetic features as well as treatment response and survival. Results: 14 of 100 patients diagnosed with AML receiving standard induction chemotherapy had evidence of blast vacuolization. Positivity for vacuolization correlated with a CD15 positive immunophenotype and with a higher incidence of high-risk AML according to the European LeukemiaNet risk stratification. AML patients with blast vacuolization had a poor blast clearance after standard induction chemotherapy and poor survival. Discussion: In conclusion, our findings demonstrate that vacuolization can easily be determined in myeloid leukemia blasts and may be a useful biomarker to predict AML risk groups as well as early treatment response rates and survival. [ABSTRACT FROM AUTHOR]

Published

2019

82. Wikipedia network analysis of cancer interactions and world influence.

Author

Rollin, Guillaume, Lages, José, and Shepelyansky, Dima L.

Subjects

*DRUGS, *CANCER, *LUNG cancer, *HYPERLINKS, *PROSTATE cancer

Abstract

We apply the Google matrix algorithms for analysis of interactions and influence of 37 cancer types, 203 cancer drugs and 195 world countries using the network of 5 416 537 English Wikipedia articles with all their directed hyperlinks. The PageRank algorithm provides a ranking of cancers which has 60% and 70% overlaps with the top 10 deadliest cancers extracted from World Health Organization GLOBOCAN 2018 and Global Burden of Diseases Study 2017, respectively. The recently developed reduced Google matrix algorithm gives networks of interactions between cancers, drugs and countries taking into account all direct and indirect links between these selected 435 entities. These reduced networks allow to obtain sensitivity of countries to specific cancers and drugs. The strongest links between cancers and drugs are in good agreement with the approved medical prescriptions of specific drugs to specific cancers. We argue that this analysis of knowledge accumulated in Wikipedia provides useful complementary global information about interdependencies between cancers, drugs and world countries. [ABSTRACT FROM AUTHOR]

Published

2019

83. Human cord blood (hCB)-CD34+ humanized mice fail to reject human acute myeloid leukemia cells.

Author

Tanaskovic, Olga, Verga Falzacappa, Maria Vittoria, and Pelicci, Pier Giuseppe

Subjects

*CORD blood, *ACUTE myeloid leukemia, *BONE marrow, *MICE, *BONE marrow transplantation, *IMMUNE system

Abstract

Since their appearance, humanized mice carrying human immune system seemed promising tools to study the crosstalk between cancer and immunity. The NOD-scidIL2Rgammanull (NSG) mice engrafted with human cord blood (hCB)-CD34+ cells have been proposed to be a valuable tool to reproduce human immune system in mouse. However, the lack of solid evidences on the functionality of their human immune components limits their usage in immune-oncology. We report that (hCB)-CD34+ cells lose their ability to propagate and originate bone marrow-derived human immune cells after two serial transplantations in NSG mice. We demonstrate that transplants of bone marrow patient-derived acute myeloid leukemias (hAMLs) grow very similarly in the humanized (hCB)-CD34+ NSG and parental NSG mice. The similar extent of engraftment and development of leukemias in (hCB)-CD34+ NSG and controls suggests a poor human immune response against not compatible hAMLs. Our findings suggest that (hCB)-CD34+ NSG mice are transient and/or incomplete carriers of the human immune system and, therefore, represent a suboptimal tool to study the interaction between tumor and immune cells. [ABSTRACT FROM AUTHOR]

Published

2019

84. Changes in intracellular folate metabolism during high-dose methotrexate and Leucovorin rescue therapy in children with acute lymphoblastic leukemia.

Author

Oosterom, Natanja, de Jonge, Robert, Smith, Desiree E. C., Pieters, Rob, Tissing, Wim J. E., Fiocco, Marta, van Zelst, Bertrand D., van den Heuvel-Eibrink, Marry M., and Heil, Sandra G.

Subjects

*LYMPHOBLASTIC leukemia, *ACUTE leukemia, *FOLINIC acid, *METABOLISM, *METHOTREXATE, *ERYTHROCYTES

Abstract

Background: Methotrexate (MTX) is an important anti-folate agent in pediatric acute lymphoblastic leukemia (ALL) treatment. Folinic acid rescue therapy (Leucovorin) is administered after MTX to reduce toxicity. Previous studies hypothesized that Leucovorin could ‘rescue’ both normal healthy cells and leukemic blasts from cell death. We assessed whether Leucovorin is able to restore red blood cell folate levels after MTX. Methods: We prospectively determined erythrocyte folate levels (5-methyltetrahydrofolate (THF) and non-methyl THF) and serum folate levels in 67 children with ALL before start (T0) and after stop (T1) of HD-MTX and Leucovorin courses. Results: Erythrocyte folate levels increased between T0 and T1 (mean ± SD: 416.7 ± 145.5 nmol/L and 641.2 ± 196.3 nmol/L respectively, p<0.001). This was due to an increase in 5-methyl THF levels (mean increase: 217.7 ± 209.5 nmol/L, p<0.001), whereas non-methyl THF levels did not change (median increase: 0.6 nmol/L [-9.9–11.1], p = 0.676). Serum folate levels increased between T0 and T1 (median increase: 29.2 nmol/L [32.9–74.0], p<0.001). Results were not significantly affected by age, sex, ALL immunophenotype and MTHFR c.677C>T genotype. Conclusion: Intracellular folate levels accumulate after HD-MTX and Leucovorin therapy in children with ALL, suggesting that Leucovorin restores the intracellular folate pool. Future studies are necessary to assess concomitant lower uptake of MTX. [ABSTRACT FROM AUTHOR]

Published

2019

85. Acute lymphoid and myeloid leukemia in a Brazilian Amazon population: Epidemiology and predictors of comorbidity and deaths.

Author

Silva-Junior, Alexander Leonardo, Alves, Fabíola Silva, Kerr, Marlon Wendell Athaydes, Xabregas, Lilyane Amorim, Gama, Fábio Magalhães, Rodrigues, Maria Gabriela Almeida, Torres, Alexandre Santos, Tarragô, Andréa Monteiro, Sampaio, Vanderson Souza, Carvalho, Maria Perpétuo Socorro Sampaio, Fraiji, Nelson Abrahim, Malheiro, Adriana, and Costa, Allyson Guimarães

Subjects

*ACUTE myeloid leukemia, *MEDICAL databases, *COMORBIDITY, *LYMPHOCYTIC leukemia, *EPIDEMIOLOGY, *ACUTE leukemia, *CHILDHOOD cancer

Abstract

Introduction: Leukemia is the most common cancer in children and has the highest rates of incidence in industrialized countries, followed by developing countries. This epidemiologic profile can mainly be attributed to the availability of diagnostic resources. In Brazil, leukemia diagnosis is a challenge due to financial viability, lack of hemovigilance services in isolated regions and the vast size of the territory. Its incidence in the state of Amazonas has been increasing since 2010. Therefore, this study aims to describe the epidemiological pattern and spatial distribution of patients with acute lymphoid leukemia and acute myeloid leukemia in Amazonas and identify the predictors of comorbidity and death. Materials and methods: A retrospective cross-sectional study was carried out based on patients’ data which was obtained from the database of a referral center for the period of 2005 to 2015. Variables included age, gender, ethnicity, civil status, schooling, income, location of residence, subtype of leukemia, comorbidities, and date of death. The spatial distribution was performed using QGIS v.2.18. Stata software was used for univariable and multivariable logistic regression to evaluate the association between both comorbidities and death for all characteristic groups of ALL and AML. Results: The group that was studied was composed of 577 ALL and 266 AML patients. For both, most patients were male, with a schooling period of 1–4 years, received<1 minimum wage, and lived mostly in Manaus, followed by the municipality of Tefé. There was no association between the development of comorbidities and analyzed variables in patients with ALL. AML patients that were >60 years old and with family history of the disease had the highest risk of developing comorbidities (OR = 5.06, p = 0.038; OR = 2.44, p = 0.041, respectively). Furthermore, patients with ALL and in the 41-50-year age group had a higher risk of death (OR = 31.12; p = 0.001). No association between death and explanatory variables were found in patients with AML. In addition, significant difference was observed in time to death (chi2 = 4,098.32, p = 0.000), with 50% of patients with AML dying within two years after diagnosis, whereas in ALL, this percentual of death only is reached in approximately 5 years. Conclusion: Our study describes the data of patients with acute leukemia in Amazonas, a remote region in the north of Brazil. In addition, it highlights the importance of hemovigilance in an Amazon region state, while focusing on peripheral areas which don't have prevention, diagnosis and treatment tools for this disease. [ABSTRACT FROM AUTHOR]

Published

2019

86. A comparative proteomic study of plasma in Colombian childhood acute lymphoblastic leukemia.

Author

Calderon-Rodríguez, Sandra Isabel, Sanabria-Salas, María Carolina, and Umaña-Perez, Adriana

Subjects

*LYMPHOBLASTIC leukemia, *ACUTE leukemia, *BLOOD proteins, *EXTRACELLULAR matrix proteins, *CHILDHOOD cancer, *BLOOD coagulation factors

Abstract

Acute lymphoblastic leukemia (ALL) is the most common childhood cancer. Owing to the incorporation of risk-adapted therapy and the arrival of new directed agents, the cure rate and survival of patients with ALL have improved dramatically, get near to 90%. In Latin American countries, the mortality rates of ALL are high, for example in Colombia, during the last decade, ALL has been the most prevalent cancer among children between 0–14 years of age. In the face of this public health problem and coupled with the fact that the knowledge of the proteome of the child population is little, our investigation proposes the study of the plasma proteome of Colombian children diagnosed with B-cell ALL (B-ALL) to determine potential disease markers that could reflect processes altered by the presence of the disease or in response to it. A proteomic study by LC-MS/MS and quantification by label-free methods were performed in search of proteins differentially expressed between healthy children and those diagnosed with B-ALL. We quantified a total of 472 proteins in depleted blood plasma, and 25 of these proteins were differentially expressed (fold change >2, Bonferroni-adjusted P-values <0.05). Plasma Aggrecan core protein, alpha-2-HS-glycoprotein, coagulation factor XIII A chain and gelsolin protein were examined by ELISA assay and compared to shotgun proteomics results. Our data provide new information on the plasma proteome of Colombian children. Additionally, these proteins may also have certain potential as illness markers or as therapeutic targets in subsequent investigations. [ABSTRACT FROM AUTHOR]

Published

2019

87. Racial/ethnic, age and sex disparities in leukemia survival among adults in the United States during 1973-2014 period.

Author

Utuama, Ovie, Mukhtar, Fahad, Pham, Yen Thi-Hai, Dabo, Bashir, Manani, Priyashi, Moser, Jenna, Michael-Asalu, Abimbola, Tran, Chi TD, Le, Linh C., Le, Thanh V., Vu, Khanh Truong, Park, Jong Y., Boffetta, Paolo, Zheng, Wei, Shu, Xiao-Ou, and Luu, Hung N.

Subjects

*AGE differences, *LEUKEMIA, *CHRONIC myeloid leukemia, *LYMPHOBLASTIC leukemia, *RACE, *PROPORTIONAL hazards models, *FRAIL elderly

Abstract

There has been marked improvement in leukemia survival, particularly among children in recent time. However, the long-term trends in survival among adult leukemia patients and the associated sex and racial survival disparities are not well understood. We, therefore, evaluated the secular trends in survival improvement of leukemia patients from 1973 through 2014, using Surveillance Epidemiology and End-Result Survey Program (SEER) data. ICD-O-3 morphology codes were used to group leukemia into four types: acute lymphoblastic leukemia (ALL), acute myeloid leukemia (AML), chronic lymphocytic leukemia (CLL), chronic myeloid leukemia (CML). Survival analysis for each leukemia type stratified by race/ethnicity, age, sex was performed to generate relative survival probability estimates for the baseline time period of 1973 through 1979. Hazard ratios (HR) and respective 95% confidence intervals (CIs) for survival within subsequent 10-year time periods by race, age and sex were calculated using Cox proportional hazard models. Of the 83,255 leukemia patients for the current analysis, the 5-year survival of patients with ALL, AML, CLL, and CML during 1973–1979 were 42.0%, 6.5%, 66.5%, and 20.9%, respectively. Compared to the baseline, there were substantial improvements of leukemia-specific survival in 2010–2014 among African-American (81.0%) and Asian (80.0%) patients with CML and among 20–49 year of age with CLL (96.0%). African-American patients, those with AML and those older than 75 years of age had the lowest survival improvements. Asians experienced some of the largest survival improvements during the study period. Others, including African-American and the elderly, have not benefited as much from advances in leukemia treatment. [ABSTRACT FROM AUTHOR]

Published

2019

88. How have advances in CT dosimetry software impacted estimates of CT radiation dose and cancer incidence? A comparison of CT dosimetry software: Implications for past and future research.

Author

Maxwell, Susannah, Fox, Richard, McRobbie, Donald, Bulsara, Max, Doust, Jenny, O’Leary, Peter, Slavotinek, John, Stubbs, John, and Moorin, Rachael

Subjects

*RADIATION dosimetry, *RADIATION doses, *IONIZING radiation, *HUMAN body, *BLAND-Altman plot

Abstract

Objective: Organ radiation dose from a CT scan, calculated by CT dosimetry software, can be combined with cancer risk data to estimate cancer incidence resulting from CT exposure. We aim to determine to what extent the use of improved anatomical representation of the adult human body “phantom” in CT dosimetry software impacts estimates of radiation dose and cancer incidence, to inform comparison of past and future research. Methods: We collected 20 adult cases for each of three CT protocols (abdomen/pelvis, chest and head) from each of five public hospitals (random sample) (January-April inclusive 2010) and three private clinics (self-report). Organ equivalent and effective dose were calculated using both ImPACT (mathematical phantom) and NCICT (voxelised phantom) software. Bland-Altman plots demonstrate agreement and Passing-Bablok regression reports systematic, proportional or random differences between results. We modelled the estimated lifetime attributable risk of cancer from a single exposure for each protocol, using age-sex specific risk-coefficients from the Biologic Effects of Ionizing Radiation VII report. Results: For the majority of organs used in epidemiological studies of cancer incidence, the NCICT software (voxelised) provided higher dose estimates. Across the lifespan NCICT resulted in cancer estimates 2.9%-6.6% and 14.8%-16.3% higher in males and females (abdomen/pelvis) and 7.6%-19.7% and 12.9%-26.5% higher in males and females respectively (chest protocol). For the head protocol overall cancer estimates were lower for NCICT, but with greatest disparity, >30% at times. Conclusion: When the results of previous studies estimating CT dose and cancer incidence are compared to more recent, or future, studies the dosimetry software must be considered. Any change in radiation dose or cancer risk may be attributable to the software and phantom used, rather than—or in addition to—changes in scanning practice. Studies using dosimetry software to estimate radiation dose should describe software comprehensively to facilitate comparison with past and future research. [ABSTRACT FROM AUTHOR]

Published

2019

89. Modeling dynamics and alternative treatment strategies in acute promyelocytic leukemia.

Author

JrYoshinari, Gerson Hiroshi, Fassoni, Artur César, Mello, Luis Fernando, and Rego, Eduardo M.

Subjects

*ACUTE promyelocytic leukemia, *ALTERNATIVE medicine, *THERAPEUTICS, *ACUTE leukemia, *CYTOLOGY, *NATALIZUMAB

Abstract

Acute Promyelocytic Leukemia (APL) is a rare and potentially lethal condition in which risk-based therapy often leads to better outcomes. Because of its rarity and relatively high overall survival rate, prospective randomized trials to investigate alternative APL treatment schedules are challenging. Mathematical models may provide useful information in this regard. We collected clinical data from 38 patients treated for APL under the International Consortium on Acute Leukemia (ICAL) protocol and laboratory data during induction therapy. We propose a mathematical model that represents the dynamics of leukocytes in peripheral blood and the effect of ICAL treatment on the disease’s dynamics. We observe that our cohort presents demographic characteristics and clinical outcomes similar to previous clinical trials on APL. Over a follow-up period of 41.8 months, the relapse-free survival and overall survival at two years are both found to be 78.7%. For two selected patients, the model produces a good fit to the clinical data. Information such as the response to treatment and risk of relapse can be derived from the model, and this may assist in clinical practice and the design of clinical trials. [ABSTRACT FROM AUTHOR]

Published

2019

90. PAX5 is part of a functional transcription factor network targeted in lymphoid leukemia.

Author

Okuyama, Kazuki, Strid, Tobias, Kuruvilla, Jacob, Somasundaram, Rajesh, Cristobal, Susana, Smith, Emma, Prasad, Mahadesh, Fioretos, Thoas, Lilljebjörn, Henrik, Soneji, Shamit, Lang, Stefan, Ungerbäck, Jonas, and Sigvardsson, Mikael

Subjects

*LYMPHOCYTIC leukemia, *TRANSCRIPTION factors, *CHIMERIC proteins, *DNA-binding proteins, *GENE expression, *KARYOTYPES

Abstract

One of the most frequently mutated proteins in human B-lineage leukemia is the transcription factor PAX5. These mutations often result in partial rather than complete loss of function of the transcription factor. While the functional dose of PAX5 has a clear connection to human malignancy, there is limited evidence for that heterozygote loss of PAX5 have a dramatic effect on the development and function of B-cell progenitors. One possible explanation comes from the finding that PAX5 mutated B-ALL often display complex karyotypes and additional mutations. Thus, PAX5 might be one component of a larger transcription factor network targeted in B-ALL. To investigate the functional network associated with PAX5 we used BioID technology to isolate proteins associated with this transcription factor in the living cell. This identified 239 proteins out of which several could be found mutated in human B-ALL. Most prominently we identified the commonly mutated IKZF1 and RUNX1, involved in the formation of ETV6-AML1 fusion protein, among the interaction partners. ChIP- as well as PLAC-seq analysis supported the idea that these factors share a multitude of target genes in human B-ALL cells. Gene expression analysis of mouse models and primary human leukemia suggested that reduced function of PAX5 increased the ability of an oncogenic form of IKZF1 or ETV6-AML to modulate gene expression. Our data reveals that PAX5 belong to a regulatory network frequently targeted by multiple mutations in B-ALL shedding light on the molecular interplay in leukemia cells. [ABSTRACT FROM AUTHOR]

Published

2019

91. Telomere length and its correlation with gene mutations in chronic lymphocytic leukemia in a Korean population.

Author

Song, Da Young, Kim, Jung-Ah, Jeong, Dajeong, Yun, Jiwon, Kim, Sung-Min, Lim, Kyumin, Park, Si Nae, Im, Kyongok, Choi, Sungbin, Yoon, Sung-Soo, and Lee, Dong Soon

Subjects

*CHRONIC lymphocytic leukemia, *TELOMERES, *KARYOTYPES, *BONE marrow cells, *FLUORESCENCE in situ hybridization, *CYTOLOGY

Abstract

Telomere length (TL) is a prognostic indicator in Caucasian chronic lymphocytic leukemia (CLL), but its significance in Asian CLL remains unknown. To investigate the prognostic significance of TL and its correlation with cytogenetic aberrations and somatic mutations, we analyzed TL measurements at the cellular level by interphase fluorescence in situ hybridization in patients with CLL in Korea. The present study enrolled 110 patients (41 females and 69 males) diagnosed with CLL according to the World Health Organization criteria (2001–2017). TLs of bone marrow nucleated cells at the single-cell level were measured by quantitative fluorescence in situ hybridization (Q-FISH) in 71 patients. The correlations of TL with clinical characteristics, cytogenetic aberrations, genetic mutations, and overall survival were assessed. The median value of mean TL in CLL patients (T/C ratio 7.46 (range 1.19–18.14) was significantly shorter than that in the normal controls (T/C ratio 15.28 (range 8.59–24.93) (p < 0.001). Shorter TLs were associated with complex karyotypes (p = 0.030), del(11q22) (p = 0.023), presence of deletion and/or mutation in ATM and/or TP53 (p = 0.019), and SH2B3 mutation (p = 0.015). A shorter TL was correlated with lower hemoglobin levels and adverse survival (mean TL < 9.35, p = 0.021). When the proportion of cells with extremely short TLs (< 7.61) was greater than 90%, CLL patients showed poor survival (p = 0.002). Complex karyotypes, TP53 mutation, and the number of mutated genes were determined to be significant adverse variables by multivariable Cox analysis (p = 0.011, p = 0.002, and p = 0.002, respectively). TL was attrited in CLL, and attrited telomeres were correlated with adverse survival and other well-known adverse prognostic factors. We infer that TL is an independent adverse prognostic predictor in Korean CLL. [ABSTRACT FROM AUTHOR]

Published

2019

92. CRLF2 rearrangement in Ph-like acute lymphoblastic leukemia predicts relative glucocorticoid resistance that is overcome with MEK or Akt inhibition.

Author

Meyer, Lauren K., Delgado-Martin, Cristina, Maude, Shannon L., Shannon, Kevin M., Teachey, David T., and Hermiston, Michelle L.

Subjects

*LYMPHOBLASTIC leukemia, *ACUTE leukemia, *THERAPEUTICS, *CYTOKINE receptors, *CHROMOSOMAL rearrangement, *GLUCOCORTICOIDS

Abstract

Philadelphia chromosome-like (Ph-like) acute lymphoblastic leukemia (ALL) is a genetically heterogeneous subtype of B-cell ALL characterized by chromosomal rearrangements and mutations that result in aberrant cytokine receptor and kinase signaling. In particular, chromosomal rearrangements resulting in the overexpression of cytokine receptor-like factor 2 (CRLF2) occur in 50% of Ph-like ALL cases. CRLF2 overexpression is associated with particularly poor clinical outcomes, though the molecular basis for this is currently unknown. Glucocorticoids (GCs) are integral to the treatment of ALL and GC resistance at diagnosis is an important negative prognostic factor. Given the importance of GCs in ALL therapy and the poor outcomes for patients with CRLF2 overexpression, we hypothesized that the aberrant signal transduction associated with CRLF2 overexpression might mediate intrinsic GC insensitivity. To test this hypothesis, we exposed Ph-like ALL cells from patient-derived xenografts to GCs and found that CRLF2 rearranged (CRLF2R) leukemias uniformly demonstrated reduced GC sensitivity in vitro. Furthermore, targeted inhibition of signal transduction with the MEK inhibitor trametinib and the Akt inhibitor MK2206, but not the JAK inhibitor ruxolitinib, was sufficient to augment GC sensitivity. These data suggest that suboptimal GC responses may in part underlie the poor clinical outcomes for patients with CRLF2 overexpression and provide rationale for combination therapy involving GCs and signal transduction inhibitors as a means of enhancing GC efficacy. [ABSTRACT FROM AUTHOR]

Published

2019

93. Increased methotrexate intolerance in juvenile idiopathic arthritis compared to acute lymphoblastic leukaemia in children.

Author

Kyvsgaard, Nini, Mikkelsen, Torben Stamm, Thastum, Mikael, Christensen, Anne Estmann, Wehner, Peder Skov, Nysom, Karsten, and Herlin, Troels

Subjects

*JUVENILE idiopathic arthritis, *DRUG side effects, *PHYSICIANS, *MEDICAL personnel

Abstract

Objectives: To analyse the internal consistency of an adaption of the methotrexate intolerance severity score (MISS); and to describe and compare the level of methotrexate intolerance evaluated by the MISS in Danish children with juvenile idiopathic arthritis (JIA) or acute lymphoblastic leukaemia (ALL), treated with low-dose methotrexate (MTX). Methods: Cross-sectional study of children diagnosed with JIA or ALL, treated with low-dose MTX, aged 9 years or above, and cognitively intact. The patient’s parents completed the MISS. MTX intolerance was defined as a total MISS score above 6. Results: We enrolled 120 children with JIA and 23 children with ALL. The MISS had a good internal consistency in the JIA group. The median MISS score was higher in the JIA group than in the ALL group (JIA: 8; ALL: 1; p<0.0001); and the JIA group had a larger proportion of MTX intolerant children than the ALL group (JIA: 73/120; ALL: 4/23; p<0.001). Within both the JIA group and the ALL group, the MISS total score was not significantly correlated with age, MTX dose or the duration of low-dose MTX treatment. Conclusion: In the JIA group the level of MTX intolerance was higher and more attributed to anticipatory, associative and behavioural symptoms than in the ALL group. The MISS may help to uncover whether MTX intolerance is present and which aspects are affected in the individual patient, thus guiding intervention. The MISS may also be applicable within leukaemia care. [ABSTRACT FROM AUTHOR]

Published

2019

94. Acute myeloid leukemia immunopeptidome reveals HLA presentation of mutated nucleophosmin.

Author

Narayan, Rupa, Olsson, Niclas, Wagar, Lisa E., Medeiros, Bruno C., Meyer, Everett, Czerwinski, Debra, Khodadoust, Michael S., Zhang, Lichao, Schultz, Liora, Davis, Mark M., Elias, Joshua E., and Levy, Ron

Subjects

*ACUTE myeloid leukemia, *ALLELES, *KILLER cell receptors, *MASS spectrometry, *SOMATIC mutation, *MYELOID leukemia, *LEUCOCYTES

Abstract

Somatic mutations in cancer are a potential source of cancer specific neoantigens. Acute myeloid leukemia (AML) has common recurrent mutations shared between patients in addition to private mutations specific to individuals. We hypothesized that neoantigens derived from recurrent shared mutations would be attractive targets for future immunotherapeutic approaches. Here we sought to study the HLA Class I and II immunopeptidome of thirteen primary AML tumor samples and two AML cell lines (OCI-AML3 and MV4-11) using mass spectrometry to evaluate for endogenous mutation-bearing HLA ligands from common shared AML mutations. We identified two endogenous, mutation-bearing HLA Class I ligands from nucleophosmin (NPM1). The ligands, AVEEVSLRK from two patient samples and C(cys)LAVEEVSL from OCI-AML3, are predicted to bind the common HLA haplotypes, HLA-A*03:01 and HLA-A*02:01 respectively. Since NPM1 is mutated in approximately one-third of patients with AML, the finding of endogenous HLA ligands from mutated NPM1 supports future studies evaluating immunotherapeutic approaches against this shared target, for this subset of patients with AML. [ABSTRACT FROM AUTHOR]

Published

2019

95. Distribution of endogenous gammaretroviruses and variants of the Fv1 restriction gene in individual mouse strains and strain subgroups.

Author

Skorski, Matthew, Bamunusinghe, Devinka, Liu, Qingping, Shaffer, Esther, and Kozak, Christine A.

Subjects

*MOUSE leukemia viruses, *GENES, *ENDOGENOUS retroviruses, *DISEASE incidence, *COMPLEMENT receptors, *LABORATORY mice

Abstract

Inbred laboratory mouse strains carry endogenous retroviruses (ERVs) classed as ecotropic, xenotropic or polytropic mouse leukemia viruses (E-, X- or P-MLVs). Some of these MLV ERVs produce infectious virus and/or contribute to the generation of intersubgroup recombinants. Analyses of selected mouse strains have linked the appearance of MLVs and virus-induced disease to the strain complement of MLV E-ERVs and to host genes that restrict MLVs, particularly Fv1. Here we screened inbred strain DNAs and genome assemblies to describe the distribution patterns of 45 MLV ERVs and Fv1 alleles in 58 classical inbred strains grouped in two ways: by common ancestry to describe ERV inheritance patterns, and by incidence of MLV-associated lymphomagenesis. Each strain carries a unique set of ERVs, and individual ERVs are present in 5–96% of the strains, often showing lineage-specific distributions. Two ERVs are alternatively present as full-length proviruses or solo long terminal repeats. High disease incidence strains carry the permissive Fv1n allele, tested strains have highly expressed E-ERVs and most have the Bxv1 X-ERV; these three features are not present together in any low-moderate disease strain. The P-ERVs previously implicated in P-MLV generation are not preferentially found in high leukemia strains, but the three Fv1 alleles that restrict inbred strain E-MLVs are found only in low-moderate leukemia strains. This dataset helps define the genetic basis of strain differences in spontaneous lymphomagenesis, describes the distribution of MLV ERVs in strains with shared ancestry, and should help annotate sequenced strain genomes for these insertionally polymorphic and functionally important proviruses. [ABSTRACT FROM AUTHOR]

Published

2019

96. Антитялова имунотерапия в съвременното лечение на левкемиите и лимфомите при деца и юноши

Author

Аврамова, Б.

Abstract

The successful treatment of hematological cancers in the last decades, especially of acute lymphoblastic leukemia in children, is a result from the stratification of the patients in risk groups on the basis of clinical and laboratory markers at the time of diagnosis, and also the response to induction therapy. The traditional chemotherapy has a considerable role in the cure of the patients from the standard and intermediate groups, but is not enough for the high risk patients - primary resistant or relapsed. The innovations in cytogenetic and molecular genetic diagnosis identified in the last years new targets of the diseases and their correspond treatment agents. The target therapy include two basic groups - antibody immune models and cellulare therapy. These new keys treatment modalities enter increasingly in the clinical practice and provide a long term survival of the most high - risk patients. We present a review for the role, treatment design, mechanism of action and side effects of the most popular monoclonal antibodies for the treatment of leukemia and lymphomas in children. [ABSTRACT FROM AUTHOR]

Published

2019

97. SIRT1 regulates metabolism and leukemogenic potential in CML stem cells.

Author

Abraham, Ajay, Shaowei Qiu, Chacko, Balu K., Hui Li, Paterson, Andrew, Jianbo He, Agarwal, Puneet, Shah, Mansi, Welner, Robert, Darley-Usmar, Victor M., Bhatia, Ravi, Qiu, Shaowei, Li, Hui, and He, Jianbo

Subjects

*STEM cells, *CHRONIC myeloid leukemia, *HEMATOPOIETIC stem cells, *OXIDATIVE phosphorylation, *CELL transformation, *DASATINIB, *NILOTINIB, *MITOCHONDRIAL pathology, *ANIMALS, *DRUG resistance in cancer cells, *GENES, *MICE, *MITOCHONDRIA, *GENETIC mutation, *PROTEINS, *TRANSFERASES, *OXYGEN consumption, *PROTEIN kinase inhibitors, *PHARMACODYNAMICS

Abstract

Chronic myeloid leukemia (CML) results from hematopoietic stem cell transformation by the BCR-ABL kinase. Despite the success of BCR-ABL tyrosine kinase inhibitors (TKIs) in treating CML patients, leukemia stem cells (LSCs) resist elimination and persist as a major barrier to cure. Previous studies suggest that overexpression of the sirtuin 1 (SIRT1) deacetylase may contribute to LSC maintenance in CML. Here, by genetically deleting SIRT1 in transgenic CML mice, we definitively demonstrated an important role for SIRT1 in leukemia development. We identified a previously unrecognized role for SIRT1 in mediating increased mitochondrial oxidative phosphorylation in CML LSCs. We showed that mitochondrial alterations were kinase independent and that TKI treatment enhanced inhibition of CML hematopoiesis in SIRT1-deleted mice. We further showed that the SIRT1 substrate PGC-1α contributed to increased oxidative phosphorylation and TKI resistance in CML LSCs. These results reveal an important role for SIRT1 and downstream signaling mechanisms in altered mitochondrial respiration in CML LSCs. [ABSTRACT FROM AUTHOR]

Published

2019

98. Donor KIR2DS1 reduces the risk of transplant related mortality in HLA-C2 positive young recipients with hematological malignancies treated by myeloablative conditioning.

Author

Tordai, Attila, Bors, Andras, Kiss, Katalin Piroska, Balassa, Katalin, Andrikovics, Hajnalka, Batai, Arpad, Szilvasi, Aniko, Rajczy, Katalin, Inotai, Dora, Torbagyi, Eva, Lengyel, Lilla, Barta, Aniko, Remenyi, Peter, and Masszi, Tamas

Subjects

*HEMATOLOGIC malignancies, *KILLER cell receptors, *HEMATOPOIETIC stem cell transplantation, *KILLER cells, *PROGRESSION-free survival, *IMMUNOGLOBULIN receptors

Abstract

Background: Recognition of HLA-C2 group alleles on recipient cells by activating killer immunoglobulin like receptors, KIR2DS1 on donor natural killer cells may lead to increased graft-versus-leukemia effect or immunomodulation in patients treated by allogeneic hematopoietic stem cell transplantation (allo-HSCT) influencing disease free and overall survival (OS). Objective: In the present study, 314 consecutive, allo-HSCT recipient and donor pairs were included with retrospective donor KIR-genotyping and clinical parameters analyzes. Results: After a median follow-up of 23.6 months, recipients with HLA-C2 group allele (rC2) showed improved (p = 0.046) OS if transplanted with KIR2DS1 positive donors (d2DS1) compared to those without one or both of this genetic attribute. Within the myeloablative conditioning (MAC) subgroup (n = 227), rC2 homozygous+d2DS1 patients (n = 14) showed a 5 years OS of 93% followed by rC2 heterozygous+d2DS1 patients (n = 48, 65%) compared to rC2 and/or d2DS1 negatives (47%, p = 0.018). Multivariate analyses indicated rC2+d2DS1 positivity as an independent predictor of OS (HR:0.47, 0.26–0.86, p = 0.014) besides donor type, presence of CMV-reactivation or chemoresistant disease. Among MAC-treated patients, the combined rC2+d2DS1 presence was associated with a markedly decreased cumulative incidence of transplant related mortality (p = 0.0045). Conclusion: The combination of rC2+d2DS1 may be a favorable genetic constellation in allo-HSCT with MAC potentially reducing transplant related mortality. [ABSTRACT FROM AUTHOR]

Published

2019

99. Convergent genetic aberrations in murine and human T lineage acute lymphoblastic leukemias.

Author

Huang, Benjamin J., Wandler, Anica M., Meyer, Lauren K., Dail, Monique, Daemen, Anneleen, Sampath, Deepak, Li, Qing, Wang, Xinyue, Wong, Jasmine C., Nakitandwe, Joy, Downing, James R., Zhang, Jinghui, Taylor, Barry S., and Shannon, Kevin

Subjects

*LYMPHOBLASTIC leukemia, *SOMATIC mutation, *ACUTE leukemia, *THERAPEUTICS, *CARCINOGENESIS, *LEUKEMIA, *DRUG efficacy

Abstract

The lack of predictive preclinical models is a fundamental barrier to translating knowledge about the molecular pathogenesis of cancer into improved therapies. Insertional mutagenesis (IM) in mice is a robust strategy for generating malignancies that recapitulate the extensive inter- and intra-tumoral genetic heterogeneity found in advanced human cancers. While the central role of "driver" viral insertions in IM models that aberrantly increase the expression of proto-oncogenes or disrupt tumor suppressors has been appreciated for many years, the contributions of cooperating somatic mutations and large chromosomal alterations to tumorigenesis are largely unknown. Integrated genomic studies of T lineage acute lymphoblastic leukemias (T-ALLs) generated by IM in wild-type (WT) and Kras mutant mice reveal frequent point mutations and other recurrent non-insertional genetic alterations that also occur in human T-ALL. These somatic mutations are sensitive and specific markers for defining clonal dynamics and identifying candidate resistance mechanisms in leukemias that relapse after an initial therapeutic response. Primary cancers initiated by IM and resistant clones that emerge during in vivo treatment close key gaps in existing preclinical models, and are robust platforms for investigating the efficacy of new therapies and for elucidating how drug exposure shapes tumor evolution and patterns of resistance. [ABSTRACT FROM AUTHOR]

Published

2019

100. Lymphocyte counts may predict a good response to mesenchymal stromal cells therapy in graft versus host disease patients.

Author

Hinden, Liad, Avner, Mordechai, Stepensky, Polina, Or, Reuven, and Almogi-Hazan, Osnat

Subjects

*LYMPHOCYTE count, *GRAFT versus host disease, *STROMAL cells, *CELLULAR therapy, *HEMATOPOIETIC stem cell transplantation, *THERAPEUTICS

Abstract

Steroid-resistant GvHD is one of the most significant causes of mortality following allogeneic Hematopoietic Stem Cell Transplantation (HSCT). Treatment with mesenchymal stromal cells (MSC) seems to be a promising solution, however the results from clinical studies are still equivocal. Better selection of candidate patients and improving monitoring of patients following MSC administration can increase treatment effectiveness. In order to determine which characteristics can be used to predict a good response and better monitoring of patients, blood samples were taken prior to therapy, one week and one month after therapy, from 26 allogeneic HSCT patients whom contracted GvHD and were treated with MSCs. Samples were examined for differential blood counts, bilirubin levels and cell surface markers. Serum cytokine levels were also measured. We found that the level of lymphocytes, in particular T and NK cells, may predict a good response to therapy. A better response was observed among patients who expressed low levels of IL-6 and IL-22, Th17 related cytokines, prior to therapy. Patients with high levels of bilirubin prior to therapy showed a poorer response. The results of this study may facilitate early prediction of success or failure of the treatment, and subsequently, will improve selection of patients for MSC therapy. [ABSTRACT FROM AUTHOR]

Published

2019