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Title:
AZD3514, an oral selective androgen receptor down-regulator in patients with castration-resistant prostate cancer – results of two parallel first-in-human phase I studies | Investigational New Drugs
Description:
Background AZD3514 is a first-in-class, orally bio-available, androgen-dependent and -independent androgen receptor inhibitor and selective androgen-receptor down-regulator (SARD). Methods In study 1 and 2, castration-resistant prostate cancer (CRPC) patients (pts) were initially recruited into a once daily (QD) oral schedule (A). In study 1, pharmacokinetic assessments led to twice daily (BID) dosing (schedule B) to increase exposure. Study 2 explored a once daily schedule. Results In study 1, 49 pts were 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 1000 mg QD. 2000 mg BID was considered non-tolerable due to grade (G) 2 toxicities (nausea [N], vomiting [V]). No adverse events (AEs) met the dose-limiting toxicity (DLT) definition. Thirteen pts received AZD3514 in study 2, with starting doses of 250 mg QD. The most frequent drug-related AEs were N: G1/2 in 55/70 pts (79 %); G3 in 1 pt (1.4 %); & V: G1/2 in 34/70 pts (49 %) & G3 in 1 pt (1.4 %). PSA declines (≥50 %) were documented in 9/70 patients (13 %). Objective soft tissue responses per RECIST1.1 were observed in 4/24 (17 %) pts in study 1. Conclusion AZD3514 has moderate anti-tumour activity in pts with advanced CRPC but with significant levels of nausea and vomiting. However, anti-tumour activity as judged by significant PSA declines, objective responses and durable disease stabilisations, provides the rationale for future development of SARD compounds.
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Keywords {🔍}
cancer, prostate, article, google, scholar, pubmed, receptor, androgen, research, castrationresistant, azd, study, astrazeneca, patients, bono, metastatic, clin, cas, pts, abiraterone, central, enzalutamide, oncol, phase, med, jones, res, activity, access, resistance, grant, astellas, janssen, privacy, cookies, content, downregulator, chemotherapy, fizazi, scher, engl, doinejmoa, eur, sanofi, institute, publish, search, drugs, selective, results,
Topics {✒️}
castration-resistant prostate cancer month download article/chapter frequent drug-related aes moderate anti-tumour activity metastatic prostate cancer overcoming mutation-based resistance selective androgen-receptor prostate cancer foundation androgen-directed therapy full article pdf anti-tumour activity dna binding domain mutant androgen receptor related subjects bradbury rh progressive prostate cancer treating prostate cancer advanced prostate cancer prostate cancer uk privacy choices/manage cookies drug development unit loddick sa cancer cell 16 full-length receptor akt inhibitor azd5363 scotland cancer centre rational drug design biomedical research grant cancer research uk beer tm swiss cancer league article investigational de bono js kitasato university school clin cancer res androgen receptor netherlands cancer institute european economic area scope submit manuscript pharmacokinetic assessments led dose-limiting toxicity durable disease stabilisations anti-tumor activity steroid hormone receptors goodman ob jr response evaluation criteria revised recist guideline tumor cells circulate ken-ichi tabata received consulting fees
Questions {❓}
- Attard G, Cooper CS, de Bono JS (2009) Steroid hormone receptors in prostate cancer: a hard habit to break?
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headline:AZD3514, an oral selective androgen receptor down-regulator in patients with castration-resistant prostate cancer – results of two parallel first-in-human phase I studies
description:
Background AZD3514 is a first-in-class, orally bio-available, androgen-dependent and -independent androgen receptor inhibitor and selective androgen-receptor down-regulator (SARD). Methods In study 1 and 2, castration-resistant prostate cancer (CRPC) patients (pts) were initially recruited into a once daily (QD) oral schedule (A). In study 1, pharmacokinetic assessments led to twice daily (BID) dosing (schedule B) to increase exposure. Study 2 explored a once daily schedule. Results In study 1, 49 pts were 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 1000 mg QD. 2000 mg BID was considered non-tolerable due to grade (G) 2 toxicities (nausea [N], vomiting [V]). No adverse events (AEs) met the dose-limiting toxicity (DLT) definition. Thirteen pts received AZD3514 in study 2, with starting doses of 250 mg QD. The most frequent drug-related AEs were N: G1/2 in 55/70 pts (79 %); G3 in 1 pt (1.4 %); & V: G1/2 in 34/70 pts (49 %) & G3 in 1 pt (1.4 %). PSA declines (≥50 %) were documented in 9/70 patients (13 %). Objective soft tissue responses per RECIST1.1 were observed in 4/24 (17 %) pts in study 1. Conclusion AZD3514 has moderate anti-tumour activity in pts with advanced CRPC but with significant levels of nausea and vomiting. However, anti-tumour activity as judged by significant PSA declines, objective responses and durable disease stabilisations, provides the rationale for future development of SARD compounds.
datePublished:2015-04-30T00:00:00Z
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keywords:
(5) Castration-resistant prostate cancer
Phase I
First-in-human
AZD3514
Selective androgen receptor down-regulator
Oncology
Pharmacology/Toxicology
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headline:AZD3514, an oral selective androgen receptor down-regulator in patients with castration-resistant prostate cancer – results of two parallel first-in-human phase I studies
description:
Background AZD3514 is a first-in-class, orally bio-available, androgen-dependent and -independent androgen receptor inhibitor and selective androgen-receptor down-regulator (SARD). Methods In study 1 and 2, castration-resistant prostate cancer (CRPC) patients (pts) were initially recruited into a once daily (QD) oral schedule (A). In study 1, pharmacokinetic assessments led to twice daily (BID) dosing (schedule B) to increase exposure. Study 2 explored a once daily schedule. Results In study 1, 49 pts were 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 1000 mg QD. 2000 mg BID was considered non-tolerable due to grade (G) 2 toxicities (nausea [N], vomiting [V]). No adverse events (AEs) met the dose-limiting toxicity (DLT) definition. Thirteen pts received AZD3514 in study 2, with starting doses of 250 mg QD. The most frequent drug-related AEs were N: G1/2 in 55/70 pts (79 %); G3 in 1 pt (1.4 %); & V: G1/2 in 34/70 pts (49 %) & G3 in 1 pt (1.4 %). PSA declines (≥50 %) were documented in 9/70 patients (13 %). Objective soft tissue responses per RECIST1.1 were observed in 4/24 (17 %) pts in study 1. Conclusion AZD3514 has moderate anti-tumour activity in pts with advanced CRPC but with significant levels of nausea and vomiting. However, anti-tumour activity as judged by significant PSA declines, objective responses and durable disease stabilisations, provides the rationale for future development of SARD compounds.
datePublished:2015-04-30T00:00:00Z
dateModified:2015-04-30T00:00:00Z
pageStart:679
pageEnd:690
sameAs:https://doi.org/10.1007/s10637-015-0235-5
keywords:
(5) Castration-resistant prostate cancer
Phase I
First-in-human
AZD3514
Selective androgen receptor down-regulator
Oncology
Pharmacology/Toxicology
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type:Organization
name:M. Niwakawa
affiliation:
name:Shizuoka Cancer Center Hospital
address:
name:Division of Urology, Shizuoka Cancer Center Hospital, Shizuoka, Japan
type:PostalAddress
type:Organization
name:S. A. Smith
affiliation:
name:AstraZeneca
address:
name:AstraZeneca, Macclesfield, UK
type:PostalAddress
type:Organization
name:J. Graham
affiliation:
name:The Beatson West of Scotland Cancer Centre
address:
name:The Beatson West of Scotland Cancer Centre, Glasgow, UK
type:PostalAddress
type:Organization
name:M. Ong
affiliation:
name:The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research
address:
name:Prostate Targeted Therapy Group and Drug Development Unit, The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research, Sutton, UK
type:PostalAddress
type:Organization
name:R. D. Finkelman
affiliation:
name:AstraZeneca
address:
name:AstraZeneca, Wilmington, USA
type:PostalAddress
type:Organization
name:J. H. M. Schellens
affiliation:
name:The Netherlands Cancer Institute
address:
name:The Netherlands Cancer Institute, Amsterdam, The Netherlands
type:PostalAddress
type:Organization
name:Utrecht Institute for Pharmaceutical Sciences (UIPS)
address:
name:Utrecht Institute for Pharmaceutical Sciences (UIPS), Utrecht, The Netherlands
type:PostalAddress
type:Organization
name:A. Zivi
affiliation:
name:The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research
address:
name:Prostate Targeted Therapy Group and Drug Development Unit, The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research, Sutton, UK
type:PostalAddress
type:Organization
name:M. Crespo
affiliation:
name:The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research
address:
name:Prostate Targeted Therapy Group and Drug Development Unit, The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research, Sutton, UK
type:PostalAddress
type:Organization
name:R. Riisnaes
affiliation:
name:The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research
address:
name:Prostate Targeted Therapy Group and Drug Development Unit, The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research, Sutton, UK
type:PostalAddress
type:Organization
name:D. Nava-Rodrigues
affiliation:
name:The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research
address:
name:Prostate Targeted Therapy Group and Drug Development Unit, The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research, Sutton, UK
type:PostalAddress
type:Organization
name:M. D. Malone
affiliation:
name:AstraZeneca
address:
name:AstraZeneca, Macclesfield, UK
type:PostalAddress
type:Organization
name:C. Dive
affiliation:
name:Cancer Research UK Manchester Institute
address:
name:Cancer Research UK Manchester Institute, Manchester, UK
type:PostalAddress
type:Organization
name:R. Sloane
affiliation:
name:Cancer Research UK Manchester Institute
address:
name:Cancer Research UK Manchester Institute, Manchester, UK
type:PostalAddress
type:Organization
name:D. Moore
affiliation:
name:Cancer Research UK Manchester Institute
address:
name:Cancer Research UK Manchester Institute, Manchester, UK
type:PostalAddress
type:Organization
name:J. J. Alumkal
affiliation:
name:Knight Cancer Institute at Oregon Health & Science University
address:
name:Knight Cancer Institute at Oregon Health & Science University, Oregon, USA
type:PostalAddress
type:Organization
name:A. Dymond
affiliation:
name:AstraZeneca
address:
name:AstraZeneca, Macclesfield, UK
type:PostalAddress
type:Organization
name:P. A. Dickinson
affiliation:
name:AstraZeneca
address:
name:AstraZeneca, Macclesfield, UK
type:PostalAddress
type:Organization
name:M. Ranson
affiliation:
name:The Christie NHS Foundation Trust
address:
name:The Christie NHS Foundation Trust, Manchester, UK
type:PostalAddress
type:Organization
name:G. Clack
affiliation:
name:AstraZeneca
address:
name:AstraZeneca, Macclesfield, UK
type:PostalAddress
type:Organization
name:J. de Bono
affiliation:
name:The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research
address:
name:Prostate Targeted Therapy Group and Drug Development Unit, The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research, Sutton, UK
type:PostalAddress
type:Organization
name:T. Elliott
affiliation:
name:The Christie NHS Foundation Trust
address:
name:The Christie NHS Foundation Trust, Manchester, UK
type:PostalAddress
type:Organization
email:[email protected]
PostalAddress:
name:Prostate Targeted Therapy Group and Drug Development Unit, The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research, Sutton, UK
name:The Beatson West of Scotland Cancer Centre, Glasgow, UK
name:The Netherlands Cancer Institute, Amsterdam, The Netherlands
name:Department of Urology, Kitasato University School of Medicine, Sagamihara, Japan
name:Division of Urology, Shizuoka Cancer Center Hospital, Shizuoka, Japan
name:AstraZeneca, Macclesfield, UK
name:The Beatson West of Scotland Cancer Centre, Glasgow, UK
name:Prostate Targeted Therapy Group and Drug Development Unit, The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research, Sutton, UK
name:AstraZeneca, Wilmington, USA
name:The Netherlands Cancer Institute, Amsterdam, The Netherlands
name:Utrecht Institute for Pharmaceutical Sciences (UIPS), Utrecht, The Netherlands
name:Prostate Targeted Therapy Group and Drug Development Unit, The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research, Sutton, UK
name:Prostate Targeted Therapy Group and Drug Development Unit, The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research, Sutton, UK
name:Prostate Targeted Therapy Group and Drug Development Unit, The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research, Sutton, UK
name:Prostate Targeted Therapy Group and Drug Development Unit, The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research, Sutton, UK
name:AstraZeneca, Macclesfield, UK
name:Cancer Research UK Manchester Institute, Manchester, UK
name:Cancer Research UK Manchester Institute, Manchester, UK
name:Cancer Research UK Manchester Institute, Manchester, UK
name:Knight Cancer Institute at Oregon Health & Science University, Oregon, USA
name:AstraZeneca, Macclesfield, UK
name:AstraZeneca, Macclesfield, UK
name:The Christie NHS Foundation Trust, Manchester, UK
name:AstraZeneca, Macclesfield, UK
name:Prostate Targeted Therapy Group and Drug Development Unit, The Royal Marsden NHS Foundation Trust and The Institute of Cancer Research, Sutton, UK
name:The Christie NHS Foundation Trust, Manchester, UK
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