ANZCTR - Registration

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Trial registered on ANZCTR

Registration number

ACTRN12619000006145

Ethics application status

Approved

Date submitted

20/12/2018

Date registered

8/01/2019

Date last updated

19/02/2021

Date data sharing statement initially provided

8/01/2019

Type of registration

Prospectively registered

Titles & IDs

Public title

A study designed to test a new oxygen delivery device (NHFO2) and assess comfort of breathing in patients with long term respiratory disease

Scientific title

Algorithm feasibility of a novel oxygen delivery system using comfort mode and closed-loop oxygen control in participants with chronic lung disease

Secondary ID [1]

None

Universal Trial Number (UTN)

U1111-1223-6230

Trial acronym

NHFO2: Algorithm 2

Linked study record

Health condition

Health condition(s) or problem(s) studied:

COPD

Interstitial Lung Disease

Bronchiectasis

Condition category

Condition code

Respiratory

Chronic obstructive pulmonary disease

Respiratory

Other respiratory disorders / diseases

Intervention/exposure

Study type

Interventional

Description of intervention(s) / exposure

This feasibility study will evaluate the comfort mode of the NHFO2 device both with and without closed-loop oxygen control. The device uses two internal algorithms; one related to closed-loop oxygen control and one related to comfort mode. NHFO2 is a newly developed device which delivers heated, humidified high flow oxygen via nasal cannulae. The device has a closed-loop oxygen control option where the FiO2 is automatically titrated to achieve a set patient target SpO2.

The device also has a comfort mode in which the flow is altered. This mode is hypothesized to improve user comfort. Different levels of comfort mode can be selected (0-5).

The FiO2 and flow rate can also be adjusted manually.

The device will be applied by a medically qualified study investigator. This study will involve 2 groups of participants. 3 participants will be recruited to group A. Up to 5 participants will be recruited to group B. The fidelity of the study will be monitored internally according to MRINZ Standard Operating Procedures.

GROUP A:
Group A participants will undergo a single test evaluating the comfort of the NHFO2 device at different flow rates with comfort mode enabled and disabled. Participants enrolled in Group A will be those that have a diagnosis of chronic respiratory disease who do not have resting hypoxaemia and do not require long term oxygen therapy. The first visit will be a screening visit to assess eligibility.

Potential patients will attend the MRINZ facility at Wellington Hospital for Visit 1, in which the PIS will be discussed, written informed consent will be completed, demographic data collected, baseline, weight, SpO2 and heart rate measured and spirometry completed. The screening visit will last around one hour.

If eligible, participants will be invited for a second visit, using the NHFO2 device. Participants will attend for a single testing visit with no repeat visits. At the testing visit, the participant will be allocated to Test A1 (see Table below)

Test A1: (16 runs, 48 mins)
21% FiO2 delivered at varying flow rates (L/min) and at different levels of comfort mode
Run 1 Flow 10 FiO2 21 Comfort Mode 0 Time 3
Run 2 Flow 10 FiO2 21 Comfort Mode 5 Time 3
Run 3 Flow 25 FiO2 21 Comfort Mode 0 Time 3
Run 4 Flow 25 FiO2 21 Comfort Mode 5 Time 3
Run 5 Flow 35 FiO2 21 Comfort Mode 0 Time 3
Run 6 Flow 35 FiO2 21 Comfort Mode 1 Time 3
Run 7 Flow 35 FiO2 21 Comfort Mode 3 Time 3
Run 8 Flow 35 FiO2 21 Comfort Mode 5 Time 3
Run 9 Flow 45 FiO2 21 Comfort Mode 0 Time 3
Run 10 Flow 45 FiO2 21 Comfort Mode 5 Time 3
Run 11 Flow 55 FiO2 21 Comfort Mode 0 Time 3
Run 12 Flow 55 FiO2 21 Comfort Mode 1 Time 3
Run 13 Flow 55 FiO2 21 Comfort Mode 3 Time 3
Run 14 Flow 55 FiO2 21 Comfort Mode 5 Time 3
Run 15 Flow 70 FiO2 21 Comfort Mode 0 Time 3
Run 16 Flow 70 FiO2 21 Comfort Mode 5 Time 3

During each run, participants will receive an oxygen concentration (FiO2) of 21% (room air) at a set temperature between 35-37°C as determined by participant preference, at different flow rates and at different levels of comfort mode.

At the end of each run, participants will be asked to rate their level of comfort of breathing, using a visual analogue scale. Participants will also be asked to rate the degree of noise produced by the device on a visual analogue scale after runs that test the device using flow rate of 45L/min or above.

The total duration of visit two will be a maximum of three hours. If required, at the discretion of the investigators, the test or individual runs within the test may be repeated or skipped up to a maximum testing period of 3 hours per visit.

GROUP B:
Group B participants will undergo five tests evaluating the varying modes of the NHFO2 device. Participants enrolled in Group B will be those that have a diagnosis of chronic respiratory disease who are hypoxiaemic at rest and are prescribed long-term oxygen therapy. This will allow closed-loop oxygen control to be tested in these participants at rest.

The first visit will be a screening visit to assess eligibility and determine target SpO2 range.
Potential patients will attend the MRINZ facility at Wellington Hospital for visit one in which the PIS will be discussed, written informed consent will be completed, demographic data collected, baseline height and weight measured, transcutaneous CO2, SpO2, heart rate measured and spirometry completed. The duration of the screening visit will be approximately one and a half hours.

The second visit will be for testing the NHFO2 device. Each participant will be allocated one or more of the five tests B1-5 (see below), up to a maximum visit duration of 3 hours. The allocation will be at the discretion of the sponsor, and will be decided in advance of the second visit. The tests will be allocated depending upon the sponsor's requirement to test different flow rates, FiO2 and comfort modes in order to optimize their device and algorithm development. If required, at the discretion of the investigators or sponsor, each test or individual runs within each test may be repeated or skipped up to a maximum testing period of 3 hours per visit.

At the end of each run, participants will be asked to rate their level of comfort of breathing, using a visual analogue scale. Participants will also be asked to rate the degree of noise produced by the device on a visual analogue scale after run 5 and 8 in Test B1 and runs 7-10 in Test B5. Participants can be requested to return for up to one further testing visit if required to make a total of 5 testing visits among group B participants.

A summary of the 5 tests are described below:
Test B1: (8 runs, 48 mins)
21% FiO2 delivered at varying flow rates (L/min) and at different levels of comfort mode

Run 1 Flow 35 FiO2 21% Comfort Mode 0 Time 6
Run 2 Flow 35 FiO2 21% Comfort Mode 1 Time 6
Run 3 Flow 35 FiO2 21% Comfort Mode 3 Time 6
Run 4 Flow 35 FiO2 21% Comfort Mode 5 Time 6
Run 5 Flow 55 FiO2 21% Comfort Mode 0 Time 6
Run 6 Flow 55 FiO2 21% Comfort Mode 1 Time 6
Run 7 Flow 55 FiO2 21% Comfort Mode 3 Time 6
Run 8 Flow 55 FiO2 21% Comfort Mode 5 Time 6

Test B2: (10 runs, 60 mins)
Manual ramping of FiO2 at fixed flow rate (L/min) with comfort mode disabled and enabled

Run 1 Flow 35 FiO2 21 Comfort Mode 0 Time 6
Run 2 Flow 35 FiO2 21 Comfort Mode 5 Time 6
Run 3 Flow 35 FiO2 26 Comfort Mode 0 Time 6
Run 4 Flow 35 FiO2 26 Comfort Mode 5 Time 6
Run 5 Flow 35 FiO2 31 Comfort Mode 0 Time 6
Run 6 Flow 35 FiO2 31 Comfort Mode 5 Time 6
Run 7 Flow 35 FiO2 36 Comfort Mode 0 Time 6
Run 8 Flow 35 FiO2 36 Comfort Mode 5 Time 6
Run 9 Flow 35 FiO2 41 Comfort Mode 0 Time 6
Run 10 Flow 35 FiO2 41 Comfort Mode 5 Time 6

Test B3: (2 runs, up to 2 hours)
Closed-loop control of SpO2 at fixed flow (L/min) with comfort mode disabled and enabled

Run 1 Flow 35 FiO2 Closed-loop Comfort Mode 0 Time upto 60
Run 2 Flow 35 FiO2 Closed-loop Comfort Mode 5 Time upto 60

Test B4: (9 runs, 21 mins)
Closed-loop control of SpO2, delivered at 35L/min with comfort mode disabled and enabled while mouth breathing, nose breathing and talking

Run 1 Flow 35 FiO2 Closed-loop Comfort Mode 0 Breathing Activity Mouth, Time 2
Run 2 Flow 35 FiO2 Closed-loop Comfort Mode 5 Breathing Activity Mouth, Time 3
Run 3 Flow 35 FiO2 Closed-loop Comfort Mode 0 Breathing Activity Rest, Time 2
Run 4 Flow 35 FiO2 Closed-loop Comfort Mode 0 Breathing Activity Nose, Time 2
Run 5 Flow 35 FiO2 Closed-loop Comfort Mode 5 Breathing Activity Nose, Time 3
Run 6 Flow 35 FiO2 Closed-loop Comfort Mode 0 Breathing Activity Rest, Time 2
Run 7 Flow 35 FiO2 Closed-loop Comfort Mode 0 Breathing Activity Talking, Time 2
Run 8 Flow 35 FiO2 Closed-loop Comfort Mode 5 Breathing Activity Talking, Time 3
Run 9 Flow 35 FiO2 Closed-loop Comfort Mode 0 Breathing Activity Rest, Time 2

Test B5: (10 runs, 60 mins)
Closed-loop control of SpO2 at different flow rates (L/min) with comfort mode disabled and enabled

Run 1 Flow 35 FiO2 Closed-loop Comfort Mode 0 Time 6
Run 2 Flow 35 FiO2 Closed-loop Comfort Mode 5 Time 6
Run 3 Flow 15 FiO2 Closed-loop Comfort Mode 0 Time 6
Run 4 Flow 15 FiO2 Closed-loop Comfort Mode 5 Time 6
Run 5 Flow 25 FiO2 Closed-loop Comfort Mode 0 Time 6
Run 6 Flow 25 FiO2 Closed-loop Comfort Mode 5 Time 6
Run 7 Flow 45 FiO2 Closed-loop Comfort Mode 0 Time 6
Run 8 Flow 45 FiO2 Closed-loop Comfort Mode 5 Time 6
Run 9 Flow 55 FiO2 Closed-loop Comfort Mode 0 Time 6
Run 10 Flow 55 FiO2 Closed-loop Comfort Mode 5 Time 6

Intervention code [1]

Treatment: Devices

Comparator / control treatment

No control group
The two participant arms will not be compared. There is no control group. The outcome measures are designed to assess device efficacy in both groups of participants.

Control group

Uncontrolled

Outcomes

Primary outcome [1]

Group A: Comfort scores assessed using Visual Analogue Scale

Timepoint [1]

Group A: Immediately after each run

Primary outcome [2]

Group B: Comfort scores assessed using Visual Analogue Scale

Timepoint [2]

Group B: Immediately after each run

Secondary outcome [1]

Group A: Participants’ impression of device noise levels assessed using Visual Analogue Scale

Timepoint [1]

Group A: Immediately after each run performed with a flow rate of equal o greater than 45 L/min, on comfort mode level 0 and 5.

Secondary outcome [2]

Group B: Participants’ impression of device noise levels assessed using Visual Analogue Scale

Timepoint [2]

Group B: Immediately after run 5 and 8 in Test B1 and run 7-10 in Test B5

Secondary outcome [3]

Group B: Minimum SpO2 as measured by the NHFO2 device.

Timepoint [3]

Calculated for the duration of each run after testing visit is completed

Secondary outcome [4]

Group B: Maximum SpO2 as measured by the NHFO2 device.

Timepoint [4]

Calculated for the duration of each run after testing visit is completed

Secondary outcome [5]

Group B: Mean SpO2 as measured by the NHFO2 device.

Timepoint [5]

Calculated for the duration of each run after testing visit is completed

Secondary outcome [6]

Group B: % of time spent within allocated SPO2 target range, as measured by NHFO2 device

Transcutaneous CO2 will be measured using a V-Sign ear clip sensor and SenTec device (SenTec, Switzerland) during the screening visit. Transcutaneous CO2 will be used to determine target SpO2 range during oxygen therapy as demonstrated below.

If Transcutaneous CO2 is > 45mmHg (hypercapnia), then SpO2 target range is 88% - 92%
If Transcutaneous CO2 is equal ot < 45mmHg (normocapnia), then SpO2 target range is 92% - 96%

Timepoint [6]

Calculated for the duration of each run in Test B3, B4 and B5 after testing visit is completed

Secondary outcome [7]

Group B: Minimum PtCO2 as measured by the SenTec device

Timepoint [7]

Calculated for the duration of each run after testing visit is completed

Secondary outcome [8]

Group B: Maximum PtCO2 as measured by the SenTec device

Timepoint [8]

Calculated for the duration of each run after testing visit is completed

Secondary outcome [9]

Group B: Mean PtCO2 as measured by the SenTec device

Timepoint [9]

Calculated for the duration of each run after testing visit is completed

Secondary outcome [10]

Group B: Minimum Heart Rate as measured by the NHFO2 device

Timepoint [10]

Calculated for the duration of each run after testing visit is completed

Secondary outcome [11]

Group B: Maximum Heart Rate as measured by the NHFO2 device

Timepoint [11]

Calculated for the duration of each run after testing visit is completed

Secondary outcome [12]

Group B: Mean Heart Rate as measured by the NHFO2 device

Timepoint [12]

Calculated for the duration of each run after testing visit is completed

Secondary outcome [13]

Group B: Mean respiratory rate as measured by the RespiTrace system,

Timepoint [13]

Calculated for the duration of each run after testing visit is completed

Eligibility

Key inclusion criteria

Group A
1. Doctor’s diagnosis of a chronic respiratory disease such as COPD, bronchiectasis and Interstitial Lung Disease
2. Stable respiratory state with no exacerbation in last 4 weeks

Group B
1. Doctor’s diagnosis of a chronic respiratory disease such as COPD, bronchiectasis and Interstitial Lung Disease
2. Prescribed long term oxygen therapy (LTOT) for use at rest
3. Stable respiratory state with no exacerbation in last 4 weeks
4. Hypercapnic (PtCO2 >45mmHg), with SpO2 <88% at rest breathing room air OR Normocapnic (PtCO2 less than or equal to 45mmHg), with SpO2<92% at rest breathing room air

Minimum age

18 Years

Maximum age

No limit

Sex

Both males and females

Can healthy volunteers participate?

Key exclusion criteria

Group A and B
1. Age <18
2. Cognitive impairment
3. Diagnosis of a notifiable disease (eg. hepatitis, TB, rheumatic fever, HIV, gastroenteritis)
4. The presence of an implantable Medical Device (eg. pacemaker, defibrillator, neurostimulator or insulin pump)
5. Known infection or colonization with multidrug resistant bacteria, Pseudomonas species, Burkholderia Cepacia or mycobacteria
6. The presence of an implantable Medical Device (eg. Pacemaker, defibrillator, neurostimulator, or insulin pump).
7. Any other condition which, at the investigator’s discretion, is believed may present a safety risk or impact the feasibility of the study or the study results.

Group B ONLY
1. Inability to tolerate an interruption in oxygen therapy
2. Requirement for more than 4L/min LTOT at rest

Study design

Purpose of the study

Treatment

Allocation to intervention

Non-randomised trial

Procedure for enrolling a subject and allocating the treatment (allocation concealment procedures)

Allocation is not concealed

Methods used to generate the sequence in which subjects will be randomised (sequence generation)

Not applicable

Masking / blinding

Blinded (masking used)

Who is / are masked / blinded?

The people receiving the treatment/s

Intervention assignment

Other

Other design features

Participants will not be aware of which settings are being used for each run of each test. This will reduce the risk of biasing participants impression of comfort of breathing and device noise at different levels of comfort mode..

Phase

Not Applicable

Type of endpoint/s

Efficacy

Statistical methods / analysis

As this is a study designed to determine efficacy and comfort of a medical device, no power calculation has been undertaken for statistical significance.

For the primary outcomes of both group A and group B, comfort scores will determined after each run. No formal statistical analysis will be undertaken. Comfort scores will be used to inform Fisher & Paykel regarding the tolerability of the device.

For secondary outcomes, minimum, maximum, mean of SpO2, heart rate, respiratory rate and transcutaneous CO2 will be measured.

For SpO2, the proportion of total time spent within target range while using NHFO2 in closed-loop control mode, will be calculated and expressed along with 95% confidence intervals.

Noise scores will be determined after certain runs. No formal statistical analysis will be undertaken. Noise scores will be used to inform Fisher & Paykel regarding the tolerability of the device.

Recruitment

Recruitment status

Recruiting

Date of first participant enrolment

Anticipated

21/01/2019

Actual

15/04/2019

Date of last participant enrolment

Anticipated

Actual

Date of last data collection

Anticipated

Actual

Sample size

Target

Accrual to date

Final

Recruitment outside Australia

Country [1]

New Zealand

State/province [1]

Wellington

Funding & Sponsors

Funding source category [1]

Commercial sector/Industry

Name [1]

Fisher and Paykel

Address [1]

15 Maurice Paykel Place
East Tamaki, Auckland 2013

Country [1]

New Zealand

Primary sponsor type

Commercial sector/Industry

Name

Fisher and Paykel

Address

15 Maurice Paykel Place
East Tamaki, Auckland 2013

Country

New Zealand

Secondary sponsor category [1]

None

Name [1]

Address [1]

Country [1]

Ethics approval

Ethics application status

Approved

Ethics committee name [1]

Southern Health and Disability Ethics Committee

Ethics committee address [1]

133 Molesworth Street
Thorndon
Wellington 6011

Ethics committee country [1]

New Zealand

Date submitted for ethics approval [1]

21/12/2018

Approval date [1]

08/02/2019

Ethics approval number [1]

19/STH/6

Summary

Brief summary


In some people with lung disease such as chronic obstructive pulmonary disease (COPD/emphysema), levels of oxygen in the blood can be low and we know that giving these people extra oxygen can help this problem and improve their health.

At the moment we give a set amount of oxygen to patients which is not easy to adjust and may be too much or too little.

To help this problem, a new device has been developed by Fisher and Paykel Healthcare, which is able to automatically adjust the amount of oxygen it gives, depending on blood oxygen levels at the time.

The device gives a warm mixture of air and oxygen at a high flow through small prongs, which sit just inside the nostrils.

Sometimes this high flow can be uncomfortable. Fisher and Paykel have therefore developed a feature called “comfort mode” which may make using the device more comfortable.

This study is designed to test how well this new “comfort mode” works and whether you find it easier to breathe using this new feature.

Trial website

Trial related presentations / publications

Public notes

Contacts

Principal investigator

Name

Dr James Harper

Address

Medical Research Institute of New Zealand
Level 7 CSB, Wellington Hospital,
Riddiford Street, Newtown,
Wellington 6021

Country

New Zealand

Phone

+64 4 805 0232

Fax

[email protected]

Contact person for public queries

Name

James Harper

Address

Medical Research Institute of New Zealand
Level 7 CSB, Wellington Hospital,
Riddiford Street, Newtown,
Wellington 6021

Country

New Zealand

Phone

+64 4 805 0232

Fax

[email protected]

Contact person for scientific queries

Name

James Harper

Address

Medical Research Institute of New Zealand
Level 7 CSB, Wellington Hospital,
Riddiford Street, Newtown,
Wellington 6021

Country

New Zealand

Phone

+64 4 805 0232

Fax

[email protected]

Data sharing statement

Will individual participant data (IPD) for this trial be available (including data dictionaries)?

No/undecided IPD sharing reason/comment

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.

Trial Review

Documents added manually

Documents added automatically