Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT04718324 |
| Other study ID # |
UUBreast02 |
| Secondary ID |
|
| Status |
Completed |
| Phase |
Phase 3
|
| First received |
|
| Last updated |
|
| Start date |
September 1, 2019 |
| Est. completion date |
April 30, 2021 |
Study information
| Verified date |
May 2021 |
| Source |
Uppsala University |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
In recent years, large interest in the conduct and focus of clinical trials has focused to
patient related outcomes and value-based healthcare. Patient Reported Outcome MeasureS,
(PROMs) has become one of the standard instruments used for measuring outcomes; multiple
PROMS have been extensively validated and are used in many clinical studies, but also in
clinical routine. Additionally, Patient Reported Experience MeasureS (PREMS) allow for
real-time feedback on the integration of care and can subsequently drive changes in health
provision systems. In the present trial, the mode of delivery of PROMS is examined in terms
of effectivity and patient experience (PREMS) in the setting of breast disease.
Description:
In recent years, large interest in the conduct and focus of clinical trials has focused to
patient related outcomes and value-based healthcare. Patient Reported Outcome MeasureS,
(PROMs) has become one of the standard instruments used for measuring outcomes; multiple
PROMS have been extensively validated and are used in many clinical studies, but also in
clinical routine. This is certainly the case for patients with breast disease, and in
particular, breast cancer, where therapeutic advances in systemic and locoregional treatment
have dramatically improved survival outcomes and shifted the interest in patient wellness,
quality of life and health economy. However, their introduction and implementation require
the development of certain logistics involving delivery to the patients, data procession and
finally inclusion in patient journals and/or trial case report forms (CRFs).Additionally,
Patient Reported Experience MeasureS (PREMS) allow for real-time feedback on the integration
of care and can subsequently drive changes in health provision systems.
Currently, the paper-version of these PROMs, pPROMs, has been the standard version. With this
comes some advantages, such as the ability to save and store filled PROMS, and for patients
to fill them out when it suits them best, not having to answer all questions at once. At the
same time, there are also disadvantages, such as that storing and processing the data is a
tedious and resource-consuming task. Additionally, patients occasionally find it inconvenient
to return the pPROMS by post; finally, the consumption of paper is not viewed as a
environmentally friendly behaviour. At the same time and in the new era of digitalization,
internet-based studies, such as surveys, become more popular. Most validated PROMS have been
utilised in several occasions, and there is an effort for their standardisation in health
care. These e-PROMs (electronic PROMs) seem to be more time-efficient since they do not have
to be processed manually, but instead can be directly connected to digital systems which
transform raw data (patient response) to big data and scores. It is also a more
environment-friendly option since there is no need to print the questionnaires on paper or
send them via mail to the patients and then back to the research centre. The question is how
patients feel about these electronic versions and if their implementation may simplify PROMS,
both for patients and healthcare givers and researchers alike. Even though the older
generation at greater length is connected to the internet than before, and are more used to
handling it, there are still those who are not comfortable with these new digital services.
Despite this being a reasonable hypothesis, no trials have examined this subject, that is to
map the patients' attitudes toward participating in studies, nor which form is the preferred
one, ePROMs or pPROMS. It would be reasonable to hypothesize that a more convenient mode of
delivery would facilitate patients and would therefore increase response rates. Additionally,
there is no randomized data on the optimal mode of PROMS delivery and process as far as
monetary, personnel and structural resources are concerned
Reference population for the trial are women from the breast radiology unit, breast
outpatient clinic and breast cancer patients from the oncology department of the
participating sites. Patients will be asked to participate to this study through a letter
sent they receive when receiving their appointment to the respective clinic/department. All
patients are asked, regardless of diagnosis, sex or age; at this point, the researchers are
not aware of individual information. If they consent, participants are randomised to either
e-PROMs or pPROMs.
Trial hypothesis is that ePROMs are more convenient and time-efficient and that with these
investigators can increase the response rate from 65% (which was observed in a pilot study
previously conducted at the breast outpatient clinic at Uppsala University Hospital) to
80%.The trial is designed as a superiority trial to detect for a 0.15 difference between
arms, with a 2-sided p-value=0.05 and 80% power. Sample size calculation was performed with
(SampleSize4ClinicalTrials and TrialSize packages). This responds to 109 patients per arm.
Patient allocation (1:1) is performed through permuted block randomisation performed on the R
statistical software (randomizeR package) in blocks of 8.
Patients that provide oral and written consent for the trial are anonymised and receive a
unique study number. They willingly provide contact details (address and e-mail address), in
order to receive PROMS after randomization. Patients may decline mode of PROMS delivery, if
they prefer otherwise. Patient preference is registered. In analyses, the
"intention-to-treat" principle will be followed, but per protocol analyses is intended if the
crossover is deemed significant (>10%).
Data process and analysis
Once filled out, the anonymised ePROMs will be automatically stored to the Uppsala University
servers. They are extractable as a Microsoft Excel data sheet. pPROMS will be stored in paper
form in a safe location at the participating site. All raw data from both arms will be
transferred in an Excel database. This raw data will be processed through algorithms specific
to each PROMS to allow for the calculation of the respective PROMS scores.
The time required for this procedure will be registered for statistical analyses.
Patient data to be utilised in the analysis is age and site of recruitment. Other data to be
registered are monetary costs for pPROMS postal, monetary costs for pPROMS related consumable
materials and hourly cost for the documentation and registration of PROMS in patient
electronic journals.
Data and patient safety
Patient data will be treated according to the General Data Protection Regulation (GDPR). The
trial is not expected to affect treatment of patients or affect diagnostic work-up or
treatment modality. Participants will not receive monetary compensation. For participants
that are wishing it, PROMS scores will be included in their journals.
Publication
Trial results are expected to be submitted for publication in peer-reviewed journals.
Positive and negative results as well as subgroup analyses for primary characteristics such
as patient age are expected to be reported.
