Effect of Postprandial Insulin Administration of Faster-acting Insulin Analogue Versus Pre-prandial Administration of Acting-insulin Analogue in Cystic Fibrosis Related Diabetes
NCT ID: NCT04381429
Last Updated: 2025-03-05
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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TERMINATED
PHASE4
38 participants
INTERVENTIONAL
2020-08-17
2025-01-20
Brief Summary
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Recent progress in the development of new insulins mimicking the physiological secretion more closely has led to ultra-fast insulins (fast aspart), allowing for postprandial hyperglycaemia to be better controlled. In Type 1 diabetics treated with basal-bolus, faster-acting aspart insulin injected after a meal enabled metabolic control comparable to injection of aspart insulin prior to the meal. Fast apart insulin is of particular interest with regard to CFRD, wherein postprandial hyperglycaemia occurs early. In CFRD, these insulins are likewise advantageous in that they can be injected after the meal, thus permitting more flexibility in patients with highly varied diets. Moreover, the insulin dose can be adapted depending on dietary intake, thus preventing hypoglycaemia secondary to highly-varied carbohydrate intakes. Due to its flexibility, this insulin therapy is likely to be better accepted by patients with cystic fibrosis.
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Detailed Description
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Patients with cystic fibrosis related diabetes and treated by multiple insulin injection (minimal three insulin injection per day or basal bolus insulin regimen) or insulin pump with CGM from over 3 months were included in an open, randomized, two-treatments - 4 periods of 3 months - 2 groups cross-over superiority study. Each group of patients will test both insulin treatments (A = pre prandial Aspart insulin, F = post prandial Faster-acting aspart insulin) in alternating periods with the following sequences: Group 1: A-F-A-F, Group 2: F-A-F-A The patients will be randomized to either one or the other sequence, which defines the groups, and take A or F in each of the 4 periods of the study. Each treatment period will last 3 months.
CGM (free style libre, Abott) will be performed for 2 weeks at baseline and after each 4 months period.
Conditions
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Study Design
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RANDOMIZED
CROSSOVER
TREATMENT
NONE
Study Groups
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Group 1: A-F-A-F
The study is an open, randomized, two-treatment - 4 periods of 3 months - 2 group cross-over superiority study.
All patients will test both insulin treatments (A and F) in alternating periods.
The patients of group 1 will start with pre-prandial aspart insulin (NovoRapid).
Each treatment period will last 3 months.
A-F-A-F (NovoRapid-FIASP-NovoRapid-FIASP)
A = pre-prandial aspart insulin (NovoRapid) F = post prandial Faster-acting aspart insulin (FIASP)
Groupe 2: F-A-F-A
The study is an open, randomized, two-treatment - 4 periods of 3 months - 2 group cross-over superiority study.
All patients will test both insulin treatments (A and F) in alternating periods.
The patients of group 2 will start with post prandial Faster-acting aspart insulin (FIASP).
F-A-F-A (FIASP-NovoRapid-FIASP-NovoRapid)
A = pre-prandial aspart insulin (NovoRapid) F = post prandial Faster-acting aspart insulin (FIASP)
Interventions
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A-F-A-F (NovoRapid-FIASP-NovoRapid-FIASP)
A = pre-prandial aspart insulin (NovoRapid) F = post prandial Faster-acting aspart insulin (FIASP)
F-A-F-A (FIASP-NovoRapid-FIASP-NovoRapid)
A = pre-prandial aspart insulin (NovoRapid) F = post prandial Faster-acting aspart insulin (FIASP)
Other Intervention Names
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Eligibility Criteria
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Inclusion Criteria
* Patient treated by multiple insulin injections (minimal three insulin injections per day or basal bolus insulin regimen) or insulin pump
* Patient with CGM from over 3 months (at the signature of the study's informed consent) or patient not wearing a CGM device, but agreeing a CGM at the inclusion and at the end of each treatment period of 3 months
* Naive patient of Fiasp or patient under Fiasp, having carried out a run-in period of one month with rapid acting insulin treatment
* Affiliated to a social security scheme
* Subject able to understand the objectives and the risks related to the research and to give a dated and signed informed consent
* Subject having been informed of the results of the prior medical examination
* Written informed consent, dated and signed before initiating any trial-related procedure (if the subject is a minor, the consent must be signed by the 2 legal representative and the patient if he/she is able to give consent)
Exclusion Criteria
* Patient with cystic fibrosis related diabetes treated with 2 injections / day
* Patient with an HbA1C greater than 12% who demonstrate therapeutic non-compliance
* Patient pregnant (positive urinary pregnancy test) or wishing to pregnancy
* Contraindication to Aspart insulin
* Patient on lung transplant waiting list or transplanted within one year prior to the inclusion visit
* Patient who started treatment with Trikafta® within 3 months prior to the inclusion visit
* Patient who cannot be followed during 12 months
* Subject in exclusion period (determined by previous or current clinical study)
* Impossibility of giving the subject enlightened information (subject in emergency situation, difficulties of understanding, cognitive impairment...)
* Subject under the protection of justice
* Subject under guardianship or curatorship
10 Years
ALL
No
Sponsors
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University Hospital, Strasbourg, France
OTHER
Responsible Party
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Locations
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Hôpitaux Universitaires de Strasbourg
Strasbourg, , France
Countries
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Other Identifiers
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7546
Identifier Type: -
Identifier Source: org_study_id
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