Your search keyword '"Glen Clack"' showing total 50 results

1. Abstract PS13-05: A phase 2 study of oral paclitaxel and encequidar (oPac+E) in the treatment of cutnaeous angiosarcoma: The breast angiosarcoma subgroup

Author

Vinod Ravi, Michael Wagner, Tom Wei-Wu Chen, Herbert H Loong, Robert Mennel, Cheuh-Chuan Yen, Glen Clack, David Cutler, Rudolf Kwan, and Wing=Kai CHan

Subjects

Cancer Research, medicine.medical_specialty, Taxane, business.industry, Phases of clinical research, Neutropenia, medicine.disease, Gastroenterology, Breast cancer, Oncology, Tolerability, Internal medicine, medicine, Angiosarcoma, Progression-free survival, business, Progressive disease

Abstract

Background Cutaneous angiosarcomas are highly aggressive malignant tumors with poor prognosis. Currently there is no FDA-approved treatment. oPac+E is a combination of oral paclitaxel and a novel oral P-glycoprotein inhibitor, Encequidar. Materials and Methods: This is a phase-2 study evaluating the activity, safety and tolerability of oPac 205mg/m2 + E 12.9 mg once daily for 3 consecutive days weekly for patients with unresectable cutaneous angiosarcoma. Tumour response was evaluated every 6 weeks using RECIST and photography. Results: From Aug-2018 to May-2020, 7 of 26 enrolled patients (pts) had breast cutaneous angiosarcoma. All had previous breast cancer, mastectomy and radiotherapy and/or adjuvant chemotherapy, no prior taxane for angiosacoma and no metastatic disease. Median age was 66 yrs (range 49-76). Best objective response rates were: complete response (CR) 43% (3/7 pts), partial response (PR) 14% (1/7 pts), stable disease (SD) 43% (3/7 pts), progressive disease (PD) 0%. Furthermore, 3 pts (43%) who had inoperable lesions were deemed operable after Oraxol treatment and received curative intent surgical resection. Median progression free survival (PFS) was 17 weeks. oPac+E was generally well tolerated. Grade-3 treatment related adverse events (AEs) occurred in 5 pts: diarrhea=1, fatigue=2, neutropenia =1, dyspnea=1, dehydration=1, pneumonitis=1. Grade-4 AE were neutropenia in 2 pts. Grade-2 paraesthesia=1. All pts fully recovered. Dose reductions were needed in 3 subjects. No patients discontinued treatment due to AEs. To date no patients died. Conclusions: oPac+E may provide an effective oral treatment for radiation-associated breast angiosarcoma, with a high clinical benefit rate (CR + PR+ SD=100%), durable response and enabled resection of unresectable tumors. It is generally well tolerated even in elderly patients; with low incidence of neuropathy. It may allow patients to avoid hospital IV chemotherapy visits and the option of home treatment. Citation Format: Vinod Ravi, Michael Wagner, Tom Wei-Wu Chen, Herbert H Loong, Robert Mennel, Cheuh-Chuan Yen, Glen Clack, David Cutler, Rudolf Kwan, Wing=Kai CHan. A phase 2 study of oral paclitaxel and encequidar (oPac+E) in the treatment of cutnaeous angiosarcoma: The breast angiosarcoma subgroup [abstract]. In: Proceedings of the 2020 San Antonio Breast Cancer Virtual Symposium; 2020 Dec 8-11; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2021;81(4 Suppl):Abstract nr PS13-05.

Published

2021

2. Ceralasertib (AZD6738), an Oral ATR Kinase Inhibitor, in Combination with Carboplatin in Patients with Advanced Solid Tumors: A Phase I Study

Author

Brunella Felicetti, Paul Frewer, Juanita Lopez, Anthony El-Khouiery, Glen Clack, Christine Stephens, Simon J. Hollingsworth, Matthew G Krebs, Alan Lau, Andrew Goldwin, Alienor Berges, Jean-Charles Soria, Gemma N Jones, Sophie Postel-Vinay, Itziar Irurzun-Arana, Emma Dean, Sy Amy Cheung, Timothy A. Yap, Andrew J. Pierce, and Simon Smith

Subjects

Cancer Research, medicine.medical_specialty, Indoles, Neutropenia, Maximum Tolerated Dose, Anemia, Morpholines, Ataxia Telangiectasia Mutated Proteins, Gastroenterology, Carboplatin, chemistry.chemical_compound, Pharmacokinetics, Internal medicine, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Adverse effect, Protein Kinase Inhibitors, Sulfonamides, Manchester Cancer Research Centre, business.industry, ResearchInstitutes_Networks_Beacons/mcrc, Nuclear Proteins, Common Terminology Criteria for Adverse Events, medicine.disease, Thrombocytopenia, Pyrimidines, Oncology, Tolerability, chemistry, Pharmacodynamics, Sulfoxides, business

Abstract

Purpose: This study reports the safety, tolerability, MTD, recommended phase II dose (RP2D), pharmacokinetic/pharmacodynamic profile, and preliminary antitumor activity of ceralasertib combined with carboplatin in patients with advanced solid tumors. It also examined exploratory predictive and pharmacodynamic biomarkers. Patients and Methods: Eligible patients (n = 36) received a fixed dose of carboplatin (AUC5) with escalating doses of ceralasertib (20 mg twice daily to 60 mg once daily) in 21-day cycles. Sequential and concurrent combination dosing schedules were assessed. Results: Two ceralasertib MTD dose schedules, 20 mg twice daily on days 4–13 and 40 mg once daily on days 1–2, were tolerated with carboplatin AUC5; the latter was declared the RP2D. The most common treatment-emergent adverse events (Common Terminology Criteria for Adverse Events grade ≥3) were anemia (39%), thrombocytopenia (36%), and neutropenia (25%). Dose-limiting toxicities of grade 4 thrombocytopenia (n = 2; including one grade 4 platelet count decreased) and a combination of grade 4 thrombocytopenia and grade 3 neutropenia occurred in 3 patients. Ceralasertib was quickly absorbed (tmax ∼1 hour), with a terminal plasma half-life of 8–11 hours. Upregulation of pRAD50, indicative of ataxia telangiectasia mutated (ATM) activation, was observed in tumor biopsies during ceralasertib treatment. Two patients with absent or low ATM or SLFN11 protein expression achieved confirmed RECIST v1.1 partial responses. Eighteen of 34 (53%) response-evaluable patients had RECIST v1.1 stable disease. Conclusions: The RP2D for ceralasertib plus carboplatin was established as ceralasertib 40 mg once daily on days 1–2 administered with carboplatin AUC5 every 3 weeks, with pharmacokinetic and pharmacodynamic studies confirming pharmacodynamic modulation and preliminary evidence of antitumor activity observed.

Published

2021

3. 265P Study of samuraciclib (CT7001), a first-in-class, oral, selective inhibitor of CDK7, in combination with fulvestrant in patients with advanced hormone receptor positive HER2 negative breast cancer (HR+BC)

Author

Sahirzeeshan Ali, E. Ainscow, Ash Bahl, Sagar Sardesai, Janine Mansi, H-T. Arkenau, M. Lehnert, P. Richards, Simon Lord, S. McIntosh, Glen Clack, R. C. Coombes, Sacha J Howell, Laura M. Kenny, Z. Mitri, Rinath Jeselsohn, Joyce O'Shaughnessy, Matthew G Krebs, Carlo Palmieri, and William J. Gradishar

Subjects

Oncology, medicine.medical_specialty, Fulvestrant, business.industry, HER2 negative, Hematology, medicine.disease, Breast cancer, Hormone receptor, Internal medicine, medicine, In patient, Cyclin-dependent kinase 7, business, medicine.drug

Published

2021

4. PATRIOT: A phase I study to assess the tolerability, safety and biological effects of a specific ataxia telangiectasia and Rad3-related (ATR) inhibitor (AZD6738) as a single agent and in combination with palliative radiation therapy in patients with solid tumours

Author

Martin Forster, Kabir Mohammed, Glen Clack, Clare Peckitt, Simon Smith, Kevin J. Harrington, James Spicer, Udai Banerji, Magnus T. Dillon, J. Guevara, Mark P Saunders, Z. Boylan, and D. Smith

Subjects

0301 basic medicine, Oncology, Drug, medicine.medical_specialty, Palliative Radiation Therapy, media_common.quotation_subject, medicine.medical_treatment, R895-920, DNA damage response, ATR inhibition, Article, Medical physics. Medical radiology. Nuclear medicine, 03 medical and health sciences, Phase I, 0302 clinical medicine, Internal medicine, medicine, Radiology, Nuclear Medicine and imaging, Single agent, RC254-282, Radiosensitization, media_common, business.industry, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Phase i study, Clinical trial, Radiation therapy, 030104 developmental biology, Tolerability, 030220 oncology & carcinogenesis, business, Ataxia telangiectasia and Rad3 related

Abstract

Highlights • Summary of a protocol for a phase I study combining the ATR inhibitor and palliative radiotherapy. • Study design is discussed. • Study aims and objectives, brief eligibility criteria, DLT criteria and dose escalation is discussed. • Brief summary of translational research to be carried out., PATRIOT is a phase I study of the ATR inhibitor, AZD6738, as monotherapy, and in combination with palliative radiotherapy. Here, we describe the protocol for this study, which opened in 2014 and is currently recruiting and comprises dose escalation of both drug and radiotherapy, and expansion cohorts.

Published

2018

5. 230MO First in human, modular study of samuraciclib (CT7001), a first-in-class, oral, selective inhibitor of CDK7, in patients with advanced solid malignancies

Author

Ash Bahl, Iain R. Macpherson, M. Lehnert, M. J. Fuchter, Glen Clack, Matthew G Krebs, Simon Lord, Agm Barrett, R. C. Coombes, S. McIntosh, Sahirzeeshan Ali, E. Ainscow, Paul A. Dickinson, Richard D. Baird, and Laura M. Kenny

Subjects

Oncology, Class (computer programming), medicine.medical_specialty, business.industry, Internal medicine, Medicine, In patient, Hematology, First in human, Modular design, business

Published

2021

6. Clinical pharmacology profile of an oral selective androgen receptor down-regulator, AZD3514: Implications on the design of ongoing castrate-resistant prostate cancer clinical studies

Author

Michael Dymond, Gareth James, Glen Clack, Angela W. Dymond, Simon Smith, Paul A. Dickinson, Masako Hirata, and Marc-Antoine Fabre

Subjects

Androgen receptor, Oncology, medicine.medical_specialty, Clinical pharmacology, law, business.industry, Internal medicine, Regulator, medicine, Castrate-resistant prostate cancer, General Medicine, business, law.invention

Published

2016

7. Systems Pharmacology Modeling of Prostate-Specific Antigen in Patients With Prostate Cancer Treated With an Androgen Receptor Antagonist and Down-Regulator

Author

Hitesh Mistry, Glen Clack, J. Young, Paul A. Dickinson, and M-A Fabre

Subjects

0301 basic medicine, education.field_of_study, business.industry, Population, Pharmacology, urologic and male genital diseases, medicine.disease, Androgen receptor, 03 medical and health sciences, Prostate cancer, Prostate-specific antigen, 030104 developmental biology, 0302 clinical medicine, Antigen, 030220 oncology & carcinogenesis, Modeling and Simulation, Dihydrotestosterone, LNCaP, Cancer research, Medicine, Pharmacology (medical), Androgen Receptor Antagonists, business, education, medicine.drug

Abstract

First-in-human (FIH) studies with AZD3514, a selective androgen receptor (AR) down-regulator, showed decreases of >30% in the prostate-specific antigen (PSA) in some patients. A modeling approach was adopted to understand these observations and define the optimum clinical use hypothesis for AZD3514 for clinical testing. Initial empirical modeling showed that only baseline PSA correlated significantly with this biological response, whereas drug concentration did not. To identify the mechanistic cause of this observation, a mechanism-based model was first developed, which described the effects of AZD3514 on AR protein and PSA mRNA levels in LNCaP cells with and without dihydrotestosterone (DHT). Second, the mechanism-based model was linked to a population pharmacokinetic (PK) model; PSA effects of clinical doses were subsequently simulated under different clinical conditions. This model was used to adjust the design of the ongoing clinical FIH study and direct the backup program.

Published

2016

8. A phase II study of oraxol in the treatment of unresectable cutaneous angiosarcoma

Author

Chueh-Chuan Yen, Tom Wei-Wu Chen, Glen Clack, David M. Cutler, Min-Fun Rudolf Kwan, Wing Kai Chan, Vinod Ravi, Herbert H. Loong, Robert G. Mennel, and Michael R. Wagner

Subjects

Oncology, Cancer Research, Poor prognosis, medicine.medical_specialty, business.industry, Phases of clinical research, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Paclitaxel, chemistry, 030220 oncology & carcinogenesis, Internal medicine, medicine, Angiosarcoma, business, 030215 immunology

Abstract

11517 Background: Oraxol is a combination of oral paclitaxel and a novel oral P-glycoprotein inhibitor, HM30181A. Cutaneous angiosarcomas are highly aggressive malignant tumors with poor prognosis. Currently there is no FDA-approved treatment. Methods: This is an open label study evaluating the activity, safety and tolerability of Oraxol 205mg/m2 administered orally, once daily, for 3 consecutive days per week. Planned treatment is for 25 weeks. Subjects included in this study had not received prior therapy with a taxane and did not have metastatic disease. Tumour response was evaluated at 6 weekly intervals using RECIST and photography. A Simon two stage design was used. Results: 18 of 24 enrolled patients (pts); male/female 11/7; median age 77 years (range 56-93), were evaluable at time of analysis. Subjects were recruited during an 18 month period, from Aug-2018 to Jan-2020. Best objective response rates were: CR 22% (n = 4), PR 11% (n = 2), SD 67% (n = 12), PD 0%. 42% of pts with SD had durability > 13 weeks (range 13-25). Median PFS was 38 weeks. All pts remain alive at time of reporting. Furthermore, 5 pts (28%) who had inoperable lesions were deemed operable after Oraxol and received surgical resection. Oraxol was generally well tolerated. Most common adverse events (AEs) G>3 were: diarrhea (n = 1), fatigue (n = 3), neutropenia (n = 9), leucopenia (n = 5), lymphopenia (n = 5). Serious AEs were G3 pneumonia in 2 subjects and G4 neutropenia in 2 subjects, one of which was febrile. All events fully resolved. Neuropathy was uncommon: n = 2 (G1 = 1 @ day 10, G2 = 1 @ day 64). Dose reductions were recorded in 7 subjects. 2 subjects discontinued treatment due to AEs; both asymptomatic pneumonitis seen on CT, which recovered after discontinuation. Following the initial positive results, the protocol has been amended to change the maximum recruitment of subjects from 25 to 43. Conclusions: Oraxol provides an orally administered treatment option for angiosarcoma, with a high and durable clinical benefit rate (CR + PR+ long SD). It is generally well tolerated even in an older patient population; particularly with respect to the the low incidence of neuropathy compared to IV paclitaxel. Recruitment is ongoing. Clinical trial information: NCT03544567 . [Table: see text]

Published

2020

9. Modular phase I/II clinical trial evaluating the selective MET-kinase inhibitor OMO-1 in patients with advanced malignancies: Safety and proof of mechanism

Author

Timothy Perera, Eric Angevin, Martin Forster, Glen Clack, Martijn P. Lolkema, Matthew G Krebs, Sarah P. Blagden, Elizabeth Ruth Plummer, Marc Tjwa, Filip de Vos, Ellen Jansen, Annegret Van der Aa, Eric Ciamporcero, Marion Libouban, and Ann Meulemans

Subjects

Cancer Research, Kinase, business.industry, Mechanism (biology), Cancer, medicine.disease, Clinical trial, Phase i ii, Oncology, medicine, Cancer research, In patient, Treatment resistance, business

Abstract

3062 Background: MET kinase is a therapeutic target in a range of cancer indications; it is a primary oncogenic driver and a mechanism of therapy resistance. OMO-1 is a highly potent, selective oral inhibitor of MET kinase and Organic Cation Transporter 2 (OCT2). Methods: This study assesses the safety, tolerability, pharmacokinetics (PK) and preliminary activity of OMO-1 in patients (pts) with advanced malignancies (NCT03138083). Module 1 data, evaluating ascending doses of OMO-1 monotherapy, are reported here. Results: As of January 16, 2019, 34 pts were enrolled at 5 twice-daily (BD) dose levels of OMO-1: 100, 200, 250, 350, and 400 mg, including 10 with MET gene amplified or mutated tumours. OMO-1 was generally well tolerated between 100 - 250 mg BD; pts were in the study for an average of 94 days (range: 15-291 days) and 20/34 pts discontinued due to disease progression. Most frequently-reported AEs were nausea (17/34), vomiting (14/34) and fatigue (14/34), mainly G1-2. Notably, no peripheral oedema, cardiovascular events or non-malignancy related LFT abnormalities were observed. A total of 36 SAEs were reported: 17 in 11 subjects were considered related to OMO-1, and included nausea (3/17), vomiting (4/17), chills, diarrhoea, influenza-like illness (2/17), increased blood bilirubin, blood creatinine (3/17) and neutrophil count, and sepsis. A dose of 250 mg BD was determined as the recommended Phase 2 dose (RP2D); doses ≥350mg BD were not in keeping with optimum long-term dosing: at 400 mg BD, 2/3 subjects experienced influenza-like illness (G2 and G3) and at 350 mg BD 2/5 subjects had G2 fatigue and nausea/vomiting. OMO-1 has a half-life of 2.5-3 hrs and plasma exposure is dose-proportional without accumulation. Elevated creatinine was observed across all dose levels, consistent with OCT2 inhibition. IHC analysis on paired tumour biopsies from a MET-mutated NSCLC pt dosed at 200 mg BD showed near-complete inhibition of phosphorylated MET, without affecting total MET. Conclusions: OMO-1 has a favourable safety profile at a RP2D of 250mg BD. Expansion cohorts for MET mutated/amplified tumour types are enrolling. Clinical trial information: NCT03138083.

Published

2019

10. Differentiated pharmacokinetic and pharmacodynamic properties of a highly selective MET kinase inhibitor, OMO-1: Implications for efficacy and safety

Author

Marc Tjwa, Annegret Van der Aa, Glen Clack, Timothy Perera, Martijn P. Lolkema, Ann Meulemans, Marion Libouban, Eric Ciamporcero, and Ellen Jansen

Subjects

Cancer Research, Oncology, Pharmacokinetics, Kinase, business.industry, Pharmacodynamics, medicine, Cancer, Treatment resistance, Pharmacology, medicine.disease, business, Highly selective

Abstract

e14674 Background: The MET kinase is an established therapeutic target in a range of cancer indications, being a primary oncogenic and therapy resistance driver. Methods: OMO-1 is a highly potent, selective oral inhibitor of MET kinase and Organic Cation Transporter 2 (OCT2) that is currently being explored in a Phase I/II study (NCT03138083). Results: Pre-clinical data for OMO-1 indicates that anti-tumor efficacy against MET driven tumor models does not require 24/7 exposure in the plasma. PK/PD assessments indicate that OMO-1 efficacy is AUC driven. Exposures above a trough concentration of ~600ng/ml for a period of 6-8hr and an AUC of 3000ng.h/ml result in complete target inhibition sufficient to induce regression or stasis of MET driven in-vivo models. Dosing of OMO-1 at 12.5mg/kg BD 4hr apart, or split over 4 doses 2hr apart, with a dosing-free period of 18-20hr was sufficient to obtain the effects preclinically. The ongoing Phase I/II study in patients with solid tumours utilised learnings from the pre-clinical and FIH study (NCT01964872) where ascending single doses and multiple doses were evaluated. The selected starting dose for the patient study (100mg BD, 4 hr apart) achieved exposures above the predicted MBAD. Paired tumor biopsies were obtained from a higher dose level (200mg BD). A MET exon 14 skipping mutation NSCLC patient at this dosed demonstrated near-complete inhibition of phospho MET accompanied by signs of clinical benefit and lesion shrinkage, thereby matching the preclinical data. Certain ‘class effect’ adverse events, such as edema, were not observed. Conclusions: OMO-1 is an oral, potent MET TKI with a novel dosing regime, identified during preclinical optimization (BD 4hr apart), that demonstrates encouraging signs of clinical activity without certain ‘class-specific’ adverse events. Further evaluation of this differentiated and efficacious agent is warranted and ongoing.

Published

2019

11. Biomarker Utility of Circulating Tumor Cells in Metastatic Cutaneous Melanoma

Author

Jeffrey Cummings, Raffaele Califano, Andrew Hughes, Caroline Dive, Jessica Booth, Glen Clack, Leila Khoja, Paul Lorigan, Matthew Lancashire, and Cong Zhou

Subjects

Adult, Male, Oncology, medicine.medical_specialty, Pathology, Skin Neoplasms, Dermatology, Biochemistry, Circulating tumor cell, Predictive Value of Tests, Internal medicine, Biomarkers, Tumor, Prevalence, medicine, Humans, Melanoma, neoplasms, Molecular Biology, Aged, Proportional Hazards Models, Aged, 80 and over, Univariate analysis, business.industry, Proportional hazards model, Incidence, Incidence (epidemiology), Hazard ratio, Cell Biology, Middle Aged, Neoplastic Cells, Circulating, Prognosis, medicine.disease, Predictive value of tests, Multivariate Analysis, Biomarker (medicine), Female, Reagent Kits, Diagnostic, Drug Monitoring, business

Abstract

The incidence of melanoma is increasing worldwide. Advances in targeted agents and immunotherapy have improved outcomes in metastatic disease, but biomarkers are required to optimize treatment. We determined the prevalence of circulating tumor cells (CTCs) and explored their utility as prognostic and pharmacodynamic biomarkers. A total of 101 patients with metastatic cutaneous melanoma were recruited prospectively. CTC number was determined using the CellSearch platform and melanoma kits in samples taken at baseline and serially during treatment. CTC numbers ranged between 0 and 36 per 7.5 ml blood; 26% of patients had ≥ 2 CTCs. Baseline CTC number was prognostic for median overall survival (OS) in univariate analysis (2.6 vs. 7.2 months (P

Published

2013

12. Continual reassessment method for dose escalation clinical trials in oncology:A comparison of prior skeleton approaches using AZD3514 data

Author

Julia Young, Glen Clack, Gareth James, Stefan Symeonides, and Jayne Marshall

Subjects

Oncology, Male, medicine.medical_specialty, Cancer Research, Maximum Tolerated Dose, Phases of clinical research, Antineoplastic Agents, Phase 1, 01 natural sciences, Bayesian, Continual reassessment method, 010104 statistics & probability, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Dose escalation, Genetics, Humans, Computer Simulation, 0101 mathematics, Skeleton, Clinical Trials, Phase I as Topic, Dose-Response Relationship, Drug, business.industry, Androgen Antagonists, Bayes Theorem, Models, Theoretical, Skeleton (computer programming), Clinical trial, Pyridazines, Prostatic Neoplasms, Castration-Resistant, 030220 oncology & carcinogenesis, Maximum tolerated dose, business, Algorithms, Research Article

Abstract

Background The continual reassessment method (CRM) requires an underlying model of the dose-toxicity relationship (“prior skeleton”) and there is limited guidance of what this should be when little is known about this association. In this manuscript the impact of applying the CRM with different prior skeleton approaches and the 3 + 3 method are compared in terms of ability to determine the true maximum tolerated dose (MTD) and number of patients allocated to sub-optimal and toxic doses. Methods Post-hoc dose-escalation analyses on real-life clinical trial data on an early oncology compound (AZD3514), using the 3 + 3 method and CRM using six different prior skeleton approaches. Results All methods correctly identified the true MTD. The 3 + 3 method allocated six patients to both sub-optimal and toxic doses. All CRM approaches allocated four patients to sub-optimal doses. No patients were allocated to toxic doses from sigmoidal, two from conservative and five from other approaches. Conclusions Prior skeletons for the CRM for phase 1 clinical trials are proposed in this manuscript and applied to a real clinical trial dataset. Highly accurate initial skeleton estimates may not be essential to determine the true MTD, and, as expected, all CRM methods out-performed the 3 + 3 method. There were differences in performance between skeletons. The choice of skeleton should depend on whether minimizing the number of patients allocated to suboptimal or toxic doses is more important. Trial registration NCT01162395, Trial date of first registration: July 13, 2010. Electronic supplementary material The online version of this article (doi:10.1186/s12885-016-2702-6) contains supplementary material, which is available to authorized users.

Published

2016

13. Lipid profiles within the SABRE trial of anastrozole with and without risedronate

Author

Catherine Van Poznak, David H. Barlow, Glen Clack, Richard Eastell, and Andreas Makris

Subjects

Adult, Cancer Research, medicine.medical_specialty, Antineoplastic Agents, Hormonal, Population, Anastrozole, Breast Neoplasms, Gastroenterology, Article, chemistry.chemical_compound, Breast cancer, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, Nitriles, medicine, Humans, education, Triglycerides, Aged, education.field_of_study, Intention-to-treat analysis, Bone Density Conservation Agents, medicine.diagnostic_test, Cholesterol, business.industry, Cholesterol, HDL, Etidronic Acid, Cholesterol, LDL, Middle Aged, Triazoles, medicine.disease, Lipids, Risedronate Sodium, Treatment Outcome, Endocrinology, Oncology, chemistry, Risedronic acid, Female, lipids (amino acids, peptides, and proteins), business, Lipid profile, Risedronic Acid, medicine.drug

Abstract

Lipid profiles in women with early breast cancer receiving anastrozole with or without risedronate were examined within an international Phase III/IV study to assess for possible treatment related changes. Postmenopausal women with hormone receptor-positive breast cancer were assigned to 1 of 3 strata by risk of fragility fracture. Patients with the highest risk for fracture received anastrozole plus risedronate (A + R). Moderate-risk patients were randomized in a double-blind manner to A + R or anastrozole and placebo (A + P). Lower-risk patients received anastrozole (A) alone. Serial fasting blood samples were assessed for changes in lipid parameters relative to baseline after 12 months of treatment with anastrozole with or without risedronate. Samples were centrally analyzed for low-density lipoprotein cholesterol (LDL-cholesterol), high-density lipoprotein (HDL) cholesterol, total cholesterol (TC) and triglycerides (TG). Analysis was performed as primary analysis population for lipids (A plus A + P), lipid intention to treat population and secondary population (A + R). Of the 119 patients treated with A plus A + P, there were 66 patients eligible for inclusion in the primary analysis population. Of the 115 patients treated with secondary population (A + R) there were 65 patients eligible for lipid profiling. For LDL-cholesterol, HDL-cholesterol, TC and TG there were no significant changes between the baseline and 12 months assessments to suggest that any of these therapies have a negative impact on the lipid profile. In this study of postmenopausal women with early breast cancer receiving adjuvant anastrozole with or without risedronate, there was no adverse effect on LDL-cholesterol, HDL-cholesterol, TC or TG values over the 12 months monitoring period.

Published

2012

14. Effects of Src kinase inhibition by saracatinib (AZD0530) on bone turnover in advanced malignancy in a Phase I study

Author

Fatma Gossiel, Glen Clack, José Baselga, Renee Iacona, Richard Eastell, Martin Rimmer, Richard D. Finkelman, and Rosemary A. Hannon

Subjects

Adult, Male, medicine.medical_specialty, Histology, Bone disease, Physiology, Endocrinology, Diabetes and Metabolism, Gastroenterology, Bone resorption, Bone remodeling, Young Adult, chemistry.chemical_compound, N-terminal telopeptide, Osteoclast, Neoplasms, Internal medicine, Biomarkers, Tumor, medicine, Humans, Benzodioxoles, Protein Kinase Inhibitors, Aged, Creatinine, Dose-Response Relationship, Drug, business.industry, Middle Aged, medicine.disease, Dose–response relationship, src-Family Kinases, medicine.anatomical_structure, Endocrinology, chemistry, Quinazolines, Female, Bone Remodeling, business, Type I collagen

Abstract

Saracatinib (AZD0530) is an orally active once-daily Src kinase inhibitor which modulates key signaling pathways in cancer cells. In a Phase I study in patients with advanced solid malignancies resistant to standard treatment we assessed the effect of saracatinib on bone turnover. Fifty-one patients were randomized into three parallel groups to receive saracatinib 50, 125 or 175 mg/day. After a single dose followed by a 7-day washout, patients received once-daily doses for 21 days. Bone turnover markers were measured in serum and urine samples collected before dosing on days 1, 2, 3, 17 and 28. Samples were available at baseline and more than one other time point for 44 patients. Bone resorption markers were significantly decreased by saracatinib. Serum cross-linked C-terminal telopeptide of type I collagen (sCTX) changed in the 50, 125 and 175 mg/day groups by -36% (95% CI -58, -4), -64% (95% CI -75, -48) and -75% (95% CI -83, -61), respectively, at day 28. Urinary cross-linked N-terminal telopeptide of type I collagen/creatinine ratio (uNTX/Cr) changed in the 50, 125 and 175 mg/day groups by; -13% (95% CI -33, 13), -48% (95% CI -59, -34) and -50% (95% CI -62, -35), respectively, at day 28. The significant decreases in bone resorption markers indicate that suppression of Src kinase inhibits osteoclast activity in patients with advanced cancer. This result suggests that saracatinib may have therapeutic benefit in metastatic bone disease.

Published

2012

15. Analysis of Circulating Tumor Cells in Patients with Non-small Cell Lung Cancer Using Epithelial Marker-Dependent and -Independent Approaches

Author

Daisuke Nonaka, Robert Sloane, Jian-Mei Hou, Lee Lancashire, Fiona H Blackhall, Lynsey Priest, Glen Clack, Andrew Hughes, Caroline Dive, Alison Backen, Timothy H Ward, Matthew G Krebs, and Malcolm R Ranson

Subjects

Male, Pulmonary and Respiratory Medicine, Pathology, medicine.medical_specialty, Lung Neoplasms, Cell Separation, Adenocarcinoma, Metastasis, chemistry.chemical_compound, Circulating tumor cell, Non-small cell lung cancer, Carcinoma, Non-Small-Cell Lung, ISET, medicine, Carcinoma, Biomarkers, Tumor, Humans, Proliferation Marker, Epithelial–mesenchymal transition, Prospective Studies, Lung cancer, Aged, Cell Proliferation, CellSearch, business.industry, Circulating tumor cells, Epithelial cell adhesion molecule, Epithelial Cells, Adenocarcinoma, Bronchiolo-Alveolar, Middle Aged, medicine.disease, Neoplastic Cells, Circulating, Prognosis, chemistry, Oncology, Carcinoma, Squamous Cell, Female, business

Abstract

Introduction: Epithelial circulating tumor cells (CTCs) are detectable in patients with non-small cell lung cancer (NSCLC). However, epithelial to mesenchymal transition, a widely reported prerequisite for metastasis, may lead to an underestimation of CTC number. We compared directly an epithelial marker-dependent (CellSearch) and a marker-independent (isolation by size of epithelial tumor cells [ISET]) technology platform for the ability to identify CTCs. Molecular characteristics of CTCs were also explored. Methods: Paired peripheral blood samples were collected from 40 chemonaive, stages IIIA to IV NSCLC patients. CTCs were enumerated by Epithelial Cell Adhesion Molecule-based immunomagnetic capture (CellSearch, Veridex) and by filtration (ISET, RareCell Diagnostics). CTCs isolated by filtration were assessed by immunohistochemistry for epithelial marker expression (cytokeratins, Epithelial Cell Adhesion Molecule, epidermal growth factor receptor) and for proliferation status (Ki67). Results: CTCs were detected using ISET in 32 of 40 (80%) patients compared with 9 of 40 (23%) patients using CellSearch. A subpopulation of CTCs isolated by ISET did not express epithelial markers. Circulating tumor microemboli (CTM, clusters of ≥3 CTCs) were observed in 43% patients using ISET but were undetectable by CellSearch. Up to 62% of single CTCs were positive for the proliferation marker Ki67, whereas cells within CTM were nonproliferative. Conclusions: Both technology platforms detected NSCLC CTCs. ISET detected higher numbers of CTCs including epithelial marker negative tumor cells. ISET also isolated CTM and permitted molecular characterization. Combined with our previous CellSearch data confirming CTC number as an independent prognostic biomarker for NSCLC, we propose that this complementary dual technology approach to CTC analysis allows more complete exploration of CTCs in patients with NSCLC.

Published

2012

16. Identification of an RNF43 mutated gastric cancer patient population with potential sensitivity to porcupine inhibitor RXC004 and development of a complimentary ctDNA liquid biopsy assay for patient screening

Author

R. Armer, Caroline Phillips, J. Bradford, S. Woodcock, B. Thompson, A. Thomason, Glen Clack, B. Chaffey, Inder Bhamra, L. Little, H. McKeever, and M. Bingham

Subjects

Pathology, medicine.medical_specialty, biology, medicine.diagnostic_test, business.industry, Patient screening, Cancer, Hematology, medicine.disease, Patient population, Oncology, biology.animal, Biopsy, Cancer research, Medicine, Liquid biopsy, business, Porcupine

Published

2017

17. Evaluation and Prognostic Significance of Circulating Tumor Cells in Patients With Non–Small-Cell Lung Cancer

Author

Roberta Ferraldeschi, Lee Lancashire, Lynsey Priest, Timothy H Ward, Alastair Greystoke, Fiona H Blackhall, Jian-Mei Hou, Matthew G Krebs, Glen Clack, Andrew Hughes, Caroline Dive, Malcolm R Ranson, and Robert Sloane

Subjects

Adult, Male, Oncology, Cancer Research, medicine.medical_specialty, Pathology, Lung Neoplasms, Time Factors, medicine.medical_treatment, Kaplan-Meier Estimate, Risk Assessment, Disease-Free Survival, chemistry.chemical_compound, Circulating tumor cell, Predictive Value of Tests, Risk Factors, Carcinoma, Non-Small-Cell Lung, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, Biomarkers, Tumor, Carcinoma, medicine, Humans, Prospective Studies, Stage (cooking), Lung cancer, Prospective cohort study, Aged, Neoplasm Staging, Proportional Hazards Models, Aged, 80 and over, Chemotherapy, Immunomagnetic Separation, business.industry, Cancer, Epithelial cell adhesion molecule, Middle Aged, Neoplastic Cells, Circulating, medicine.disease, Treatment Outcome, England, chemistry, Female, business, Cell Adhesion Molecules

Abstract

Purpose Lung cancer is the leading cause of cancer-related death worldwide. Non–small-cell lung cancer (NSCLC) lacks validated biomarkers to predict treatment response. This study investigated whether circulating tumor cells (CTCs) are detectable in patients with NSCLC and what their ability might be to provide prognostic information and/or early indication of patient response to conventional therapy. Patients and Methods In this single-center prospective study, blood samples for CTC analysis were obtained from 101 patients with previously untreated, stage III or IV NSCLC both before and after administration of one cycle of standard chemotherapy. CTCs were measured using a semiautomated, epithelial cell adhesion molecule–based immunomagnetic technique. Results The number of CTCs in 7.5 mL of blood was higher in patients with stage IV NSCLC (n = 60; range, 0 to 146) compared with patients with stage IIIB (n = 27; range, 0 to 3) or IIIA disease (n = 14; no CTCs detected). In univariate analysis, progression-free survival was 6.8 v 2.4 months with P < .001, and overall survival (OS) was 8.1 v 4.3 months with P < .001 for patients with fewer than five CTCs compared with five or more CTCs before chemotherapy, respectively. In multivariate analysis, CTC number was the strongest predictor of OS (hazard ratio [HR], 7.92; 95% CI, 2.85 to 22.01; P < .001), and the point estimate of the HR was increased with incorporation of a second CTC sample that was taken after one cycle of chemotherapy (HR, 15.65; 95% CI, 3.63 to 67.53; P < .001). Conclusion CTCs are detectable in patients with stage IV NSCLC and are a novel prognostic factor for this disease. Further validation is warranted before routine clinical application.

Published

2011

18. Long-term effects of anastrozole on bone mineral density: 7-year results from the ATAC trial

Author

John R. Mackey, Anthony Howell, Glen Clack, Richard Eastell, Matthias W. Beckmann, Robert E. Coleman, Jack Cuzick, and Judith E. Adams

Subjects

musculoskeletal diseases, medicine.medical_specialty, Antineoplastic Agents, Hormonal, medicine.drug_class, Urology, Anastrozole, Breast Neoplasms, Lumbar vertebrae, Bone resorption, Time, Bone Density, Nitriles, Humans, Medicine, Bone Resorption, Bone mineral, Hip, Lumbar Vertebrae, Aromatase inhibitor, business.industry, Hematology, Triazoles, musculoskeletal system, medicine.disease, Surgery, Osteopenia, Tamoxifen, medicine.anatomical_structure, Oncology, Selective estrogen receptor modulator, Female, business, medicine.drug

Abstract

Background This ‘Arimidex’, Tamoxifen, Alone or in Combination (ATAC) trial sub-study examined the effects of anastrozole and tamoxifen on bone mineral density (BMD) following 5 years of treatment. Patients and methods Lumbar spine and total hip BMD were assessed at years 6 and 7 in a total of 71 eligible patients. In total, 50 patients had evaluable data. Results Following anastrozole treatment, the lumbar spine median BMD increased by 2.35% (P = 0.04) and 4.02% (P = 0.0004) at years 6 and 7, while total hip median BMD increased by 0.71% (P = 0.3) and 0.5% (P = 0.8). After tamoxifen treatment, lumbar spine median BMD decreased by 0.79% (P = 0.2) and 0.30% (P = 0.9) at years 6 and 7, while total hip median BMD decreased by 2.09% (P = 0.0003) and 2.52% (P = 0.0002). Patients with a normal BMD or who were osteopenic at 5 years did not become osteoporotic. Conclusions Anastrozole treatment-related bone loss did not continue into the off-treatment follow-up period. The recovery in lumbar spine BMD and absence of further loss at the hip is consistent with the reduction in the annual rate of fracture observed after treatment cessation in the main ATAC trial.

Published

2011

19. Circulating Tumor Cells as a Window on Metastasis Biology in Lung Cancer

Author

Matthew G Krebs, Fiona H Blackhall, Robert Sloane, Glen Clack, Malcolm R Ranson, Lynsey Priest, Timothy H Ward, Jian-Mei Hou, Andrew Hughes, and Caroline Dive

Subjects

Male, Pathology, medicine.medical_specialty, Lung Neoplasms, Cell Survival, Short Communication, Vimentin, Pathology and Forensic Medicine, Metastasis, Mesoderm, Circulating tumor cell, Biomarkers, Tumor, medicine, Humans, Neoplasm Metastasis, Lung cancer, Aged, biology, business.industry, Cancer, Epithelial Cells, Cell migration, Anatomical pathology, Middle Aged, Neoplastic Cells, Circulating, medicine.disease, Apoptosis, biology.protein, Female, business

Abstract

Circulating tumor cell (CTC) number in metastatic cancer patients yields prognostic information consistent with enhanced cell migration and invasion via loss of adhesion, a feature of epithelial-to-mesenchymal transition (EMT). Tumor cells also invade via collective migration with maintained cell-cell contacts and consistent with this is the circulating tumor microemboli (CTM; contiguous groups of tumor cells) that are observed in metastatic cancer patients. Using a blood filtration approach, we examined markers of EMT (cytokeratins, E-cadherin, vimentin, neural cadherin) and prevalence of apoptosis in CTCs and CTM to explore likely mechanism(s) of invasion in lung cancer patients and address the hypothesis that cells within CTM have a survival advantage. Intra-patient and inter-patient heterogeneity was observed for EMT markers in CTCs and CTM. Vimentin was only expressed in some CTCs, but in the majority of cells within CTM; E-cadherin expression was lost, cytoplasmic or nuclear, and rarely expressed at the surface of the cells within CTM. A subpopulation of CTCs was apoptotic, but apoptosis was absent within CTM. This pilot study suggests that EMT is not prosecuted homogeneously in tumor cells within the circulation of lung cancer patients and that collective migration and enhanced survival of cells within CTM might contribute to lung cancer metastasis. Multiplex analysis and further detailed exploration of metastatic potential and EMT in CTCs/CTM is now warranted in a larger patient cohort.

Published

2011

20. Current status and future potential of somatic mutation testing from circulating free DNA in patients with solid tumours

Author

Malcolm R Ranson, Timothy H Ward, Glen Clack, Caroline Dive, William G. Newman, A. Hughes, Ruth E Board, Gillian Ellison, Kyaw Aung, and Emma Donald

Subjects

Somatic cell, business.industry, Robustness (evolution), Review, Bioinformatics, DNA sequencing, Human genetics, Germline mutation, Cell-free fetal DNA, Genetics, Mutation testing, Medicine, Genetics(clinical), Personalized medicine, business, Genetics (clinical)

Abstract

Genetic alterations can determine the natural history of cancer and its treatment response. With further advances in DNA sequencing technology, multiple novel genetic alterations will be discovered which could be exploited as prognostic, predictive and pharmacodynamic biomarkers in the development and use of cancer therapeutics. As such, the importance in clinical practice of efficient and robust somatic mutation testing in solid tumours cannot be overemphasized in the current era of personalized medicine. However, significant challenges remain regarding the testing of genetic biomarkers in clinical practice. Reliance on archived formalin fixed, paraffin embedded tumour, obtained from diagnostic biopsies, for testing somatic genetic alterations could restrict the scientific community in asking relevant questions about a patient’s cancer biology. Problems inherent with using formalin fixed, archival tissue are well recognized and difficult to resolve. It could be argued that to achieve rapid and efficient incorporation of genetic biomarkers into clinical practice, somatic mutation testing in cancer patients should be simpler, less invasive using a readily available clinical sample, whilst maintaining robustness and reproducibility. In this regard, use of circulating free DNA (cfDNA) from plasma or serum as an alternative and/or additional source of DNA to test cancer specific genetic alterations is an attractive proposition. In light of encouraging results from recent studies, this mini review will discuss the current role and future potential of somatic mutation testing from circulating or cell free DNA derived from the blood of patients with solid tumours.

Published

2010

21. Abstract 4791: OMO-1, a potent, highly selective, orally bioavailable, MET kinase inhibitor with a favorable preclinical toxicity profile, shows both monotherapy activity, against MET pathway-driven tumors, and EGFR TKI combination activity in acquired resistance models

Author

Timothy Perera, Tinne Verhulst, Boudewijn Janssens, Glen Clack, Marion Libouban, Eleonora Jovcehva, Souichi Ogata, Berthold Wroblowski, Desiree De Lange, Laurence Anne Mevellec, and Tianbao Lu

Subjects

Cancer Research, Kinase, business.industry, medicine.medical_treatment, Cancer, Tumor initiation, medicine.disease, Targeted therapy, Metastasis, Oncology, medicine, Cancer research, Erlotinib, business, IC50, medicine.drug, EGFR inhibitors

Abstract

Activation of the MET/HGF pathway has been linked to tumor initiation, metastasis, angiogenesis and resistance to therapeutic agents. Here we present pharmacological characterization of OMO-1 (formerly JNJ-38877618), a potent, highly selective, orally bioavailable MET kinase inhibitor with nM binding affinity (Kd=1.4 nM) and enzyme inhibitory activity against wt and M1268T mutant MET (2 and 3 nM IC50). MET inhibitory effects were assessed in proliferation, colony formation and motility assays. OMO-1 displayed nM potency against MET Ampl/mutant and therapy resistant models. In vivo, OMO-1 induced complete inhibition of tumor growth in 3 models: the SNU5 MET amp gastric, U87-MG HGF autocrine glioblastoma and Hs746T MET exon 14 skipping mutant gastric cancer. OMO-1 induced regression of large MET amplified EBC-1 SqNSCLC where OMO-1 led to dose- and time-dependent inhibition of MET kinase activation, with the duration of target shut down considerably exceeding plasma exposure times. Combination treatments were well tolerated and improved EGFR targeted therapy. Although single agent OMO-1 had no effect on NSCLC HCC827 EGFR, combination with Erlotinib led to delayed onset of tumor recurrence. The acquired EGFR inhibitor resistant model HCC827-ER1 was determined to be MET amplified. OMO-1 and erlotinib both inhibited tumor growth of this model whilst combination induced tumor regression. In an EGFR inhibitor resistant PDX having MET amplification, single agent OMO-1 caused tumour stasis whereas MetMab/erlotinib only led to tumor growth delay. The potent preclinical activity we have observed, supports ongoing clinical development of OMO-1 in patients with MET pathway-driven tumors. Citation Format: Marion Libouban, Eleonora Jovcehva, Desiree De Lange, Boudewijn Janssens, Tinne Verhulst, Souichi Ogata, Berthold Wroblowski, Laurence Mevellec, Tianbao Lu, Glen Clack, Timothy Perera. OMO-1, a potent, highly selective, orally bioavailable, MET kinase inhibitor with a favorable preclinical toxicity profile, shows both monotherapy activity, against MET pathway-driven tumors, and EGFR TKI combination activity in acquired resistance models [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 4791.

Published

2018

22. A modular, multi-arm, multi-part, first time in patient study to evaluate the safety and tolerability of the dual MET kinase/OCT2 inhibitor, OMO-1, alone and in combination with anti-cancer treatments, in patients with locally advanced, unresectable or metastatic solid malignancies

Author

Matthew G Krebs, Rebecca Kristeleit, Filip de Vos, Martin Forster, Joachim G.J.V. Aerts, Shankar Balaratnam, Ann Meulemans, Prashanth Hari Dass, Nadina Tinsley, Sarah P. Blagden, Martijn P. Lolkema, Marion Libouban, Tim Perera, Elizabeth Ruth Plummer, Glen Clack, Eric Angevin, and Yvette Drew

Subjects

Oncology, Cancer Research, medicine.medical_specialty, business.industry, Kinase, Locally advanced, Cancer, Highly selective, medicine.disease, Tolerability, In vivo, Internal medicine, medicine, Single agent, In patient, business

Abstract

TPS2614Background: OMO-1, a highly selective, oral, small molecule MET kinase/OCT2 inhibitor, demonstrated single agent cellular and in vivo anti-tumour activity, including regression in MET driven...

Published

2018

23. Biomarkers in oncology drug development

Author

Robin D. Whittaker, Glen Clack, Dereck Amakye, Darren Hodgson, and Athula Herath

Subjects

Drug, Cancer Research, medicine.medical_specialty, Drug Industry, business.industry, Chemistry, Pharmaceutical, media_common.quotation_subject, Reviews, General Medicine, Pharmacology, Patient population, Oncology, Drug Design, Genetics, Animals, Humans, Molecular Medicine, Medicine, Oncology drug, Biomarker (medicine), Medical physics, business, Biomarkers, media_common

Abstract

Biomarker measurements have become an essential component of oncology drug development, particularly so in this era of targeted therapies. Such measurements ensure that clinical studies are testing our biological hypotheses and can help make the difficult decisions required to choose which drugs to stop developing or de-prioritise. For those drugs taken forward, biomarker measurements may also help choose the appropriate dose, schedule and patient population. In this review we discuss the intrinsic properties of biological sample based efficacy measurements and how these relate to their implementation in oncology drug development by way of points to consider and examples.

Published

2008

24. Effect of Anastrozole on Bone Mineral Density: 5-Year Results From the Anastrozole, Tamoxifen, Alone or in Combination Trial 18233230

Author

Judith E. Adams, Anthony Howell, Matthias W. Beckmann, Glen Clack, John R. Mackey, Richard Eastell, Jack Cuzick, Rosemary A. Hannon, and Robert E. Coleman

Subjects

musculoskeletal diseases, Cancer Research, medicine.medical_specialty, medicine.drug_class, Urology, Anastrozole, Breast Neoplasms, Bone Density, Antineoplastic Combined Chemotherapy Protocols, Nitriles, medicine, Adjuvant therapy, Humans, Neoplasm Invasiveness, Prospective Studies, Bone mineral, Aromatase inhibitor, business.industry, Triazoles, Antiestrogen, Surgery, Postmenopause, Tamoxifen, Treatment Outcome, Oncology, Tolerability, Chemotherapy, Adjuvant, Selective estrogen receptor modulator, Case-Control Studies, Female, business, medicine.drug

Abstract

Purpose The Arimidex, Tamoxifen, Alone or in Combination (ATAC) trial (median follow-up, 68 months) has shown that adjuvant anastrozole has superior efficacy and better tolerability than tamoxifen. However, anastrozole reduces circulating estrogen, and low estradiol levels are associated with decreased bone mineral density (BMD) and increased fracture risk. It is therefore important to understand the effects of long-term aromatase inhibitor therapy on BMD. Patients and Methods This prospective substudy of the ATAC trial assessed BMD changes in postmenopausal women with invasive primary breast cancer receiving anastrozole (1 mg/d) or tamoxifen (20 mg/d) as adjuvant therapy for 5 years. Lumbar spine and total hip BMD were assessed at baseline and after 1, 2, and 5 years. Results One hundred ninety-seven women from the monotherapy arms of the ATAC trial were recruited onto the bone substudy, and 108 were included in the primary analysis. Among anastrozole-treated patients, there was a decrease in median BMD from baseline to 5 years in lumbar spine (−6.08%) and total hip (−7.24%) compared with the tamoxifen group (lumbar spine, +2.77%; total hip, +0.74%). No patients with normal BMD at baseline became osteoporotic at 5 years. Conclusion Anastrozole is associated with accelerated bone loss over the 5-year treatment period. However, although patients with pre-existing osteopenia are likely to require monitoring and bone-protection strategies, patients with normal BMD would not appear to require monitoring beyond the recommendation for healthy postmenopausal women. The effect of anastrozole on bone should be weighed against its superior efficacy and better tolerability profile versus tamoxifen in the main ATAC trial.

Published

2008

25. A Prototypical Process for Creating Evidentiary Standards for Biomarkers and Diagnostics

Author

D Raunig, James T. Mayne, D Fu, Lawrence J. Lesko, S Furlong, P Sager, Robert A. Dean, Glen Clack, CD Lathia, J Bloom, D Amakye, K Zerba, CA Altar, Lois Hinman, C Girman, J Meyer, D Bounos, S Madani, Viswanath Devanarayan, P Wong, and SA Williams

Subjects

Quality Control, Drug Industry, Process (engineering), Drug Evaluation, Preclinical, Nanotechnology, Risk Assessment, Biomarkers, Pharmacological, law.invention, Food and drug administration, law, Animals, Humans, Medicine, Pharmacology (medical), Cooperative Behavior, Program Development, Pharmacology, Clinical Trials as Topic, Clinical pharmacology, Diagnostic Tests, Routine, United States Food and Drug Administration, business.industry, Reproducibility of Results, United States, Engineering ethics, business, Biomarkers

Abstract

A framework for developing evidentiary standards for qualification of biomarkers is a key need identified in the Food and Drug Administration's Critical Path Initiative.1 This article describes a systematic framework that was developed by Pharmaceutical Research and Manufacturers of America (PhRMA) committees and tested at a workshop in collaboration with the Food and Drug Administration and academia. With some necessary refinements, this could be applied to create an appropriately individualized evidentiary standard for any biomarker purpose. Clinical Pharmacology & Therapeutics (2008); doi:10.1038/sj.clpt.6100451

Published

2007

26. Tissue collection in drug discovery and development research

Author

Glen Clack and Christopher Womack

Subjects

Cancer Research, medicine.medical_specialty, business.industry, Mechanism (biology), Drug discovery, Emerging technologies, Phases of clinical research, Pharmacology, Clinical trial, Oncology, Drug development, Medicine, Medical physics, Tissue Collection, business, Pharmaceutical industry

Abstract

A major step in targeted cancer drug discovery is demonstrating ‘proof of mechanism’. Tissue samples are an integral part of current drug development. At the Biotherapy Development Association Meeting in March 2007, the benefits and problems of tissue related endpoint inclusion in clinical drug development were discussed; Academic, Regulatory Authority and Pharmaceutical Industry representation being present. It was agreed that the public supports the use of human tissue in research; cooperation and collaboration are essential to ensure that tissue samples are collected and available for research; tissue sampling should be mandatory for clinical trials; and that tissue remaining from diagnostic, surgical and clinical trial based sampling should be made available for research. Until existing or new technologies provide utility for alternative sampling, access to human tissue samples of consistent quality will underpin the success of cancer drug pipelines in the era of molecular biological biomarkers and personalised medicine.

Published

2007

27. The impact of delay in cryo-fixation on biomarkers of Src tyrosine kinase activity in human breast and bladder cancers

Author

Tamsin Boyce, Emma Duffield, Francesco Pinto, Tim P. Green, John L. Robertson, Vivien Jacobs, Glen Clack, Robert Jones, Michael Fennell, and John Kelly

Subjects

Male, Cancer Research, Pathology, medicine.medical_specialty, Time Factors, Tissue Fixation, Biopsy, Breast Neoplasms, Toxicology, Breast cancer, Freezing, Humans, Medicine, Pharmacology (medical), Phosphorylation, Phosphotyrosine, Aged, Aged, 80 and over, Immunoassay, Pharmacology, Bladder cancer, medicine.diagnostic_test, business.industry, Kinase, Cancer, Middle Aged, medicine.disease, src-Family Kinases, Urinary Bladder Neoplasms, Oncology, Focal Adhesion Protein-Tyrosine Kinases, Cancer research, Immunohistochemistry, Female, Paxillin, business, Tyrosine kinase, Biomarkers, Proto-oncogene tyrosine-protein kinase Src

Abstract

Demonstration of pharmacodynamic activity of new, targeted cancer drugs in tumour tissue is potentially important in guiding early drug development. However, delays between tumour sampling and sample fixation may result in variability of pharmacodynamic biomarkers. The aim of this study, was to assess the impact of delays in fixation on biomarkers of Src kinase activity. A total of 20 patients with locally advanced breast cancer and 5 with early bladder cancer had multiple tissue samples taken which were fixed at documented time points up to 60 min after biopsy. These were examined to determine if the amount of Paxillin, phospho-Paxillin, phospho-focal adhesion kinase (FAK) and total phospho-Tyrosine changed over time, using a quantitative lysate immunoassay. In breast cancer, there was an increase in the amount of phospho-Paxillin (60% per h; P = 0.019) up to 60 min after biopsy. The amount of total Paxillin decreased (28% per h; P = 0.034) over the same time course. In early bladder cancer, no changes were noted in any endpoints up to 45 min. Standardisation of the time taken between biopsy and fixation may be critical, particularly in studies using phosphorylated protein biomarkers.

Published

2007

28. The value of integrating pre-clinical data to predict nausea and vomiting risk in humans as illustrated by AZD3514, a novel androgen receptor modulator

Author

Daniel Muthas, Glen Clack, Simon A. Smith, Damian G. Deavall, Claire Grant, Pete Newham, and Lorna Ewart

Subjects

0301 basic medicine, Male, Nausea, Vomiting, Drug Evaluation, Preclinical, Clinical manifestation, Pharmacology, Toxicology, Bioinformatics, 03 medical and health sciences, Prostate cancer, Dogs, Predictive Value of Tests, medicine, Animals, Humans, Retching, Pica (disorder), Rats, Wistar, Gastric emptying, Dose-Response Relationship, Drug, business.industry, Ferrets, medicine.disease, Rats, Androgen receptor, Pyridazines, 030104 developmental biology, Receptors, Androgen, Models, Animal, Female, medicine.symptom, business

Abstract

Nausea and vomiting are components of a complex mechanism that signals food avoidance and protection of the body against the absorption of ingested toxins. This response can also be triggered by pharmaceuticals. Predicting clinical nausea and vomiting liability for pharmaceutical agents based on pre-clinical data can be problematic as no single animal model is a universal predictor. Moreover, efforts to improve models are hampered by the lack of translational animal and human data in the public domain. AZD3514 is a novel, orally-administered compound that inhibits androgen receptor signaling and down-regulates androgen receptor expression. Here we have explored the utility of integrating data from several pre-clinical models to predict nausea and vomiting in the clinic. Single and repeat doses of AZD3514 resulted in emesis, salivation and gastrointestinal disturbances in the dog, and inhibited gastric emptying in rats after a single dose. AZD3514, at clinically relevant exposures, induced dose-responsive "pica" behaviour in rats after single and multiple daily doses, and induced retching and vomiting behaviour in ferrets after a single dose. We compare these data with the clinical manifestation of nausea and vomiting encountered in patients with castration-resistant prostate cancer receiving AZD3514. Our data reveal a striking relationship between the pre-clinical observations described and the experience of nausea and vomiting in the clinic. In conclusion, the emetic nature of AZD3514 was predicted across a range of pre-clinical models, and the approach presented provides a valuable framework for predicition of clinical nausea and vomiting.

Published

2015

29. Effect of an Aromatase Inhibitor on BMD and Bone Turnover Markers: 2-Year Results of the Anastrozole, Tamoxifen, Alone or in Combination (ATAC) Trial (18233230)

Author

Richard Eastell, Rosemary A. Hannon, Jack Cuzick, Judith E. Adams, Mitch Dowsett, and Glen Clack

Subjects

Risk, medicine.medical_specialty, Antineoplastic Agents, Hormonal, medicine.drug_class, Endocrinology, Diabetes and Metabolism, Osteoporosis, Urology, Anastrozole, Breast Neoplasms, Bone remodeling, Fractures, Bone, Breast cancer, Bone Density, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, Nitriles, medicine, Humans, Orthopedics and Sports Medicine, Aged, Hip, Lumbar Vertebrae, Aromatase inhibitor, Aromatase Inhibitors, business.industry, Middle Aged, Triazoles, medicine.disease, Antiestrogen, Postmenopause, Radiography, Osteopenia, Tamoxifen, Endocrinology, Female, Bone Remodeling, business, Biomarkers, medicine.drug

Abstract

Aromatase inhibitors reduce estrogen levels in postmenopausal women with breast cancer. Residual estrogen is an important determinant of bone turnover. Adjuvant anastrozole was associated with significant BMD loss and increased bone remodeling, whereas tamoxifen reduced bone marker levels. Introduction: In the Anastrozole, Tamoxifen, Alone or in Combination (ATAC) trial after a median follow-up of 68 months, a significant improvement in disease-free survival was observed with anastrozole treatment (hazard ratio [HR], 0.87; 95% CI, 0.78–0.97; p = 0.01). Anastrozole was also associated with tolerability benefits compared with tamoxifen, but with higher fracture rates. The HR of anastrozole compared with tamoxifen after 60 months of treatment was 1.49 (95% CI, 1.25–1.77). Materials and Methods: This prospectively designed subprotocol (n = 308) of ATAC assessed changes in BMD and bone turnover markers in postmenopausal women with invasive primary breast cancer receiving anastrozole 1 mg/day, tamoxifen 20 mg/day, or combination treatment with both agents for 5 years. Patients with osteoporosis were excluded (osteopenia permitted at the investigators discretion). Lumbar spine and total hip BMD was assessed at baseline and after 1 and 2 years; bone turnover markers (serum C-telopeptide, urinary N-telopeptide [NTX], free deoxypyridinoline, serum procollagen type-1 N-propeptide, bone alkaline phosphatase [ALP]) were assessed at baseline and after 3, 6, and 12 months. Results were expressed as median percentage change. Results: After 2 years of anastrozole treatment, BMD was lost at lumbar spine (median 4.1% loss) and total hip (median 3.9% loss) sites; increases of 2.2% and 1.2%, respectively, were observed with tamoxifen. After 1 year of anastrozole treatment, increased bone remodeling was observed (NTX, +15%; 95% CI, 3–25%; bone ALP, +20%; 95% CI, 14–25%); decreased bone remodeling was observed with tamoxifen (NTX, −52%; 95% CI, −62% to −33%; bone ALP, −16%; 95% CI, −24% to −11%). Conclusions: Anastrozole is associated with significant BMD loss and a small increase in bone turnover, whereas tamoxifen (and the combination) is associated with increased BMD and decreased remodeling. These data may explain the increased fracture risk observed with anastrozole treatment in the ATAC trial. The impact of anastrozole on bone should be weighed against its overall superior efficacy and tolerability as observed in the main ATAC trial.

Published

2006

30. PATRIOT: A phase I study to assess the tolerability, safety and biological effects of a specific ataxia telangiectasia and Rad3-related (ATR) inhibitor (AZD6738) as a single agent and in combination with palliative radiation therapy in patients with solid tumours

Author

Lorna Grove, James Spicer, Sally Ellis, Sola Adeleke, Martin Forster, Jennifer Laude, Simon Smith, Glen Clack, Z. Viney, Kevin J. Harrington, Lyndall McLellan, George Lazaridis, and Magnus T. Dillon

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, education.field_of_study, Cell cycle checkpoint, Palliative Radiation Therapy, business.industry, medicine.medical_treatment, Population, G2-M DNA damage checkpoint, Clinical trial, Radiation therapy, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Tolerability, 030220 oncology & carcinogenesis, Internal medicine, Medicine, business, education, Ataxia telangiectasia and Rad3 related, Biomedical engineering

Abstract

Tumour control rates from radiation therapy (RT) are limited by normal tissue toxicities. Novel strategies are required to selectively sensitize tumour cells to radiation-induced DNA damage. The G2 cell cycle checkpoint is an attractive target for this, as normal cells will be protected by their intact G1 checkpoint, which is lost in the majority of cancer cells. ATR is an important mediator of the G2 checkpoint. Preclinical data suggest that ATR inhibition will sensitise to DNA damaging therapies, including RT. This multi-part phase 1 trial aims to assess safety and tolerability and preliminary anti-tumour activity of the ATR inhibitor AZD6738 as monotherapy and in combination with palliative RT, escalating both drug and radiation dose at a dose-fractionation relevant to radical treatment. The design aims to test a novel agent at the earliest stage of clinical development and assess safety in combination with RT, with the aim of moving to a radically-treated population if tolerated. Methods: Participants have advanced solid tumours without standard systemic therapy options. The trial comprises three parts: parts A and B will assess AZD6738 as a single agent in dose escalation to MTD (part A), followed by expansion cohorts enriched for defective DNA damage response (part B). Part C will assess AZD6738 in combination with palliative RT in which participants will receive 20 Gy in 10 fractions, with per cohort escalation of drug dose to monotherapy MTD if tolerated. At the highest tolerated combination dose, the RT dose will be escalated to 30 Gy in 15 fractions. Maintenance AZD6738 post-RT will be tested at the highest tolerated combination dose. The study opened in August 2014. The study is dose escalating in part A and part C has opened and treated its first patient. Part B will open when dose escalation has completed. PATRIOT is sponsored by The Royal Marsden, funded by the Cancer Research UK/AstraZeneca Combinations Alliance and supported by supply of free drug and distribution costs from Astra Zeneca. Clinical trial information: NCT02223923

Published

2016

31. The Androgen Receptor in Castration-Resistant Prostate Cancer: Still a Clinical Opportunity?

Author

Glen Clack and Richard D. Finkelman

Subjects

Oncology, Cancer Research, medicine.medical_specialty, medicine.drug_class, business.industry, Disease, medicine.disease, Androgen, Androgen receptor, Prostate cancer, chemistry.chemical_compound, Endocrinology, Castration, chemistry, Internal medicine, medicine, business, Receptor, Chemical castration, Testosterone

Abstract

Prostate cancer is a leading cause of cancer death in men, with an estimate of about 241,000 new cases and 34,000 deaths due to prostate cancer in the United States in 2011 [1]. Prostate cancer is dependent on the androgen receptor (AR); the androgen axis shown to be a key driver of the disease [2]. This principle was first established more than 70 years ago by the demonstration that surgical castration will retard the progression of disease [3]. Prostate cancer typically responds well to suppression of testosterone. Surgical castration is effective in lowering testosterone production but suffers from its psychological impact and irreversibility; thus treatment of the early stages of advanced disease in the Western world is typically based on ‘chemical’ castration with luteinising hormone releasing hormone (LHRH) agonists. These agents suppress luteinising hormone release and markedly reduce testicular testosterone production. Even with effective surgical or chemical castration, however, some residual androgen production

Published

2012

32. Circulating melanoma cells and survival in metastatic melanoma

Author

M. Malone, I. Karydis, Gerald V. Doyle, Mark Connelly, Frank A. W. Coumans, Leon W.M.M. Terstappen, Glen Clack, M.R. Middleton, Chandra Rao, T. Bui, Medical Cell Biophysics, and Other departments

Subjects

Adult, Male, Cancer Research, Pathology, medicine.medical_specialty, Skin Neoplasms, CD34, Cell Count, Andrology, chemistry.chemical_compound, Antigen, medicine, Humans, DAPI, Neoplasm Metastasis, Melanoma, Survival analysis, Whole blood, Aged, Cell Proliferation, Retrospective Studies, Aged, 80 and over, business.industry, Cancer, Middle Aged, medicine.disease, Neoplastic Cells, Circulating, Prognosis, Survival Analysis, Oncology, chemistry, Case-Control Studies, CD146, Female, business, Melanoma-Specific Antigens, METIS-275551

Abstract

A validated assay for the enumeration of circulating melanoma cells (CMCs) may facilitate the development of more effective therapies for metastatic melanoma patients. In this study CD146(+) cells were immunomagnetically enriched from 7.5 ml of blood. Isolated cells were fluorescently stained with DAPI, anti-molecular weight melanoma-associated antigen (HMW-MAA). anti-CD45 and CD34 and Ki67. CMCs were identified as CD146(+), HMW-MAA(+), CD45(-), CD34(-), Ki67(-/+) cells. Eighty-eight percent of spiked SK-MEL28 cells in 7.5 ml blood were recovered. In all 55 healthy donors = 2 CMCs per 7.5 ml of whole blood, as compared with the group with

Published

2011

33. Prevention of aromatase inhibitor-induced bone loss using risedronate: the SABRE trial

Author

Rosemary A. Hannon, Glen Clack, Catherine Van Poznak, Andreas Makris, David H. Barlow, Richard Eastell, John R. Mackey, J. Apffelstaedt, and Mario Campone

Subjects

musculoskeletal diseases, Cancer Research, medicine.medical_specialty, medicine.drug_class, Hormone Replacement Therapy, Osteoporosis, Urology, Anastrozole, Breast Neoplasms, Placebo, Fractures, Bone, Double-Blind Method, Bone Density, Nitriles, Vitamin D and neurology, Medicine, Humans, Osteoporosis, Postmenopausal, Aged, Neoplasm Staging, Bone mineral, Aromatase inhibitor, Bone Density Conservation Agents, business.industry, Aromatase Inhibitors, Etidronic Acid, Middle Aged, Triazoles, medicine.disease, Prognosis, Surgery, Osteopenia, Postmenopause, Survival Rate, Treatment Outcome, Oncology, Risedronic acid, Female, business, Risedronic Acid, medicine.drug

Abstract

Purpose To investigate the management of bone health in women with early breast cancer (EBC) who were scheduled to receive anastrozole. Patients and Methods Postmenopausal women with hormone receptor–positive EBC were assigned to one of three strata by risk of fragility fracture. Patients with the highest risk (H) received anastrozole 1 mg/d plus risedronate 35 mg/wk orally. Patients with moderate-risk (M) were randomly assigned in a double-blind manner to anastrozole and risedronate (A + R) or to anastrozole and placebo (A + P). Patients with lower-risk (L) received anastrozole (A) alone. Calcium and vitamin D were recommended for all patients. Lumbar spine and total hip bone mineral density (BMD) were assessed at baseline, 12 months, and 24 months. Results At 24 months, in the M group, treatment with A + R resulted in a significant increase in lumbar spine and total hip BMD compared with A + P treatment (2.2% v −1.8%; treatment ratio, 1.04; P < .0001; and 1.8% v −1.1%; treatment ratio, 1.03; P < .0001, respectively). In the H stratum, lumbar spine and total hip BMD increased significantly (3.0%; P = .0006; and 2.0%; P = .0104, respectively). Patients in the L stratum showed a significant decrease in lumbar spine BMD (−2.1%; P = .0109) and a numerical decrease in total hip BMD (−0.4%; P = .5988). Safety profiles for anastrozole and risedronate were similar to those already established. Conclusion In postmenopausal women at risk of fragility fracture who were receiving adjuvant anastrozole for EBC, the addition of risedronate at doses established for preventing and treating osteoporosis resulted in favorable effects in BMD during 24 months.

Published

2010

34. Effects of the Src kinase inhibitor saracatinib (AZD0530) on bone turnover in healthy men: a randomized, double-blind, placebo-controlled, multiple-ascending-dose phase I trial

Author

J. Andrew Lockton, Richard Eastell, Richard D. Finkelman, Glen Clack, Rosemary A. Hannon, Martin Rimmer, and Alan Swaisland

Subjects

Adult, Male, medicine.medical_specialty, Bone disease, Endocrinology, Diabetes and Metabolism, Osteoporosis, Urology, Placebo, Bone resorption, Drug Administration Schedule, Bone remodeling, chemistry.chemical_compound, Double-Blind Method, Osteoclast, Internal medicine, medicine, Humans, Orthopedics and Sports Medicine, Benzodioxoles, Enzyme Inhibitors, Creatinine, business.industry, medicine.disease, medicine.anatomical_structure, Endocrinology, chemistry, Quinazolines, Bone Remodeling, business, Men's Health, Type I collagen, Biomarkers

Abstract

Src is a nonreceptor tyrosine kinase thought to be essential for osteoclast function and bone resorption. We investigated the effect of the orally available Src inhibitor saracatinib (AZD0530) on bone turnover in healthy men. The study was part of a randomized, double-blind, placebo-controlled multiple-ascending-dose phase I trial of saracatinib. Fifty-nine healthy men (mean age 34.6 years) were divided into five cohorts; four with 12 subjects and one with 11 subjects, and randomized within each cohort in the ratio 3:1 to receive a single dose of saracatinib or placebo, respectively, followed 7 to 10 days later with daily doses for a further 10 to 14 days. Dosing levels of saracatinib ascended by cohort (60 to 250 mg). Markers of bone turnover were measured predose and 24 and 48 hours after the initial single dose and immediately before and 24 and 48 hours and 10 to 14 days after the final dose. Data from 44 subjects were included in the analysis. There was a dose-dependent decrease in bone resorption markers [serum cross-linked C-telopeptide of type I collagen (sCTX) and urinary cross-linked N-telopeptide of type I collagen normalized to creatinine (uNTX/Cr)]. At a dose of 250 mg (maximum tolerated dose), sCTX decreased by 88% [95% confidence interval (CI) 84-91%] and uNTX/Cr decreased by 67% (95% CI 53-77%) from baseline 24 hours after the final dose. There was no significant effect on bone formation markers. There were no significant adverse events. We conclude that inhibition of Src reduces osteoclastic bone resorption in humans. Saracatinib is a potentially useful treatment for diseases characterized by increased bone resorption, such as metastatic bone disease and osteoporosis.

Published

2009

35. Effects of third generation aromatase inhibitors on bone health and other safety parameters: results of an open, randomised, multi-centre study of letrozole, exemestane and anastrozole in healthy postmenopausal women

Author

Richard Eastell, Anna Miyamoto, Richard D. Finkelman, Glen Clack, Eugene V. McCloskey, Geza Lakner, Rosemary A. Hannon, and William D. Fraser

Subjects

Cancer Research, medicine.medical_specialty, medicine.drug_class, Anastrozole, Bone resorption, Bone and Bones, Bone remodeling, Body Mass Index, chemistry.chemical_compound, Exemestane, Internal medicine, Adrenal Glands, Nitriles, Medicine, Humans, Aromatase, Bone Resorption, Aromatase inhibitor, biology, business.industry, Aromatase Inhibitors, Letrozole, Middle Aged, Triazoles, Antiestrogen, Alkaline Phosphatase, Lipids, Androstadienes, Postmenopause, Endocrinology, Oncology, chemistry, biology.protein, Female, Bone Remodeling, business, Biomarkers, medicine.drug

Abstract

Given potential differences between the skeletal and other effects of the third generation aromatase inhibitors (AIs), we conducted an open, randomised Phase I study, comparing the effects of three licensed AIs on bone turnover markers, lipid profiles and adrenal function. Treatment comparisons were undertaken in 90 healthy postmenopausal women with normal bone mineral density who received once daily oral anastrozole (1mg, n=29), letrozole (2.5mg, n=29) or exemestane (25mg, n=32) for 24weeks with a subsequent 12week washout period. All three AIs induced increases in bone resorption markers, but no significant differences were observed in their effects on bone turnover markers. Greater differences were observed in lipid metabolism. Notably, exemestane, but not anastrozole or letrozole, significantly increased the LDL:HDL cholesterol ratio by 12weeks, largely mediated by a decrease in HDL-cholesterol. Further, long-term clinical studies are required to determine the impact, if any, of the differences observed between the AIs

Published

2007

36. ATR inhibitor AZD6738

Author

Christine Stephens, Glen Clack, Andrew J. Pierce, Simon Smith, and Alan Lau

Subjects

Genome instability, DNA damage, business.industry, DNA replication, Hematology, G2-M DNA damage checkpoint, DNA Replication Fork, Cell biology, Oncology, Cancer cell, Cancer research, Medicine, CHEK1, business, Ataxia telangiectasia and Rad3 related

Abstract

AZD6738 is a potent and selective orally bio-available inhibitor of ataxia telangiectasia and rad3 related (ATR),a key serine/threonine protein kinase involved in DNA damage response signalling caused by DNA replication associated stress. Activation of ATR at stalled replication forks leads to suppression of replication fork origin firing, promotes repair and activates S/G1/G2-cell cycle checkpoints to prevent premature mitosis and maintain genomic integrity. Failure to resolve this damage leads to genomic instability and if sufficiently high, cell death. Cancer cells undergoing high levels of replication associated DNA damage or in cells with deficiencies in ATM-dependent repair pathways are hypothesised to be more reliant on ATR for survival and specific inhibition of ATR may lead to enhanced anti-tumour activity. In patients with malignant disease, an ATR inhibitor has the potential to: • Have monotherapy activity, through synthetic lethality or by exploiting on-going aberrant DNA replication structures leading to dependency on ATR • Act synergistically in combination with DNA damaging therapies, either systemic therapies or a localised DNA damaging therapy, such as radiotherapy which activate ATR • Act as a maintenance therapeutic after either of the above. AZD6738 monotherapy response across cell line panels in vitro shows a wide range of sensitivities and is well tolerated at efficacious doses in vivo. ATM-deficient cells are enriched for greater sensitivity to AZD6738 which offers a potential testable patient selection hypothesis. However, AZD6738 also shows enhanced activity in some (but not all) ATM-proficient cells such those from haematological malignancies. In addition, combination of AZD6738 with radiation induces regression in both ATM-deficient and ATM-proficient models (albeit at different AZD6738 doses). Anti-tumour activity of AZD6738 may, therefore, also be seen more broadly than ATM-deficiency particularly in combinations. Here we describe the 2 clinical studies with AZD6738 that will test the monotherapy and combination therapy (potentiation of DNA damage) hypotheses, along with an overview of the pre-clinical in vitro and in vivo data supporting this.

Published

2015

37. The ATAC ('Arimidex', Tamoxifen, Alone or in Combination) adjuvant breast cancer trial: first results of the endometrial sub-protocol following 2 years of treatment

Author

Glen Clack, Michael Wells, S. Pollard, Tracy Jackson, Mark Lansdown, K. Philips, Sean Duffy, Michel Coibion, and André Macedo Bianco

Subjects

medicine.medical_specialty, medicine.drug_class, medicine.medical_treatment, Urology, Anastrozole, Breast Neoplasms, Endometrium, Breast cancer, Polyps, Risk Factors, Antineoplastic Combined Chemotherapy Protocols, Nitriles, medicine, Humans, Gynecology, Aromatase inhibitor, business.industry, Endometrial cancer, Rehabilitation, Obstetrics and Gynecology, Hormone replacement therapy (menopause), Middle Aged, Triazoles, medicine.disease, Antiestrogen, Endometrial Neoplasms, Tamoxifen, Reproductive Medicine, Chemotherapy, Adjuvant, Female, business, Progestin, medicine.drug

Abstract

Background: Tamoxifen treatment results in a doubling of the risk of endometrial cancer after 1-2 years of treatment and a quadrupling after 5 years. Anastrozole, a third-generation aromatase inhibitor, with superior efficacy to tamoxifen, may also offer tolerability benefits in terms of effects on the endometrium. Methods and results: A sub-protocol of the ATAC trial compared the incidence/type of intrauterine changes following treatment with these agents in a subgroup of patients (n = 285) from the main trial. After 2 years anastrozole treatment, endometrial thickness remained ≤ 5 mm (baseline: 3.0 mm); in patients receiving tamoxifen, endometrial thickness increased by 3.2 mm to 7.0 mm, with a similar trend in the combination group. At baseline, 26/285 patients (9.1%) had endometrial abnormalities, most commonly polyps. After 2 years the number of endometrial abnormalities appeared lower with anastrozole treatment compared with tamoxifen although these differences were not statistically significant (odds ratio: 0.44; 95% confidence interval 0.146, 1.314; P = 0.14). Most abnormalities occurred within the first year of treatment (anastrozole: 4/6; tamoxifen: 7/10; combination: 10/16; total: 21/32). Fewer patients in the anastrozole group (1.4%) required medical intervention (tamoxifen 12.5%; combination 13.6%). Conclusions: Fewer endometrial abnormalities occurred during 2 years treatment with anastrozole compared with tamoxifen although statistical significance was not reached in this sub-protocol analysis.

Published

2005

38. The ATAC ('Arimidex', Tamoxifen, Alone or in Combination) adjuvant breast cancer trial: baseline endometrial sub-protocol data on the effectiveness of transvaginal ultrasonography and diagnostic hysteroscopy

Author

S. Pollard, Michel Coibion, Glen Clack, Tracy Jackson, Mark Lansdown, Michael Wells, André Macedo Bianco, K. Philips, and Sean Duffy

Subjects

medicine.medical_specialty, Antineoplastic Agents, Hormonal, Urology, Anastrozole, Breast Neoplasms, Hysteroscopy, Endometrium, Sensitivity and Specificity, Breast cancer, Clinical Protocols, Double-Blind Method, Nitriles, medicine, Humans, Ultrasonography, Gynecology, medicine.diagnostic_test, business.industry, Rehabilitation, Obstetrics and Gynecology, Anatomical pathology, Triazoles, Antiestrogen, medicine.disease, Tamoxifen, medicine.anatomical_structure, Reproductive Medicine, Chemotherapy, Adjuvant, Female, business, Endometrial biopsy, medicine.drug

Abstract

BACKGROUND: The ‘Arimidex’, Tamoxifen, Alone or in Combination (ATAC) trial is a randomized, doubleblind trial comparing anastrozole (‘Arimidex’), alone or in combination with tamoxifen, relative to tamoxifen alone as 5 year adjuvant treatment for post-menopausal women with early breast cancer. Since tamoxifen is associated with endometrial pathology, the ATAC endometrial sub-protocol was initiated to establish the background prevalence of intrauterine pathology, and to assess prospectively the incidence and nature of intrauterine changes following endocrine therapy. Another aim was to provide data from which advice could be generated on the best endometrium screening method for patients receiving tamoxifen. METHODS: Patients underwent endometrial assessments at entry to the sub-protocol. The baseline investigations comprised transvaginal ultrasound scanning (TVUS), a hysteroscopy and an endometrial biopsy. RESULTS: A total of 285 gynaecologically asymptomatic women from 31 centres in 10 countries entered the endometrial sub-protocol. The mean uterine volume was 47.7 cm 3 . The median endometrial thickness overall was 3 mm. Twenty-four histologically confirmed, pathological changes were observed. Twenty-three pathologies were confirmed by TVUS, and 21 were identified by hysteroscopy and confirmed by histopathology. Women with or without intrauterine pathology had median endometrial thickness of 5 and 3 mm respectively. CONCLUSIONS: The presence of pathology was associated with increased endometrial thickness. The relative sensitivity and specificity of hysteroscopy and endometrial thickness for the diagnosis of endometrial pathology was comparable to other studies. If screening of the endometrium prior to treatment is appropriate, this study supports the use of an endometrial thickness of 3 mm, as assessed by TVUS, as a threshold for needing further investigation. This study demonstrates that if the endometrial thickness is >3 mm, hysteroscopy and biopsy is the optimal method of detecting intrauterine pathology in women with breast cancer who are about to commence endocrine treatment.

Published

2004

39. The ATAC adjuvant breast cancer trial in postmenopausal women: baseline endometrial subprotocol data

Author

Michel Coibion, Glen Clack, Tracy Jackson, Jack Cuzick, Mark Lansdown, Michael Wells, André Macedo Bianco, S. Pollard, K. Philips, and Sean Duffy

Subjects

Adult, medicine.medical_specialty, Antineoplastic Agents, Hormonal, medicine.medical_treatment, Population, Anastrozole, Breast Neoplasms, Hysteroscopy, Breast cancer, Clinical Protocols, Double-Blind Method, Antineoplastic Combined Chemotherapy Protocols, Nitriles, medicine, Endometrial Polyp, Humans, education, Aged, Gynecology, Aged, 80 and over, education.field_of_study, medicine.diagnostic_test, business.industry, Obstetrics and Gynecology, Hormone replacement therapy (menopause), Middle Aged, Triazoles, medicine.disease, Menopause, Postmenopause, Tamoxifen, Chemotherapy, Adjuvant, Female, business, medicine.drug

Abstract

Objective The ATAC (Arimidex, Tamoxifen, Alone or in Combination) trial is a randomised, double-blind trial comparing ‘Arimidex’ (anastrozole), alone or in combination with tamoxifen, relative to tamoxifen alone as a five year adjuvant treatment for postmenopausal women with early breast cancer. Because tamoxifen is associated with endometrial pathology, the ATAC endometrial subprotocol was initiated to establish the background prevalence of pathology, and to assess prospectively the incidence and nature of intrauterine changes before and following endocrine therapy. Setting International. Population and Study Design Two hundred and eighty-five women entered the subprotocol: the mean age was 60 years (range 44–80 years); 113 women (40%) had taken hormone replacement therapy prior to randomisation, and 238 women were parous (84%). The age at onset of the menopause was 32–58 years, with the majority becoming menopausal between 46 and 55 years of age. Two hundred and seventy-two women had a hysteroscopy before they commenced trial medication. Hysteroscopy was performed successfully in 265 women. In six women, failure of hysteroscopy at baseline led to withdrawal from the study. Three of the women who withdrew had a pipelle biopsy taken. Therefore, the total number of endometrial biopsies at baseline was 268. Main outcome measures To assess the demographic characteristics of women entering the endometrial subprotocol and their hysteroscopic and histological findings before commencing trial medication. Results At hysteroscopy, there was a diagnosis of endometrial polyps in 34 women (13%), fibroids in 16 women (6%) and one case of suspicious endometrium, which was confirmed as a polyp on histology. Only 21 of the 34 polyps seen hysteroscopically were proven histologically (62% accuracy of hysteroscopy). Final histology found the prevalence of endometrial diagnostic categories as follows: 123 inactive endometrium (46%), 20 benign polyps (7%), 17 secretory endometrium (6%), 7 proliferative endometrium (3%), 3 atypical hyperplasia (2 in a polyp), 1 simple hyperplasia (in a polyp) and 1 fibroid. The remaining women had pipelle samples with insufficient tissue obtained, indicating a normal endometrial cavity. Conclusion This is the first study of such size in gynaecologically asymptomatic breast cancer patients. This paper describes the findings in individual patients before any trial treatment was given. In this baseline group, 82% (219/268) of women had a normal endometrial cavity; 18% (49/268) had endometrial activity (proliferative or secretory endometrium in 9%) or an intracavity abnormality (hyperplasia, polyps and a fibroid in 9%). In total, 36% of biopsies had insufficient tissue for diagnosis, which in combination with a normal hysteroscopy was classed as normal. The appearance of a polyp hysteroscopically in this group was not proven histologically in approximately 40% of cases. The development of uterine pathology over time in the ATAC study will subsequently be assessed against the findings of this baseline paper.

Published

2003

40. Assessment Of Circulating Free DNA (CFDNA) and Circulating Melanoma Cells (CMCS) as Prognostic Biomarkers in Metastatic Cutaneous Melanoma

Author

Cong Zhou, Matthew Lancashire, Glen Clack, A. Hughes, Leila Khoja, Robert Sloane, Paul Lorigan, Caroline Dive, Kyaw Aung, and Gerard Brady

Subjects

Oncology, medicine.medical_specialty, Metastatic Cutaneous Melanoma, business.industry, Melanoma, Hematology, medicine.disease, Exact test, Circulating free DNA, Internal medicine, medicine, In patient, Sample collection, business, Survival analysis, Whole blood

Abstract

Background cfDNA is detectable in patients with metastatic cutaneous melanoma and its plasma concentration could potentially predict their clinical outcomes. We assessed the correlation between cfDNA concentration and patients' overall survival and clinical characteristics including known poor prognostic factors in melanoma. Prognostic value of CMCs number and its association with cfDNA level was also explored. Methods Pre-treatment blood samples from 50 patients with metastatic cutaneous melanoma were collected prospectively. cfDNA was extracted from 1 ml of plasma using QIAamp Circulating Nucleic Acids Kit (Qiagen, Hilden, Germany) and quantified by RNase P qPCR (ABI Life Technologies, Foster City, NJ, USA). CMC enumeration per 7.5 ml whole blood was performed within 96 hours of sample collection using the CellSearch Melanoma Kit (Veridex, NJ, USA). Correlation between cfDNA concentration and clinical characteristics and CMC number was performed using χ2-test and Fisher's exact test where appropriate. Survival curves were produced and compared by the Kaplan-Meier method and log-rank test respectively. Results The median concentration of cfDNA was 6.8 ng/ml (range 0-205.8) and median CMC number was 0/7.5ml (range 0-16). Patients with cfDNA concentration of >75% percentile had significantly shorter overall survival compared to those with cfDNA level Conclusions Plasma cfDNA concentration and presence of CMC in 7.5 ml whole blood can predict patient's survival outcomes in metastatic cutaneous melanoma. No association was found between these two biomarkers and this highlights the possibility that they may represent different tumour biological process. Disclosure G. Brady: has an advisory role in Epistem and owns shares in Epistem. G. Clack: employee of Astra-Zeneca pharamceuticals and ownes stock in Astra-zeneca. A. Hughes: Employee of Astra-Zeneca and ownes stock in Astra-Zeneca. All other authors have declared no conflicts of interest.

Published

2012

41. A randomized, open, parallel-group trial to compare the endocrine effects of oral anastrozole (Arimidex) with intramuscular formestane in postmenopausal women with advanced breast cancer

Author

John F.R. Robertson, R. Perez-Carrion, Mitchell Dowsett, Glen Clack, L. Calvo, D.A Vorobiof, D.J. Dodwell, and Ulrich R. Kleeberg

Subjects

Adult, medicine.medical_specialty, Randomization, medicine.drug_class, Urology, Anastrozole, Administration, Oral, Estrone, Antineoplastic Agents, Breast Neoplasms, Formestane, Injections, Intramuscular, chemistry.chemical_compound, Internal medicine, Nitriles, medicine, Humans, Aged, Aged, 80 and over, Aromatase inhibitor, business.industry, Androstenedione, Estrogens, Hematology, Middle Aged, Triazoles, Antiestrogen, Endocrinology, Oncology, Tolerability, chemistry, Female, Intramuscular injection, business, medicine.drug

Abstract

Summary Background: This study provides a direct randomized comparison of a new-generation, non-steroidal aromatase inhibitor, anastrozole (Arimidex®), with a steroidal aromatase inhibitor (formestane) with respect to oestrogen (oestradiol, oestrone, and oestrone sulphate) suppression and tolerability. Patients and methods: Sixty postmenopausal women with advanced breast cancer were randomized to receive either anastrozole 1 mg once daily orally (n = 29), or formestane 250 mg once every two weeks by intramuscular injection (n = 31). Treatment was continued until progression of disease or withdrawal from the study. The primary endpoints of this study were oestradiol suppression and tolerability. The secondary endpoints included oestrone and oestrone sulphate suppression. All laboratory analyses were conducted 'blind' of the randomized drug treatment. Results: Anastrozole produced a greater and more consistent suppression of oestradiol levels compared with formestane. Based on two- and four-week measurements, the mean fall from baseline (pre-dose) in oestradiol level was 79% and 58% in the anastrozole and formestane groups, respectively (P = 0.0001). After four weeks of treatment, oestrone and oestrone sulphate levels were also suppressed to a greater extent by anastrozole compared with formestane (oestrone: 85% versus 67%, respectively, P - 0.0043; oestrone sulphate: 92% versus 67%, respectively, P = 0.0007). No statistical differences were seen between the two drugs in the incidence of adverse events. Conclusions: Anastrozole provides a more consistent and significantly more effective suppression of oestradiol compared with formestane. Similar results were observed for oestrone and oestrone sulphate. The clinical significance of these differences in total oestrogen suppression remains to be established.

Published

1999

42. A first-in-human study of the oral selective androgen receptor down-regulating drug (SARD) AZD3514 in patients with castration-resistant prostate cancer (CRPC)

Author

Malcolm R Ranson, Ruud van der Noll, Tony Elliott, Robert Jones, Johann S. de Bono, Michael D. Malone, Glen Clack, Michael Ong, Angela W. Dymond, Richard D. Finkelman, Aurelius Omlin, Joshi J. Alumkal, Jan H.M. Schellens, Mateus Crespo, Andrea Zivi, Janet Graham, and Andrew Dickinson

Subjects

Drug, Oncology, Cancer Research, medicine.medical_specialty, business.industry, media_common.quotation_subject, First in human, Pharmacology, SARD AZD3514, Castration resistant, medicine.disease, Androgen receptor, Prostate cancer, Internal medicine, medicine, In patient, business, media_common

Abstract

4511 Background: AZD3514 is a first in class, orally bio-available drug that inhibits androgen-dependent and –independent androgen receptor (AR) signaling through two distinct mechanisms; inhibition of ligand-driven nuclear AR translocation and down-regulation of AR levels. Methods: A rolling six design was employed initially using a once a day (QD) schedule (A). PK assessments led to a change to twice daily (BD) dosing (B) to increase exposure. PK profiles were studied over 96 hours after a single dose and over 24 hours at start of/following 21 days continuous dosing. PD analyses included PSA and CTC quantification. Results: 49 CRPC patients (pts) have been treated with escalating doses of AZD3514 (A 35 pts, B 14 pts). Starting doses were 100 mg (A) and 1000 mg (B). The AZD3514 formulation was switched from capsules to tablets at 1000mg (QD). 2000mg BD was considered non-tolerable due to multiple grade 2 toxicities (nausea [N], vomiting [V], fatigue). No adverse events (AEs) met the DLT definition. The most frequent drug-related AE’s were N; G1/2 36/49 (73%), G3 2/49 (4%) and V; G1/2 24/49 (49%) & G3 3/49 (6%). N/V were managed with oral anti-emetics. Dose proportional increases in plasma concentrations were observed following a single dose. Geometric mean (%CV) Cmax and AUC at MTD were 9,608 (38.5) ng/mL and 61,734 (40.6) ng.hr/mL, respectively. Compared with single dose continuous dosing led to a mean decrease of 26% in exposure. Maximum PSA and CTC declines are summarized below. Objective soft tissue responses per RECIST1.1 were observed in 2/26 (8%) pts. One pt with abiraterone resistant disease remained on study for 19 months. At 6 and 12 months 21 (43%) and 8 (16%) pts remained on study without evidence of bone or soft tissue progression, respectively. Conclusions: AZD3514 has antitumor activity in patients with advanced CRPC. Clinical trial information: NCT01162395. [Table: see text]

Published

2013

43. Circulating Melanoma Cells (CMCS) in Mucosal and Uveal Melanomas

Author

Paul Lorigan, Alexander J. Kvist, Glen Clack, A. Hughes, Patrick Shenjere, Raffaele Califano, Roy Milner, S Bramley, Caroline Dive, and Leila Khoja

Subjects

Neuroblastoma RAS viral oncogene homolog, GNA11, biology, business.industry, Melanoma, Hematology, medicine.disease, Metastasis, Oncology, biology.protein, Cancer research, medicine, Neoplasm, Immunohistochemistry, Antibody, Vemurafenib, business, medicine.drug

Abstract

Background Melanoma subtypes are increasingly defined by genetic alterations (BRAF mutations in 50% and NRAS in 20% of cutaneous, c-Kit aberrations in acral and mucosal and GNA11 mutations in uveal melanomas. Targeted therapies such as vemurafenib in cutaneous and imatinib in mucosal melanomas have emerged. CMCs are a potential biomarker to assess response to treatment, monitor disease relapse and provide new targets for drug development. Molecular characterisation of CMCs may provide utility as a predictive biomarker to drug treatment. Methods The CellSearch marker dependent platform (Veridex, USA) enriches for CMCs utilising Melcam antibody for CMC capture and High Molecular Weight Melanoma associated Antigen (HMW-MAA) antibody for CMC detection. MART-1 was used as an additional CMC kit detection marker. The ISET marker independent platform (Isolation by Cell Size, Rarecells, France) enriches for CMCs based on cell size. Immunohistochemistry with CD45 and CD144 (leukocyte and endothelial cell markers) and S100 (melanoma marker) was performed to identify CMC characteristic staining and morphology. Results Twenty-three patients with metastatic disease were recruited prospectively (mucosal n = 13, uveal n = 10). CellSearch detected CMCs in 6/11mucosal (range 0-125, mean 21 median 1) and 7/10 uveal (range 0-510, mean 57 median 3) melanomas. MART-1 positive CMCs were detected in both subtypes but circulating tumour microemboli (CTM) were found only in mucosal melanomas. ISET detected CMCs in 10/12 mucosal (range 0-26, mean 4 median 2) and 7/10 uveal (range 0-19, mean 7 median 3) melanomas. CMCs were both S100+ and S100-. No CTM were detected by ISET. Comparison of the platforms in 20 patients (n = 10 of each mucosal and uveal melanomas) revealed variability in CMC detection between platforms (Spearman's correlation p = 0.17). Conclusions This is the first report of CMC detection by CellSearch in mucosal and uveal melanomas. Comparison with ISET revealed no relationship between numbers of CMCs detected in the same patients by each platform thus indicating significant CMC heterogeneity in CMC marker expression and size. Circulating tumour microemboli may indicate collective cell migration thus probing the biology of metastases formation. Disclosure G. Clack: Ownes stocks in Astra-Zeneca pharmaceuticals. A. Hughes: ownes shares in Astra-Zeneca pharmaceuticals. All other authors have declared no conflicts of interest.

Published

2012

44. Pancreatic circulating tumor cells: Where are they?

Author

Andrew Hughes, Caroline Dive, Nicola de Liguori Carino, Christy Mitchinson, Juan W. Valle, Karen Morris, Damien Brown, Glen Clack, Leila Khoja, Cong Zhou, Derek A. O'Reilly, and Rahul Deshpande

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Circulating tumor cell, Oncology, Paired samples, business.industry, Portal vein, Medicine, Portal circulation, Pancreatic carcinoma, business, Peripheral

Abstract

e21037 Background: We previously demonstrated that circulating tumor cell (CTC) numbers in advanced pancreatic carcinoma were low in contrast to other epithelial carcinomas. We hypothesized that pancreatic CTCs may sequest in the liver and conceived a study to explore CTC number in the peripheral and portal circulations of patients undergoing Whipple’s surgery. Methods: Seventeen patients undergoing Whipple’s surgery were recruited prospectively after informed written consent. Blood was collected intra-operatively from the portal vein prior to tumor mobilization and from the peripheral circulation. Paired samples were analysed for CTC number (CellSearch system, Veridex, USA), and M30/M65 biomarkers of cell death. Results: Of 17 patients 6 had cholangiocarcinomas and 11 had pancreatic adenocarcinomas (5 inoperable). CTC number in the portal circulation was consistently higher than in the peripheral circulation. All patients with cholangiocarcinoma had no CTCs in the peripheral circulation but two patients had 139 and 21 CTCs in the portal circulation. Five patients with pancreatic carcinoma had no CTCs in the peripheral circulation but 1 CTC in 2 patients, 4 CTCs in 2 patients and 32 and 731 CTCs were seen in 2 other patients in the portal circulation. Five patients had no CTCs in both circulations and the remaining patient had 1 CTC in the peripheral circulation and 4 CTCs in the portal circulation. Where present, circulating tumour microemboli were detected in the portal circulation only. M65 levels were higher in the portal circulation indicating higher levels of cell death. M30 levels did not differ significantly between circulations but appeared to correlate with portal CTC number. Conclusions: This is the first study to enumerate CTCs in peripheral and portal circulations in pancreato-biliary carcinomas. Higher CTC numbers are present in the portal circulation suggesting CTC sequestration in the liver. Five patients with pancreatic cancer (2 of whom were inoperable) had no CTCs in either circulation, a finding consistent with the poor vascularity and dense stromal characteristics of this carcinoma. Nonetheless the portal circulation may be a potential source for CTC characterisation including genomic analysis to further define tumor biology.

Published

2012

45. Managing cancer treatment-induced bone loss: 24-month results from the Study of Anastrozole with the Bisphosphonate RisedronatE (SABRE)

Author

C. Van Poznak, J. Apffelstaedt, Glen Clack, Richard Eastell, John R. Mackey, Rosemary A. Hannon, and Mario Campone

Subjects

Gynecology, Bone mineral, Cancer Research, medicine.medical_specialty, business.industry, medicine.medical_treatment, Osteoporosis, Urology, Cancer, Anastrozole, Bisphosphonate, medicine.disease, Cancer treatment, Oncology, medicine, skin and connective tissue diseases, business, Adjuvant, medicine.drug, Hormone

Abstract

Abstract #1137 Aim: To investigate the management of bone health in postmenopausal women with early breast cancer (BCA) scheduled to receive anastrozole. Methods: Postmenopausal women with hormone receptor-positive early BCA were assigned to 1 of 3 strata depending on their pre-existing risk of fragility fracture. Patients (pts) with a bone mineral density (BMD) T-score Citation Information: Cancer Res 2009;69(2 Suppl):Abstract nr 1137.

Published

2009

46. Interaction between body mass index and bone turnover during aromatase inhibition: Evidence from the letrozole (L), exemestane (E), and anastrozole (A) pharmacodynamics (LEAP) trial

Author

Glen Clack, Eugene V. McCloskey, Rosemary A. Hannon, R. Eastell, G. Lakner, and A. Miyamoto

Subjects

Cancer Research, medicine.medical_specialty, biology, business.industry, Letrozole, Anastrozole, Bone resorption, Bone remodeling, chemistry.chemical_compound, Endocrinology, Oncology, Exemestane, chemistry, Pharmacodynamics, Internal medicine, biology.protein, medicine, Aromatase, business, Tamoxifen, medicine.drug

Abstract

560 Background: High body mass index (BMI) protects against postmenopausal osteoporotic fracture, mediated in part by higher endogenous levels of oestradiol. Third-generation aromatase inhibitors (AIs) show superior efficacy and tolerability than tamoxifen in the adjuvant treatment of postmenopausal women with hormone receptor-positive early breast cancer. We examined the interactions between BMI and bone turnover during treatment with 3 aromatase inhibitors in the LEAP trial, an open, randomized, pharmacodynamic study in postmenopausal women. Methods: Healthy volunteers from the UK and Hungary with normal bone density and BMI between 18 and 34 kg/m2 were randomized to receive A (1 mg/day), L (2.5 mg/day), or E (25 mg/day) orally, once daily for 24 weeks. Effects on bone resorption (log transformed serum C-telopeptide crosslinks, CTX) and bone formation (bone alkaline phosphatase and propeptide of type I procollagen, PINP) were compared. Changes in biochemical markers of bone resorption and formation during treatment were all statistically inter- correlated (p No significant financial relationships to disclose.

Published

2007

47. Src kinase activity in early breast cancer (EBC): A quantitative luminometric and immunohistochemical (IHC) approach

Author

Vivien Jacobs, M. Fennell, Glen Clack, J M Dixon, Robert Jones, Tim P. Green, A. Marshall, and O. Young

Subjects

Cancer Research, Pathology, medicine.medical_specialty, business.industry, medicine.disease, Breast cancer, Oncology, Cancer cell, Cancer research, medicine, Immunohistochemistry, business, Proto-oncogene tyrosine-protein kinase Src, Early breast cancer

Abstract

13010 Background: Src kinase expression and activity is increased in many solid tumors including breast cancer, and Src kinase has a role in the regulation of cancer cell invasion. Thus, Src kinase is a potential therapeutic target. Targeting cancer cell invasion may be of particular value in early disease, although drug effects are unlikely to be measurable by conventional endpoints, for example tumor regression. This prospective study aimed to establish robust measures of Src activity in invasion-related pathways in tissue derived from EBC and to assess the variability between these measures, in order to establish a methodology for pharmacodynamic assessment of Src inhibition in clinical disease. Methods: Duplicate sets of core biopsies were taken from 30 patients, both at diagnosis and surgery. Biopsies were fixed immediately in either liquid nitrogen (luminometric analysis) or pre-cooled isopentane (IHC analysis). Formalin-fixed, paraffin-embedded tissue (FFPET) was also collected at the time of diagnosis. Levels of phospho-paxillin, phospho-focal adhesion kinase (FAK), total phosphotyrosine and total paxillin were measured in lysed tumor tissue using the Luminex system. Expression of activated Src, phospho-paxillin, phospho-FAK, total paxillin and total FAK was determined in sections of frozen tissue and FFPET, and assessed semi-quantitatively by visual examination. An analysis of variance (ANOVA) model was fitted to the Luminex data ( Table ). Results: All tumors expressed active Src, and there was a high level of expression, but low variability, of paxillin, FAK, phospho-paxillin and phospho-FAK. The subcellular localization of these markers could also be assessed in FFPET sections. Conclusion: The results indicate the feasibility of assessing the effect of a Src inhibitor on invasion-related endpoints in women awaiting surgery for EBC. [Table: see text] [Table: see text]

Published

2006

48. The letrozole (L), exemestane (E), and anastrozole (A) pharmacodynamics (LEAP) trial: A direct comparison of bone biochemical measurements between aromatase inhibitors (AIs) in healthy postmenopausal women

Author

Glen Clack, Eugene V. McCloskey, A. Miyamoto, G. Lakner, Rosemary A. Hannon, and R. Eastell

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Postmenopausal women, biology, business.industry, Letrozole, Anastrozole, Pharmacology, chemistry.chemical_compound, Pharmacodynamic Study, Exemestane, chemistry, Internal medicine, Pharmacodynamics, medicine, biology.protein, Aromatase, business, Serum markers, medicine.drug

Abstract

555 Background: The LEAP trial is an open, randomized, multicenter, Phase I pharmacodynamic study comparing the effects of the AIs L, E and A on safety parameters, such as serum markers of bone formation and resorption, lipid profiles, and adrenal function in healthy postmenopausal women with normal bone mineral density at the spine and hip. Elevated bone biochemical levels indicate high turnover of bone, and correlate with a loss in bone mineral density. It has been suggested that there are differences between the effect of the steroidal AIs (E) and non-steroidal AIs (A and L) on bone turnover, with steroidal AIs having a less negative effect. Methods: Healthy volunteersfrom the UK and Hungarywere randomized to receive A (1 mg/day), L (2.5 mg/day), or E (25 mg/day) orally, once daily for 24 weeks. Changes from baseline in log-transformed bone alkaline phosphatase (ALP), serum C-telopeptide crosslinks (CTX), parathyroid hormone (PTH) and propeptide of type I procollagen (PINP) at 24 weeks on A, were compared with those on L and E by ANCOVA, adjusting for treatment, baseline measurement, BMI, smoking status and baseline estradiol. No adjustments were made for multiple comparisons. Results: A total of 102 healthy volunteers were recruited, with 90 participants evaluable at 24 weeks (29 A, 29 L, 32 E). Participant demographics were similar between the treatment groups in terms of age, years since menopause, and history of hysterectomy and oophorectomy. Bone biochemical measurement changes are presented in the table . With the exception of PTH, where there is a greater decrease in PTH with E than with A (p=0.04), there were no statistically significant differences between the AIs. Conclusions: The steroidal and non-steroidal AIs appear to have similar effects on bone biochemical measurements, and thus bone turnover. All three licensed AIs result in increases in bone turnover. [Table: see text] [Table: see text]

Published

2006

49. Phase I ascending single and multiple dose studies to assess the safety, tolerability and pharmacokinetics of AZD0530, a highly selective, dual-specific Src-Abl inhibitor

Author

A. L. Marshall, Glen Clack, M. Macpherson, N. J. Gallagher, Roger B. H. Tootell, D. Smethurst, and J. A. Lockton

Subjects

Cancer Research, ABL, business.industry, Safety tolerability, Pharmacology, Multiple dose, Highly selective, Small molecule, Oncology, Pharmacokinetics, hemic and lymphatic diseases, Medicine, business, Proto-oncogene tyrosine-protein kinase Src

Abstract

3125 Background: AZD0530 is a highly selective, dual-specific, orally available, small molecule inhibitor of Src kinase and Bcr-Abl. Methods: Two studies were conducted in healthy male volunteers t...

Published

2005

50. The effect of AZD0530, a highly selective, orally available Src/Abl kinase inhibitor, on biomarkers of bone resorption in healthy males

Author

M. Macpherson, A. L. Marshall, Glen Clack, Rosemary A. Hannon, R. Eastell, and N. J. Gallagher

Subjects

Cancer Research, ABL, business.industry, Kinase, Cell growth, Adhesion, Highly selective, Small molecule, Bone resorption, Oncology, hemic and lymphatic diseases, Cancer research, Medicine, business, Proto-oncogene tyrosine-protein kinase Src

Abstract

3041 Background: AZD0530 is a highly selective, dual-specific, orally available small molecule inhibitor of Src kinase and Bcr-Abl. Src kinase activity modulates cell proliferation, adhesion, motil...

Published

2005