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1. Supplementary figure legends and supplementary methods from Efficacy of a Covalent ERK1/2 Inhibitor, CC-90003, in KRAS-Mutant Cancer Models Reveals Novel Mechanisms of Response and Resistance

Author

Ellen H. Filvaroff, Gordon L. Bray, Konstantinos Mavrommatis, Tao Shi, Winfried Elis, Mehnaz Malek, Lisa Beebe, Lixin Qiao, Terri Jones, Carmen Barnes, Matt Labenski, Yumin Dai, and Ida Aronchik

Abstract

Supplementary figure legends and supplementary materials and methods

Published
2023
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2. Supplementary Tables and Figures from Efficacy of a Covalent ERK1/2 Inhibitor, CC-90003, in KRAS-Mutant Cancer Models Reveals Novel Mechanisms of Response and Resistance

Author

Ellen H. Filvaroff, Gordon L. Bray, Konstantinos Mavrommatis, Tao Shi, Winfried Elis, Mehnaz Malek, Lisa Beebe, Lixin Qiao, Terri Jones, Carmen Barnes, Matt Labenski, Yumin Dai, and Ida Aronchik

Abstract

Table S1. Summary of CC-90003 specificity data resulting from cellular and biochemical assays. Table S2. Response of BRAF mutant cell lines to CC-90003 ERK 1/2 inhibition. Table S3. Summary of dose finding efficacy study in HCT-116 xenograft model. Figure S1. CC-90003 Mass spectrometry analysis of CC-90003 covalent ERK1/2 binding. Figure S2. CC-90003 Inhibits proliferation and induces apoptosis in a panel of KRAS mutant Lung, Pancreatic and Colorectal cancer cell lines. Figure S3. Assessment of ERK inhibitor PD markers in BRAF and KRAS mutant Cancer Models. Figure S4. CC-90003 inhibits proliferation of a subset of BRAF and KRAS mutant cell lung cancer lines and induces cell death more robustly, compared to published inhibitors. Figure S5. CC-90003 inhibits colony formation in a set of KRAS mutant PDX models ex vivo. Figure S6. CC-90003 does not reduce body weights of animals bearing KRAS mutant PDX derived tumors. Figure S7. Genes differentially expressed in CXF-243 PDX model compared to other models used in the study. Figure S8. Genes differentially expressed in CXF-243, CXF-975 and CXF-1034 PDX models compared to other models used in the study. Figure S9. Combination of CC-90003 with EGFR inhibitor Afatinib and NK inhibitor JNK-IN-8. Figure S10. Quantification of Western Blot data in Figure 4. Figure S11. CC-90003 does not reduce body weights of animals bearing LXFA-1674 KRAS mutant lung cancer PDX derived tumors. Figure S12. Regrowth of LXFA-1674 KRAS mutant lung cancer PDX derived tumors following discontinuation of treatment by Docetaxel and CC-90003 combination with Docetaxel. Figure S13. CC-90003 alone and in combination with Docetaxel modulates stemness program in ex vivo serial passaging Mammocult assay.

Published
2023
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3. Data from Efficacy of a Covalent ERK1/2 Inhibitor, CC-90003, in KRAS-Mutant Cancer Models Reveals Novel Mechanisms of Response and Resistance

Author

Ellen H. Filvaroff, Gordon L. Bray, Konstantinos Mavrommatis, Tao Shi, Winfried Elis, Mehnaz Malek, Lisa Beebe, Lixin Qiao, Terri Jones, Carmen Barnes, Matt Labenski, Yumin Dai, and Ida Aronchik

Abstract

As a critical signaling node, ERK1/2 are attractive drug targets, particularly in tumors driven by activation of the MAPK pathway. Utility of targeting the MAPK pathway has been demonstrated by clinical responses to inhibitors of MEK1/2 or RAF kinases in some mutant BRAF-activated malignancies. Unlike tumors with mutations in BRAF, those with mutations in KRAS (>30% of all cancers and >90% of certain cancer types) are generally not responsive to inhibitors of MEK1/2 or RAF. Here, a covalent ERK1/2 inhibitor, CC-90003, was characterized and shown to be active in preclinical models of KRAS-mutant tumors. A unique occupancy assay was used to understand the mechanism of resistance in a KRAS-mutant patient-derived xenograft (PDX) model of colorectal cancer. Finally, combination of CC-90003 with docetaxel achieved full tumor regression and prevented tumor regrowth after cessation of treatment in a PDX model of lung cancer. This effect corresponded to changes in a stemness gene network, revealing a potential effect on tumor stem cell reprograming.Implications:Here, a covalent ERK1/2 inhibitor (CC-90003) is demonstrated to have preclinical efficacy in models of KRAS-mutant tumors, which present a therapeutic challenge for currently available therapies.

Published
2023
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4. Supplementary Figure 4 from A Randomized Phase II Trial of Vismodegib versus Placebo with FOLFOX or FOLFIRI and Bevacizumab in Patients with Previously Untreated Metastatic Colorectal Cancer

Author

Jennifer A. Low, Gordon L. Bray, Richard A. Graham, Robert L. Yauch, Howard M. Mackey, Mark M. Zalupski, Mary F. Mulcahy, Robert C. Hermann, Ira Gore, Irfan Firdaus, Lowell L. Hart, Johanna C. Bendell, and Jordan Berlin

Abstract

PDF file - 30K, Estimated maximal concentration (Cmax) and total area under the concentration-time curve (AUClast) of total and free oxaliplatin with and without vismodegib

Published
2023
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5. Supplementary Figure 2 from A Randomized Phase II Trial of Vismodegib versus Placebo with FOLFOX or FOLFIRI and Bevacizumab in Patients with Previously Untreated Metastatic Colorectal Cancer

Author

Jennifer A. Low, Gordon L. Bray, Richard A. Graham, Robert L. Yauch, Howard M. Mackey, Mark M. Zalupski, Mary F. Mulcahy, Robert C. Hermann, Ira Gore, Irfan Firdaus, Lowell L. Hart, Johanna C. Bendell, and Jordan Berlin

Abstract

PDF file - 25K, A comparison of steady-state 5-FU concentrations with and without vismodegib co-treatment

Published
2023
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6. Supplementary Figure 3 from Phase I Study of CC-486 Alone and in Combination with Carboplatin or nab-Paclitaxel in Patients with Relapsed or Refractory Solid Tumors

Author

Johanna C. Bendell, Eric Laille, Kejian Liu, Aaron Nguyen, Jorge DiMartino, Gordon L. Bray, Patricia M. LoRusso, Miguel Martin, W. Jeff Edenfield, Jose A. Lopez-Martin, Ron H.J. Mathijssen, Bert O'Neil, Christophe Le Tourneau, Nicolas Isambert, Jan H.M. Schellens, Pamela N. Munster, Elisabeth I. Heath, Drew W. Rasco, and Daniel D. Von Hoff

Abstract

Correlation analysis between pharmacodynamic and pharmacokinetic findings in part 1

Published
2023
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7. Supplementary Figure 2 from Phase I Study of CC-486 Alone and in Combination with Carboplatin or nab-Paclitaxel in Patients with Relapsed or Refractory Solid Tumors

Author

Johanna C. Bendell, Eric Laille, Kejian Liu, Aaron Nguyen, Jorge DiMartino, Gordon L. Bray, Patricia M. LoRusso, Miguel Martin, W. Jeff Edenfield, Jose A. Lopez-Martin, Ron H.J. Mathijssen, Bert O'Neil, Christophe Le Tourneau, Nicolas Isambert, Jan H.M. Schellens, Pamela N. Munster, Elisabeth I. Heath, Drew W. Rasco, and Daniel D. Von Hoff

Abstract

Mean paclitaxel plasma concentrations following nab-paclitaxel administration alone or with CC-486 in part 1 arm B

Published
2023
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8. Supplementary Tables 1-8 from Phase I Study of CC-486 Alone and in Combination with Carboplatin or nab-Paclitaxel in Patients with Relapsed or Refractory Solid Tumors

Author

Johanna C. Bendell, Eric Laille, Kejian Liu, Aaron Nguyen, Jorge DiMartino, Gordon L. Bray, Patricia M. LoRusso, Miguel Martin, W. Jeff Edenfield, Jose A. Lopez-Martin, Ron H.J. Mathijssen, Bert O'Neil, Christophe Le Tourneau, Nicolas Isambert, Jan H.M. Schellens, Pamela N. Munster, Elisabeth I. Heath, Drew W. Rasco, and Daniel D. Von Hoff

Abstract

Table S1. CC-486 Plus Carboplatin Dose Levels in Part 1 Arm A Table S2. CC-486 Plus nab-Paclitaxel Dose Levels in Part 1 Arm B Table S3. CC-486 Dose Levels in Part 1 Arm C Table S4. Number of Patients With Treatment Emergent Adverse Events for Part 1 Table S5. Number of Patients With Treatment-Emergent Adverse Events in Any Treatment Arm in Part 2 Table S6. Mean CC-486 Plasma Pharmacokinetic Parameters Table S7. Efficacy of CC-486 Alone or in Combination With Carboplatin or nab-Paclitaxel in Part 2 Table S8. Prior Treatment History of NPV Patients

Published
2023
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9. Supplementary Figure 1 from Phase I Study of CC-486 Alone and in Combination with Carboplatin or nab-Paclitaxel in Patients with Relapsed or Refractory Solid Tumors

Author

Johanna C. Bendell, Eric Laille, Kejian Liu, Aaron Nguyen, Jorge DiMartino, Gordon L. Bray, Patricia M. LoRusso, Miguel Martin, W. Jeff Edenfield, Jose A. Lopez-Martin, Ron H.J. Mathijssen, Bert O'Neil, Christophe Le Tourneau, Nicolas Isambert, Jan H.M. Schellens, Pamela N. Munster, Elisabeth I. Heath, Drew W. Rasco, and Daniel D. Von Hoff

Abstract

Mean total carboplatin plasma concentration following carboplatin administration alone or with CC-486 in part 1 arm A

Published
2023
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10. Supplementary Figure 3 from A Randomized Phase II Trial of Vismodegib versus Placebo with FOLFOX or FOLFIRI and Bevacizumab in Patients with Previously Untreated Metastatic Colorectal Cancer

Author

Jennifer A. Low, Gordon L. Bray, Richard A. Graham, Robert L. Yauch, Howard M. Mackey, Mark M. Zalupski, Mary F. Mulcahy, Robert C. Hermann, Ira Gore, Irfan Firdaus, Lowell L. Hart, Johanna C. Bendell, and Jordan Berlin

Abstract

PDF file - 33K, Estimated maximal concentration (Cmax) and total area under the concentration-time curve (AUClast) of irinotecan (and metabolites SN-38 and SN-38G) with and without vismodegib

Published
2023
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11. Supplementary Figure 5 from A Randomized Phase II Trial of Vismodegib versus Placebo with FOLFOX or FOLFIRI and Bevacizumab in Patients with Previously Untreated Metastatic Colorectal Cancer

Author

Jennifer A. Low, Gordon L. Bray, Richard A. Graham, Robert L. Yauch, Howard M. Mackey, Mark M. Zalupski, Mary F. Mulcahy, Robert C. Hermann, Ira Gore, Irfan Firdaus, Lowell L. Hart, Johanna C. Bendell, and Jordan Berlin

Abstract

PDF file - 25K, A comparison of serum concentrations of bevacizumab with and without vismodegib co-treatment

Published
2023
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12. Supplementary Table 1 from A Randomized Phase II Trial of Vismodegib versus Placebo with FOLFOX or FOLFIRI and Bevacizumab in Patients with Previously Untreated Metastatic Colorectal Cancer

Author

Jennifer A. Low, Gordon L. Bray, Richard A. Graham, Robert L. Yauch, Howard M. Mackey, Mark M. Zalupski, Mary F. Mulcahy, Robert C. Hermann, Ira Gore, Irfan Firdaus, Lowell L. Hart, Johanna C. Bendell, and Jordan Berlin

Abstract

PDF file - 57K, A summary of primer/probes used for qRT-PCR profiling of Hh pathway genes

Published
2023
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13. Data from A Randomized Phase II Trial of Vismodegib versus Placebo with FOLFOX or FOLFIRI and Bevacizumab in Patients with Previously Untreated Metastatic Colorectal Cancer

Author

Jennifer A. Low, Gordon L. Bray, Richard A. Graham, Robert L. Yauch, Howard M. Mackey, Mark M. Zalupski, Mary F. Mulcahy, Robert C. Hermann, Ira Gore, Irfan Firdaus, Lowell L. Hart, Johanna C. Bendell, and Jordan Berlin

Abstract

Purpose: Vismodegib, a Hedgehog pathway inhibitor, has preclinical activity in colorectal cancer (CRC) models. This trial assessed the efficacy, safety, and pharmacokinetics of adding vismodegib to first-line treatment for metastatic CRC (mCRC).Experimental design: Patients were randomized to receive vismodegib (150 mg/day orally) or placebo, in combination with FOLFOX or FOLFIRI chemotherapy plus bevacizumab (5 mg/kg) every 2 weeks until disease progression or intolerable toxicity. The primary endpoint was progression-free survival (PFS). Key secondary objectives included evaluation of predictive biomarkers and pharmacokinetic drug interactions.Results: A total of 199 patients with mCRC were treated on protocol (124 FOLFOX, 75 FOLFIRI). The median PFS hazard ratio (HR) for vismodegib treatment compared with placebo was 1.25 (90% CI: 0.89–1.76; P = 0.28). The overall response rates for placebo-treated and vismodegib-treated patients were 51% (90% CI: 43–60) and 46% (90% CI: 37–55), respectively. No vismodegib-associated benefit was observed in combination with either FOLFOX or FOLFIRI. Increased tumor tissue Hedgehog expression did not predict clinical benefit. Grade 3 to 5 adverse events reported for more than 5% of patients that occurred more frequently in the vismodegib-treated group were fatigue, nausea, asthenia, mucositis, peripheral sensory neuropathy, weight loss, decreased appetite, and dehydration. Vismodegib did not alter the pharmacokinetics of FOLFOX, FOLFIRI, or bevacizumab.Conclusions: Vismodegib does not add to the efficacy of standard therapy for mCRC. Compared with placebo, treatment intensity was lower for all regimen components in vismodegib-treated patients, suggesting that combined toxicity may have contributed to lack of efficacy. Clin Cancer Res; 19(1); 258–67. ©2012 AACR.

Published
2023
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14. Supplementary Methods Data from Phase I Study of CC-486 Alone and in Combination with Carboplatin or nab-Paclitaxel in Patients with Relapsed or Refractory Solid Tumors

Author

Johanna C. Bendell, Eric Laille, Kejian Liu, Aaron Nguyen, Jorge DiMartino, Gordon L. Bray, Patricia M. LoRusso, Miguel Martin, W. Jeff Edenfield, Jose A. Lopez-Martin, Ron H.J. Mathijssen, Bert O'Neil, Christophe Le Tourneau, Nicolas Isambert, Jan H.M. Schellens, Pamela N. Munster, Elisabeth I. Heath, Drew W. Rasco, and Daniel D. Von Hoff

Abstract

Pharmacodynamic Assessments

Published
2023
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15. Supplementary Figure 1 from A Randomized Phase II Trial of Vismodegib versus Placebo with FOLFOX or FOLFIRI and Bevacizumab in Patients with Previously Untreated Metastatic Colorectal Cancer

Author

Jennifer A. Low, Gordon L. Bray, Richard A. Graham, Robert L. Yauch, Howard M. Mackey, Mark M. Zalupski, Mary F. Mulcahy, Robert C. Hermann, Ira Gore, Irfan Firdaus, Lowell L. Hart, Johanna C. Bendell, and Jordan Berlin

Abstract

PDF file - 24K, A comparison of vismodegib steady-state plasma concentrations (Css) between patients receiving FOLFOX and FOLFIRI

Published
2023
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17. Data from Phase I Study of CC-486 Alone and in Combination with Carboplatin or nab-Paclitaxel in Patients with Relapsed or Refractory Solid Tumors

Author

Johanna C. Bendell, Eric Laille, Kejian Liu, Aaron Nguyen, Jorge DiMartino, Gordon L. Bray, Patricia M. LoRusso, Miguel Martin, W. Jeff Edenfield, Jose A. Lopez-Martin, Ron H.J. Mathijssen, Bert O'Neil, Christophe Le Tourneau, Nicolas Isambert, Jan H.M. Schellens, Pamela N. Munster, Elisabeth I. Heath, Drew W. Rasco, and Daniel D. Von Hoff

Abstract

Purpose: This large two-part, three-arm phase I study examined the safety and tolerability of CC-486 (an oral formulation of azacitidine, a hypomethylating agent) alone or in combination with the cytotoxic agents, carboplatin or nab-paclitaxel, in patients with advanced unresectable solid tumors.Patients and Methods: Part 1 (n = 57) was a dose escalation of CC-486 alone (arm C) or with carboplatin (arm A) or nab-paclitaxel (arm B). The primary endpoint was safety, MTD, and recommended part 2 dose (RP2D) of CC-486. In part 2 (n = 112), the primary endpoint was the safety and tolerability of CC-486 administered at the RP2D for each treatment arm, in tumor-specific expansion cohorts. Secondary endpoints included pharmacokinetics, pharmacodynamics, and antitumor activity of CC-486.Results: At pharmacologically active doses CC-486 in combination with carboplatin or nab-paclitaxel had a tolerable safety profile and no drug–drug interactions. The CC-486 RP2D was determined as 300 mg (every day, days 1–14/21) in combination with carboplatin (arm A) or as monotherapy (arm C); and 200 mg in the same dosing regimen in combination with nab-paclitaxel (arm B). Albeit limited by the small sample size, CC-486 monotherapy resulted in partial responses (three/eight) and stable disease (four/eight) in patients with nasopharyngeal cancer. Three of the stable disease responses lasted more than 150 days.Conclusions: CC-486 is well tolerated alone or in combination with carboplatin or nab-paclitaxel. Exploratory analyses suggest clinical activity of CC-486 monotherapy in nasopharyngeal cancer and provided the basis for an ongoing phase II clinical trial (ClinicalTrials.gov identifier: NCT02269943). Clin Cancer Res; 24(17); 4072–80. ©2018 AACR.

Published
2023
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18. Efficacy of a Covalent ERK1/2 Inhibitor, CC-90003, in KRAS-Mutant Cancer Models Reveals Novel Mechanisms of Response and Resistance

Author

Carmen Maria Barnes, Ellen Filvaroff, Shi Tao, Mehnaz Malek, Gordon L. Bray, Winfried Elis, Yumin Dai, Konstantinos Mavrommatis, Lixin Qiao, Terri Jones, Ida Aronchik, Beebe Lisa, and Matt Labenski

Subjects
0301 basic medicine, MAPK/ERK pathway, Cancer Research, MAP Kinase Signaling System, Colorectal cancer, Mutant, Mice, Nude, medicine.disease_cause, Proto-Oncogene Proteins p21(ras), Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, medicine, Animals, Humans, Lung cancer, Molecular Biology, Mutation, Chemistry, Cancer, medicine.disease, 030104 developmental biology, Oncology, Docetaxel, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer research, Female, KRAS, medicine.drug
Abstract

As a critical signaling node, ERK1/2 are attractive drug targets, particularly in tumors driven by activation of the MAPK pathway. Utility of targeting the MAPK pathway has been demonstrated by clinical responses to inhibitors of MEK1/2 or RAF kinases in some mutant BRAF-activated malignancies. Unlike tumors with mutations in BRAF, those with mutations in KRAS (>30% of all cancers and >90% of certain cancer types) are generally not responsive to inhibitors of MEK1/2 or RAF. Here, a covalent ERK1/2 inhibitor, CC-90003, was characterized and shown to be active in preclinical models of KRAS-mutant tumors. A unique occupancy assay was used to understand the mechanism of resistance in a KRAS-mutant patient-derived xenograft (PDX) model of colorectal cancer. Finally, combination of CC-90003 with docetaxel achieved full tumor regression and prevented tumor regrowth after cessation of treatment in a PDX model of lung cancer. This effect corresponded to changes in a stemness gene network, revealing a potential effect on tumor stem cell reprograming. Implications: Here, a covalent ERK1/2 inhibitor (CC-90003) is demonstrated to have preclinical efficacy in models of KRAS-mutant tumors, which present a therapeutic challenge for currently available therapies.

Published
2019
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19. A Phase 3, Randomized, Double-Blind, Placebo-Controlled Study to Assess the Efficacy and Safety of Entospletinib in Combination with Intensive Induction and Consolidation Chemotherapy in Adults with Newly Diagnosed N ucleophosmin 1-mutated Acute Myeloid Leukemia

Author

Pavan Kumar, Gordon L. Bray, Wendy Stock, Eytan M. Stein, John C. Byrd, Thomas Oellerich, Jorge E. Cortes, Mark D. Minden, Jenna Elder, and Jorge F. DiMartino

Subjects
Oncology, medicine.medical_specialty, Entospletinib, business.industry, Immunology, Placebo-controlled study, Myeloid leukemia, Consolidation Chemotherapy, Cell Biology, Hematology, Newly diagnosed, Biochemistry, Double blind, Internal medicine, Medicine, business
Abstract

Background: Spleen tyrosine kinase (SYK) is a component of both lymphoid and myeloid cell signaling pathways and has been implicated in the pathogenesis of a subset of acute myeloid leukemia (AML) defined by dysregulated expression of the HOXA9 and MEIS1 transcription factors. Entospletinib (ENTO) is an oral, selective SYK inhibitor that is acceptably tolerated when administered with intensive induction and consolidation in newly diagnosed AML patients. In a phase 2 study, following induction with cytarabine and daunorubicin (7+3) plus ENTO, higher rates of complete response (CR) or CR with incomplete hematologic recovery (CRi) were observed in patients with rearrangements of the KMT2A (MLL) gene (MLL-r) and mutations of the nucleophosmin 1 (NPM1) gene, both of which are associated with aberrant expression of HOXA9 and MEIS1, as compared to patients without these mutations. In an exploratory analysis, patients with HOXA9/MEIS1 expression levels above the median experienced superior overall survival (OS) as compared to patients with expression levels below the median. In the AGILITY trial, we hypothesize that the addition of ENTO to intensive induction/consolidation in newly diagnosed patients with NPM1-mutated AML will improve the rate of CR without evidence of measurable residual disease (MRD-negative CR) post-induction and duration of event-free survival (EFS). Methods: AGILITY will be a global, multi-center, double-blind, placebo-controlled trial of ENTO in combination with cytarabine plus daunorubicin or idarubicin induction (7+3) and age-adjusted high-dose cytarabine (HiDAC) consolidation in newly diagnosed AML patients aged 18-75 years who are candidates for intensive induction and harbor a documented NPM1 mutation based on local or central mutation testing. Patients with co-mutated FLT3 (internal tandem duplication or tyrosine kinase domain) and for whom midostaurin with 7+3 is indicated are excluded. Patients will be stratified based on age ( An independent data-monitoring committee will monitor emerging safety and efficacy data from this trial on an ongoing basis. Disclosures Byrd: Vincerx Pharmaceuticals: Current equity holder in publicly-traded company, Membership on an entity's Board of Directors or advisory committees; Novartis, Trillium, Astellas, AstraZeneca, Pharmacyclics, Syndax: Consultancy, Honoraria; Newave: Membership on an entity's Board of Directors or advisory committees. Cortes: Bristol Myers Squibb, Daiichi Sankyo, Jazz Pharmaceuticals, Astellas, Novartis, Pfizer, Takeda, BioPath Holdings, Incyte: Consultancy, Research Funding; Novartis: Consultancy, Research Funding; Bio-Path Holdings, Inc.: Consultancy, Membership on an entity's Board of Directors or advisory committees; Pfizer: Consultancy, Research Funding; Takeda: Consultancy, Research Funding; Sun Pharma: Consultancy, Research Funding. Minden: Astellas: Consultancy. Oellerich: Roche: Consultancy; Gilead: Research Funding; Kronos Bio, Inc.: Consultancy; Merck KGaA: Consultancy, Research Funding. Stein: Syros Pharmaceuticals, Inc.: Consultancy; Daiichi Sankyo: Consultancy; PinotBio: Consultancy; Celgene: Consultancy; Bristol Myers Squibb: Consultancy; Jazz Pharmaceuticals: Consultancy; Foghorn Therapeutics: Consultancy; Blueprint Medicines: Consultancy; Gilead Sciences, Inc.: Consultancy; Abbvie: Consultancy; Janssen Pharmaceuticals: Consultancy; Genentech: Consultancy; Syndax Pharmaceuticals: Consultancy; Agios Pharmaceuticals, Inc: Consultancy; Novartis: Consultancy; Astellas: Consultancy. Elder: PharPoint Research, Inc.: Current Employment. Kumar: Kronos Bio, Inc.: Current Employment, Current equity holder in publicly-traded company. Bray: Kronos Bio, Inc.: Consultancy. DiMartino: Kronos Bio, Inc.: Current Employment, Current equity holder in publicly-traded company. Stock: Pfizer: Consultancy, Honoraria, Research Funding; amgen: Honoraria; agios: Honoraria; jazz: Honoraria; kura: Honoraria; kite: Honoraria; morphosys: Honoraria; servier: Honoraria; syndax: Consultancy, Honoraria; Pluristeem: Consultancy, Honoraria. OffLabel Disclosure: Entospletinib is an investigational therapy

Published
2021
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20. Phase I Study of CC-486 Alone and in Combination with Carboplatin or nab-Paclitaxel in Patients with Relapsed or Refractory Solid Tumors

Author

Aaron N. Nguyen, Johanna C. Bendell, Patricia LoRusso, Christophe Le Tourneau, Miguel Martin, Drew W. Rasco, W. Jeff Edenfield, Pamela N. Munster, Jose A. Lopez-Martin, Bert H. O'Neil, Gordon L. Bray, Elisabeth I. Heath, Eric Laille, Jorge DiMartino, Kejian Liu, Jan H.M. Schellens, Nicolas Isambert, Daniel D. Von Hoff, Ron H.J. Mathijssen, Medical Oncology, The Translational Genomics Research Institute (TGen), South Texas Accelerated Research Therapeutics [San Antonio, Texas] (START), Karmanos Cancer Institute (Detroit), Department of Medicine [San Francisco], University of California [San Francisco] (UCSF), University of California-University of California, Netherlands Cancer Institute (NKI), Antoni van Leeuwenhoek Hospital, Centre Régional de Lutte contre le cancer Georges-François Leclerc [Dijon] (UNICANCER/CRLCC-CGFL), UNICANCER, Département d'Oncologie Médicale [Institut Curie, Paris], Institut Curie [Paris], Indiana University School of Medicine, Indiana University System, Erasmus MC Cancer Institute, Rotterdam, 12 de Octubre University Hospital, Greenville Memorial Hospital [University of South Carolina, Greenville] (GHS), East Carolina University [Greenville] (ECU), University of North Carolina System (UNC)-University of North Carolina System (UNC), Hospital General Universitario 'Gregorio Marañón' [Madrid], Celgene Corporation, and Sarah Cannon Research Institute [Nashville, Tennessee]

Subjects
0301 basic medicine, Oncology, Male, Cancer Research, oral azacitidine, design, Carboplatin, chemistry.chemical_compound, 0302 clinical medicine, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, Clinical endpoint, 6.2 Cellular and gene therapies, Cancer, trial, Middle Aged, myelodysplastic syndromes, 3. Good health, Treatment Outcome, Tolerability, 030220 oncology & carcinogenesis, 6.1 Pharmaceuticals, Azacitidine, Female, acute myeloid-leukemia, safety, medicine.medical_specialty, Paclitaxel, Maximum Tolerated Dose, Clinical Trials and Supportive Activities, Oncology and Carcinogenesis, [SDV.CAN]Life Sciences [q-bio]/Cancer, Article, Disease-Free Survival, Drug Administration Schedule, 03 medical and health sciences, 5-azacytidine, Pharmacokinetics, SDG 3 - Good Health and Well-being, Clinical Research, Internal medicine, Albumins, medicine, cancer, Humans, Oncology & Carcinogenesis, Aged, therapy, business.industry, nasopharyngeal carcinoma, Evaluation of treatments and therapeutic interventions, medicine.disease, Clinical trial, 030104 developmental biology, Hypomethylating agent, chemistry, Pharmacodynamics, business
Abstract

Purpose: This large two-part, three-arm phase I study examined the safety and tolerability of CC-486 (an oral formulation of azacitidine, a hypomethylating agent) alone or in combination with the cytotoxic agents, carboplatin or nab-paclitaxel, in patients with advanced unresectable solid tumors. Patients and Methods: Part 1 (n = 57) was a dose escalation of CC-486 alone (arm C) or with carboplatin (arm A) or nab-paclitaxel (arm B). The primary endpoint was safety, MTD, and recommended part 2 dose (RP2D) of CC-486. In part 2 (n = 112), the primary endpoint was the safety and tolerability of CC-486 administered at the RP2D for each treatment arm, in tumor-specific expansion cohorts. Secondary endpoints included pharmacokinetics, pharmacodynamics, and antitumor activity of CC-486. Results: At pharmacologically active doses CC-486 in combination with carboplatin or nab-paclitaxel had a tolerable safety profile and no drug–drug interactions. The CC-486 RP2D was determined as 300 mg (every day, days 1–14/21) in combination with carboplatin (arm A) or as monotherapy (arm C); and 200 mg in the same dosing regimen in combination with nab-paclitaxel (arm B). Albeit limited by the small sample size, CC-486 monotherapy resulted in partial responses (three/eight) and stable disease (four/eight) in patients with nasopharyngeal cancer. Three of the stable disease responses lasted more than 150 days. Conclusions: CC-486 is well tolerated alone or in combination with carboplatin or nab-paclitaxel. Exploratory analyses suggest clinical activity of CC-486 monotherapy in nasopharyngeal cancer and provided the basis for an ongoing phase II clinical trial (ClinicalTrials.gov identifier: NCT02269943). Clin Cancer Res; 24(17); 4072–80. ©2018 AACR.

Published
2018
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21. A phase Ia study of CC-90003, a selective extracellular signal-regulated kinase (ERK) inhibitor, in patients with relapsed or refractory BRAF or RAS-mutant tumors

Author

Patricia LoRusso, Johanna C. Bendell, Xiaoling Wu, Eric Laille, Ida Aronchik, Gordon L. Bray, Nanette H Hock, Monica M. Mita, Ellen Filvaroff, Edward S. Kim, and Grant A. McArthur

Subjects
0301 basic medicine, Neuroblastoma RAS viral oncogene homolog, MAPK/ERK pathway, Cancer Research, medicine.medical_specialty, Hematology, medicine.diagnostic_test, business.industry, Mutant, Cardiac echo, medicine.disease_cause, Gastroenterology, Peripheral blood mononuclear cell, Transaminase, 03 medical and health sciences, 030104 developmental biology, Oncology, Internal medicine, medicine, KRAS, business
Abstract

2577 Background: CC-90003 is an irreversible inhibitor of ERK 1/2 with potent anti-proliferative activity in KRAS and BRAF mutant tumor models. We conducted a first-in-human study of CC-90003 in patients with RAS or BRAF mutant tumors. Methods: Patients received escalating doses of oral CC-90003 on a 21/28 day cycle. Standard safety (adverse events, chemistry/hematology, physical findings, ECGs and cardiac ECHO/MUGA scans) and PK parameters were assessed. Response was assessed per RECIST 1.1. A proprietary ELISA-based assay measured ERK levels unbound to CC-90003 in peripheral blood mononuclear cells. Results: Nineteen patients (median age: 60 yrs) harboring KRAS (n = 15), NRAS (n = 1), or BRAF (n = 3) mutant tumors received CC-90003 doses from 20 to 160 mg /day. The MTD was 120 mg based on the occurrence of Grade 3 transaminase elevations (n = 2) and hypertension (n = 1) observed at 160 mg (the NTD). Patients completed a median of 2 cycles (range: 1 to 5). AEs (mostly Grade 1 or 2) reported in ≥ 3 patients included constitutional (asthenia, fatigue), gastrointestinal (anorexia, nausea/vomiting, diarrhea), hepatic (transaminase elevations) and neurologic (dizziness, gait disturbance, paresthesias) toxicities. Grade 1-3 neurotoxicity was observed primarily at doses from 80 to 160 mg/day and resolved with dose reduction/interruption. PK parameters were highly variable, with AUC and Cmax increasing overall, with increasing dose. CC-90003 accumulation was observed after multiple doses. There were no objective responses. Levels of free ERK were reduced by ≥80% compared to baseline by C1D8 at doses ≥ 80 mg/day. Conclusions: ERK inhibition may be an attractive target for the management of mutant RAS or BRAF-driven tumors, however proof-of-concept demonstration for CC-90003 was limited by a lack of objective responses, an unfavorable PK profile and unanticipated neurotoxicity. Clinical trial information: NCT02313012.

Published
2017
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22. Dulanermin with rituximab in patients with relapsed indolent B-cell lymphoma: an open-label phase 1b/2 randomised study

Author

Avi Ashkenazi, Andrea Janíková, Myron S Czucman, Ian W. Flinn, Sean K. Kelley, Michelle A. Fanale, John F. Seymour, S. N. Holden, David Belada, Chan Yoon Cheah, Amy V. Kapp, and Gordon L Bray

Subjects
medicine.medical_specialty, Lymphoma, B-Cell, Follicular lymphoma, Antineoplastic Agents, Gastroenterology, TNF-Related Apoptosis-Inducing Ligand, 03 medical and health sciences, 0302 clinical medicine, International Prognostic Index, Recurrence, Internal medicine, Geographic site, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, B-cell lymphoma, Lymphoma, Follicular, Dulanermin, Czech Republic, business.industry, Australia, Hematology, medicine.disease, United States, 3. Good health, Surgery, Treatment Outcome, Tolerability, Italy, 030220 oncology & carcinogenesis, Rituximab, Chills, France, Poland, medicine.symptom, business, 030215 immunology, medicine.drug, New Zealand
Abstract

Summary Background Dulanermin—a non-polyhistidine-tagged soluble recombinant human apoptosis ligand 2 (Apo2L) or tumour-necrosis-factor-related apoptosis-inducing-ligand (TRAIL)—has pro-apoptotic activity in a range of cancers and synergistic preclinical activity with rituximab against lymphoma in vivo. We aimed to assess the safety, pharmacokinetics, and efficacy of dulanermin and rituximab in patients with relapsed indolent B-cell non-Hodgkin lymphoma. Methods We did an open-label phase 1b/2 randomised study. Four study centres in the USA enrolled patients into phase 1b, and 27 study centres in the USA, Italy, Australia, France, Czech Republic, New Zealand, and Poland enrolled patients into phase 2. In phase 1b, patients (age ≥18 years) with indolent B-cell non-Hodgkin lymphoma with stable disease or better lasting at least 6 months after the most recent rituximab-containing regimen were included. In phase 2, patients (age ≥18 years) with follicular lymphoma grades 1–3a were included. In phase 1b, patients received 4 mg/kg or 8 mg/kg intravenous dulanermin on days 1–5 of up to four 21-day cycles and intravenous rituximab 375 mg/m 2 weekly for up to eight doses. In phase 2, patients were randomly assigned (1:1:1) centrally by an interactive voice response system to dulanermin (8 mg/kg for a maximum of four 21-day cycles), rituximab (375 mg/m 2 weekly for up to eight doses), or both in combination, stratified by baseline follicular lymphoma International Prognostic Index (0–3 vs 4–5) and geographic site (USA vs non-USA). The primary endpoints of the phase 1b study were the safety, tolerability, and pharmacokinetics of dulanermin with rituximab. The primary endpoint of phase 2 was the proportion of patients who achieved an objective response. All patients who received any dose of study drug were included in safety analyses. Efficacy analyses were per protocol. Treatment was open label; all patients and investigators were unmasked to treatment allocation. This study is registered with ClinicalTrials.gov, NCT00400764. Findings Between June 6, 2006, and Feb 15, 2007, 12 patients were enrolled in phase 1b, and between April 4, 2007, and April 20, 2009, 60 patients were enrolled in phase 2, of whom 59 were included in safety analyses and 58 in efficacy analyses. No dose-limiting toxic effects were noted in phase 1b. The most common grade 1–2 adverse events in phase 1b were fatigue (nine; 75%), rash (five; 42%), and chills, decreased appetite, diarrhoea, and nausea (four each; 33%). 19 grade 3 or higher adverse effects were noted in five (42%) patients, with 14 occurring in one patient. After treatment with 8 mg/kg of dulanermin, in six patients the mean serum peak concentration was 80 μg/mL, dropping below the minimum detectable concentration (2 ng/mL) within 24 h after the dose. The mean steady state peak and trough concentrations of rituximab were 461 μg/mL (SD 97·5) and 303 μg/mL (92·8), respectively. In phase 2, eight (14%) of 59 patients experienced 12 grade 3 or higher adverse events. In phase 2, objective responses were noted in 14 of 22 (63·6%, 95% CI 41·8–81·3) patients treated with rituximab only, 16 of 25 (64·0%, 43·1–81·5) treated with dulanermin and rituximab, and one of 11 (9·1%, 0·5–39·0) treated with dulanermin only. The study was terminated early, on May 5, 2010, because of an absence of efficacy in the combination group. Interpretation The addition of dulanermin to rituximab in patients with indolent B-cell non-Hodgkin lymphoma was tolerable but did not lead to increased objective responses. This combination is not being developed further in non-Hodgkin lymphoma. Funding Genentech and Amgen.

Published
2014

23. Pharmacokinetics of Recombinant Factor VIII (Recombinate) Using One-stage Clotting and Chromogenic Factor VIII Assay

Author

T W Barrowcliffe, Daphne Owens, C. R. M. Hay, C. A. Lee, Gordon L. Bray, Edward D. Gomperts, Paul Giangrande, Phillip Schroth, and Peter William Collins

Subjects
Chromatography, medicine.diagnostic_test, Chromogenic, business.industry, Hematology, Recombinant factor viii, law.invention, Pharmacokinetics, law, In vivo, Immunology, Recombinant DNA, Bioassay, Potency, Medicine, business, Partial thromboplastin time
Abstract

SummaryIn a study designed to demonstrate the safety and pharmacokinetics of a recombinant factor VIII (Recombinate) manufactured in Andover, MA and Thousand Oaks, CA, two different methods of factor VIII assay (one-stage clotting and Chromogenic substrate) were compared in vivo. The study was performed in four centres in the UK: London, Oxford, Cardiff and Manchester. Two pharmacokinetic studies, at least one week apart, were performed in 30 patients with severe haemophilia A (VIII:C < 2 IU/dl). A dose of 50 IU/kg was administered with sampling pre-infusion, and +0.25, 0.5, 1, 3, 6, 9, 12 and 24 h post-infusion. The aggregate 60 pharmacokinetic study showed a half-life of 12.7 and 13.0 h (p = 0.28) and recovery of 127 and 161 IU/dl (p = 0.0001) using one-stage clotting or chromogenic substrate respectively. In a supplementary experiment, 20 post-infusion samples were re-assayed by 1-stage and chromogenic assay using two plasma (20th British plasma standard and an “in-house” pooled normal plasma) and two concentrate standards, derived from the same type, but different batch of infused concentrate (Recombinate) and pre-diluted in either individual pre-infusion sample or in pooled commercial haemophilic plasma. The use of the Recombinate concentrate standard overcame the significant difference in FVIII levels between 1-stage and chromogenic assay methods when a plasma standard was used (p

Published
1999
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24. Use of Fibrin Sealant in Thermal Injury

Author

Gordon L. Bray, Areta Kowal-Vern, Martin Lee, Edward D. Gomperts, Richard L. Gamelli, Victoria McGill, and David G. Greenhalgh

Subjects
Adult, Male, medicine.medical_specialty, Blood transfusion, Adolescent, medicine.medical_treatment, Blood Loss, Surgical, Fibrin Tissue Adhesive, Fibrin, Blood-Borne Pathogens, Humans, Medicine, Blood Transfusion, Hospital Costs, Child, Fibrin glue, General Nursing, Body surface area, Infection Control, biology, Hemostatic Techniques, business.industry, Rehabilitation, Albumin, Skin Transplantation, Length of Stay, Surgery, Treatment Outcome, Child, Preschool, General Health Professions, Emergency Medicine, biology.protein, Skin grafting, Female, Burns, business, Packed red blood cells, Total body surface area
Abstract

Fibrin glue is hemostatic in skin grafting and other therapeutic situations. This prospective, open-labeled comparative study involved thermally injured patients: 34 patients received fibrin sealant (FS) and 61 did not, at Loyola University Medical Center, Maywood, Illinois, and Shriners Burn Institute, Cincinnati, Ohio. FS-treated patients were 23.6 +/- 16.8 years old, versus 20.8 +/- 16.8 years for controls. The percentage of total body surface areas burn was 10.0% +/- 4.5% in the study patients versus 10.9% +/- 7.9% in the controls. The FS group did not receive packed red blood cell transfusions, albumin infusion, or topical bovine thrombin (TBT). The control group received 1.56 +/- 2.1 units of packed red blood cells, 186 +/- 194 ml 5% albumin, and TBT (20,000 units) 2.6 +/- 0.8 kits during excision and grafting procedures. The estimated blood loss/graft ration was 0.50 +/- 0.30 ml/cm2 (median = 0.46) for the study group versus 0.98 +/- 2.4 ml/cm2 (median = 0.56) for the control group (p = 0.14); for patients more than 16 years of age, this difference was significant (p = 0.03). FS may be a viable alternative to standard hemostatic techniques, because it reduced the need for blood transfusion, alloantigen exposure, and blood-borne viral infection risk. FS also eliminated the need for TBT and epinephrine, did not have an adverse impact on the surgical outcome, and tended to improve the cost differential.

Published
1997
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25. Pharmacokinetic In Vivo Comparison Using 1-Stage and Chromogenic Substrate Assays with Two Formulations of Hemofil-M

Author

T W Barrowcliffe, John Pasi, Dale Owens, P Lilley, Anthony R. Hubbard, Gordon L. Bray, L Von Tilberg, Edward D. Gomperts, C. A. Lee, and Geoffrey Kemball-Cook

Subjects
Pathology, medicine.medical_specialty, Chromatography, medicine.diagnostic_test, business.industry, Chromogenic, Hematology, Vial, Crossover study, Dosage form, Pharmacokinetics, In vivo, Medicine, Potency, business, Partial thromboplastin time
Abstract

SummaryIn a study to demonstrate the safety and pharmacokinetics (half-life and recovery) of two different method M purified AHF (Hemofil-M) concentrates processed in the USA and Spain, two different methods of factor VIII assay (one-stage clotting and chromogenic) have been compared in vivo. The study was a single centre blinded, randomised, crossover study. Twelve patients with severe haemophilia A (VIII: C

Published
1996
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26. A phase I safety and pharmacokinetic study of the death receptor 5 agonistic antibody PRO95780 in patients with advanced malignancies

Author

Gordon L Bray, D. Ross Camidge, Michael S. Gordon, Tanyifor M. Tohnya, Blythe Durbin, S. Gail Eckhardt, Razelle Kurzrock, Roy S. Herbst, Josephine Ing, David S. Mendelson, Jason Sager, and Avi Ashkenazi

Subjects
Male, Cancer Research, medicine.medical_specialty, Maximum Tolerated Dose, Antineoplastic Agents, Antibodies, Monoclonal, Humanized, Gastroenterology, Transaminase, Pharmacokinetics, Internal medicine, Neoplasms, Medicine, Humans, Trough Concentration, Adverse effect, Aged, Aged, 80 and over, business.industry, Cancer, Antibodies, Monoclonal, Middle Aged, medicine.disease, Receptors, TNF-Related Apoptosis-Inducing Ligand, Endocrinology, Oncology, Tolerability, Toxicity, Monoclonal, Female, business
Abstract

Purpose: PRO95780 is a fully human IgG1 monoclonal antibody that triggers the extrinsic apoptosis pathway through death receptor 5. This first-in-human study assessed the safety, tolerability, pharmacokinetics, and any early evidence of efficacy of PRO95780 in patients with advanced malignancies. Experimental Design: Target concentrations were predicted to occur at 10 mg/kg. Patients received up to eight cycles of PRO95780 i.v. using a 3+3 dose escalation design at 1 to 20 mg/kg every 14 days (every 28 days in cycle 1; stage 1), with cohort expansion at either the maximum tolerated dose or 10 mg/kg, whichever was lower (stage 2). Patients were evaluated for response every other cycle. Results: The maximum tolerated dose was not reached within this study. Four (8%) of 50 patients reported adverse events of greater than grade 2 at least possibly related to PRO95780, including 2 patients with reversible grade 3 transaminase elevation. The mean terminal half-life was 8.8 to 19.3 days, with dose-dependent increases in exposure (peak plasma concentration and area under the concentration) across 1 to 15 mg/kg. Most patients treated with 10 mg/kg or above achieved trough concentration above the target efficacious concentration at day 15 with moderate accumulation after multiple doses. No objective responses occurred, although three minor responses were observed in patients with colorectal and granulosa cell ovarian cancers (each treated with 4 mg/kg) and chondrosarcoma (10 mg/kg). Conclusions: PRO95780 is safe and well tolerated at doses up to 20 mg/kg. Evidence of activity was noted in several different tumor types at 4 and 10 mg/kg. Pharmacokinetic analysis supports a dosing regimen of 10 to 15 mg/kg every 2 to 3 weeks. Clin Cancer Res; 16(4); 1256–63

Published
2010

28. Comparison of the erythropoietin response in children with aplastic anemia, transient erythroblastopenia, and iron deficiency

Author

Gordon L. Bray, Regina O'Donnell, and Barbara J. Taylor

Subjects
medicine.medical_specialty, Anemia, Red-Cell Aplasia, Pure, Gastroenterology, Hemoglobins, hemic and lymphatic diseases, Internal medicine, medicine, Humans, Aplastic anemia, Child, Erythropoietin, Analysis of Variance, Anemia, Hypochromic, Transient erythroblastopenia of childhood, business.industry, Anemia, Aplastic, Infant, Iron deficiency, medicine.disease, Transient erythroblastopenia, Iron-deficiency anemia, Child, Preschool, Pediatrics, Perinatology and Child Health, Immunology, Hemoglobin, business, medicine.drug
Abstract

To assess the effects of decreased erythrocyte production on the levels of serum erythropoietin in children, we measured simultaneous hemoglobin concentrations and erythropoietin in 18 children with iron deficiency anemia, 17 children with transient erythroblastopenia of childhood (TEC), and 7 children with aplastic anemia. In all but two patients (one with TEC; one with aplastic anemia), erythropoietin was measured at diagnosis, before institution of specific therapy for the anemia. There was a statistically significant inverse linear correlation between log10 erythropoietin and hemoglobin values for all patient groups (r = 0.904 to 0.912; p less than 0.005). A comparison of the slopes of the regressions for each patient group by analysis of covariance revealed a significantly steeper slope for the iron deficiency group (-0.553) versus the TEC (-0.287) and aplastic anemia (-0.256) groups (p = 0.0001). The difference in erythropoietin levels appeared greatest in patients whose presenting hemoglobin level was greater than 5 gm/dl. Decline in serum erythropoietin levels was more precipitous in the less severely anemic patients with iron deficiency anemia than in the patients with TEC or aplastic anemia. These data reveal quantitative and qualitative differences in the relationship between serum erythropoietin and hemoglobin levels when children with severe iron deficiency anemia versus those with TEC or aplastic anemia are considered, even though all three conditions are characterized by hypoproliferation of erythrocytes.

Published
1992
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30. Erythropoietin Deficiency: A Complication of Cisplatin Therapy and Its Treatment with Recombinant Human Erythropoietin

Author

Gordon L. Bray and Gregory H. Reaman

Subjects
Adult, Male, inorganic chemicals, medicine.medical_specialty, Adolescent, Anemia, medicine.medical_treatment, Renal function, Pharmacology, hemic and lymphatic diseases, Internal medicine, medicine, Humans, Child, Erythropoietin, neoplasms, Cisplatin, Chemotherapy, Myelosuppressive Chemotherapy, business.industry, Hematology, medicine.disease, Recombinant Proteins, female genital diseases and pregnancy complications, Endocrinology, medicine.anatomical_structure, Oncology, Pediatrics, Perinatology and Child Health, Toxicity, Bone marrow, business, medicine.drug
Abstract

Cisplatin (CDDP) has been implicated in the development of anemia via several mechanisms of action, including shortening of red cell (RBC) survival and direct toxicity of the drug on RBC bone marrow precursors. Recent studies and case reports suggest an association between CDDP and the development of hyporegenerative anemia as a consequence of relative erythropoietin (EPO) deficiency. To study the effects of CDDP on the relationship between serum EPO and hemoglobin (Hb) concentration, we measured levels of EPO in 12 patients (1-21 years of age) who were treated with cumulative doses of CDDP ranging from 300 to 720 mg/m2 for a variety of pediatric malignancies. Post-CDDP glomerular filtration rates (GFR) varied from 29 to 143 ml/min/1.73 m2 for 11 of the 12 patients studied. At the completion of CDDP therapy, an inverse linear relationship between log(10) serum EPO and Hb was noted among those patients who retained at least 40-50% of their pre-CDDP therapy GFR. One patient with chronic renal failure at the completion of CDDP therapy (GFR 25-35 ml/min/1.73 m2) exhibited a chronic transfusion-dependent, hyporegenerative anemia that was due to persistently low levels of EPO. Institution of recombinant human (r-Hu) EPO therapy resulted in an abrupt cessation of this patient's RBC transfusion dependency. Additional studies are needed to further characterize the effects of CDDP on EPO production and secretion and to determine optimal dosing schedules for r-Hu EPO in pediatric patients who receive CDDP and other myelosuppressive chemotherapy.

Published
1991
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31. Normal and disordered coagulation in the neonate

Author

Gordon L. Bray

Subjects
medicine.medical_specialty, Pediatrics, Fetus, Neonatal Diseases, Mechanism (biology), business.industry, medicine.medical_treatment, Immunology, Hematology, medicine.disease, Thrombosis, Plasma products, Fibrinolysis, medicine, Coagulation (water treatment), Intensive care medicine, business, Coagulation Disorder
Abstract

Over the past 10–15 yr, improvements in perinatal and neonatal care and in the laboratory diagnosis and monitoring of coagulation disorders have lead to significant reductions in morbidity and mortality from bleeding and thrombosis in sick and low birth-weight infants. Recent advances in our understanding of the normal developmental changes that occur in the coagulation mechanism of the fetus and newborn now allow for more intelligent and rational approaches to the treatment of disordered coagulation and fibrinolysis. This review will focus on current knowledge of the normal changes that occur in the coagulation mechanism during late fetal development and early infancy. Subsequent discussion will deal with how developmental aspects of the coagulation mechanism impact upon morbidity and mortality from common neonatal diseases. The diagnosis and management of specific bleeding and thrombotic syndromes of neonates will also be discussed. Finally, a brief overview of the indications for use of plasma products in neonatal medicine will be presented.

Published
1991
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33. A prospective study of human immunodeficiency virus type 1 infection and the development of AIDS in subjects with hemophilia

Author

Goedert, James J., Kessler, Craig M., Aledort, Louis M., Biggar, Robert J., Andes, W. Abe, White, Gilbert C., II, Drummond, James E., Vaidya, Kampala, Mann, Dean L., Eyster, M. Elaine, Ragni, Margaret V., Lederman, Michael M., Cohen, Alan R., Gordon, L. Bray, Rosenberg, Philip S., Friedman, Robert M., Hilgartner, Margaret W., Blattner, William A., Kroner, Barbara, and Gail, Mitchell H.

Subjects
AIDS (Disease) -- Demographic aspects, HIV antigens -- Measurement, HIV (Viruses)
Abstract

AIDS (acquired immunodeficiency syndrome) has been shown to be caused by the human immunodeficiency virus (HIV). However, the onset of the disease does not necessarily occur shortly after the person becomes infected. Infection by the virus itself is judged by the presence of specific antibodies that are produced by the body against the infection, and by the number of a particular class of lymphocytes (a type of white blood cell; the measurement is known as the CD4+ cell count). The rate of individuals developing AIDS after detection of HIV antibodies in their blood (seroconversion) has been studied in a group of individuals for whom the precise time of infection is known, namely hemophiliacs. Unlike individuals who have a high-risk lifestyle (e.g., homosexuals or drug users), patients with hemophilia usually become infected with HIV by medical treatment with contaminated human blood products; treatment records often allow determination of the time of infection. Out of a group of 1,219 individuals with hemophilia or similar conditions, 319 individuals for whom the date of HIV seroconversion was known were studied in detail. Statistical analysis of this group led to the finding that the risk of AIDS is directly related to age in individuals that seroconvert. The risk of an individual developing full-blown AIDS after infection is 2.67 per 100 person-years for the total population, 0.83 for persons between 1 and 11, and 5.66 for individuals 35 to 70. The common predictors, the number of CD4+ lymphocytes and a decrease in the quantity of antibodies produced against the virus (anti-p24 or anti- gp120), were valid indicators of increasing risk of AIDS in adults. Adolescents, on the other hand, had a lower rate of antibody loss, and a lower rate of AIDS after loss of anti-p24. There is thus evidence that the disease is more devastating among older individuals, and that children and adolescents are more resistant to developing AIDS. The article also speculates on the meaning of these findings, and suggests that the problems of AIDS are related to the re-initiation of previous infections that have been accumulated during a longer life.

Published
1989

34. Antibodies to heterologous proteins in hemophilia A patients receiving recombinant factor VIII (Recombinate)

Author

Gordon L. Bray, Edward D. Gomperts, Kirsten Christiansen, Hanne Berg Ravn, and Jørgen Ingerslev

Subjects
Adult, Male, Heterologous, Antibodies, Heterophile, CHO Cells, Hemophilia A, Immunoglobulin G, law.invention, Mice, Cricetulus, Immune system, Antibody Specificity, law, Cricetinae, Coagulopathy, Animals, Humans, Medicine, Prospective Studies, Bovine serum albumin, Child, Factor VIII, biology, business.industry, Chinese hamster ovary cell, Serum Albumin, Bovine, Hematology, medicine.disease, Recombinant Proteins, Antibodies, Anti-Idiotypic, Culture Media, Child, Preschool, Immunology, Recombinant DNA, biology.protein, Cattle, Immunization, Antibody, Drug Contamination, business
Abstract

SummaryAs a consequence of the manufacturing process, trace quantities of Chinese hamster ovary cell protein, bovine serum albumin and murine immunoglobulin G are present in Recombinate™ recombinant human factor VIII (rhFVIII). The development of antibodies (Abs) to these heterologous proteins was evaluated during long-term rhFVIII therapy of hemophilia A in 68 previously treated and 73 previously untreated patients. Ab prevalence was also assessed in 157 non-hemophilic subjects. Abs against heterologous proteins could be detected in varying percentages of patients and non-hemophilic subjects. Abs arose in patients sporadically, and levels were typically low. There were no adverse events associated with development or presence of anti-heterologous protein Abs. These data indicate that sustained immune responses to trace levels of heterologous proteins are very infrequent during long-term rhFVIII therapy.

Published
2002

35. 551 Phase 1B study of CC-486 (oral azacitidine) in tumors associated with a viral etiology

Author

S.R. Hatty, Johanna C. Bendell, Kejian Liu, J.H.M. Schellens, D. D. Von Hoff, J. Tomaro, Jose A. Lopez-Martin, Gordon L. Bray, J.F. Di Martino, N. Isambert, Drew W. Rasco, R. Sarmiento, C. Le Tourneau, Pamela N. Munster, and Aaron N. Nguyen

Subjects
Cisplatin, Cancer Research, Reporter gene, Chemistry, Poly ADP ribose polymerase, Molecular biology, Oral Azacitidine, Blot, Oncology, Apoptosis, medicine, Electrophoretic mobility shift assay, Etoposide, medicine.drug
Abstract

Materials and Methods: The use of plant extracts to alleviate inflammatory diseases is centuries old and continues to this day, therefore we screened thirty-four methanolic plant extracts for inhibition of constitutive NF-uB activity by a NF-uB-luciferase reporter gene assay. There was strong inhibition of NF-uB activity by Nuphar lutea L. SM. (Nuphar), leaf and rhizome extracts. An active fraction containing a mixture of dimeric sesquiterpene thioalkaloids was purified by solvent extraction, pH adjustment silica gel chromatography and HPLC. Oneand twodimensional NMR spectroscopy indicated the presence of nupharidine, 6-hydroxythionuphlutine as a major component. Results: Nupharidine showed a dose dependent inhibition of NF-uB activity by luciferase reporter gene assay as well as reduction of nuclear NF-uB subunits expression as tested by western blots and immunohistochemistry. Diminution of DNA binding was demonstrated by Electro Mobility Shift Assay (EMSA). Nupharidine inhibited both inducible and constitutive NF-uB activation and affected the canonical and alternative pathways. Suppression of NF-uB was not cell type specific. Conclusions: Induction of apoptosis by Nupharidine was demonstrated by time and dose dependent cleavage of procaspase-9 and PARP. Synergistic cytotoxicity of nupharidine with cisplatin and etoposide was demonstrated, therefore suggesting its possible use as a ‘sensitizer’ in anticancer treatment.

Published
2014
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36. Multicenter trial to evaluate the safety and potential efficacy of pooled human fibrin sealant for the treatment of burn wounds

Author

Martin Lee, Martin Macphee, John B. Lynch, Richard L. Gamelli, Gordon L. Bray, John F. Hansbrough, Sidney F. Miller, Bruce M. Achauer, Mehan Delavari, and David G. Greenhalgh

Subjects
Adult, Male, medicine.medical_specialty, Adolescent, medicine.medical_treatment, Detergents, Fibrin Tissue Adhesive, Fibrin, law.invention, Randomized controlled trial, law, Multicenter trial, medicine, Humans, Prospective Studies, Child, Aged, Wound Healing, biology, business.industry, Sealant, Skin Transplantation, Middle Aged, Hemostasis, Surgical, Surgery, Clinical trial, Virus Diseases, Hemostasis, biology.protein, Solvents, Skin grafting, Female, Tissue Adhesives, Tissue Preservation, Wound healing, business, Burns
Abstract

Objective The primary purpose of this multicenter study was to evaluate the safety and potential efficacy of a solvent/detergent-treated commercial fibrin sealant (human) for topical hemostasis in skin grafting. Methods The study involved a prospective evaluation of changes in viral titers in patients with burns less than 15% after treatment with fibrin sealant (human). Each patient served as his/her own control for an unblinded, randomized comparison of donor site hemostasis and healing. Preoperative serum was obtained to screen for viral titers. At autografting, the recipient site and one of two randomly chosen donor sites were treated with fibrin sealant (human). The use of other hemostatic agents, including epinephrine was prohibited. Each donor site was covered with gauze to collect blood for estimation of the relative amount of bleeding. The healing of the graft and donor sites was observed. Viral titers and wounds were checked monthly for 6 months, and at 9 and 12 months postoperatively. Results Viral titers for human immunodeficiency virus; hepatitis A, B, and C; Epstein-Barr virus; and cytomegalovirus were obtained before and after treatment. Of 47 patients, 34 completed the full year of observation. After treatment, there were no seroconversions to any of the aforementioned viruses. Bleeding at the recipient site appeared well controlled with fibrin sealant (human). Although investigators felt that fibrin sealant (human) improved donor site hemostasis, differences in hemoglobin measurements of blood-soaked dressings failed to reach significance. No differences were noted with regard to acceleration of donor site healing, graft take, or scar maturation at the two groups of donor sites. Anecdotally, the maturation of the recipient site appeared to be accelerated. Conclusion Fibrin sealant (human) is safe for use during excision and grafting, and its topical hemostatic potential needs to be examined in patients with larger burns. Its role in scar maturation also needs to be investigated.

Published
1999

37. Loss of high-responder inhibitors in patients with severe hemophilia A and human immunodeficiency virus type 1 infection: a report from the Multi-Center Hemophilia Cohort Study

Author

Goedert Jj, Margaret W. Hilgartner, Barbara Kroner, Gordon L. Bray, M. E. Eyster, LW Aledort, S Arkin, and Margaret V. Ragni

Subjects
Adult, medicine.medical_specialty, HIV Infections, Bethesda unit, Hemophilia A, Gastroenterology, Cohort Studies, Isoantibodies, Internal medicine, Immunopathology, Coagulopathy, Medicine, Humans, Child, Retrospective Studies, Factor VIII, business.industry, Infant, Hematology, medicine.disease, Titer, Hemostasis, Child, Preschool, Immune System, Immunology, HIV-1, Viral disease, business, Natural history study, Cohort study
Abstract

To evaluate the effects of human immunodeficiency virus type 1 (HIV-1) infection on the loss of factor VIII alloantibodies, we identified 77 patients with a history of inhibitors from among a large cohort of HIV-1-infected participants enrolled in a natural history study of HIV-1 infection in hemophilia. Fifty-six patients were high responders with inhibitors titers greater than 5 Bethesda Units (BU) measured on at least one occasion. From May 1985 to December 1989, 13 of the high-responder patients were rechallenged with factor VIII concentrates after several years of treatment with other plasma products. All exhibited excellent hemostasis upon reinstitution of factor VIII. Seven of the 13 patients (11.3–46.3 years of age) were in the advanced stages of HIV-1 infection at the time of rechallenge. Inhibitor titers measured subsequent to the reinstitution of factor VIII were consistently less than 1 BU in five of these seven patients. The remaining six patients (6.1–57.5 years of age) had mild to moderate CD4+ lymphocyte depletion (absolute CD4+ cells: 262–935/ mm3) at the time of factor VIII rechallenge. Follow-up inhibitor titers were negative 7–42 months after consistent factor VIII use in these six patients. The lack of anamnestic response to factor VIII in all 13 patients who were rechallenged indicates that HIV-1-infected patients who have a history of high-responder inhibitors frequently benefit from the reintroduction of factor VIII use for the control of bleeding, regardless of their stage of HIV-1 disease. © 1993 Wiley-Liss, Inc.

Published
1993

38. Comparison of High Responder Inhibitor Frequency in Recent Studies of Previously Untreated Patients with Hemophilia A

Author

Gordon L. Bray, Edward D. Gomperts, and Hartmut J. Ehrlich

Subjects
congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, High responder, business.industry, Vascular biology, Hematology, medicine.disease, Gastroenterology, Thrombosis, Surgery, hemic and lymphatic diseases, Internal medicine, medicine, business
Abstract

Comparison of High Responder Inhibitor Frequency in Recent Studies of Previously Untreated Patients with Hemophilia A

Published
1998
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41. Incidence of Lymphomas and Other Cancers in HIV-Infected and HIV-Uninfected Patients With Hemophilia

Author

W. Abe Andes, Angelos Hatzakis, M. Elaine Eyster, Gordon L. Bray, Wolfgang Schramm, Craig M. Kessler, Alan R. Cohen, Margaret W. Hilgartner, Gilbert C. White, Charles S. Rabkin, James J. Goedert, Louis M. Aledort, Philippe de Moerloose, Katie W. Hedberg, S. Eichinger, Marilyn J. Manco-Johnson, Barbara Kroner, William A. Blattner, Michael M. Lederman, and University of Groningen

Subjects
medicine.medical_specialty, medicine.medical_treatment, Population, PAPILLOMAVIRUS, KAPOSIS-SARCOMA, DISEASE, Acquired immunodeficiency syndrome (AIDS), Internal medicine, medicine, Coagulopathy, education, NON-HODGKIN LYMPHOMA, RISK, education.field_of_study, business.industry, Incidence (epidemiology), Immunosuppression, General Medicine, medicine.disease, Lymphoma, AIDS, HUMAN-IMMUNODEFICIENCY-VIRUS, Immunology, RENAL-TRANSPLANT RECIPIENTS, Viral disease, business, Cohort study
Abstract

Objective. —To determine the types and rates of cancers occurring in excess in the presence of infection with the human immunodeficiency virus type 1 (HIV-1). Design. —Cohort analytic study of HIV-infected and HIV-uninfected subjects followed for up to 12 years. Setting. —Fifteen hemophilia treatment centers. Patients. —A total of 1701 patients with hemophilia, of whom 1065 (63%) were HIV-1 seropositive. Main Outcome Measures. —Morphologic classification and incidence rates of cancers. Main Results. —The incidence of non-Hodgkin's lymphoma after HIV seroconversion averaged 0.15 case per 100 person-years (95% confidence interval [CI], 0.08 to 0.25) and rose exponentially with increasing duration of HIV infection. Although the greatest absolute risk of lymphoma was in the oldest age group, the relative increase compared with general population rates was 38-fold in subjects 10 to 39 years old and 12-fold in older subjects ( P + T-lymphocyte levels for lymphoma cases were similar to HIV-positive subjects without the acquired immunodeficiency syndrome (AIDS) who had been infected for the same length of time. The incidence of Kaposi's sarcoma was increased 200-fold (95% CI, 20 to 700). The incidence of cancers other than non-Hodgkin's lymphoma and Kaposi's sarcoma were not increased in the HIV-positive subjects (ratio of observed to expected cases, 0.9 [95% CI, 0.4 to 1.9]). The HIV-negative subjects had no significant increase in cancer incidence. Conclusions. —HIV infection has restricted effects on cancer incidence that are only partly explained by immunosuppression. Paradoxically, improvements in therapy of HIV infection that prolong survival may lead to further increases in HIVassociated lymphoma. ( JAMA . 1992;267:1090-1094)

Published
1992
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42. Hemorrhage Involving the Upper Airway in Hemophilia

Author

Diane J. Nugent and Gordon L. Bray

Subjects
Male, medicine.medical_specialty, Hemorrhage, Hemophilia B, 03 medical and health sciences, 0302 clinical medicine, Hematoma, 030225 pediatrics, medicine, Sore throat, Coagulopathy, Humans, business.industry, Incidence (epidemiology), Pharyngeal Diseases, medicine.disease, Dysphagia, Surgery, Radiography, Child, Preschool, Pediatrics, Perinatology and Child Health, medicine.symptom, Presentation (obstetrics), business, Airway, Complication
Abstract

Bleeding involving the upper airway is a rare, highly emergent complication of hemophilia. This report describes the occurrence of two distinct episodes in a patient with severe factor IX deficiency. Clinical data from other cases described in the literature is summarized with regard to predisposing factors, age of incidence, presenting symptomatology, diagnosis, and management. Pertinent features of this bleeding complication include: high prevalence involving the pediatric population, presentation with non-specific symptoms (e.g., sore throat, dysphagia) early in the course of the bleeding episode, progression to complete upper respiratory obstruction if not recognized and treated, and the need for relatively high levels of the deficient coagulation factor for a period of at least 7 days to ensure resolution of the hematoma. The diagnosis is confirmed by observing retropharyngeal soft-tissue widening on lateral neck x-ray or alternatively, via cervical computed tomography.

Published
1986
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43. Danazol fails to increase factor VIII or IX levels in a double-blind crossover study of patients with haemophilia A and B

Author

Arthur R. Thompson, Diane J. Nugent, Richard B. Counts, Maribel J. Clements, and Gordon L. Bray

Subjects
medicine.medical_specialty, Haemophilia A, Fibrinogen, Placebo, Hemophilia A, Hemophilia B, Factor IX, Double-Blind Method, hemic and lymphatic diseases, Internal medicine, Pregnadienes, Medicine, Humans, Haemophilia B, Danazol, Factor VIII, medicine.diagnostic_test, business.industry, Hematology, medicine.disease, Crossover study, Endocrinology, Drug Evaluation, business, Partial thromboplastin time, medicine.drug
Abstract

Twenty-one patients, 14 with haemophilia A and seven with haemophilia B, completed a double-blind crossover study to evaluate the effects of danazol on factor VIII and factor IX levels. Clotting and immunoradiometric assays were used to measure factor levels at baseline, 2 weeks and 8 weeks on both danazol and placebo. Fibrinogen, plasminogen and activated partial thromboplastin time were measured on all patients during placebo and danazol treatment. Although plasminogen levels rose significantly (P less than 0.01) and fibrinogen decreased (P less than 0.01), factor VIII and IX levels did not change. While on danazol, three patients had increased bleeding and shortened euglobulin lysis times compared to their baseline levels. We conclude that danazol does not raise factor VIII or IX levels and increases bleeding in some patients.

Published
1986

44. A prospective study of human immunodeficiency virus type 1 infection and the development of AIDS in subjects with hemophilia

Author

Gordon L. Bray, Kampala Vaidya, Barbara Kroner, W. Abe Andes, Craig M. Kessler, Philip S. Rosenberg, Alan R. Cohen, Mitchell H. Gail, Robert M. Friedman, Robert J. Biggar, Michael M. Lederman, William A. Blattner, James E. Drummond, Margaret W. Hilgartner, Margaret V. Ragni, Gilbert C. White, James J. Goedert, Dean L. Mann, M. Elaine Eyster, and Louis M. Aledort

Subjects
Adult, CD4-Positive T-Lymphocytes, Pediatrics, medicine.medical_specialty, Time Factors, Adolescent, Human immunodeficiency virus (HIV), HIV Core Protein p24, Gene Products, gag, HIV Antibodies, HIV Envelope Protein gp120, medicine.disease_cause, Hemophilia A, Cohort Studies, Acquired immunodeficiency syndrome (AIDS), HIV Seropositivity, medicine, Humans, Multicenter Studies as Topic, Prospective Studies, Seroconversion, Prospective cohort study, Child, Aged, Acquired Immunodeficiency Syndrome, business.industry, Viral Core Proteins, Age Factors, Infant, General Medicine, Middle Aged, medicine.disease, P24 antigen, Child, Preschool, Immunology, Cohort, Viral disease, Interferons, business, Drug Contamination, Biomarkers, Cohort study
Abstract

We evaluated a multicenter cohort of 1219 subjects with hemophilia or related disorders prospectively, focusing on 319 subjects with documented dates of seroconversion to human immunodeficiency virus type 1 (HIV-1). The incidence rate of the acquired immunodeficiency syndrome (AIDS) after seroconversion was 2.67 per 100 person-years and was directly related to age (from 0.83 in persons 1 to 11 years old up to 5.66 in persons 35 to 70 years old; Ptrend = 0.00003). The annual incidence of AIDS ranged from zero during the first year after seroconversion to 7 percent during the eighth year, with eight-year cumulative rates (+/- SE) of 13.3 +/- 5.3 percent for ages 1 to 17, 26.8 +/- 6.4 percent for ages 18 to 34, and 43.7 +/- 16.4 percent for ages 35 to 70. Serial immunologic and virologic markers (total numbers of CD4 lymphocytes, presence of serum interferon or HIV-1 p24 antigen, and low or absent serum levels of anti-p24 or anti-gp120) predicted a high risk for the subsequent development of AIDS. Adults 35 to 70 years old had a higher incidence of low CD4 counts than younger subjects (P less than or equal to 0.005), whereas adolescents had a low rate of anti-p24 loss (P = 0.0007) and subjects 1 to 17 years old had a lower incidence of AIDS after loss of anti-p24 (P = 0.03). These findings not only demonstrate that the risk of AIDS is related directly to age but also suggest that older adults are disproportionately affected during the earlier phases of HIV disease, that adolescents may have a low replication rate of HIV, and that children and adolescents may tolerate severe immunodeficiency better because they have fewer other infections or because of some unmeasured, age-dependent cofactor or immune alteration in the later phase of HIV disease.

Published
1989

45. LOSS OF NATURALLY ACQUIRED HEPATITIS B SURFACE ANTI-BODY (ANTI-HBs) IN TWO HEMOPHILIACS WITH AIDS RELATED COMPLEX

Author

Gregory Reaman and Gordon L. Bray

Subjects
Anti hbs, biology, business.industry, Pediatrics, Perinatology and Child Health, Immunology, AIDS-related complex, biology.protein, Medicine, Hepatitis B, Antibody, business, medicine.disease, Virology
Abstract

LOSS OF NATURALLY ACQUIRED HEPATITIS B SURFACE ANTI-BODY (ANTI-HBs) IN TWO HEMOPHILIACS WITH AIDS RELATED COMPLEX

Published
1987
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