Diabetes Mellitus, Type 1
Conditions
Brief summary
The main objective is to determine the feasibility of dasiglucagon in a bi-hormonal reactive closed loop system for automated glucose regulation (artificial pancreas; AP®) in patients with diabetes mellitus type 1. Safety parameters and pharmacodynamics are compared between Dasiglucagon and GlucaGen®. This study is a single-center, double-blinded, randomized, cross over trial in 12 subjects. The subjects will be randomized to receive either dasiglucagon or GlucaGen® for the first three day study period and switch to the alternate treatment after a wash-out treatment.
Detailed description
Background of the study: Inreda Diabetic B.V. (Goor, The Netherlands) developed a bi-hormonal reactive closed loop system to automate glucose regulation (artificial pancreas; AP) in patients with diabetes mellitus type 1. In the current CE-marked AP, GlucaGen® (Novo Nordisk, Denmark) is used as glucagon. This glucagon formulation is not stable and therefore fibrillation and infusion set occlusion could occur, resulting in reduced glucagon action with risk for hypoglycemia. Dasiglucagon (Zealand Pharma, Denmark) is a glucagon analog stable in aqueous solution and does therefore not suffer from fibrillation. Objective of the study: The main objective is to determine the feasibility of dasiglucagon in the Inreda AP-system. Secondary objectives are to assess safety parameters, differences in pharmacodynamics between dasiglucagon and GlucaGen® and differences in AP related outcomes. Study design: This study is a single-center, double-blinded, randomized, cross over trial which will be performed out-patient. Study population: The study population will comprise 12 subjects with diabetes type 1 using the AP system. Inclusion criteria are subjects from 18 years and older and treated with the Inreda AP system for a minimum of 1 month. Intervention: The intervention contains use of dasiglucagon administered by the Inreda AP-system. The subject will be randomized to receive either dasiglucagon or GlucaGen® during the first three days. After a wash-out period of four days, the subject will be switched to the alternate treatment. During both study periods subjects have to keep a diary, perform exercise, keep a WiFi access point with them, and have some eating restrictions. Primary study parameters/outcome of the study: Main parameter to express feasibility is the time in range (3.9 - 10.0 mmol/l), which will be compared between the dasiglucagon and reference glucagon. Secondary study parameters/outcome of the study: * Safety will be expressed as side effects of dasiglucagon compared to side effects of GlucaGen. * The amount of extra food intakes to prevent/ combat hypoglycemia. * Pharmacodynamics will be expressed in proportion of time spent in hypo-/hyperglycemia, median/mean glucose value, glycemic variability and PD curves, which will all be compared between the dasiglucagon and reference glucagon. * AP related outcomes will be expressed in daily administered (maintenance) dosage of insulin/glucagon and the percentage of time that the closed loop algorithm is active.
Interventions
DRUGDasiglucagon
Use of dasiglucagon in the AP system.
DRUGGlucaGen
Use of GlucaGen in the AP system.
Sponsors
Inreda Diabetic B.V.
Study design
Allocation
RANDOMIZED
Intervention model
CROSSOVER
Primary purpose
OTHER
Masking
QUADRUPLE (Subject, Caregiver, Investigator, Outcomes Assessor)
Masking description
Investigational Medicinal Product dasiglucagon and control GlucaGen are masked as either treatment A or B. Only the assistant researcher who does the preparation and allocation of the drugs has this key.
Intervention model description
Three days treatment A, four days wash out period (standard treatment), three days treatment B.
Eligibility
Sex/Gender
ALL
Age
18 Years to 75 Years
Healthy volunteers
No
Inclusion criteria
* Diagnosed with diabetes mellitus type 1; * Treated with the Inreda AP system for a minimum of 1 month; * Age between 18 and 75 years; * Adequate contraception is required (only applicable for female participants); * Willing and able to sign informed consent. Since subjects are treated with the Inreda AP, the following inclusion criteria will be met: * Treated with SAP or CSII for a minimum of 6 months; * HbA1c \< 97 mmol/mol; * BMI \< 35 kg/m2; * No use of acetaminophen, as this may influence the sensor glucose measurements.
Exclusion criteria
* Impaired awareness of hypoglycemia (score ≥ 4) according to Gold and/or Clarke questionnaire \[3\], \[4\]; * Pregnancy and/or breastfeeding; * Use of oral antidiabetic agents; * Pheochromocytoma; * Insulinoma; * Severe liver/heart/renal failure; * Alcohol abuse; * Hypersensitivity reactions to dasiglucagon, glucagon or any of the excipients;
Design outcomes
Primary
| Measure | Time frame | Description |
|---|---|---|
| Time in range | 3 days | Time of glucose concentration in the range 3.9-10.0 mmol/L in % |
Secondary
| Measure | Time frame | Description |
|---|---|---|
| Extra food intakes (food intake diary) | 3 days | The participant is instructed to eat the same meals in the intervention and control period. Except extra food intakes when needed to prevent/combat hypoglycemia. Food intakes not present in the other period are extra food intakes. |
| Pharmacodynamics - hypo/hyper | 3 days | Time spent in hypo-/hyperglycemia in percent |
| Pharmacodynamics - glucose value | 3 days | Median glucose value in mmol/L |
| Side effects | 3 days | Side effects of dasiglucagon and GlucaGen |
| Pharmacodynamics - PD curves | 3 days | Pharmacodynamics curves |
| AP related parameters - doses | 3 days | Daily administered dose of insulin and glucagon in units |
| AP related parameters - algorithm | 3 days | Time that algorithm is active in percent |
| Pharmacodynamics - glycemic variability | 3 days | Coefficient of variation (Standard deviation divided by the mean) in percent |
Countries
Netherlands
Outcome results
None listed