Process Innovation Improves Trial Operation Efficiency

Background: Despite the fact that unaddressed delays in clinical trial operation could severely compromise the overall effort invested, there seems to be a lack of concerted effort in reforming such delays. This study evaluated the composite effect of initiatives in reforming trial operation efficie...

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Published in	Therapeutic innovation & regulatory science Vol. 50; no. 4; pp. 510 - 514
Main Authors	Choi, Yun Jung, Kim, Kyu-pyo, Park, Sumi, Park, MiYeon, Kim, Sulhwa, Kim, Younkyoung, Bae, Kyun-Seop, Beck, Sung-Ho, Choi, Ki-Eun, Chung, Jong Woo, Lim, Young–Suk, Kim, Tae Won
Format	Journal Article
Language	English
Published	Los Angeles, CA SAGE Publications 01.07.2016 Springer International Publishing Springer Nature B.V
Subjects	Accreditation Authorship Biomedical research Clinical trials Drug Safety and Pharmacovigilance Efficiency Informed consent Initiatives Pharmacotherapy Pharmacy Product Development and Innovation: Original Research Review boards Risk management Studies United States > US preliminary review project manager clinical trial operation clinical trial activation clinical trial timeline
Online Access	Get full text
ISSN	2168-4790 2168-4804 2168-4804
DOI	10.1177/2168479016634148

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Abstract	Background: Despite the fact that unaddressed delays in clinical trial operation could severely compromise the overall effort invested, there seems to be a lack of concerted effort in reforming such delays. This study evaluated the composite effect of initiatives in reforming trial operation efficiency. Methods: A high-volume academic medical center in Korea has implemented various initiatives to improve the trial operation efficiency by expediting times from institutional review board (IRB) submission to approval, from IRB submission to trial open for subject enrollment, and from trial open to first patient-in. The initiatives include implementation of the protocol preliminary review, parallel processing of the clinical trial agreement review in line with the protocol submission to the IRB, and involvement of project manager for operational risk management. Times from IRB submission to approval, from IRB submission to trial open, and from trial open to first patient-in before and after implementation of initiatives were compared. Results: The median time required in IRB approval was meaningfully shorter in the postinitiative group (19 vs 14 days; P < .001). The median times from IRB submission to trial open for subject enrollment and from trial open to first patient-in were reduced significantly in the postinitiative group (trial open: 25 vs 18 days, P < .001; first patient-in: 111.5 vs 100 days, P = .014). Conclusions: The initiatives were effective in reforming trial operational efficiency. Additional studies to address the cause of operational delay and modifiable factors influencing subject enrollment are needed to further improve operational efficiency.
AbstractList	Background: Despite the fact that unaddressed delays in clinical trial operation could severely compromise the overall effort invested, there seems to be a lack of concerted effort in reforming such delays. This study evaluated the composite effect of initiatives in reforming trial operation efficiency. Methods: A high-volume academic medical center in Korea has implemented various initiatives to improve the trial operation efficiency by expediting times from institutional review board (IRB) submission to approval, from IRB submission to trial open for subject enrollment, and from trial open to first patient-in. The initiatives include implementation of the protocol preliminary review, parallel processing of the clinical trial agreement review in line with the protocol submission to the IRB, and involvement of project manager for operational risk management. Times from IRB submission to approval, from IRB submission to trial open, and from trial open to first patient-in before and after implementation of initiatives were compared. Results: The median time required in IRB approval was meaningfully shorter in the postinitiative group (19 vs 14 days; P < .001). The median times from IRB submission to trial open for subject enrollment and from trial open to first patient-in were reduced significantly in the postinitiative group (trial open: 25 vs 18 days, P < .001; first patient-in: 111.5 vs 100 days, P = .014). Conclusions: The initiatives were effective in reforming trial operational efficiency. Additional studies to address the cause of operational delay and modifiable factors influencing subject enrollment are needed to further improve operational efficiency. Background: Despite the fact that unaddressed delays in clinical trial operation could severely compromise the overall effort invested, there seems to be a lack of concerted effort in reforming such delays. This study evaluated the composite effect of initiatives in reforming trial operation efficiency. Methods: A high-volume academic medical center in Korea has implemented various initiatives to improve the trial operation efficiency by expediting times from institutional review board (IRB) submission to approval, from IRB submission to trial open for subject enrollment, and from trial open to first patient-in. The initiatives include implementation of the protocol preliminary review, parallel processing of the clinical trial agreement review in line with the protocol submission to the IRB, and involvement of project manager for operational risk management. Times from IRB submission to approval, from IRB submission to trial open, and from trial open to first patient-in before and after implementation of initiatives were compared. Results: The median time required in IRB approval was meaningfully shorter in the postinitiative group (19 vs 14 days; P < .001). The median times from IRB submission to trial open for subject enrollment and from trial open to first patient-in were reduced significantly in the postinitiative group (trial open: 25 vs 18 days, P < .001; first patient-in: 111.5 vs 100 days, P = .014). Conclusions: The initiatives were effective in reforming trial operational efficiency. Additional studies to address the cause of operational delay and modifiable factors influencing subject enrollment are needed to further improve operational efficiency. This study evaluated the composite effect of initiatives in reforming trial operation efficiency. A high-volume academic medical center in Korea has implemented various initiatives to improve the trial operation efficiency by expediting times from institutional review board (IRB) submission to approval, from IRB submission to trial open for subject enrollment, and from trial open to first patient-in. The initiatives include implementation of the protocol preliminary review, parallel processing of the clinical trial agreement review in line with the protocol submission to the IRS, and involvement of project manager for operational risk management. Times from IRB submission to approval, from IRB submission to trial open, and from trial open to first patient-in before and after implementation of initiatives were compared. Results: The median time required in IRS approval was meaningfully shorter in the postinitiative group (19 vs 14 days; PC .00 I). The median times from IRS submission to trial open for subject enrollment and from trial open to first patient-in were reduced significantly in the postinitiative group. Background Despite the fact that unaddressed delays in clinical trial operation could severely compromise the overall effort invested, there seems to be a lack of concerted effort in reforming such delays. This study evaluated the composite effect of initiatives in reforming trial operation efficiency. Methods A high-volume academic medical center in Korea has implemented various initiatives to improve the trial operation efficiency by expediting times from institutional review board (IRB) submission to approval, from IRB submission to trial open for subject enrollment, and from trial open to first patient-in. The initiatives include implementation of the protocol preliminary review, parallel processing of the clinical trial agreement review in line with the protocol submission to the IRB, and involvement of project manager for operational risk management. Times from IRB submission to approval, from IRB submission to trial open, and from trial open to first patient-in before and after implementation of initiatives were compared. Results The median time required in IRB approval was meaningfully shorter in the postinitiative group (19 vs 14 days; P <.001). The median times from IRB submission to trial open for subject enrollment and from trial open to first patient-in were reduced significantly in the postinitiative group (trial open: 25 vs 18 days, P <.001; first patient-in: 111.5 vs 100 days, P =.014). Conclusions The initiatives were effective in reforming trial operational efficiency. Additional studies to address the cause of operational delay and modifiable factors influencing subject enrollment are needed to further improve operational efficiency. Despite the fact that unaddressed delays in clinical trial operation could severely compromise the overall effort invested, there seems to be a lack of concerted effort in reforming such delays. This study evaluated the composite effect of initiatives in reforming trial operation efficiency.BACKGROUNDDespite the fact that unaddressed delays in clinical trial operation could severely compromise the overall effort invested, there seems to be a lack of concerted effort in reforming such delays. This study evaluated the composite effect of initiatives in reforming trial operation efficiency.A high-volume academic medical center in Korea has implemented various initiatives to improve the trial operation efficiency by expediting times from institutional review board (IRB) submission to approval, from IRB submission to trial open for subject enrollment, and from trial open to first patient-in. The initiatives include implementation of the protocol preliminary review, parallel processing of the clinical trial agreement review in line with the protocol submission to the IRB, and involvement of project manager for operational risk management. Times from IRB submission to approval, from IRB submission to trial open, and from trial open to first patient-in before and after implementation of initiatives were compared.METHODSA high-volume academic medical center in Korea has implemented various initiatives to improve the trial operation efficiency by expediting times from institutional review board (IRB) submission to approval, from IRB submission to trial open for subject enrollment, and from trial open to first patient-in. The initiatives include implementation of the protocol preliminary review, parallel processing of the clinical trial agreement review in line with the protocol submission to the IRB, and involvement of project manager for operational risk management. Times from IRB submission to approval, from IRB submission to trial open, and from trial open to first patient-in before and after implementation of initiatives were compared.The median time required in IRB approval was meaningfully shorter in the postinitiative group (19 vs 14 days; P < .001). The median times from IRB submission to trial open for subject enrollment and from trial open to first patient-in were reduced significantly in the postinitiative group (trial open: 25 vs 18 days, P < .001; first patient-in: 111.5 vs 100 days, P = .014).RESULTSThe median time required in IRB approval was meaningfully shorter in the postinitiative group (19 vs 14 days; P < .001). The median times from IRB submission to trial open for subject enrollment and from trial open to first patient-in were reduced significantly in the postinitiative group (trial open: 25 vs 18 days, P < .001; first patient-in: 111.5 vs 100 days, P = .014).The initiatives were effective in reforming trial operational efficiency. Additional studies to address the cause of operational delay and modifiable factors influencing subject enrollment are needed to further improve operational efficiency.CONCLUSIONSThe initiatives were effective in reforming trial operational efficiency. Additional studies to address the cause of operational delay and modifiable factors influencing subject enrollment are needed to further improve operational efficiency. Despite the fact that unaddressed delays in clinical trial operation could severely compromise the overall effort invested, there seems to be a lack of concerted effort in reforming such delays. This study evaluated the composite effect of initiatives in reforming trial operation efficiency. A high-volume academic medical center in Korea has implemented various initiatives to improve the trial operation efficiency by expediting times from institutional review board (IRB) submission to approval, from IRB submission to trial open for subject enrollment, and from trial open to first patient-in. The initiatives include implementation of the protocol preliminary review, parallel processing of the clinical trial agreement review in line with the protocol submission to the IRB, and involvement of project manager for operational risk management. Times from IRB submission to approval, from IRB submission to trial open, and from trial open to first patient-in before and after implementation of initiatives were compared. The median time required in IRB approval was meaningfully shorter in the postinitiative group (19 vs 14 days; P < .001). The median times from IRB submission to trial open for subject enrollment and from trial open to first patient-in were reduced significantly in the postinitiative group (trial open: 25 vs 18 days, P < .001; first patient-in: 111.5 vs 100 days, P = .014). The initiatives were effective in reforming trial operational efficiency. Additional studies to address the cause of operational delay and modifiable factors influencing subject enrollment are needed to further improve operational efficiency.
Author	Choi, Yun Jung Kim, Kyu-pyo Choi, Ki-Eun Kim, Sulhwa Kim, Younkyoung Chung, Jong Woo Lim, Young–Suk Park, MiYeon Beck, Sung-Ho Kim, Tae Won Park, Sumi Bae, Kyun-Seop
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References	Choi, Jeon, Kim 2015; 49 Abrams, Mooney, Zwiebel 2013; 105 Glickman, McHutchison, Peterson 2009; 360 Cheng, Dietrich, Dilts 2010; 16 Dilts, Sandler 2006; 24 Getz, Wenger, Campo, Seguine, Kaitin 2008; 15 Dilts, Sandler, Cheng 2009; 27 Dilts, Sandler (CR4) 2006; 24 Abrams, Mooney, Zwiebel (CR1) 2013; 105 CR5 Cheng, Dietrich, Dilts (CR2) 2010; 16 Getz, Wenger, Campo, Seguine, Kaitin (CR3) 2008; 15 Choi, Jeon, Kim (CR7) 2015; 49 Glickman, McHutchison, Peterson (CR8) 2009; 360 Dilts, Sandler, Cheng (CR6) 2009; 27 YJ Choi (50040510_CR7) 2015; 49 SW Glickman (50040510_CR8) 2009; 360 KA Getz (50040510_CR3) 2008; 15 DM Dilts (50040510_CR6) 2009; 27 JS Abrams (50040510_CR1) 2013; 105 DM Dilts (50040510_CR4) 2006; 24 SK Cheng (50040510_CR2) 2010; 16 50040510_CR5
References_xml	– volume: 24 start-page: 4545 year: 2006 end-page: 4552 article-title: Invisible barriers to clinical trials: the impact of structural, infrastructural, and procedural barriers to opening oncology clinical trials publication-title: J Clin Oncol – volume: 360 start-page: 816 year: 2009 end-page: 823 article-title: Ethical and scientific implications of the globalization of clinical research publication-title: N Engl J Med – volume: 105 start-page: 954 year: 2013 end-page: 959 article-title: Implementation of timeline reforms speeds initiation of National Cancer Institute-sponsored trials publication-title: J Natl Cancer Inst – volume: 27 start-page: 1761 year: 2009 end-page: 1766 article-title: Steps and time to process clinical trials at the Cancer Therapy Evaluation Program publication-title: J Clin Oncol – volume: 49 start-page: 234 year: 2015 end-page: 238 article-title: A trial activation initiative to accelerate trial opening in an academic medical center publication-title: Therapeutic Innovation & Regulatory Science – volume: 16 start-page: 5557 year: 2010 end-page: 5563 article-title: A sense of urgency: evaluating the link between clinical trial development time and the accrual performance of Cancer Therapy Evaluation Program (NCI-CTEP) sponsored studies publication-title: Clin Cancer Res – volume: 15 start-page: 450 year: 2008 end-page: 457 article-title: Assessing the impact of protocol design changes on clinical trial performance publication-title: Am J Ther – volume: 360 start-page: 816 year: 2009 end-page: 823 ident: CR8 article-title: Ethical and scientific implications of the globalization of clinical research publication-title: N Engl J Med doi: 10.1056/NEJMsb0803929 – volume: 105 start-page: 954 year: 2013 end-page: 959 ident: CR1 article-title: Implementation of timeline reforms speeds initiation of National Cancer Institute-sponsored trials publication-title: J Natl Cancer Inst doi: 10.1093/jnci/djt137 – ident: CR5 – volume: 16 start-page: 5557 year: 2010 end-page: 5563 ident: CR2 article-title: A sense of urgency: evaluating the link between clinical trial development time and the accrual performance of Cancer Therapy Evaluation Program (NCI-CTEP) sponsored studies publication-title: Clin Cancer Res doi: 10.1158/1078-0432.CCR-10-0133 – volume: 27 start-page: 1761 year: 2009 end-page: 1766 ident: CR6 article-title: Steps and time to process clinical trials at the Cancer Therapy Evaluation Program publication-title: J Clin Oncol doi: 10.1200/JCO.2008.19.9133 – volume: 49 start-page: 234 year: 2015 end-page: 238 ident: CR7 article-title: A trial activation initiative to accelerate trial opening in an academic medical center publication-title: Therapeutic Innovation & Regulatory Science doi: 10.1177/2168479014554399 – volume: 24 start-page: 4545 year: 2006 end-page: 4552 ident: CR4 article-title: Invisible barriers to clinical trials: the impact of structural, infrastructural, and procedural barriers to opening oncology clinical trials publication-title: J Clin Oncol doi: 10.1200/JCO.2005.05.0104 – volume: 15 start-page: 450 year: 2008 end-page: 457 ident: CR3 article-title: Assessing the impact of protocol design changes on clinical trial performance publication-title: Am J Ther doi: 10.1097/MJT.0b013e31816b9027 – volume: 105 start-page: 954 year: 2013 ident: 50040510_CR1 publication-title: J Natl Cancer Inst doi: 10.1093/jnci/djt137 – volume: 16 start-page: 5557 year: 2010 ident: 50040510_CR2 publication-title: Clin Cancer Res doi: 10.1158/1078-0432.CCR-10-0133 – volume: 49 start-page: 234 year: 2015 ident: 50040510_CR7 publication-title: Therapeutic Innovation & Regulatory Science doi: 10.1177/2168479014554399 – ident: 50040510_CR5 – volume: 24 start-page: 4545 year: 2006 ident: 50040510_CR4 publication-title: J Clin Oncol doi: 10.1200/JCO.2005.05.0104 – volume: 27 start-page: 1761 year: 2009 ident: 50040510_CR6 publication-title: J Clin Oncol doi: 10.1200/JCO.2008.19.9133 – volume: 360 start-page: 816 year: 2009 ident: 50040510_CR8 publication-title: N Engl J Med doi: 10.1056/NEJMsb0803929 – volume: 15 start-page: 450 year: 2008 ident: 50040510_CR3 publication-title: Am J Ther doi: 10.1097/MJT.0b013e31816b9027
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Snippet	Background: Despite the fact that unaddressed delays in clinical trial operation could severely compromise the overall effort invested, there seems to be a... Background Despite the fact that unaddressed delays in clinical trial operation could severely compromise the overall effort invested, there seems to be a lack... Despite the fact that unaddressed delays in clinical trial operation could severely compromise the overall effort invested, there seems to be a lack of... This study evaluated the composite effect of initiatives in reforming trial operation efficiency. A high-volume academic medical center in Korea has... Background: Despite the fact that unaddressed delays in clinical trial operation could severely compromise the overall effort invested, there seems to be a...
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Title	Process Innovation Improves Trial Operation Efficiency
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