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1. North American Blastic Plasmacytoid Dendritic Cell Neoplasm Consortium: position on standards of care and areas of need

Author

Naveen Pemmaraju, Hagop Kantarjian, Kendra Sweet, Eunice Wang, Jayastu Senapati, Nathaniel R. Wilson, Marina Konopleva, Arthur E. Frankel, Vikas Gupta, Ruben Mesa, Matthew Ulrickson, Edward Gorak, Sumeet Bhatia, Tulin Budak-Alpdogan, James Mason, Maria Teresa Garcia-Romero, Norma Lopez-Santiago, Gabriela Cesarman-Maus, Pankit Vachhani, Sangmin Lee, Vijaya Raj Bhatt, William Blum, Roland B. Walter, Dale Bixby, Ivana Gojo, Madeleine Duvic, Raajit K. Rampal, Marcos de Lima, James Foran, Amir T. Fathi, Aric Cameron Hall, Meagan A. Jacoby, Jeffrey Lancet, Gabriel Mannis, Anthony S. Stein, Alice Mims, David Rizzieri, Rebecca Olin, Alexander Perl, Gary Schiller, Paul Shami, Richard M. Stone, Stephen Strickland, Matthew J. Wieduwilt, Naval Daver, Farhad Ravandi, Sumithira Vasu, Monica Guzman, Gail J. Roboz, Joseph Khoury, Muzaffar Qazilbash, Phyu P. Aung, Branko Cuglievan, Yazan Madanat, Mohamed A. Kharfan-Dabaja, Anna Pawlowska, Justin Taylor, Martin Tallman, Prajwal Dhakal, and Andrew A. Lane

Subjects
Immunology, Cell Biology, Hematology, Biochemistry
Abstract

Blastic plasmacytoid dendritic cell neoplasm (BPDCN) is a rare hematologic malignancy with historically poor outcomes and no worldwide consensus treatment approach. Unique among most hematologic malignancies for its frequent cutaneous involvement, BPDCN can also invade other extramedullary compartments, including the central nervous system. Generally affecting older adults, many patients are unfit to receive intensive chemotherapy, and although hematopoietic stem cell transplantation is preferred for younger, fit individuals, not all are eligible. One recent therapeutic breakthrough is that all BPDCNs express CD123 (IL3Rα) and that this accessible surface marker can be pharmacologically targeted. The first-in-class agent for BPDCN, tagraxofusp, which targets CD123, was approved in December 2018 in the United States for patients with BPDCN aged ≥2 years. Despite favorable response rates in the frontline setting, many patients still relapse in the setting of monotherapy, and outcomes in patients with relapsed/refractory BPDCN remain dismal. Therefore, novel approaches targeting both CD123 and other targets are actively being investigated. To begin to formally address the state of the field, we formed a new collaborative initiative, the North American BPDCN Consortium (NABC). This group of experts, which includes a multidisciplinary panel of hematologists/oncologists, hematopoietic stem cell transplant physicians, pathologists, dermatologists, and pediatric oncologists, was tasked with defining the current standard of care in the field and identifying the most important research questions and future directions in BPDCN. The position findings of the NABC’s inaugural meetings are presented herein.

Published
2023

2. Data from Matrix Metalloproteinase–Activated Anthrax Lethal Toxin Inhibits Endothelial Invasion and Neovasculature Formation during In vitro Morphogenesis

Author

Arthur E. Frankel, Nicholas S. Duesbery, Samuel H. Davis, Arlynn F. Mulne, Terry C. Lairmore, Cynthia J. Meininger, Thomas H. Bugge, Shihui Liu, Stephen H. Leppla, and Randall W. Alfano

Abstract

Solid tumor growth is dependent on angiogenesis, the formation of neovasculature from existing vessels. Endothelial activation of the extracellular signal–regulated kinase 1/2, c-jun NH2-terminal kinase, and p38 mitogen-activated protein kinase pathways is central to this process, and thus presents an attractive target for the development of angiogenesis inhibitors. Anthrax lethal toxin (LeTx) has potent catalytic mitogen-activated protein kinase inhibition activity. Preclinical studies showed that LeTx induced potent tumor growth inhibition via the inhibition of xenograft vascularization. However, LeTx receptors and the essential furin-like activating proteases are expressed in many normal tissues, potentially limiting the specificity of LeTx as an antitumor agent. To circumvent nonspecific LeTx activation and simultaneously enhance tumor vascular targeting, a substrate preferably cleaved by the gelatinases class of matrix metalloproteinases (MMP) was substituted for the furin LeTx activation site. In vivo efficacy studies showed that this MMP-activated LeTx inhibited tumor xenografts growth via the reduced migration of endothelial cells into the tumor parenchyma. Here we have expanded on these initial findings by showing that this MMP-activated LeTx reduces endothelial proangiogenic MMP expression, thus causing a diminished proteolytic capacity for extracellular matrix remodeling and endothelial differentiation into capillary networks. Additionally, our data suggest that inhibition of the c-jun NH2-terminal kinase and p38, but not extracellular signal–regulated kinase-1/2, pathways is significant in the antiangiogenic activity of the MMP-activated LeTx. Collectively, these results support the clinical development of the MMP-activated LeTx for the treatment of solid tumors. (Mol Cancer Res 2009;7(4):452–61)

Published
2023

3. Supplementary Data from Matrix Metalloproteinase–Activated Anthrax Lethal Toxin Inhibits Endothelial Invasion and Neovasculature Formation during In vitro Morphogenesis

Author

Arthur E. Frankel, Nicholas S. Duesbery, Samuel H. Davis, Arlynn F. Mulne, Terry C. Lairmore, Cynthia J. Meininger, Thomas H. Bugge, Shihui Liu, Stephen H. Leppla, and Randall W. Alfano

Abstract

Supplementary Data from Matrix Metalloproteinase–Activated Anthrax Lethal Toxin Inhibits Endothelial Invasion and Neovasculature Formation during In vitro Morphogenesis

Published
2023

4. Supplementary Figures S1-S3 from Matrix Metalloproteinase–Activated Anthrax Lethal Toxin Inhibits Endothelial Invasion and Neovasculature Formation during In vitro Morphogenesis

Author

Arthur E. Frankel, Nicholas S. Duesbery, Samuel H. Davis, Arlynn F. Mulne, Terry C. Lairmore, Cynthia J. Meininger, Thomas H. Bugge, Shihui Liu, Stephen H. Leppla, and Randall W. Alfano

Abstract

Supplementary Figures S1-S3 from Matrix Metalloproteinase–Activated Anthrax Lethal Toxin Inhibits Endothelial Invasion and Neovasculature Formation during In vitro Morphogenesis

Published
2023

5. Data from Cytotoxicity of the matrix metalloproteinase–activated anthrax lethal toxin is dependent on gelatinase expression and B-RAF status in human melanoma cells

Author

Arthur E. Frankel, Nicholas S. Duesbery, Jennifer L. Bromberg-White, Keiran S. Smalley, Meenhard Herlyn, Thomas H. Bugge, Shihui Liu, Stephen H. Leppla, and Randall W. Alfano

Abstract

Anthrax lethal toxin (LeTx) shows potent mitogen-activated protein kinase pathway inhibition and apoptosis in melanoma cells that harbor the activating V600E B-RAF mutation. LeTx is composed of two proteins, protective antigen and lethal factor. Uptake of the toxin into cells is dependent on proteolytic activation of protective antigen by the ubiquitously expressed furin or furin-like proteases. To circumvent nonspecific LeTx activation, a substrate preferably cleaved by gelatinases was substituted for the furin LeTx activation site. Here, we have shown that the toxicity of this matrix metalloproteinase (MMP)–activated LeTx is dependent on host cell surface MMP-2 and MMP-9 activity as well as the presence of the activating V600E B-RAF mutation, making this toxin dual specific. This additional layer of tumor cell specificity would potentially decrease systemic toxicity from the reduction of nonspecific toxin activation while retaining antitumor efficacy in patients with V600E B-RAF melanomas. Moreover, our results indicate that cell surface-associated gelatinase expression can be used to predict sensitivity among V600E B-RAF melanomas. This finding will aid in the better selection of patients that will potentially respond to MMP-activated LeTx therapy. [Mol Cancer Ther 2008;7(5):1218–26]

Published
2023

6. Data from HIF-2 Complex Dissociation, Target Inhibition, and Acquired Resistance with PT2385, a First-in-Class HIF-2 Inhibitor, in Patients with Clear Cell Renal Cell Carcinoma

Author

James Brugarolas, Ivan Pedrosa, Tao Wang, Payal Kapur, Renée M. McKay, Brian I. Rini, Robert A. Figlin, Oscar Reig Torras, Tiffani McKenzie, Song Zhang, Sanjeeva Kalva, Arthur E. Frankel, Yull Arriaga, Oluwatomilade Fatunde, Jenny Chang, Yue Zhang, Yin Xi, Qing Yuan, Ananth J. Madhuranthakam, Haley Hill, Allison Joyce, Nirmish Singla, Layton Woolford, Zhiqun Xie, Alana Christie, Alberto Diaz de Leon, Yuanqing Ma, and Kevin D. Courtney

Abstract

Purpose:The heterodimeric transcription factor HIF-2 is arguably the most important driver of clear cell renal cell carcinoma (ccRCC). Although considered undruggable, structural analyses at the University of Texas Southwestern Medical Center (UTSW, Dallas, TX) identified a vulnerability in the α subunit, which heterodimerizes with HIF1β, ultimately leading to the development of PT2385, a first-in-class inhibitor. PT2385 was safe and active in a first-in-human phase I clinical trial of patients with extensively pretreated ccRCC at UTSW and elsewhere. There were no dose-limiting toxicities, and disease control ≥4 months was achieved in 42% of patients.Patients and Methods:We conducted a prospective companion substudy involving a subset of patients enrolled in the phase I clinical trial at UTSW (n = 10), who were treated at the phase II dose or above, involving multiparametric MRI, blood draws, and serial biopsies for biochemical, whole exome, and RNA-sequencing studies.Results:PT2385 inhibited HIF-2 in nontumor tissues, as determined by a reduction in erythropoietin levels (a pharmacodynamic marker), in all but one patient, who had the lowest drug concentrations. PT2385 dissociated HIF-2 complexes in ccRCC metastases, and inhibited HIF-2 target gene expression. In contrast, HIF-1 complexes were unaffected. Prolonged PT2385 treatment resulted in the acquisition of resistance, and we identified a gatekeeper mutation (G323E) in HIF2α, which interferes with drug binding and precluded HIF-2 complex dissociation. In addition, we identified an acquired TP53 mutation elsewhere, suggesting a possible alternate mechanism of resistance.Conclusions:These findings demonstrate a core dependency on HIF-2 in metastatic ccRCC and establish PT2385 as a highly specific HIF-2 inhibitor in humans. New approaches will be required to target mutant HIF-2 beyond PT2385 or the closely related PT2977 (MK-6482).

Published
2023

7. Supplementary Figure 2 from Inhibition of Tumor Angiogenesis by the Matrix Metalloproteinase–Activated Anthrax Lethal Toxin in an Orthotopic Model of Anaplastic Thyroid Carcinoma

Author

Arthur E. Frankel, Fiemu Nwariaku, Ian C. Mitchell, Nicholas S. Duesbery, Terry C. Lairmore, Janelle M. Ortiz, Thomas H. Bugge, Shihui Liu, Stephen H. Leppla, and Randall W. Alfano

Abstract

Supplementary Figure 2 from Inhibition of Tumor Angiogenesis by the Matrix Metalloproteinase–Activated Anthrax Lethal Toxin in an Orthotopic Model of Anaplastic Thyroid Carcinoma

Published
2023

8. Figure S1 from HIF-2 Complex Dissociation, Target Inhibition, and Acquired Resistance with PT2385, a First-in-Class HIF-2 Inhibitor, in Patients with Clear Cell Renal Cell Carcinoma

Author

James Brugarolas, Ivan Pedrosa, Tao Wang, Payal Kapur, Renée M. McKay, Brian I. Rini, Robert A. Figlin, Oscar Reig Torras, Tiffani McKenzie, Song Zhang, Sanjeeva Kalva, Arthur E. Frankel, Yull Arriaga, Oluwatomilade Fatunde, Jenny Chang, Yue Zhang, Yin Xi, Qing Yuan, Ananth J. Madhuranthakam, Haley Hill, Allison Joyce, Nirmish Singla, Layton Woolford, Zhiqun Xie, Alana Christie, Alberto Diaz de Leon, Yuanqing Ma, and Kevin D. Courtney

Abstract

Supplementary Figure S1. Pharmacodynamic analyses and illustrative mpMRI studies.

Published
2023

11. Tables S2-S9 from HIF-2 Complex Dissociation, Target Inhibition, and Acquired Resistance with PT2385, a First-in-Class HIF-2 Inhibitor, in Patients with Clear Cell Renal Cell Carcinoma

Author

James Brugarolas, Ivan Pedrosa, Tao Wang, Payal Kapur, Renée M. McKay, Brian I. Rini, Robert A. Figlin, Oscar Reig Torras, Tiffani McKenzie, Song Zhang, Sanjeeva Kalva, Arthur E. Frankel, Yull Arriaga, Oluwatomilade Fatunde, Jenny Chang, Yue Zhang, Yin Xi, Qing Yuan, Ananth J. Madhuranthakam, Haley Hill, Allison Joyce, Nirmish Singla, Layton Woolford, Zhiqun Xie, Alana Christie, Alberto Diaz de Leon, Yuanqing Ma, and Kevin D. Courtney

Abstract

Supplementary Tables S2-S9.

Published
2023

12. Supplementary Data Legends from HIF-2 Complex Dissociation, Target Inhibition, and Acquired Resistance with PT2385, a First-in-Class HIF-2 Inhibitor, in Patients with Clear Cell Renal Cell Carcinoma

Author

James Brugarolas, Ivan Pedrosa, Tao Wang, Payal Kapur, Renée M. McKay, Brian I. Rini, Robert A. Figlin, Oscar Reig Torras, Tiffani McKenzie, Song Zhang, Sanjeeva Kalva, Arthur E. Frankel, Yull Arriaga, Oluwatomilade Fatunde, Jenny Chang, Yue Zhang, Yin Xi, Qing Yuan, Ananth J. Madhuranthakam, Haley Hill, Allison Joyce, Nirmish Singla, Layton Woolford, Zhiqun Xie, Alana Christie, Alberto Diaz de Leon, Yuanqing Ma, and Kevin D. Courtney

Abstract

Supplementary Data Legends

Published
2023

13. Data from Inhibition of Tumor Angiogenesis by the Matrix Metalloproteinase–Activated Anthrax Lethal Toxin in an Orthotopic Model of Anaplastic Thyroid Carcinoma

Author

Arthur E. Frankel, Fiemu Nwariaku, Ian C. Mitchell, Nicholas S. Duesbery, Terry C. Lairmore, Janelle M. Ortiz, Thomas H. Bugge, Shihui Liu, Stephen H. Leppla, and Randall W. Alfano

Abstract

Patients with anaplastic thyroid carcinoma (ATC) typically succumb to their disease months after diagnosis despite aggressive therapy. A large percentage of ATCs have been shown to harbor the V600E B-Raf point mutation, leading to the constitutive activation of the mitogen-activated protein kinase pathway. ATC invasion, metastasis, and angiogenesis are in part dependent on the gelatinase class of matrix metalloproteinases (MMP). The explicit targeting of these two tumor markers may provide a novel therapeutic strategy for the treatment of ATC. The MMP-activated anthrax lethal toxin (LeTx), a novel recombinant protein toxin combination, shows potent mitogen-activated protein kinase pathway inhibition in gelatinase-expressing V600E B-Raf tumor cells in vitro. However, preliminary in vivo studies showed that the MMP-activated LeTx also exhibited dramatic antitumor activity against xenografts that did not show significant antiproliferative responses to the LeTx in vitro. Here, we show that the MMP-activated LeTx inhibits orthotopic ATC xenograft progression in both toxin-sensitive and toxin-resistant ATC cells via reduced endothelial cell recruitment and subsequent tumor vascularization. This in turn translates to an improved long-term survival that is comparable with that produced by the multikinase inhibitor sorafenib. Our results also indicate that therapy with the MMP-activated LeTx is extremely effective against advanced tumors with well-established vascular networks. Taken together, these results suggest that the MMP-activated LeTx-mediated endothelial cell targeting is the primary in vivo antitumor mechanism of this novel toxin. Therefore, the MMP-activated LeTx could be used not only in the clinical management of V600E B-Raf ATC but potentially in any solid tumor. Mol Cancer Ther; 9(1); 190–201

Published
2023

19. Supplementary Fig. S2 from Cytotoxicity of the matrix metalloproteinase–activated anthrax lethal toxin is dependent on gelatinase expression and B-RAF status in human melanoma cells

Author

Arthur E. Frankel, Nicholas S. Duesbery, Jennifer L. Bromberg-White, Keiran S. Smalley, Meenhard Herlyn, Thomas H. Bugge, Shihui Liu, Stephen H. Leppla, and Randall W. Alfano

Abstract

Supplementary Fig. S2 from Cytotoxicity of the matrix metalloproteinase–activated anthrax lethal toxin is dependent on gelatinase expression and B-RAF status in human melanoma cells

Published
2023

20. Supplementary Figure 1 from Inhibition of Tumor Angiogenesis by the Matrix Metalloproteinase–Activated Anthrax Lethal Toxin in an Orthotopic Model of Anaplastic Thyroid Carcinoma

Author

Arthur E. Frankel, Fiemu Nwariaku, Ian C. Mitchell, Nicholas S. Duesbery, Terry C. Lairmore, Janelle M. Ortiz, Thomas H. Bugge, Shihui Liu, Stephen H. Leppla, and Randall W. Alfano

Abstract

Supplementary Figure 1 from Inhibition of Tumor Angiogenesis by the Matrix Metalloproteinase–Activated Anthrax Lethal Toxin in an Orthotopic Model of Anaplastic Thyroid Carcinoma

Published
2023

21. Figure S4 from HIF-2 Complex Dissociation, Target Inhibition, and Acquired Resistance with PT2385, a First-in-Class HIF-2 Inhibitor, in Patients with Clear Cell Renal Cell Carcinoma

Author

James Brugarolas, Ivan Pedrosa, Tao Wang, Payal Kapur, Renée M. McKay, Brian I. Rini, Robert A. Figlin, Oscar Reig Torras, Tiffani McKenzie, Song Zhang, Sanjeeva Kalva, Arthur E. Frankel, Yull Arriaga, Oluwatomilade Fatunde, Jenny Chang, Yue Zhang, Yin Xi, Qing Yuan, Ananth J. Madhuranthakam, Haley Hill, Allison Joyce, Nirmish Singla, Layton Woolford, Zhiqun Xie, Alana Christie, Alberto Diaz de Leon, Yuanqing Ma, and Kevin D. Courtney

Abstract

Supplementary Figure S4. p53 mutation in Pt27 metastasis progressing on PT2385.

Published
2023

22. Table S1 from HIF-2 Complex Dissociation, Target Inhibition, and Acquired Resistance with PT2385, a First-in-Class HIF-2 Inhibitor, in Patients with Clear Cell Renal Cell Carcinoma

Author

James Brugarolas, Ivan Pedrosa, Tao Wang, Payal Kapur, Renée M. McKay, Brian I. Rini, Robert A. Figlin, Oscar Reig Torras, Tiffani McKenzie, Song Zhang, Sanjeeva Kalva, Arthur E. Frankel, Yull Arriaga, Oluwatomilade Fatunde, Jenny Chang, Yue Zhang, Yin Xi, Qing Yuan, Ananth J. Madhuranthakam, Haley Hill, Allison Joyce, Nirmish Singla, Layton Woolford, Zhiqun Xie, Alana Christie, Alberto Diaz de Leon, Yuanqing Ma, and Kevin D. Courtney

Abstract

Supplementary Table S1. Multiparametric magnetic resonance imaging (mpMRI) acquisition parameters.

Published
2023

23. Supplementary Fig. S1 from Cytotoxicity of the matrix metalloproteinase–activated anthrax lethal toxin is dependent on gelatinase expression and B-RAF status in human melanoma cells

Author

Arthur E. Frankel, Nicholas S. Duesbery, Jennifer L. Bromberg-White, Keiran S. Smalley, Meenhard Herlyn, Thomas H. Bugge, Shihui Liu, Stephen H. Leppla, and Randall W. Alfano

Abstract

Supplementary Fig. S1 from Cytotoxicity of the matrix metalloproteinase–activated anthrax lethal toxin is dependent on gelatinase expression and B-RAF status in human melanoma cells

Published
2023

25. Figure S2 from HIF-2 Complex Dissociation, Target Inhibition, and Acquired Resistance with PT2385, a First-in-Class HIF-2 Inhibitor, in Patients with Clear Cell Renal Cell Carcinoma

Author

James Brugarolas, Ivan Pedrosa, Tao Wang, Payal Kapur, Renée M. McKay, Brian I. Rini, Robert A. Figlin, Oscar Reig Torras, Tiffani McKenzie, Song Zhang, Sanjeeva Kalva, Arthur E. Frankel, Yull Arriaga, Oluwatomilade Fatunde, Jenny Chang, Yue Zhang, Yin Xi, Qing Yuan, Ananth J. Madhuranthakam, Haley Hill, Allison Joyce, Nirmish Singla, Layton Woolford, Zhiqun Xie, Alana Christie, Alberto Diaz de Leon, Yuanqing Ma, and Kevin D. Courtney

Abstract

Supplementary Figure S2. PT2385 does not affect HIF-1 complexes.

Published
2023

26. Figure S3 from HIF-2 Complex Dissociation, Target Inhibition, and Acquired Resistance with PT2385, a First-in-Class HIF-2 Inhibitor, in Patients with Clear Cell Renal Cell Carcinoma

Author

James Brugarolas, Ivan Pedrosa, Tao Wang, Payal Kapur, Renée M. McKay, Brian I. Rini, Robert A. Figlin, Oscar Reig Torras, Tiffani McKenzie, Song Zhang, Sanjeeva Kalva, Arthur E. Frankel, Yull Arriaga, Oluwatomilade Fatunde, Jenny Chang, Yue Zhang, Yin Xi, Qing Yuan, Ananth J. Madhuranthakam, Haley Hill, Allison Joyce, Nirmish Singla, Layton Woolford, Zhiqun Xie, Alana Christie, Alberto Diaz de Leon, Yuanqing Ma, and Kevin D. Courtney

Abstract

Supplementary Figure S3. HIF-2a resistance mutation in Pt35 metastasis progressing on PT2385.

Published
2023

27. Data from Systematic Urokinase-Activated Anthrax Toxin Therapy Produces Regressions of Subcutaneous Human Non–Small Cell Lung Tumor in Athymic Nude Mice

Author

Arthur E. Frankel, Stephen H. Leppla, Ravibhushan Singh, Thomas H. Bugge, Shihui Liu, Janelle Ortiz, and Yunpeng Su

Abstract

The novel recombinant anthrax toxin, PrAgU2/FP59, composed of the urokinase-activated protective antigen and a fusion protein of Pseudomonas exotoxin and lethal factor was tested for anti–lung cancer efficacy in an in vivo human tumor model. Male athymic nude mice (age 4–6 weeks) were inoculated s.c. with 10 million H1299 non–small cell lung cancer (NSCLC) cells in the left flank. When tumor volumes reached 200 mm3 (6–8 days), i.p. injection of 100 μL saline or different ratios and doses of PrAgU2/FP59 in 100 μL saline were given every 3 days for four doses and an additional dose at day 29. Animals were monitored twice daily and tumor measurements were made by calipers. The maximum tolerated doses of PrAgU2/FP59 differed dependent on the ratios of PrAgU2 to FP59 over the range of 3:1 to 25:1, respectively. At tolerated doses, tumor regressions were seen in all animals. Complete histologic remission lasting 60 days occurred in 30% of animals. PrAgU2/FP59 showed dramatic anti-NSCLC efficacy and warrants further clinical development for therapy of patients with advanced NSCLC. [Cancer Res 2007;67(7):3329–36]

Published
2023

29. Capillary morphogenesis gene 2 (CMG2) mediates growth factor-induced angiogenesis by regulating endothelial cell chemotaxis

Author

Lorna M. Cryan, Tsz-Ming Tsang, Jessica Stiles, Lauren Bazinet, Sai Lun Lee, Samuel Garrard, Erika Madrian, Cody Roberts, Jessie Payne, Andrew Jensen, Arthur E. Frankel, P. Christine Ackroyd, Kenneth A. Christensen, and Michael S. Rogers

Subjects
Mice, Cancer Research, Neovascularization, Pathologic, Receptors, Peptide, Physiology, Chemotaxis, Clinical Biochemistry, Animals, Endothelial Cells, Intercellular Signaling Peptides and Proteins, Ligands
Abstract

Anthrax protective antigen (PA) is a potent inhibitor of pathological angiogenesis with an unknown mechanism. In anthrax intoxication, PA interacts with capillary morphogenesis gene 2 (CMG2) and tumor endothelial marker 8 (TEM8). Here, we show that CMG2 mediates the antiangiogenic effects of PA and is required for growth-factor-induced chemotaxis. Using specific inhibitors of CMG2 and TEM8 interaction with natural ligand, as well as mice with the CMG2 or TEM8 transmembrane and intracellular domains disrupted, we demonstrate that inhibiting CMG2, but not TEM8 reduces growth-factor-induced angiogenesis in the cornea. Furthermore, the antiangiogenic effect of PA was abolished when the CMG2, but not the TEM8, gene was disrupted. Binding experiments demonstrated a broad ligand specificity for CMG2 among extracellular matrix (ECM) proteins. Ex vivo experiments demonstrated that CMG2 (but not TEM8) is required for PA activity in human dermal microvascular endothelial cell (HMVEC-d) network formation assays. Remarkably, blocking CMG2-ligand binding with PA or CRISPR knockout abolishes endothelial cell chemotaxis but not chemokinesis in microfluidic migration assays. These effects are phenocopied by Rho inhibition. Because CMG2 mediates the chemotactic response of endothelial cells to peptide growth factors in an ECM-dependent fashion, CMG2 is well-placed to integrate growth factor and ECM signals. Thus, CMG2 targeting is a novel way to inhibit angiogenesis.

Published
2022

30. Bioinformatic Analysis Underpinning the Frequent Occurrence of Immune Thrombocytopenic Purpura in COVID-19 Patients

Author

Arthur E, Frankel, Dennis, Wylie, Bjoern, Peters, Daniel, Marrama, and Chul, Ahn

Subjects
Purpura, Thrombocytopenic, Idiopathic, SARS-CoV-2, COVID-19, Computational Biology, Humans, Pandemics
Abstract

Secondary immune thrombocytopenic purpura (ITP) associated with coronavirus disease 2019 (COVID-19) is a rare but serious complication of the pandemic. Diagnostic criteria include clinical and laboratory findings. Early treatment is often effective, but rare severe bleeding and death can occur. An autoimmune mechanism is likely.To determine a role for molecular mimicry in producing disease.Hexapeptide and heptapeptide matches between severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) and platelet N-glycosylated proteins and other human proteins were assessed.Shared viral and platelet glycoprotein peptides were found. Copy frequency of these peptides in the human proteome was low for many of the candidate molecular mimics.The data support a contribution of molecular mimicry in COVID-19 ITP autoimmunity and offer avenues for in vitro diagnostic assay development. The continuation of the pandemic necessitates additional understanding of COVID-19 ITP as well as studies on diagnosis and mitigation.

Published
2022

31. Blastic plasmacytoid dendritic cell neoplasms: results of an international survey on 398 adult patients

Author

Tomohiro Aoki, Mohamad Sobh, Alix Baugier de Materre, Carlo Cota, Kamel Laribi, Arthur E. Frankel, Caterina Giovanna Valentini, David Ghez, Ritsuro Suzuki, T. Petrella, Livio Pagano, Ronan Le Calloch, Kengo Takeuchi, and Lorenzo Cerroni

Subjects
Adult, medicine.medical_specialty, Palliative care, Clinical Trials and Observations, medicine.medical_treatment, Plasmacytoid dendritic cell, Hematopoietic stem cell transplantation, Transplantation, Autologous, immune system diseases, hemic and lymphatic diseases, Internal medicine, medicine, Humans, Chemotherapy, Acute leukemia, business.industry, Hematopoietic Stem Cell Transplantation, Dendritic Cells, Hematology, medicine.disease, Lymphoma, Radiation therapy, Transplantation, Leukemia, Myeloid, Acute, Settore MED/15 - MALATTIE DEL SANGUE, Acute Disease, Blastic plasmocitoid dendritic cell leukemia, business
Abstract

The purpose of this study is to describe the clinical and prognostic features and to evaluate the outcome of different therapeutic approaches among patients with blastic plasmacytoid dendritic cell neoplasm (BPDCN) who have been diagnosed and treated in different institutions. A total of 398 patients from 75 centers were included in the study. Treatment consisted of non-Hodgkin lymphoma (NHL)–like regimens in 129 (32.8%) patients and acute leukemia (AL)–like regimens in 113 (23.5%) patients. In 61 (15.5%) and 16 (4.1%) patients, chemotherapy was followed by allogeneic and autologous hematopoietic stem cell transplantation (HSCT), respectively. Twenty-seven (6.9%) patients received radiotherapy, 6 (1.5%) received new agents, and 62 (15.7%) received palliative care. After a median follow-up of 12 months, median overall survival (OS) was 18 months. Patients who received NHL/AL-like regimens, followed by allogeneic HSCT, had the best outcome; median OS was not reached. OS was 65 months for patients who underwent autologous HSCT; 18 months and 14 months, respectively, for those treated with AL-like and NHL-like regimens without consolidation; and 4 months for those receiving palliative care (P < .001). In BPDCN, chemotherapy with lymphoma- or AL-like regimens, followed by transplantation, represents the therapeutic strategy associated with the best outcome. Consolidation with allogeneic HSCT, when feasible, appears superior to autologous HSCT.

Published
2020

32. HIF-2 Complex Dissociation, Target Inhibition, and Acquired Resistance with PT2385, a First-in-Class HIF-2 Inhibitor, in Patients with Clear Cell Renal Cell Carcinoma

Author

Renée M. McKay, Yue Zhang, Ivan Pedrosa, Brian I. Rini, James Brugarolas, Alana Christie, Nirmish Singla, Alberto Diaz de Leon, Haley Hill, Yull Edwin Arriaga, Robert A. Figlin, Sanjeeva P. Kalva, Zhiqun Xie, Layton Woolford, Tao Wang, Kevin D. Courtney, Yin Xi, Qing Yuan, Oscar Reig Torras, Arthur E. Frankel, Yuanqing Ma, Oluwatomilade Fatunde, Payal Kapur, Tiffani McKenzie, Ananth J. Madhuranthakam, Jenny Chang, Song Zhang, and Allison Joyce

Subjects
Male, 0301 basic medicine, Cancer Research, Mutant, Phases of clinical research, Drug resistance, Article, 03 medical and health sciences, 0302 clinical medicine, Basic Helix-Loop-Helix Transcription Factors, medicine, Carcinoma, Humans, Neoplasm, Prospective Studies, Sulfones, Multiparametric Magnetic Resonance Imaging, Carcinoma, Renal Cell, Transcription factor, Aged, Clinical Trials, Phase I as Topic, business.industry, Middle Aged, medicine.disease, Kidney Neoplasms, Clear cell renal cell carcinoma, 030104 developmental biology, Oncology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Indans, Cancer research, Female, business, Blood drawing
Abstract

Purpose: The heterodimeric transcription factor HIF-2 is arguably the most important driver of clear cell renal cell carcinoma (ccRCC). Although considered undruggable, structural analyses at the University of Texas Southwestern Medical Center (UTSW, Dallas, TX) identified a vulnerability in the α subunit, which heterodimerizes with HIF1β, ultimately leading to the development of PT2385, a first-in-class inhibitor. PT2385 was safe and active in a first-in-human phase I clinical trial of patients with extensively pretreated ccRCC at UTSW and elsewhere. There were no dose-limiting toxicities, and disease control ≥4 months was achieved in 42% of patients. Patients and Methods: We conducted a prospective companion substudy involving a subset of patients enrolled in the phase I clinical trial at UTSW (n = 10), who were treated at the phase II dose or above, involving multiparametric MRI, blood draws, and serial biopsies for biochemical, whole exome, and RNA-sequencing studies. Results: PT2385 inhibited HIF-2 in nontumor tissues, as determined by a reduction in erythropoietin levels (a pharmacodynamic marker), in all but one patient, who had the lowest drug concentrations. PT2385 dissociated HIF-2 complexes in ccRCC metastases, and inhibited HIF-2 target gene expression. In contrast, HIF-1 complexes were unaffected. Prolonged PT2385 treatment resulted in the acquisition of resistance, and we identified a gatekeeper mutation (G323E) in HIF2α, which interferes with drug binding and precluded HIF-2 complex dissociation. In addition, we identified an acquired TP53 mutation elsewhere, suggesting a possible alternate mechanism of resistance. Conclusions: These findings demonstrate a core dependency on HIF-2 in metastatic ccRCC and establish PT2385 as a highly specific HIF-2 inhibitor in humans. New approaches will be required to target mutant HIF-2 beyond PT2385 or the closely related PT2977 (MK-6482).

Published
2020

33. The Human Microbiota in Multiple Myeloma and Proteasome Inhibitors

Author

Morie A. Gertz, Omar Alkharabsheh, Arthur E. Frankel, Mohammed A. Aljama, and M. Hasib Sidiqi

Subjects
medicine.medical_treatment, Plasma Cells, Disease, Gut flora, digestive system, Somatic evolution in cancer, medicine, Humans, Antineoplastic Agents, Alkylating, Multiple myeloma, Gastrointestinal tract, biology, business.industry, NF-kappa B, Human microbiome, Hematology, General Medicine, Immunotherapy, biology.organism_classification, medicine.disease, Gastrointestinal Microbiome, Proteasome, Immunology, Cytokines, Multiple Myeloma, business, Proteasome Inhibitors, Signal Transduction
Abstract

The gut microbiota plays a significant role in health and disease, including cancer development and treatment. The importance of the gut microbiota in the efficacy and toxicity of novel therapies and immunotherapy is increasingly recognized. Plasma cells in multiple myeloma have the potential to survive in the gastrointestinal tract for long periods of time. The nature of the gut microbiota impacts the degree of antigen stimulation of these cells and may play a role in mutation development and clonal evolution. Furthermore, myeloma therapies such as proteasome inhibitors and alkylating agents, commonly used to treat patients, are frequently associated with gastrointestinal adverse events. Herein we review the gut microbiota and its role in hematopoiesis, pathogenesis of myeloma, and efficacy/toxicity of anti-myeloma therapies.

Published
2019

34. Roles of the cGAS-STING Pathway in Cancer Immunosurveillance and Immunotherapy

Author

Arthur E. Frankel, Minghao Li, Zhijian J. Chen, and Seoyun Yum

Subjects
0301 basic medicine, Cancer Research, Innate immune system, ATP synthase, biology, business.industry, medicine.medical_treatment, Cancer, Cell Biology, Immunotherapy, medicine.disease, eye diseases, Immunosurveillance, 03 medical and health sciences, Sting, 030104 developmental biology, 0302 clinical medicine, Oncology, Cancer immunotherapy, 030220 oncology & carcinogenesis, Stimulator of interferon genes, Cancer research, medicine, biology.protein, business
Abstract

Cyclic GMP-AMP synthase (cGAS) is a cytosolic DNA sensor that initiates innate immune responses. DNA-bound cGAS produces cyclic GMP-AMP (cGAMP), which activates stimulator of interferon genes (STING) to induce inflammatory cytokines and other immune mediators. cGAS detects DNA without sequence specificity and responds to both cytosolic foreign DNA from pathogens and self-DNA leaked into the cytosol due to genome instability or cellular damage. Because of the diverse sources of cytosolic DNA, the cGAS-STING pathway plays a critical role during infection, autoimmune diseases, and senescence. Moreover, cGAS detects tumor-derived DNA and stimulates endogenous antitumor immunity. Thus, the cGAS-STING pathway is a promising target for cancer immunotherapy. Here, we review the role of the cGAS-STING pathway in various diseases and highlight various approaches targeting the cGAS-STING pathway for cancer therapy.

Published
2019

35. First-in-human study of the safety, pharmacokinetics, and pharmacodynamics of first-in-class fatty acid synthase inhibitor TVB-2640 alone and with a taxane in advanced tumors

Author

George Kemble, Natalie Cook, Kathleen N. Moore, Andrew Brenner, Jeffrey R. Infante, Shubham Pant, Emma Dean, Hendrik-Tobias Arkenau, Erkut Borazanci, Katharine Grimmer, Howard A. Burris, Manish R. Patel, Juanita Lopez, Gerald Steven Falchook, Peter Schmid, William McCulloch, Arthur E. Frankel, and Marie O'Farrell

Subjects
medicine.medical_specialty, Medicine (General), 01 natural sciences, Gastroenterology, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Breast cancer, R5-920, Clinical trials, Pharmacokinetics, Internal medicine, medicine, 030212 general & internal medicine, 0101 mathematics, Lung cancer, Adverse effect, Pharmacology, Taxane, Performance status, business.industry, Drug mechanisms, 010102 general mathematics, General Medicine, medicine.disease, Docetaxel, Paclitaxel, chemistry, Gynecological cancers, business, Biomarkers, medicine.drug, Research Paper, Small molecule agents
Abstract

Background We conducted a first-in-human dose-escalation study with the oral FASN inhibitor TVB-2640 to determine the maximum tolerated dose (MTD) and recommended phase 2 dose (RP2D), as monotherapy and with a taxane. Methods This completed open-label outpatient study was conducted at 11 sites in the United States and United Kingdom. Patients with previously-treated advanced metastatic solid tumors and adequate performance status and organ function were eligible. TVB-2640 was administered orally daily until PD. Dose escalation initially followed an accelerated titration design that switched to a standard 3 + 3 design after Grade 2 toxicity occurred. Disease-specific cohorts were enrolled at the MTD. Statistical analyses were primarily descriptive. Safety analyses were performed on patients who received at least 1 dose of study drug. (Clinicaltrials.gov identifier NCT02223247) Findings The study was conducted from 21 November 2013 to 07 February 2017. Overall, 136 patients received TVB-2640, 76 as monotherapy (weight-based doses of 60 mg/m2 to 240 mg/m2 and flat doses of 200 and 250 mg) and 60 in combination, (weight-based doses of 60 mg/m2 to 100 mg/m2 and flat dose of 200 mg) (55 paclitaxel, 5 docetaxel). DLTs with TVB-2640 were reversible skin and ocular effects. The MTD/RP2D was 100 mg/m2. The most common TEAEs (n,%) with TVB-2640 monotherapy were alopecia (46; 61%), PPE syndrome (35; 46%), fatigue (28; 37%), decreased appetite (20; 26%), and dry skin (17; 22%), and with TVB-2640+paclitaxel were fatigue (29 ; 53%), alopecia (25; 46%), PPE syndrome (25; 46%), nausea (22; 40%), and peripheral neuropathy (20; 36%). One fatal case of drug-related pneumonitis occurred with TVB-2640+paclitaxel; no other treatment-related deaths occurred. Target engagement (FASN inhibition) and inhibition of lipogenesis were demonstrated with TVB-2640. The disease control rate (DCR) with TVB-2640 monotherapy was 42%; no patient treated with monotherapy had a complete or partial response (CR or PR). In combination with paclitaxel, the PR rate was 11% and the DCR was 70%. Responses were seen across multiple tumor types, including in patients with KRASMUT NSCLC, ovarian, and breast cancer. Interpretation TVB-2640 demonstrated potent FASN inhibition and a predictable and manageable safety profile, primarily characterized by non-serious, reversible adverse events affecting skin and eyes. Further investigation of TVB-2640 in patients with solid tumors, particularly in KRASMUT lung, ovarian, and breast cancer, is warranted. Funding This trial was funded by 3-V Biosciences, Inc. (now known as Sagimet Biosciences Inc.).

Published
2021

36. Response to pegylated interferon in a COVID-19-positive elderly woman with primary myelofibrosis treated with ruxolitinib

Author

Kayla Desuza, Yushuang Xie, Davey M. Smith, Hans Carl Hasselbalch, Arthur E. Frankel, Aaron F. Carlin, Eknath Naik, Khaled Deeb, Renuka Reddy, and Richard T. Silver

Subjects
Medicine (General), medicine.medical_specialty, Ruxolitinib, Coronavirus disease 2019 (COVID-19), Combination therapy, ruxolitinib, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), viruses, Case Report, Case Reports, 030204 cardiovascular system & hematology, Asymptomatic, Gastroenterology, 03 medical and health sciences, R5-920, 0302 clinical medicine, Pegylated interferon, Interferon, COVID‐19, Internal medicine, Medicine, Viral rna, Myelofibrosis, business.industry, COVID-19, General Medicine, interferon, medicine.disease, 030220 oncology & carcinogenesis, medicine.symptom, business, medicine.drug
Abstract

An 83‐year‐old female had asymptomatic SARS‐CoV‐2 infection while taking ruxolitinib. She remained RT‐PCR positive for viral RNA for >120 days, and Pegylated interferon for 4 weeks led to viral RNA clearance. The observations support combination therapy of ruxolitinib + interferon for COVID‐19., An 83‐year‐old female had asymptomatic SARS‐CoV‐2 infection while taking ruxolitinib. She remained RT‐PCR positive for viral RNA for > 120 days, and Pegylated interferon for 4 weeks led to viral RNA clearance. The observations support combination therapy of ruxolitinib + interferon for COVID‐19.

Published
2021

37. Response to pegylated interferon in a COVID-19 positive male with metastatic jejunal neuroendocrine tumor treated with everolimus

Author

Wai C. Yip, Hans Carl Hasselbalch, Arthur E. Frankel, and Eknath Naik

Subjects
Medicine (General), Coronavirus disease 2019 (COVID-19), Combination therapy, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), viruses, Case Report, Case Reports, 030204 cardiovascular system & hematology, infectious diseases, 03 medical and health sciences, R5-920, 0302 clinical medicine, Pegylated interferon, Interferon, medicine, Viral rna, Everolimus, business.industry, General Medicine, 030220 oncology & carcinogenesis, oncology, Cancer research, Medicine, pharmacology, business, medicine.drug, Clearance
Abstract

A 61‐year‐old male on everolimus had chronic SARS‐CoV‐2 infection. Addition of pegylated interferon cleared viral RNA and supports combination therapy with everolimus plus interferon for COVID‐19.

Published
2021

38. A Phase I/Ib Trial of PD 0332991 (Palbociclib) and T-DM1 in HER2-Positive Advanced Breast Cancer After Trastuzumab and Taxane Therapy

Author

Arthur E. Frankel, Melanie Hullings, Nisha Unni, Melissa Rodriguez, Thomas W. Froehlich, Dawn Klemow, Kiran Batra, Sunati Sahoo, Barbara Haley, and Chul Ahn

Subjects
0301 basic medicine, Oncology, Adult, Bridged-Ring Compounds, Cancer Research, medicine.medical_specialty, Maximum Tolerated Dose, Pyridines, Antineoplastic Agents, Breast Neoplasms, Palbociclib, Ado-Trastuzumab Emtansine, Piperazines, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Trastuzumab, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Taxane, business.industry, Cancer, Middle Aged, medicine.disease, 030104 developmental biology, 030220 oncology & carcinogenesis, Neratinib, Toxicity, Female, Taxoids, Pertuzumab, business, medicine.drug
Abstract

Background Preclinical breast cancer models with acquired HER2 resistance exhibit decreased proliferation with CDK4/6 inhibition in tumors with intact Rb and low p16 levels. Adding cytotoxic agents like T-DM1 enhances the inhibitory CDK4/6 cytostatic effect. Patients and Methods A phase I/Ib 3+3 dose escalation/expansion trial of palbociclib and T-DM1 identified 150 mg on days 5 to 18 as the palbociclib maximal tolerated dose combined with day 1 intravenous T-DM1 in 21-day treatment cycles. Patients were previously treated with trastuzumab and a taxane with no limitation on prior therapy lines, including prior pertuzumab, lapitinib, neratinib, and T-DM1. Median age was 54 years and two-thirds were estrogen receptor positive. Primary objectives included maximum tolerated dose as determined by dose-limiting toxicity, and secondary end points of safety, toxicity, response rate, response duration, and progression-free survival. Results From May 2014 to August 2018, 18 total patients were treated. The median number of cycles was 6.5 (1–22). A maximum tolerated dose was not reached. The most common G3 toxicity of more than 10% incidence was hematologic. Overall response rate (complete response + partial response) was 33% (95% confidence interval, 13%–59%). Median duration of response in responders was not reached and median-progression free survival was 6 months (95% confidence interval, 2.5–11.6). Conclusions The combination of day 1 T-DM1 and days 5 to 18 palbociclib is safe, tolerable, and active in previously treated HER2-positive relapsed patients. Observed hematologic toxicity is manageable. The trial response rate confirms that a CDK 4/6 inhibitor can resensitize HER2-resistant breast cancer.

Published
2020

39. Genetically Engineered Toxins

Author

Arthur E. Frankel

Subjects
Diphtheria toxin, Corynebacterium diphtheriae, biology, Molecular cloning, biology.organism_classification, medicine.disease_cause, Fusion protein, Virology, humanities, Microbiology, chemistry.chemical_compound, Ricin, chemistry, Fusion Toxin, medicine, Pseudomonas exotoxin, Escherichia coli
Abstract

Strategies and techniques - general methods, Robert F. Weaver, cloning strategies, Richard Intres and John W. Crabb, protein engineering strategies, Marc Whitlow, general strategies in in vivo animal modelling, Daniel A. Vallera and Bruce R. Blazar ricin - molecular cloning of ricin, Lynne R. Roberts, et al, expression of plant-derived ribosome-inactivating proteins in heterologous systems, Michael Piatak, Jr, and Noriyuki Habuka, the structure of plant toxins as a guide to rational design, Jon D. Robertus, chemical and genetic characterization of the enzymatic activity associated with ricin A chain, Lawrence Greenfield, chimeric proteins containing ricin A chain, J. Michael Lord, et al plant hemitoxins - studies on ribosome-inactivating proteins from Saponaria officinalis, Marco R. Soria, et al, cloning and expression of trichosanthin and - momorcharin cDNA, Pang-Chui shaw, et al, cloning and expression of a Luffa ribosome-inactivating-related protein, Bi-Yu Li and S. Ramakrishnan fungal ribotoxins - the Aspergillus ribonucleolytic toxins (ribotoxins), Bernard Lamy, et al, an efficient expression system for -sarcin in Escherichia coli, Yaeta Endo, et al diphtheria toxin - diphtheria toxin cloning and expression in corynebacterium diphtheriae, Lawrence Greenfield, diphtheria toxin expression in Escherichia coli, Lawrence Greenfield, the structure of diphtheria toxin as a guide to rational design, Peter J. Nicholls and Richard J. Youle, protein engineering of diphtheria toxin - development of receptor-specific cytotoxic agents for the treatment of human disease, John R. Murphy , et all, in vivo studies with chimeric toxins - interleukin-2 fusion toxins as immunosuppressive agents, Michael E. Shapiro, et al, initial clinical experiences with an interleukin-2 fusion toxin (DAB 486-IL-2), Carole M. Meneghetti and C.F. Le Maistre pseudomonas exotoxins - pseudomonas aeruginosa exotoxin A, G. Jiliani Chaudry, et al, expression of growth factor - toxin fusion proteins, Gwynneth M. Edwards, et al, the structure of pseudomonas exotoxin A as a guide to rational design, Peter J. Nichols and Richard J. Youle, generation of chimeric toxins, David FitzGerald, et al conclusions - genetically engineered toxins in perspective, Sjur Olsnes and Arthur E. Frankel, Appendix - primary amino acid sequences of toxins, Paul Sehnke and Alexander Tonevistsky.

Published
2020

41. Metagenomic Shotgun Sequencing and Unbiased Metabolomic Profiling Identify Specific Human Gut Microbiota and Metabolites Associated with Immune Checkpoint Therapy Efficacy in Melanoma Patients

Author

Yang Xie, Laura A. Coughlin, Arthur E. Frankel, Andrew Y. Koh, Eugene P. Frenkel, Jiwoong Kim, and Thomas W. Froehlich

Subjects
0301 basic medicine, Cancer Research, biology, Melanoma, Faecalibacterium prausnitzii, Ipilimumab, Pembrolizumab, Gut flora, biology.organism_classification, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282, Immune checkpoint, 3. Good health, 03 medical and health sciences, 030104 developmental biology, Immunology, parasitic diseases, medicine, Microbiome, Nivolumab, medicine.drug
Abstract

This is the first prospective study of the effects of human gut microbiota and metabolites on immune checkpoint inhibitor (ICT) response in metastatic melanoma patients. Whereas many melanoma patients exhibit profound response to ICT, there are fewer options for patients failing ICT—particularly with BRAF-wild-type disease. In preclinical studies, specific gut microbiota promotes regression of melanoma in mice. We therefore conducted a study of the effects of pretreatment gut microbiota and metabolites on ICT Response Evaluation Criteria in Solid Tumors response in 39 metastatic melanoma patients treated with ipilimumab, nivolumab, ipilimumab plus nivolumab (IN), or pembrolizumab (P). IN yielded 67% responses and 8% stable disease; P achieved 23% responses and 23% stable disease. ICT responders for all types of therapies were enriched for Bacteroides caccae . Among IN responders, the gut microbiome was enriched for Faecalibacterium prausnitzii, Bacteroides thetaiotamicron , and Holdemania filiformis . Among P responders, the microbiome was enriched for Dorea formicogenerans . Unbiased shotgun metabolomics revealed high levels of anacardic acid in ICT responders. Based on these pilot studies, both additional confirmatory clinical studies and preclinical testing of these bacterial species and metabolites are warranted to confirm their ICT enhancing activity.

Published
2017

42. A STING-activating nanovaccine for cancer immunotherapy

Author

Jayanthi S. Lea, Hua Wang, Haocheng Cai, Xiang Chen, Arthur E. Frankel, Min Luo, Jinming Gao, Gang Huang, Zhijian J. Chen, Yang Xin Fu, Chensu Wang, Yang Li, Matthew R. Porembka, Mingjian Du, Zhaohui Wang, and Zhigang Lu

Subjects
0301 basic medicine, THP-1 Cells, medicine.medical_treatment, Biomedical Engineering, Bioengineering, 02 engineering and technology, CD8-Positive T-Lymphocytes, Cancer Vaccines, Article, Mice, 03 medical and health sciences, chemistry.chemical_compound, Cancer immunotherapy, Antigen, Neoplasms, medicine, Animals, Humans, Cytotoxic T cell, General Materials Science, Electrical and Electronic Engineering, Adaptor Proteins, Signal Transducing, Mice, Knockout, Phagocytes, Immunity, Cellular, biology, business.industry, Melanoma, Membrane Proteins, Neoplasms, Experimental, Immunotherapy, 021001 nanoscience & nanotechnology, Condensed Matter Physics, medicine.disease, Atomic and Molecular Physics, and Optics, Neoplasm Proteins, 3. Good health, 030104 developmental biology, chemistry, Stimulator of interferon genes, Cancer research, biology.protein, Nanoparticles, Growth inhibition, Antibody, 0210 nano-technology, business
Abstract

The generation of tumour-specific T cells is critically important for cancer immunotherapy. A major challenge in achieving a robust T-cell response is the spatiotemporal orchestration of antigen cross-presentation in antigen-presenting cells with innate stimulation. Here, we report a minimalist nanovaccine, comprising a simple physical mixture of an antigen and a synthetic polymeric nanoparticle, PC7A NP, which generates a strong cytotoxic T-cell response with low systemic cytokine expression. Mechanistically, the PC7A NP achieves efficient cytosolic delivery of tumour antigens to antigen-presenting cells in draining lymph nodes, leading to increased surface presentation while simultaneously activating type I interferon-stimulated genes. This effect is dependent on stimulator of interferon genes (STING), but not the Toll-like receptor or the mitochondrial antiviral-signalling protein (MAVS) pathway. The nanovaccine led to potent tumour growth inhibition in melanoma, colon cancer and human papilloma virus-E6/E7 tumour models. The combination of the PC7A nanovaccine and an anti-PD-1 antibody showed great synergy, with 100% survival over 60 days in a TC-1 tumour model. Rechallenging of these tumour-free animals with TC-1 cells led to complete inhibition of tumour growth, suggesting the generation of long-term antitumour memory. The STING-activating nanovaccine offers a simple, safe and robust strategy in boosting anti-tumour immunity for cancer immunotherapy.

Published
2017

43. Digoxin Plus Trametinib Therapy Achieves Disease Control in BRAF Wild-Type Metastatic Melanoma Patients

Author

Chul Ahn, Vijayashree Ramesh, Arthur E. Frankel, Jennifer G. Gill, Stacy Yuan, Sean J. Morrison, Thomas W. Froehlich, and Ugur Eskiocak

Subjects
Adult, Male, Proto-Oncogene Proteins B-raf, 0301 basic medicine, Oncology, Neuroblastoma RAS viral oncogene homolog, Digoxin, Original article, Cancer Research, medicine.medical_specialty, Combination therapy, Pyridones, medicine.medical_treatment, Pyrimidinones, lcsh:RC254-282, Mice, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Animals, Humans, Neoplasm Metastasis, Adverse effect, Melanoma, neoplasms, Aged, Neoplasm Staging, Aged, 80 and over, Trametinib, business.industry, MEK inhibitor, Immunotherapy, Middle Aged, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Xenograft Model Antitumor Assays, Rash, Disease Models, Animal, Treatment Outcome, 030104 developmental biology, 030220 oncology & carcinogenesis, Retreatment, Immunology, Female, medicine.symptom, business, medicine.drug
Abstract

This is the first prospective study of a combination therapy involving a cardenolide and a MEK inhibitor for metastatic melanoma. Whereas BRAF mutant melanomas can exhibit profound responses to treatment with BRAF and MEK inhibitors, there are fewer options for BRAF wild-type melanomas. In preclinical studies, we discovered that cardenolides synergize with MEK inhibitor to promote the regression of patient-derived xenografts irrespective of BRAF mutation status. We therefore conducted a phase 1B study of digoxin 0.25 mg and trametinib 2 mg given orally once daily in 20 patients with advanced, refractory, BRAF wild-type melanomas. The most common adverse events were rash, diarrhea, nausea, and fatigue. The response rate was 4/20 or 20% with response durations of 2, 4, 6, and 8 months. The disease control rate (including partial responses and stable disease) was 13/20 or 65% of patients, including 5/6 or 83% of patients with NRAS mutant melanomas and 8/14 or 57% of NRAS wild-type melanomas. Patients with stable disease had disease control for 2, 2, 2, 4, 5, 6, 7, 10, and 10 months. Xenografts from four patients recapitulated the treatment responses observed in patients. Based on these pilot results, an expansion arm of digoxin plus MEK inhibitor is warranted for NRAS mutant metastatic melanoma patients who are refractory or intolerant of immunotherapy. Key points Digoxin plus trametinib is well tolerated and achieves a high rate of disease control in BRAF wild-type metastatic melanoma patients.

Published
2017

44. Academic Cancer Center Phase I Program Development

Author

Michael J. Pishvaian, Robert T. Chen, Chul Ahn, Matthew J. Riese, David Smith, A. Craig Lockhart, John Sarantopoulos, Jordan Berlin, Ulka N. Vaishampayan, Nilofer S. Azad, Daruka Mahadevan, Mansoor N. Saleh, John A. Thompson, Matthew H. Taylor, Keith T. Flaherty, Arthur E. Frankel, George J. Weiner, and Eugene P. Frenkel

Subjects
Cancer Research, media_common.quotation_subject, MEDLINE, Phase (combat), 03 medical and health sciences, 0302 clinical medicine, Neoplasms, medicine, Humans, Center (algebra and category theory), 030212 general & internal medicine, Program Development, media_common, Academic Medical Centers, Clinical Trials as Topic, Medical education, ComputingMilieux_THECOMPUTINGPROFESSION, business.industry, Rubric, Cancer, medicine.disease, United States, Clinical trial, Oncology, Work (electrical), 030220 oncology & carcinogenesis, Commentary, Bureaucracy, business
Abstract

This commentary assesses the factors necessary for the effectiveness of academic phase I cancer programs. The metrics presented here may be useful as a rubric for new and established programs., Multiple factors critical to the effectiveness of academic phase I cancer programs were assessed among 16 academic centers in the U.S. Successful cancer centers were defined as having broad phase I and I/II clinical trial portfolios, multiple investigator‐initiated studies, and correlative science. The most significant elements were institutional philanthropic support, experienced clinical research managers, robust institutional basic research, institutional administrative efforts to reduce bureaucratic regulatory delays, phase I navigators to inform patients and physicians of new studies, and a large cancer center patient base. New programs may benefit from a separate stand‐alone operation, but mature phase I programs work well when many of the activities are transferred to disease‐oriented teams. The metrics may be useful as a rubric for new and established academic phase I programs.

Published
2017

45. Abstract P6-11-09: Heavily pre-treated breast cancer patients show promising responses in the first in human study of the first-In-class fatty acid synthase (FASN) inhibitor, TVB-2640 in combination with paclitaxel

Author

Peter Schmid, Kathleen N. Moore, Andrew Brenner, Arthur E. Frankel, Gerald Steven Falchook, H. A. Burris, Katharine Grimmer, Juanita Lopez, George Kemble, EM Dean, J. R. Infante, William McCulloch, Erkut Borazanci, Steven J.M. Jones, Manish R. Patel, and H.-T. Arkenau

Subjects
0301 basic medicine, FASN Inhibitor TVB-2640, Cancer Research, medicine.medical_specialty, Pharmacology, Gastroenterology, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Breast cancer, Internal medicine, medicine, Pneumonitis, Taxane, business.industry, Cancer, medicine.disease, 030104 developmental biology, Oncology, Docetaxel, Paclitaxel, chemistry, 030220 oncology & carcinogenesis, Toxicity, business, medicine.drug
Abstract

Introduction FASN inhibition is a novel approach to cancer treatment involving selective disruption of palmitate biosynthesis that, in tumor cells, leads to apoptosis. TVB-2640 is an oral, first-in-class, small molecule reversible inhibitor of FASN that demonstrates in vivo antitumor effects. We previously reported the results of dose escalation and now present evidence of preliminary activity in breast cancer patients treated in the dose expansion cohort. Methods This ongoing international, multicenter Phase I trial enrolls patients (pts) with advanced solid tumors with adequate organ function. TVB-2640 is given orally once daily at the MTD (100 mg/m2) as monotherapy (mono) or in combination (combo) with weekly IV paclitaxel (80 mg/m2). Results The most common AE's observed [mono, N=53; combo, N=47] were: alopecia (57%), palmar-plantar erythrodysesthesia (PPE) (36%), dry eye (13%) and increased lacrimation (11%). Gr. 3 toxicities include corneal edema (3%) and PPE (10%). Other toxicities were ≤ Gr. 2 and only minor GI symptoms occurred. All toxicities were reversible on dose interruption and no enhancement of common paclitaxel toxicity was observed when given with TVB-2640. Rare cases of pneumonitis in combination have been observed but the contribution of TVB-2640 to this effect is uncertain. 14 breast cancer patients were enrolled and treated in combination with weekly paclitaxel while 3 breast patients were given monotherapy (during the dose escalation phase). Among patients treated in combination, three (3) confirmed RECIST partial responses (cPR) were seen and multiple cases of prolonged stable disease (SD) (≥16 wks) despite heavy pre-treatment and taxane resistance in all but 2 cases. One ER+, PR+, Her2+ patient achieved a cPR and was on study for 26 weeks. One ER-/PR-/Her2+ patient whose previous best response to paclitaxel treatment was SD for 24 weeks, reached a cPR at week 12, discontinued paclitaxel at week 21 and remains on monotherapy TVB-2640 with a sustained cPR at week 29. The third responder with cPR is an ER+, PR+, HER2- patient whose previous taxane treatment lasted 15 weeks (response unknown) and she remains on study at week 24. Of the remaining 11 patients, 10 achieved SD > 12 weeks and 8 of the 10 maintained that response for 16-45 weeks. The ongoing SD patient at week 45, discontinued paclitaxel at week 35 and remains on monotherapy TVB-2640. Summary TVB-2640 demonstrated multiple cPRs and prolonged SD when combined with weekly paclitaxel in 93% of patients treated. Further exploration of response in patients recently progressed on a taxane (progression within the prior 6 months) and safety with TVB-2640 in combination with docetaxel is being explored. Citation Format: Brenner AJ, Falchook G, Patel M, Infante JR, Arkenau H-T, Dean EM, Borazanci E, Lopez JS, Moore K, Schmid P, Frankel AE, Jones S, McCulloch W, Kemble G, Grimmer K, Burris H. Heavily pre-treated breast cancer patients show promising responses in the first in human study of the first-In-class fatty acid synthase (FASN) inhibitor, TVB-2640 in combination with paclitaxel [abstract]. In: Proceedings of the 2016 San Antonio Breast Cancer Symposium; 2016 Dec 6-10; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2017;77(4 Suppl):Abstract nr P6-11-09.

Published
2017

46. Exosomal markers (CD63 and CD9) expression and their prognostic significance using immunohistochemistry in patients with pancreatic ductal adenocarcinoma

Author

Meir Mizrahi, Arun Bhardwaj, Mary Wyatt, Moh’d Khushman, Mary C. Patton, Arthur E. Frankel, Kelley Sherling, Kelly Roveda, William R. Taylor, Bin Wang, Sachin Pai, Brittany Case, Girijesh Kumar Patel, Ajay P. Singh, Robert Donnell, Steven McClellan, Seema Singh, Marcus C.B. Tan, Cindy Nelson, and Javier A. Laurini

Subjects
0301 basic medicine, Oncology, medicine.medical_specialty, CD63, business.industry, Gastroenterology, Cancer, medicine.disease, Primary tumor, Metastasis, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Pancreatic tumor, 030220 oncology & carcinogenesis, Internal medicine, embryonic structures, medicine, Immunohistochemistry, Original Article, Progression-free survival, Pancreas, business
Abstract

Background: Exosomes are important mediators of intercellular communications and play pivotal roles in cancer progression, metastasis and chemoresistance. CD63 and CD9 are widely accepted exosomal markers. In patients with pancreatic ductal adenocarcinoma (PDAC), positive correlation between CD9 expression and overall survival (OS) was reported. CD63 expression was conserved in all patients with no reported prognostic significance. This study explored the prognostic significance of CD63 and CD9 expression using immunohistochemistry (IHC) in patients with PDAC of mixed racial background. Methods: Between 2012 and 2016, 49 patients with PDAC had available tissues for CD63 and CD9 staining using IHC. Two pathologists independently scored the CD63 and CD9 expression. Staining intensity was graded from 1–3 and staining percentage was estimated in 10% increments. Mean Quick-score (Q-score) (Intensity X Percentage of staining) was calculated. Results: The mean Q-score for CD63 and CD9 are higher in primary tumor from the pancreas compared to pancreatic tumor from metastatic sites (185 vs . 102, P=0.0002) and (48 vs . 20, P=0.0418) respectively. We fitted Cox proportion hazard regression models to investigate the impact of the covariates CD63 and CD9 on progression free survival (PFS) and OS. CD63 has significant impact on PFS (P=0.0135) and OS (P=0.003). The higher the CD63 Q-score, the longer the PFS and OS. CD9 doesn’t have significant impact on PFS (P=0.5734) or OS (P=0.2682). The mean CD63 and CD9 Q-scores are slightly higher in African American (AA) compared to Caucasians (157 vs . 149, P=0.76) and (45 vs . 29, P=0.43) respectively. Conclusions: CD63 and CD9 expression is higher in primary tumor from the pancreas compared to pancreatic tumor from metastatic sites. There is correlation between CD63 expression (but not CD9 in this cohort) and PFS and OS. To our knowledge, this is the first study to show prognostic significance of CD63 expression in patients with PDAC using IHC. A trend of higher expression of CD63 and CD9 among AA compared to Caucasians was also noticed.

Published
2019

47. Autoimmune Bell's Palsy Following Immunotherapy For Metastatic Melanoma: A Report of 2 Cases

Author

Arthur E. Frankel and Daniel Zieman

Subjects
0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, medicine.medical_treatment, Immunology, Ipilimumab, Autoimmune Diseases, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Antineoplastic Agents, Immunological, Internal medicine, Bell's palsy, Antineoplastic Combined Chemotherapy Protocols, Bell Palsy, Immunology and Allergy, Medicine, Humans, Melanoma, Aged, Pharmacology, business.industry, Binimetinib, Immunotherapy, Middle Aged, medicine.disease, Immune checkpoint, Discontinuation, 030104 developmental biology, Nivolumab, chemistry, 030220 oncology & carcinogenesis, Female, business, medicine.drug
Abstract

By targeting receptors that serve to downregulate the cellular immune system, monoclonal antibodies such as ipilimumab and nivolumab have transformed the management of metastatic melanoma, and their use is referred to as immune checkpoint therapy (ICT). However, because the antitumoral activity of these agents is achieved through the reversal of mechanisms that naturally serve to temper the immune response, the potential for adverse reactions secondary to autoimmunity is of clinical significance. Neurological immune-related adverse events (irAEs) may occur consequent to ICT, and the development of autoimmune Bell's palsy is a specific, uncommon manifestation of the body's immune response against the seventh cranial nerve, resulting in acute paresis of facial muscles. We describe 2 cases of autoimmune Bell's palsy following the administration of combination ICT using ipilimumab and nivolumab in 2 patients with metastatic melanoma. The use of a steroid taper in addition to the cessation of combination immunotherapy resulted in resolution of symptoms for both patients. In the first case, the patient was subsequently started on nivolumab monotherapy but developed autoimmune polyneuropathy, and immunotherapy was discontinued indefinitely. In the second case, the initiation of nivolumab monotherapy following resolution of symptoms resulted in an inadequate antitumoral response. Subsequent transition to treatment with encorafenib/binimetinib initially provided a positive response but also required discontinuation secondary to irAEs. Both of these cases demonstrate the potential for autoimmune Bell's palsy as a consequence of combination ICT and provide evidence of successful treatment of this irAE through temporary discontinuation of immunotherapy and administration of steroids.

Published
2019

48. Cancer Immune Checkpoint Inhibitor Therapy and the Gut Microbiota

Author

Amit Reddy, Arthur E. Frankel, Bruce L. Roberts, Maureen Hayes, Andrew Y. Koh, John Lightcap, Sachin Kumar Deshmukh, Brooks D. Rabideau, Steven McClellan, T. Grant Glover, and Seema Singh

Subjects
0301 basic medicine, immune checkpoint inhibitor therapy, Immune checkpoint inhibitors, medicine.medical_treatment, Review Article, Gut flora, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, Immune system, Cancer immunotherapy, Neoplasms, cytotoxic T-lymphocytes, medicine, Animals, Humans, cancer, Cytotoxic T cell, dendritic cells, gut microbiota, biology, Cancer, medicine.disease, biology.organism_classification, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Gastrointestinal Microbiome, 3. Good health, Colonic bacteria, 030104 developmental biology, Complementary and alternative medicine, Oncology, Immune System, 030220 oncology & carcinogenesis, Immunology, biology.protein, Immunotherapy, Antibody
Abstract

The past decade has seen tremendous advances in both our understanding of cancer immunosuppressive microenvironments and colonic bacteria facilitated by immune checkpoint inhibitor antibodies and next generation sequencing, respectively. Because an important role of the host immune system is to communicate with and regulate the gut microbial community, it should not come as a surprise that the behavior of one is coupled to the other. In this review, we will attempt to dissect some of the studies demonstrating cancer immunotherapy modulation by specific gut microbes and discuss possible molecular mechanisms for this effect.

Published
2019

49. The Prevalence of DPYD*9A(c.85TC) Genotype and the Genotype-Phenotype Correlation in Patients with Gastrointestinal Malignancies Treated With Fluoropyrimidines: Updated Analysis

Author

Peter J. Hosein, Girijesh Kumar Patel, Ajay P. Singh, William R. Taylor, Bin Wang, Gwendolyn A. McMillin, Sachin Pai, Arthur E. Frankel, Moh’d Khushman, Anu Singh Maharjan, Cindy Nelson, and Saad Awan

Subjects
Adult, Male, medicine.medical_specialty, Antimetabolites, Antineoplastic, Heterozygote, Dihydropyrimidine Dehydrogenase Deficiency, Drug-Related Side Effects and Adverse Reactions, Genotyping Techniques, Colorectal cancer, Gastroenterology, Polymorphism, Single Nucleotide, Severity of Illness Index, 03 medical and health sciences, symbols.namesake, Young Adult, 0302 clinical medicine, Internal medicine, Genotype, Antineoplastic Combined Chemotherapy Protocols, medicine, Dihydropyrimidine dehydrogenase, Humans, Genotyping, Fisher's exact test, Capecitabine, Dihydrouracil Dehydrogenase (NADP), Genetic Association Studies, Aged, Gastrointestinal Neoplasms, Retrospective Studies, Aged, 80 and over, business.industry, Homozygote, Cancer, Middle Aged, medicine.disease, Oncology, 030220 oncology & carcinogenesis, Cohort, symbols, 030211 gastroenterology & hepatology, DPYD, Female, Fluorouracil, business
Abstract

Introduction The dihydropyrimidine dehydrogenase gene (DPYD)*9A (c.85T>C) genotype is relatively common. The correlation between DPYD*9A genotype and dihydropyrimidine dehydrogenase (DPD) deficiency phenotype is controversial. In a cohort of 28 patients, DPYD*9A was the most commonly diagnosed variant (13 patients [46%]) and there was a noticeable genotype-phenotype correlation. In this study we genotyped a larger cohort of a mixed racial background to explore the prevalence of DPYD*9A variant and to confirm the genotype-phenotype correlation. Patients and Methods Between 2011 and 2018, in addition to genotyping for high-risk DPYD variants (DPYD*2A, DPYD*13 and DPYD*9B), genotyping for DPYD*9A variant was performed on 113 patients with gastrointestinal malignancies treated with fluoropyrimidines. Fluoropyrimidines-associated toxicity was graded according to the National Cancer Institute Common Terminology Criteria for Adverse Events (version 5.0). Fisher exact test was used for statistical analysis. Results Heterozygous and homozygous DPYD*9A genotypes were identified in 46 (41%) and 11 (10%) patients, respectively. Among patients with DPYD*9A genotypes (n = 57), men and women represented 30 (53%) and 27 (47%) patients, respectively. Caucasian, African American, and other ethnicities represented 29 (50.9%), 26 (45.6%), and 2 (3.5%) patients, respectively. Grade 3/4 toxicities were experienced in 26 patients with DPYD*9A genotype (3 patients had homozygous status) and in 20 patients with wild type DPYD*9A (P = .4405). In patients who received full-dose fluoropyrimidines (n = 85), Grade 3/4 toxicities were experienced in 22 patients with DPYD*9A genotype (2 patients had homozygous status), and in 17 patients with wild type DPYD (P = .8275). Conclusion In our updated analysis, the prevalence of heterozygous and homozygous DPYD*9A genotypes were 41% and 10%, respectively. The correlation between DPYD*9A genotype and DPD clinical phenotype was not reproduced. The noticeable correlation that we previously reported is likely because of small sample size and selection bias.

Published
2019

50. Enasidenib in mutant IDH2 relapsed or refractory acute myeloid leukemia

Author

Daniel A. Pollyea, Gail J. Roboz, Anthony S. Stein, Robert H. Collins, Daniel J. DeAngelo, Manish R. Patel, Mikkael A. Sekeres, Eytan M. Stein, Sam Agresta, Courtney D. DiNardo, Ronan T. Swords, Richard Stone, Arthur E. Frankel, Ross L. Levine, Qiang Xu, Amir T. Fathi, Martin S. Tallman, Ian W. Flinn, Hagop M. Kantarjian, Alessandra Tosolini, Bruno C. Medeiros, Stéphane de Botton, Christophe Willekens, Katharine E. Yen, Jessica K. Altman, Paresh Vyas, and Robert Knight

Subjects
0301 basic medicine, Oncology, medicine.medical_specialty, Myeloid, Immunology, Pharmacology, Enasidenib, Biochemistry, IDH2, 03 medical and health sciences, 0302 clinical medicine, Refractory, Internal medicine, Medicine, Adverse effect, business.industry, Myeloid leukemia, Cell Biology, Hematology, medicine.disease, Leukemia, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Pharmacodynamics, business
Abstract

Recurrent mutations in isocitrate dehydrogenase 2 (IDH2) occur in ∼12% of patients with acute myeloid leukemia (AML). Mutated IDH2 proteins neomorphically synthesize 2-hydroxyglutarate resulting in DNA and histone hypermethylation, which leads to blocked cellular differentiation. Enasidenib (AG-221/CC-90007) is a first-in-class, oral, selective inhibitor of mutant-IDH2 enzymes. This first-in-human phase 1/2 study assessed the maximum tolerated dose (MTD), pharmacokinetic and pharmacodynamic profiles, safety, and clinical activity of enasidenib in patients with mutant-IDH2 advanced myeloid malignancies. We assessed safety outcomes for all patients and clinical efficacy in the largest patient subgroup, those with relapsed or refractory AML, from the phase 1 dose-escalation and expansion phases of the study. In the dose-escalation phase, an MTD was not reached at doses ranging from 50 to 650 mg per day. Enasidenib 100 mg once daily was selected for the expansion phase on the basis of pharmacokinetic and pharmacodynamic profiles and demonstrated efficacy. Grade 3 to 4 enasidenib-related adverse events included indirect hyperbilirubinemia (12%) and IDH-inhibitor–associated differentiation syndrome (7%). Among patients with relapsed or refractory AML, overall response rate was 40.3%, with a median response duration of 5.8 months. Responses were associated with cellular differentiation and maturation, typically without evidence of aplasia. Median overall survival among relapsed/refractory patients was 9.3 months, and for the 34 patients (19.3%) who attained complete remission, overall survival was 19.7 months. Continuous daily enasidenib treatment was generally well tolerated and induced hematologic responses in patients for whom prior AML therapy had failed. Inducing differentiation of myeloblasts, not cytotoxicity, seems to drive the clinical efficacy of enasidenib. This trial was registered at www.clinicaltrials.gov as #NCT01915498.

Published
2019

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