Using systematic data categorisation to quantify the types of data collected in clinical trials: The DataCat project

Evelyn Crowley; Shaun Treweek; Katie Banister; Suzanne Breeman; Lynda Constable; Seonaidh Cotton; Anne Duncan; Adel El Feky; Heidi Gardner; Kirsteen Goodman; Doris Lanz; Alison McDonald; Emma Ogburn; Kath Starr; Natasha Stevens; Marie Valente; Gordon Fernie

doi:10.1186/s13063-020-04388-x

Using systematic data categorisation to quantify the types of data collected in clinical trials: The DataCat project

Evelyn Crowley
, Shaun Treweek
, Katie Banister
, Suzanne Breeman
, Lynda Constable
, Seonaidh Cotton
, Anne Duncan
, Adel El Feky
, Heidi Gardner
, Kirsteen Goodman
, Doris Lanz
, Alison McDonald
, Emma Ogburn
, Kath Starr
, Natasha Stevens
, Marie Valente
, Gordon Fernie

School of Medicine

Research output: Contribution to journal › Article › peer-review

Abstract

Background: Data collection consumes a large proportion of clinical trial resources. Each data item requires time and effort for collection, processing and quality control procedures. In general, more data equals a heavier burden for trial staff and participants. It is also likely to increase costs. Knowing the types of data being collected, and in what proportion, will be helpful to ensure that limited trial resources and participant goodwill are used wisely. Aim: The aim of this study is to categorise the types of data collected across a broad range of trials and assess what proportion of collected data each category represents. Methods: We developed a standard operating procedure to categorise data into primary outcome, secondary outcome and 15 other categories. We categorised all variables collected on trial data collection forms from 18, mainly publicly funded, randomised superiority trials, including trials of an investigational medicinal product and complex interventions. Categorisation was done independently in pairs: one person having in-depth knowledge of the trial, the other independent of the trial. Disagreement was resolved through reference to the trial protocol and discussion, with the project team being consulted if necessary. Key results: Primary outcome data accounted for 5.0% (median)/11.2% (mean) of all data items collected. Secondary outcomes accounted for 39.9% (median)/42.5% (mean) of all data items. Non-outcome data such as participant identifiers and demographic data represented 32.4% (median)/36.5% (mean) of all data items collected. Conclusion: A small proportion of the data collected in our sample of 18 trials was related to the primary outcome. Secondary outcomes accounted for eight times the volume of data as the primary outcome. A substantial amount of data collection is not related to trial outcomes. Trialists should work to make sure that the data they collect are only those essential to support the health and treatment decisions of those whom the trial is designed to inform.

Original language	English
Article number	535
Journal	Trials
Volume	21
Issue number	1
DOIs	https://doi.org/10.1186/s13063-020-04388-x
Publication status	Published - 16 Jun 2020

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Crowley, E., Treweek, S., Banister, K., Breeman, S., Constable, L., Cotton, S., Duncan, A., El Feky, A., Gardner, H., Goodman, K., Lanz, D., McDonald, A., Ogburn, E., Starr, K., Stevens, N., Valente, M., & Fernie, G. (2020). Using systematic data categorisation to quantify the types of data collected in clinical trials: The DataCat project. Trials, 21(1), Article 535. https://doi.org/10.1186/s13063-020-04388-x

@article{680b01374f954352affc73a98d1067b7,

title = "Using systematic data categorisation to quantify the types of data collected in clinical trials: The DataCat project",

abstract = "Background: Data collection consumes a large proportion of clinical trial resources. Each data item requires time and effort for collection, processing and quality control procedures. In general, more data equals a heavier burden for trial staff and participants. It is also likely to increase costs. Knowing the types of data being collected, and in what proportion, will be helpful to ensure that limited trial resources and participant goodwill are used wisely. Aim: The aim of this study is to categorise the types of data collected across a broad range of trials and assess what proportion of collected data each category represents. Methods: We developed a standard operating procedure to categorise data into primary outcome, secondary outcome and 15 other categories. We categorised all variables collected on trial data collection forms from 18, mainly publicly funded, randomised superiority trials, including trials of an investigational medicinal product and complex interventions. Categorisation was done independently in pairs: one person having in-depth knowledge of the trial, the other independent of the trial. Disagreement was resolved through reference to the trial protocol and discussion, with the project team being consulted if necessary. Key results: Primary outcome data accounted for 5.0\% (median)/11.2\% (mean) of all data items collected. Secondary outcomes accounted for 39.9\% (median)/42.5\% (mean) of all data items. Non-outcome data such as participant identifiers and demographic data represented 32.4\% (median)/36.5\% (mean) of all data items collected. Conclusion: A small proportion of the data collected in our sample of 18 trials was related to the primary outcome. Secondary outcomes accounted for eight times the volume of data as the primary outcome. A substantial amount of data collection is not related to trial outcomes. Trialists should work to make sure that the data they collect are only those essential to support the health and treatment decisions of those whom the trial is designed to inform.",

author = "Evelyn Crowley and Shaun Treweek and Katie Banister and Suzanne Breeman and Lynda Constable and Seonaidh Cotton and Anne Duncan and \{El Feky\}, Adel and Heidi Gardner and Kirsteen Goodman and Doris Lanz and Alison McDonald and Emma Ogburn and Kath Starr and Natasha Stevens and Marie Valente and Gordon Fernie",

note = "Publisher Copyright: {\textcopyright} 2020 The Author(s).",

year = "2020",

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doi = "10.1186/s13063-020-04388-x",

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Crowley, E, Treweek, S, Banister, K, Breeman, S, Constable, L, Cotton, S, Duncan, A, El Feky, A, Gardner, H, Goodman, K, Lanz, D, McDonald, A, Ogburn, E, Starr, K, Stevens, N, Valente, M & Fernie, G 2020, 'Using systematic data categorisation to quantify the types of data collected in clinical trials: The DataCat project', Trials, vol. 21, no. 1, 535. https://doi.org/10.1186/s13063-020-04388-x

TY - JOUR

T1 - Using systematic data categorisation to quantify the types of data collected in clinical trials

T2 - The DataCat project

AU - Crowley, Evelyn

AU - Treweek, Shaun

AU - Banister, Katie

AU - Breeman, Suzanne

AU - Constable, Lynda

AU - Cotton, Seonaidh

AU - Duncan, Anne

AU - El Feky, Adel

AU - Gardner, Heidi

AU - Goodman, Kirsteen

AU - Lanz, Doris

AU - McDonald, Alison

AU - Ogburn, Emma

AU - Starr, Kath

AU - Stevens, Natasha

AU - Valente, Marie

AU - Fernie, Gordon

PY - 2020/6/16

Y1 - 2020/6/16

N2 - Background: Data collection consumes a large proportion of clinical trial resources. Each data item requires time and effort for collection, processing and quality control procedures. In general, more data equals a heavier burden for trial staff and participants. It is also likely to increase costs. Knowing the types of data being collected, and in what proportion, will be helpful to ensure that limited trial resources and participant goodwill are used wisely. Aim: The aim of this study is to categorise the types of data collected across a broad range of trials and assess what proportion of collected data each category represents. Methods: We developed a standard operating procedure to categorise data into primary outcome, secondary outcome and 15 other categories. We categorised all variables collected on trial data collection forms from 18, mainly publicly funded, randomised superiority trials, including trials of an investigational medicinal product and complex interventions. Categorisation was done independently in pairs: one person having in-depth knowledge of the trial, the other independent of the trial. Disagreement was resolved through reference to the trial protocol and discussion, with the project team being consulted if necessary. Key results: Primary outcome data accounted for 5.0% (median)/11.2% (mean) of all data items collected. Secondary outcomes accounted for 39.9% (median)/42.5% (mean) of all data items. Non-outcome data such as participant identifiers and demographic data represented 32.4% (median)/36.5% (mean) of all data items collected. Conclusion: A small proportion of the data collected in our sample of 18 trials was related to the primary outcome. Secondary outcomes accounted for eight times the volume of data as the primary outcome. A substantial amount of data collection is not related to trial outcomes. Trialists should work to make sure that the data they collect are only those essential to support the health and treatment decisions of those whom the trial is designed to inform.

AB - Background: Data collection consumes a large proportion of clinical trial resources. Each data item requires time and effort for collection, processing and quality control procedures. In general, more data equals a heavier burden for trial staff and participants. It is also likely to increase costs. Knowing the types of data being collected, and in what proportion, will be helpful to ensure that limited trial resources and participant goodwill are used wisely. Aim: The aim of this study is to categorise the types of data collected across a broad range of trials and assess what proportion of collected data each category represents. Methods: We developed a standard operating procedure to categorise data into primary outcome, secondary outcome and 15 other categories. We categorised all variables collected on trial data collection forms from 18, mainly publicly funded, randomised superiority trials, including trials of an investigational medicinal product and complex interventions. Categorisation was done independently in pairs: one person having in-depth knowledge of the trial, the other independent of the trial. Disagreement was resolved through reference to the trial protocol and discussion, with the project team being consulted if necessary. Key results: Primary outcome data accounted for 5.0% (median)/11.2% (mean) of all data items collected. Secondary outcomes accounted for 39.9% (median)/42.5% (mean) of all data items. Non-outcome data such as participant identifiers and demographic data represented 32.4% (median)/36.5% (mean) of all data items collected. Conclusion: A small proportion of the data collected in our sample of 18 trials was related to the primary outcome. Secondary outcomes accounted for eight times the volume of data as the primary outcome. A substantial amount of data collection is not related to trial outcomes. Trialists should work to make sure that the data they collect are only those essential to support the health and treatment decisions of those whom the trial is designed to inform.

UR - https://www.scopus.com/pages/publications/85086686457

U2 - 10.1186/s13063-020-04388-x

DO - 10.1186/s13063-020-04388-x

M3 - Article

C2 - 32546192

AN - SCOPUS:85086686457

SN - 1468-6708

VL - 21

JO - Trials

JF - Trials

IS - 1

M1 - 535

ER -

Using systematic data categorisation to quantify the types of data collected in clinical trials: The DataCat project

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