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51. The Intriguing Clinical Success of BCL-2 Inhibition in Acute Myeloid Leukemia

Author

Brett M. Stevens, Daniel A. Pollyea, Clayton A. Smith, Shanshan Pei, and Craig T. Jordan

Subjects
0301 basic medicine, Cancer Research, business.industry, Myeloid leukemia, Cell Biology, medicine.disease, Clinical success, 03 medical and health sciences, Leukemia, 030104 developmental biology, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, Cancer research, Medicine, business
Abstract

Over the past several decades numerous preclinical and clinical studies have pursued new approaches for the treatment of acute myeloid leukemia (AML). While some degree of clinical response has been demonstrated for many therapies, for the most part, fundamental changes in the treatment landscape have been lacking. Recently, the use of the BCL-2 inhibitor venetoclax has emerged as a potent therapy for a majority of newly diagnosed AML patients. Venetoclax regimens have shown broad response rates with deep and durable remissions, with a superior toxicity profile compared with traditional intensive chemotherapy agents. Numerous ongoing studies are now using venetoclax in combination with a wide range of other agents as investigators seek even more effective and well-tolerated regimens. Notably, however, while the empirical results of BCL-2 inhibition are encouraging, the mechanisms that have led to these successful clinical outcomes remain unclear. Intriguingly, the activity of venetoclax in AML patients appears to go beyond simply modulating canonical antiapoptosis mechanisms; in addition, the efficacy of venetoclax is linked to its combined use with conventional low-intensity backbone therapies. This article will evaluate the state of the field, provide a summary of key considerations, and propose directions for future studies.

Published
2021

52. Targeting Energy Metabolism in Cancer Stem Cells: Progress and Challenges in Leukemia and Solid Tumors

Author

Courtney L. Jones, Anagha Inguva, and Craig T. Jordan

Subjects
Myeloid, Energy metabolism, Biology, Article, 03 medical and health sciences, 0302 clinical medicine, Cancer stem cell, hemic and lymphatic diseases, Genetics, medicine, Humans, 030304 developmental biology, Leukemia Stem Cell, 0303 health sciences, Leukemia, Extramural, Cell Biology, Hematopoietic Stem Cells, medicine.disease, Leukemia, Myeloid, Acute, Haematopoiesis, medicine.anatomical_structure, Neoplastic Stem Cells, Cancer research, Molecular Medicine, Stem cell, Energy Metabolism, 030217 neurology & neurosurgery
Abstract

Malignant stem cells have long been considered a key therapeutic target in leukemia. Therapeutic strategies designed to target the fundamental biology of leukemia stem cells while sparing normal hematopoietic cells may provide better outcomes for leukemia patients. One process in leukemia stem cell biology that has intriguing therapeutic potential is energy metabolism. In this article we discuss the metabolic properties of leukemia stem cells and how targeting energy metabolism may provide more effective therapeutic regimens for leukemia patients. In addition, we highlight the similarities and differences in energy metabolism between leukemia stem cells and malignant stem cells from solid tumors.

Published
2021

53. The propriety of upgrading responses to venetoclax + azacitidine in newly diagnosed patients with acute myeloid leukemia

Author

Jeffrey Schowinsky, Christine McMahon, Maria L. Amaya, Craig T. Jordan, Amanda Winters, Marc Schwartz, Evan Cherry, Jonathan A. Gutman, Daniel A. Pollyea, Diana Abbott, and Clayton A. Smith

Subjects
Oncology, Cancer Research, medicine.medical_specialty, Azacitidine, Context (language use), Newly diagnosed, Intensive chemotherapy, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, hemic and lymphatic diseases, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Response criteria, Sulfonamides, Venetoclax, business.industry, Myeloid leukemia, Hematology, Bridged Bicyclo Compounds, Heterocyclic, Leukemia, Myeloid, Acute, chemistry, 030220 oncology & carcinogenesis, business, 030215 immunology, medicine.drug
Abstract

Widely-used response criteria, conditional upon count recovery, were developed for acute myeloid leukemia (AML) in the context of intensive chemotherapy (IC). Extending these definitions to continuously-administered venetoclax-based therapies might underestimate responses. Best practices for venetoclax-based therapies mandate interruption after an end-of-cycle 1 bone marrow biopsy shows morphologic remission with cytopenias. We analyzed 435 patients with newly-diagnosed AML and follow-up response assessments. Of the 101 who responded to venetoclax + azacitidine, overall survival for patients whose response was upgraded due to count recovery during a 14-day post-disease assessment period, from complete remission (CR) with incomplete recovery of blood counts to CR, was not different compared to patients who did not need the 14-day period for count recovery. These results were distinct from 138 IC patients. Although sample sizes for the comparison groups were small, and conclusions are exploratory and must be verified, these findings support consideration of new response criteria for venetoclax-based regimens.

Published
2020

56. Higher-Dose Venetoclax with Measurable Residual Disease-Guided Azacitidine Discontinuation in Newly Diagnosed Patients with Acute Myeloid Leukemia: Phase 2 Hiddav Study

Author

Jonathan A. Gutman, Amanda C. Winters, Andrew Kent, Maria L. Amaya, Christine M. McMahon, Clayton Smith, Craig T Jordan, Brett M. Stevens, Mohammad Minhajuddin, Shanshan Pei, Jeffrey Schowinsky, Jennifer Tobin, Kelly O'Brien, Angela Falco, Elizabeth Taylor, Constance Brecl, Phuong Ho, Connor Sohalski, Jessica Dell-Martin, Olivia Ondracek, Diana Abbott, and Daniel A. Pollyea

Subjects
Immunology, Cell Biology, Hematology, Biochemistry
Published
2022

59. MDS-associated SF3B1 mutations enhance proinflammatory gene expression in patient blast cells

Author

Brian P. O'Connor, Brett M. Stevens, Frank Fang-Yao Lee, Brenna R. Hedin, Scott Alper, Jennifer R. Knapp, Daniel A. Pollyea, Chelsea Harris, Craig T. Jordan, Aik Choon Tan, Hyunmin Kim, and Eric M. Pietras

Subjects
0301 basic medicine, Spliceosome, RNA Splicing, Immunology, Gene Expression, Inflammation, Biology, Article, Proinflammatory cytokine, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, hemic and lymphatic diseases, Precursor cell, Gene expression, medicine, Humans, Immunology and Allergy, Gene, Stem Cells, Cell Biology, Phosphoproteins, 030104 developmental biology, Myelodysplastic Syndromes, 030220 oncology & carcinogenesis, Mutation, RNA splicing, Spliceosomes, Cancer research, Cytokines, RNA Splicing Factors, Inflammation Mediators, medicine.symptom
Abstract

Two factors known to contribute to the development of myelodysplastic syndrome (MDS) and other blood cancers are (i) somatically acquired mutations in components of the spliceosome and (ii) increased inflammation. Spliceosome genes, including SF3B1, are mutated at high frequency in MDS and other blood cancers; these mutations are thought to be neomorphic or gain-of-function mutations that drive disease pathogenesis. Likewise, increased inflammation is thought to contribute to MDS pathogenesis; inflammatory cytokines are strongly elevated in these patients, with higher levels correlating with worsened patient outcome. In the current study, we used RNAseq to analyze pre-mRNA splicing and gene expression changes present in blast cells isolated from MDS patients with or without SF3B1 mutations. We determined that SF3B1 mutations lead to enhanced proinflammatory gene expression in these cells. Thus, these studies suggest that SF3B1 mutations could contribute to MDS pathogenesis by enhancing the proinflammatory milieu in these patients.

Published
2020

60. Fatty acid metabolism underlies venetoclax resistance in acute myeloid leukemia stem cells

Author

Courtney L. Jones, Madeline Goosman, Amanda Winters, Shanshan Pei, Clayton A. Smith, Diana Abbott, Michael R. Savona, Haobin Ye, Angelo D'Alessandro, Daniel A. Pollyea, Anna Krug, Michael W. Becker, Craig T. Jordan, Austin E. Gillen, Rachel Culp-Hill, and Brett M. Stevens

Subjects
Cancer Research, Azacitidine, Article, chemistry.chemical_compound, Downregulation and upregulation, Antineoplastic Combined Chemotherapy Protocols, Humans, Medicine, Amino Acids, neoplasms, Beta oxidation, Sulfonamides, Fatty acid metabolism, business.industry, Venetoclax, Stem Cells, Fatty Acids, Myeloid leukemia, Bridged Bicyclo Compounds, Heterocyclic, Leukemia, Myeloid, Acute, Oncology, chemistry, Ven, Cancer research, Stem cell, business, medicine.drug
Abstract

Venetoclax with azacitidine (ven/aza) has emerged as a promising treatment regimen for acute myeloid leukemia (AML), with a high percentage of clinical remissions in newly diagnosed patients. However, approximately 30% of newly diagnosed patients and the majority of patients who have relapsed do not achieve remission with ven/aza. We previously reported that ven/aza efficacy is based on eradication of AML stem cells through a mechanism involving inhibition of amino acid metabolism, a process required in primitive AML cells to drive oxidative phosphorylation. Herein we demonstrate that resistance to ven/aza occurs via upregulation of fatty acid oxidation (FAO), which occurs either due to RAS pathway mutations or as a compensatory adaptation in relapsed disease. Utilization of FAO obviates the need for amino acid metabolism, thereby rendering ven/aza ineffective. Pharmacological inhibition of FAO restores sensitivity to ven/aza in drug-resistant AML cells. We propose inhibition of FAO as a therapeutic strategy to address ven/aza resistance. Jordan and colleagues show the role of increased fatty acid metabolism in AML stem cells, in both intrinsic and acquired resistance to combination venetoclax and azacitidine, and find that cells can be re-sensitized by inhibiting fatty acid oxidation.

Published
2020

61. Monocytic Subclones Confer Resistance to Venetoclax-Based Therapy in Patients with Acute Myeloid Leukemia

Author

Travis Nemkov, John M. Ashton, Nabilah Khan, Anna Krug, Maria L. Amaya, Jeffrey Schowinsky, Jonathan A. Gutman, Shanshan Pei, Andrew Hammes, Kent Riemondy, Diana Abbott, Brett M. Stevens, Anagha Inguva, Courtney L. Jones, Biniam Adane, Ryan M. Sheridan, Angelo D'Alessandro, Jihye Kim, Michael R. Savona, J Ponder, Daniel A. Pollyea, Clayton A. Smith, Mohammad Minhajuddin, Haley E. Ramsey, James C. Costello, Annika Gustafson, Rui Fu, Amanda Winters, Austin E. Gillen, Haobin Ye, Jason R. Myers, and Craig T. Jordan

Subjects
0301 basic medicine, Azacitidine, Article, Pathogenesis, Transcriptome, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, hemic and lymphatic diseases, Biological property, Humans, Medicine, MCL1, In patient, neoplasms, Aged, Sulfonamides, Venetoclax, business.industry, Myeloid leukemia, Bridged Bicyclo Compounds, Heterocyclic, Leukemia, Myeloid, Acute, 030104 developmental biology, Oncology, chemistry, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer research, business, medicine.drug
Abstract

Venetoclax-based therapy can induce responses in approximately 70% of older previously untreated patients with acute myeloid leukemia (AML). However, up-front resistance as well as relapse following initial response demonstrates the need for a deeper understanding of resistance mechanisms. In the present study, we report that responses to venetoclax +azacitidine in patients with AML correlate closely with developmental stage, where phenotypically primitive AML is sensitive, but monocytic AML is more resistant. Mechanistically, resistant monocytic AML has a distinct transcriptomic profile, loses expression of venetoclax target BCL2, and relies on MCL1 to mediate oxidative phosphorylation and survival. This differential sensitivity drives a selective process in patients which favors the outgrowth of monocytic subpopulations at relapse. Based on these findings, we conclude that resistance to venetoclax + azacitidine can arise due to biological properties intrinsic to monocytic differentiation. We propose that optimal AML therapies should be designed so as to independently target AML subclones that may arise at differing stages of pathogenesis. Significance: Identifying characteristics of patients who respond poorly to venetoclax-based therapy and devising alternative therapeutic strategies for such patients are important topics in AML. We show that venetoclax resistance can arise due to intrinsic molecular/metabolic properties of monocytic AML cells and that such properties can potentially be targeted with alternative strategies.

Published
2020

62. Therapeutic resistance in acute myeloid leukemia cells is mediated by a novel ATM/mTOR pathway regulating oxidative phosphorylation

Author

Hae J Park, Mark A Gregory, Vadym Zaberezhnyy, Andrew Goodspeed, Craig T Jordan, Jeffrey S Kieft, and James DeGregori

Subjects
General Immunology and Microbiology, General Neuroscience, TOR Serine-Threonine Kinases, Apoptosis, General Medicine, General Biochemistry, Genetics and Molecular Biology, Oxidative Phosphorylation, Leukemia, Myeloid, Acute, fms-Like Tyrosine Kinase 3, Drug Resistance, Neoplasm, Cell Line, Tumor, hemic and lymphatic diseases, Mutation, Tumor Microenvironment, Humans, Everolimus, Phosphorylation, Protein Kinase Inhibitors
Abstract

While leukemic cells are susceptible to various therapeutic insults, residence in the bone marrow microenvironment typically confers protection from a wide range of drugs. Thus, understanding the unique molecular changes elicited by the marrow is of critical importance towards improving therapeutic outcomes. In the present study, we demonstrate that aberrant activation of oxidative phosphorylation serves to induce therapeutic resistance in FLT3 mutant human AML cells challenged with FLT3 inhibitor drugs. Importantly, our findings show that AML cells are protected from apoptosis following FLT3 inhibition due to marrow-mediated activation of ATM, which in turn up-regulates oxidative phosphorylation via mTOR signaling. mTOR is required for the bone marrow stroma-dependent maintenance of protein translation, with selective polysome enrichment of oxidative phosphorylation transcripts, despite FLT3 inhibition. To investigate the therapeutic significance of this finding, we tested the mTOR inhibitor everolimus in combination with the FLT3 inhibitor quizartinib in primary human AML xenograft models. While marrow resident AML cells were highly resistant to quizartinib alone, the addition of everolimus induced profound reduction in tumor burden and prevented relapse. Taken together, these data provide a novel mechanistic understanding of marrow-based therapeutic resistance, and a promising strategy for improved treatment of FLT3 mutant AML patients.

Published
2022

63. Integrative Analysis of Drug Response and Clinical Outcome in Acute Myeloid Leukemia

Author

Daniel Bottomly, Nicola Long, Anna Reister Schultz, Stephen E. Kurtz, Cristina E. Tognon, Kara Johnson, Melissa Abel, Anupriya Agarwal, Sammantha Avaylan, Erik Benton, Aurora Blucher, Uma Borate, Theodore Braun, Jordana Brown, Jade Bryant, Russell Burke, Amy Carlos, Bill H. Chang, Hyun Jun Cho, Stephen Christy, Cody Coblentz, Aaron M. Cohen, Amanda d’Almeida, Rachel Cook, Alexey Danilov, Kim-Hien T. Dao, Michie Degnin, James Dibb, Christopher A. Eide, Isabel A. English, Stuart Hagler, Heath Harrelson, Rachel Henson, Hibery Ho, Sunil Joshi, Brian Junio, Andy Kaempf, Yoko Kosaka, Ted Laderas, Matt Lawhead, Hyunjung Lee, Jessica T. Leonard, Chenwei Lin, Evan F. Lind, Selina Qiuying Liu, Pierrette Lo, Marc M. Loriaux, Samuel Luty, Julia E. Maxson, Tara Macey, Jacqueline Martinez, Jessica Minnier, Andrea Monteblanco, Motomi Mori, Quinlan Morrow, Dylan Nelson, Justin Ramsdill, Angela Rofelty, Alexandra Rogers, Peter Ryabinin, Jennifer N. Saultz, David A. Sampson, Samantha L. Savage, Robert Schuff, Robert Searles, Rebecca L. Smith, Stephen E. Spurgeon, Tyler Sweeney, Ronan T. Swords, Aashis Thapa, Karina Thiel-Klare, Elie Traer, Jake Wagner, Beth Wilmot, Joelle Wolf, Guanming Wu, Amy Yates, Haijiao Zhang, Christopher Cogle, Robert H. Collins, Michael W. Deininger, Christopher S. Hourigan, Craig T. Jordan, Tara L. Lin, Micaela E. Martinez, Rachel R. Pallapati, Daniel Pollyea, Tony Pomicter, Justin M. Watts, Scott Weir, Brian J. Druker, Shannon K. McWeeney, and Jeffrey W. Tyner

Published
2022

65. The STAT3-MYC axis promotes survival of leukemia stem cells by regulating SLC1A5 and oxidative phosphorylation

Author

Anagha Inguva, Fabia Gamboni, Brett M. Stevens, Daniel A. Pollyea, Steffanie L. Furtek, Courtney L. Jones, Anna Krug, Philip Reigan, Haobin Ye, Mohammad Minhajuddin, Amanda Winters, Maria L. Amaya, Craig T. Jordan, Shanshan Pei, and Angelo D'Alessandro

Subjects
Amino Acid Transport System ASC, STAT3 Transcription Factor, Programmed cell death, Cell Survival, Immunology, Population, Biochemistry, Oxidative Phosphorylation, Minor Histocompatibility Antigens, Proto-Oncogene Proteins c-myc, medicine, Tumor Cells, Cultured, Humans, Progenitor cell, education, STAT3, education.field_of_study, Myeloid Neoplasia, biology, Chemistry, Cell Biology, Hematology, medicine.disease, Haematopoiesis, Leukemia, Leukemia, Myeloid, Acute, STAT protein, Cancer research, biology.protein, Neoplastic Stem Cells, Stem cell, Signal Transduction
Abstract

Acute myeloid leukemia (AML) is characterized by the presence of leukemia stem cells (LSCs), and failure to fully eradicate this population contributes to disease persistence/relapse. Prior studies have characterized metabolic vulnerabilities of LSCs, which demonstrate preferential reliance on oxidative phosphorylation (OXPHOS) for energy metabolism and survival. In the present study, using both genetic and pharmacologic strategies in primary human AML specimens, we show that signal transducer and activator of transcription 3 (STAT3) mediates OXPHOS in LSCs. STAT3 regulates AML-specific expression of MYC, which in turn controls transcription of the neutral amino acid transporter gene SLC1A5. We show that genetic inhibition of MYC or SLC1A5 acts to phenocopy the impairment of OXPHOS observed with STAT3 inhibition, thereby establishing this axis as a regulatory mechanism linking STAT3 to energy metabolism. Inhibition of SLC1A5 reduces intracellular levels of glutamine, glutathione, and multiple tricarboxylic acid (TCA) cycle metabolites, leading to reduced TCA cycle activity and inhibition of OXPHOS. Based on these findings, we used a novel small molecule STAT3 inhibitor, which binds STAT3 and disrupts STAT3-DNA, to evaluate the biological role of STAT3. We show that STAT3 inhibition selectively leads to cell death in AML stem and progenitor cells derived from newly diagnosed patients and patients who have experienced relapse while sparing normal hematopoietic cells. Together, these findings establish a STAT3-mediated mechanism that controls energy metabolism and survival in primitive AML cells.

Published
2021

66. PU.1 enforces quiescence and limits hematopoietic stem cell expansion during inflammatory stress

Author

Jason R. Myers, Eric M. Pietras, Rachel L Gessner, Katia E. Niño, James DeGregori, Nouraiz Ahmed, Pavel Davizon-Castillo, James S. Chavez, Hyunmin Kim, Taylor S. Mills, Zhonghe Ke, Robert S. Welner, Brett M. Stevens, Timm Schroeder, Beau M Idler, Dirk Loeffler, Giovanny Hernandez, Kelly C. Higa, John M. Ashton, Craig T. Jordan, Hideaki Nakajima, and Jennifer L. Rabe

Subjects
Immunology, Stem Cells & Regeneration, Innate immunity and inflammation, Biology, Article, Proinflammatory cytokine, Mice, Stress, Physiological, Proto-Oncogene Proteins, medicine, Immunology and Allergy, Animals, Homeostasis, Transcription factor, Cell Proliferation, Inflammation, Innate immune system, Cell Cycle, Hematopoietic stem cell, Cell Differentiation, Cell cycle, Hematopoietic Stem Cells, Cell Cycle Gene, Immunity, Innate, Cell biology, Hematopoiesis, Mice, Inbred C57BL, Haematopoiesis, medicine.anatomical_structure, Trans-Activators, Stem cell
Abstract

Hematopoietic stem cells (HSCs) are capable of entering the cell cycle to replenish the blood system in response to inflammatory cues; however, excessive proliferation in response to chronic inflammation can lead to either HSC attrition or expansion. The mechanism(s) that limit HSC proliferation and expansion triggered by inflammatory signals are poorly defined. Here, we show that long-term HSCs (HSCLT) rapidly repress protein synthesis and cell cycle genes following treatment with the proinflammatory cytokine interleukin (IL)-1. This gene program is associated with activation of the transcription factor PU.1 and direct PU.1 binding at repressed target genes. Notably, PU.1 is required to repress cell cycle and protein synthesis genes, and IL-1 exposure triggers aberrant protein synthesis and cell cycle activity in PU.1-deficient HSCs. These features are associated with expansion of phenotypic PU.1-deficient HSCs. Thus, we identify a PU.1-dependent mechanism triggered by innate immune stimulation that limits HSC proliferation and pool size. These findings provide insight into how HSCs maintain homeostasis during inflammatory stress., Journal of Experimental Medicine, 218 (6), ISSN:0022-1007, ISSN:1540-0069, ISSN:1540-9538

Published
2021

67. Venetoclax and azacitidine followed by allogeneic transplant results in excellent outcomes and may improve outcomes versus maintenance therapy among newly diagnosed AML patients older than 60

Author

Daniel A, Pollyea, Amanda, Winters, Christine, McMahon, Marc, Schwartz, Craig T, Jordan, Rachel, Rabinovitch, Diana, Abbott, Clayton A, Smith, and Jonathan A, Gutman

Subjects
Leukemia, Myeloid, Acute, Sulfonamides, Antineoplastic Combined Chemotherapy Protocols, Azacitidine, Humans, Allografts, Bridged Bicyclo Compounds, Heterocyclic, Retrospective Studies
Abstract

The combination of venetoclax (ven) and azacitidine (aza) has resulted in high response rates in the upfront treatment of AML in patients age 75 and patients unfit for intensive chemotherapy. Given the poor historical outcomes in patients age ≥ 60 treated with induction chemotherapy, ven/aza has become our institutional preference for the initial treatment of non-core binding factor (CBF) AML patients age ≥ 60. The benefit of allogeneic stem cell transplant (SCT) in patients who achieve response to ven/aza is uncertain. We report outcomes of SCT-eligible patients treated at our center. Between 1/2015 and 1/2020, 119 newly diagnosed non-CBF AML patients age ≥ 60 received ven/aza as initial therapy. 21 patients underwent SCT; 31 additional patients were potentially SCT eligible but deferred SCT. Overall survival (OS) was significantly greater among SCT patients (median survival not reached) versus potentially SCT eligible patients not undergoing SCT (median 518 days) (p = 0.01). Our data suggest that ven/aza followed by SCT in newly diagnosed AML patients older than ≥ 60 results in excellent outcomes and likely improves outcomes over maintenance therapy. Ongoing investigation will further refine the optimal timing of and selection of patients for SCT based on prognostic disease features and response assessments.

Published
2021

68. Real-world experience of venetoclax with azacitidine for untreated patients with acute myeloid leukemia

Author

Brett M. Stevens, Mark D. Ewalt, Diana Abbott, Daniel A. Pollyea, Stephanie Chase, Jennifer Tobin, Molly Nakic, Chelsey Boggs, Jeffrey Schowinsky, Bradford Siegele, Steven R. Schuster, Jonathan A. Gutman, Keri Halsema, Enkhtsetseg Purev, Lindsey Lyle, Jeff Kaiser, Clayton A. Smith, Amanda Winters, Julie Rosser, Craig T. Jordan, and Vishal Rana

Subjects
Male, medicine.medical_specialty, Neoplasm, Residual, Myeloid, Clinical Trials and Observations, Azacitidine, chemistry.chemical_compound, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, Humans, Medicine, Genetic Testing, Aged, Aged, 80 and over, Sulfonamides, business.industry, Venetoclax, Remission Induction, Myeloid leukemia, Induction chemotherapy, Hematology, Middle Aged, Bridged Bicyclo Compounds, Heterocyclic, Prognosis, medicine.disease, Clinical trial, Leukemia, Myeloid, Acute, Leukemia, Regimen, Treatment Outcome, medicine.anatomical_structure, chemistry, Female, business, Follow-Up Studies, medicine.drug
Abstract

Venetoclax is approved for older untreated acute myeloid leukemia (AML) patients. Venetoclax was available prior to approval off-label. We assessed our single-institution off-label experience with venetoclax/azacitidine, comparing outcomes with a clinical trial cohort that administered this regimen at the same institution. Thirty-three untreated AML patients unfit or unwilling to receive induction chemotherapy and prescribed venetoclax/azacitidine off-trial were retrospectively analyzed and compared with 33 patients who received the same therapy on trial. Outcomes were compared, and comparisons were made to a theoretical scenario in which off-trial patients received induction. Digital droplet polymerase chain reaction evaluated measurable residual disease (MRD). Off-trial venetoclax was attainable in nearly all patients for whom this was desired. The complete remission (CR)/CR with incomplete blood count recovery rate was 63.3% for off-trial patients who received treatment and 84.9% for trial patients (P = .081). The median overall survival for off-trial patients who received treatment was 381 days (95% confidence interval [CI], 174, not reached) vs 880 days (95% CI, 384, not reached) for trial patients (P = .041). Prior exposure to hypomethylating agents was associated with worse outcomes. Response rates with venetoclax/azacitidine were not inferior to a theoretical scenario in which patients received induction, and early death rates were less than expected with induction. MRD negativity was achievable. Newly diagnosed AML patients treated in a “real-world” scenario with off-trial venetoclax/azacitidine had inferior outcomes compared with patients treated in the setting of a clinical trial. Additionally, this therapy may be as effective, and less toxic, when compared with induction chemotherapy.

Published
2019

69. Targeting Glutamine Metabolism and Redox State for Leukemia Therapy

Author

Sarah Gehrke, Hae J. Park, Vadym Zaberezhnyy, James DeGregori, Kirk C. Hansen, Biniam Adane, Mark A. Gregory, Angelo D'Alessandro, Craig T. Jordan, and Travis Nemkov

Subjects
0301 basic medicine, Cancer Research, Myeloid, Cell Survival, Glutamine, Antineoplastic Agents, Apoptosis, Mice, Transgenic, Article, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cell Line, Tumor, hemic and lymphatic diseases, medicine, Animals, Humans, Molecular Targeted Therapy, Arsenic trioxide, neoplasms, Cell Proliferation, Leukemia, Chemistry, Glutaminase, Myeloid leukemia, medicine.disease, Xenograft Model Antitumor Assays, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Homoharringtonine, Cancer research, Energy Metabolism, Reactive Oxygen Species, Oxidation-Reduction
Abstract

Purpose: Acute myeloid leukemia (AML) is a hematologic malignancy characterized by the accumulation of immature myeloid precursor cells. AML is poorly responsive to conventional chemotherapy and a diagnosis of AML is usually fatal. More effective and less toxic forms of therapy are desperately needed. AML cells are known to be highly dependent on the amino acid glutamine for their survival. These studies were directed at determining the effects of glutaminase inhibition on metabolism in AML and identifying general weaknesses that can be exploited therapeutically. Experimental Design: AML cancer cell lines, primary AML cells, and mouse models of AML and acute lymphoblastic leukemia (ALL) were utilized. Results: We show that blocking glutamine metabolism through the use of a glutaminase inhibitor (CB-839) significantly impairs antioxidant glutathione production in multiple types of AML, resulting in accretion of mitochondrial reactive oxygen species (mitoROS) and apoptotic cell death. Moreover, glutaminase inhibition makes AML cells susceptible to adjuvant drugs that further perturb mitochondrial redox state, such as arsenic trioxide (ATO) and homoharringtonine (HHT). Indeed, the combination of ATO or HHT with CB-839 exacerbates mitoROS and apoptosis, and leads to more complete cell death in AML cell lines, primary AML patient samples, and in vivo using mouse models of AML. In addition, these redox-targeted combination therapies are effective in eradicating ALL cells in vitro and in vivo. Conclusions: Targeting glutamine metabolism in combination with drugs that perturb mitochondrial redox state represents an effective and potentially widely applicable therapeutic strategy for treating multiple types of leukemia.

Published
2019

70. Sequential azacitidine and lenalidomide for patients with relapsed and refractory acute myeloid leukemia: Clinical results and predictive modeling using computational analysis

Author

Shireen Vali, Diana Abbott, Andrew Hammes, Derek Schatz, Gregory Hemenway, Neeraj Kumar Singh, Clayton A. Smith, Taher Abbasi, Brett M. Stevens, Jonathan A. Gutman, Daniel A. Pollyea, Craig T. Jordan, Christopher R. Cogle, Aaron Fullerton, Amanda Winters, Nicholas Miltgen, Qi Wei, and Leylah Drusbosky

Subjects
Adult, Male, Oncology, Cancer Research, medicine.medical_specialty, Adolescent, Azacitidine, Phases of clinical research, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Refractory, Predictive Value of Tests, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Clinical endpoint, Humans, Lenalidomide, Aged, Retrospective Studies, Aged, 80 and over, Salvage Therapy, business.industry, Mortality rate, Computational Biology, Myeloid leukemia, Hematology, Middle Aged, Survival Rate, Leukemia, Myeloid, Acute, Regimen, Drug Resistance, Neoplasm, Myelodysplastic Syndromes, 030220 oncology & carcinogenesis, Female, Neoplasm Recurrence, Local, business, Follow-Up Studies, 030215 immunology, medicine.drug
Abstract

Background Patients with relapsed and refractory (R/R) acute myeloid leukemia (AML) have limited treatment options. Genomically-defined personalized therapies are only applicable for a minority of patients. Therapies without identifiable targets can be effective but patient selection is challenging. The sequential combination of azacitidine with high-dose lenalidomide has shown activity; we aimed to determine the efficacy of this genomically-agnostic regimen in patients with R/R AML, with the intention of applying sophisticated methods to predict responders. Methods Thirty-seven R/R AML/myelodysplastic syndrome patients were enrolled in a phase 2 study of azacitidine with lenalidomide. The primary endpoint was complete remission (CR) and CR with incomplete blood count recovery (CRi) rate. A computational biological modeling (CBM) approach was applied retrospectively to predict outcomes based on the understood mechanisms of azacitidine and lenalidomide in the setting of each patients’ disease. Findings Four of 37 patients (11%) had a CR/CRi; the study failed to meet the alternative hypothesis. Significant toxicity was observed in some cases, with three treatment-related deaths and a 30-day mortality rate of 14%. However, the CBM method predicted responses in 83% of evaluable patients, with a positive and negative predictive value of 80% and 89%, respectively. Interpretation Sequential azacitidine and high-dose lenalidomide is effective in a minority of R/R AML patients; it may be possible to predict responders at the time of diagnosis using a CBM approach. More efforts to predict responses in non-targeted therapies should be made, to spare toxicity in patients unlikely to respond and maximize treatments for those with limited options.

Published
2019

71. Why are hypomethylating agents or low-dose cytarabine and venetoclax so effective?

Author

Daniel A. Pollyea and Craig T. Jordan

Subjects
0301 basic medicine, Drug, Oncology, medicine.medical_specialty, Myeloid, media_common.quotation_subject, Low dose cytarabine, Newly diagnosed, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Bridged Bicyclo Compounds, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, media_common, Sulfonamides, Dose-Response Relationship, Drug, Venetoclax, business.industry, Cytarabine, Myeloid leukemia, Hematology, Bridged Bicyclo Compounds, Heterocyclic, medicine.disease, Leukemia, Myeloid, Acute, Leukemia, 030104 developmental biology, medicine.anatomical_structure, chemistry, Neoplastic Stem Cells, business, 030215 immunology
Abstract

Venetoclax with backbone therapies have shown promising efficacy for newly diagnosed, previously untreated, older, unfit acute myeloid leukemia patients. This review discusses this data and potential reasons for the efficacy of these venetoclax-based combinations.Venetoclax with hypomethylators and low-dose cytarabine have resulted in high response rates, promising response durations, and significant overall survival in relatively small, uncontrolled studies. There is emerging data that these responses are due to the effective targeting of leukemia stem cells through an alteration of the metabolic environment that is poorly tolerated by this population.Venetoclax with a backbone therapy in older, untreated patients with acute myeloid leukemia has shown promising efficacy in preliminary clinical trials, and at least partially works through a novel mechanism that can target the leukemia stem cell population. Future investigations will help elucidate the mechanism and the contributions being made by each agent in the regimen.

Published
2019

72. Abstract 3956: MYC inhibition overcomes IMiD resistance in heterogeneous multiple myeloma populations

Author

Lorraine N. Davis, Zachary J. Walker, Denis Ohlstrom, Brett M. Stevens, Peter A. Forsberg, Tomer M. Mark, Craig T. Jordan, and Daniel W. Sherbenou

Subjects
Cancer Research, Oncology
Abstract

Introduction: Multiple myeloma (MM) is a plasma cell malignancy that remains incurable, with patients enduring multiple relapses and development of drug resistance. Immunomodulatory drugs (IMiDs) are critical anti-MM agents. IMiDs act by inducing CRBN-dependent proteasomal degradation of the transcription factors IKZF1 and IKZF3, which leads to IRF4 and MYC downregulation (collectively termed the “Ikaros axis”). Although CRBN aberrations occur, whether they are a functional mechanism of resistance in patients remains unclear. Based on the importance of CRBN in IMiD response, we hypothesized that IMiD treatment fails to downregulate the Ikaros axis in IMiD-resistant MM cells. Methods: To measure IMiD-induced Ikaros axis downregulation, we designed an intracellular flow cytometry assay that measured relative IKZF1, IKZF3, IRF4 and MYC protein levels in MM cells following ex vivo pomalidomide (Pom) treatment. We established this assay using IMiD-sensitive parental and dose-escalated Pom resistant MM1S and H929 cell lines before utilizing it in patient samples (isolated mononuclear cells). To assess the Ikaros axis in the context of MM intratumoral heterogeneity, we used mass cytometry to simultaneously characterize MM subpopulations in patient samples. Lastly, we determined ex vivo drug sensitivity in patient samples via flow cytometry. Results: Our hypothesis was supported in MM cell lines, as sensitive parental lines showed a significant decrease in all Ikaros axis protein levels following Pom treatment, while resistant lines showed no IMiD-induced decrease in any Ikaros axis protein. However, when assessed in CD38+CD138+ cells from patient samples, Pom treatment caused a significant decrease in IKZF1, IKZF3 and IRF4 regardless of IMiD sensitivity. Mass cytometry in patient samples revealed that individual Ikaros axis proteins were differentially expressed between subpopulations. When correlating this with ex vivo Pom sensitivity of MM subpopulations, we observed that low IKZF1 and IKZF3 corresponded to Pom resistance. Interestingly, most of these resistant populations still expressed MYC. We therefore assessed whether IMiD resistant MM was MYC dependent by treating Pom resistant MM cells with MYCi975. In 88% (7/8) of patient samples tested, IMiD resistant MM cells were sensitive to MYC inhibition. Conclusions: Our findings did not support our initial hypothesis, as IMiD-induced IKZF1 and IKZF3 degradation remains intact in IMiD resistant MM cells from patient samples. However, our data support a mechanism where the Ikaros axis no longer drives MYC expression in IMiD-resistant MM. Therefore, we propose that the critical mediator of IMiD resistance is conversion to a cell state where MYC expression is Ikaros axis independent. This suggests targeting MYC directly or via the as yet uncharacterized mechanism controlling MYC may be an effective strategy to eradicate IMiD resistant MM. Citation Format: Lorraine N. Davis, Zachary J. Walker, Denis Ohlstrom, Brett M. Stevens, Peter A. Forsberg, Tomer M. Mark, Craig T. Jordan, Daniel W. Sherbenou. MYC inhibition overcomes IMiD resistance in heterogeneous multiple myeloma populations [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2022; 2022 Apr 8-13. Philadelphia (PA): AACR; Cancer Res 2022;82(12_Suppl):Abstract nr 3956.

Published
2022

73. Microvasculature-on-a-Chip: Bridging the interstitial blood-lymph interface via mechanobiological stimuli

Author

Barbara Bachmann, Heinz Redl, Haddadi Sisakht B, Sarah Spitz, Wolfgang Holnthoner, Wanzenboeck Hd, Michael Harasek, Craig T. Jordan, Patrick Schuller, and Peter Ertl

Subjects
Immune system, Lymphatic system, medicine.anatomical_structure, Interstitial space, Chemistry, In vivo, Drug delivery, Cell, medicine, Lymph, Interstitial fluid flow, Cell biology
Abstract

After decades of simply being referred to as the body’s sewage system, the lymphatic system has recently been recognized as a key player in numerous physiological and pathological processes. As an essential site of immune cell interactions, the lymphatic system is a potential target for next-generation drug delivery approaches in treatments for cancer, infections, and inflammatory diseases. However, the lack of cell-based assays capable of recapitulating the required biological complexity combined with unreliable in vivo animal models currently hamper scientific progress in lymph-targeted drug delivery. To gain more in-depth insight into the blood-lymph interface, we established an advanced chip-based microvascular model to study mechanical stimulation’s importance on lymphatic sprout formation. Our microvascular model’s key feature is the co-cultivation of spatially separated 3D blood and lymphatic vessels under controlled, unidirectional interstitial fluid flow while allowing signaling molecule exchange similar to the in vivo situation. We demonstrate that our microphysiological model recreates biomimetic interstitial fluid flow, mimicking the route of fluid in vivo, where shear stress within blood vessels pushes fluid into the interstitial space, which is subsequently transported to the nearby lymphatic capillaries. Results of our cell culture optimization study clearly show an increased vessel sprouting number, length, and morphological characteristics under dynamic cultivation conditions and physiological relevant mechanobiological stimulation. For the first time, a microvascular on-chip system incorporating microcapillaries of both blood and lymphatic origin in vitro recapitulates the interstitial blood-lymph interface.

Published
2021

74. Enriching for human acute myeloid leukemia stem cells using reactive oxygen species-based cell sorting

Author

Craig T. Jordan, Courtney L. Jones, Cristiana O’Brien, and Brett M. Stevens

Subjects
Mice, SCID, Stem cells, Biology, General Biochemistry, Genetics and Molecular Biology, Mice, Antigen, Mice, Inbred NOD, Protocol, medicine, Animals, Humans, lcsh:Science (General), Cancer, chemistry.chemical_classification, Reactive oxygen species, General Immunology and Microbiology, General Neuroscience, Myeloid leukemia, Cell sorting, Flow Cytometry, medicine.disease, Leukemia, Myeloid, Acute, Leukemia, Metabolism, chemistry, Neoplastic Stem Cells, Cancer research, Stem cell, Reactive Oxygen Species, Flow cytometry/mass cytometry, lcsh:Q1-390
Abstract

Summary Isolation of leukemia stem cells presents a challenge due to the heterogeneity of the immunophenotypic markers commonly used to identify blood stem cells. Several studies have reported that relative levels of reactive oxygen species (ROS) can be used to enrich for stem cell populations, suggesting a potential alternative to surface antigen-based methods. Here, we describe a protocol to enrich for stem cells from human acute myeloid leukemia specimens using relative levels of ROS. This protocol provides consistent enrichment of leukemia stem cells. For complete details on the use and execution of this protocol, please refer to Lagadinou et al. (2013) and Pei et al. (2018)., Graphical abstract, Highlights • Low levels of reactive oxygen species are a hallmark of stem cells • Relative levels of reactive oxygen species allow for enrichment of leukemia stem cells • This protocol is an alternative to surface antigen-based methods, Isolation of leukemia stem cells presents a challenge due to the heterogeneity of the immunophenotypic markers commonly used to identify blood stem cells. Several studies have reported that relative levels of reactive oxygen species (ROS) can be used to enrich for stem cell populations, suggesting a potential alternative to surface antigen-based methods. Here, we describe a protocol to enrich for stem cells from human acute myeloid leukemia specimens using relative levels of ROS. This protocol provides consistent enrichment of leukemia stem cells.

Published
2021

75. MERTK inhibition alters the PD-1 axis and promotes anti-leukemia immunity

Author

Douglas K. Graham, Lauren S. Page, Rebecca E. Parker, Madeline G. Huey, Curtis J. Henry, Deborah DeRyckere, H. Shelton Earp, Kristen M. Jacobsen, Stephen V. Frye, Alisa B. Lee-Sherick, Amanda A. Hill, Craig T. Jordan, and Xiaodong Wang

Subjects
0301 basic medicine, CD4-Positive T-Lymphocytes, medicine.drug_class, medicine.medical_treatment, Programmed Cell Death 1 Receptor, Context (language use), CD8-Positive T-Lymphocytes, Tyrosine-kinase inhibitor, Monocytes, 03 medical and health sciences, Mice, 0302 clinical medicine, Cancer immunotherapy, Cell Line, Tumor, medicine, Tumor Microenvironment, Animals, Humans, Protein Kinase Inhibitors, biology, c-Mer Tyrosine Kinase, Chemistry, Macrophages, FOXP3, Forkhead Transcription Factors, General Medicine, MERTK, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, Mice, Inbred C57BL, Leukemia, 030104 developmental biology, Integrin alpha M, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Medicine, Immunotherapy, Corrigendum, CD8, Gene Deletion, Research Article
Abstract

MERTK is ectopically expressed and promotes survival in acute lymphoblastic leukemia (ALL) cells and is thus a potential therapeutic target. Here we demonstrate both direct therapeutic effects of MERTK inhibition on leukemia cells and induction of anti-leukemia immunity via suppression of the coinhibitory PD-1 axis. A MERTK-selective tyrosine kinase inhibitor, MRX-2843, mediated therapeutic anti-leukemia effects in immunocompromised mice bearing a MERTK-expressing human leukemia xenograft. In addition, inhibition of host MERTK by genetic deletion (Mertk-/- mice) or treatment with MRX-2843 significantly decreased tumor burden and prolonged survival in immune-competent mice inoculated with a MERTK-negative ALL, suggesting immune-mediated therapeutic activity. In this context, MERTK inhibition led to significant decreases in expression of the coinhibitory ligands PD-L1 and PD-L2 on CD11b+ monocytes/macrophages in the leukemia microenvironment. Furthermore, although T cells do not express MERTK, inhibition of MERTK indirectly decreased PD-1 expression on CD4+ and CD8+ T cells and decreased the incidence of splenic FOXP3+ Tregs at sites of leukemic infiltration, leading to increased T cell activation. These data demonstrate direct and immune-mediated therapeutic activities in response to MERTK inhibition in ALL models and provide validation of a translational agent targeting MERTK for modulation of tumor immunity.

Published
2020

76. Exploiting Protein Translation Dependence in Multiple Myeloma with Omacetaxine-based Therapy

Author

Denis Ohlstrom, Peter A. Forsberg, Lorraine N Davis, Daniel W. Sherbenou, Zachary J. Walker, Andrew Hammes, Beau M Idler, Craig T. Jordan, Tomer M Mark, Michael J VanWyngarden, Clayton A. Smith, Brett M. Stevens, and Shelby C. Bearrows

Subjects
0301 basic medicine, Cancer Research, Primary Cell Culture, Article, Proto-Oncogene Proteins c-myc, 03 medical and health sciences, Immunomodulating Agents, Mice, 0302 clinical medicine, In vivo, Bone Marrow, Antineoplastic Combined Chemotherapy Protocols, medicine, Tumor Cells, Cultured, Animals, Humans, Multiple myeloma, Protein Synthesis Inhibitors, business.industry, Daratumumab, Drug Synergism, medicine.disease, Xenograft Model Antitumor Assays, Chimeric antigen receptor, 030104 developmental biology, Oncology, Proteasome, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Protein Biosynthesis, Interferon Regulatory Factors, Cancer research, Biomarker (medicine), Drug Screening Assays, Antitumor, business, Homoharringtonine, Multiple Myeloma, Ex vivo, IRF4, Signal Transduction
Abstract

Purpose:The prognosis of patients with multiple myeloma who are resistant to proteasome inhibitors, immunomodulatory drugs (IMiD), and daratumumab is extremely poor. Even B-cell maturation antigen–specific chimeric antigen receptor T-cell therapies provide only a temporary benefit before patients succumb to their disease. In this article, we interrogate the unique sensitivity of multiple myeloma cells to the alternative strategy of blocking protein translation with omacetaxine.Experimental Design:We determined protein translation levels (n = 17) and sensitivity to omacetaxine (n = 51) of primary multiple myeloma patient samples. Synergy was evaluated between omacetaxine and IMiDs in vitro, ex vivo, and in vivo. Underlying mechanism was investigated via proteomic analysis.Results:Almost universally, primary patient multiple myeloma cells exhibit >2.5-fold increased rates of protein translation compared with normal marrow cells. Ex vivo treatment with omacetaxine resulted in >50% reduction in viable multiple myeloma cells. In this cohort, high levels of translation serve as a biomarker for patient multiple myeloma cell sensitivity to omacetaxine. Unexpectedly, omacetaxine demonstrated synergy with IMiDs in multiple myeloma cell lines in vitro. In addition, in an IMiD-resistant relapsed patient sample, omacetaxine/IMiD combination treatment resensitized the multiple myeloma cells to the IMiD. Proteomic analysis found that the omacetaxine/IMiD combination treatment produced a double-hit on the IRF4/c-MYC pathway, which is critical to multiple myeloma survival.Conclusions:Overall, protein translation inhibitors represent a potential new drug class for myeloma treatment and provide a rationale for conducting clinical trials with omacetaxine alone and in combination with IMiDs for patients with relapsed/refractory multiple myeloma.

Published
2020

77. ETV6 germline mutations cause HDAC3/NCOR2 mislocalization and upregulation of interferon response genes

Author

Courtney L. Jones, Craig T. Jordan, Michael U. Callaghan, Jesse W. Rowley, Jorge Di Paola, Gregory Kirkpatrick, Joy M. Fulbright, Madhvi Rajpurkar, Brett M. Stevens, Eric M. Pietras, Marlie H. Fisher, Kenneth Jones, Christopher C. Porter, Arthur Gutierrez-Hartmann, and Megan A. Cooper

Subjects
0301 basic medicine, Repressor, Biology, Histone Deacetylases, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Downregulation and upregulation, Megakaryocyte, medicine, Humans, Genetic Predisposition to Disease, Nuclear Receptor Co-Repressor 2, Child, Transcription factor, Gene, Bone Marrow Diseases, Germ-Line Mutation, Proto-Oncogene Proteins c-ets, General Medicine, Hematology, Thrombocytopenia, Repressor Proteins, ETV6, Haematopoiesis, Protein Transport, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Interferon Regulatory Factors, Cancer research, Medicine, Transcription, Megakaryocytes, Research Article
Abstract

ETV6 is an ETS family transcription factor that plays a key role in hematopoiesis and megakaryocyte development. Our group and others have identified germline mutations in ETV6 resulting in autosomal dominant thrombocytopenia and predisposition to malignancy; however, molecular mechanisms defining the role of ETV6 in megakaryocyte development have not been well established. Using a combination of molecular, biochemical, and sequencing approaches in patient-derived PBMCs, we demonstrate abnormal cytoplasmic localization of ETV6 and the HDAC3/NCOR2 repressor complex that led to overexpression of HDAC3-regulated interferon response genes. This transcriptional dysregulation was also reflected in patient-derived platelet transcripts and drove aberrant proplatelet formation in megakaryocytes. Our results suggest that aberrant transcription may predispose patients with ETV6 mutations to bone marrow inflammation, dysplasia, and megakaryocyte dysfunction., Germline mutations in transcription factor ETV6 cause cytoplasmic localization of the HDAC3/NCOR2 complex, substantively altering the transcriptional signature of blood cells.

Published
2020

78. Nicotinamide Metabolism Mediates Resistance to Venetoclax in Relapsed Acute Myeloid Leukemia Stem Cells

Author

Rachel Culp-Hill, Mohammad Minhajuddin, Daniel A. Pollyea, Diana Abbott, Anagha Inguva, Shanshan Pei, Travis Nemkov, Amanda Winters, Michael W. Becker, Fabia Gamboni, Angelo D'Alessandro, Sarah Gehrke, Clayton A. Smith, Annika Gustafson, James DeGregori, Brett M. Stevens, Haobin Ye, Julie A. Reisz, Anna Krug, Maria L. Amaya, Courtney L. Jones, and Craig T. Jordan

Subjects
Niacinamide, Azacitidine, Nicotinamide phosphoribosyltransferase, Biology, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Genetics, medicine, Humans, 030304 developmental biology, 0303 health sciences, Sulfonamides, Nicotinamide, Venetoclax, Stem Cells, Myeloid leukemia, Cell Biology, medicine.disease, Bridged Bicyclo Compounds, Heterocyclic, Leukemia, Haematopoiesis, Leukemia, Myeloid, Acute, chemistry, Cancer research, Neoplastic Stem Cells, Molecular Medicine, Stem cell, 030217 neurology & neurosurgery, medicine.drug
Abstract

We previously demonstrated that leukemia stem cells (LSCs) in de novo acute myeloid leukemia (AML) patients are selectively reliant on amino acid metabolism and that treatment with the combination of venetoclax and azacitidine (ven/aza) inhibits amino acid metabolism, leading to cell death. In contrast, ven/aza fails to eradicate LSCs in relapsed/refractory (R/R) patients, suggesting altered metabolic properties. Detailed metabolomic analysis revealed elevated nicotinamide metabolism in relapsed LSCs, which activates both amino acid metabolism and fatty acid oxidation to drive OXPHOS, thereby providing a means for LSCs to circumvent the cytotoxic effects of ven/aza therapy. Genetic and pharmacological inhibition of nicotinamide phosphoribosyltransferase (NAMPT), the rate-limiting enzyme in nicotinamide metabolism, demonstrated selective eradication of R/R LSCs while sparing normal hematopoietic stem/progenitor cells. Altogether, these findings demonstrate that elevated nicotinamide metabolism is both the mechanistic basis for ven/aza resistance and a metabolic vulnerability of R/R LSCs.

Published
2020

79. PU.1 enforces quiescence and limits hematopoietic stem cell expansion during inflammatory stress

Author

Zhonghe Ke, James DeGregori, Jason R. Myers, Robert S. Welner, Eric M. Pietras, Rachel L Gessner, Kelly C. Higa, Dirk Loeffler, Craig T. Jordan, Hideaki Nakajima, Beau M Idler, Taylor S. Mills, Jennifer L. Rabe, Giovanny Hernandez, Nouraiz Ahmed, John M. Ashton, Brett M. Stevens, James S. Chavez, Timm Schroeder, and Hyunmin Kim

Subjects
Hematopoietic stem cell, Inflammation, Cell cycle, Biology, medicine.disease_cause, medicine.disease, Cell Cycle Gene, Cell biology, Leukemia, medicine.anatomical_structure, medicine, medicine.symptom, Carcinogenesis, Psychological repression, Homeostasis
Abstract

SummaryLoss of hematopoietic stem cell (HSC) quiescence and resulting clonal expansion are common initiating events in the development of hematological malignancy. Likewise, chronic inflammation related to aging, disease and/or tissue damage is associated with leukemia progression, though its role in oncogenesis is not clearly defined. Here, we show that PU.1-dependent repression of protein synthesis and cell cycle genes in HSC enforces homeostatic protein synthesis levels and HSC quiescence in response to IL-1 stimulation. These genes are constitutively de-repressed in PU.1-deficient HSC, leading to activation of protein synthesis, loss of quiescence and aberrant expansion of HSC. Taken together, our data identify a mechanism whereby HSC regulate their cell cycle activity and pool size in response to chronic inflammatory stress.

Published
2020

80. Delivery of a model lipophilic membrane cargo to bone marrow via cell-derived microparticles

Author

Ping Ren, Chunyan Yang, Dmitri Simberg, Robert I. Scheinman, Hanmant Gaikwad, Craig T. Jordan, Laren A. Lofchy, Fangfang Chen, Jingshi Shen, Chun Wan, Guankui Wang, and J Ponder

Subjects
Cell- and Tissue-Based Therapy, Pharmaceutical Science, Bone Marrow Cells, 02 engineering and technology, Jurkat cells, Article, Flow cytometry, Cell-Derived Microparticles, 03 medical and health sciences, Mice, Bone Marrow, medicine, Animals, Progenitor cell, 030304 developmental biology, 0303 health sciences, medicine.diagnostic_test, Chemistry, 021001 nanoscience & nanotechnology, medicine.disease, Flow Cytometry, Molecular biology, Leukemia, Haematopoiesis, medicine.anatomical_structure, Cell culture, Bone marrow, 0210 nano-technology
Abstract

Bone marrow (BM) is the central immunological organ and the origin of hematological diseases. Efficient and specific drug delivery to the BM is an unmet need. We tested delivery of fluorescent indocarbocyanine lipids (ICLs, DiR, DiD, DiI) as a model lipophilic cargo, via different carriers. Systemically injected T-lymphocyte cell line Jurkat delivered ICLs to the BM more efficiently than erythrocytes, and more selectively than PEGylated liposomes. Near infrared imaging showed that the delivery was restricted to the BM, lungs, liver and spleen, with no accumulation in the kidneys, brain, heart, intestines, fat tissue and pancreas. Following systemic injection of ICL-labeled cells in immunodeficient or immunocompetent mice, few cells arrived in the BM intact. However, between 5 and 10% of BM cells were ICL-positive. Confocal microscopy of intact BM confirmed that ICLs are delivered independently of the injected cells. Flow cytometry analysis showed that the lipid accumulated in both CD11b + and CD11b- cells, and in hematopoietic progenitors. In a xenograft model of acute myeloid leukemia, a single injection of 10 million Jurkat cells delivered DiD to ~15% of the tumor cells. ICL-labeled cells disappeared from blood almost immediately post-intravenous injection, but numerous cell-derived microparticles continued to circulate in blood. The microparticle particle formation was not due to the ICL labeling or complement attack and was observed after injection of both syngeneic and xenogeneic cells. Injection of microparticles produced in vitro from Jurkat cells resulted in a similar ICL delivery as the injection of intact Jurkat cells. Our results demonstrate a novel delivery paradigm wherein systemically injected cells release microparticles that accumulate in the BM. In addition, the results have important implications for studies involving systemically administered cell therapies.

Published
2020

81. Substituted oxindol-3-ylidenes as AMP-activated protein kinase (AMPK) inhibitors

Author

Philip Reigan, Donald S. Backos, Mohammed Minhajuddin, Christopher J. Matheson, Kimberly A. Casalvieri, and Craig T. Jordan

Subjects
Cell Survival, Antineoplastic Agents, AMP-Activated Protein Kinases, 01 natural sciences, Article, 03 medical and health sciences, chemistry.chemical_compound, AMP-activated protein kinase, Drug Discovery, Structure–activity relationship, Humans, Oxindole, Protein kinase A, Protein Kinase Inhibitors, 030304 developmental biology, Pharmacology, 0303 health sciences, biology, 010405 organic chemistry, Kinase, Organic Chemistry, AMPK, General Medicine, 0104 chemical sciences, Cell biology, Oxindoles, Molecular Docking Simulation, chemistry, biology.protein, Phosphorylation, Drug Screening Assays, Antitumor, K562 Cells, Tyrosine kinase, Protein Binding
Abstract

AMP-activated protein kinase (AMPK) is a central metabolic regulator that promotes cancer growth and survival under hypoxia and plays a role in the maintenance of cancer stem cells. A major challenge to interrogating the potential of targeting AMPK in cancer is the lack of potent and selective small molecule inhibitors. Compound C has been widely used as an AMPK inhibitor, but it lacks potency and has a poor selectivity profile. The multi-kinase inhibitor, sunitinib, has demonstrated potent nanomolar inhibition of AMPK activity and has scope for modification. Here, we have designed and synthesized several series of oxindoles to determine the structural requirements for AMPK inhibition and to improve selectivity. We identified two potent, novel oxindole-based AMPK inhibitors that were designed to interact with the DFG motif in the ATP-binding site of AMPK, this key feature evades interaction with the common recptor tyrosine kinase targets of sunitinib. Cellular engagement of AMPK by these oxindoles was confirmed by the inhibition of phosphorylation of acetyl-CoA carboxylase (ACC), a known substrate of AMPK, in myeloid leukemia cells. Interestingly, although AMPK is highly expressed and activated in K562 cells these oxindole-based AMPK inhibitors did not impact cell viability or result in significant cytotoxicity. Our studies serve as a platform for the further development of oxindole-based AMPK inhibitors with therapeutic potential.

Published
2020

82. The Hepatic Microenvironment Uniquely Protects Leukemia Cells through Induction of Growth and Survival Pathways Mediated by LIPG

Author

Brett M. Stevens, H. Leighton Grimes, Anagha Inguva, Erik De Bloois, Angelo D'Alessandro, Uwe Christians, Daniel A. Pollyea, Haobin Ye, Chih-Hsing Chou, Jessica Ponder, Anna Krug, Mohammad Minhajuddin, Björn Schniedewind, Shanshan Pei, Rachel Culp-Hill, Craig T. Jordan, and Maria L. Amaya

Subjects
0301 basic medicine, Endothelial lipase, medicine.medical_treatment, Disease, Biology, Article, Pathogenesis, 03 medical and health sciences, Mice, 0302 clinical medicine, medicine, Tumor Microenvironment, Animals, Humans, Cell Proliferation, chemistry.chemical_classification, Chemotherapy, Leukemia, Lipase, medicine.disease, Survival pathways, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Enzyme, Oncology, chemistry, Liver, 030220 oncology & carcinogenesis, Cancer research, Infiltration (medical)
Abstract

Due to the disseminated nature of leukemia, malignant cells are exposed to many different tissue microenvironments, including a variety of extramedullary sites. In the present study, we demonstrate that leukemic cells residing in the liver display unique biological properties and also contribute to systemic changes that influence physiologic responses to chemotherapy. Specifically, the liver microenvironment induces metabolic adaptations via upregulating expression of endothelial lipase in leukemia cells, which not only stimulates tumor cell proliferation through polyunsaturated fatty acid–mediated pathways, but also promotes survival by stabilizing antiapoptotic proteins. Additionally, hepatic infiltration and tissue damage caused by malignant cells induces release of liver-derived enzymes capable of degrading chemotherapy drugs, an event that further protects leukemia cells from conventional therapies. Together, these studies demonstrate a unique role for liver in modulating the pathogenesis of leukemic disease and suggest that the hepatic microenvironment may protect leukemia cells from chemotherapeutic challenge. Significance: The studies presented herein demonstrate that the liver provides a microenvironment in which leukemia cells acquire unique metabolic properties. The adaptations that occur in the liver confer increased resistance to chemotherapy. Therefore, we propose that therapies designed to overcome liver-specific metabolic changes will yield improved outcomes for patients with leukemia. This article is highlighted in the In This Issue feature, p. 211

Published
2020

83. Measurement of ex vivo resistance to proteasome inhibitors, IMiDs, and daratumumab during multiple myeloma progression

Author

Brett M. Stevens, Daniel W. Sherbenou, Tomer M Mark, Andrew Hammes, Michael J VanWyngarden, Diana Abbott, Peter A. Forsberg, Christophe J. Langouët-Astrié, Craig T. Jordan, Zachary J. Walker, Clayton A. Smith, and Brent E. Palmer

Subjects
Drug, Oncology, medicine.medical_specialty, Lymphoid Neoplasia, business.industry, media_common.quotation_subject, Daratumumab, Antibodies, Monoclonal, Hematology, Drug resistance, medicine.disease, medicine.anatomical_structure, Internal medicine, medicine, Humans, Bone marrow, Viability assay, Neoplasm Recurrence, Local, business, Multiple Myeloma, Proteasome Inhibitors, Multiple myeloma, Whole Bone Marrow, Ex vivo, media_common
Abstract

The oncogenic drivers and progression factors in multiple myeloma (MM) are heterogeneous and difficult to target therapeutically. Many different MM drugs have emerged, however, that attack various phenotypic aspects of malignant plasma cells. These drugs are administered in numerous, seemingly interchangeable combinations. Although the availability of many treatment options is useful, no clinical test capable of optimizing and sequencing the treatment regimens for an individual patient is currently available. To overcome this problem, we developed a functional ex vivo approach to measure patients’ inherent and acquired drug resistance. This method, which we termed myeloma drug sensitivity testing (My-DST), uses unselected bone marrow mononuclear cells with a panel of drugs in clinical use, followed by flow cytometry to measure myeloma-specific cytotoxicity. We found that using whole bone marrow cultures helped preserve primary MM cell viability. My-DST was used to profile 55 primary samples at diagnosis or at relapse. Sensitivity or resistance to each drug was determined from the change in MM viability relative to untreated control samples. My-DST identified progressive loss of sensitivity to immunomodulatory drugs, proteasome inhibitors, and daratumumab through the disease course, mirroring the clinical development of resistance. Prospectively, patients’ ex vivo drug sensitivity to the drugs subsequently received was sensitive and specific for clinical response. In addition, treatment with

Published
2020

84. Pro-inflammatory cytokine blockade attenuates myeloid expansion in a murine model of rheumatoid arthritis

Author

Jorge Di Paola, Michelle Zanche, Jason R. Myers, Brett M. Stevens, James S. Chavez, Susan Kuldanek, John M. Ashton, Eric M. Pietras, Giovanny Hernandez, James Hagman, Jennifer L. Rabe, Taylor S. Mills, Craig T. Jordan, V. Michael Holers, Courtney J. Fleenor, Leila Noetzli, Gregory Kirkpatrick, Kristine A. Kuhn, Widian K. Jubair, Biniam Adane, and Charles A. Dinarello

Subjects
Myeloid, medicine.medical_treatment, Inflammatory arthritis, lnfectious Diseases and Global Health Radboud Institute for Molecular Life Sciences [Radboudumc 4], Inflammation, Systemic inflammation, Autoimmune Diseases, Arthritis, Rheumatoid, Mice, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Humans, Lymphopoiesis, 030304 developmental biology, 0303 health sciences, Anakinra, business.industry, Articles, Hematology, medicine.disease, Arthritis, Experimental, Hematopoiesis, 3. Good health, Disease Models, Animal, Cytokine, medicine.anatomical_structure, Rheumatoid arthritis, Immunology, Cytokines, medicine.symptom, business, 030215 immunology, medicine.drug
Abstract

Contains fulltext : 229479.pdf (Publisher’s version ) (Open Access) Rheumatoid arthritis (RA) is a debilitating autoimmune disease characterized by chronic inflammation and progressive destruction of joint tissue. It is also characterized by aberrant blood phenotypes including anemia and suppressed lymphopoiesis that contribute to morbidity in RA patients. However, the impact of RA on hematopoietic stem cells (HSC) has not been fully elucidated. Using a collagen-induced mouse model of human RA, we identified systemic inflammation and myeloid overproduction associated with activation of a myeloid differentiation gene program in HSC. Surprisingly, despite ongoing inflammation, HSC from arthritic mice remain in a quiescent state associated with activation of a proliferation arrest gene program. Strikingly, we found that inflammatory cytokine blockade using the interleukin-1 receptor antagonist anakinra led to an attenuation of inflammatory arthritis and myeloid expansion in the bone marrow of arthritic mice. In addition, anakinra reduced expression of inflammation-driven myeloid lineage and proliferation arrest gene programs in HSC of arthritic mice. Altogether, our findings show that inflammatory cytokine blockade can contribute to normalization of hematopoiesis in the context of chronic autoimmune arthritis.

Published
2020

85. Functional genomic landscape of acute myeloid leukaemia

Author

Robert H. Collins, Deirdre Devine, Beth Wilmot, Justin Ramsdill, Erik Segerdell, Bruno C. Medeiros, Brian J. Druker, Dylan Nelson, Micaela E. Martinez, Ryan C. Johnson, Robert Schuff, Robert P. Searles, Scott Weir, James Dibb, Elie Traer, Pierrette Lo, Haijiao Zhang, Rachel Henson, Tara A. Macey, Isabel English, Cody Coblentz, Christopher A. Eide, Ceilidh Nichols, Aurora Blucher, Ryan M. Winters, David L. Wiest, Corinne Visser, Michael W. Deininger, Stephen E. Kurtz, Daniel A. Pollyea, Justin M. Watts, Amy S. Carlos, Denise C. Connolly, Andy Kaempf, Angela Rofelty, Samuel B. Luty, Rachel J. Cook, Jill Peters, Kristen Werth, Shannon K. McWeeney, Joseph Carroll, Samantha L. Savage, Ronan T. Swords, Uma Borate, Aashis Thapa, Abdusebur Jemal, Joelle Wolf, Patricia Kropf, Rebecca Smith, Tyler Sweeney, Russell T. Burke, Rachel R. Pallapati, Anna Reister Schultz, Kim Hien T. Dao, Daniel Bottomly, Cristina E. Tognon, Alexey V. Danilov, Jason M. Glover, Jason D. MacManiman, Michie Degnin, Amy Yates, Libbey White, David K. Edwards, Anupriya Agarwal, Christopher R. Cogle, Kevin Watanabe-Smith, Leylah Drusbosky, Nicola Long, Motomi Mori, Christopher S. Hourigan, Tara L. Lin, Chenwei Lin, Jacqueline Martinez, Bill H. Chang, Richie Carpenter, Stephen E. Spurgeon, Brian Junio, Marc M. Loriaux, Craig T. Jordan, Hibery Ho, Selina Qiuying Liu, Melissa L. Abel, Amanda d’Almeida, Jake Wagner, Jade Bryant, Jeffrey W. Tyner, Jessica Leonard, and Kara Johnson

Subjects
Male, 0301 basic medicine, Myeloid, Gene regulatory network, Datasets as Topic, Genomics, Computational biology, Biology, Article, DNA Methyltransferase 3A, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, Proto-Oncogene Proteins, hemic and lymphatic diseases, medicine, Humans, Exome, DNA (Cytosine-5-)-Methyltransferases, Molecular Targeted Therapy, Exome sequencing, Regulation of gene expression, Multidisciplinary, Serine-Arginine Splicing Factors, Genome, Human, Sequence Analysis, RNA, Nuclear Proteins, medicine.disease, Human genetics, 3. Good health, Gene Expression Regulation, Neoplastic, Repressor Proteins, Leukemia, Myeloid, Acute, Leukemia, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Core Binding Factor Alpha 2 Subunit, Female, Nucleophosmin
Abstract

The implementation of targeted therapies for acute myeloid leukaemia (AML) has been challenging because of the complex mutational patterns within and across patients as well as a dearth of pharmacologic agents for most mutational events. Here we report initial findings from the Beat AML programme on a cohort of 672 tumour specimens collected from 562 patients. We assessed these specimens using whole-exome sequencing, RNA sequencing and analyses of ex vivo drug sensitivity. Our data reveal mutational events that have not previously been detected in AML. We show that the response to drugs is associated with mutational status, including instances of drug sensitivity that are specific to combinatorial mutational events. Integration with RNA sequencing also revealed gene expression signatures, which predict a role for specific gene networks in the drug response. Collectively, we have generated a dataset—accessible through the Beat AML data viewer (Vizome)—that can be leveraged to address clinical, genomic, transcriptomic and functional analyses of the biology of AML. Analyses of samples from patients with acute myeloid leukaemia reveal that drug response is associated with mutational status and gene expression; the generated dataset provides a basis for future clinical and functional studies of this disease.

Published
2018

86. IL-1 Via IRAK1/4 Sustains Acute Myeloid Leukemia Stem Cells Following Treatment and Relapse

Author

Tzu-Chieh Ho, Laura M. Calvi, Michael W. Becker, Yu-Chiao Chiu, Mark W. LaMere, Naxin Guo, Jing Wang, Hiroki Kawano, Nikolay V. Dokholyan, Rakesh K. Singh, and Craig T. Jordan

Subjects
business.industry, hemic and lymphatic diseases, Immunology, Cancer research, Medicine, Myeloid leukemia, IRAK1, Cell Biology, Hematology, Stem cell, business, Biochemistry
Abstract

Current treatment options for relapsed acute myeloid leukemia (AML) are limited and ineffective for the majority of patients. In AML, primitive leukemia stem cells (LSCs) and pre-leukemic populations are able to maintain the disease and drive relapse. Thus, therapies targeting LSC populations may increase the overall survival of AML patients. In this study, we aim to identify the drivers favoring LSC expansion following treatment and relapse and develop potential therapies for AML. The transcriptome analyses of 12 pairs of functionally defined LSC fractions at diagnosis and relapse revealed significant changes of IL-1 signaling in AML patients. We demonstrated that the protein expression levels of interleukin-1 receptor type I (IL1R1) and its complex member interleukin-1 receptor accessory protein (IL1RAP) were both up-regulated in human leukemia stem and progenitor cells (LSPCs) at diagnosis or in relapse compared to normal hematopoietic stem and progenitor cells (HSPCs). Knockdown of IL1R1 and IL1RAP suppressed the clonogenicity and engraftment growth of primary human AML cells but showed low impacts on HSPCs in the normal bone marrow. Additionally, knockout of IL1R1 in leukemia MLL-AF9 mice significantly reduced the LSC frequency and prolonged the overall survival rate. To target IL-1/TLR signaling in LSCs, we performed iterative structure-activity relationship (SAR) guided medicinal chemistry, in silico modeling and leukemia cell line reporter assays to screen and identify a novel interleukin-1 receptor-associated kinase 1/4 (IRAK1/4) inhibitor (termed UR241-2). UR241-2 robustly inhibits IL-1/TLR signaling in AML cells including the activation of NF-κB following IL-1 stimulation. UR241-2 repressed LSPC function as assessed by colony-forming unit assays in primary human AML cells at diagnosis and in relapse while minimally impacting normal HSPC function. Taken together, our findings demonstrate the important role of IL-1/TLR signaling in supporting AML LSC expansion following treatment and relapse and suggest that targeting IL-1/TLR signaling using the novel IRAK1/4 inhibitor, UR241-2, can target LSC function to improve patient outcomes in AML. Disclosures No relevant conflicts of interest to declare.

Published
2021

87. Outcomes Are Similar Following Allogeneic Hematopoietic Stem Cell Transplant for Newly Diagnosed Patients Who Received Venetoclax + Azacitidine Versus Intensive Chemotherapy

Author

Jonathan A. Gutman, Craig T. Jordan, Daniel A. Pollyea, Diana Abbott, Mohd Minhajuddin, Grace Bosma, and Amanda Winters

Subjects
Oncology, medicine.medical_specialty, Venetoclax, business.industry, Immunology, Azacitidine, Cell Biology, Hematology, Newly diagnosed, Intensive chemotherapy, Biochemistry, chemistry.chemical_compound, chemistry, Internal medicine, medicine, Allogeneic hematopoietic stem cell transplant, business, health care economics and organizations, medicine.drug
Abstract

Background: Venetoclax-based therapy regimens are now FDA-approved for treatment of acute myeloid leukemia (AML) in older patients or those unfit to tolerate intensive chemotherapy (IC). Remission rates are high at 60-70% but relapses do frequently occur. Outcomes for newly-diagnosed patients who receive venetoclax-based therapies and proceed to a potentially curative allogeneic stem cell transplant (SCT) have largely been unreported. In the current study we compare outcomes of patients who received SCT following either IC or venetoclax + azacitidine (ven/aza) at the University of Colorado Hospital. Methods: Patients 18 years or older who received SCT in first remission of AML between 2010-2020 were included in the analysis. Patients were stratified into the IC arm if they initially received a backbone of cytarabine and an anthracycline; some patients in this cohort received IC in combination with other targeted agents. Patients who received ven/aza as first-line therapy followed by SCT were grouped in a separate cohort. Demographic and clinical information - including flow cytometry-based (MCF) MRD - was extracted from the electronic medical record. Comparisons of demographic and clinical variables between IC and ven/aza groups were made with t-test, Chi-squared, or Fisher's exact test depending on the nature of the variable. Relapse-free (RFS) and overall (OS) survival were calculated from the day of SCT to the respective endpoint or last documented follow-up using log-rank statistics. Finally, a Cox proportional hazards model was used to assess the interplay between variables pre- and post-SCT. P-values Results: We identified 179 patients who received SCT for AML in first remission. Of these patients, 151 received IC and 28 received ven/aza prior to SCT. Patients in the ven/aza group had higher median age than those in the IC group, as well as a higher proportion with adverse ELN genetic risk scoring. Patients in the ven/aza group received less intensive conditioning regimens. Sex, rates of MCF MRD negativity pre-BMT, incidence of severe acute or chronic GVHD, and causes of death were not significantly different between the two groups. There was no difference between the two groups in post-transplant RFS or OS (Figure 1). In a multivariate Cox model of pre-transplant variables predicting OS, the only factor that achieved significance was pre-SCT MCF MRD; the induction regimen was not a multivariate factor. Negative MCF MRD going into SCT was associated with decreased likelihood of relapse, GVHD, and death, respectively. Conclusions: In our cohort of AML patients receiving SCT, we found that ven/aza as a pre-transplant therapy yielded equivalent post-transplant outcomes compared to IC, in a population of older age and with higher ELN genetic risk. MCF MRD pre-SCT was confirmed as a key prognostic factor for post-SCT outcome. These findings support ongoing use of ven/aza as a first line therapy for elderly patients with AML as well as its exploration as a candidate therapy for younger patients. Figure 1 Figure 1. Disclosures Pollyea: Takeda: Honoraria, Membership on an entity's Board of Directors or advisory committees, Other; Aprea: Honoraria, Membership on an entity's Board of Directors or advisory committees; Kiadis: Honoraria, Membership on an entity's Board of Directors or advisory committees; Novartis: Consultancy, Honoraria, Membership on an entity's Board of Directors or advisory committees; Syndax: Honoraria, Membership on an entity's Board of Directors or advisory committees; Amgen: Honoraria; Agios: Other, Research Funding; Karyopharm: Consultancy, Honoraria, Membership on an entity's Board of Directors or advisory committees; Teva: Research Funding; AbbVie: Consultancy, Honoraria, Membership on an entity's Board of Directors or advisory committees, Research Funding; Curis, Servier: Other; Pfizer: Research Funding; Syros: Consultancy, Honoraria, Membership on an entity's Board of Directors or advisory committees; Astellas: Honoraria, Membership on an entity's Board of Directors or advisory committees; Bristol Myers Squibb: Honoraria, Membership on an entity's Board of Directors or advisory committees; Celgene: Honoraria, Other: advisory board; Foghorn: Honoraria, Membership on an entity's Board of Directors or advisory committees; Genentech: Consultancy, Honoraria, Membership on an entity's Board of Directors or advisory committees; Gilead: Consultancy, Honoraria, Other: advisory board; Jazz: Honoraria, Membership on an entity's Board of Directors or advisory committees, Other: advisory board.

Published
2021

88. Targeting MDS Stem Cells with Omacetaxine and Azacitidine for Newly Diagnosed High Grade Patients: Phase 1 Trial Results and Preliminary Mechanistic Studies

Author

Brett M. Stevens, Amanda C. Winters, Mohammad Minhajuddin, Maria L. Amaya, Christine M. McMahon, Jonathan A. Gutman, Clayton Smith, Deng Wang, Connor Adkins, Olivia Ondracek, Craig T. Jordan, and Daniel A. Pollyea

Subjects
Immunology, Cell Biology, Hematology, Biochemistry
Abstract

Background Myelodysplastic syndrome (MDS) arises from and is perpetuated by malignant stem cells. Curative therapy requires eradication of this population, but this is not achieved with currently available medical therapies. MDS stem cells possess unique molecular properties that can be therapeutically exploited, but in general these strategies have not been explored clinically. Our recent in vitro studies showed that combination treatment with the protein synthesis inhibitor omacetaxine (oma) and the hypomethylating agent (HMA) azacitidine (aza) efficiently targeted MDS stem cells with minimal impact on normal stem cells. Based on these findings we conducted a Phase 1 clinical trial for MDS patients with concomitant oma + aza (NCT03564873). Methods Patients were eligible if they had newly diagnosed MDS with ≥5% blasts. Aza was given at 75 mg/m 2 IV days 1-7 of a 28-day cycle; oma was given subcutaneously twice daily on days 1-7 of a 28-day cycle with 4 dose cohorts (0.75, 1.0 and 1.25 mg/m 2, and a de-escalation cohort of 0.5 mg/m 2). Dose escalation was based on a 3+3 design. Bone marrow biopsies occurred at baseline and day 8 and 28 of cycle 1, and at the conclusion of odd-numbered cycles. The primary endpoint was the maximum tolerated dose (MTD) of oma with aza. Responses were assessed according to 2006 IWG criteria with hematologic improvement (HI). Using pre- and post-treatment patient samples, advanced single cell techniques including mass cytometry and antibody-based single-cell RNA sequencing (CITE-Seq) were used to elucidate mechanisms of sensitivity and resistance. High sensitivity DNA sequencing techniques were used to understand clonal evolution and detect measurable residual disease (MRD). Results Nine patients were required to complete phase 1. See Table 1 for baseline characteristics. Two patients in cohort 1 experienced dose limiting toxicity (DLT) (grade 3 hypoxia and grade 3 respiratory failure). De-escalation to cohort 0 resulted in one DLT event (grade 4 GI bleed) among the six patients treated in this cohort. The MTD was established as 0.5 mg/m 2 oma days 1-7. Adverse events are detailed in Table 2. Median number of cycles was 2 (1-3). 8/9 patients achieved a marrow CR; 5 had HI. 6 patients proceeded to transplantation and none have relapsed with median time from transplant of 772 (183-1158) days. Median response duration is 587 days (29-938). 5 remain alive. MRD negativity, as measured with droplet digital PCR (sensitivity up to 0.1%), was achieved in 2 out of 4 patients measured. Both MRD negative patients had complete clearance of mutated splice factor genes; we previously showed no ability to clear these mutations (0/13 patients) using venetoclax+aza in AML (Nature Medicine (2018) 24:1859-1866). Baseline analysis of patient specimens by single cell transcriptomics demonstrates a distinct population of MDS stem cells (Figure 1A). This subset has overlapping transcriptional properties with known AML stem cell profiles as highlighted by increased geneset expression. Within the stem cell compartment, we observed up-regulation of protein synthesis pathways (Figure 1B) (e.g. KEGG ribosome pathway in MDS stem cells), indicating that oma/aza treatment may specifically target the malignant stem cell population. Subsequent studies are investigating the use of CITEseq as a means to evaluate drug response, which will provide very high resolution analyses of transcriptional signatures in MDS patients. By specifically monitoring eradication of MDS stem cells during the course of treatment, it should be possible to predict therapeutic efficacy and response duration while elucidating genes that correspond to oma/aza sensitivity and resistance. Conclusions Phase 2 of this study is ongoing; 23 newly-diagnosed high risk MDS patients will be enrolled with a primary endpoint to determine the overall response rate. In addition a ten-patient HMA failure expansion cohort will be enrolled to determine preliminary toxicity and efficacy assessments. Correlative studies will seek to determine the impact of this regimen on the MDS stem cell population and the mechanism of this impact. Figure 1 Figure 1. Disclosures McMahon: Takeda: Membership on an entity's Board of Directors or advisory committees. Smith: Syros: Research Funding; Kura: Research Funding; Argenx: Research Funding. Pollyea: Foghorn: Honoraria; Gilead: Consultancy, Honoraria; Celgene: Honoraria; Bristol Myers Squibb: Honoraria; Genentech: Consultancy, Honoraria; Jazz: Honoraria; AbbVie: Consultancy, Honoraria, Research Funding; Amgen: Honoraria; Astellas: Honoraria; Aprea: Honoraria; Karyopharm: Consultancy, Honoraria; Kiadis: Honoraria; Novartis: Consultancy, Honoraria; Syndax: Honoraria; Syros: Consultancy, Honoraria; Takeda: Honoraria; Teva: Research Funding. OffLabel Disclosure: Omacetaxine for MDS

Published
2021

89. Lysosomal Acid Lipase a (LIPA) Modulates Leukemia Stem Cell (LSC) Response to Venetoclax/TKI Combination Therapy in Blast Phase Chronic Myeloid Leukemia

Author

Craig T. Jordan, Anagha Inguva, Brett M. Stevens, Maria L. Amaya, Maura Gasparetto, Shanshan Pei, Haobin Ye, Amanda Winters, Anna Krug, Clayton A. Smith, Biniam Adane, Daniel A. Pollyea, Daniel W. Sherbenou, Mohd Minhajuddin, and Nabilah Khan

Subjects
Leukemia Stem Cell, Combination therapy, Venetoclax, business.industry, Immunology, Lysosomal Acid Lipase, Cell Biology, Hematology, Blast Phase Chronic Myeloid Leukemia, Biochemistry, chemistry.chemical_compound, chemistry, Cancer research, Medicine, business
Abstract

Chronic myeloid leukemia (CML) is a heterogeneous disease, initiated by reciprocal translocation of chromosome 9 and 22, resulting in the generation of a BCR-ABL fusion protein and constitutive activation of the ABL kinase. ABL tyrosine kinase inhibitors (TKIs) have been very successful in suppressing CML disease. However, TKIs may not eliminate leukemia stem cells (LSCs), as evidenced by the frequent re-emergence of the disease upon TKI discontinuation. Moreover, blast phase CML (bpCML) remains a formidable challenge in disease management. Recent clinical evidence suggests that the BCL2 inhibitor venetoclax (Ven) in combination with ABL-targeting tyrosine kinase inhibitors (TKI) can eradicate bpCML LSCs. However, the exact mechanism by which this combination may targets LSCs is not known. In this report, we confirm the efficacy and LSC-targeting capacity of Ven/TKI combination in preclinical models of bpCML and we further identify that inhibition of free fatty acid (FFA) mobilization pathways may provide enhanced efficacy against LSCs. To establish the efficacy of Ven/TKI combination, we treated bpCML samples with Ven+Dasatinib (Das) combination for 24h, this resulted in a significant decrease in the viability of bulk and primitive populations (CD34+, CD38+). Patient-derived xenografts of bpCML samples in NSGS-mice, were treated with Ven/Das as well as single agents. The result showed a significant decrease in leukemia burden in the combination treated group, compared to either drug alone, albeit, some resistant cells survived in the combo treated group. Furthermore, using a syngeneic mouse model of bpCML, co-expressing Bcr-Abl and Nup98-HOXA9 translocations, the mouse leukemic cells treated with Ven/Dasatinib combination demonstrated a significant loss of viability of the bulk as well as phenotypically defined LSCs (Lin-/Sca1+). Treatment of leukemic mice with Ven/Das had a significant survival benefit and remained disease free at 80 days post treatment. We also showed significant survival benefits of Ven/ponatinib in NSGS-mice harboring syngeneic bpCML cells with the T315I gatekeeper mutation. Treatment of normal mice with Ven/Das combo did not affect the colony forming ability of LSK cells from the bone marrow, indicating a leukemia-specific response. Based on these results, we conclude that Ven/TKI combination effects were due to direct targeting of the LSC population. To investigate the potential mechanism of Ven/TKI activity in LSC targeting, we performed gene expression studies using RNA-seq based methods after short term treatment. Our findings indicated that the LSC population from Ven/TKI-treated mice showed enrichment of a gene signature associated with lysosome biology. Pre-treatment of mouse leukemia cells with bafilomycin, an inhibitor of lysosome function, resulted in increased sensitivity to Ven/TKI combo. Intriguingly, we also found significant induction of lysosomal acid lipase (LIPA), an enzyme involved in the generation of free fatty acids for energy needs. Metabolomic analysis of LSCs isolated after short term treatment with Ven/TKI, showed that a number of fatty acids were up-regulated in the Ven/Das treated group compared to control. Knocking down Lipa using CRISPR technology resulted in increased sensitivity to Ven/TKI combination, whereas overexpression of Lipa resulted in decreased sensitivity to the Ven/TKI combination, implicating Lipa upregulation and a resultant increase in free fatty acids as a protective response to Ven/TKI treatment. Furthermore, knocking down CPT1A, an important free fatty acid mitochondrial transporter, resulted in increased sensitivity to Ven/TKI combination both in mouse and primary human leukemic cells, leading to the hypothesis that activation of fatty acid processing through enhanced Lipa activity may represent a compensatory response to venetoclax based therapies in bpCML. In summary, we demonstrate the preclinical efficacy of Ven/TKI combination therapies for targeting of bpCML LSCs. Furthermore, our data suggest that blocking upregulation of free fatty acids through mechanisms such as inhibition of LIPA activity, might synergize with Ven/TKI combinations to eradicate LSCs, allowing for more durable response. Our findings provide a therapeutic rationale for blocking pathways involved in free fatty acids generation, as a potential strategy for increasing remission duration. Disclosures Pollyea: Amgen: Consultancy; Janssen: Consultancy; Genentech: Consultancy; AbbVie: Consultancy, Research Funding; Syndax: Consultancy; Daiichi Sankyo: Consultancy; Takeda: Consultancy; Pfizer: Consultancy; Celgene/BMS: Consultancy; Agios: Consultancy; Karyopharm: Consultancy; Novartis: Consultancy; Glycomimetics: Other. Smith: Syros: Research Funding; Kura: Research Funding; Argenx: Research Funding.

Published
2021

90. Unique Metabolic Vulnerabilities of Myelodysplastic Syndrome Stem Cells

Author

Craig T. Jordan, Krysta L. Engel, Angelo D'Alessandro, Brett M. Stevens, Daniel A. Pollyea, Scott Alper, Rachel Culp-Hill, and Austin E. Gillen

Subjects
Immunology, Cancer research, Cell Biology, Hematology, Stem cell, Biology, Biochemistry
Abstract

Background: The mechanisms that cause the progression of myelodysplastic syndrome (MDS) are poorly understood. Little is known about major signaling networks and energy metabolism in MDS cells as patients progress from low risk (LR) to high risk (HR) disease and from high risk to secondary acute myelogenous leukemia (sAML). As many as 30% of HR MDS patients progress to sAML and a portion of LR MDS patients progress to HR. The goal of this project is preventing progression by identifying MDS-specific targets for therapy. A deeper understanding of the metabolic properties of leukemia stem cells (LSCs) in AML has shown these cells are uniquely vulnerable to venetoclax and azacitidine (Ven/Aza) (Pollyea et al, Nat. Medicine, 2018) and metabolic changes cause resistance to Ven/Aza (Stevens et al, Nat. Cancer, 2021). Little however is known about the contribution of metabolism to the pathogenesis of MDS. The contributing factors to progression including metabolic properties, transcriptional programs, and immunophenotype are examined in this study. Methods: Bone marrow specimens from MDS patients at various disease stages, including serial samples during progression, were obtained. Single cell techniques including mass cytometry, antibody based single cell RNA sequencing (CITE-Seq) and transcriptional profiling with RNA sequencing were used to elucidate novel mechanisms of progression. Selective targeting of primitive MDS cells was tested using several agents. Results: Our previous work characterizing MDS stem cells (MDSC) showed significant similarities between MDSCs and AML LSCs (Stevens et al, Nat. Communications, 2018). However, little is known about lower risk disease. In order to understand transcriptional changes and their relationship to metabolism across pathogenesis, the transcriptome of blasts from patients with LR, intermediate (INT), or HR IPSS scores was investigated. The first major transcriptional difference identified was enrichment of glycolysis pathway at LR and INT stage. In contrast, HR MDS demonstrated enrichment of oxidative phosphorylation. Furthermore, comparison of intermediate to HR MDS showed increased RNA polymerase and Ribosome pathways at the HR stage. These changes demonstrate the progressive alteration of metabolic properties during MDS pathogenesis with cells first relying on mechanisms associated with normal stem cells (i.e. glycolysis) and later transitioning to a state associated with AML stem cells (i.e. reliance on oxidative phosphorylation). Using serial specimens of patients of who progressed from LR to HR MDS we performed CITE-Seq and mass cytometry. CITE-seq in serial specimens showed up-regulation of protein translation and oxidative phosphorylation in a subset of MDS stem and progenitor cells (CD34+ at transcript and antibody level) present at LR stage and conserved at HR stage (Fig 1A-C). MDSCs also acquired surface antigens including CD99 and CD52 upon progression from LR to HR. Analysis of the mass cytometry data showed significant overlap with CITE-Seq data including increased CD123+ and MCL1 expression in MDS stem cells upon progression. In order to understand therapeutic vulnerabilities as they relate to progression, we investigated ex vivo drug response in LR and HR specimens. MDS samples were challenged with two regimens, Ven/Aza, a regimen known to inhibit OXPHOS; and omacetaxine and azacitidine (Oma/Aza), which inhibits translation. CITE-seq showed that MDSC were selectively sensitive to these agents (Fig 1D). Importantly, addition of either drug regimen caused ablation of MDSC at LR and HR stages and these changes were most profound in cells with LSC properties. Based on preclinical findings, we are investigating MDS patients treated with Ven/Aza or Oma/Aza via CITE-seq and metabolomics for correlation of clinical response with properties of MDSC. Preliminary studies show that patients that respond to Oma/Aza present with a population of MDSC with transcriptional signatures of protein translation and LSCs (Fig. 1E). Studies are underway to investigate overlapping properties of ven/aza resistance in AML to resistance in MDS specifically investigating fatty acid metabolism in MDSC. Conclusions: Analysis of MDS patient bone marrow reveals acquisition of aberrant metabolic properties at both low and high risk stages of disease. These distinct aspects of MDSC biology create unique and targetable features. Figure 1 Figure 1. Disclosures Pollyea: Genentech: Consultancy; Novartis: Consultancy; Pfizer: Consultancy; Janssen: Consultancy; Karyopharm: Consultancy; Syndax: Consultancy; Takeda: Consultancy; Daiichi Sankyo: Consultancy; Celgene/BMS: Consultancy; Amgen: Consultancy; AbbVie: Consultancy, Research Funding; Agios: Consultancy; Glycomimetics: Other.

Published
2021

91. Antitumor properties of novel sesquiterpene lactone analogs as NFκB inhibitors that bind to the IKKβ ubiquitin-like domain (ULD)

Author

Craig T. Jordan, Earl J. Morris, Jessica Ponder, Harikrishna Nakshatri, Meenakshisundaram Balasubramaniam, Narsimha Reddy Penthala, Soma Shekar Dachavaram, Peter A. Crooks, and Poornima Bhat-Nakshatri

Subjects
Stereochemistry, Protein subunit, Antineoplastic Agents, Sesquiterpene lactone, 01 natural sciences, Article, Lactones, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Protein Domains, Ubiquitin, Cell Line, Tumor, Drug Discovery, Humans, Parthenolide, Phosphorylation, Cell Proliferation, 030304 developmental biology, Pharmacology, chemistry.chemical_classification, 0303 health sciences, Binding Sites, biology, 010405 organic chemistry, Organic Chemistry, NF-kappa B, Transcription Factor RelA, General Medicine, 0104 chemical sciences, Molecular Docking Simulation, chemistry, Cell culture, Cytoplasm, biology.protein, Thermodynamics, Drug Screening Assays, Antitumor, Growth inhibition, Sesquiterpenes
Abstract

Melampomagnolide B (MMB, 3) is a parthenolide (PTL, 1) based sesquiterpene lactone that has been used as a template for the synthesis of a plethora of lead anticancer agents owing to its reactive C-10 primary hydroxyl group. Such compounds have been shown to inhibit the IKKβ subunit, preventing phosphorylation of the cytoplasmic IκB inhibitory complex. The present study focuses on the synthesis and in vitro antitumor properties of novel benzyl and phenethyl carbamates of MMB (7a-7k). Screening of these MMB carbamates identified analogs with potent growth inhibition properties against a panel of 60 human cancer cell lines (71% of the molecules screened had GI(50) values

Published
2021

92. Succinamide derivatives of melampomagnolide B and their anti-cancer activities

Author

Shraddha Thakkar, Venumadhav Janganati, Peter A. Crooks, Craig T. Jordan, and Jessica Ponder

Subjects
0301 basic medicine, Colorectal cancer, Stereochemistry, Clinical Biochemistry, Down-Regulation, Pharmaceutical Science, Transcription factor complex, Antineoplastic Agents, Apoptosis, Biochemistry, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cell Line, Tumor, Drug Discovery, medicine, Humans, Parthenolide, Molecular Biology, Binding Sites, Melanoma, Organic Chemistry, Cancer, Succinates, medicine.disease, Amides, Protein Structure, Tertiary, Molecular Docking Simulation, Leukemia, 030104 developmental biology, chemistry, Cell culture, 030220 oncology & carcinogenesis, Molecular Medicine, I-kappa B Proteins, Drug Screening Assays, Antitumor, Sesquiterpenes
Abstract

A series of succinamide derivatives of melampomagnolide B have been synthesized by coupling MMB monosuccinate (2) with various heterocyclic amines to afford compounds 3a–3l. MMB monosuccinate was also reacted with terminal diaminoalkanes to afford dimeric succinamido analogs of MMB (4a–4h). These succinamide analogs of MMB were evaluated for their anti-cancer activity against a panel of sixty human cancer cell lines. Analogs 3d–3i and dimers 4f–4g exhibited promising anti-cancer activity with GI50 values ranging from 0.28-33.5 μM against most of the cell lines in the panel. The dimeric analogs 4f and 4g were identified as lead compounds with GI50 values in the nanomolar range (GI50 = 280–980 nM) against several cell lines in the panel; i.e. leukemia cell lines CCRF-CEM, HL-60(TB), K-562, MOLT-4, RPMI-8226 and SR; and solid tumor cell lines NCI-H522 (non-small cell lung cancer), SW-620 and HCT-116 (colon cancer), LOX IMVI (melanoma), RXF 393 (renal cancer), and MCF7, BT-549 and MDA-MB-468 (breast cancer). Succinamide analogs 3a, 3c–3l and 4b–4h were also evaluated for their apoptotic activity against M9-ENL1 acute myelogenous leukemia cells; compounds 3h–3j and 4g were equipotent with parthenolide, exhibiting LC50 values in the range 4.1–8.1 μM. Molecular docking studies indicate that these molecules interact covalently with the highly conserved Cys-46 residue of the N-terminal lobe (1–109) of human IKKβ to inhibit the NFκB transcription factor complex, resulting in down-regulation of anti-apoptotic genes under NFκB control.

Published
2017

93. Therapeutic targeting of acute myeloid leukemia stem cells

Author

Daniel A. Pollyea and Craig T. Jordan

Subjects
0301 basic medicine, Myeloid, Immunology, Pharmacology, Biology, Therapeutic targeting, Biochemistry, 03 medical and health sciences, medicine, Humans, Molecular Targeted Therapy, Myeloid leukemia, Cell Biology, Hematology, Limiting, medicine.disease, Leukemia, Myeloid, Acute, Leukemia, 030104 developmental biology, medicine.anatomical_structure, Drug development, Neoplastic Stem Cells, Stem cell, Clinical evaluation, Neuroscience, Signal Transduction
Abstract

For more than 50 years, investigators have considered a malignant stem cell as the potential origin of and a key therapeutic target for acute myeloid leukemia (AML) and other forms of cancer.1-4 The nature and existence of tumor-initiating cells for leukemia and other malignancies have long been the subject of intense and rigorous study; indeed, the promise of the potential to eradicate such cells is clear. However, until recently, deficiencies in our understanding of the nature of these cell populations, coupled with a limited ability to therapeutically exploit their weaknesses, have been limiting factors in realizing the goal of targeting leukemic stem cells (LSCs). Exciting new insights into the fundamental underpinnings of LSCs are now being made in an era in which drug development pipelines offer the potential to specifically target pathways of significance. Therefore, the focus in this new era, characterized by the confluence of understanding LSCs and the ability to target them, is shifting from “if it can be done” to “how it will be done.” Moving from a theoretical stage to this hopeful era of possibilities, new challenges expectedly arise, and our focus now must shift to determining the best strategy by which to target LSCs, with their well-documented heterogeneity and readily evident intra- and interpatient variability. The purpose of this review is therefore both to summarize the key scientific findings pertinent to AML LSC targeting and to consider methods of clinical evaluation that will be most effective for identifying successful LSC-directed therapies.

Published
2017

94. Venetoclax Is Safe and Tolerable As Post-Transplant Maintenance Therapy for AML Patients at High Risk for Relapse

Author

Daniel A. Pollyea, Craig T. Jordan, Amanda Winters, Andrew Kent, Jonathan A. Gutman, and Clayton A. Smith

Subjects
medicine.medical_specialty, Venetoclax, Maintenance dose, business.industry, Immunology, Decitabine, Cell Biology, Hematology, Biochemistry, Transplantation, chemistry.chemical_compound, Maintenance therapy, chemistry, Median follow-up, Internal medicine, Cohort, medicine, Adverse effect, business, medicine.drug
Abstract

Relapse is the most common cause of mortality in patients undergoing allogeneic stem cell transplantation (ASCT) for acute myeloid leukemia (AML). The presence of measurable residual disease (MRD) at the time of transplant is associated with very high relapse rates, and novel strategies to address relapse risk are needed for these patients. Venetoclax has demonstrated single agent activity in AML, and venetoclax combined with azacitidine, decitabine, or low dose cytarabine is FDA approved to treat newly diagnosed patients >75yrs or older and those unfit for induction. Given the ability of venetoclax to target leukemic stem cells combined with its favorable toxicity profile and ease of administration, we have initiated off label post-transplant venetoclax maintenance for AML patients with MRD at the time of transplant. We report outcomes of our experience to date. Venetoclax therapy is planned to be initiated approximately 40-80 days post-ASCT upon count recovery (ANC>1000 109/L and platelets>100 109/L) and recovery from early ASCT toxicity. Dose is initiated at 100 mg daily for one week and titrated up by 100 mg weekly to a final maintenance dose of 400 mg daily. Therapy is planned until one year post-ASCT. Since February 2019, we have administered venetoclax to 23 post-ASCT patients (22 AML (6 with prior diagnosis of MDS) and 1 MDS), median age 65 (range 19-73). Venetoclax therapy was initiated beginning median 67 days (range 36-146) after ASCT. 16 patients underwent transplant following one line of therapy (twelve of whom received venetoclax azacitadine), 5 patients received 2 lines of therapy, and 2 patients received 3 lines of therapy. Three patients were second transplants. Donor sources were cord (n=14), haplo cord (n=5), and matched related donor (n=4). 7 patients underwent myeloablative, 14 reduced-intensity, and 2 non-myeloablative conditioning. All patients had MRD at time of transplant (15 by cytogenetics/FISH, 10 by flow cytometry, and 6 by digital droplet PCR). At time of transplant, 1 patient was aplastic, 6 were in morphologic leukemia free state (MLFS), one was in complete remission with incomplete count recovery (CRi), 15 were in complete remission (CR), and 1 had MDS with ringed sideroblasts with multilineage dysplasia. Patient data is summarized in Table 1. Median follow up among survivors is 219 days (range 92-439). Details of individual patients' courses on venetoclax are summarized in Figure 1. In total, 11 patients were still on venetoclax at the time of this analysis, and 4 had completed the planned 1 year of treatment. 3/23 (11%) had the drug permanently discontinued due to potential adverse effects in the setting of additional post-ASCT complications. Four patients relapsed 191, 288, 325, and 367 days post-transplant and all died, and 3 patients experienced transplant related mortality 146, 164, and 307 days post-ASCT. 6 month overall survival (OS) and relapse free survival (RFS) were both 87%. Venetoclax was temporarily held or dose-reduced in 11/23 (47.8%) patients due to adverse events (AEs). 14/23 (61%) patients experienced at least one AE that could be potentially attributed to venetoclax. Most common AEs were cytopenias (7/23, 30%) and diarrhea (7/23, 30%). 12 patients experienced grade 2-4 acute GVHD (3 grade 3). 10 of these patients developed GVHD symptoms prior to starting venetoclax. 5/7 patients who held venetoclax due to diarrhea had acute GVHD prior to initiation of ventoclax, and whether the diarrhea was GVHD or venetoclax related was unclear. Three patients have developed chronic GVHD (2 mild and 1 severe). Our preliminary data suggests venetoclax is tolerable in the post-ASCT maintenance setting without unexpected side effects. In this small cohort, GVHD rates are comparable to historical controls. Ongoing follow-up will continue to examine the safety and efficacy of this approach. Disclosures Pollyea: Novartis: Consultancy; Karyopharm: Consultancy; Takeda: Consultancy; Janssen: Consultancy; Amgen: Consultancy; Pfizer: Consultancy; Agios: Consultancy; 47: Consultancy, Research Funding; Genentech: Consultancy; Glycomimetics: Other; Celgene/BMS: Consultancy; Syndax: Consultancy; Syros: Consultancy; Abbvie: Consultancy, Research Funding; Daiichi Sankyo: Consultancy. OffLabel Disclosure: off label venetoclax post-transplant maintenance

Published
2020

95. Microfluidic nutrient gradient–based three-dimensional chondrocyte culture-on-a-chip as an in vitro equine arthritis model

Author

Peter Ertl, Sinan Gueltekin, Bahram Haddadi, S. Junttila, A. Gyenesei, Michael Harasek, Eva Haltmayer, Iris Ribitsch, Florien Jenner, B. Galik, Craig T. Jordan, Monika Egerbacher, Barbara Bachmann, and J. Rosser

Subjects
Biomedical Engineering, Primary cells, Bioengineering, SOX9, Osteoarthritis, Matrix (biology), Organ-on-a-chip, Tissue-on-a-Chip, Chondrocyte, Biomaterials, In vivo, Full Length Article, medicine, Molecular Biology, lcsh:QH301-705.5, Aggrecan, lcsh:R5-920, Chemistry, Organ-on-a-Chip, Cartilage, Cell Biology, medicine.disease, Cell biology, medicine.anatomical_structure, lcsh:Biology (General), lcsh:Medicine (General), Biotechnology
Abstract

In this work, we describe a microfluidic three-dimensional (3D) chondrocyte culture mimicking in vivo articular chondrocyte morphology, cell distribution, metabolism, and gene expression. This has been accomplished by establishing a physiologic nutrient diffusion gradient across the simulated matrix, while geometric design constraints of the microchambers drive native-like cellular behavior. Primary equine chondrocytes remained viable for the extended culture time of 3 weeks and maintained the low metabolic activity and high Sox9, aggrecan, and Col2 expression typical of articular chondrocytes. Our microfluidic 3D chondrocyte microtissues were further exposed to inflammatory cytokines to establish an animal-free, in vitro osteoarthritis model. Results of our study indicate that our microtissue model emulates the basic characteristics of native cartilage and responds to biochemical injury, thus providing a new foundation for exploration of osteoarthritis pathophysiology in both human and veterinary patients. Keywords: Organ-on-a-Chip, Cartilage, Primary cells, Tissue-on-a-Chip

Published
2019

96. Myelodysplastic syndrome-associated spliceosome gene mutations enhance innate immune signaling

Author

Craig T. Jordan, Emily C. Wheeler, Chelsea Harris, Brenna R. Hedin, Matthew J. Walter, Rafael Bejar, Lesly De Arras, Sigrid Katz, Jennifer L. Rabe, Scott Alper, Eric M. Pietras, and Daniel A. Pollyea

Subjects
Lipopolysaccharides, Spliceosome, RNA Splicing, Gene mutation, Biology, 03 medical and health sciences, Mice, 0302 clinical medicine, medicine, Missense mutation, Animals, Humans, Online Only Articles, Gene, Inflammation, Innate immune system, Serine-Arginine Splicing Factors, Myelodysplastic syndromes, NF-kappa B p50 Subunit, Hematology, medicine.disease, Phosphoproteins, Splicing Factor U2AF, Phenotype, Immunity, Innate, RAW 264.7 Cells, Myelodysplastic Syndromes, RNA splicing, Mutation, Cancer research, Spliceosomes, Cytokines, RNA Splicing Factors, K562 Cells, 030215 immunology
Abstract

Genes encoding spliceosome components including SF3B1, U2AF1 , and SRSF2 , are frequently somatically mutated in myelodysplastic syndromes (MDS), other hematologic malignancies, and solid tumors.[1][1] Typically these are mutually exclusive, heterozygous, missense, hotspot mutations that result in

Published
2019

97. Inhibition of Amino Acid Metabolism Selectively Targets Human Leukemia Stem Cells

Author

Craig T. Jordan, Travis Nemkov, Biniam Adane, James DeGregori, Daniel A. Pollyea, Haobin Ye, Brett M. Stevens, Angelo D'Alessandro, Dominik Reinhold, Shanshan Pei, Clayton A. Smith, Courtney L. Jones, Julie A. Reisz, Nabilah Khan, Rachel Culp-Hill, and Anna Krug

Subjects
0301 basic medicine, Cancer Research, Population, Antineoplastic Agents, Oxidative phosphorylation, Article, Oxidative Phosphorylation, 03 medical and health sciences, chemistry.chemical_compound, Mice, hemic and lymphatic diseases, Cell Line, Tumor, Metabolome, Animals, Humans, Amino Acids, education, chemistry.chemical_classification, education.field_of_study, Sulfonamides, Fatty acid metabolism, Chemistry, Catabolism, Fatty Acids, Myeloid leukemia, Biological Transport, Cell Biology, Bridged Bicyclo Compounds, Heterocyclic, Lipid Metabolism, Amino acid, Leukemia, Myeloid, Acute, 030104 developmental biology, Oncology, Proto-Oncogene Proteins c-bcl-2, Cancer research, Azacitidine, Neoplastic Stem Cells, Female, Stem cell, Glycolysis
Abstract

In this study we interrogated the metabolome of human acute myeloid leukemia (AML) stem cells to elucidate properties relevant to therapeutic intervention. We demonstrate that amino acid uptake, steady-state levels, and catabolism are all elevated in the leukemia stem cell (LSC) population. Furthermore, LSCs isolated from de novo AML patients are uniquely reliant on amino acid metabolism for oxidative phosphorylation and survival. Pharmacological inhibition of amino acid metabolism reduces oxidative phosphorylation and induces cell death. In contrast, LSCs obtained from relapsed AML patients are not reliant on amino acid metabolism due to their ability to compensate through increased fatty acid metabolism. These findings indicate that clinically relevant eradication of LSCs can be achieved with drugs that target LSC metabolic vulnerabilities.

Published
2019

98. Cysteine depletion targets leukemia stem cells through inhibition of electron transport complex II

Author

Angelo D'Alessandro, Daniel A. Pollyea, Julie A. Reisz, Courtney L. Jones, Craig T. Jordan, Brett M. Stevens, Shanshan Pei, Annika Gustafson, James DeGregori, Nabilah Khan, and Rachel Culp-Hill

Subjects
0301 basic medicine, Immunology, SDHA, Oxidative phosphorylation, Biochemistry, Oxidative Phosphorylation, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Adenosine Triphosphate, Humans, Cysteine, Progenitor cell, Cysteine metabolism, Chemistry, Electron Transport Complex II, Myeloid leukemia, Cell Biology, Hematology, Glutathione, Cell biology, Succinate Dehydrogenase, Leukemia, Myeloid, Acute, 030104 developmental biology, 030220 oncology & carcinogenesis, Neoplastic Stem Cells, Stem cell, Energy Metabolism, Reactive Oxygen Species, Oxidation-Reduction, Biomarkers
Abstract

We have previously demonstrated that oxidative phosphorylation is required for the survival of human leukemia stem cells (LSCs) from patients with acute myeloid leukemia (AML). More recently, we demonstrated that LSCs in patients with de novo AML rely on amino acid metabolism to drive oxidative phosphorylation. Notably, although overall levels of amino acids contribute to LSC energy metabolism, our current findings suggest that cysteine may be of particular importance for LSC survival. We demonstrate that exogenous cysteine is metabolized exclusively to glutathione. Upon cysteine depletion, glutathione synthesis is impaired, leading to reduced glutathionylation of succinate dehydrogenase A (SDHA), a key component of electron transport chain complex (ETC) II. Loss of SDHA glutathionylation impairs ETC II activity, thereby inhibiting oxidative phosphorylation, reducing production of ATP, and leading to LSC death. Given the role of cysteine in driving LSC energy production, we tested cysteine depletion as a potential therapeutic strategy. Using a novel cysteine-degrading enzyme, we demonstrate selective eradication of LSCs, with no detectable effect on normal hematopoietic stem/progenitor cells. Together, these findings indicate that LSCs are aberrantly reliant on cysteine to sustain energy metabolism, and that targeting this axis may represent a useful therapeutic strategy.

Published
2019

99. Rational Design of a Parthenolide-based Drug Regimen That Selectively Eradicates Acute Myelogenous Leukemia Stem Cells

Author

Clayton A. Smith, Daniel A. Pollyea, Craig T. Jordan, Mohammad Minhajuddin, Kirk C. Hansen, Fred K. Hagen, Subhajyoti De, Jonathan A. Gutman, John M. Ashton, Vinod Kumar Yadav, Travis Nemkov, Shanshan Pei, Biniam Adane, Brett M. Stevens, Angelo D'Alessandro, Nabilah Khan, and Peter A. Crooks

Subjects
Male, 0301 basic medicine, Myeloid, NF-E2-Related Factor 2, Deoxyglucose, Pharmacology, Biology, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, Myelogenous, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Parthenolide, Molecular Biology, Sirolimus, Gene Expression Regulation, Leukemic, Molecular Bases of Disease, Cell Biology, medicine.disease, Temsirolimus, Neoplasm Proteins, Up-Regulation, Leukemia, Myeloid, Acute, Regimen, Leukemia, 030104 developmental biology, medicine.anatomical_structure, chemistry, Drug development, Neoplastic Stem Cells, Female, Additions and Corrections, Stem cell, Sesquiterpenes, NADP, medicine.drug
Abstract

Although multidrug approaches to cancer therapy are common, few strategies are based on rigorous scientific principles. Rather, drug combinations are largely dictated by empirical or clinical parameters. In the present study we developed a strategy for rational design of a regimen that selectively targets human acute myelogenous leukemia (AML) stem cells. As a starting point, we used parthenolide, an agent shown to target critical mechanisms of redox balance in primary AML cells. Next, using proteomic, genomic, and metabolomic methods, we determined that treatment with parthenolide leads to induction of compensatory mechanisms that include up-regulated NADPH production via the pentose phosphate pathway as well as activation of the Nrf2-mediated oxidative stress response pathway. Using this knowledge we identified 2-deoxyglucose and temsirolimus as agents that can be added to a parthenolide regimen as a means to inhibit such compensatory events and thereby further enhance eradication of AML cells. We demonstrate that the parthenolide, 2-deoxyglucose, temsirolimus (termed PDT) regimen is a potent means of targeting AML stem cells but has little to no effect on normal stem cells. Taken together our findings illustrate a comprehensive approach to designing combination anticancer drug regimens.

Published
2016

100. Evolution of acute myelogenous leukemia stem cell properties after treatment and progression

Author

Monica L. Guzman, Michael W. Becker, Jason H. Mendler, Jane L. Liesveld, Mark W. LaMere, Eunice S. Wang, Brett M. Stevens, John M. Ashton, Tzu-Chieh Ho, Jianhua Zhao, Meir Wetzler, Jason R. Myers, Craig T. Jordan, Kristen M. O'Dwyer, and Jennifer J.D. Morrissette

Subjects
Adult, Male, 0301 basic medicine, Myeloid, Immunology, Plenary Paper, Mice, SCID, Biochemistry, Immunophenotyping, Cohort Studies, Mice, Young Adult, 03 medical and health sciences, Myelogenous, 0302 clinical medicine, Mice, Inbred NOD, Recurrence, Cancer stem cell, Biomarkers, Tumor, medicine, Animals, Humans, Prospective Studies, Aged, Aged, 80 and over, business.industry, Cancer, Cell Biology, Hematology, Middle Aged, medicine.disease, Chemotherapy regimen, Transplantation, Leukemia, Myeloid, Acute, Leukemia, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Disease Progression, Neoplastic Stem Cells, Cancer research, Female, sense organs, business, Neoplasm Transplantation
Abstract

Most cancers evolve over time as patients initially responsive to therapy acquire resistance to the same drugs at relapse. Cancer stem cells have been postulated to represent a therapy-refractory reservoir for relapse, but formal proof of this model is lacking. We prospectively characterized leukemia stem cell populations (LSCs) from a well-defined cohort of patients with acute myelogenous leukemia (AML) at diagnosis and relapse to assess the effect of the disease course on these critical populations. Leukemic samples were collected from patients with newly diagnosed AML before therapy and after relapse, and LSC frequency was assessed by limiting dilution analyses. LSC populations were identified using fluorescent-labeled cell sorting and transplantation into immunodeficient NOD/SCID/interleukin 2 receptor γ chain null mice. The surface antigen expression profiles of pretherapy and postrelapse LSCs were determined for published LSC markers. We demonstrate a 9- to 90-fold increase in LSC frequency between diagnosis and relapse. LSC activity at relapse was identified in populations of leukemic blasts that did not demonstrate this activity before treatment and relapse. In addition, we describe genetic instability and exceptional phenotypic changes that accompany the evolution of these new LSC populations. This study is the first to characterize the evolution of LSCs in vivo after chemotherapy, identifying a dramatic change in the physiology of primitive AML cells when the disease progresses. Taken together, these findings provide a new frame of reference by which to evaluate candidate AML therapies in which both disease control and the induction of more advanced forms of disease should be considered.

Published
2016

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