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Please use this identifier to cite or link to this item: http://hdl.handle.net/11434/2041
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dc.contributor.authorYannakou, Costas-
dc.contributor.otherBenajiba, Lena-
dc.contributor.otherCaraway, Hetty-
dc.contributor.otherHamad, Nada-
dc.contributor.otherStein, Eytan-
dc.contributor.otherBurroughs, Amy-
dc.contributor.otherHaris, Scott-
dc.contributor.otherLane, Hayley-
dc.contributor.otherNgyuen, Dorothy-
dc.contributor.otherStuart, Monic-
dc.contributor.otherVargas, Jesse-
dc.contributor.otherPuissant, Alexandre-
dc.contributor.otherStegmaier, Kimberly-
dc.contributor.otherDinardo, Courtney-
dc.date.accessioned2021-11-22T03:00:13Z-
dc.date.available2021-11-22T03:00:13Z-
dc.date.issued2020-12-
dc.identifier.citationBlood (2020) 136 (Supplement 1): 21.en_US
dc.identifier.urihttp://hdl.handle.net/11434/2041-
dc.description.abstractAcute myeloid leukemia (AML) and myelodysplastic syndrome (MDS) are clonal hematopoietic disorders that predominantly occur in older adults. For a limited number of fit patients, induction followed by consolidation chemotherapy and/or allogeneic stem-cell transplant (SCT) leads to cure. However, many AML patients are ineligible for aggressive therapy; up to 30% have primary refractory disease and up to 50% will relapse after front-line therapy, requiring alternative approaches. For these patients, durable long-term remission rate is low, with 5-year overall survival rates lower than 10%. Therefore, there remains an urgent unmet need for novel therapies for such patients. CB-5339 is a second generation, potent and selective, orally bioavailable small molecule inhibitor of valosin containing protein (VCP)/p97. VCP/p97 is a key cellular enzyme involved in cellular stress response pathways critical to cancer cell growth and survival such as protein homeostasis and the response to DNA damage. Inhibition of VCP/p97 in a panel of 131 cancer cell lines representing 16 cancer types revealed AML as the most exquisitely dependent disease (p=0.004) on VCP/p97 function. Further, CB-5339 demonstrated antiproliferative potency in a panel of 16 AML cell lines (IC50:100nM - 500nM). To better characterize the effects of CB-5339 on human leukemia, viability assays were performed on a set of 30 genetically diverse primary AML patient samples. Cellular viability was impacted with a similar potency across samples, irrespective of underlying genetic abnormalities (mean IC50: 423nM). In vivo, CB-5339 treatment resulted in decreased circulating leukemic cells and significantly prolonged survival in an MLL-AF9 syngeneic AML mouse model (p=0.02). In addition, evidence of synergy was exhibited with standard of care AML therapy, a combination of an anthracycline and cytarabine. This triple combination regimen resulted in a 96% mean relative decrease in leukemic burden compared to control mice and significantly prolonged mice survival compared to each regimen alone (p<0.0001). Importantly, CB-5339 was well tolerated as evidenced by stable weight curves and absence of significant myelosuppression. Here, we present a phase 1 study to evaluate CB-5339 in patients with relapsed/refractory (R/R) AML and intermediate or higher-risk MDS.en_US
dc.subjectAcute Myeloid Leukemia (AML)en_US
dc.subjectMyelodysplastic Syndrome (MDS)en_US
dc.subjectAllogeneic Stem-Cell Transplant (SCT)en_US
dc.subjectConsolidation Chemotherapyen_US
dc.subject(VCP)/p97 Proteinen_US
dc.subjectCB-5339 Inhibitoren_US
dc.subjectClonal Hematopoietic Disordersen_US
dc.subjectMyelosuppressionen_US
dc.subjectRelapsed/Refractory (R/R) AMLen_US
dc.subjectPhase 1 Clinical Trialen_US
dc.subjectSingle-Participant Cohorten_US
dc.subjectDose Expansion Phaseen_US
dc.subjectTwice Daily (BID)en_US
dc.subjectIntraparticipant Dose Escalationen_US
dc.subjectPharmacodynamic (PD) Biomarkersen_US
dc.subjectPK/PD Relationshipen_US
dc.subjectEpworth Centre for Immunotherapies and Snowdome Laboratoriesen_US
dc.subjectDepartment of Molecular Oncology and Cancer Immunology, Epworth HealthCareen_US
dc.subjectCancer Services Clinical Institute, Epworth HealthCare, Victoria, Australiaen_US
dc.titleA phase I study to evaluate the safety and pharmacokinetic profiles of CB-5339 in participants with relapsed/refractory acute myeloid leukemia or relapsed/refractory intermediate or high-risk myelodysplastic syndrome.en_US
dc.typeConference Posteren_US
dc.identifier.doi10.1182/blood-2020-140636en_US
dc.description.affiliatesAPHP, INSERM U944, Institute of Hematology - St Louis Hospital, PARIS, Franceen_US
dc.description.affiliatesTaussig Cancer Institute, Cleveland Clinic, Department of Hematology and Medical Oncology, Cleveland, OHen_US
dc.description.affiliatesDepartment of Haematology, St. Vincent's Hospital, Sydney, Australiaen_US
dc.description.affiliatesUniversity of New South Wales, Sydney, Australiaen_US
dc.description.affiliatesDepartment of Medicine, Leukemia Service, Memorial Sloan Kettering Cancer Center, New York, NYen_US
dc.description.affiliatesDepartment of Molecular Oncology and Cancer Immunology, Epworth HealthCare, East Melbourne, Australiaen_US
dc.description.affiliatesCleave Therapeutics, Inc., San Francisco, CAen_US
dc.description.affiliatesCleave Therapeutics, Inc., San Diego, CAen_US
dc.description.affiliatesDana-Farber Cancer Institute, Boston, MAen_US
dc.description.affiliatesDepartment of Leukemia, The University of Texas MD Anderson Cancer Center, Houston, TXen_US
dc.type.studyortrialClinical Trialen_US
dc.description.conferencenameASH Meeting 2020en_US
dc.description.conferencelocationGeorgia World Congress Center, Atlanta, Georgia, United Statesen_US
dc.type.contenttypeTexten_US
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