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1. TMIGD2 is an orchestrator and therapeutic target on human acute myeloid leukemia stem cells

Author

Hao Wang, R. Alejandro Sica, Gurbakhash Kaur, Phillip M. Galbo, Zhixin Jing, Christopher D. Nishimura, Xiaoxin Ren, Ankit Tanwar, Bijan Etemad-Gilbertson, Britta Will, Deyou Zheng, David Fooksman, and Xingxing Zang

Subjects
Science
Abstract

Abstract Acute myeloid leukemia (AML) is initiated and sustained by a hierarchy of leukemia stem cells (LSCs), and elimination of this cell population is required for curative therapies. Here we show that transmembrane and immunoglobulin domain containing 2 (TMIGD2), a recently discovered co-stimulatory immune receptor, is aberrantly expressed by human AML cells, and can be used to identify and enrich functional LSCs. We demonstrate that TMIGD2 is required for the development and maintenance of AML and self-renewal of LSCs but is not essential for normal hematopoiesis. Mechanistically, TMIGD2 promotes proliferation, blocks myeloid differentiation and increases cell-cycle of AML cells via an ERK1/2-p90RSK-CREB signaling axis. Targeting TMIGD2 signaling with anti-TMIGD2 monoclonal antibodies attenuates LSC self-renewal and reduces leukemia burden in AML patient-derived xenograft models but has negligible effect on normal hematopoietic stem/progenitor cells. Thus, our studies reveal the function of TMIGD2 in LSCs and provide a promising therapeutic strategy for AML.

Published
2024
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3. Study of efficacy and longevity of immune response to third and fourth doses of COVID-19 vaccines in patients with cancer: A single arm clinical trial

Author

Astha Thakkar, Kith Pradhan, Benjamin Duva, Juan Manuel Carreno, Srabani Sahu, Victor Thiruthuvanathan, Sean Campbell, Sonia Gallego, Tushar D Bhagat, Johanna Rivera, Gaurav Choudhary, Raul Olea, Maite Sabalza, Lauren C Shapiro, Matthew Lee, Ryann Quinn, Ioannis Mantzaris, Edward Chu, Britta Will, Liise-anne Pirofski, Florian Krammer, Amit Verma, and Balazs Halmos

Subjects
SARS CoV-2, COVID-19, vaccine, immunocompromised, cancer, Medicine, Science, Biology (General), QH301-705.5
Abstract

Background: Cancer patients show increased morbidity with COVID-19 and need effective immunization strategies. Many healthcare regulatory agencies recommend administering ‘booster’ doses of COVID-19 vaccines beyond the standard two-dose series, for this group of patients. Therefore, studying the efficacy of these additional vaccine doses against SARS-CoV-2 and variants of concern is of utmost importance in this immunocompromised patient population Methods: We conducted a prospective single arm clinical trial enrolling patients with cancer that had received two doses of mRNA or one dose of AD26.CoV2.S vaccine and administered a third dose of mRNA vaccine. We further enrolled patients that had no or low responses to three mRNA COVID vaccines and assessed the efficacy of a fourth dose of mRNA vaccine. Efficacy was assessed by changes in anti-spike antibody, T-cell activity, and neutralization activity, which were again assessed at baseline and 4 weeks. Results: We demonstrate that a third dose of COVID-19 vaccine leads to seroconversion in 57% of patients that were seronegative after primary vaccination series. The immune response is durable as assessed by anti-SARS-CoV-2 (anti-S) antibody titers, T-cell activity, and neutralization activity against wild-type (WT) SARS-CoV2 and BA1.1.529 at 6 months of follow-up. A subset of severely immunocompromised hematologic malignancy patients that were unable to mount an adequate immune response (titer

Published
2023
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4. Activation of targetable inflammatory immune signaling is seen in myelodysplastic syndromes with SF3B1 mutations

Author

Gaurav S Choudhary, Andrea Pellagatti, Bogos Agianian, Molly A Smith, Tushar D Bhagat, Shanisha Gordon-Mitchell, Srabani Sahu, Sanjay Pandey, Nishi Shah, Srinivas Aluri, Ritesh Aggarwal, Sarah Aminov, Leya Schwartz, Violetta Steeples, Robert N Booher, Murali Ramachandra, Maria Samson, Milagros Carbajal, Kith Pradhan, Teresa V Bowman, Manoj M Pillai, Britta Will, Amittha Wickrema, Aditi Shastri, Robert K Bradley, Robert E Martell, Ulrich G Steidl, Evripidis Gavathiotis, Jacqueline Boultwood, Daniel T Starczynowski, and Amit Verma

Subjects
IRAK4, SF3B1, MDS, AML, CA4948, Emavusertib, Medicine, Science, Biology (General), QH301-705.5
Abstract

Background: Mutations in the SF3B1 splicing factor are commonly seen in myelodysplastic syndromes (MDS) and acute myeloid leukemia (AML), yet the specific oncogenic pathways activated by mis-splicing have not been fully elucidated. Inflammatory immune pathways have been shown to play roles in the pathogenesis of MDS, though the exact mechanisms of their activation in splicing mutant cases are not well understood. Methods: RNA-seq data from SF3B1 mutant samples was analyzed and functional roles of interleukin-1 receptor-associated kinase 4 (IRAK4) isoforms were determined. Efficacy of IRAK4 inhibition was evaluated in preclinical models of MDS/AML. Results: RNA-seq splicing analysis of SF3B1 mutant MDS samples revealed retention of full-length exon 6 of IRAK4, a critical downstream mediator that links the Myddosome to inflammatory NF-kB activation. Exon 6 retention leads to a longer isoform, encoding a protein (IRAK4-long) that contains the entire death domain and kinase domain, leading to maximal activation of NF-kB. Cells with wild-type SF3B1 contain smaller IRAK4 isoforms that are targeted for proteasomal degradation. Expression of IRAK4-long in SF3B1 mutant cells induces TRAF6 activation leading to K63-linked ubiquitination of CDK2, associated with a block in hematopoietic differentiation. Inhibition of IRAK4 with CA-4948, leads to reduction in NF-kB activation, inflammatory cytokine production, enhanced myeloid differentiation in vitro and reduced leukemic growth in xenograft models. Conclusions: SF3B1 mutation leads to expression of a therapeutically targetable, longer, oncogenic IRAK4 isoform in AML/MDS models. Funding: This work was supported by Cincinnati Children’s Hospital Research Foundation, Leukemia Lymphoma Society, and National Institute of Health (R35HL135787, RO1HL111103, RO1DK102759, RO1HL114582), Gabrielle’s Angel Foundation for Cancer Research, and Edward P. Evans Foundation grants to DTS. AV is supported by Edward P. Evans Foundation, National Institute of Health (R01HL150832, R01HL139487, R01CA275007), Leukemia and Lymphoma Society, Curis and a gift from the Jane and Myles P. Dempsey family. AP and JB are supported by Blood Cancer UK (grants 13042 and 19004). GC is supported by a training grant from NYSTEM. We acknowledge support of this research from The Einstein Training Program in Stem Cell Research from the Empire State Stem Cell Fund through New York State Department of Health Contract C34874GG. MS is supported by a National Institute of Health Research Training and Career Development Grant (F31HL132420).

Published
2022
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6. Stem cell mutations can be detected in myeloma patients years before onset of secondary leukemias

Author

Ashwin Sridharan, Carolina D. Schinke, George Georgiev, Mariana Da Silva Ferreira, Victor Thiruthuvanathan, Ian MacArthur, Tushar D. Bhagat, Gaurav S. Choudhary, Srinivas Aluri, Jiahao Chen, Kith Pradhan, Yu Xia, Maya Panjikaran, Gregory Sims, Chirag K. Bhagat, Ryan Bender, Lauryn Keeler, Armin Graber, Christoph Heuck, Frederick A. Fletcher, Daisy Alapat, Niels Weinhold, Sarah K. Johnson, Amittha Wickrema, Bart Barlogie, Gareth J. Morgan, Aditi Shastri, Ulrich Steidl, Britta Will, and Amit Verma

Subjects
Specialties of internal medicine, RC581-951
Abstract

Abstract: Therapy-related acute myeloid leukemia and myelodysplastic syndromes (t-AML/t-MDS) are secondary hematologic malignancies associated with poor prognosis, warranting insights into their predisposing conditions and cells of origin. We identified patients with myeloma who developed t-AML/t-MDS and analyzed their stem and progenitor cells collected years before the onset of secondary disease. We demonstrate that aberrant stem cells with high CD123 expression can be detected long before the onset of overt leukemia. Rigorous sorting, followed by targeted sequencing, resulted in ultradeep functional depth of sequencing and revealed preexisting mutant hematopoietic stem cell (HSC) clones, mainly harboring TP53 mutations, that became the dominant population at the time of leukemic presentation. Taken together, these data show that HSCs can act as reservoirs for leukemia-initiating cells many years before the onset of myeloid leukemia.

Published
2019
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7. Proteome-wide analysis of chaperone-mediated autophagy targeting motifs.

Author

Philipp Kirchner, Mathieu Bourdenx, Julio Madrigal-Matute, Simoni Tiano, Antonio Diaz, Boris A Bartholdy, Britta Will, and Ana Maria Cuervo

Subjects
Biology (General), QH301-705.5
Abstract

Chaperone-mediated autophagy (CMA) contributes to the lysosomal degradation of a selective subset of proteins. Selectivity lies in the chaperone heat shock cognate 71 kDa protein (HSC70) recognizing a pentapeptide motif (KFERQ-like motif) in the protein sequence essential for subsequent targeting and degradation of CMA substrates in lysosomes. Interest in CMA is growing due to its recently identified regulatory roles in metabolism, differentiation, cell cycle, and its malfunctioning in aging and conditions such as cancer, neurodegeneration, or diabetes. Identification of the subset of the proteome amenable to CMA degradation could further expand our understanding of the pathophysiological relevance of this form of autophagy. To that effect, we have performed an in silico screen for KFERQ-like motifs across proteomes of several species. We have found that KFERQ-like motifs are more frequently located in solvent-exposed regions of proteins, and that the position of acidic and hydrophobic residues in the motif plays the most important role in motif construction. Cross-species comparison of proteomes revealed higher motif conservation in CMA-proficient species. The tools developed in this work have also allowed us to analyze the enrichment of motif-containing proteins in biological processes on an unprecedented scale and discover a previously unknown association between the type and combination of KFERQ-like motifs in proteins and their participation in specific biological processes. To facilitate further analysis by the scientific community, we have developed a free web-based resource (KFERQ finder) for direct identification of KFERQ-like motifs in any protein sequence. This resource will contribute to accelerating understanding of the physiological relevance of CMA.

Published
2019
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8. A large gene network in immature erythroid cells is controlled by the myeloid and B cell transcriptional regulator PU.1.

Author

Sandeep N Wontakal, Xingyi Guo, Britta Will, Minyi Shi, Debasish Raha, Milind C Mahajan, Sherman Weissman, Michael Snyder, Ulrich Steidl, Deyou Zheng, and Arthur I Skoultchi

Subjects
Genetics, QH426-470
Abstract

PU.1 is a hematopoietic transcription factor that is required for the development of myeloid and B cells. PU.1 is also expressed in erythroid progenitors, where it blocks erythroid differentiation by binding to and inhibiting the main erythroid promoting factor, GATA-1. However, other mechanisms by which PU.1 affects the fate of erythroid progenitors have not been thoroughly explored. Here, we used ChIP-Seq analysis for PU.1 and gene expression profiling in erythroid cells to show that PU.1 regulates an extensive network of genes that constitute major pathways for controlling growth and survival of immature erythroid cells. By analyzing fetal liver erythroid progenitors from mice with low PU.1 expression, we also show that the earliest erythroid committed cells are dramatically reduced in vivo. Furthermore, we find that PU.1 also regulates many of the same genes and pathways in other blood cells, leading us to propose that PU.1 is a multifaceted factor with overlapping, as well as distinct, functions in several hematopoietic lineages.

Published
2011
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9. Lenalidomide and Eltrombopag for Treatment of Low- or Intermediate-Risk Myelodysplastic Syndrome: Result of a Phase II Clinical Trial

Author

Jesus D. Gonzalez-Lugo, Suman Kambhampati, Abdulraheem Yacoub, William B. Donnellan, Jesus Berdeja, Prafulla Bhagat, Karen Fehn, Cassady Remy, Sakshi Jasra, Mohammed Kazemi, Kith Pradhan, Mimi Kim, Ioannis Mantzaris, R. Alejandro Sica, Nishi Shah, Mendel Goldfinger, Noah Kornblum, Kira Gritsman, Ira Braunschweig, Ulrich Steidl, Britta Will, Aditi Shastri, and Amit Verma

Subjects
Cancer Research, Oncology
Abstract

Purpose: Thrombocytopenia is a serious complication of myelodysplastic syndromes (MDS) associated with an increased bleeding risk and worse prognosis. Eltrombopag (ELT), a thrombopoietin receptor agonist, can increase platelet counts and reverse anti-megakaryopoietic effects of lenalidomide (LEN) in preclinical studies. We hypothesized ELT would reduce the incidence of thrombocytopenia in MDS. Patients and Methods: We conducted a Phase II multicenter trial of ELT and LEN in adult patients with low- or intermediate-1–risk MDS with symptomatic or transfusion-dependent anemia or thrombocytopenia (NCT01772420). Thrombocytopenic patients were started on ELT and subsequently treated with LEN after platelets were increased. Patients without thrombocytopenia were started on LEN monotherapy and treated with ELT if they became thrombocytopenic. Results: Fifty-two patients were enrolled; mean age was 71 years (range 34–93). Overall response rate (ORR) in the intention-to-treat population was 35% (18/52). ELT monotherapy led to ORR of 33.3% (7/21), 29% achieving hematologic improvement (HI)-Platelets, and 24% bilineage responses. LEN monotherapy had 38% ORR (6/16) with all responders achieving HI-Erythroid. Fifteen patients received both ELT and LEN with ORR of 33.3%, 20% achieved HI-Erythroid, and 20% HI-Platelets with 13% bilineage responses. Median duration of response was 40 weeks for ELT (range 8–ongoing), 41 weeks (25–ongoing) for LEN, and 88 weeks (8.3–ongoing) for ELT/LEN. Non-hematologic grade 3–4 treatment-related adverse events were infrequent. Among patients on ELT, 2 had major bleeding events, 1 had a reversible increase in peripheral blasts, and 1 developed marrow fibrosis after 6 years on ELT. Conclusions: ELT and LEN are well tolerated and effective in achieving hematologic improvement in patients with low-/intermediate-risk MDS.

Published
2022

10. The cost of competency?

Author

Yun-Ruei Kao and Britta Will

Subjects
General Biochemistry, Genetics and Molecular Biology
Published
2023

11. Supplementary Data from PU.1-Dependent Enhancer Inhibition Separates Tet2-Deficient Hematopoiesis from Malignant Transformation

Author

Britta Will, Amit Verma, Amittha Wickrema, Aaron D. Viny, Ross L. Levine, Chi Zhang, Aditi Paranjpe, Mario Pujato, Victor J. Thiruthuvanathan, Jong Jin Jeong, Aliona Zintiridou, Tushar D. Bhagat, Kith Pradhan, Boris A. Bartholdy, and Maria M. Aivalioti

Abstract

Supplementary Data from PU.1-Dependent Enhancer Inhibition Separates Tet2-Deficient Hematopoiesis from Malignant Transformation

Published
2023

12. Supplementary Figure from PU.1-Dependent Enhancer Inhibition Separates Tet2-Deficient Hematopoiesis from Malignant Transformation

Author

Britta Will, Amit Verma, Amittha Wickrema, Aaron D. Viny, Ross L. Levine, Chi Zhang, Aditi Paranjpe, Mario Pujato, Victor J. Thiruthuvanathan, Jong Jin Jeong, Aliona Zintiridou, Tushar D. Bhagat, Kith Pradhan, Boris A. Bartholdy, and Maria M. Aivalioti

Abstract

Supplementary Figure from PU.1-Dependent Enhancer Inhibition Separates Tet2-Deficient Hematopoiesis from Malignant Transformation

Published
2023

13. Data from PU.1-Dependent Enhancer Inhibition Separates Tet2-Deficient Hematopoiesis from Malignant Transformation

Author

Britta Will, Amit Verma, Amittha Wickrema, Aaron D. Viny, Ross L. Levine, Chi Zhang, Aditi Paranjpe, Mario Pujato, Victor J. Thiruthuvanathan, Jong Jin Jeong, Aliona Zintiridou, Tushar D. Bhagat, Kith Pradhan, Boris A. Bartholdy, and Maria M. Aivalioti

Abstract

Cytosine hypermethylation in and around DNA-binding sites of master transcription factors, including PU.1, occurs in aging hematopoietic stem cells following acquired loss-of-function mutations of DNA methyl-cytosine dioxygenase ten–eleven translocation-2 (TET2), albeit functional relevance has been unclear. We show that Tet2-deficient mouse hematopoietic stem and progenitor cells undergo malignant transformation upon compromised gene regulation through heterozygous deletion of an upstream regulatory region (UREΔ/WT) of the PU.1 gene. Although compatible with multilineage blood formation at young age, Tet2-deficient PU.1 UREΔ/WT mice develop highly penetrant, transplantable acute myeloid leukemia (AML) during aging. Leukemic stem and progenitor cells show hypermethylation at putative PU.1-binding sites, fail to activate myeloid enhancers, and are hallmarked by a signature of genes with impaired expression shared with human AML. Our study demonstrates that Tet2 and PU.1 jointly suppress leukemogenesis and uncovers a methylation-sensitive PU.1-dependent gene network as a unifying molecular vulnerability associated with AML.Significance:We identify moderately impaired PU.1 mRNA expression as a biological modality predisposing Tet2-deficient hematopoietic stem and progenitor cells to malignant transformation. Our study furthermore uncovers a methylation-sensitive PU.1 gene network as a common feature of myeloid leukemia potentially allowing for the identification of patients at risk for malignant transformation.See related commentary by Schleicher and Pietras, p. 378.This article is highlighted in the In This Issue feature, p. 369

Published
2023

14. Supplementary Figures S1-S2 from Lenalidomide and Eltrombopag for Treatment of Low- or Intermediate-Risk Myelodysplastic Syndrome: Result of a Phase II Clinical Trial

Author

Amit Verma, Aditi Shastri, Britta Will, Ulrich Steidl, Ira Braunschweig, Kira Gritsman, Noah Kornblum, Mendel Goldfinger, Nishi Shah, R. Alejandro Sica, Ioannis Mantzaris, Mimi Kim, Kith Pradhan, Mohammed Kazemi, Sakshi Jasra, Cassady Remy, Karen Fehn, Prafulla Bhagat, Jesus Berdeja, William B. Donnellan, Abdulraheem Yacoub, Suman Kambhampati, and Jesus D. Gonzalez-Lugo

Abstract

Supplemental Figure 1. Overall Survival Responders vs Non-Responders Supplemental Figure 2. Overall Survival Among Groups

Published
2023

15. Data from Lenalidomide and Eltrombopag for Treatment of Low- or Intermediate-Risk Myelodysplastic Syndrome: Result of a Phase II Clinical Trial

Author

Amit Verma, Aditi Shastri, Britta Will, Ulrich Steidl, Ira Braunschweig, Kira Gritsman, Noah Kornblum, Mendel Goldfinger, Nishi Shah, R. Alejandro Sica, Ioannis Mantzaris, Mimi Kim, Kith Pradhan, Mohammed Kazemi, Sakshi Jasra, Cassady Remy, Karen Fehn, Prafulla Bhagat, Jesus Berdeja, William B. Donnellan, Abdulraheem Yacoub, Suman Kambhampati, and Jesus D. Gonzalez-Lugo

Abstract

Purpose:Thrombocytopenia is a serious complication of myelodysplastic syndromes (MDS) associated with an increased bleeding risk and worse prognosis. Eltrombopag (ELT), a thrombopoietin receptor agonist, can increase platelet counts and reverse anti-megakaryopoietic effects of lenalidomide (LEN) in preclinical studies. We hypothesized ELT would reduce the incidence of thrombocytopenia in MDS.Patients and Methods:We conducted a Phase II multicenter trial of ELT and LEN in adult patients with low- or intermediate-1–risk MDS with symptomatic or transfusion-dependent anemia or thrombocytopenia (NCT01772420). Thrombocytopenic patients were started on ELT and subsequently treated with LEN after platelets were increased. Patients without thrombocytopenia were started on LEN monotherapy and treated with ELT if they became thrombocytopenic.Results:Fifty-two patients were enrolled; mean age was 71 years (range 34–93). Overall response rate (ORR) in the intention-to-treat population was 35% (18/52). ELT monotherapy led to ORR of 33.3% (7/21), 29% achieving hematologic improvement (HI)-Platelets, and 24% bilineage responses. LEN monotherapy had 38% ORR (6/16) with all responders achieving HI-Erythroid. Fifteen patients received both ELT and LEN with ORR of 33.3%, 20% achieved HI-Erythroid, and 20% HI-Platelets with 13% bilineage responses. Median duration of response was 40 weeks for ELT (range 8–ongoing), 41 weeks (25–ongoing) for LEN, and 88 weeks (8.3–ongoing) for ELT/LEN. Non-hematologic grade 3–4 treatment-related adverse events were infrequent. Among patients on ELT, 2 had major bleeding events, 1 had a reversible increase in peripheral blasts, and 1 developed marrow fibrosis after 6 years on ELT.Conclusions:ELT and LEN are well tolerated and effective in achieving hematologic improvement in patients with low-/intermediate-risk MDS.

Published
2023

16. Supp tables 1-5 from Epigenetically Aberrant Stroma in MDS Propagates Disease via Wnt/β-Catenin Activation

Author

Amit Verma, Michael G. Kharas, H. Joachim Deeg, Marc H.G.P. Raaijmakers, Ulrich Steidl, Britta Will, Jacqueline Boultwood, Andrea Pellagatti, Siddhartha Mukherjee, John M. Greally, Jinghang Zhang, Kith Pradhan, Yiting Yu, Konrad Hochedlinger, Peter Aplan, Kira Gritsman, Cecilia Yeung, Amittha Wickrema, Davendra Sohal, Orsi Giricz, Prafulla Bhagat, Robert Lopez, Remi Laurence, Vineeth Sukrithan, Iaonnis Mantzaris, Nandini Ramachandra, Suman Kambhampati, Remco M. Hoogenboezem, Mathijs A. Sanders, A. Mario Marcondes, Elianna Amin, Patrick Tivnan, Gaurav S. Choudhary, Dagny Von Ahrens, A. Trevor Barlowe, Matthias Bartenstein, Si Chen, and Tushar D. Bhagat

Abstract

Supp Table 1: MDS Patient Disease Characteristics Supp Table 2: Pathways affected by hypermethylation in MDS stroma Supp Table 3: Genes that are methylated and underexpressed in MDS stroma Supp Table 4. MDS patient characteristics for primary MSC sample isolation Supp table 5: WNT Targets

Published
2023

17. Supp Methods from Epigenetically Aberrant Stroma in MDS Propagates Disease via Wnt/β-Catenin Activation

Author

Amit Verma, Michael G. Kharas, H. Joachim Deeg, Marc H.G.P. Raaijmakers, Ulrich Steidl, Britta Will, Jacqueline Boultwood, Andrea Pellagatti, Siddhartha Mukherjee, John M. Greally, Jinghang Zhang, Kith Pradhan, Yiting Yu, Konrad Hochedlinger, Peter Aplan, Kira Gritsman, Cecilia Yeung, Amittha Wickrema, Davendra Sohal, Orsi Giricz, Prafulla Bhagat, Robert Lopez, Remi Laurence, Vineeth Sukrithan, Iaonnis Mantzaris, Nandini Ramachandra, Suman Kambhampati, Remco M. Hoogenboezem, Mathijs A. Sanders, A. Mario Marcondes, Elianna Amin, Patrick Tivnan, Gaurav S. Choudhary, Dagny Von Ahrens, A. Trevor Barlowe, Matthias Bartenstein, Si Chen, and Tushar D. Bhagat

Abstract

Supplementary Methods

Published
2023

18. Data from Phase II Study of the ALK5 Inhibitor Galunisertib in Very Low-, Low-, and Intermediate-Risk Myelodysplastic Syndromes

Author

Amit Verma, Britta Will, Ashwin Sridharan, Ulrich Steidl, Kith Pradhan, Tushar D. Bhagat, Mariana da Silva Ferreira, Allicia C. Girvan, Ivelina Gueorguieva, Susan C. Guba, Aristoteles Giagounidis, Alan Chiang, Yumin Zhao, Jan Janssen, Michael M. Lahn, Ann L. Cleverly, Rami S. Komrokji, Uwe Platzbecker, David Valcárcel, and Valeria Santini

Abstract

Purpose:Overactivation of TGF-β signaling is observed in myelodysplastic syndromes (MDS) and is associated with dysplastic hematopoietic differentiation. Galunisertib, a first-in-class oral inhibitor of the TGF-β receptor type 1 kinase (ALK5) has shown effectiveness in preclinical models of MDS and acceptable toxicity in phase I studies of solid malignancies.Patients and Methods:A phase II multicenter study of galunisertib was conducted in patients with very low-, low-, or intermediate-risk MDS by the Revised International Prognostic Scoring System criteria with hemoglobin ≤ 10.0 g/dL. Patients received oral galunisertib 150 mg twice daily for 14 days on/14 days off.Results:Ten of 41 evaluable patients (24.4%; 95% confidence interval, 12.4–40.3) achieved hematologic improvement erythroid response by International Working Group (IWG) 2006 criteria. A total of 18 of 41 patients (43.9%) achieved erythroid response as per IWG 2000 criteria. Nine of 28 (32.1%) of transfusion-dependent patients had hematologic improvement. A total of 18 of 41 (44%) patients had a significant reduction in fatigue. Overall median duration of response was 90 days in all patients. Rigorous stem and progenitor flow cytometry showed that patients with an early stem cell differentiation block were more likely to respond to galunisertib. The most common treatment-emergent adverse events were grade 1 or 2 in 20 (49%) of 41 patients, including any-grade fatigue (8/41, 20%), diarrhea (7/41, 17%), pyrexia (5/41, 12%), and vomiting (5/41, 12%).Conclusions:In summary, galunisertib treatment has an acceptable safety profile and was associated with hematologic improvements in lower- and intermediate-risk MDS, with responses in heavily transfusion-dependent patients and in those with signs of an early stem cell differentiation block.

Published
2023

19. Data from Epigenetically Aberrant Stroma in MDS Propagates Disease via Wnt/β-Catenin Activation

Author

Amit Verma, Michael G. Kharas, H. Joachim Deeg, Marc H.G.P. Raaijmakers, Ulrich Steidl, Britta Will, Jacqueline Boultwood, Andrea Pellagatti, Siddhartha Mukherjee, John M. Greally, Jinghang Zhang, Kith Pradhan, Yiting Yu, Konrad Hochedlinger, Peter Aplan, Kira Gritsman, Cecilia Yeung, Amittha Wickrema, Davendra Sohal, Orsi Giricz, Prafulla Bhagat, Robert Lopez, Remi Laurence, Vineeth Sukrithan, Iaonnis Mantzaris, Nandini Ramachandra, Suman Kambhampati, Remco M. Hoogenboezem, Mathijs A. Sanders, A. Mario Marcondes, Elianna Amin, Patrick Tivnan, Gaurav S. Choudhary, Dagny Von Ahrens, A. Trevor Barlowe, Matthias Bartenstein, Si Chen, and Tushar D. Bhagat

Abstract

The bone marrow microenvironment influences malignant hematopoiesis, but how it promotes leukemogenesis has not been elucidated. In addition, the role of the bone marrow stroma in regulating clinical responses to DNA methyltransferase inhibitors (DNMTi) is also poorly understood. In this study, we conducted a DNA methylome analysis of bone marrow–derived stromal cells from myelodysplastic syndrome (MDS) patients and observed widespread aberrant cytosine hypermethylation occurring preferentially outside CpG islands. Stroma derived from 5-azacytidine–treated patients lacked aberrant methylation and DNMTi treatment of primary MDS stroma enhanced its ability to support erythroid differentiation. An integrative expression analysis revealed that the WNT pathway antagonist FRZB was aberrantly hypermethylated and underexpressed in MDS stroma. This result was confirmed in an independent set of sorted, primary MDS-derived mesenchymal cells. We documented a WNT/β-catenin activation signature in CD34+ cells from advanced cases of MDS, where it associated with adverse prognosis. Constitutive activation of β-catenin in hematopoietic cells yielded lethal myeloid disease in a NUP98–HOXD13 mouse model of MDS, confirming its role in disease progression. Our results define novel epigenetic changes in the bone marrow microenvironment, which lead to β-catenin activation and disease progression of MDS. Cancer Res; 77(18); 4846–57. ©2017 AACR.

Published
2023

20. Supp Figs 1-5 from Epigenetically Aberrant Stroma in MDS Propagates Disease via Wnt/β-Catenin Activation

Author

Amit Verma, Michael G. Kharas, H. Joachim Deeg, Marc H.G.P. Raaijmakers, Ulrich Steidl, Britta Will, Jacqueline Boultwood, Andrea Pellagatti, Siddhartha Mukherjee, John M. Greally, Jinghang Zhang, Kith Pradhan, Yiting Yu, Konrad Hochedlinger, Peter Aplan, Kira Gritsman, Cecilia Yeung, Amittha Wickrema, Davendra Sohal, Orsi Giricz, Prafulla Bhagat, Robert Lopez, Remi Laurence, Vineeth Sukrithan, Iaonnis Mantzaris, Nandini Ramachandra, Suman Kambhampati, Remco M. Hoogenboezem, Mathijs A. Sanders, A. Mario Marcondes, Elianna Amin, Patrick Tivnan, Gaurav S. Choudhary, Dagny Von Ahrens, A. Trevor Barlowe, Matthias Bartenstein, Si Chen, and Tushar D. Bhagat

Abstract

Supp Fig 1 : SFRP1 methylation with coculture Supp Fig 2 : Validation of methylation changes with stroma and leukemic cell coculture Supp Fig 3: FRZB upregulation in MDS stroma after 5-Azacytidine treatment SuppFig 4: FRZB knockdown leads to partial inhibition of erythroid differentiation induced by treatment of MDS stromawith 5-Aza SuppFig 5: The expression of WNT signature genes in MDS and control marrow derived CD34+ cells

Published
2023

21. Supplementary Tables and Figures from Phase II Study of the ALK5 Inhibitor Galunisertib in Very Low-, Low-, and Intermediate-Risk Myelodysplastic Syndromes

Author

Amit Verma, Britta Will, Ashwin Sridharan, Ulrich Steidl, Kith Pradhan, Tushar D. Bhagat, Mariana da Silva Ferreira, Allicia C. Girvan, Ivelina Gueorguieva, Susan C. Guba, Aristoteles Giagounidis, Alan Chiang, Yumin Zhao, Jan Janssen, Michael M. Lahn, Ann L. Cleverly, Rami S. Komrokji, Uwe Platzbecker, David Valcárcel, and Valeria Santini

Abstract

Supp Tables and Figs

Published
2023

22. Supplementary Figures 1-4 from Methylome Profiling Reveals Distinct Alterations in Phenotypic and Mutational Subgroups of Myeloproliferative Neoplasms

Author

Amit Verma, Alison Moliterno, Ulrich Steidl, John M. Greally, Ari M. Melnick, Jaroslaw P. Maciejewski, Michael McDevitt, Animesh Pardanani, Masako Suzuki, Yongkai Mo, Britta Will, Davendra Sohal, Tushar D. Bhagat, Li Zhou, Yiting Yu, Maximilian Christopeit, Sanchari Bhattacharyya, and Sangeeta Nischal

Abstract

PDF file - 646K, Supp Fig 1: Pathways involved by hypermethylated genes in PV / ET. Supp Fig 2: Validation of HELP assay findings by MassArray bisulfite analysis Supp Fig 3: Pathways involved by genes that are overexpressed and hypomethylated at promoters by the Jak2V617F mutant. Supp Fig 4: Jak2V617F mutation does not have significant effects on global DNA methylation profiles

Published
2023

23. Supplementary Tables 1-7 from Methylome Profiling Reveals Distinct Alterations in Phenotypic and Mutational Subgroups of Myeloproliferative Neoplasms

Author

Amit Verma, Alison Moliterno, Ulrich Steidl, John M. Greally, Ari M. Melnick, Jaroslaw P. Maciejewski, Michael McDevitt, Animesh Pardanani, Masako Suzuki, Yongkai Mo, Britta Will, Davendra Sohal, Tushar D. Bhagat, Li Zhou, Yiting Yu, Maximilian Christopeit, Sanchari Bhattacharyya, and Sangeeta Nischal

Abstract

PDF file - 846K, Supplementary Table 1: Genes hypermethylated in PV / ET Supplementary Table 2: Genes hypermethylated in PMF Supplementary Table 3: Genes hypomethylated in PMF Supplementary Table 4: Genes hypermethylated in PMF cases with ASXL1 mutations / deletions Supp Table 5: Biological pathways affected by hypermethylated genes in ASXL1 mutated/deleted cases of PMF Supplementary Table 6: Genes hypermethylated in MPN cases with TET2 mutations Supp Table 7: Biological pathways affected by hypermethylated genes in TET2 mutated cases of MPNs

Published
2023

24. Asxl1 loss cooperates with oncogenic Nras in mice to reprogram the immune microenvironment and drive leukemic transformation

Author

Ross L. Levine, Jing Zhang, Fabao Liu, Alexis Vedder, Xin Gao, Sergey Nikolaev, Mrinal M. Patnaik, Abhishek A. Mangaonkar, Yun Zhou, Kalyan Vara Ganesh Nadiminti, Anthony M. Hunter, Terra L. Lasho, Wei Xu, Evan Flietner, Erik A. Ranheim, Xiaona You, Ruiqi Liao, Klaus Geissler, Eric Padron, Nathalie Droin, Guangyao Kong, Moritz Binder, Eric Solary, Maria E. Balasis, Christy Finke, Britta Will, Omar Abdel-Wahab, Adhithi Rajagopalan, Zhi Wen, and David T. Yang

Subjects
Neuroblastoma RAS viral oncogene homolog, Myeloid, T cell, Immunology, Biology, Biochemistry, GTP Phosphohydrolases, Mice, TIGIT, hemic and lymphatic diseases, Tumor Microenvironment, medicine, Animals, Humans, Monomeric GTP-Binding Proteins, Myeloid Neoplasia, Membrane Proteins, Myeloid leukemia, Leukemia, Myelomonocytic, Chronic, Cell Biology, Hematology, medicine.disease, Immune checkpoint, Repressor Proteins, Disease Models, Animal, Leukemia, Myeloid, Acute, Leukemia, Phenotype, medicine.anatomical_structure, Mutation, Cancer research, CD80, Signal Transduction
Abstract

Mutations in chromatin regulator ASXL1 are frequently identified in myeloid malignancies, in particular ∼40% of patients with chronic myelomonocytic leukemia (CMML). ASXL1 mutations are associated with poor prognosis in CMML and significantly co-occur with NRAS mutations. Here, we show that concurrent ASXL1 and NRAS mutations defined a population of CMML patients who had shorter leukemia-free survival than those with ASXL1 mutation only. Corroborating this human data, Asxl1−/− accelerated CMML progression and promoted CMML transformation to acute myeloid leukemia (AML) in NrasG12D/+ mice. NrasG12D/+;Asxl1−/− (NA) leukemia cells displayed hyperactivation of MEK/ERK signaling, increased global levels of H3K27ac, upregulation of Flt3. Moreover, we find that NA-AML cells overexpressed all the major inhibitory immune checkpoint ligands: programmed death-ligand 1 (PD-L1)/PD-L2, CD155, and CD80/CD86. Among them, overexpression of PD-L1 and CD86 correlated with upregulation of AP-1 transcription factors (TFs) in NA-AML cells. An AP-1 inhibitor or short hairpin RNAs against AP-1 TF Jun decreased PD-L1 and CD86 expression in NA-AML cells. Once NA-AML cells were transplanted into syngeneic recipients, NA-derived T cells were not detectable. Host-derived wild-type T cells overexpressed programmed cell death protein 1 (PD-1) and T-cell immunoreceptor with immunoglobulin and ITIM domains (TIGIT) receptors, leading to a predominant exhausted T-cell phenotype. Combined inhibition of MEK and BET resulted in downregulation of Flt3 and AP-1 expression, partial restoration of the immune microenvironment, enhancement of CD8 T-cell cytotoxicity, and prolonged survival in NA-AML mice. Our study suggests that combined targeted therapy and immunotherapy may be beneficial for treating secondary AML with concurrent ASXL1 and NRAS mutations.

Published
2022

25. Glutaminase inhibition in combination with azacytidine in myelodysplastic syndromes: Clinical efficacy and correlative analyses

Author

Marina Konopleva, Courtney DiNardo, Tushar Bhagat, Natalia Baran, Alessia Lodi, Kapil Saxena, Tianyu Cai, Xiaoping Su, Anna Skwarska, Veronica Guerra, Vinitha Kuruvilla, Sergej Konoplev, Shanisha Gordon-Mitchell, Kith Pradhan, Srinivas Aluri, Meghan Collins, Shannon Sweeney, Jonathan Busquet, Atul Rathore, Qing Deng, Michael Green, Steven Grant, Susan Demo, Gaurav Choudhary, Srabani Sahu, Beamon Agarwal, Mason Spodek, Victor Thiruthuvanathan, Britta Will, Ulrich Steidl, George Tippett, Jan Burger, Gautam Borthakur, Elias Jabbour, Naveen Pemmaraju, Tapan Kadia, Steven Kornblau, Naval Daver, Kiran Naqvi, Nicholas Short, Guillermo Garcia-Manero, Stefano Tiziani, and Amit Verma

Abstract

Malignancies can become reliant on glutamine as an alternative energy source and as a facilitator of aberrant DNA methylation, thus implicating glutaminase (GLS) as a potential therapeutic target. We demonstrate preclinical synergy of telaglenastat (CB-839), a selective GLS inhibitor, when combined with azacytidine (AZA), in vitro and in vivo, followed by a phase Ib/II study of the combination in patients with advanced MDS. Treatment with telaglenastat/AZA led to an ORR of 70% with CR/mCRs in 53% patients and a median overall survival of 11.6 months. scRNAseq and flow cytometry demonstrated a myeloid differentiation program at the stem cell level in clinical responders. Expression of non-canonical glutamine transporter, SLC38A1, was found to be overexpressed in MDS stem cells; was associated with clinical responses to telaglenastat/AZA and predictive of worse prognosis in a large MDS cohort. These data demonstrate the safety and efficacy of a combined metabolic and epigenetic approach in MDS.

Published
2023

26. Lenalidomide and Eltrombopag for Treatment of Low or Intermediate Risk Myelodysplastic Syndrome: Result of a Phase 2 Clinical Trial

Author

Jesus D, Gonzalez-Lugo, Suman, Kambhampati, Abdulraheem, Yacoub, William B, Donnellan, Jesus, Berdeja, Prafulla, Bhagat, Karen, Fehn, Cassady, Remy, Sakshi, Jasra, Mohammed, Kazemi, Kith, Pradhan, Mimi, Kim, Ioannis, Mantzaris, R Alejandro, Sica, Nishi, Shah, Mendel, Goldfinger, Noah, Kornblum, Kira, Gritsman, Ira, Braunschweig, Ulrich, Steidl, Britta, Will, Aditi, Shastri, and Amit, Verma

Abstract

Thrombocytopenia is a serious complication of MDS associated with an increased bleeding risk and worse prognosis. Eltrombopag (ELT), a thrombopoietin receptor agonist, can increase platelet counts and reverse anti-megakaryopoietic effects of lenalidomide (LEN) in preclinical studies. We hypothesized ELT would reduce the incidence of thrombocytopenia in MDS.We conducted a phase 2 multicenter trial of ELT and LEN in adult patients with low or intermediate-1-risk MDS with symptomatic or transfusion-dependent anemia or thrombocytopenia (NCT01772420). Thrombocytopenic patients were started on ELT and subsequently treated with LEN after platelets were increased. Patients without thrombocytopenia were started on LEN monotherapy and treated with ELT if they became thrombocytopenic.52 patients were enrolled; mean age was 71 years (range 34-93). ORR in the ITT population was 35% (18/52). ELT monotherapy led to ORR of 33.3% (7/21), 29% achieving HI-Platelets, and 24% bilineage responses. LEN monotherapy had 38% ORR (6/16) with all responders achieving HI-Erythroid. 15 patients received both ELT and LEN with ORR of 33.3%, 20% achieved HI-Erythroid, and 20% HI-Platelets with 13% bilineage responses. Median duration of response was 40 weeks for ELT (range 8-ongoing), 41 weeks (25-ongoing) for LEN, and 88 weeks (8.3-ongoing) for ELT/LEN. Non-hematological grade 3-4 treatment-related adverse events were infrequent. Among patients on ELT, 2 had major bleeding events, 1 had a reversible increase in peripheral blasts, and 1 developed marrow fibrosis after 6 years on ELT.ELT and LEN are well tolerated and effective in achieving hematological improvement in patients with low/intermediate-risk MDS.

Published
2022

27. Megakaryopoiesis impairment through acute innate immune signaling activation by azacitidine

Author

Ujunwa Cynthia Okoye-Okafor, Komal K. Javarappa, Dimitrios Tsallos, Joseph Saad, Daozheng Yang, Chi Zhang, Lumie Benard, Victor J. Thiruthuvanathan, Sally Cole, Stephen Ruiz, Madhuri Tatiparthy, Gaurav Choudhary, Stefanie DeFronzo, Boris A. Bartholdy, Celine Pallaud, Pedro Marques Ramos, Aditi Shastri, Amit Verma, Caroline A. Heckman, Britta Will, Institute for Molecular Medicine Finland, University of Helsinki, and Helsinki Institute of Life Science HiLIFE

Subjects
Leukemia, Myeloid, Acute, Myelodysplastic Syndromes, Immunology, Azacitidine, Humans, 1182 Biochemistry, cell and molecular biology, Immunology and Allergy, 3111 Biomedicine, Thrombocytopenia, Immunity, Innate
Abstract

Publisher Copyright: © 2022 Okoye-Okafor et al. Thrombocytopenia, prevalent in the majority of patients with myeloid malignancies, such as myelodysplastic syndrome (MDS) or acute myeloid leukemia (AML), is an independent adverse prognostic factor. Azacitidine (AZA), a mainstay therapeutic agent for stem cell transplant–ineligible patients with MDS/AML, often transiently induces or further aggravates disease-associated thrombocytopenia by an unknown mechanism. Here, we uncover the critical role of an acute type-I interferon (IFN-I) signaling activation in suppressing megakaryopoiesis in AZA-mediated thrombocytopenia. We demonstrate that megakaryocytic lineage-primed progenitors present IFN-I receptors and, upon AZA exposure, engage STAT1/SOCS1-dependent downstream signaling prematurely attenuating thrombopoietin receptor (TPO-R) signaling and constraining megakaryocytic progenitor cell growth and differentiation following TPO-R stimulation. Our findings directly implicate RNA demethylation and IFN-I signal activation as a root cause for AZA-mediated thrombocytopenia and suggest mitigation of TPO-R inhibitory innate immune signaling as a suitable therapeutic strategy to support platelet production, particularly during the early phases of AZA therapy.

Published
2022

30. To Degrade or Not to Degrade DNMT3A

Author

Yuhong, Ma and Britta, Will

Subjects
Cytosine, Oncology, embryonic structures, DNA, DNA (Cytosine-5-)-Methyltransferases, DNA Methylation, Article, DNA Methyltransferase 3A
Abstract

Clonal hematopoiesis is a prevalent age-related condition associated with greatly increased risk of hematologic disease; mutations in DNA methyltransferase 3A (DNMT3A) are the most common driver of this state. DNMT3A variants occur across the gene with some particularly associated with malignancy, but the functional relevance and mechanisms of pathogenesis of the majority of mutations is unknown. Here, we systematically investigated the methyltransferase activity and protein stability of 253 disease-associated DNMT3A mutations, finding that 74% were loss-of-function mutations. Half of these variants exhibited reduced protein stability and, as a class, correlated with greater clonal expansion and AML development. We investigated the mechanisms underlying the instability using a CRISPR screen and uncovered regulated destruction of DNMT3A mediated by the DCAF8 E3 ubiquitin ligase adaptor. We establish a new paradigm to classify novel variants that has prognostic and potential therapeutic significance for patients with hematologic disease.

Published
2022

31. Author response: Activation of targetable inflammatory immune signaling is seen in myelodysplastic syndromes with SF3B1 mutations

Author

Andrea Pellagatti, Gaurav S Choudhary, Bogos Agianian, Molly A Smith, Tushar D Bhagat, Shanisha Gordon-Mitchell, Srabani Sahu, Sanjay Pandey, Nishi Shah, Srinivas Aluri, Ritesh Aggarwal, Sarah Aminov, Leya Schwartz, Violetta Steeples, Robert N Booher, Murali Ramachandra, Maria Samson, Milagros Carbajal, Kith Pradhan, Teresa V Bowman, Manoj M Pillai, Britta Will, Amittha Wickrema, Aditi Shastri, Robert K Bradley, Robert E Martell, Ulrich G Steidl, Evripidis Gavathiotis, Jacqueline Boultwood, Daniel T Starczynowski, and Amit Verma

Published
2022

32. Efficacy and longevity of immune response to 3rd COVID-19 vaccine and effectiveness of a 4th dose in severely immunocompromised patients with cancer

Author

Astha Thakkar, Kith Pradhan, Benjamin Duva, Juan Manuel Carreño, Srabani Sahu, Victor Thiruthuvanathan, Sean Campbell, Sonia Gallego, Tushar D Bhagat, Johanna Rivera, Gaurav Choudhary, Raul Olea, Maite Sabalza, Lauren C. Shapiro, Matthew Lee, Ryann Quinn, Ioannis Mantzaris, Edward Chu, Britta Will, Liise-anne Pirofski, Florian Krammer, Amit Verma, and Balazs Halmos

Abstract

Cancer patients show increased morbidity with COVID-19 and need effective immunization strategies. We demonstrate that a 3rd dose of COVID-19 vaccine leads to seroconversion in 57% of patients that were seronegative after primary vaccination. The immune response is durable as assessed by anti-S antibody titers, T-cell activity and neutralization activity against wild-type SARS-CoV2 and BA1.1.529 at 6 months of follow up. A subset of severely immunocompromised hematologic malignancy patients were unable to mount adequate immune response after the 3rd dose and were treated with a 4th dose in a prospective clinical trial which led to adequate immune-boost in 67% of patients. Low baseline IgM levels and CD19 counts were associated with inadequate seroconversion. Booster doses induced limited neutralization activity against the Omicron variant. These results indicate that vaccine booster-induced immunity is durable in cancer patients and additional doses can further stimulate immunity in a subset of hematologic malignancy patients.Statement of significanceWe demonstrate that a 3rd dose of vaccine leads to seroconversion in 57% of negative patients with durable immune responses at 6 months. A 4th dose of vaccine can seroconvert hematologic malignancy patients with higher baseline IgM and CD19 levels.

Published
2022

33. Chaperone-mediated autophagy sustains hematopoietic stem cell function

Author

Victor Thiruthuvanathan, Susmita Kaushik, Edward Nieves, Yun Ruei Kao, Julie A. Reisz, Qian Wang, Britta Will, Ana Maria Cuervo, Angelo D'Alessandro, Shuxian Dong, Inmaculada Tasset, Evripidis Gavathiotis, Aliona Zintiridou, Monika Dzieciatkowska, and Antonio Diaz

Subjects
Adult, Male, 0301 basic medicine, Aging, autophagy, Cell, Chaperone-Mediated Autophagy, Biology, Article, Linoleic Acid, Mice, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Chaperone-mediated autophagy, lysosomes, Downregulation and upregulation, stem cells, lipid metabolism, medicine, Animals, Humans, Rejuvenation, chaperones, protein quality control, Cell Self Renewal, Cells, Cultured, health care economics and organizations, Aged, Multidisciplinary, Autophagy, Middle Aged, Hematopoietic Stem Cells, Research Highlight, humanities, Cell biology, Transplantation, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, protein degradation, Female, Stem cell, Energy Metabolism, Multiple Myeloma, Glycolysis, 030217 neurology & neurosurgery, Function (biology)
Abstract

The activation of mostly quiescent haematopoietic stem cells (HSCs) is a prerequisite for life-long production of blood cells1. This process requires major molecular adaptations to allow HSCs to meet the regulatory and metabolic requirements for cell division2-4. The mechanisms that govern cellular reprograming upon stem-cell activation, and the subsequent return of stem cells to quiescence, have not been fully characterized. Here we show that chaperone-mediated autophagy (CMA)5, a selective form of lysosomal protein degradation, is involved in sustaining HSC function in adult mice. CMA is required for protein quality control in stem cells and for the upregulation of fatty acid metabolism upon HSC activation. We find that CMA activity in HSCs decreases with age and show that genetic or pharmacological activation of CMA can restore the functionality of old mouse and human HSCs. Together, our findings provide mechanistic insights into a role for CMA in sustaining quality control, appropriate energetics and overall long-term HSC function. Our work suggests that CMA may be a promising therapeutic target for enhancing HSC function in conditions such as ageing or stem-cell transplantation.

Published
2021

35. Blocking UBE2N abrogates oncogenic immune signaling in acute myeloid leukemia

Author

Laura Barreyro, Avery M. Sampson, Chiharu Ishikawa, Kathleen M. Hueneman, Kwangmin Choi, Mario A. Pujato, Somchai Chutipongtanate, Michael Wyder, Wendy D. Haffey, Eric O’Brien, Mark Wunderlich, Vighnesh Ramesh, Ellen M. Kolb, Cem Meydan, Yaseswini Neelamraju, Lyndsey C. Bolanos, Susanne Christie, Molly A. Smith, Madeline Niederkorn, Tomoya Muto, Santosh Kesari, Francine E. Garrett-Bakelman, Boris Bartholdy, Britta Will, Matthew T. Weirauch, James C. Mulloy, Zartash Gul, Stephen Medlin, Rhett A. Kovall, Ari M. Melnick, John P. Perentesis, Kenneth D. Greis, Elmar Nurmemmedov, William L. Seibel, and Daniel T. Starczynowski

Subjects
Leukemia, Myeloid, Acute, Ubiquitin-Conjugating Enzymes, Humans, Oncogenes, General Medicine, Cell Proliferation, Signal Transduction
Abstract

Dysregulation of innate immune signaling pathways is implicated in various hematologic malignancies. However, these pathways have not been systematically examined in acute myeloid leukemia (AML). We report that AML hematopoietic stem and progenitor cells (HSPCs) exhibit a high frequency of dysregulated innate immune-related and inflammatory pathways, referred to as oncogenic immune signaling states. Through gene expression analyses and functional studies in human AML cell lines and patient-derived samples, we found that the ubiquitin-conjugating enzyme UBE2N is required for leukemic cell function in vitro and in vivo by maintaining oncogenic immune signaling states. It is known that the enzyme function of UBE2N can be inhibited by interfering with thioester formation between ubiquitin and the active site. We performed in silico structure-based and cellular-based screens and identified two related small-molecule inhibitors UC-764864/65 that targeted UBE2N at its active site. Using these small-molecule inhibitors as chemical probes, we further revealed the therapeutic efficacy of interfering with UBE2N function. This resulted in the blocking of ubiquitination of innate immune- and inflammatory-related substrates in human AML cell lines. Inhibition of UBE2N function disrupted oncogenic immune signaling by promoting cell death of leukemic HSPCs while sparing normal HSPCs in vitro. Moreover, baseline oncogenic immune signaling states in leukemic cells derived from discrete subsets of patients with AML exhibited a selective dependency on UBE2N function in vitro and in vivo. Our study reveals that interfering with UBE2N abrogates leukemic HSPC function and underscores the dependency of AML cells on UBE2N-dependent oncogenic immune signaling states.

Published
2022

37. Stem cell mutations can be detected in myeloma patients years before onset of secondary leukemias

Author

Bart Barlogie, Tushar D. Bhagat, Armin Graber, Ryan Bender, Gaurav Choudhary, Frederick A. Fletcher, Maya Panjikaran, Victor Thiruthuvanathan, Daisy Alapat, Lauryn Keeler, Sarah K. Johnson, Ulrich Steidl, Chirag K Bhagat, Amittha Wickrema, Christoph Heuck, Jiahao Chen, George I. Georgiev, Ian C. MacArthur, Carolina Schinke, Aditi Shastri, Britta Will, Srinivas Aluri, Ashwin Sridharan, Gregory Sims, Niels Weinhold, Mariana da Silva Ferreira, Yu Xia, Amit Verma, Gareth J. Morgan, and Kith Pradhan

Subjects
0301 basic medicine, Myeloid, Hematopoiesis and Stem Cells, 03 medical and health sciences, 0302 clinical medicine, hemic and lymphatic diseases, Humans, Medicine, Progenitor cell, Multiple myeloma, business.industry, Myelodysplastic syndromes, Myeloid leukemia, Hematopoietic stem cell, Neoplasms, Second Primary, Hematology, Hematopoietic Stem Cells, medicine.disease, Leukemia, Myeloid, Acute, Leukemia, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Mutation, Cancer research, Stem cell, Multiple Myeloma, business
Abstract

Therapy-related acute myeloid leukemia and myelodysplastic syndromes (t-AML/t-MDS) are secondary hematologic malignancies associated with poor prognosis, warranting insights into their predisposing conditions and cells of origin. We identified patients with myeloma who developed t-AML/t-MDS and analyzed their stem and progenitor cells collected years before the onset of secondary disease. We demonstrate that aberrant stem cells with high CD123 expression can be detected long before the onset of overt leukemia. Rigorous sorting, followed by targeted sequencing, resulted in ultradeep functional depth of sequencing and revealed preexisting mutant hematopoietic stem cell (HSC) clones, mainly harboring TP53 mutations, that became the dominant population at the time of leukemic presentation. Taken together, these data show that HSCs can act as reservoirs for leukemia-initiating cells many years before the onset of myeloid leukemia.

Published
2019

38. PU.1-Dependent Enhancer Inhibition Separates Tet2-Deficient Hematopoiesis from Malignant Transformation

Author

Maria M. Aivalioti, Boris A. Bartholdy, Kith Pradhan, Tushar D. Bhagat, Aliona Zintiridou, Jong Jin Jeong, Victor J. Thiruthuvanathan, Mario Pujato, Aditi Paranjpe, Chi Zhang, Ross L. Levine, Aaron D. Viny, Amittha Wickrema, Amit Verma, and Britta Will

Subjects
General Medicine, In the Spotlight, Dioxygenases, Hematopoiesis, DNA-Binding Proteins, Cytosine, Leukemia, Myeloid, Acute, Mice, Cell Transformation, Neoplastic, Enhancer Elements, Genetic, Proto-Oncogene Proteins, Trans-Activators, Animals, Humans
Abstract

Cytosine hypermethylation in and around DNA-binding sites of master transcription factors, including PU.1, occurs in aging hematopoietic stem cells following acquired loss-of-function mutations of DNA methyl-cytosine dioxygenase ten–eleven translocation-2 (TET2), albeit functional relevance has been unclear. We show that Tet2-deficient mouse hematopoietic stem and progenitor cells undergo malignant transformation upon compromised gene regulation through heterozygous deletion of an upstream regulatory region (UREΔ/WT) of the PU.1 gene. Although compatible with multilineage blood formation at young age, Tet2-deficient PU.1 UREΔ/WT mice develop highly penetrant, transplantable acute myeloid leukemia (AML) during aging. Leukemic stem and progenitor cells show hypermethylation at putative PU.1-binding sites, fail to activate myeloid enhancers, and are hallmarked by a signature of genes with impaired expression shared with human AML. Our study demonstrates that Tet2 and PU.1 jointly suppress leukemogenesis and uncovers a methylation-sensitive PU.1-dependent gene network as a unifying molecular vulnerability associated with AML. Significance: We identify moderately impaired PU.1 mRNA expression as a biological modality predisposing Tet2-deficient hematopoietic stem and progenitor cells to malignant transformation. Our study furthermore uncovers a methylation-sensitive PU.1 gene network as a common feature of myeloid leukemia potentially allowing for the identification of patients at risk for malignant transformation. See related commentary by Schleicher and Pietras, p. 378. This article is highlighted in the In This Issue feature, p. 369

Published
2021

39. Cytoplasmic labile iron accumulates in aging stem cells perturbing a key rheostat for identity control

Author

Victor Thiruthuvanathan, Madhuri Tatiparthy, Simone Sidoli, Ulrich Steidl, Yun-Ruei Kao, Maria M. Aivalioti, Angelo D'Alessandro, Julie A. Reisz, Aliona Zintiridou, Rajni Kumari, Yuhong Ma, Jiahao Chen, Britta Will, and Stephanie Stransky

Subjects
Regulation of gene expression, Cell division, biology, Chemistry, Immunology, Identity (social science), Cell Biology, Hematology, Biochemistry, Cell biology, Haematopoiesis, Histone, Cytoplasm, Key (cryptography), biology.protein, Stem cell, Control (linguistics), Mitosis, Intracellular, Adult stem cell
Abstract

Bone marrow resident and rarely dividing hematopoietic stem cells (HSC) harbor an extensive self-renewal capacity to sustain life-long blood formation, albeit their function declines during ageing. Various molecular mechanisms confer stem cell identity, ensure long-term maintenance and are known to be deregulated in aged stem cells. How these programs are coordinated, particularly during cell division, and what triggers their ageing-associated dysfunction has been unknown. We have previously uncovered that iron chelator exposure increases the number of functional HSC ex vivo and in vivo (Kao et al., Science Transl Med 2018). While ensuring a sufficient amount of redox active, readily available iron which is required in numerous electron transfer reactions governing fundamental cellular processes, cells tightly regulate the size of the intracellular labile iron pool (LIP) to limit adverse ROS generation. Perturbations in the ability to limit intracellular iron is detrimental for cells and known to compromise HSC maintenance and function via altered redox signaling and increased macromolecule oxidation and damage. The HSC stimulatory effects of iron chelator (IC) treatment and the well characterized central roles of redox active intracellular iron in sustaining basic cell function prompted us to examine a potential regulatory role of the LIP in controlling somatic stem cell function. In this study, we quantified LIP in young and aged HSC and monitored iron homoeostasis pathway activation, hallmarked by the stabilization of transferrin receptor (Tfrc) mRNA, in stem cells for which we developed a single molecule RNA fluorescence in situ hybridization (smRNA FISH) assay enabling the quantification of Tfrc dynamics with unparalleled resolution and sensitivity. We have further used experimental LIP modulation in primary hematopoietic stem cell models to characterize the consequences of iron homeostasis pathway activation in young and aged stem cells; and employed integrated comparative quantitative transcriptomics (single cell RNA-seq) and proteomics along with genetic and pharmacological rescue models to identify the consequences and mechanisms of LIP size alterations. Our findings demonstrate that HSC, containing the lowest amount of cytoplasmic chelatable iron hematopoietic cells, activate a limited iron response during mitosis. Engagement of this iron homeostasis pathway elicits mobilization and β-oxidation of arachidonic acid and enhances stem cell-defining transcriptional programs governed by histone acetyl transferase Tip60/KAT5. We further find an age-associated expansion of the labile iron pool, along with loss of Tip60/KAT5-dependent gene regulation to contribute to the functional decline of ageing HSC, which can be mitigated by iron chelation. Together, our work reveals cytoplasmic redox active iron as a novel rheostat in adult stem cells; it demonstrates a role for the intracellular labile iron pool in coordinating a cascade of molecular events which reinforces HSC identity during cell division and to drive stem cell ageing when perturbed. As loss of iron homeostasis is commonly observed in the elderly, we anticipate these findings to trigger further studies into understanding and therapeutic mitigation of labile iron pool-dependent hematopoietic stem cell dysfunction in a wide range of degenerative and malignant hematologic pathologies. Disclosures D'Alessandro: Omix Thecnologies: Other: Co-founder; Rubius Therapeutics: Consultancy; Forma Therapeutics: Membership on an entity's Board of Directors or advisory committees.

Published
2021

40. No keto for AML stem cells!

Author

Britta Will

Subjects
Text mining, business.industry, Chemistry, Immunology, Cancer research, MEDLINE, Cell Biology, Hematology, Stem cell, business, Biochemistry
Published
2020

41. Mechanisms and therapeutic prospects of thrombopoietin receptor agonists

Author

James B. Bussel, Britta Will, Nichola Cooper, Amit Verma, Austin G. Kulasekararaj, John W. Semple, and Ulrich Steidl

Subjects
medicine.medical_specialty, Romiplostim, Hematology, business.industry, Myelodysplastic syndromes, Eltrombopag, medicine.disease, Thrombocytopenia, chemistry.chemical_compound, Mechanism of action, chemistry, Internal medicine, Immunology, Humans, Medicine, medicine.symptom, business, Receptor, Receptors, Thrombopoietin, Thrombopoietin, medicine.drug, Megakaryopoiesis
Abstract

The second-generation thrombopoietin (TPO) receptor agonists eltrombopag and romiplostim are potent activators of megakaryopoiesis and represent a growing treatment option for patients with thrombocytopenic hematological disorders. Both TPO receptor agonists have been approved worldwide for the treatment of children and adults with chronic immune thrombocytopenia. In the EU and USA, eltrombopag is approved for the treatment of patients with severe aplastic anemia who have had an insufficient response to immunosuppressive therapy and in the USA for the first-line treatment of severe aplastic anemia in combination with immunosuppressive therapy. Eltrombopag has also shown efficacy in several other disease settings, for example, chemotherapy-induced thrombocytopenia, selected inherited thrombocytopenias, and myelodysplastic syndromes. While both TPO receptor agonists stimulate TPO receptor signaling and enhance megakaryopoiesis, their vastly different biochemical structures bestow upon them markedly different molecular and functional properties. Here, we review and discuss results from preclinical and clinical studies on the functional and molecular mechanisms of action of this new class of drug.

Published
2019

42. HIV portends a poor prognosis in myelodysplastic syndromes

Author

Kith Pradhan, Anjali Sharma, Yanhua Wang, Ashwin Sridharan, Santiago Thibaud, Amer Assal, Amit Verma, Barry S. Zingman, Aditi Shastri, Ulrich Steidl, Rahul Polineni, Ira Braunschweig, Britta Will, Mark Chaitowitz, Justin D. Kaner, Murali Janakiram, Sakshi Jasra, Louis M. Weiss, Ioannis Mantzaris, and Harold Elias

Subjects
Male, Oncology, Cancer Research, medicine.medical_specialty, Poor prognosis, Human immunodeficiency virus (HIV), HIV Infections, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, hemic and lymphatic diseases, Internal medicine, Biomarkers, Tumor, medicine, Humans, Aged, Retrospective Studies, business.industry, Myelodysplastic syndromes, Clinical course, HIV, virus diseases, Hematology, Middle Aged, Prognosis, medicine.disease, Survival Rate, Myelodysplastic Syndromes, 030220 oncology & carcinogenesis, Mutation, Female, business, Follow-Up Studies, 030215 immunology
Abstract

Even though HIV is associated with worse prognosis in many malignancies, the clinical course of myelodysplastic syndrome (MDS) in HIV + patients has not been well studied. Determining the clinical presentation and outcomes of MDS in these patients would be important for future diagnostic strategies, as anemia and other cytopenias are commonly seen in HIV + patients. Unique data mining software was used to identify cases of MDS or AML in adult patients who were also HIV + at Albert Einstein/Montefiore Medical Center between 1 January 2003 and 1 January 2017. Using Chi-Square and Fisher's exact test, characteristics of the HIV + MDS patients were compared to 135 HIV - MDS patients from the same institution diagnosed between 1997 and 2011. Fourteen biopsy proven MDS patients were identified with concomitant HIV. HIV + MDS patients presented at a younger age (59 vs. 71 yrs

Published
2019

43. Myelodysplastic Syndrome Progression to Acute Myeloid Leukemia at the Stem Cell Level

Author

Jiahao Chen, Cristina Montagna, Britta Will, David Reynolds, Amit Verma, Yun Ruei Kao, Ulrich Steidl, Daqian Sun, Swathi Rao Narayanagari, and Tihomira I. Todorova

Subjects
0301 basic medicine, Myeloid, Biology, Models, Biological, Somatic evolution in cancer, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, 0302 clinical medicine, Cancer stem cell, hemic and lymphatic diseases, medicine, Humans, Neoplastic transformation, Stem Cells, Myelodysplastic syndromes, Myeloid leukemia, General Medicine, medicine.disease, Clone Cells, 3. Good health, Leukemia, Myeloid, Acute, Leukemia, 030104 developmental biology, medicine.anatomical_structure, Myelodysplastic Syndromes, 030220 oncology & carcinogenesis, Mutation, Disease Progression, Cancer research, Stem cell
Abstract

Myelodysplastic syndromes (MDS) frequently progress to acute myeloid leukemia (AML); however, the cells leading to malignant transformation have not been directly elucidated. As progression of MDS to AML in humans provides a biological system to determine the cellular origins and mechanisms of neoplastic transformation, we studied highly fractionated stem cell populations in longitudinal samples of patients with MDS who progressed to AML. Targeted deep sequencing combined with single-cell sequencing of sorted cell populations revealed that stem cells at the MDS stage, including immunophenotypically and functionally defined pre-MDS stem cells (pre-MDS-SC), had a significantly higher subclonal complexity compared to blast cells and contained a large number of aging-related variants. Single-cell targeted resequencing of highly fractionated stem cells revealed a pattern of nonlinear, parallel clonal evolution, with distinct subclones within pre-MDS-SC and MDS-SC contributing to generation of MDS blasts or progression to AML, respectively. Furthermore, phenotypically aberrant stem cell clones expanded during transformation and stem cell subclones that were not detectable in MDS blasts became dominant upon AML progression. These results reveal a crucial role of diverse stem cell compartments during MDS progression to AML and have implications for current bulk cell–focused precision oncology approaches, both in MDS and possibly other cancers that evolve from premalignant conditions, that may miss pre-existing rare aberrant stem cells that drive disease progression and leukemic transformation. High-resolution sequencing of longitudinal patient samples reveals subclonal mutational diversity in the stem cell compartment driving parallel evolution patterns in acute myeloid leukemia progression.

Published
2018

44. The thrombopoietin mimetic JNJ-26366821 increases megakaryopoiesis without affecting malignant myeloid proliferation

Author

Shanisha Gordon-Mitchell, Aditi Shastri, Srinivas Aluri, Weng Lang Yang, Amit Verma, Chandan Guha, Diego Adrianzen-Herrera, Tushar D. Bhagat, Gary Eichenbaum, Gaurav Choudhary, Nandini Ramachandra, Hui Zhang, Britta Will, Michelle Mahler, and Ulrich Steidl

Subjects
Cancer Research, Myeloid, Peptide, 03 medical and health sciences, Mice, 0302 clinical medicine, hemic and lymphatic diseases, Homologous chromosome, Medicine, Animals, Humans, Platelet, Thrombopoietin, Megakaryopoiesis, Cell Proliferation, chemistry.chemical_classification, business.industry, food and beverages, hemic and immune systems, Hematology, Myeloid proliferation, Leukemia, Myeloid, Acute, medicine.anatomical_structure, Oncology, chemistry, 030220 oncology & carcinogenesis, Myelodysplastic Syndromes, embryonic structures, Cancer research, business, Receptors, Thrombopoietin, 030215 immunology
Abstract

Thrombocytopenia remains a challenge in myeloid malignancies, needing safer and more effective therapies. JNJ-26366821, a pegylated synthetic peptide thrombopoietin (TPO) mimetic not homologous to endogenous TPO, has an in-vitro EC50 of 0.2 ng/mL for the TPO receptor and dose dependently elevates platelets in volunteers. We demonstrate that JNJ-26366821 increases megakaryocytic differentiation and megakaryocytic colony formation in healthy controls and samples from myelodysplastic syndrome (MDS) and acute myeloid leukemia (AML). JNJ-26366821 had no effect on proliferation of malignant myeloid cell lines at doses up to 1000 ng/mL and malignant patient-derived mononuclear cells showed no increased cell growth or leukemic colony formation capacity at concentrations between 0.2 ng/mL and 10 ng/mL. Furthermore, JNJ-26366821 did not enhance in-vivo engraftment of leukemic cells in an AML xenotransplantation murine model. Our results show that JNJ-26366821 stimulates megakaryopoiesis without causing proliferation of the malignant myeloid clones in MDS/AML and provides the rationale for clinical testing of JNJ-26366821 in myeloid malignancies.

Published
2020

45. Antisense STAT3 inhibitor decreases viability of myelodysplastic and leukemic stem cells

Author

Shanisha Gordon-Mitchell, Robert Lopez, Kith Pradhan, Minwei Ye, Lumie Bernard, Jacqueline Boultwood, A. Robert MacLeod, Pearlie K. Epling-Burnette, Tushar D. Bhagat, B. Hilda Ye, Orsolya Giricz, Andrea Pellagatti, Li-Fan Wong, Sally Cole, Yosman Dhar, Youngsoo Kim, Amit Verma, Nandini Ramachandra, Gaurav S. Choudhary, Ulrich Steidl, Jonathan Feld, Amittha Wickrema, Tianyuan Zhou, Patricia McCoon, David A. Frank, Aditi Shastri, Victor Thiruthuvanathan, Sanchari Bhattacharyya, Matthias Bartenstein, Margarida Teixeira, Britta Will, Richard Woessner, and Goutham Ravipati

Subjects
Male, STAT3 Transcription Factor, 0301 basic medicine, Cell Survival, Oligonucleotides, CD34, Mice, SCID, Biology, 03 medical and health sciences, 0302 clinical medicine, Mice, Inbred NOD, Cell Line, Tumor, hemic and lymphatic diseases, medicine, Animals, Humans, MCL1, Progenitor cell, Mice, Knockout, Gene knockdown, Myelodysplastic syndromes, Myeloid leukemia, General Medicine, medicine.disease, Xenograft Model Antitumor Assays, Neoplasm Proteins, Leukemia, Myeloid, Acute, Haematopoiesis, 030104 developmental biology, Myelodysplastic Syndromes, 030220 oncology & carcinogenesis, Neoplastic Stem Cells, Cancer research, Female, Stem cell, Research Article
Abstract

Acute myeloid leukemia (AML) and myelodysplastic syndromes (MDS) are associated with disease-initiating stem cells that are not eliminated by conventional therapies. Transcriptomic analysis of stem and progenitor populations in MDS and AML demonstrated overexpression of STAT3 that was validated in an independent cohort. STAT3 overexpression was predictive of a shorter survival and worse clinical features in a large MDS cohort. High STAT3 expression signature in MDS CD34(+) cells was similar to known preleukemic gene signatures. Functionally, STAT3 inhibition by a clinical, antisense oligonucleotide, AZD9150, led to reduced viability and increased apoptosis in leukemic cell lines. AZD9150 was rapidly incorporated by primary MDS/AML stem and progenitor cells and led to increased hematopoietic differentiation. STAT3 knockdown also impaired leukemic growth in vivo and led to decreased expression of MCL1 and other oncogenic genes in malignant cells. These studies demonstrate that STAT3 is an adverse prognostic factor in MDS/AML and provide a preclinical rationale for studies using AZD9150 in these diseases.

Published
2018

46. EXCEPTIONAL RESPONSE OF REFRACTORY ATLL WITH MDM4 AMPLIFICATION TO NOVEL STAPLED PEPTIDE DUAL MDM4/2 INHIBITOR

Author

Noah Kornblum, Ira Braunschweig, Karen Fehn, M. Aivado, L. Carjaval, Urvi A Shah, Amit Verma, D. Pinchasik, Koki Ueda, K. Ramesh, Ulrich Steidl, Swati Goel, Ana Acuna Villaorduna, H.B. Ye, Britta Will, Murali Janakiram, and Victor Thiruthuvanathan

Subjects
Cancer Research, Oncology, Refractory, Chemistry, Cancer research, Stapled peptide, Exceptional Response, Hematology, General Medicine
Published
2019

47. Lenalidomide and Eltrombopag for Treatment in Low or Intermediate Risk Myelodysplastic Syndrome: Result of a Phase 2 Study Combination Clinical Trial

Author

Cassady Remy, Mendel Goldfinger, Lizamarie Bachier-Rodriguez, Abdulraheem Yacoub, Ira Braunschweig, Mohammad Kazemi, Noah Kornblum, Amit Verma, William B. Donnellan, R. Alejandro Sica, Britta Will, Karen Fehn, Prafulla Bhagat, Ulrich Steidl, Aditi Shastri, Sakshi Jasra, Jesus D. Gonzalez-Lugo, Kira Gritsman, Suman Kambhampati, and Ioannis Mantzaris

Subjects
Oncology, medicine.medical_specialty, business.industry, Immunology, Eltrombopag, Phases of clinical research, Cell Biology, Hematology, Biochemistry, Clinical trial, chemistry.chemical_compound, chemistry, Internal medicine, Medicine, business, Intermediate risk, Lenalidomide, medicine.drug
Abstract

Introduction: Lenalidomide (LEN) is approved for treatment of Myelodysplastic Syndrome (MDS) with chromosome 5q deletion (del 5q) as it has shown to induce disease remission and transfusion independence in close to 65% of this population. For patients (pts) without del 5q, LEN has shown to reduce transfusion needs in one-quarter of pts, but its use is limited by significant thrombocytopenia, and pts with platelet counts (PLTs) Methods: Pts aged ≥18 years with low/int risk MDS per IPSS, or non-proliferative chronic myelomonocytic leukemia (CMML), with bone marrow blasts Results: 51 pts were accrued, with 44 evaluable pts. Of evaluable pts, most were male (70%), median age was 71 years (range 34-93). 42 (95%) pts had MDS and 2 (5%) CMML. 24 (55%) pts were low-risk per IPSS-R score. 28 (64%) pts were treatment-naïve and 16 (36%) had received ≥1lines of treatment, including erythropoiesis stimulating agents. 24 (55%) pts were assigned to arm A and 20 (45%) pts to arm B. ELT/LEN was well tolerated. Non-hematological grade 3-4 treatment-related adverse events were few, including G3 hyperbilirubinemia (7%), G3 transaminitis (2%), G3 diarrhea (2%), G3 arthralgias (2%). 2 pts had major bleeding events; there were 2 deaths, one attributable to pneumonia and one to gallbladder cancer. 1 of 31 pts who received ELT had a reversible increase in peripheral blasts while on treatment, and 1 pt had development of marrow fibrosis after 6 years of ELT. ITT analysis of total population (51) revealed an objective response (ORR) of 35%; ORR of 32% (9/28) in arm A (PLTs ≥50,000),and 39% (9/23) in arm B (PLTs 17 pts received ELT alone, among these ORR was 41% (7/17), with 29% achieving bilineage responses, 1 CR. 13 pts received LEN alone, ORR was 46% (6/13), of these 100% achieved RBC-TI. 14 pts received ELT/LEN combination, ORR was 36%, 2 (14%) achieved bilineage responses and 2 (14%) CR. There were 2 HIV-positive MDS pts, both achieved sustained CRs, one with ELT alone and one with ELT/LEN combination. Mean time to response was 9.4 wks (range 6-12.4) for ELT alone, 10.9 wks (range 2.4-16) for LEN alone, and 9.9 wks (range 2-20) for ELT/LEN combination. Mean duration of response was 102 wks for ELT (range 8-ongoing), 63 wks (range 25-ongoing) for LEN, and 66 wks (range 8.3-ongoing) for ELT/LEN as of last follow-up. Conclusions: Treatment with ELT/LEN demonstrates good efficacy with ORR of 40.9%, response durability and an acceptable safety profile for evaluable pts with low/int risk MDS. ELT can lead to single agent responses with an acceptable safety profile and sizable proportion of multilineage responses. One patient developed bone marrow fibrosis and one patient had a transient increase in blasts, hence, undermining these pre-existing safety concerns. Lastly, using our study schema 32% of pts were able to initiate or continue LEN achieving a 36% ORR whereas in prior studies these pts would have been excluded. Figure 1 Figure 1. Disclosures Yacoub: Agios: Membership on an entity's Board of Directors or advisory committees; Acceleron Pharma: Membership on an entity's Board of Directors or advisory committees; CTI Biopharma: Membership on an entity's Board of Directors or advisory committees; Novartis: Membership on an entity's Board of Directors or advisory committees; Incyte: Speakers Bureau. Gritsman: iOnctura: Research Funding. Shastri: Kymera Therapeutics: Research Funding; Onclive: Honoraria; GLC: Consultancy; Guidepoint: Consultancy. Verma: Celgene: Consultancy; Acceleron: Consultancy; Novartis: Consultancy; Stelexis: Consultancy, Current equity holder in publicly-traded company; Eli Lilly: Research Funding; Curis: Research Funding; Medpacto: Research Funding; Incyte: Research Funding; Stelexis: Current equity holder in publicly-traded company; Throws Exception: Current equity holder in publicly-traded company; GSK: Research Funding; BMS: Research Funding. OffLabel Disclosure: Lenalidomide has shown to be effective achieving RBC Transfusion Independence in Myelodysplastic Syndromes without deletion 5q Eltrombopag is a TPO-R agonist, its purpose in this trial is to evaluate if it would increase platelet counts in patients with Myelodisplastic Syndrome.

Published
2021

49. A myeloid tumor suppressor role for NOL3

Author

Kira Gritsman, Ulrich Steidl, Hideki Makishima, Britta Will, Richard T. Piszczatowski, Wendy M. McKimpson, Cassandra M. Hirsch, Kelly Mitchell, Christine McMahon, Boris Bartholdy, Swathi Rao Narayanagari, Richard N. Kitsis, Robert F. Stanley, Tihomira I. Todorova, Jaroslaw P. Maciejewski, and Dagmar Walter

Subjects
0301 basic medicine, Myeloid, biology, Immunology, Cell, CD34, medicine.disease, Phenotype, 3. Good health, Pathogenesis, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, medicine, biology.protein, Cancer research, Immunology and Allergy, Cyclin-dependent kinase 6, Myelofibrosis, Janus kinase
Abstract

Despite the identification of several oncogenic driver mutations leading to constitutive JAK–STAT activation, the cellular and molecular biology of myeloproliferative neoplasms (MPN) remains incompletely understood. Recent discoveries have identified underlying disease-modifying molecular aberrations contributing to disease initiation and progression. Here, we report that deletion of Nol3 (Nucleolar protein 3) in mice leads to an MPN resembling primary myelofibrosis (PMF). Nol3−/− MPN mice harbor an expanded Thy1+LSK stem cell population exhibiting increased cell cycling and a myelomonocytic differentiation bias. Molecularly, this phenotype is mediated by Nol3−/−-induced JAK–STAT activation and downstream activation of cyclin-dependent kinase 6 (Cdk6) and Myc. Nol3−/− MPN Thy1+LSK cells share significant molecular similarities with primary CD34+ cells from PMF patients. NOL3 levels are decreased in CD34+ cells from PMF patients, and the NOL3 locus is deleted in a subset of patients with myeloid malignancies. Our results reveal a novel genetic PMF-like mouse model and identify a tumor suppressor role for NOL3 in the pathogenesis of myeloid malignancies.

Published
2017

50. Epigenetically Aberrant Stroma in MDS Propagates Disease via Wnt/beta-Catenin Activation

Author

A. Trevor Barlowe, Vineeth Sukrithan, Remco Hoogenboezem, Remi Laurence, Jinghang Zhang, Britta Will, Marc H.G.P. Raaijmakers, Mathijs A. Sanders, Amit Verma, Michael G. Kharas, Si Chen, Robert Lopez, Gaurav Choudhary, Nandini Ramachandra, Prafullla Bhagat, Jacqueline Boultwood, A. Mario Marcondes, Iaonnis Mantzaris, Andrea Pellagatti, John M. Greally, Orsolya Giricz, Matthias Bartenstein, Suman Kambhampati, Cecilia Yeung, Peter D. Aplan, Konrad Hochedlinger, Kira Gritsman, Davendra Sohal, Elianna M. Amin, Tushar D. Bhagat, Siddhartha Mukherjee, Patrick Tivnan, H. Joachim Deeg, Dagny Von Ahrens, Ulrich Steidl, Amittha Wickrema, Yiting Yu, Kith Pradhan, and Hematology

Subjects
0301 basic medicine, Cancer Research, Pathology, medicine.medical_specialty, Stromal cell, Myeloid, Oncogene Proteins, Fusion, Apoptosis, Mice, Transgenic, Biology, Article, Epigenesis, Genetic, 03 medical and health sciences, Mice, Stroma, hemic and lymphatic diseases, medicine, Tumor Cells, Cultured, Animals, Humans, beta Catenin, Cell Proliferation, Wnt signaling pathway, Cell Differentiation, Mesenchymal Stem Cells, DNA Methylation, Hematopoietic Stem Cells, Wnt Proteins, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, Oncology, Frzb, Myelodysplastic Syndromes, DNA methylation, Cancer research, CpG Islands, Bone marrow
Abstract

The bone marrow microenvironment influences malignant hematopoiesis, but how it promotes leukemogenesis has not been elucidated. In addition, the role of the bone marrow stroma in regulating clinical responses to DNA methyltransferase inhibitors (DNMTi) is also poorly understood. In this study, we conducted a DNA methylome analysis of bone marrow–derived stromal cells from myelodysplastic syndrome (MDS) patients and observed widespread aberrant cytosine hypermethylation occurring preferentially outside CpG islands. Stroma derived from 5-azacytidine–treated patients lacked aberrant methylation and DNMTi treatment of primary MDS stroma enhanced its ability to support erythroid differentiation. An integrative expression analysis revealed that the WNT pathway antagonist FRZB was aberrantly hypermethylated and underexpressed in MDS stroma. This result was confirmed in an independent set of sorted, primary MDS-derived mesenchymal cells. We documented a WNT/β-catenin activation signature in CD34+ cells from advanced cases of MDS, where it associated with adverse prognosis. Constitutive activation of β-catenin in hematopoietic cells yielded lethal myeloid disease in a NUP98–HOXD13 mouse model of MDS, confirming its role in disease progression. Our results define novel epigenetic changes in the bone marrow microenvironment, which lead to β-catenin activation and disease progression of MDS. Cancer Res; 77(18); 4846–57. ©2017 AACR.

Published
2017

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