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Trial registered on ANZCTR


Registration number
ACTRN12614000615684
Ethics application status
Approved
Date submitted
3/06/2014
Date registered
10/06/2014
Date last updated
23/06/2014
Type of registration
Prospectively registered

Titles & IDs
Public title
A night-lighting intervention to reduce inpatient falls: A stepped-wedge cluster randomised controlled trial
Scientific title
A single site, stepped-wedge cluster randomised controlled trial among hospitalised patients to determine the effect of a novel night lighting solution compared to usual care on ward level rates of patient falls.
Secondary ID [1] 284729 0
none
Universal Trial Number (UTN)
U1111-1157-6331
Trial acronym
Linked study record

Health condition
Health condition(s) or problem(s) studied:
Accidental Falls 292081 0
Condition category
Condition code
Physical Medicine / Rehabilitation 292417 292417 0 0
Other physical medicine / rehabilitation
Injuries and Accidents 292418 292418 0 0
Other injuries and accidents
Public Health 292419 292419 0 0
Health service research

Intervention/exposure
Study type
Interventional
Description of intervention(s) / exposure
The intervention in this study is a modified night-lighting solution that will be installed in all patient rooms (both shared rooms and single rooms) across trial wards. We will use low-output LED strip lighting with an output wavelength of 670 nm (orange colour), which will be housed in aluminium tracks with diffuser cover strips. The spectral characteristics of the light have been determined in line with prior research on relationships between blue wavelength lighting and alertness (an unwanted effect for night lighting) [1]. The lights will be installed in multiple locations within each patient environment; the orientation and illumination characteristics are based on prior published research and on findings of a preliminary clinical acceptability study conducted by this team.

LED luminaires will be installed in the following three locations:

i. Around the exterior ensuite door-frame: To provide a visual reference point for patients attempting to mobilise to the toilet at night, we will install a continuous length of strip lighting around the exterior perimeter of the toilet door-frame.
ii. Above the washbasin in the ensuite toilet: In a horizontal section below the mirror and above the wash basin.
iii. Behind the toilet and adjacent to the toilet: To facilitate easy visualisation of the immediate area around the toilet we will install one section of lighting behind to the toilet (above the cistern) and in a second section over the grab rail (where a wall-mounted grab rail is installed along the closest adjacent wall). Due to known inter-ward variability in location of toilets, type and location of grab-rails within ensuite bathrooms, it might not be feasible to install grab rail lighting in all locations (such as when the toilet is located equidistance from both adjacent walls and bilateral fold-back grab-rails are installed on the posterior wall on either side of the toilet). In such instances, we will make pragmatic decisions on implementation feasibility and variation, which will be comprehensively catalogued by the PI in a study journal.

The lighting will be installed by hospital building and engineering service electricians such that 12 volt power-supply units and all wiring will be housed behind wall panels. While 24 hour operation of the lights is acceptable, we intend to automate the lights to gradually turn on at 5 PM and fade out at 7 AM by linking them with the hospital central timer. This will help maximise service life, reduce power consumption and eliminate the need for staff input. The on/off times have been selected to ensure that seasonal variations of sunrise and sunset times in Brisbane, Queensland are accounted for. Importantly, none of the existing lighting will be altered in any way, and staff and patients will have full use of existing lightings in patient rooms and toilets if the installed night lighting was considered inadequate or required supplementation, for example if additional light is required for patients with severe visual impairment, or if a medical emergency occurs.

The duration of the intervention period is 14 months from commencement. However, participating wards will be given the option to retain the modified night lighting at the end of the trial. I wards chose to retain the lighting, it will become part of ward infrastructure. If requested for removal, the lights will be deactivated upon trial completion and removed by RBWH building and engineering services subsequently.

1. Cajochen, C (2007). "Alerting effects of light." Sleep medicine reviews 11.6: 453-464.
Intervention code [1] 289512 0
Other interventions
Comparator / control treatment
Control participants in this study will receive standard care from the multidisciplinary team involved in the management of patients in their ward. This will include the full range of assessments, interventions and level of care appropriate to their condition as per applicable guidelines and protocols. No treatments will be withheld or modified.
Control group
Active

Outcomes
Primary outcome [1] 292284 0
Ward level 'rate of falls'. This will be compiled from:
(1) Incident reports routinely completed after inpatient falls and recorded on the Queensland Health clinical incident reporting system.
(2) Contact with ward Nurse Unit Managers (NUMs) to identify unreported falls.
(3) Extraction of relevant fall codes from the hospital admitted patient data collection (coded from medical charts).

Data on occupied bed days (OBDs) will be extracted from the RBWH Decision Support System (DSS).
Timepoint [1] 292284 0
Monthly data extraction across the 14 month trial period
Secondary outcome [1] 308620 0
The proportion of patients who become 'fallers' in trial wards. As with falls rates, this data will be compiled from:

(1) Incident reports routinely completed after inpatient falls and recorded on the Queensland Health clinical incident reporting system.
(2) Contact with ward Nurse Unit Managers (NUMs) to identify unreported falls.
(3) Extraction of relevant fall codes from the hospital admitted patient data collection (coded from medical charts).
Timepoint [1] 308620 0
Monthly data extraction across the 14 month trial period

Eligibility
Key inclusion criteria
All patients admitted in study wards during the 14 month trial period will be included.
Minimum age
No limit
Maximum age
No limit
Sex
Both males and females
Can healthy volunteers participate?
No
Key exclusion criteria
Nil patient level exclusion criteria will apply.

As the unit of recruitment for the cluster RCT is a hospital ward, data pertaining to all patients admitted to trial wards will be included in analysis.

Exclusion criteria applies to ward selection. All on-campus Royal Brisbane and Women's Hospital wards were placed on a list in descending order based on reported rates of falls over the preceding two years. Wards that were planned for refurbishment during the trial period were excluded. The top six remaining wards were approached for inclusion in this study.


Study design
Purpose of the study
Prevention
Allocation to intervention
Randomised controlled trial
Procedure for enrolling a subject and allocating the treatment (allocation concealment procedures)
We are pursuing a cluster RCT of stepped-wedge design and as a result no patient level randomisation will occur.

We will include six hospital wards in our study.
An independent statistician will generate an implementation sequence across study wards using computer randomisation software. The sequence of transition from control to intervention phase will not be revealed en bloc and but rather one ward at a time and two months prior to the date of transition. This would mean that the first ward to transition to intervention will be revealed to the study team at baseline (month ‘0’), with the transition to occur at the start of month ‘2’. Similarly, the second ward to cross over will be revealed at the start of month ‘2’ and cross over at the start of month ‘4’. This advance notification of wards due for transitioning to the intervention phase is necessary to allow adequate time for the hospital building and engineering services to complete and test the installations across all rooms in the ward (shared and single) in time for commencement of the intervention phase.
Methods used to generate the sequence in which subjects will be randomised (sequence generation)
The sequence in which wards receiving the intervention will be selected randomly using the “sample” function in R (version 3.0.2). This selection will be made by an off-site statistician who is not involved in study conduct or data collection (Adrian Barnett). He will e-mail ward names to the chief investigator every two months.

All wards will receive the intervention by the end of the trial period.
Masking / blinding
Open (masking not used)
Who is / are masked / blinded?



Intervention assignment
Other
Other design features
This trial of a roll-in stepped wedge cluster randomised controlled design as described by Hill, A. M., Waldron, N., Etherton-Beer, C., McPhail, S. M., Ingram, K., Flicker, L., & Haines, T. P. (2014). A stepped-wedge cluster randomised controlled trial for evaluating rates of falls among inpatients in aged care rehabilitation units receiving tailored multimedia education in addition to usual care: a trial protocol. BMJ open, 4(1), e004195.

Phase
Not Applicable
Type of endpoint/s
Safety/efficacy
Statistical methods / analysis
Primary outcomes for the stepped wedge will be ward level “rate of falls” and “the proportion of patients who become fallers”. The analysis of these primary outcomes will be with multi-level mixed effects generalised linear models using a Bernoulli family and logit link for the “proportion of patients who become fallers" outcome and a negative binomial family and log link for the "rate of falls" outcome. In these analyses, patient admissions will be nested within ward in the random effects part of the equation to take account of clustering of data by ward. The fixed part of the equation will examine group (intervention vs control) and adjust for time period. We will also adjust for seasonal effects on fall rates (that is, we will enter a covariate based on how many falls there were on each ward over the same time period over the previous two years).

We are limited in this study by practicality and resourcing constraints as to the number of wards available (six) and time over which we can conduct the study (14 months), and hence the overall anticipated sample is estimated to be 7,500 patients. With these sample constraints, it is appropriate to directly calculate the likely effect size that we can detect with 80% power. Power for parallel cluster randomised trial designs can be calculated by using a conventional power analysis approach and then multiplying by a design effect [1+(n-1)*p where n = the number of subjects per cluster and p = the intra-cluster correlation coefficient] to take into account the dependency of observations within clusters [Campbell, M., Grimshaw, J., & Steen, N. (2000). Sample size calculations for cluster randomised trials. Journal of health services research & policy, 5(1), 12-16.]. The stepped-wedge design also has a within-cluster element (ie. all clusters provide intervention and control data), which provides power advantages to a parallel cluster RCT in a similar way to comparison of paired with unpaired t-tests. Hence a power calculation specific to stepped wedge designs is required. One approach previously described highlights that stepped wedge designs could reduce the required sample size in cluster randomized trials [Woertman, W., de Hoop, E., Moerbeek, M., Zuidema, S. U., Gerritsen, D. L., & Teerenstra, S. (2013). Stepped wedge designs could reduce the required sample size in cluster randomized trials. Journal of clinical epidemiology, 66(7), 752-758.] but is based upon the cohort style of stepped wedge design where individual participants are repeatedly measured across the length of the study. This is not consistent with our planned study, which reflects more a cross-sectional style of stepped-wedge where individual participants are likely to only have one measurement for their involvement in the study. Fortunately, another power analysis approach based on the cross-sectional style of stepped-wedge trial examining a dichotomous outcome has been developed [Hussey, M. A., & Hughes, J. P. (2007). Design and analysis of stepped wedge cluster randomized trials. Contemporary clinical trials, 28(2), 182-191].

Using this approach, our study has 83% power to detect an absolute reduction in the proportion of patients who are fallers (experience one or more falls) from 5% (in control) to 4% (in intervention) assuming 1071 patients per time period (total n=7500), a coefficient of variation of 0.4, and using 6 clusters (wards), 7 time periods (6 steps plus baseline), and a two-tailed alpha of 0.05.

We aim to evaluate likely cost-effectiveness of the intervention and this will be achieved through cost-utility modelling and concurrent break-even and return-on-investment analysis.

Recruitment
Recruitment status
Recruiting
Date of first participant enrolment
Anticipated
Actual
Date of last participant enrolment
Anticipated
Actual
Date of last data collection
Anticipated
Actual
Sample size
Target
Accrual to date
Final
Recruitment in Australia
Recruitment state(s)
QLD
Recruitment postcode(s) [1] 8223 0
4029 - Royal Brisbane Hospital

Funding & Sponsors
Funding source category [1] 289347 0
Other Collaborative groups
Name [1] 289347 0
Australian Centre for Health Services Innovation (AusHSI)
Country [1] 289347 0
Australia
Primary sponsor type
Hospital
Name
Royal Brisbane and Women's Hospital, Queensland Health, Australia
Address
Royal Brisbane and Women’s Hospital
Cnr Butterfield St and Bowen Bridge Rd
Herston
Queensland 4029
Country
Australia
Secondary sponsor category [1] 288031 0
None
Name [1] 288031 0
Address [1] 288031 0
Country [1] 288031 0

Ethics approval
Ethics application status
Approved
Ethics committee name [1] 291115 0
Royal Brisbane and Women's Hospital Human Research Ethics Committee
Ethics committee address [1] 291115 0
Ethics committee country [1] 291115 0
Australia
Date submitted for ethics approval [1] 291115 0
Approval date [1] 291115 0
14/02/2014
Ethics approval number [1] 291115 0
HREC/13/QRBW/450

Summary
Brief summary
Trial website
Trial related presentations / publications
Public notes

Contacts
Principal investigator
Name 48922 0
Mr Satyan Chari
Address 48922 0
Safety and Quality Unit
Level 7 Block 7
Royal Brisbane and Women's Hospital
Metro North Hospital and Health Service
Herston
Queensland 4029
Country 48922 0
Australia
Phone 48922 0
+61 7 3646 5375
Fax 48922 0
+61 7 3646 1406
Email 48922 0
Contact person for public queries
Name 48923 0
Satyan Chari
Address 48923 0
Safety and Quality Unit
Level 7 Block 7
Royal Brisbane and Women's Hospital
Metro North Hospital and Health Service
Herston
Queensland 4029
Country 48923 0
Australia
Phone 48923 0
+61 7 3646 5375
Fax 48923 0
+61 7 3646 1406
Email 48923 0
Contact person for scientific queries
Name 48924 0
Satyan Chari
Address 48924 0
Safety and Quality Unit
Level 7 Block 7
Royal Brisbane and Women's Hospital
Metro North Hospital and Health Service
Herston
Queensland 4029
Country 48924 0
Australia
Phone 48924 0
+61 7 3646 5375
Fax 48924 0
+61 7 3646 1406
Email 48924 0

No information has been provided regarding IPD availability


What supporting documents are/will be available?

No Supporting Document Provided



Results publications and other study-related documents

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