Your search keyword '"Keith Dredge"' showing total 81 results

1. Phase Ib open-label, multicenter study of pixatimod, an activator of TLR9, in combination with nivolumab in subjects with microsatellite-stable metastatic colorectal cancer, metastatic pancreatic ductal adenocarcinoma and other solid tumors

Author

Matthew Burge, David Goldstein, Andrew Haydon, Nick Pavlakis, Charlotte Lemech, Edward Hammond, Darryn Bampton, Keith Dredge, Michael P Brown, Andrew Clouston, Nigel J Waterhouse, Amanda C Stanley, Lucie Leveque-El Mouttie, and Grace M Chojnowski

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Background Pixatimod is a unique activator of the Toll-like Receptor 9 pathway. This phase I trial evaluated safety, efficacy and pharmacodynamics of pixatimod and PD-1 inhibitor nivolumab in immunologically cold cancers.Methods 3+3 dose escalation with microsatellite stable metastatic colorectal cancer (MSS mCRC) and metastatic pancreatic ductal adenocarcinoma (mPDAC) expansion cohorts. Participants received pixatimod once weekly as a 1-hour intravenous infusion plus nivolumab every 2 weeks. Objectives included assessment of safety, antitumor activity, pharmacodynamics, and pharmacokinetic profile.Results Fifty-eight participants started treatment. The maximum tolerated dose of pixatimod was 25 mg in combination with 240 mg nivolumab, which was used in the expansion phases of the study. Twenty-one grade 3–5 treatment-related adverse events were reported in 12 participants (21%); one participant receiving 50 mg pixatimod/nivolumab had a treatment-related grade 5 AE. The grade 3/4 rate in the MSS mCRC cohort (n=33) was 12%. There were no responders in the mPDAC cohort (n=18). In the MSS mCRC cohort, 25 participants were evaluable (initial postbaseline assessment scans >6 weeks); of these, three participants had confirmed partial responses (PR) and eight had stable disease (SD) for at least 9 weeks. Clinical benefit (PR+SD) was associated with lower Pan-Immune-Inflammation Value and plasma IL-6 but increased IP-10 and IP-10/IL-8 ratio. In an MSS mCRC participant with PR as best response, increased infiltration of T cells, dendritic cells, and to a lesser extent NK cells, were evident 5 weeks post-treatment.Conclusions Pixatimod is well tolerated at 25 mg in combination with nivolumab. The efficacy signal and pharmacodynamic changes in MSS mCRC warrants further investigation.Trial registration number NCT05061017.

Published

2023

2. 341 A phase Ib expansion cohort of pixatimod plus nivolumab in previously treated, microsatellite stable metastatic colorectal cancer (MSS mCRC)

Author

Matthew Burge, David Goldstein, Andrew Haydon, Nick Pavlakis, Michael Brown, Charlotte Lemech, Edward Hammond, Darryn Bampton, Keith Dredge, Nigel Waterhouse, Amanda Stanley, Lucie Leveque-ElMouttie, Grace Chojnowski, and Andrew Clouson

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Published

2021

3. 340 A phase Ib study of the safety and tolerability of pixatimod plus nivolumab in subjects with advanced solid tumors with an expansion cohort in metastatic pancreatic adenocarcinoma (mPDAC)

Author

Matthew Burge, David Goldstein, Andrew Haydon, Nick Pavlakis, Michael Brown, Charlotte Lemech, Edward Hammond, Darryn Bampton, Keith Dredge, Amanda Stanley, Lucie Leveque-ElMouttie, and Grace Chojnowski

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Published

2021

4. Immunomodulatory activities of pixatimod: emerging nonclinical and clinical data, and its potential utility in combination with PD-1 inhibitors

Author

Edward Hammond, Nicole M. Haynes, Carleen Cullinane, Todd V. Brennan, Darryn Bampton, Paul Handley, Tomislav Karoli, Fleur Lanksheer, Liwen Lin, Yiping Yang, and Keith Dredge

Subjects

Pixatimod, PG545, Immunomodulatory, Tumor-associated macrophage, Dendritic cell, NK cell, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Pixatimod (PG545) is a novel clinical-stage immunomodulatory agent capable of inhibiting the infiltration of tumor-associated macrophages (TAMs) yet also stimulate dendritic cells (DCs), leading to activation of natural killer (NK) cells. Preclinically, pixatimod inhibits heparanase (HPSE) which may be associated with its inhibitory effect on TAMs whereas its immunostimulatory activity on DCs is through the MyD88-dependent TLR9 pathway. Pixatimod recently completed a Phase Ia monotherapy trial in advanced cancer patients. Methods To characterize the safety of pixatimod administered by intravenous (IV) infusion, a one month toxicology study was conducted to support a Phase Ia monotherapy clinical trial. The relative exposure (AUC) of pixatimod across relevant species was determined and the influence of route of administration on the immunomodulatory activity was also evaluated. Finally, the potential utility of pixatimod in combination with PD-1 inhibition was also investigated using the syngeneic 4T1.2 breast cancer model. Results The nonclinical safety profile revealed that the main toxicities associated with pixatimod are elevated cholesterol, triglycerides, APTT, decreased platelets and other changes symptomatic of modulating the immune system such as pyrexia, changes in WBC subsets, inflammatory changes in liver, spleen and kidney. Though adverse events such as fever, elevated cholesterol and triglycerides were reported in the Phase Ia trial, none were considered dose limiting toxicities and the compound was well tolerated up to 100 mg via IV infusion. Exposure (AUC) up to 100 mg was considered proportional with some accumulation upon repeated dosing, a phenomenon also noted in the toxicology study. The immunomodulatory activity of pixatimod was independent of the route of administration and it enhanced the effectiveness of PD-1 inhibition in a poorly immunogenic tumor model. Conclusions Pixatimod modulates innate immune cells but also enhances T cell infiltration in combination with anti-PD-1 therapy. The safety and PK profile of the compound supports its ongoing development in a Phase Ib study for advanced cancer/pancreatic adenocarcinoma with the checkpoint inhibitor nivolumab (Opdivo®). Trial registration ClinicalTrials.gov Identifier: NCT02042781. First posted: 23 January, 2014 - Retrospectively registered.

Published

2018

5. PG545, a heparan sulfate mimetic, reduces heparanase expression in vivo, blocks spontaneous metastases and enhances overall survival in the 4T1 breast carcinoma model.

Author

Edward Hammond, Ralf Brandt, and Keith Dredge

Subjects

Medicine, Science

Abstract

PG545 is a clinically relevant heparan sulfate (HS) mimetic which, in addition to possessing anti-angiogenic properties, also acts as a heparanase inhibitor which may differentiate its mechanism(s) of action from approved angiogenesis inhibitors. The degradation of HS by heparanase has been strongly implicated in cell dissemination and the metastatic process. Thus, the anti-metastatic activity of PG545 has been linked to the enzymatic function of heparanase - the only endoglycosidase known to cleave HS, an important component of the extracellular matrix (ECM) which represents a potential avenue for therapeutic intervention for certain metastatic cancer indications. Recent concerns raised about the paucity of overall survival as an endpoint in mouse models of clinically relevant metastasis led us to examine the effect of PG545 on the progression of both primary tumor growth and the spontaneously metastasizing disease in the 4T1 syngeneic breast carcinoma model in a non-surgical and surgical (mastectomy) setting. PG545 significantly inhibited primary tumor growth but importantly also inhibited lung metastasis in treated mice, an effect not observed with the tyrosine kinase inhibitor sorafenib. Importantly, PG545 significantly enhanced overall survival compared to vehicle control and the sorafenib group, suggesting PG545's inhibitory effect on heparanase is indeed a critical attribute to induce anti-metastatic activity. In addition to blocking a common angiogenic signalling pathway in tumor cells, the expression of heparanase in the primary tumor and lung was also significantly reduced by PG545 treatment. These results support the ongoing development of PG545 and highlight the potential utility in metastatic disease settings.

Published

2012

6. Supplementary Figure S1 from Inhibition of Heparanase in Pediatric Brain Tumor Cells Attenuates their Proliferation, Invasive Capacity, and In Vivo Tumor Growth

Author

Karin Forsberg-Nilsson, Israel Vlodavsky, Uri Barash, Edward Hammond, Keith Dredge, Tommie Olofsson, Di Yu, Lulu Haseeb, Soumi Kundu, and Argyris Spyrou

Abstract

Combinatorial effect of PG545 and conditioned medium (CM) on cell viability, and examination of apoptosis after downregulation of HPSE

Published

2023

7. Data from PG545, an Angiogenesis and Heparanase Inhibitor, Reduces Primary Tumor Growth and Metastasis in Experimental Pancreatic Cancer

Author

Rolf A. Brekken, Roderich E. Schwarz, Keith Dredge, Stefan Hinz, Bercin Kutluk Cenik, Niranjan Awasthi, and Katherine T. Ostapoff

Abstract

Aggressive tumor progression, metastasis, and resistance to conventional therapies lead to an extremely poor prognosis for pancreatic ductal adenocarcinoma (PDAC). Heparanase, an enzyme expressed by multiple cell types, including tumor cells in the tumor microenvironment, has been implicated in angiogenesis and metastasis, and its expression correlates with decreased overall survival in PDAC. We evaluated the therapeutic potential of PG545, an angiogenesis and heparanase inhibitor, in experimental PDAC. PG545 inhibited the proliferation, migration, and colony formation of pancreatic cancer cells in vitro at pharmacologically relevant concentrations. Heparanase inhibition also reduced the proliferation of fibroblasts but had only modest effects on endothelial cells in vitro. Furthermore, PG545 significantly prolonged animal survival in intraperitoneal and genetic models (mPDAC: LSL-KrasG12D; Cdkn2alox/lox; p48Cre) of PDAC. PG545 also inhibited primary tumor growth and metastasis in orthotopic and genetic endpoint studies. Analysis of tumor tissue revealed that PG545 significantly decreased cell proliferation, increased apoptosis, reduced microvessel density, disrupted vascular function, and elevated intratumoral hypoxia. Elevated hypoxia is a known driver of collagen deposition and tumor progression; however, tumors from PG545-treated animals displayed reduced collagen deposition and a greater degree of differentiation compared with control or gemcitabine-treated tumors. These results highlight the potent antitumor activity of PG545 and support the further exploration of heparanase inhibitors as a potential clinical strategy for the treatment of PDAC. Mol Cancer Ther; 12(7); 1190–201. ©2013 AACR.

Published

2023

8. Supplementary Figure Legends from Inhibition of Heparanase in Pediatric Brain Tumor Cells Attenuates their Proliferation, Invasive Capacity, and In Vivo Tumor Growth

Author

Karin Forsberg-Nilsson, Israel Vlodavsky, Uri Barash, Edward Hammond, Keith Dredge, Tommie Olofsson, Di Yu, Lulu Haseeb, Soumi Kundu, and Argyris Spyrou

Abstract

Supplementary Figure Legends

Published

2023

9. Supplementary Figure 1 from PG545, an Angiogenesis and Heparanase Inhibitor, Reduces Primary Tumor Growth and Metastasis in Experimental Pancreatic Cancer

Author

Rolf A. Brekken, Roderich E. Schwarz, Keith Dredge, Stefan Hinz, Bercin Kutluk Cenik, Niranjan Awasthi, and Katherine T. Ostapoff

Abstract

PDF - 153K, Example histology of liver metastases in the mPDAC model. Liver sections were stained with H&E. Scale bar, 100 um.

Published

2023

10. Data from Inhibition of Heparanase in Pediatric Brain Tumor Cells Attenuates their Proliferation, Invasive Capacity, and In Vivo Tumor Growth

Author

Karin Forsberg-Nilsson, Israel Vlodavsky, Uri Barash, Edward Hammond, Keith Dredge, Tommie Olofsson, Di Yu, Lulu Haseeb, Soumi Kundu, and Argyris Spyrou

Abstract

Curative therapy for medulloblastoma and other pediatric embryonal brain tumors has improved, but the outcome still remains poor and current treatment causes long-term complications. Malignant brain tumors infiltrate the healthy brain tissue and, thus despite resection, cells that have already migrated cause rapid tumor regrowth. Heparan sulfate proteoglycans (HSPG), major components of the extracellular matrix (ECM), modulate the activities of a variety of proteins. The major enzyme that degrades HS, heparanase (HPSE), is an important regulator of the ECM. Here, we report that the levels of HPSE in pediatric brain tumors are higher than in healthy brain tissue and that treatment of pediatric brain tumor cells with HPSE stimulated their growth. In addition, the latent, 65 kDa form of HPSE (that requires intracellular enzymatic processing for activation) enhanced cell viability and rapidly activated the ERK and AKT signaling pathways, before enzymatically active HPSE was detected. The HPSE inhibitor PG545 efficiently killed pediatric brain tumor cells, but not normal human astrocytes, and this compound also reduced tumor cell invasion in vitro and potently reduced the size of flank tumors in vivo. Our findings indicate that HPSE in malignant brain tumors affects both the tumor cells themselves and their ECM. In conclusion, HPSE plays a substantial role in childhood brain tumors, by contributing to tumor aggressiveness and thereby represents a potential therapeutic target. Mol Cancer Ther; 16(8); 1705–16. ©2017 AACR.

Published

2023

11. 721 Pixatimod (P) in combination with nivolumab (N) +/- low-dose cyclophosphamide (Cy) in advanced cancers: a phase IIA basket trial

Author

Diwakar Davar, Hong Wang, Sarah Behr, Aubrey Murano, Sarah Johnson, Amy Rose, Darryn Bampton, Keith Dredge, Hassane Zarour, John Rhee, Liza Villaruz, Yana Najjar, and Jason Luke

Published

2022

12. A netrin domain-containing protein secreted by the human hookworm Necator americanus protects against CD4 T cell transfer colitis

Author

Roland Ruscher, Keith Dredge, Martha M Cooper, Ashley Van Waardenberg, Kim Miles, Alex Loukas, Matthew A. Field, Norelle L. Daly, Geraldine Buitrago, Stephanie Ryan, Darren Pickering, Paul R. Giacomin, Linda Jones, and Claudia Cobos Caceres

Subjects

CD4-Positive T-Lymphocytes, Male, 0301 basic medicine, Necator americanus, medicine.medical_treatment, Anti-Inflammatory Agents, Inflammation, Matrix Metalloproteinase Inhibitors, RS, Hookworm Infections, 03 medical and health sciences, 0302 clinical medicine, Physiology (medical), medicine, Animals, Humans, Secretion, Colitis, Mice, Knockout, Crohn's disease, biology, Biochemistry (medical), Public Health, Environmental and Occupational Health, Helminth Proteins, General Medicine, biology.organism_classification, medicine.disease, Ulcerative colitis, Recombinant Proteins, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Cytokine, 030220 oncology & carcinogenesis, Immunology, Colitis, Ulcerative, Female, Netrins, Tumor necrosis factor alpha, medicine.symptom

Abstract

The symbiotic relationships shared between humans and their gastrointestinal parasites present opportunities to discover novel therapies for inflammatory diseases. A prime example of this phenomenon is the interaction of humans and roundworms such as the hookworm, Necator americanus. Epidemiological observations, animal studies and clinical trials using experimental human hookworm infection show that hookworms can suppress inflammation in a safe and well-tolerated way, and that the key to their immunomodulatory properties lies within their secreted proteome. Herein we describe the identification of 2 netrin domain-containing proteins from the N. americanus secretome, and explore their potential in treating intestinal inflammation in mouse models of ulcerative colitis. One of these proteins, subsequently named Na-AIP-1, was effective at suppressing disease when administered prophylactically in the acute TNBS-induced model of colitis. This protective effect was validated in the more robust CD4 T cell transfer model of chronic colitis, where prophylactic Na-AIP-1 reduced T-cell-dependent type-1 cytokine responses in the intestine and the associated intestinal pathology. Mechanistic studies revealed that depletion of CD11c+ cells abrogated the protective anticolitic effect of Na-AIP-1. Next generation sequencing of colon tissue in the T-cell transfer model of colitis revealed that Na-AIP-1 induced a transcriptomic profile associated with the downregulation of metabolic and signaling pathways involved in type-1 inflammation, notably TNF. Finally, co-culture of Na-AIP-1 with a human monocyte-derived M1 macrophage cell line resulted in significantly reduced secretion of TNF. Na-AIP-1 is now a candidate for clinical development as a novel therapeutic for the treatment of human inflammatory bowel diseases.

Published

2021

13. Abstract 367: The heparan sulfate mimetic PG545 inhibits tumor growth in both male and female mouse model of pancreatic ductal adenocarcinoma (PDAC) with sex difference in the effect on cachexia

Author

Xiaoling Zhong, Keith Dredge, John M. Chirgwin, Michael G. House, Harikrishna Nakshatri, and Teresa A. Zimmers

Subjects

Cancer Research, Oncology

Abstract

BACKGROUND: Cachexia occurs in up to 80% of PDAC patients and is characterized by weight loss mainly due to muscle and fat wasting. Cachexia leads to functional impairment, reduced anticancer therapy tolerance and increased mortality. PG545, a heparan sulfate (HS) mimetic, shows anticancer activity; however, it is unknown whether sex affects the anticancer activity and what effect PG545 has on cancer associated muscle and fat wasting. Given that many cytokines induced in patients with cancer cachexia can bind HS, the aim of this study was to assess PG545 effects on PDAC cachexia with emphasis on sex difference. METHODS: PDAC cells were injected into the pancreas of 10-week C57BL/6 male and female mice. The orthotopic tumor-bearing mice were treated with PG545 (10 mg/kg; i.p.). Body weight and body composition were monitored, and tumor and organs were collected. Skeletal muscles were cryosectioned for evaluation of cross-sectional area (CSA). C2C12 myotubes, the in vitro model of muscle wasting, were treated with PDAC cell-derived conditioned medium (CM) without or with PG545 and analyzed for the changes in size. PDAC cell proliferation was assessed by MTT assay. RESULTS: PG545 treatment markedly reduced tumor mass in both males and females compared to the vehicle controls. PG545 also reduced body weight but the difference gradually dissipated over time despite repeated dosing. However, male mice recovered from the negative effects more slowly than female mice. Similar sex difference was observed in the changes in the PG545-induced lean and fat mass loss. Of note, fat mass in PG545-treated females at the end of experiment was higher than in the vehicle controls. Furthermore, males had more reductions in muscle and fat weights than females in response to PG545. Grip strength in males was weakened by PG545 but returned to the level like that in the vehicle controls at the end, while PG545 did not weaken grip strength in females at the same time points. In addition, males, but not females, had smaller muscle fiber CSA after PG545 treatment versus their vehicle controls. In in vitro assay, PG545 inhibited PDAC cell proliferation, indicating a direct effect on cancer cells. Lastly, opposed to the in vivo effect, PG545 partly prevented myotube wasting induced by PDAC CM. CONCLUSION: PG545 has strong anti-PDAC activity in both male and female mice, at least partly through inhibition of cancer cell proliferation. Its initial negative effects on cachexia are gradually reversed with male tumor-bearing mice reversing more slowly than females. Because of the protective effect on C2C12 myotubes treated with PDAC CM, PG545 might induce some counteracting factors in vivo in the initial treatment and identification of these factors may offer molecular targets for combination therapy to counteract the negative effects while take advantage of the strong anti-cancer potential. Citation Format: Xiaoling Zhong, Keith Dredge, John M. Chirgwin, Michael G. House, Harikrishna Nakshatri, Teresa A. Zimmers. The heparan sulfate mimetic PG545 inhibits tumor growth in both male and female mouse model of pancreatic ductal adenocarcinoma (PDAC) with sex difference in the effect on cachexia [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 1 (Regular and Invited Abstracts); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(7_Suppl):Abstract nr 367.

Published

2023

14. Synthetic Heparan Sulfate Mimetic Pixatimod (PG545) Potently Inhibits SARS-CoV-2 by Disrupting the Spike-ACE2 Interaction

Author

Scott E. Guimond, Courtney J. Mycroft-West, Neha S. Gandhi, Julia A. Tree, Thuy T. Le, C. Mirella Spalluto, Maria V. Humbert, Karen R. Buttigieg, Naomi Coombes, Michael J. Elmore, Matthew Wand, Kristina Nyström, Joanna Said, Yin Xiang Setoh, Alberto A. Amarilla, Naphak Modhiran, Julian D. J. Sng, Mohit Chhabra, Paul R. Young, Daniel J. Rawle, Marcelo A. Lima, Edwin A. Yates, Richard Karlsson, Rebecca L. Miller, Yen-Hsi Chen, Ieva Bagdonaite, Zhang Yang, James Stewart, Dung Nguyen, Stephen Laidlaw, Edward Hammond, Keith Dredge, Tom M. A. Wilkinson, Daniel Watterson, Alexander A. Khromykh, Andreas Suhrbier, Miles W. Carroll, Edward Trybala, Tomas Bergström, Vito Ferro, Mark A. Skidmore, and Jeremy E. Turnbull

Subjects

General Chemical Engineering, QD, General Chemistry, R1

Abstract

Heparan sulfate (HS) is a cell surface polysaccharide recently identified as a coreceptor with the ACE2 protein for the S1 spike protein on SARS-CoV-2 virus, providing a tractable new therapeutic target. Clinically used heparins demonstrate an inhibitory activity but have an anticoagulant activity and are supply-limited, necessitating alternative solutions. Here, we show that synthetic HS mimetic pixatimod (PG545), a cancer drug candidate, binds and destabilizes the SARS-CoV-2 spike protein receptor binding domain and directly inhibits its binding to ACE2, consistent with molecular modeling identification of multiple molecular contacts and overlapping pixatimod and ACE2 binding sites. Assays with multiple clinical isolates of SARS-CoV-2 virus show that pixatimod potently inhibits the infection of monkey Vero E6 cells and physiologically relevant human bronchial epithelial cells at safe therapeutic concentrations. Pixatimod also retained broad potency against variants of concern (VOC) including B.1.1.7 (Alpha), B.1.351 (Beta), B.1.617.2 (Delta), and B.1.1.529 (Omicron). Furthermore, in a K18-hACE2 mouse model, pixatimod significantly reduced SARS-CoV-2 viral titers in the upper respiratory tract and virus-induced weight loss. This demonstration of potent anti-SARS-CoV-2 activity tolerant to emerging mutations establishes proof-of-concept for targeting the HS-Spike protein-ACE2 axis with synthetic HS mimetics and provides a strong rationale for clinical investigation of pixatimod as a potential multimodal therapeutic for COVID-19.

Published

2022

15. Synthetic Heparan Sulfate Mimetic Pixatimod (PG545) Potently Inhibits SARS-CoV-2 By Disrupting The Spike-ACE2 interaction

Author

Julia A. Tree, Jerry Turnbull, Thuy T. Le, Tom Wilkinson, Courtney J. Mycroft-West, Michael J. Elmore, Julian D. J. Sng, Mark A. Skidmore, Tomas Bergström, Spalluto Cm, Yen-Hsi Chen, Alberto A. Amarilla, Mohit Chhabra, Joanna Said, Miles W. Carroll, Ed Yates, Yin Xiang Setoh, Richard Karlsson, Rebecca L. Miller, Scott E. Guimond, Naomi Coombes, Ieva Bagdonaite, Naphak Modhiran, Ferro, Zhang Yang, Marcelo A. Lima, Kristina Nyström, Edward Hammond, Paul R. Young, James P. Stewart, Edward Trybala, Humbert Mv, Karen R. Buttigieg, Keith Dredge, Daniel Watterson, Alexander A. Khromykh, Neha S. Gandhi, and Andreas Suhrbier

Subjects

Chemistry, Cell, Heparan sulfate, Virus, Cell biology, chemistry.chemical_compound, medicine.anatomical_structure, Therapeutic index, Mechanism of action, medicine, Vero cell, medicine.symptom, Binding site, Receptor

Abstract

SummaryHeparan sulfate (HS) is a cell surface polysaccharide recently identified as a co-receptor with the ACE2 protein for recognition of the S1 spike protein on SARS-CoV-2 virus, providing a tractable new target for therapeutic intervention. Clinically-used heparins demonstrate inhibitory activity, but world supplies are limited, necessitating alternative solutions. Synthetic HS mimetic pixatimod is a drug candidate for cancer with immunomodulatory and heparanase-inhibiting properties. Here we show that pixatimod binds to and destabilizes the SARS-CoV-2 spike protein receptor binding domain (S1-RBD), and directly inhibits its binding to human ACE2, consistent with molecular modelling identification of multiple molecular contacts and overlapping pixatimod and ACE2 binding sites. Assays with multiple clinical isolates of live SARS-CoV-2 virus show that pixatimod potently inhibits infection of monkey Vero E6 and human bronchial epithelial cells at concentrations within its safe therapeutic dose range. Furthermore, in a K18-hACE2 mouse model pixatimod demonstrates that pixatimod markedly attenuates SARS-CoV-2 viral titer and COVID-19-like symptoms. This demonstration of potent anti-SARS-CoV-2 activity establishes proof-of-concept for targeting the HS-Spike protein-ACE2 axis with synthetic HS mimetics. Together with other known activities of pixatimod our data provides a strong rationale for its clinical investigation as a potential multimodal therapeutic to address the COVID-19 pandemic.

Published

2020

16. Heparanase Inhibition by Pixatimod (PG545): Basic Aspects and Future Perspectives

Author

Edward, Hammond and Keith, Dredge

Subjects

Neoplasms, Animals, Humans, Antineoplastic Agents, Saponins, Glucuronidase

Abstract

Pixatimod is an inhibitor of heparanase, a protein which promotes cancer via its regulation of the extracellular environment by enzymatic cleavage of heparan sulfate (HS) and non-enzymatic signaling. Through its inhibition of heparanase and other HS-binding signaling proteins, pixatimod blocks a number of pro-cancerous processes including cell proliferation, invasion, metastasis, angiogenesis and epithelial-mesenchymal transition. Several laboratories have found that these activities have translated into potent activity using a range of different mouse cancer models, including approximately 30 xenograft and 20 syngeneic models. Analyses of biological samples from these studies have confirmed the heparanase targeting of this agent in vivo and the broad spectrum of anti-cancer effects that heparanase blockade achieves. Pixatimod has been tested in combination with a number of approved anti-cancer drugs demonstrating its clinical potential, including with gemcitabine, paclitaxel, sorafenib, platinum agents and an anti-PD-1 antibody. Clinical testing has shown pixatimod to be well tolerated as a monotherapy, and it is currently being investigated in combination with the anti-PD-1 drug nivolumab in a pancreatic cancer phase I trial.

Published

2020

17. 340 A phase Ib study of the safety and tolerability of pixatimod plus nivolumab in subjects with advanced solid tumors with an expansion cohort in metastatic pancreatic adenocarcinoma (mPDAC)

Author

Michael C. Brown, Nick Pavlakis, Matthew Burge, Lucie Leveque-ElMouttie, Grace Chojnowski, David Goldstein, Darryn Bampton, Andrew Haydon, Charlotte Lemech, Edward Hammond, Keith Dredge, and Amanda C. Stanley

Subjects

Pharmacology, Oncology, Cancer Research, medicine.medical_specialty, business.industry, Immunology, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Metastatic Pancreatic Adenocarcinoma, Tolerability, Internal medicine, Cohort, medicine, Molecular Medicine, Immunology and Allergy, Nivolumab, business, RC254-282

Abstract

BackgroundPixatimod is a novel immunomodulatory agent which stimulates dendritic cells (DC) via Toll-Like Receptor (TLR9) pathway to activate natural killer (NK) cells.1 In combination with PD1 inhibitors, it also enhances T cell infiltration in vivo.2 We report on safety, pharmacokinetics (PK) and pharmacodynamics (PD), and antitumor activity of pixatimod plus nivolumab in advanced cancer patients (stage 1) and in an expansion cohort of mPDAC (stage 2).MethodsIn the dose escalation stage (3+3 design), eligible patients (ECOG≤1) with advanced solid malignancies who failed standard therapies received pixatimod once weekly as a 1-hour i.v. infusion plus nivolumab (240 mg, every other week) until disease progression or discontinuation due to intolerability. The primary objective was determination of the maximum tolerated dose (MTD). Secondary objectives evaluated safety, antitumor activity per RECIST v1.1, PK of pixatimod, and PD (PBMC, plasma cytokines and chemokines). Stage 2 comprised mPDAC subjects who had received no more than one prior line of chemotherapy in the metastatic setting.ResultsThe dose-escalation stage recruited 16 subjects across two cohorts (25 & 50 mg pixatimod). Two dose limiting toxicities (DLTs) in 50 mg cohort were pulmonary edema and multi-organ failure. Of note, the subject with multi-organ failure had substantially higher CA19.9, Pan-immune-Inflammatory Value (PIV = Neutrophils x Platelets x Monocytes/Lymphocytes) and interleukins (IL) IL-1α and IL-23 at baseline compared with the cohort. One DLT occurred in the 25 mg cohort, pneumonitis, which was identified as the MTD. A further 14 mPDAC subjects were recruited to the expansion stage (25 mg). Seven SAEs were reported to be possibly or likely related to the combination. No objective responses were reported in the mPDAC stage, the best response was SD (n = 3). In another submitted abstract by Lemech et al, we report two subjects in the dose escalation stage with MSS mCRC were confirmed PR, and data from the amended study to include an MSS mCRC expansion cohort will also be presented. Time versus concentration data for pixatimod in advanced cancer patients was similar to that previously reported in monotherapy setting. In mPDAC subjects, there was minimal immune activation as evidenced by a lack of change in effector memory T cells or NK cells in PBMC, plasma cytokines and chemokines.ConclusionsPixatimod is well tolerated at 25 mg in combination with nivolumab but did not provide clear clinical benefit or evidence of immune activation in the mPDAC cohort.AcknowledgementsResearch funding was provided by Zucero Therapeutics Ltd and Bristol Myers Squibb (BMS), Australia.Trial RegistrationClinical trial informationACTRN12617001573347.ReferencesBrennan TV, Lin L, Brandstadter JD, Rendell VR, Dredge K, Huang X, et al. Heparan sulfate mimetic PG545-mediated antilymphoma effects require TLR9-dependent NK cell activation. J Clin Invest 2016;126(1):207–19.Hammond E, Haynes NM, Cullinane C, Brennan TV, Bampton D, Handley P, et al. Immunomodulatory activities of pixatimod: emerging nonclinical and clinical data, and its potential utility in combination with PD-1 inhibitors. J Immunother Cancer 2018;6(1):54.Ethics ApprovalThe clinical trial entitled “An open-label, multi-centre Phase Ib study of the safety and tolerability of IV infused PG545 in combination with nivolumab in patients with advanced solid tumours with an expansion cohort in patients with metastatic pancreatic cancer. Protocol ZU545102” obtained ethics approval from the Royal Adelaide Hospital (HREC Reference number, HREC/17/RAH/195 and the CALHN Reference number, R20170515) and Bellberry Limited (Application No: 2018-08-695). All participants in the study gave informed consent before taking part in ZU545102.

Published

2021

18. 341 A phase Ib expansion cohort of pixatimod plus nivolumab in previously treated, microsatellite stable metastatic colorectal cancer (MSS mCRC)

Author

Amanda C. Stanley, Darryn Bampton, Andrew Clouson, Nick Pavlakis, Charlotte Lemech, Keith Dredge, Matthew Burge, Nigel J. Waterhouse, David Goldstein, Andrew Haydon, Lucie Leveque-ElMouttie, Grace Chojnowski, Michael P. Brown, and Edward Hammond

Subjects

Pharmacology, Oncology, Cancer Research, medicine.medical_specialty, Chemotherapy, business.industry, Colorectal cancer, medicine.medical_treatment, Immunology, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Cancer, medicine.disease, Primary tumor, Clinical trial, Tolerability, Internal medicine, medicine, Molecular Medicine, Immunology and Allergy, Nivolumab, business, RC254-282, Progressive disease

Abstract

BackgroundPixatimod is a novel immunomodulatory agent which stimulates dendritic cells (DC) via Toll-Like Receptor 9 (TLR9) pathway to activate natural killer (NK) cells.1 It also enhances T cell infiltration into tumors when combined with PD1 inhibitors in vivo.2 We report on safety, pharmacodynamics (PD), and antitumor activity of pixatimod plus nivolumab in a cohort of previously treated MSS mCRC subjects.MethodsEligible MSS mCRC patients (ECOG≤1) with a median of 3 lines of previous treatment received 25 mg pixatimod once weekly as a 1-hour i.v. infusion plus nivolumab (240 mg, every other week) until disease progression or discontinuation due to intolerability. Primary and secondary objectives included the assessment of safety and antitumor activity per RECIST v1.1 at the recommended dose, and evidence of immune activation in peripheral blood mononuclear cells (PBMC), plasma cytokines/chemokines, and paired tumor tissue biopsies, where available.ResultsThirty-three subjects with MSS mCRC (42% male) started treatment. Median age was 58 (range 35–80), median number of previous lines of chemotherapy was 3 (range 1–6), ECOG PS 0/1 was 67%/33%, 64% had target liver metastases, and primary tumor site was right-sided/transverse colon in 21% and left-sided colon/rectum 79%. Median number of cycles completed was 2 (range 0–13). Treatment-related AEs led to treatment discontinuation in 2 patients (autoimmune hepatitis and pneumonitis). Ten Grade 3 treatment-related AEs were reported in 4 subjects (12%). Thirty subjects received at least one cycle of treatment (1-month), with 25 subjects having initial post-baseline assessment scans > 6 weeks (as per RECIST v1.1). Of these, 3 subjects had confirmed partial responses and 8 had stable disease. Lower Pan-immune-Inflammatory Value (PIV = Neutrophils x Platelets x Monocytes/Lymphocytes) at screening were associated with clinical benefit (PR/SD). Post-treatment increases in plasma IP-10 and IP-10/IL-8 ratio, effector memory (CD45RA-CCR7-) CD4+ and CD8+ T cells, and Ki-67 expression in CD4+ and CD8+ T cells from PBMC were also detected in the clinical benefit cohort compared to subjects with progressive disease. Conversely, plasma levels of IL-6 were significantly lower in patients with clinical benefit. Analyses of pre- & on-treatment biopsies from the only PR patient with available paired biopsies demonstrated an increase in T cell infiltration.ConclusionsPixatimod is well tolerated at 25 mg in combination with a standard dose of nivolumab. The efficacy signal and pharmacodynamic changes in MSS mCRC warrants further investigation of pixatimod plus nivolumab for this patient population.AcknowledgementsResearch Funding provided by Zucero Therapeutics Ltd and Bristol Myers Squibb (BMS), Australia.Trial RegistrationClinical trial informationACTRN12617001573347ReferencesBrennan TV, Lin L, Brandstadter JD, Rendell VR, Dredge K, Huang X, et al. Heparan sulfate mimetic PG545-mediated antilymphoma effects require TLR9-dependent NK cell activation. J Clin Invest 2016;126(1):207–19.Hammond E, Haynes NM, Cullinane C, Brennan TV, Bampton D, Handley P, et al. Immunomodulatory activities of pixatimod: emerging nonclinical and clinical data, and its potential utility in combination with PD-1 inhibitors. J Immunother Cancer 2018;6(1):54.Ethics ApprovalThe clinical trial entitled “An open-label, multi-centre Phase Ib study of the safety and tolerability of IV infused PG545 in combination with nivolumab in patients with advanced solid tumours with an expansion cohort in patients with metastatic pancreatic cancer. Protocol ZU545102” obtained ethics approval from the Royal Adelaide Hospital (HREC Reference number, HREC/17/RAH/195 and the CALHN Reference number, R20170515) and Bellberry Limited (Application No: 2018-08-695). All participants in the study gave informed consent before taking part in ZU545102.

Published

2021

19. Heparanase Inhibition by Pixatimod (PG545): Basic Aspects and Future Perspectives

Author

Edward Hammond and Keith Dredge

Subjects

Sorafenib, Chemistry, Angiogenesis, Heparan sulfate, medicine.disease, Metastasis, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Paclitaxel, In vivo, medicine, Cancer research, Heparanase, 030212 general & internal medicine, Nivolumab, medicine.drug

Abstract

Pixatimod is an inhibitor of heparanase, a protein which promotes cancer via its regulation of the extracellular environment by enzymatic cleavage of heparan sulfate (HS) and non-enzymatic signaling. Through its inhibition of heparanase and other HS-binding signaling proteins, pixatimod blocks a number of pro-cancerous processes including cell proliferation, invasion, metastasis, angiogenesis and epithelial-mesenchymal transition. Several laboratories have found that these activities have translated into potent activity using a range of different mouse cancer models, including approximately 30 xenograft and 20 syngeneic models. Analyses of biological samples from these studies have confirmed the heparanase targeting of this agent in vivo and the broad spectrum of anti-cancer effects that heparanase blockade achieves. Pixatimod has been tested in combination with a number of approved anti-cancer drugs demonstrating its clinical potential, including with gemcitabine, paclitaxel, sorafenib, platinum agents and an anti-PD-1 antibody. Clinical testing has shown pixatimod to be well tolerated as a monotherapy, and it is currently being investigated in combination with the anti-PD-1 drug nivolumab in a pancreatic cancer phase I trial.

Published

2020

20. Sulfated glycolipid PG545 induces endoplasmic reticulum stress and augments autophagic flux by enhancing anticancer chemotherapy efficacy in endometrial cancer

Author

Boris Winterhoff, Ralf Schmidmaier, Viji Shridhar, Edward Hammond, Debarshi Roy, Sayantani Sarkar Bhattacharya, Robert Hoffmann, and Keith Dredge

Subjects

0301 basic medicine, Mice, Nude, Antineoplastic Agents, CHOP, Biochemistry, Article, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, In vivo, Cell Line, Tumor, Autophagy, medicine, Animals, Humans, Endoplasmic Reticulum Chaperone BiP, Pharmacology, Cisplatin, Dose-Response Relationship, Drug, Chemistry, Endoplasmic reticulum, Saponins, Endoplasmic Reticulum Stress, Xenograft Model Antitumor Assays, In vitro, Endometrial Neoplasms, Treatment Outcome, 030104 developmental biology, Paclitaxel, 030220 oncology & carcinogenesis, Unfolded protein response, Cancer research, Female, Glycolipids, medicine.drug

Abstract

The sulfated glycolipid PG545 shows promising antitumor activity in various cancers. This study was conducted to explore the effects and the mechanism of PG545 action in endometrial cancer (EC). PG545 exhibited strong synergy as assessed by the Chou-Talalay-Method in vitro when combined with cisplatin, or paclitaxel in both type I (Hec1B) and type II (ARK2) EC cell lines. While PG545 showed antitumor activity as monotherapy, a combination of PG545 with paclitaxel and cisplatin was highly effective in reducing the tumor burden and significantly prolonged survival of both Hec1B and ARK2 xenograft bearing mice. Mechanistically, PG545 elicits ER stress as an early response with resultant induction of autophagy. Our data demonstrated an increase in pERK, Bip/Grp78, IRE1α, Calnexin and CHOP/GADD153 within 6–24 hrs of PG545 treatment in EC cells. In parallel, PG545 also blocked FGF2 and HB-EGF mediated signaling in EC cells. Moreover, melatonin-mediated ER stress inhibition reduced PG545-mediated autophagy and PG545 in combination with cisplatin further heightened this stress response. Collectively these data indicate that PG545 exhibits strong synergistic effects with chemotherapeutics in vitro and showed promising antitumor activity in vivo. Our preclinical data indicates that in future studies PG545 can be a useful adjunct to chemotherapy in endometrial cancer.

Published

2020

21. A Phase I study of the novel immunomodulatory agent PG545 (pixatimod) in subjects with advanced solid tumours

Author

Jason D. Lickliter, Glynn Morrish, Keith Dredge, Liwen Lin, Edward Hammond, Michael P. Brown, Fleur Lankesheer, Todd V. Brennan, Yiping Yang, Michael Millward, Darryn Bampton, Paul Handley, Dredge, Keith, Brennan, Todd V, Hammond, Edward, Lickliter, Jason D, Lin, Liwen, Bampton, Darryn, Handley, Paul, Lankesheer, Fleur, Morrish, Glynn, Yang, Yiping, Brown, Michael P, and Millward, Michael

Subjects

0301 basic medicine, Oncology, Adult, Male, Cancer Research, medicine.medical_specialty, Maximum Tolerated Dose, Angiogenesis Inhibitors, Pilot Projects, Article, Cohort Studies, Immunomodulation, 03 medical and health sciences, 0302 clinical medicine, Immune system, Pharmacokinetics, Internal medicine, Neoplasms, medicine, Humans, Infusions, Intravenous, Aged, cancer immunotherapy, Dose-Response Relationship, Drug, business.industry, Cancer, Middle Aged, Saponins, medicine.disease, drug development, Clinical trial, 030104 developmental biology, Tolerability, 030220 oncology & carcinogenesis, Pharmacodynamics, Cohort, Disease Progression, Female, Cell activation, business

Abstract

Background: PG545 (pixatimod) is a novel immunomodulatory agent, which has been demonstrated to stimulate innate immune responses against tumours in preclinical ca ncer models. Methods: This Phase I study investigated the safety, tolerability, pharmacokinetics, pharmacodynamics and preliminary efficacy of PG545 monotherapy. Escalating doses of PG545 were administered to patients with advanced solid malignancies as a weekly 1-h intravenous infusion. Results: Twenty-three subjects were enroled across four cohorts (25, 50, 100 and 150 mg). Three dose-limiting toxicities (DLTs)-hypertension (2), epistaxis (1)-occurred in the 150 mg cohort. No DLTs were noted in the 100 mg cohort, which was identified as the maximum-tolerated dose. No objective responses were reported. Best response was stable disease up to 24 weeks, with the disease control rate in evaluable subjects of 38%. Exposure was proportional up to 100 mg and mean half-life was 141 h. The pharmacodynamic data revealed increases in innate immune cell activation, plasma IFNγ, TNFα, IP-10 and MCP-1. Conclusion: PG545 demonstrated a tolerable safety profile, proportional PK, evidence of immune cell stimulation and disease control in some subjects. Taken together, these data support the proposed mechanism of action, which represents a promising approach for use in combination with existing therapies. Refereed/Peer-reviewed

Published

2018

22. The heparan sulfate mimetic PG545 interferes with Wnt/β-catenin signaling and significantly suppresses pancreatic tumorigenesis alone and in combination with gemcitabine

Author

Debabrata Mukhopadhyay, Bonglee Kim, Eun Ok Kim, Viji Shridhar, Sung-Hoon Kim, Edward Hammond, Enfeng Wang, Ji Hoon Jung, Miyong Yun, Keith Dredge, Deok Beom Jung, and Jae Kwang Kim

Subjects

PG545, Beta-catenin, Carcinogenesis, pancreatic cancer, heparan sulfate mimetic, Mice, Nude, Angiogenesis Inhibitors, Biology, medicine.disease_cause, Deoxycytidine, Mice, Random Allocation, chemistry.chemical_compound, Biomimetic Materials, Pancreatic tumor, Cell Line, Tumor, Pancreatic cancer, Antineoplastic Combined Chemotherapy Protocols, medicine, Animals, Humans, Heparanase, Wnt Signaling Pathway, beta Catenin, Wnt/β-catenin, Wnt signaling pathway, gemcitabine, Correction, Drug Synergism, Heparan sulfate, Saponins, medicine.disease, Xenograft Model Antitumor Assays, Gemcitabine, Pancreatic Neoplasms, Oncology, chemistry, Cancer research, biology.protein, Female, Carcinoma, Pancreatic Ductal, medicine.drug, Research Paper

Abstract

The heparan sulfate mimetic PG545 has been shown to exert anti-angiogenic and anti-metastatic activity in vitro and in vivo cancer models. Although much of this activity has been attributed to inhibition of heparanase and heparan sulfate-binding growth factors, it was hypothesized that PG545 may additionally disrupt Wnt signaling, an important pathway underlying the malignancy of pancreatic cancer. We show that PG545, by directly interacting with Wnt3a and Wnt7a, inhibits Wnt/β-catenin signaling leading to inhibition of proliferation in pancreatic tumor cell lines. Additionally, we demonstrate for the first time that the combination of PG545 with gemcitabine has strong synergistic effects on viability, motility and apoptosis induction in several pancreatic cell lines. In an orthotopic xenograft mouse model, combination of PG545 with gemcitabine efficiently inhibited tumor growth and metastasis compared to single treatment alone. Also, PG545 treatment alone decreased the levels of β-catenin and its downstream targets, cyclin D1, MMP-7 and VEGF which is consistent with our in vitro data. Collectively, our findings suggest that PG545 exerts anti-tumor activity by disrupting Wnt/β-catenin signaling and combination with gemcitabine should be considered as a novel therapeutic strategy for pancreatic cancer treatment.

Published

2014

23. Correction: The heparan sulfate mimetic PG545 interferes with Wnt/β-catenin signaling and significantly suppresses pancreatic tumorigenesis alone and in combination with gemcitabine

Author

Keith Dredge, Ji Hoon Jung, Enfeng Wang, Debabrata Mukhopadhyay, Edward Hammond, Jae Kwang Kim, Sung-Hoon Kim, Miyong Yun, Bonglee Kim, Eun Ok Kim, Viji Shridhar, and Deok Beom Jung

Subjects

chemistry.chemical_compound, Oncology, chemistry, medicine, Cancer research, Wnt β catenin signaling, Heparan sulfate, Carcinogenesis, medicine.disease_cause, Gemcitabine, medicine.drug

Published

2019

24. Loss of HSulf-1: The Missing Link between Autophagy and Lipid Droplets in Ovarian Cancer

Author

Keith Dredge, Xiaoping He, Deok–Beom B. Jung, Thomas Dierks, Ashwani Khurana, Debarshi Roy, Susmita Mondal, Robert Hoffmann, Viji Shridhar, Edward Hammond, and Eleftheria Kalogera

Subjects

0301 basic medicine, medicine.medical_treatment, Phospholipases A2, Cytosolic, Antineoplastic Agents, Vacuole, Arachidonic Acids, Biology, Article, Sulfate binding, Carboplatin, Small hairpin RNA, 03 medical and health sciences, Mice, Downregulation and upregulation, Lipid droplet, medicine, Autophagy, Tumor Cells, Cultured, Animals, Humans, Enzyme Inhibitors, RNA, Small Interfering, Ovarian Neoplasms, Multidisciplinary, Growth factor, Lipid Droplets, Xenograft Model Antitumor Assays, 3. Good health, Cell biology, Gene Expression Regulation, Neoplastic, Drug Combinations, 030104 developmental biology, Female, Signal transduction, Sulfotransferases, Signal Transduction

Abstract

Defective autophagy and deranged metabolic pathways are common in cancer; pharmacologic targeting of these two pathways could provide a viable therapeutic option. However, how these pathways are regulated by limited availability of growth factors is still unknown. Our study shows that HSulf-1 (endosulfatase), a known tumor suppressor which attenuates heparin sulfate binding growth factor signaling, also regulates interplay between autophagy and lipogenesis. Silencing of HSulf-1 in OV202 and TOV2223 cells (ovarian cancer cell lines) resulted in increased lipid droplets (LDs), reduced autophagic vacuoles (AVs) and less LC3B puncta. In contrast, HSulf-1 proficient cells exhibit more AVs and reduced LDs. Increased LDs in HSulf-1 depleted cells was associated with increased ERK mediated cPLA2S505 phosphorylation. Conversely, HSulf-1 expression in SKOV3 cells reduced the number of LDs and increased the number of AVs compared to vector controls. Furthermore, pharmacological (AACOCF3) and ShRNA mediated downregulation of cPLA2 resulted in reduced LDs, and increased autophagy. Finally, in vivo experiment using OV202 Sh1 derived xenograft show that AACOCF3 treatment effectively attenuated tumor growth and LD biogenesis. Collectively, these results show a reciprocal regulation of autophagy and lipid biogenesis by HSulf-1 in ovarian cancer.

Published

2017

25. Inhibition of Heparanase in Pediatric Brain Tumor Cells Attenuates their Proliferation, Invasive Capacity, and

Author

Argyris, Spyrou, Soumi, Kundu, Lulu, Haseeb, Di, Yu, Tommie, Olofsson, Keith, Dredge, Edward, Hammond, Uri, Barash, Israel, Vlodavsky, and Karin, Forsberg-Nilsson

Subjects

Neovascularization, Pathologic, Brain Neoplasms, Brain, Down-Regulation, Apoptosis, Saponins, Xenograft Model Antitumor Assays, Up-Regulation, Cell Movement, Cell Line, Tumor, Focal Adhesion Protein-Tyrosine Kinases, Humans, Neoplasm Invasiveness, Phosphorylation, RNA, Small Interfering, Child, Extracellular Signal-Regulated MAP Kinases, Protein Kinases, Cell Proliferation, Glucuronidase, Signal Transduction

Abstract

Curative therapy for medulloblastoma and other pediatric embryonal brain tumors has improved, but the outcome still remains poor and current treatment causes long-term complications. Malignant brain tumors infiltrate the healthy brain tissue and, thus despite resection, cells that have already migrated cause rapid tumor regrowth. Heparan sulfate proteoglycans (HSPG), major components of the extracellular matrix (ECM), modulate the activities of a variety of proteins. The major enzyme that degrades HS, heparanase (HPSE), is an important regulator of the ECM. Here, we report that the levels of HPSE in pediatric brain tumors are higher than in healthy brain tissue and that treatment of pediatric brain tumor cells with HPSE stimulated their growth. In addition, the latent, 65 kDa form of HPSE (that requires intracellular enzymatic processing for activation) enhanced cell viability and rapidly activated the ERK and AKT signaling pathways, before enzymatically active HPSE was detected. The HPSE inhibitor PG545 efficiently killed pediatric brain tumor cells, but not normal human astrocytes, and this compound also reduced tumor cell invasion

Published

2016

26. Heparan sulfate, an endogenous TLR4 agonist, promotes acute GVHD after allogeneic stem cell transplantation

Author

Liwen Lin, Todd V. Brennan, Zhiguo Li, Xiaopei Huang, Keith Dredge, Nelson J. Chao, Yiping Yang, and Diana M. Cardona

Subjects

Male, T-Lymphocytes, medicine.medical_treatment, Immunology, Extracellular matrix component, Graft vs Host Disease, chemical and pharmacologic phenomena, Hematopoietic stem cell transplantation, Biology, Biochemistry, Lymphocyte Depletion, Mice, chemistry.chemical_compound, immune system diseases, medicine, Animals, Humans, Transplantation, Homologous, Luciferases, Receptor, Cell Proliferation, Mice, Inbred BALB C, Immunosuppression, Dendritic Cells, Cell Biology, Hematology, Heparan sulfate, Dendritic cell, Middle Aged, Flow Cytometry, Mice, Inbred C57BL, Survival Rate, Toll-Like Receptor 4, Transplantation, surgical procedures, operative, chemistry, Hematologic Neoplasms, Female, Heparitin Sulfate, Stem cell, Stem Cell Transplantation

Abstract

Graft-versus-host disease (GVHD) remains the most common cause of nonrelapse-related morbidity and mortality after allogeneic hematopoietic stem cell transplantation (allo-HSCT). Although T-cell depletion and intensive immunosuppression are effective in the control of GVHD, they are often associated with higher rates of infection and tumor recurrence. In this study, we showed that heparan sulfate (HS), an extracellular matrix component, can activate Toll-like receptor 4 on dendritic cells in vitro, leading to the enhancement of dendritic cell maturation and alloreactive T-cell responses. We further demonstrated in vivo that serum HS levels were acutely elevated at the onset of clinical GVHD in mice after allo-HSCT. Treatment with the serine protease inhibitor α1-antitrypsin decreased serum levels of HS, leading to a reduction in alloreactive T-cell responses and GVHD severity. Conversely, an HS mimetic that increased serum HS levels accelerated GVHD. In addition, in patients undergoing allo-HSCT for hematologic malignancies, serum HS levels were elevated and correlated with the severity of GVHD. These results identify a critical role for HS in promoting acute GVHD after allo-HSCT, and they suggest that modulation of HS release may have therapeutic potential for the control of clinical GVHD.

Published

2012

27. Hypoxia negatively regulates heparan sulfatase 2 expression in renal cancer cell lines

Author

Keith Dredge, Ashwani Khurana, Viji Shridhar, Han W. Tun, John A. Copland, and Laura A. Marlow

Subjects

Cancer Research, Gene knockdown, Tumor suppressor gene, Growth factor, medicine.medical_treatment, Sulfatase, Cell migration, Vimentin, Heparan sulfate, Biology, urologic and male genital diseases, medicine.disease, Molecular biology, female genital diseases and pregnancy complications, Cell biology, chemistry.chemical_compound, Clear cell renal cell carcinoma, chemistry, medicine, biology.protein, Molecular Biology

Abstract

Inactivation of von Hippel-Lindau (VHL), a tumor suppressor gene is often associated with clear cell renal cell carcinoma (ccRCC). VHL inactivation leads to multitude of responses including enhanced growth factor signaling such as bFGF2, SDF-1α, and HGF. Here, we have identified a novel VHL-inducible gene, heparan sulfatase 2 (HSulf-2) that attenuates heparan-binding growth factor such as bFGF2 signaling. VHL-mediated HIF-1 alpha degradation was essential to restore HSulf-2 expression. Mechanistically, HSulf-2 negatively regulated vimentin expression and knockdown of vimentin abolished cell migration. This study reveals a novel layer of regulation of heparan-binding growth factor signaling via modulation of heparan sulfate by HSulf-2 in ccRCC.

Published

2011

28. PG545, a dual heparanase and angiogenesis inhibitor, induces potent anti-tumour and anti-metastatic efficacy in preclinical models

Author

C Vincent, Edward Hammond, Maree T. Smith, R Brandt, Keith Dredge, Paul Handley, Vito Ferro, Ian Bytheway, Thomas J. Gonda, Dredge, K, Hammond, E, Handley, P, Gonda, TJ, Smith, MT, Vincent, C, Brandt, R, Ferro, V, and Bytheway, I

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Angiogenesis, Mice, Nude, Angiogenesis Inhibitors, Antineoplastic Agents, Mice, SCID, heparanase, Metastasis, Neovascularization, Mice, angiogenesis, chemistry.chemical_compound, In vivo, Cell Line, Tumor, Neoplasms, medicine, Animals, Humans, Heparanase, Neoplasm Metastasis, Glucuronidase, Mice, Inbred BALB C, business.industry, Cancer, Heparan sulfate, Saponins, medicine.disease, Xenograft Model Antitumor Assays, Angiogenesis inhibitor, Mice, Inbred C57BL, Treatment Outcome, anti-metastatic, Oncology, chemistry, Cancer research, heparan sulfate, anti-tumour, medicine.symptom, Translational Therapeutics, business, HT29 Cells

Abstract

Background:PG545 is a heparan sulfate (HS) mimetic that inhibits tumour angiogenesis by sequestering angiogenic growth factors in the extracellular matrix (ECM), thus limiting subsequent binding to receptors. Importantly, PG545 also inhibits heparanase, the only endoglycosidase which cleaves HS chains in the ECM. The aim of the study was to assess PG545 in various solid tumour and metastasis models.Methods:The anti-angiogenic, anti-tumour and anti-metastatic properties of PG545 were assessed using in vivo angiogenesis, solid tumour and metastasis models. Pharmacokinetic (PK) data were also generated in tumour-bearing mice to gain an understanding of optimal dosing schedules and regimens.Results:PG545 was shown to inhibit angiogenesis in vivo and induce anti-tumour or anti-metastatic effects in murine models of breast, prostate, liver, lung, colon, head and neck cancers and melanoma. Enhanced anti-tumour activity was also noted when used in combination with sorafenib in a liver cancer model. PK data revealed that the half-life of PG545 was relatively long, with pharmacologically relevant concentrations of radiolabeled PG545 observed in liver tumours.Conclusion:PG545 is a new anti-angiogenic clinical candidate for cancer therapy. The anti-metastatic property of PG545, likely due to the inhibition of heparanase, may prove to be a critical attribute as the compound enters phase I clinical trials. Refereed/Peer-reviewed

Published

2011

29. The anti-cancer agents lenalidomide and pomalidomide inhibit the proliferation and function of T regulatory cells

Author

Jake Y. Henry, Peter H. Schafer, George W. Muller, Brendan Meyer, Stephen Todryk, Angus G. Dalgleish, Marie-Christine Labarthe, Keith Dredge, J. Blake Bartlett, David I. Stirling, Deborah C. Klaschka, Roger Shen-Chu Chen, and Christine Galustian

Subjects

Cancer Research, T cell, medicine.medical_treatment, Immunology, Antineoplastic Agents, Receptors, Nerve Growth Factor, Pharmacology, T-Lymphocytes, Regulatory, Receptors, Tumor Necrosis Factor, Mice, Transforming Growth Factor beta, Cell Line, Tumor, Glucocorticoid-Induced TNFR-Related Protein, medicine, Animals, Humans, Immunology and Allergy, Cytotoxic T cell, Lenalidomide, Multiple myeloma, Mice, Inbred BALB C, business.industry, FOXP3, Forkhead Transcription Factors, Immunotherapy, Receptors, OX40, medicine.disease, Pomalidomide, Interleukin-10, Thalidomide, medicine.anatomical_structure, Oncology, Colonic Neoplasms, Female, business, Receptors, Transforming Growth Factor beta, Immunosuppressive Agents, medicine.drug

Abstract

Lenalidomide (Revlimid; CC-5013) and pomalidomide (CC-4047) are IMiDs proprietary drugs having immunomodulatory properties that have both shown activity in cancer clinical trials; lenalidomide is approved in the United States for a subset of MDS patients and for treatment of patients with multiple myeloma when used in combination with dexamethasone. These drugs exhibit a range of interesting clinical properties, including anti-angiogenic, anti-proliferative, and pro-erythropoietic activities although exact cellular target(s) remain unclear. Also, anti-inflammatory effects on LPS-stimulated monocytes (TNF-alpha is decreased) and costimulatory effects on anti-CD3 stimulated T cells, (enhanced T cell proliferation and proinflammatory cytokine production) are observed. These drugs also cause augmentation of NK-cell cytotoxic activity against tumour-cell targets. Having shown that pomalidomide confers T cell-dependent adjuvant-like protection in a preclinical whole tumour-cell vaccine-model, we now show that lenalidomide and pomalidomide strongly inhibit T-regulatory cell proliferation and suppressor-function. Both drugs inhibit IL-2-mediated generation of FOXP3 positive CTLA-4 positive CD25high CD4+ T regulatory cells from PBMCs by upto 50%. Furthermore, suppressor function of pre-treated T regulatory cells against autologous responder-cells is abolished or markedly inhibited without drug related cytotoxicity. Also, Balb/C mice exhibit 25% reduction of lymph-node T regulatory cells after pomalidomide treatment. Inhibition of T regulatory cell function was not due to changes in TGF-beta or IL-10 production but was associated with decreased T regulatory cell FOXP3 expression. In conclusion, our data provide one explanation for adjuvant properties of lenalidomide and pomalidomide and suggest that they may help overcome an important barrier to tumour-specific immunity in cancer patients.

Published

2008

30. PI-88 and Novel Heparan Sulfate Mimetics Inhibit Angiogenesis

Author

Anaud Gautam, Ligong Liu, Vito Ferro, Kat Davis, Edward Hammond, Elizabeth Copeman, Cai Ping Li, Keith Dredge, Ken D. Johnstone, Ian Bytheway, and Tomislav Karoli

Subjects

Vascular Endothelial Growth Factor A, Carcinoma, Hepatocellular, Angiogenesis, Oligosaccharides, Fibroblast growth factor, chemistry.chemical_compound, Biomimetic Materials, Animals, Humans, Heparanase, Neoplasm Metastasis, Cell Proliferation, Tube formation, Matrigel, Neovascularization, Pathologic, Endothelial Cells, Hematology, Heparan sulfate, Vascular endothelial growth factor, Endothelial stem cell, Clinical Trials, Phase III as Topic, Heparin Lyase, Biochemistry, chemistry, Chemotherapy, Adjuvant, Cancer research, Fibroblast Growth Factor 1, Fibroblast Growth Factor 2, Heparitin Sulfate, Cardiology and Cardiovascular Medicine

Abstract

The heparan sulfate (HS) mimetic PI-88 is a promising inhibitor of tumor growth and metastasis expected to commence phase III clinical evaluation in 2007 as an adjuvant therapy for postresection hepatocellular carcinoma. Its anticancer properties are attributed to inhibition of angiogenesis via antagonism of the interactions of angiogenic growth factors and their receptors with HS. It is also a potent inhibitor of heparanase, an enzyme that plays a key role in both metastasis and angiogenesis. A series of PI-88 analogs have been prepared with enhanced chemical and biological properties. The new compounds consist of single, defined oligosaccharides with specific modifications designed to improve their pharmacokinetic properties. These analogs all inhibit heparanase and bind to the angiogenic fibroblast growth factor 1 (FGF-1), FGF-2, and vascular endothelial growth factor with similar affinity to PI-88. However, compared with PI-88, some of the newly designed compounds are more potent inhibitors of growth factor-induced endothelial cell proliferation and of endothelial tube formation on Matrigel. Representative compounds were also tested for antiangiogenic activity in vivo and were found to reduce significantly blood vessel formation. Moreover, the pharmacokinetic profile of several analogs was also improved, as evidenced primarily by lower clearance in comparison with PI-88. The current data support the development of HS mimetics as potent antiangiogenic anticancer agents.

Published

2007

31. PG545 enhances anti-cancer activity of chemotherapy in ovarian models and increases surrogate biomarkers such as VEGF in preclinical and clinical plasma samples

Author

Vijayalakshmi Shridhar, Jeremy Chien, Debarshi Roy, Edward Hammond, Luisa Freyer, Matthew S. Block, Boris Winterhoff, Attila Teoman, Antonia Von Bismarck, Sally A. Mullany, Susmita Mondal, Michael Millward, Darryn Bampton, Shailendra Giri, Keith Dredge, and Robert Hoffmann

Subjects

Oncology, Vascular Endothelial Growth Factor A, PG545, Cancer Research, medicine.medical_treatment, Mice, SCID, Inbred C57BL, Metastasis, chemistry.chemical_compound, Mice, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, Tumor Cells, Cultured, Cancer, Ovarian Neoplasms, Cultured, Tumor, Drug Synergism, VEGF, Tumor Cells, Up-Regulation, Vascular endothelial growth factor A, HB-EGF, Paclitaxel, 5.1 Pharmaceuticals, Public Health and Health Services, Female, Development of treatments and therapeutic interventions, medicine.drug, medicine.medical_specialty, Oncology and Carcinogenesis, SCID, Article, Rare Diseases, Ovarian cancer, Internal medicine, medicine, Biomarkers, Tumor, Animals, Humans, Oncology & Carcinogenesis, Cisplatin, Chemotherapy, Tumour microenvironment, business.industry, Saponins, medicine.disease, Xenograft Model Antitumor Assays, Clinical trial, Mice, Inbred C57BL, Orphan Drug, chemistry, business, Heparanase, Biomarkers

Abstract

BackgroundDespite the utility of antiangiogenic drugs in ovarian cancer, efficacy remains limited due to resistance linked to alternate angiogenic pathways and metastasis. Therefore, we investigated PG545, an anti-angiogenic and anti-metastatic agent which is currently in Phase I clinical trials, using preclinical models of ovarian cancer.MethodsPG545's anti-cancer activity was investigated in vitro and in vivo as a single agent, and in combination with paclitaxel, cisplatin or carboplatin using various ovarian cancer cell lines and tumour models.ResultsPG545, alone, or in combination with chemotherapeutics, inhibited proliferation of ovarian cancer cells, demonstrating synergy with paclitaxel in A2780 cells. PG545 inhibited growth factor-mediated cell migration and reduced HB-EGF-induced phosphorylation of ERK, AKT and EGFR in vitro and significantly reduced tumour burden which was enhanced when combined with paclitaxel in an A2780 model or carboplatin in a SKOV-3 model. Moreover, in the immunocompetent ID8 model, PG545 also significantly reduced ascites in vivo. In the A2780 maintenance model, PG545 initiated with, and following paclitaxel and cisplatin treatment, significantly improved overall survival. PG545 increased plasma VEGF levels (and other targets) in preclinical models and in a small cohort of advanced cancer patients which might represent a potential biomarker of response.ConclusionOur results support clinical testing of PG545, particularly in combination with paclitaxel, as a novel therapeutic strategy for ovarian cancer.

Published

2015

32. Heparan sulfate mimetic PG545-mediated antilymphoma effects require TLR9-dependent NK cell activation

Author

Todd V. Brennan, Xiaopei Huang, Liwen Lin, Joshua D. Brandstadter, Keith Dredge, Victoria R. Rendell, and Yiping Yang

Subjects

Lymphoma, Angiogenesis, Cell, Antineoplastic Agents, Lymphocyte Activation, Extracellular matrix, chemistry.chemical_compound, Mice, Cell Line, Tumor, medicine, Animals, Humans, Heparanase, Mice, Inbred BALB C, biology, TLR9, General Medicine, Heparan sulfate, Saponins, Interleukin-12, Killer Cells, Natural, Mice, Inbred C57BL, medicine.anatomical_structure, Proteoglycan, chemistry, Oligodeoxyribonucleotides, Toll-Like Receptor 9, Myeloid Differentiation Factor 88, biology.protein, Cancer research, Interleukin 12, Heparitin Sulfate, Lysosomes, Research Article

Abstract

Heparan sulfate (HS) is an essential component of the extracellular matrix (ECM), which serves as a barrier to tumor invasion and metastasis. Heparanase promotes tumor growth by cleaving HS chains of proteoglycan and releasing HS-bound angiogenic growth factors and facilitates tumor invasion and metastasis by degrading the ECM. HS mimetics, such as PG545, have been developed as antitumor agents and are designed to suppress angiogenesis and metastasis by inhibiting heparanase and competing for the HS-binding domain of angiogenic growth factors. However, how PG545 exerts its antitumor effect remains incompletely defined. Here, using murine models of lymphoma, we determined that the antitumor effects of PG545 are critically dependent on NK cell activation and that NK cell activation by PG545 requires TLR9. We demonstrate that PG545 does not activate TLR9 directly but instead enhances TLR9 activation through the elevation of the TLR9 ligand CpG in DCs. Specifically, PG545 treatment resulted in CpG accumulation in the lysosomal compartment of DCs, leading to enhanced production of IL-12, which is essential for PG545-mediated NK cell activation. Overall, these results reveal that PG545 activates NK cells and that this activation is critical for the antitumor effect of PG545. Moreover, our findings may have important implications for improving NK cell–based antitumor therapies.

Published

2015

33. Dendritic Cell Immunotherapy for Melanoma

Author

Judy C. Peng, Keith Dredge, and Ranjeny Thomas

Subjects

Pharmacology, Clinical Trials as Topic, Skin Neoplasms, business.industry, medicine.medical_treatment, Melanoma, Cancer, Dendritic Cells, General Medicine, Immunotherapy, Dendritic cell, medicine.disease, Clinical trial, Immune system, Cancer immunotherapy, Immunology, Animals, Humans, Medicine, Progenitor cell, business

Abstract

Dendritic cells (DC) are the most potent antigen-presenting cells that initiate T cell-mediated immune responses against cancer. It has been almost a decade since the first trial of DC-based cancer immunotherapy was published. Despite the many clinical trials conducted since, few solid conclusions have been reached, and no specific-immunotherapy has routinely demonstrated meaningful anti-tumour responses. Clinical-grade DC can be obtained from three distinct cell populations in the blood - monocytes, CD34(+) progenitors or direct isolation of circulating blood DC. This review discusses the science behind DC-based cancer immunotherapy, with a particular emphasis on the use of monocyte-derived DC in melanoma clinical trials, and the various potential avenues for improvement of patient clinical response rates.

Published

2006

34. Orally administered lenalidomide (CC-5013) is anti-angiogenic in vivo and inhibits endothelial cell migration and Akt phosphorylation in vitro

Author

Ling Lu, J. Blake Bartlett, Yang Tang, David I. Stirling, Angus G. Dalgleish, Keith Dredge, Simon P. Robinson, Rebecca Horsfall, Peter H. Schafer, Ling-Hua Zhang, Michael A. Shirley, and George W. Muller

Subjects

Male, Umbilical Veins, Endothelium, Angiogenesis, Administration, Oral, Angiogenesis Inhibitors, Protein Serine-Threonine Kinases, Pharmacology, Biochemistry, Rats, Sprague-Dawley, Cell Movement, In vivo, Proto-Oncogene Proteins, Animals, Humans, Medicine, Mesentery, Phosphorylation, Lenalidomide, Protein kinase B, Multiple myeloma, Dose-Response Relationship, Drug, business.industry, Cell Biology, medicine.disease, Rats, Thalidomide, Endothelial stem cell, Kinetics, medicine.anatomical_structure, Area Under Curve, Endothelium, Vascular, Cardiology and Cardiovascular Medicine, business, Proto-Oncogene Proteins c-akt, medicine.drug

Abstract

The thalidomide analogue and immunomodulatory drug (IMiD) lenalidomide (CC-5013, REVLIMID) is emerging as a useful treatment for a number of cancers and has recently entered phase III trials for multiple myeloma. It has been suggested that the anti-tumor effect of lenalidomide is related to its anti-angiogenic potency. In this regard, we have previously shown that lenalidomide inhibits angiogenesis in both rat and human in vitro models but does not affect endothelial cell proliferation. We now show that oral administration of lenalidomide attenuates growth factor-induced angiogenesis in vivo; the rat mesenteric window assay was utilized to show that lenalidomide significantly inhibits vascularization in a dose-dependent manner. We also found that lenalidomide significantly inhibits growth factor-induced endothelial cell migration. This correlates with the inhibitory effect of lenalidomide on growth factor-induced Akt phosphorylation, thereby providing a potential mechanism for its anti-migratory and subsequent anti-angiogenic effects. These data further support the use of lenalidomide as an orally administered drug for the effective treatment of angiogenesis-dependent conditions, including cancer, and suggest a potential mechanism of action.

Published

2005

35. Thalidomide Derived Immunomodulatory Drugs (IMiDs) as Potential Therapeutic Agents

Author

J Blake Marriott, Angus G. Dalgleish, and Keith Dredge

Subjects

Clinical Trials, Phase I as Topic, Side effect, Tumor Necrosis Factor-alpha, business.industry, Endocrinology, Diabetes and Metabolism, Angiogenesis Inhibitors, Clinical settings, Bioinformatics, Thalidomide, Adjuvants, Immunologic, Neoplasms, medicine, Humans, Immunology and Allergy, business, medicine.drug

Abstract

Thalidomide is known to be effective in the treatment of a number of conditions, including leprosy and various cancers. The exact mechanisms of action remain unclear although these are known to include anti-tumour necrosis factor (TNF)-alpha, T cell costimulatory, anti-angiogenic and anti-tumour activities. However, thalidomide is being superceded by novel structural derivatives which have been designed to have improved immunomodulatory activity and side effect profiles. These are currently being characterised and some are entering the clinic in phase I/II studies. One novel group of structural analogues are classified as the Immunomodulatory Drugs (IMiDs). This review describes the emerging immunological, anti-angiogenic and direct anti-tumour properties of thalidomide and the characterisation and clinical application of its IMiD analogues. We describe the laboratory studies which have led to the characterisation and development of IMiDs into potentially clinically relevant drugs. Early trial data suggests that these compounds may themselves become established therapies, particularly in certain cancers. Furthermore, ongoing studies will determine how best to apply these compounds to the appropriate clinical settings. We will describe the various clinical studies of lead compounds that are in progress and speculate as to the potential and future development of these exciting compounds.

Published

2003

36. HSulf-1 deficiency dictates a metabolic reprograming of glycolysis and TCA cycle in ovarian cancer

Author

Debarshi Roy, Katherine Stilles, Val J. Lowe, Thomas Dierks, Ashwani Khurana, Samuel Leung, Susmita Mondal, Viji Shridhar, Edward Hammond, Steve E. Kalloger, Juliana Camacho-Pereira, Keith Dredge, Seth Padmabandu, Deepak Nagrath, Joelle Baddour, Blake Gilks, Lifeng Yang, and Eduardo N. Chini

Subjects

PG545, Glucose uptake, Citric Acid Cycle, Biology, Mice, Cell Line, Tumor, Animals, Humans, Glycolysis, Cell Proliferation, Mice, Knockout, Ovarian Neoplasms, HSulf-1, Pyruvate dehydrogenase complex, Microarray Analysis, Warburg effect, 3. Good health, Citric acid cycle, HB-EGF, ovarian cancer, c-Myc, Oncology, Biochemistry, Anaerobic glycolysis, biology.protein, Phosphorylation, GLUT1, Female, Sulfotransferases, Signal Transduction, Research Paper

Abstract

Warburg effect has emerged as a potential hallmark of many cancers. However, the molecular mechanisms that led to this metabolic state of aerobic glycolysis, particularly in ovarian cancer (OVCA) have not been completely elucidated. HSulf-1 predominantly functions by limiting the bioavailability of heparan binding growth factors and hence their downstream signaling. Here we report that HSulf-1, a known putative tumor suppressor, is a negative regulator of glycolysis. Silencing of HSulf-1 expression in OV202 cell line increased glucose uptake and lactate production by upregulating glycolytic genes such as Glut1, HKII, LDHA, as well as metabolites. Conversely, HSulf-1 overexpression in TOV21G cells resulted in the down regulation of glycolytic enzymes and reduced glycolytic phenotype, supporting the role of HSulf-1 loss in enhanced aerobic glycolysis. HSulf-1 deficiency mediated glycolytic enhancement also resulted in increased inhibitory phosphorylation of pyruvate dehydrogenase (PDH) thus blocking the entry of glucose flux into TCA cycle. Consistent with this, metabolomic and isotope tracer analysis showed reduced glucose flux into TCA cycle. Moreover, HSulf-1 loss is associated with lower oxygen consumption rate (OCR) and impaired mitochondrial function. Mechanistically, lack of HSulf-1 promotes c-Myc induction through HB-EGF-mediated p-ERK activation. Pharmacological inhibition of c-Myc reduced HB-EGF induced glycolytic enzymes implicating a major role of c-Myc in loss of HSulf-1 mediated altered glycolytic pathway in OVCA. Similarly, PG545 treatment, an agent that binds to heparan binding growth factors and sequesters growth factors away from their ligand also blocked HB-EGF signaling and reduced glucose uptake in vivo in HSulf-1 deficient cells.

Published

2015

37. An open-label, multi-center phase I study of the safety and tolerability of the novel immunomodulatory agent PG545 in subjects with advanced solid tumors

Author

Liwen Lin, Edward Hammond, Yiping Yang, Todd V. Brennan, Michael P. Brown, Keith Dredge, Darryn Bampton, Michael Millward, and Jason D. Lickliter

Subjects

0301 basic medicine, Cancer Research, business.industry, TLR9, Pharmacology, Phase i study, 03 medical and health sciences, 030104 developmental biology, Oncology, Tolerability, Medicine, Center (algebra and category theory), Immunomodulatory Agent, Open label, business

Abstract

3083 Background: PG545 (pixatimod, pINN) is a novel immunomodulatory agent which stimulates dendritic cells (DC) via TLR9/IL-12 pathway to activate natural killer (NK) cells. It also inhibits tumour-associated macrophages in cancer models. We report on safety, PK, PD, and antitumor activity of PG545 monotherapy. Methods: In this dose escalation (3+3 design) study, eligible pts (ECOG≤1) with advanced solid malignancies who failed standard therapies received PG545 once weekly as a 1-hour i.v. infusion until disease progression or discontinuation due to intolerability. The primary objective was determination of the maximum tolerated dose (MTD). Secondary objectives evaluated safety, antitumor activity based on RECIST (1.1) criteria, PK and PD (plasmacytoid DC & NKp46+NK cells from PBMC, and plasma cytokines/chemokines). Results: The study recruited 23 subjects across four cohorts (25, 50, 100 & 150 mg). Three dose limiting toxicities (DLTs) - hypertension (2), epistaxis (1) - occurred in the 150 mg cohort, which was identified as a non-tolerated dose level. No DLTs occurred in the 100 mg cohort, which was identified as the MTD. Six SAEs were reported to be possibly or likely related to PG545 treatment. No RECIST 1.1 objective responses were reported; best response was prolonged stable disease up to 24 weeks (mCRC), with disease control rate in evaluable subjects of 38% (6/16) at eight weeks. Exposure (AUC0-last) was proportional up to 100mg and mean half-life was 144 hours. At 50 and 100mg dose levels, two subjects in each cohort exhibited up to 4-fold increased numbers of NKp46+NK cells, IFN-α-producing pDCs, and increases (up to 25-fold) in plasma IFN-γ, TNF-α, IP-10 and MCP-1. Conclusions: PG545 is well tolerated up to 100 mg once-weekly via i.v. infusion. Human exposure data at 50mg and 100mg reach exposures consistent with those required for preclinical efficacy. Preliminary PD data support the proposed mechanism of action, which represents a promising approach to improve the efficacy of existing therapies. These data, and the absence of toxicities associated with chemo- or immunotherapies, support the development of PG545 in combination clinical trials. Clinical trial information: NCT02042781.

Published

2017

38. The role of heparanase and sulfatases in the modification of heparan sulfate proteoglycans within the tumour microenvironment and opportunities for novel cancer therapeutics

Author

Edward Hammond, Ashwani Khurana, Viji Shridhar, and Keith Dredge

Subjects

Cancer Research, Heparan sulfate, Review Article, Tumor initiation, Biology, SULF1, tumor microenvironment targeting, lcsh:RC254-282, Metastasis, Extracellular matrix, chemistry.chemical_compound, medicine, Heparanase, Tumor microenvironment, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Cell biology, carbohydrates (lipids), Oncology, chemistry, Tumor progression, Immunology, cancer therapy, Sulf2

Abstract

Heparan sulfate proteoglycans (HSPGs) are an integral and dynamic part of normal tissue architecture at the cell surface and within the extracellular matrix (ECM). The modification of HSPGs in the tumour microenvironment is known to result not just in structural but also functional consequences which significantly impact cancer progression. As substrates for the key enzymes sulfatases and heparanase, the modification of HSPGs is typically characterised by the degradation of heparan sulfate (HS) chains/sulfation patterns via the endo–6-O-sulfatases (Sulf1 and Sulf2) or by heparanase, an endo-glycosidase that cleaves the HS polymers releasing smaller fragments from HSPG complexes. Numerous studies have demonstrated how these enzymes actively influence cancer cell proliferation, signalling, invasion and metastasis. The activity or expression of these enzymes have been reported to be modified in a variety of cancers. Such observations are consistent with the degradation of normal architecture and basement membranes which are typically compromised in metastatic disease. Moreover, recent studies elucidating the requirements for these proteins in tumour initiation and progression exemplify their importance in the development and progression of cancer. Thus, as the influence of the tumour microenvironment in cancer progression becomes more apparent, the focus on targeting enzymes that degrade HSPGs highlights one approach to maintain normal tissue architecture, inhibit tumour progression and block metastasis. This review discusses the role of these enzymes in the context of the tumour microenvironment and their promise as therapeutic targets for the treatment of cancer.

Published

2014

39. Differential effect of a single high dose of the tricyclic antidepressant imipramine on interleukin-1β and tumor necrosis factor-α secretion following an in vivo lipopolysaccharide challenge in rats

Author

Keith Dredge, Brian E. Leonard, Thomas J. Connor, and John P. Kelly

Subjects

Lipopolysaccharides, Male, Imipramine, medicine.medical_specialty, medicine.medical_treatment, Immunology, Antidepressive Agents, Tricyclic, Pharmacology, Proinflammatory cytokine, Rats, Sprague-Dawley, In vivo, Internal medicine, medicine, Animals, Tumor Necrosis Factor-alpha, business.industry, Interleukin, Interleukin-10, Rats, Interleukin 10, Endocrinology, Cytokine, Tumor necrosis factor alpha, Corticosterone, business, Glucocorticoid, Interleukin-1, medicine.drug

Abstract

Tricyclic antidepressants (TCAs) of which imipramine is one, are commonly used in the treatment of depressive disorders and other forms of psychiatric illness. There have been many reports regarding the suppressive effects of TCAs on immune function. However, information is still limited regarding the effects of TCAs on the immune system, as many of the studies conducted to date have concentrated on in vitro exposure to such drugs, or ex vivo measures of immunity following drug administration. Thus in the present investigation, an in vivo challenge with bacterial lipopolysaccharide (LPS) (100 microg/kg; i.p.) was used to assess immunocompetence following administration of a single high dose of the TCA, imipramine (100 mg/kg, p.o.). The results demonstrated that imipramine pretreatment inhibits LPS-induced increases in serum concentrations of the proinflammatory cytokine, tumor necrosis factor (TNF)-alpha both 3 and 6 h, following administration. However, LPS-induced interleukin (IL)-1beta secretion was not significantly altered following imipramine treatment at either of the timepoints examined. In addition, serum concentrations of corticosterone and the antiinflammatory cytokine IL-10 were measured, and imipramine treatment failed to alter either basal, or LPS-induced increases in these immunosuppressive agents. In conclusion, although IL-1beta and TNF-alpha are both macrophage-derived proinflammatory cytokines, the present study demonstrates a differential sensitivity of these cytokines to the suppressive effects of the TCA imipramine. Furthermore, the suppressive effects of imipramine on LPS-induced TNF-alpha secretion could not be attributed to either increased glucocorticoid levels, or increased secretion of the antiinflammatory cytokine IL-10. The relevance of these findings to antidepressant-induced immunotoxicity are discussed.

Published

1999

40. PG545, an angiogenesis and heparanase inhibitor, reduces primary tumor growth and metastasis in experimental pancreatic cancer

Author

Katherine T. Ostapoff, Keith Dredge, Roderich E. Schwarz, Niranjan Awasthi, Stefan Hinz, Rolf A. Brekken, and Bercin Kutluk Cenik

Subjects

Cancer Research, medicine.medical_specialty, Angiogenesis, Cell Survival, Angiogenesis Inhibitors, Mice, SCID, Biology, Metastasis, Mice, Random Allocation, Mice, Inbred NOD, Internal medicine, Pancreatic cancer, Cell Line, Tumor, Genetic model, medicine, Animals, Humans, Heparanase, Neoplasm Metastasis, Cell Proliferation, Glucuronidase, Tumor microenvironment, Saponins, medicine.disease, Primary tumor, Mice, Inbred C57BL, Pancreatic Neoplasms, Disease Models, Animal, Endocrinology, Oncology, Tumor progression, Cancer research, Carcinoma, Pancreatic Ductal

Abstract

Aggressive tumor progression, metastasis, and resistance to conventional therapies lead to an extremely poor prognosis for pancreatic ductal adenocarcinoma (PDAC). Heparanase, an enzyme expressed by multiple cell types, including tumor cells in the tumor microenvironment, has been implicated in angiogenesis and metastasis, and its expression correlates with decreased overall survival in PDAC. We evaluated the therapeutic potential of PG545, an angiogenesis and heparanase inhibitor, in experimental PDAC. PG545 inhibited the proliferation, migration, and colony formation of pancreatic cancer cells in vitro at pharmacologically relevant concentrations. Heparanase inhibition also reduced the proliferation of fibroblasts but had only modest effects on endothelial cells in vitro. Furthermore, PG545 significantly prolonged animal survival in intraperitoneal and genetic models (mPDAC: LSL-KrasG12D; Cdkn2alox/lox; p48Cre) of PDAC. PG545 also inhibited primary tumor growth and metastasis in orthotopic and genetic endpoint studies. Analysis of tumor tissue revealed that PG545 significantly decreased cell proliferation, increased apoptosis, reduced microvessel density, disrupted vascular function, and elevated intratumoral hypoxia. Elevated hypoxia is a known driver of collagen deposition and tumor progression; however, tumors from PG545-treated animals displayed reduced collagen deposition and a greater degree of differentiation compared with control or gemcitabine-treated tumors. These results highlight the potent antitumor activity of PG545 and support the further exploration of heparanase inhibitors as a potential clinical strategy for the treatment of PDAC. Mol Cancer Ther; 12(7); 1190–201. ©2013 AACR.

Published

2013

41. PG545, a heparan sulfate mimetic, reduces heparanase expression in vivo, blocks spontaneous metastases and enhances overall survival in the 4T1 breast carcinoma model

Author

Ralf Brandt, Edward Hammond, and Keith Dredge

Subjects

Lung Neoplasms, Angiogenesis, Glycobiology, Cancer Treatment, lcsh:Medicine, Angiogenesis Inhibitors, Biochemistry, Tyrosine-kinase inhibitor, Metastasis, Immunoenzyme Techniques, chemistry.chemical_compound, Mice, Antineoplastic Combined Chemotherapy Protocols, Drug Discovery, Basic Cancer Research, Breast Tumors, Medicine, lcsh:Science, Cells, Cultured, Glucuronidase, Multidisciplinary, Neovascularization, Pathologic, Heparan sulfate, Sorafenib, Primary tumor, Oncology, Disease Progression, Female, Oncology Agents, Antiangiogenesis Therapy, medicine.drug, Research Article, Biotechnology, Niacinamide, Drugs and Devices, Drug Research and Development, medicine.drug_class, Antineoplastic Agents, Enzyme-Linked Immunosorbent Assay, Polysaccharides, Human Umbilical Vein Endothelial Cells, Animals, Humans, Heparanase, Biology, business.industry, Phenylurea Compounds, lcsh:R, Cancer, Mammary Neoplasms, Experimental, Cancers and Neoplasms, Saponins, medicine.disease, chemistry, Pharmacodynamics, Immunology, Cancer research, lcsh:Q, business

Abstract

PG545 is a clinically relevant heparan sulfate (HS) mimetic which, in addition to possessing anti-angiogenic properties, also acts as a heparanase inhibitor which may differentiate its mechanism(s) of action from approved angiogenesis inhibitors. The degradation of HS by heparanase has been strongly implicated in cell dissemination and the metastatic process. Thus, the anti-metastatic activity of PG545 has been linked to the enzymatic function of heparanase - the only endoglycosidase known to cleave HS, an important component of the extracellular matrix (ECM) which represents a potential avenue for therapeutic intervention for certain metastatic cancer indications. Recent concerns raised about the paucity of overall survival as an endpoint in mouse models of clinically relevant metastasis led us to examine the effect of PG545 on the progression of both primary tumor growth and the spontaneously metastasizing disease in the 4T1 syngeneic breast carcinoma model in a non-surgical and surgical (mastectomy) setting. PG545 significantly inhibited primary tumor growth but importantly also inhibited lung metastasis in treated mice, an effect not observed with the tyrosine kinase inhibitor sorafenib. Importantly, PG545 significantly enhanced overall survival compared to vehicle control and the sorafenib group, suggesting PG545's inhibitory effect on heparanase is indeed a critical attribute to induce anti-metastatic activity. In addition to blocking a common angiogenic signalling pathway in tumor cells, the expression of heparanase in the primary tumor and lung was also significantly reduced by PG545 treatment. These results support the ongoing development of PG545 and highlight the potential utility in metastatic disease settings.

Published

2012

42. Hypoxia negatively regulates heparan sulfatase 2 expression in renal cancer cell lines

Author

Ashwani, Khurana, Han W, Tun, Laura, Marlow, John A, Copland, Keith, Dredge, and Viji, Shridhar

Subjects

Base Sequence, Von Hippel-Lindau Tumor Suppressor Protein, Cell Line, Tumor, Blotting, Western, Down-Regulation, Humans, Sulfatases, urologic and male genital diseases, female genital diseases and pregnancy complications, Cell Hypoxia, Kidney Neoplasms, Article

Abstract

Inactivation of von Hippel-Lindau (VHL), a tumor suppressor gene is often associated with clear cell renal cell carcinoma (ccRCC). VHL inactivation leads to multitude of responses including enhanced growth factor signaling such as bFGF2, SDF-1α, and HGF. Here, we have identified a novel VHL-inducible gene, heparan sulfatase 2 (HSulf-2) that attenuates heparan-binding growth factor such as bFGF2 signaling. VHL-mediated HIF-1 alpha degradation was essential to restore HSulf-2 expression. Mechanistically, HSulf-2 negatively regulated vimentin expression and knockdown of vimentin abolished cell migration. This study reveals a novel layer of regulation of heparan-binding growth factor signaling via modulation of heparan sulfate by HSulf-2 in ccRCC.

Published

2011

43. Synthesis and biological evaluation of polysulfated oligosaccharide glycosides as inhibitors of angiogenesis and tumor growth

Author

Ken D. Johnstone, Francis C. K. Chiu, Ligong Liu, David M. Shackleford, Tomislav Karoli, Keith Dredge, Elizabeth Copeman, Susan A. Charman, Cai Ping Li, William N. Charman, Job Harenberg, Ian Bytheway, Vito Ferro, Kat Davis, Thomas J. Gonda, Edward Hammond, Edmund Kostewicz, Johnstone, Ken D, Karoli, Tomislav, Liu, Ligong, Dredge, Keith, Copeman, Elizabeth, Li, Cai Ping, Davis, Kat, Hammond, Edward, Bytheway, Ian, Kostewicz, Edmund, Chiu, Francis CK, Shackleford, David M, Charman, Susan A, Charman, William N, Harenberg, Job, Gonda, Thomas J, and Ferro, Vito

Subjects

Male, Vascular Endothelial Growth Factor A, Angiogenesis, Melanoma, Experimental, Neovascularization, Physiologic, Oligosaccharides, Angiogenesis Inhibitors, In Vitro Techniques, Sulfuric Acid Esters, Rats, Sprague-Dawley, chemistry.chemical_compound, angiogenesis, Mice, Structure-Activity Relationship, Sulfation, In vivo, Drug Discovery, Structure–activity relationship, Tetrasaccharide, Animals, Humans, Glycosides, Blood Coagulation, Glucuronidase, Neovascularization, Pathologic, Molecular Mimicry, Biological activity, Heparan sulfate, Xenograft Model Antitumor Assays, Rats, Mice, Inbred C57BL, tumor growth, chemistry, Biochemistry, Drug Resistance, Neoplasm, Molecular Medicine, Fibroblast Growth Factor 1, Fibroblast Growth Factor 2, Heparitin Sulfate, Ex vivo, Protein Binding

Abstract

A series of polysulfated penta- and tetrasaccharide glycosides containing α(13)/α(12)-linked mannose residues were synthesized as heparan sulfate (HS) mimetics and evaluated for their ability to inhibit angiogenesis. The compounds bound tightly to angiogenic growth factors (FGF-1, FGF-2, and VEGF) and strongly inhibited heparanase activity. In addition, the compounds exhibited potent activity in cell-based and ex vivo assays indicative of angiogenesis, with tetrasaccharides exhibiting activity comparable to that of pentasaccharides. Selected compounds also showed good antitumor activity in vivo in a mouse melanoma (solid, tumor) model resistant to the phase III HS mimetic 1 (muparfostat, formerly known as PI-88). The lipophilic modifications also resulted in reduced anticoagulant activity, a common side effect of HS mimetics, and conferred a reasonable pharmacokinetic profile in the rat, as exemplified by the sulfated octyl tetrasaccharide 5. The data support the further investigation of this class of compounds as potential antiangiogenic, anticancer therapeutics. Refereed/Peer-reviewed

Published

2010

44. ChemInform Abstract: An Improved Synthetic Route to the Potent Angiogenesis Inhibitor Benzyl Manα(1→3)Manα(1→3)-Manα (1→3)Manα(1→2)-Man Hexadecasulfate

Author

Ligong Liu, Ken D. Johnstone, Jon K. Fairweather, Keith Dredge, and Vito Ferro

Subjects

chemistry.chemical_classification, Sulfation, Chemistry, Stereochemistry, Block (telecommunications), Monosaccharide, General Medicine, Oligosaccharide, Angiogenesis inhibitor

Abstract

An improved synthetic route to α(1→3)/α(1→2)-linked mannooligosaccharides has been developed and applied to a more efficient preparation of the potent anti-angiogenic sulfated pentasaccharide, benzyl Manα(1→3)-Manα(1→3)-Manα(1→3)-Manα(1→2)-Man hexadecasulfate, using only two monosaccharide building blocks. Of particular note are improvements in the preparation of both building blocks and a simpler, final deprotection strategy. The route also provides common intermediates for the introduction of aglycones other than benzyl, either at the building block stage or after oligosaccharide assembly. The anti-angiogenic activity of the synthesized target compound was confirmed via the rat aortic assay.

Published

2009

45. The PG500 series: novel heparan sulfate mimetics as potent angiogenesis and heparanase inhibitors for cancer therapy

Author

Ken D. Johnstone, Norbert Wimmer, Keith Dredge, Cai Ping Li, Vito Ferro, Kat Davis, Thomas J. Gonda, Ligong Liu, Anand Gautam, Ian Bytheway, Paul Handley, Edward Hammond, Dredge, K, Hammond, E, Davis, K, Li, CP, Liu, L, Johnstone, K, Handley, P, Wimmer, N, Gonda, TJ, Gautam, A, Ferro, V, and Bytheway, I

Subjects

Vascular Endothelial Growth Factor A, Angiogenesis, Drug Evaluation, Preclinical, Antineoplastic Agents, heparanase, Cell Line, Neovascularization, chemistry.chemical_compound, angiogenesis, Structure-Activity Relationship, In vivo, Cell Line, Tumor, Neoplasms, Drug Discovery, medicine, Structure–activity relationship, Humans, Pharmacology (medical), Heparanase, Cell Proliferation, Glucuronidase, Pharmacology, Neovascularization, Pathologic, Rational design, Anticoagulants, Heparan sulfate, Oncology, Biochemistry, chemistry, Drug development, cancer therapy, Fibroblast Growth Factor 1, Fibroblast Growth Factor 2, heparan sulfate, Heparitin Sulfate, medicine.symptom

Abstract

Heparan sulfate mimetics, which we have called the PG500 series, have been developed to target the inhibition of both angiogenesis and heparanase activity. This series extends the technology underpinning PI-88, a mixture of highly sulfated oligosaccharides which reached Phase III clinical development for hepatocellular carcinoma. Advances in the chemistry of the PG500 series provide numerous advantages over PI-88. These new compounds are fully sulfated, single entity oligosaccharides attached to a lipophilic moiety, which have been optimized for drug development. The rational design of these compounds has led to vast improvements in potency compared to PI-88, based on in vitro angiogenesis assays and in vivo tumor models. Based on these and other data, PG545 has been selected as the lead clinical candidate for oncology and is currently undergoing formal preclinical development as a novel treatment for advanced cancer. Refereed/Peer-reviewed

Published

2009

46. Antiangiogenic Therapy for Melanoma

Author

Angus G. Dalgleish and Keith Dredge

Subjects

business.industry, Melanoma, Antiangiogenic therapy, Cancer research, Medicine, business, medicine.disease

Published

2007

47. CC-1088 Celgene

Author

Keith, Dredge

Subjects

Inflammation, Clinical Trials as Topic, Drug Industry, Withholding Treatment, 3',5'-Cyclic-AMP Phosphodiesterases, Phosphodiesterase Inhibitors, Contraindications, Myelodysplastic Syndromes, Animals, Humans, Cyclic Nucleotide Phosphodiesterases, Type 4, Thalidomide

Abstract

CC-1088, a thalidomide analog inhibitor of phosphodiesterase 4, was being developed by Celgene for the potential treatment of inflammatory diseases and myelodysplastic syndromes, and had undergone clinical trials. By April 2005, however, the company was no longer developing CC-1088, with CC-10004 presumed to be the preferred compound.

Published

2005

48. AE-941 (AEterna)

Author

Keith, Dredge

Subjects

Clinical Trials as Topic, Lung Neoplasms, Tissue Extracts, Carcinoma, Non-Small-Cell Lung, Animals, Humans, Antineoplastic Agents, Drugs, Investigational

Abstract

AEterna is developing AE-941, an angiogenesis inhibitor derived from the ultrafiltration of liquid shark cartilage, with matrix metalloprotease (MMP)-2, MMP-9 and vascular endothelial growth factor inhibitory properties, for the potential treatment of non-small-cell lung cancer.

Published

2004

49. The evolution of thalidomide and its IMiD derivatives as anticancer agents

Author

Keith Dredge, J. Blake Bartlett, and Angus G. Dalgleish

Subjects

Clinical Trials as Topic, business.industry, Tumor Necrosis Factor-alpha, Applied Mathematics, General Mathematics, T-Lymphocytes, Anti-Inflammatory Agents, Angiogenesis Inhibitors, Antineoplastic Agents, Pharmacology, medicine.disease, Thalidomide, Neoplasms, Medicine, Effective treatment, Humans, business, Multiple Myeloma, Lenalidomide, Multiple myeloma, medicine.drug

Abstract

Thalidomide was originally used to treat morning sickness, but was banned in the 1960s for causing serious congenital birth defects. Remarkably, thalidomide was subsequently discovered to have anti-inflammatory and anti-angiogenic properties, and was identified as an effective treatment for multiple myeloma. A series of immunomodulatory drugs — created by chemical modification of thalidomide — have been developed to overcome the original devastating side effects. Their powerful anticancer properties mean that these drugs are now emerging from thalidomide's shadow as useful anticancer agents.

Published

2004

50. Phase I study to determine the safety, tolerability and immunostimulatory activity of thalidomide analogue CC-5013 in patients with metastatic malignant melanoma and other advanced cancers

Author

Keith Dredge, A Polychronis, A G Dalgleish, H Kristeleit, David I. Stirling, G W Muller, J B Bartlett, Jerome B. Zeldis, S Nicholson, Hardev Pandha, I A Clarke, and Agnieszka Michael

Subjects

Oncology, Adult, Male, Vascular Endothelial Growth Factor A, Cancer Research, medicine.medical_specialty, Skin Neoplasms, Adolescent, Maximum Tolerated Dose, T-Lymphocytes, Angiogenesis Inhibitors, immunomodulation, Metastasis, chemistry.chemical_compound, Clinical, Internal medicine, Neoplasms, thalidomide, T-cell activation, medicine, Humans, CC-5013, Adverse effect, Lenalidomide, Melanoma, Aged, Aged, 80 and over, business.industry, Middle Aged, phase I, medicine.disease, cytokines, Vascular endothelial growth factor, Thalidomide, Regimen, chemistry, Tolerability, Toxicity, Immunology, Female, Fibroblast Growth Factor 2, Immunization, Safety, business, medicine.drug

Abstract

We assessed the safety, tolerability and efficacy of the immunomodulatory drug, CC-5013 (REVIMID trade mark ), in the treatment of patients with metastatic malignant melanoma and other advanced cancers. A total of 20 heavily pretreated patients received a dose-escalating regimen of oral CC-5013. Maximal tolerated dose, toxicity and clinical responses were evaluated and analysis of peripheral T-cell surface markers and serum for cytokines and proangiogenic factors were performed. CC-5013 was well tolerated. In all, 87% of adverse effects were classified as grade 1 or grade 2 according to Common Toxicity Criteria and there were no serious adverse events attributable to CC-5013 treatment. Six patients failed to complete the study, three because of disease progression, two withdrew consent and one was entered inappropriately and withdrawn from the study. The remaining 14 patients completed treatment without dose reduction, with one patient achieving partial remission. Evidence of T-cell activation was indicated by significantly increased serum levels of sIL-2 receptor, granulocyte-macrophage colony-stimulating factor, interleukin-12 (IL-12), tumour necrosis factor-alpha and IL-8 in nine patients from whom serum was available. However, levels of proangiogenic factors vascular endothelial growth factor and basic foetal growth factor were not consistently affected. This study demonstrates the safety, tolerability and suggests the clinical activity of CC-5013 in the treatment of refractory malignant melanoma. Furthermore, this is the first report demonstrating T-cell stimulatory activity of this class of compound in patients with advanced cancer.

Published

2004