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Trial registered on ANZCTR
Registration number
ACTRN12619000740190
Ethics application status
Approved
Date submitted
22/03/2019
Date registered
17/05/2019
Date last updated
10/05/2021
Date data sharing statement initially provided
17/05/2019
Type of registration
Prospectively registered
Titles & IDs
Public title
Studies of apnoea in the newborn: Delivery of positive inflating pressure as early rescue
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Scientific title
The SANDPIPER study: Delivery of positive inflation pressure as early rescue triggered by respiratory pause in preterm infants <30 weeks gestation on bubble CPAP
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Secondary ID [1]
297613
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Nil Known
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Universal Trial Number (UTN)
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Trial acronym
SANDPIPER study
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Linked study record
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Health condition
Health condition(s) or problem(s) studied:
Apnoea of prematurity
311882
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Condition category
Condition code
Respiratory
310471
310471
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0
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Other respiratory disorders / diseases
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Reproductive Health and Childbirth
310777
310777
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0
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Complications of newborn
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Intervention/exposure
Study type
Interventional
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Description of intervention(s) / exposure
This will be a 16 hour crossover study consisting of 4 periods, each of 4 hours duration. Both the first and second halves of the study will consist of a control and intervention epoch at random. During each intervention epoch, positive inflating pressure (PIP) triggered by 3 seconds of apnoea will be delivered either singly (sPIP) or repetitively (rPIP, up to 3 inflations). The maximum pressure of 18 cmH2O will be delivered via a PIP generating device, coupled to the existing CPAP circuit. A minimum washout period of 15 minutes will occur between each epochs.
To monitor fidelity, UTAS researchers will be on-site during intervention period. Additionally, CPAP pressures are measured and recorded throughout the 16 hour study period. Bedside staff are not required to monitor or manage the PIP generator beyond their usual interaction with the normal CPAP circuit.
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Intervention code [1]
313852
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Treatment: Devices
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Comparator / control treatment
Two 4 hour epochs of standard care - CPAP only, without rescue positive inflation pressure (PIP). CPAP setting would be determined by bedside staff based on clinical needs, and will vary from patient to patient, ranging from 5 to 10cmH2O.
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Control group
Active
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Outcomes
Primary outcome [1]
319341
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Change in frequency of apnoea lasting >5 seconds, expressed as events per hour , and quantified both on a per study and per infant basis will be compared between each epoch.
Events of apnoea will be determined and recorded via the Dräger Infinity monitor - a standard clinical monitoring device - and a modified Graseby MR10 respiratory monitor.
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Assessment method [1]
319341
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Timepoint [1]
319341
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End of the study period for each infant - approximately 16 hours.
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Secondary outcome [1]
367833
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Change in frequency of apnoea lasting >10 seconds, expressed as events per hour , and quantified both on a per study and per infant basis will be compared between each epoch.
Events of apnoea will be determined and recorded via the Dräger Infinity monitor - a standard clinical monitoring device - and a modified Graseby MR10 respiratory monitor.
This outcome will be used to assess the effectiveness of the intervention.
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Assessment method [1]
367833
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Timepoint [1]
367833
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End of the study period for each infant - approximately 16 hours.
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Secondary outcome [2]
368922
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Change in frequency of apnoea as per a consensus definition (>20 seconds or >10 seconds if accompanied by hypoxia and/or bradycardia), expressed as events per hour , and quantified both on a per study and per infant basis will be compared between each epoch.
Events of apnoea will be determined and recorded via the Dräger Infinity monitor - a standard clinical monitoring device - and a modified Graseby MR10 respiratory monitor.
This outcome will be used to assess the effectiveness of the intervention.
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Assessment method [2]
368922
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Timepoint [2]
368922
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End of the study period for each infant - approximately 16 hours.
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Secondary outcome [3]
368923
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Total duration of apnoea lasting >5 seconds will be compared between each epoch.
Events of apnoea will be determined and recorded via the Dräger Infinity monitor - a standard clinical monitoring device- and a modified Graseby MR10 respiratory monitor.
This outcome will be used to assess the effectiveness of the intervention.
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Assessment method [3]
368923
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Timepoint [3]
368923
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End of the study period for each infant - approximately 16 hours.
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Secondary outcome [4]
368924
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Change in frequency of hypoxia (SpO2 <85%) within 60 seconds of apnoea onset, expressed as events per hour, and quantified both on a per study and per infant basis will be compared between each epoch.
Events of apnoea will be determined and recorded via the Dräger Infinity monitor - a standard clinical monitoring device- and a modified Graseby MR10 respiratory monitor.
These outcomes will be used to assess the effectiveness of the intervention.
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Assessment method [4]
368924
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Timepoint [4]
368924
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End of the study period for each infant - approximately 16 hours.
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Secondary outcome [5]
368925
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Change in frequency of bradycardia (HR<100bpm) within 60 seconds of apnoea onset, expressed as events per hour, and quantified both on a per study and per infant basis will be compared between each epoch.
Events of apnoea will be determined and recorded via the Dräger Infinity monitor - a standard clinical monitoring device.
This outcome will be used to assess the effectiveness of the intervention.
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Assessment method [5]
368925
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Timepoint [5]
368925
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End of the study period for each infant - approximately 16 hours.
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Secondary outcome [6]
368926
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Proportion of time during which the abdominal capsule recording was missing and/or uninterpretable.
Recordings will be made using a modified Graseby MR10 respiratory monitor.
This outcome will be used to assess the functionality of the PIP generator device.
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Assessment method [6]
368926
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Timepoint [6]
368926
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End of the study period for each infant - approximately 16 hours.
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Secondary outcome [7]
368927
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Average delivered peak inflating pressure over each intervention periods.
Delivered pressure will be measured and recorded with a Fisher and Paykel Proxytrack.
This outcome will be used to assess the functionality of the PIP generator device.
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Assessment method [7]
368927
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Timepoint [7]
368927
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End of the study period for each infant - approximately 16 hours.
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Secondary outcome [8]
368928
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Frequency of instances where measured inflating pressure is <3 cm H2O above background CPAP level.
Delivered pressure will be measured and recorded with a Fisher and Paykel Proxytrack.
This outcome will be used to assess the functionality of the PIP generator device.
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Assessment method [8]
368928
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Timepoint [8]
368928
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End of the study period for each infant - approximately 16 hours.
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Secondary outcome [9]
368929
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Frequency of instances where there are no change in respiratory signal following PIP generation.
Respiration waveform and pulse will be recorded via the Dräger Infinity monitor - a standard clinical monitoring device- and a modified Graseby MR10 respiratory monitor. Delivered pressure will be measured and recorded with a Fisher and Paykel Proxytrack.
This outcome will be used to assess the functionality of the PIP generator device.
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Assessment method [9]
368929
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Timepoint [9]
368929
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End of the study period for each infant - approximately 16 hours.
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Secondary outcome [10]
368930
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Incidence of actuation of positive inflating pressure during the expiratory phase.
Respiratory waveforms will be recorded via the Dräger Infinity monitor - a standard clinical monitoring device. Delivered pressure will be measured and recorded with a Fisher and Paykel Proxytrack.
This outcome will be used to assess the safety of the PIP generator.
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Assessment method [10]
368930
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Timepoint [10]
368930
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End of the study period for each infant - approximately 16 hours.
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Secondary outcome [11]
368931
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Requirement to de-activate PIP generator or cease intervention by UTAS researcher or bedside staff.
This outcome will measured from the electronic logs of PIP generator function, and will be used to assess the safety of the PIP generator.
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Assessment method [11]
368931
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Timepoint [11]
368931
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End of the study period for each infant - approximately 16 hours.
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Secondary outcome [12]
370504
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Change in frequency of apnoea lasting >15 seconds, expressed as events per hour, and quantified both on a per study and per infant basis will be compared between each epoch.
Events of apnoea will be determined and recorded via the Dräger Infinity monitor - a standard clinical monitoring device - and a modified Graseby MR10 respiratory monitor.
This outcome will be used to assess the effectiveness of the intervention.
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Assessment method [12]
370504
0
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Timepoint [12]
370504
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End of the study period for each infant - approximately 16 hours.
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Secondary outcome [13]
370505
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Change in frequency of hypoxia (SpO2 <80%) within 60 seconds of apnoea onset, expressed as events per hour, and quantified both on a per study and per infant basis will be compared between each epoch.
Events of apnoea will be determined and recorded via the Dräger Infinity monitor - a standard clinical monitoring device- and a modified Graseby MR10 respiratory monitor.
These outcomes will be used to assess the effectiveness of the intervention.
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Assessment method [13]
370505
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Timepoint [13]
370505
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End of the study period for each infant - approximately 16 hours.
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Eligibility
Key inclusion criteria
- Birth gestation <30 weeks
- Chronological age < /=4 months
- Supported with bubble CPAP
- Having frequent respiratory pauses 5+ seconds duration, resulting in episodes of hypoxia (SpO2 <85) and/or bradycardia (heart rate <100 bpm) at least twice per hour.
- Research team available to commence study
- Agreement of treating clinician that the infant is suitable for involvement in the study
- Signed parental consent
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Minimum age
No limit
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Maximum age
4
Months
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Sex
Both males and females
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Can healthy volunteers participate?
No
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Key exclusion criteria
Change in mode of respiratory support, including use of non-triggered continuous non-invasive positive pressure ventilation (NIPPV) being contemplated in next 24 hours
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Study design
Purpose of the study
Treatment
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Allocation to intervention
Randomised controlled trial
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Procedure for enrolling a subject and allocating the treatment (allocation concealment procedures)
Allocation is not concealed
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Methods used to generate the sequence in which subjects will be randomised (sequence generation)
The sequence of interventions will be determined using randomisation schedule provided by the collaborating statistician at Menzies Institute for Medical Research, University of Tasmania.
The randomisation will be constrained such that the first and second 8 hour blocks of the 16 hour study each contains a period of CPAP.
Access to the randomisation will be restricted, and the intervention sequence will only be revealed once preparation of the bedspace and the infant has been completed. The randomisation for the second of two 16 hour crossover studies will only be revealed once the first study is completed.
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Masking / blinding
Open (masking not used)
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Who is / are masked / blinded?
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Intervention assignment
Crossover
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Other design features
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Phase
Not Applicable
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Type of endpoint/s
Safety/efficacy
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Statistical methods / analysis
Sample size calculations for the SANDPIPER study are based in part on the data generated in preterm infants in the SANTO-B study, where there were 9.3±11 respiratory pause events per hour in preterm infants on CPAP, as noted above. Given the crossover nature of the study design, the crux of the analysis will be a comparison of the difference in event numbers between the intervention periods and the standard CPAP periods. Assuming that the difference in event frequency between intervention and control groups has a standard deviation of 5 per hour, and applying standard paired statistical methodology, then detection of a difference in event frequency of 3 per hour with 80% power and a=0.05 would require the conduct of 22 studies. Given that this calculation does not take into account the lack of independence of studies performed in the same infant, we will plan to perform 40 studies in at least 20 infants. This will also allow collection of sufficient data (~640 hrs of recordings) to perform our analyses.
Note that our projection of a 3 per hour decrease in the rate of respiratory pauses would represent a meaningful clinical improvement in the frequency of this potentially destabilising complication in preterm infants on CPAP.
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Recruitment
Recruitment status
Recruiting
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Date of first participant enrolment
Anticipated
3/06/2019
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Actual
16/07/2019
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Date of last participant enrolment
Anticipated
31/12/2021
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Actual
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Date of last data collection
Anticipated
31/12/2021
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Actual
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Sample size
Target
20
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Accrual to date
16
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Final
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Recruitment in Australia
Recruitment state(s)
TAS
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Recruitment hospital [1]
13310
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Royal Hobart Hospital - Hobart
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Recruitment postcode(s) [1]
25883
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7000 - Hobart
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Funding & Sponsors
Funding source category [1]
302158
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Hospital
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Name [1]
302158
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Royal Hobart Hospital
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Address [1]
302158
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Royal Hobart Hospital, 48 Liverpool St, Hobart, Tasmania 7000
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Country [1]
302158
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Australia
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Primary sponsor type
University
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Name
University of Tasmania
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Address
University of Tasmania
Private Bag 51
HOBART TAS 7001
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Country
Australia
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Secondary sponsor category [1]
302187
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None
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Name [1]
302187
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Address [1]
302187
0
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Country [1]
302187
0
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Ethics approval
Ethics application status
Approved
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Ethics committee name [1]
302837
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Tasmanian Health and Medical Human Research Ethics Committee (HREC)
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Ethics committee address [1]
302837
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Menzies Institute for Medical Research, 17 Liverpool St, Hobart, Tasmania 7000
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Ethics committee country [1]
302837
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Australia
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Date submitted for ethics approval [1]
302837
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18/02/2019
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Approval date [1]
302837
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10/05/2019
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Ethics approval number [1]
302837
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H0017948
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Summary
Brief summary
We will investigate whether delivery of positive inflation pressure (PIP) (singly or repeated), triggered by a 3 second pause in respiration, can re-establish breathing efforts in preterm infants on continuous positive airway pressure (CPAP), a form of non-invasive respiratory support. The study will involve infants born at <30 weeks gestation who require CPAP support, and are having episodes of respiratory pauses. We will conduct a 16 hours crossover study comparing the use of a device to generate PIP with standard CPAP support. The study will be in blocks of 4 hours (randomly assigned) in which PIP is delivered singly, repeatedly (up to 3), or not at all (standard CPAP). We hypothesise that PIP will improve the regularity of breathing, and shorten the duration of respiratory pauses.
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Trial website
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Trial related presentations / publications
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Public notes
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Contacts
Principal investigator
Name
91562
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Prof Peter Dargaville
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Address
91562
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Department of Paediatrics, Royal Hobart Hospital, 48 Liverpool St, Hobart, TAS 7000
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Country
91562
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Australia
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Phone
91562
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+61361667546
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Fax
91562
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Email
91562
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[email protected]
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Contact person for public queries
Name
91563
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Peter Dargaville
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Address
91563
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Department of Paediatrics, Royal Hobart Hospital, 48 Liverpool St, Hobart, TAS 7000
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Country
91563
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Australia
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Phone
91563
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+61361667546
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Fax
91563
0
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Email
91563
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[email protected]
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Contact person for scientific queries
Name
91564
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Peter Dargaville
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Address
91564
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Department of Paediatrics, Royal Hobart Hospital, 48 Liverpool St, Hobart, TAS 7000
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Country
91564
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Australia
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Phone
91564
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+61361667546
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Fax
91564
0
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Email
91564
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[email protected]
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Data sharing statement
Will individual participant data (IPD) for this trial be available (including data dictionaries)?
No
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No/undecided IPD sharing reason/comment
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What supporting documents are/will be available?
No Supporting Document Provided
Results publications and other study-related documents
Documents added manually
No documents have been uploaded by study researchers.
Documents added automatically
No additional documents have been identified.
Download to PDF