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NCT02871089

Closed Loop From Onset in Type 1 Diabetes

Sponsor: University of Cambridge

View on ClinicalTrials.gov

Summary

The purpose of the study is to use a novel treatment approach, the artificial pancreas, after diagnosis of type 1 diabetes (T1D) to improve glucose control with the anticipated improvements of residual C-peptide secretion. This is an open-label, multicentre, single-period, randomised, parallel group design study. It is expected that a total of up to 190 subjects (aiming for 96 randomised subjects) will be recruited within ten working days of diagnosis of type 1 diabetes through paediatric diabetes centres in the UK. Half of the participants aged 10 to 16.9 years will be treated by conventional insulin injections and the other half by the artificial pancreas (closed loop insulin delivery system). Each treatment will last 24 months. All participants completing the 24 month study period will be invited to continue in an optional extension phase with the treatment allocated at randomisation for a further 24 months. Subjects in the intervention group will receive additional training on components of the artificial pancreas, i.e. insulin pump and continuous glucose monitoring (CGM), prior to starting closed loop insulin delivery. Subjects in the control intervention group will continue with standard therapy, i.e. multiple daily injection therapy. The study includes up to 14 visits and 1 telephone/email contact for subjects completing the study. After run-in and randomisation, visits will be conducted every 3 months in both arms. Beta-cell function will be assessed by serial measurement of C-peptide in response to a standardised mixed meal tolerance test (MMTT). MMTTs will be conducted at baseline, 6-,12- and 24 months post diagnosis. The primary outcome is the between group difference in the area under the stimulated C-peptide curve (AUC) of the MMTT at 12 month post diagnosis. Secondary outcomes include between group differences in stimulated C-peptide AUC over 24 months, differences in glycaemic control as assessed by HbA1c, time spent in glucose target range, glucose variability, hypo- and hyperglycaemia as recorded by periodically applied CGM, as well as insulin requirements and change in bodyweight. Additionally, cognitive, emotional and behavioural characteristics of participating subjects and parents will be assessed, and a cost utility analysis on the benefits of closed loop insulin delivery will be performed. Safety evaluation comprises assessment of the frequency of severe hypoglycaemic episodes, diabetic ketoacidosis (DKA) and number, nature and severity of other adverse events.

Official title: An Open-label, Multicentre, Randomised, Single-period, Parallel Design Study to Assess the Effect of Closed Loop Insulin Delivery From Onset of Type 1 Diabetes in Youth on Residual Beta Cell Function Compared to Standard Insulin Therapy

Key Details

Gender

All

Age Range

10 Years - 16 Years

Study Type

INTERVENTIONAL

Enrollment

Start Date

2017-01

Completion Date

2024-07-31

Last Updated

2024-05-16

Healthy Volunteers

Conditions

Diabetes Mellitus Type 1 Diabetes

Interventions

DEVICE

Closed-loop system (Florence M or CamAPS FX)

The automated closed-loop system (FlorenceM) will consist of: * Sensor augmented Medtronic insulin pump 640G (Medtronic Minimed, CA, USA) incorporating the Medtronic Enlite/Guardian 3 real time CGM and glucose suspend feature. * An Android smartphone containing the Cambridge model predictive algorithm and communicating wirelessly with the insulin pump using a proprietary translator device. The automated closed-loop system (CamAPS FX) will consist of: * Dana R or RS insulin pump * Dexcom G6 real-time CGM * CamAPS FX App on an unlocked android smartphone. Rapid acting insulin analogue will be used (insulin aspart, insulin lispro, insulin glulisine or similar or ultra-rapid insulin analogue).

OTHER

Multiple Daily Injections

Rapid acting insulin analogue and long acting insulin analogue will be subcutaneously administered using CE-marked insulin pen devices in accordance with the manufacturer's instructions for their intended purposes. Participants will be given long acting analogue (insulin glargine, insulin detemir or similar) once or twice daily according to their needs and boluses of rapid acting analogue (insulin aspart, insulin lispro, insulin glulisine or similar or ultra-rapid insulin analogue) when carbohydrates are consumed.

Inclusion Criteria: 1. Diagnosis of type 1 diabetes within previous 21 days. Day 1 will be defined as the day insulin was first administered. Type 1 diabetes will be defined according to WHO criteria using standard diagnostic practice. \[WHO definition: 'The aetiological type named type 1 encompasses the majority of cases with are primarily due to beta-cell destruction, and are prone to ketoacidosis. Type 1 includes those cases attributable to an autoimmune process, as well as those with beta-cell destruction for which neither an aetiology nor a pathogenesis is known (idiopathic). It does not include those forms of beta-cell destruction or failure to which specific causes can be assigned (e.g. cystic fibrosis, mitochondrial defects, etc.).'\] 2. The subject is at least 10 years and not older than 16.9 years 3. The subject/carer is willing to perform regular capillary blood glucose monitoring, with at least 4 blood glucose measurements taken every day 4. The subject is literate in English 5. The subject is willing to wear glucose sensor 6. The subject is willing to wear closed loop system at home 7. The subject is willing to follow study specific instructions 8. The subject is willing to upload pump and CGM data at regular intervals Exclusion Criteria: 1. Physical or psychological condition likely to interfere with the normal conduct of the study and interpretation of the study results as judged by the investigator 2. Current treatment with drugs known to interfere with glucose metabolism, e.g. systemic corticosteroids, non-selective beta-blockers and MAO inhibitors etc. 3. Known or suspected allergy to insulin 4. Regular use of acetaminophen 5. Lack of reliable telephone facility for contact 6. Pregnancy, planned pregnancy, or breast feeding 7. Living alone 8. Severe visual impairment 9. Severe hearing impairment 10. Medically documented allergy towards the adhesive (glue) of plasters or unable to tolerate tape adhesive in the area of sensor placement 11. Serious skin diseases (e.g. psoriasis vulgaris, bacterial skin diseases) located at places of the body, which potentially are possible to be used for localisation of the glucose sensor 12. Illicit drugs abuse 13. Prescription drugs abuse 14. Alcohol abuse 15. Sickle cell disease, haemoglobinopathy, receiving red blood cell transfusion or erythropoietin within 3 months prior to time of screening 16. Eating disorder such as anorexia or bulimia 17. Milk protein allergy

Locations (7)

Southampton Children's Hospital

Southampton, Hampshire, United Kingdom

Nottingham Children's Hospital

Nottingham, Nottinghamshire, United Kingdom

John Radcliffe Hospital

Oxford, Oxfordshire, United Kingdom

Alder Hey Children's NHS Foundation Trust

Liverpool, West Derby, United Kingdom

St James's University Hospital

Leeds, West Yorkshire, United Kingdom

Cambridge University Hospitals NHS Foundation Trust

Cambridge, United Kingdom

Royal Hospital for Sick Children

Edinburgh, United Kingdom