@article{abdfd29a449441d9bb876bcb12d69b40,
title = "High-dose vitamin D supplementation to prevent prostate cancer progression in localised cases with low-to-intermediate risk of progression on active surveillance (ProsD): Protocol of a phase II randomised controlled trial",
abstract = "Introduction:Active surveillance (AS) for patients with prostate cancer (PC) with low risk of PC death is an alternative to radical treatment. A major drawback of AS is the uncertainty whether a patient truly has low risk PC based on biopsy alone. Multiparametric MRI scan together with biopsy, appears useful in separating patients who need curative therapy from those for whom AS may be safe. Two small clinical trials have shown short-term high-dose vitamin D supplementation may prevent PC progression. There is no substantial evidence for its long-term safety and efficacy, hence its use in the care of men with PC on AS needs assessment. This protocol describes the ProsD clinical trial which aims to determine if oral high-dose vitamin D supplementation taken monthly for 2 years can prevent PC progression in cases with low-to-intermediate risk of progression. Method and analysis:This is an Australian national multicentre, 2:1 double-blinded placebo-controlled phase II randomised controlled trial of monthly oral high-dose vitamin D supplementation (50 000 IU cholecalciferol), in men diagnosed with localised PC who have low-to-intermediate risk of disease progression and are being managed by AS. This trial will assess the feasibility, efficacy and safety of supplementing men with an initial oral loading dose of 500 000 IU cholecalciferol, followed by a monthly oral dose of 50 000 IU during the 24 months of AS. The primary trial outcome is the commencement of active therapy for clinical or non-clinical reason, within 2 years of AS. ",
author = "Visalini Nair-Shalliker and Smith, {David P.} and Val Gebski and Patel, {Manish I.} and Mark Frydenberg and Yaxley, {John W.} and Robert Gardiner and David Espinoza and Kimlin, {Michael G.} and Michael Fenech and David Gillatt and Henry Woo and Armstrong, {Bruce K.} and Krishan Rasiah and Nader Awad and James Symons and Howard Gurney",
note = "Funding Information: Contributors HG is the principal investigator of ProsD. VN-S, MiF and BKA conceived the initial concept of this trial and in conjunction with HG, DPS, MIP, JWY, MaF, DG, RG and MGK developed the rationale for this trial. VN-S and HG led the development of the trial protocol and drafted this manuscript. VN-S and DPS were involved in coordinating all aspects of this trial, data collection and management. VG and DE were responsible for the statistical design of the trial, protocol development and setup the IVRS system for blinding and randomising participants. MiF was responsible for the processing of all blood specimens and undertaking the genome damage assays. MIP, MaF, JWY, DG, HW, KR, NA and JS contributed to recruiting high volume of participants to this trial. All authors have contributed to the development of the study protocol and this manuscript. Funding This work was funded by the Movember Clinical Trials Award and administered through the Prostate Cancer Foundation Australia (CTA1315). Competing interests None declared. Publisher Copyright: {\textcopyright} BMJ Publishing Group Limited 2021",
year = "2021",
month = mar,
day = "2",
doi = "10.1136/bmjopen-2020-044055",
language = "English",
volume = "11",
pages = "1--9",
journal = "BMJ Open",
issn = "2044-6055",
publisher = "BMJ Publishing Group",
number = "3",
}