Closing the Loop in Adults With Type 1 Diabetes Under Free Living Conditions

Type 1 Diabetes Clinical Trial

— AP@Home04_P3  

Official title:

A Multi-centre, Randomised, Two-period, Crossover Study to Evaluate Home Use of Closed-loop Applying Faster Insulin Aspart Versus Standard Insulin Aspart

Clinical Trial Details — Status: Completed

Administrative data

• NCT number: NCT04055480
• Other study ID #: 136248_APHome04
• Status: Completed
• Phase: N/A
• Start date: August 10, 2019
• Est. completion date: August 30, 2020

Study information

• Verified date: August 2020
• Source: University of Cambridge
• Contact: n/a
• Is FDA regulated: No
• Study type: Interventional

Clinical Trial Summary

The main objective of this study is to determine whether home use of day and night closed loop insulin delivery under free living conditions applying faster insulin aspart (FiAsp) is non-inferior to home use of closed-loop applying standard insulin aspart.

This is a double-blind, multi-centre, randomised, crossover design study, involving a run-in period followed by two study periods during which glucose levels will be controlled either by an automated closed-loop system using standard rapid acting insulin analogue or by an automated closed-loop system using faster insulin aspart in random order.

Subjects will receive appropriate training in the safe use of closed-loop insulin delivery system. Subjects will have regular contact with the study team during the home study phase including 24/7 telephone support.

The primary outcome is time spent in target range between 3.9 and 10.0 mmol/L as recorded by CGM during home stay. Secondary outcomes are the HbA1c, time spent with glucose levels above and below target, as recorded by CGM, and other CGM based metrics.

Description:

Purpose of clinical trial The purpose is to determine whether home use of day and night closed loop applying faster insulin aspart is not inferior to home use of closed loop applying standard insulin aspart.

Study objectives The study objective is to compare day and night automated closed-loop glucose control using faster acting insulin aspart with closed loop control using standard insulin aspart.

1. EFFICACY: The objective is to assess the efficacy of day and night automated closed-loop glucose control applying standard rapid-acting insulin analogue in maintaining CGM glucose levels within the target range from 3.9 to 10.0 mmol/l, as compared to day and night closed-loop using faster acting insulin aspart

2. SAFETY: The objective is to evaluate the safety of day and night automated closed-loop glucose control in terms of episodes of severe hypoglycaemia, hyperglycaemia and other adverse events and adverse device effects.

3. UTILITY: The objective is to determine the percentage of time when closed-loop was operational, and usability and acceptance of the closed-loop system.

Study Design A double-blind, multi-centre, randomised, two-period crossover study, contrasting day and night automated closed-loop glucose control applying standard rapid acting insulin analogue with day and night closed-loop control applying faster acting insulin aspart.

Study Efficacy Endpoints The primary outcome is the time spent in the target glucose range from 3.9 to 10.0 mmol/l based on CGM glucose levels during the free living phase.

Secondary outcomes include time spent above and below the target glucose range, based on CGM levels.

Safety Evaluation Frequency of severe hypoglycaemic episodes as defined by American Diabetes Association, frequency of severe hyperglycaemia (>20 mmol/l) and / or significant ketosis (plasma ketones >3mmol/l) and nature and severity of other adverse events.

Utility Evaluation Percentage of time spent in closed-loop. Usability and acceptance of the closed-loop system will be assessed using a patient experience questionnaire at the end of the second intervention. Additionally, human factor questionnaires will be administered following recruitment and at the end of each intervention arm.

Sample Size 24 adults completing the study. Up to 30 subjects will be recruited to allow for dropouts.

Maximum duration of study for a subject 20 weeks (5 months)

Recruitment The subjects will be recruited through the adult diabetes outpatient clinics or other established methods at participating centres.

Consent Participants will be asked to provide written informed consent.

Baseline Assessment Eligible subjects will undergo a baseline evaluation including a blood sample for the measurement of HbA1c, renal, liver functions, full blood count, thyroid functions and coeliac antibody screen (if not done in the previous 3 months). Urine pregnancy test will be done in females. Additional centre specific assessments will also be undertaken. Human factor questionnaires will be administered.

Study Training and Run-in Period Training sessions on the use of study CGM, insulin pump and closed-loop system will be provided by the research team. During the 2-4 weeks run-in period, subjects will use study CGM and insulin pump and will have regular contact with the research team. At the end of the run-in period, for compliance and to assess the ability of the subject to use the CGM and study pump safely, before the start of the first home study phase, at least 7 days of CGM data need to be recorded and safe use of study insulin pump demonstrated. CGM and insulin pump data during the run-in period will be used to assess baseline glucose control and optimise treatment before the start of the first home study phase.

Competency Assessment Competency on the use of study insulin pump, study CGM and closed-loop system will be evaluated using a competency assessment tool developed by the research team. Further training may be delivered as required.

Randomisation Eligible subjects will be randomised using randomisation software to the use of closed-loop with faster acting aspart or to closed-loop with standard insulin aspart.

Automated closed-loop Training on the use of closed-loop will be provided by the research team. Automated closed-loop control will be commenced and during the 2-3 hour training the participant will operate the system under the supervision of the clinical team. Competency on the use of closed-loop system will be evaluated. Subjects will be advised to use automated closed-loop system for next 8 weeks

Cross-over Assessment At the end of the first intervention human factor questionnaires will be administered.

There will be no washout period in phase 3 extension.

End of study assessments A patient experience questionnaire will be given at the end of the second intervention. Additionally human factor questionnaires will be administered.

Procedures for safety monitoring during trial Standard operating procedures for monitoring and reporting of all adverse events and adverse device events will be in place, including serious adverse events (SAE), serious adverse device effects (SADE) and specific adverse events (AE) such as severe hypoglycaemia.

Subjects will be asked to test and record blood ketones if their finger-stick glucose is above 14 mmol/l as part of the safety assessment for hyperglycaemia.

A data monitoring and ethics committee (DMEC) will be informed of all serious adverse events and any unanticipated adverse device/method effects that occur during the study and will review compiled adverse event data at periodic intervals.

Criteria for withdrawal of patients on safety grounds

A subject may terminate participation in the study at any time without necessarily giving a reason and without any personal disadvantage. An investigator can stop the participation of a subject after consideration of the benefit/risk ratio. Possible reasons are:

• Serious adverse events

• Significant protocol violation or noncompliance

• Failure to satisfy competency assessment

• Decision by the investigator, or the sponsor, that termination is in the subject's best medical interest

• Pregnancy, planned pregnancy, or breast feeding

• Allergic reaction to insulin

• Technical grounds (e.g. subject relocates)

Recruitment information / eligibility

• Status: Completed
• Enrollment: 25
• Est. completion date: August 30, 2020
• Est. primary completion date: June 15, 2020
• Accepts healthy volunteers: No
• Gender: All
• Age group: 18 Years and older

Eligibility

Inclusion Criteria:

1. The subject has type 1 diabetes as defined by WHO

2. The subject is 18 years of age or older

3. The subject will have been on an insulin pump for at least 6 months with good knowledge of insulin self-adjustment including carbohydrate counting

4. The subject is treated with one of the rapid acting or ultra-rapid acting insulin analogues (Insulin Aspart, faster acting insulin Aspart, Insulin Lispro or Insulin Glulisine)

5. HbA1c <10% (86mmol/mol) for phase 3, based on analysis from central laboratory or equivalent

6. The subject is willing to perform regular finger-prick blood glucose monitoring, with at least 2 measurements per day

7. The subject is willing to wear closed-loop system at home and at work place

8. The subject is willing to follow study specific instructions including the use of bolus calculator for all meals / snacks

9. The subject is willing to upload pump and CGM data at regular intervals

10. Female subjects of child bearing age should be on effective contraception and must have a negative urine-HCG pregnancy test at screening.

Exclusion Criteria:

1. Non-type 1 diabetes mellitus

2. Subjects who are living alone

3. Any other physical or psychological disease or condition likely to interfere with the normal conduct of the study and interpretation of the study results

4. Current treatment with drugs known to have significant interference with glucose metabolism, such as systemic corticosteroids, as judged by the investigator

5. Known or suspected allergy against insulin or previous reaction to FiAsp

6. Subjects with clinically significant nephropathy (eGFR < 45ml/min), neuropathy or active retinopathy (defined as presence of maculopathy or more than background diabetic retinopathy changes) as judged by the investigator

7. More than one episode of severe hypoglycaemia as defined by American Diabetes Association (42) in preceding 12 months (Severe hypoglycaemia is defined as an event requiring assistance of another person to actively administer carbohydrates, glucagon, or take other corrective actions including episodes of hypoglycaemia severe enough to cause unconsciousness, seizures or attendance at hospital.)

8. Total daily insulin dose > 2 IU/kg/day

9. Subject is pregnant or breast feeding or planning pregnancy within next 10 months

10. Severe visual impairment

11. Severe hearing impairment

12. Lack of reliable telephone facility for contact

13. Subject not proficient in English (UK), French (Switzerland) or German (Germany, Switzerland and Austria)

Additional exclusion criteria specific for Austria

1. Positive results on urine drug screen (amphetamines/metamphetamines, barbiturates, benzodiazepines, cannabinoids, cocaine, opiates).

2. Positive alcohol breath test.

3. Positive reaction to any of the following tests: hepatitis B surface (HBs) antigen, anti-hepatitis C virus (anti-HCV) antibodies, anti-human immunodeficiency virus (HIV) 1 antibodies, anti-HIV2 antibodies.

Related Conditions & MeSH terms

• Diabetes Mellitus, Type 1
• Type 1 Diabetes

Intervention

Device:
• Closed-loop using standard rapid-acting insulin
Closed-loop using standard rapid-acting insulin
• Closed-loop using faster insulin aspart
Closed-loop using faster insulin aspart

Locations

Country	Name	City	State
Austria	Medical University of Graz	Graz
Switzerland	Inselspital, Bern University Hospital	Bern
United Kingdom	Cambridge University Hospitals NHS Foundation Trust	Cambridge
United Kingdom	Manchester Royal Infirmary, Central Manchester University Hospitals NHS Foundation Trust	Manchester

Sponsors (4)

Lead Sponsor	Collaborator
University of Cambridge	Manchester University NHS Foundation Trust, Medical University of Graz, University Hospital Inselspital, Berne

Countries where clinical trial is conducted

Austria,  Switzerland,  United Kingdom, 

Outcome

Type	Measure	Description	Time frame	Safety issue
Other	Safety evaluation will comprise the number of episodes of hypoglycaemia, significant ketonemia (>3.0mmol/l) as well as nature and severity of any other adverse events.		Through study completion, an average of 5 months
Other	Utility evaluation is the frequency and duration of use of the closed-loop system at home.		8 week intervention period
Primary	Time spent in the target glucose range from 3.9 to 10.0 mmol/l based on subcutaneous glucose monitoring (CGM).		8 week intervention period
Secondary	Time spent above target glucose (3.9 to 10.0 mmol/l) based on continuous subcutaneous glucose monitoring (CGM)		8 week intervention period
Secondary	Time spent below target glucose (3.9 to 10.0 mmol/l) based on continuous subcutaneous glucose monitoring (CGM)		8 week intervention period
Secondary	Average, standard deviation and coefficient of variation of glucose levels based on continuous subcutaneous glucose monitoring		8 week intervention period
Secondary	The time with glucose levels < 3.5 mmol/l <3.0mmol/l and <2.8 mmol/l based on continuous subcutaneous glucose monitoring		8 week intervention period
Secondary	The time with glucose levels in the significant hyperglycaemia, as based on continuous subcutaneous glucose monitoring (glucose levels > 16.7 mmol/l)		8 week intervention period
Secondary	Low Blood Glucose Index (LBGI) based on continuous subcutaneous glucose monitoring		8 week intervention period
Secondary	Total, basal and bolus insulin dose		8 week intervention period