Prediabetic State Clinical Trial
Official title:
Autoimmune Diabetes Accelerator Prevention Trial - adAPT Stage 1
The autoimmune diabetes ACCELERATOR PREVENTION TRIAL (adAPT) is based on the accelerator
hypothesis. The trial is designed to establish whether metformin, an oral hypoglycaemic agent
that is known to reduce insulin demand in type 2 diabetes (T2D), can do the same in children
at risk of type 1 diabetes (T1D) and thereby prevent disease.
The first phase of adAPT will screen participants aged 5-16 years (inclusive) for
islet-related autoantibodies who are the siblings or offspring of individuals diagnosed with
T1D before the age of 25years in Scotland and England.
There are four principle islet-related antibodies associated with T1D. The presence of two or
more confers a 40% risk of developing T1D in five years. While the presence of none or one
antibody carries a similar risk for developing T1D to the general population (1 in 500 in
5years).
It is anticipated that 5% of those screened will be identified as double-antibody positive,
these participants will be invited to join the intervention phase of the study - randomised
controlled trial (RCT). Up to 200 eligible subjects could be identified by screening with a
minimum of 90 being enrolled into the RCT phase.
adAPT is a proposed three stage project. The current protocol defines the screening phase,
Stage 1 and seamless entry into Stage 2. Screening will identify children and young people at
high risk of developing T1D and invite them to participate in Stage 1 which will involve a
minimum of 4 months treatment with either metformin/placebo, however Stage1 treatment will
run seamlessly into Stage 2. Stage 1/2 treatment will last up to 21 months (to accommodate
15months screening, 4 months treatment and 2 months analysis). Post Stage1 analysis/ late
Stage 2 participation will last up to 36 months (participants enrolled early into Stage 1
will have the longest intervention).
During the Stage1 participants will be tested on three occasions (baseline, month 1 and month
4) for metabolic response using a 5-point mixed meal tolerance test (MMTT). Testing will
continue in Stage 1/2 with 3 visits further visits at months 8, 12, 18. Late Stage 2 visits
will occur on months 24, 30 & 36.
Participants will be invited to continue into Stage 3, taking treatment up to 60 months post
analysis of Stage 1 and associated protocol amendment and additional consent.
adAPT is a randomised double-blind placebo-controlled Phase IV clinical trial.
Metformin, a licensed medicine but will be tested out with its current license (off-label).
Participants will either receive metformin (liquid) or matched placebo in a double blind
manner; neither the participant or study team will know the allocation.
Metformin, the study medication, reduces the demand for insulin in Type 2 diabetes (T2D).
adAPT will test if metformin can also reduce insulin demand in children at risk of Type 1
Diabetes (T1D). adAPT has an adaptive design with each stage informing the next with
progression depend upon the previous stages outcome Stage 1 exposes each participant to
metformin or placebo for four months, following which they seamlessly enter Stage 2. However,
because recruitment rolls over 15 months many of those recruited early on will have entered
Stage 2 before some even reach Stage 1. Accordingly, the protocol and submission also
outlines Stages 2.
A successful Stage 1 will lead-on to a clinical outcome trial (Stages 2 and 3) which, if
successful, will fundamentally change our understanding of what causes diabetes and how to
prevent it. Stage 1 is required to confirm that adAPT trial design is achievable. Outcome
evaluation will be undertaken at 21 months. Stage 2 (proof-of-concept) will test if metformin
can slow-down the development of diabetes. The outcome data form Stage 1 will allow for power
to be calculated to drive the number of participants required for the study for Stages 2 (and
3). It is proposed that once the power and thus population numbers are established for Stage
2 (out with this protocol) that new participants will enter Stage 1 via screening and follow
the established trial pathway.
Diabetes biological markers will be measured and formally assessed at the end of Stage 2,
after 36 months. Stage 3 will occur if metformin treatment in Stage 2 is proven to be better
than placebo for slowing the development of diabetes. Stage 3 will further investigate the
development of diabetes between the groups, using biological markers and clinical outcomes at
five years.
Children/adolescents aged between 5-16 years (inclusive) at the time of screening and who are
siblings or offspring of people diagnosed with type 1 diabetes before the age of 25 are
eligible to be invited to participate in the screening phase of adAPT. Families/ children
will be invited to participate in screening and will informed of the study by invitation
letter (via the index T1D patient) from their designated clinician/Principal Investigator
(PI) or via their family practitioner through Scottish Primary Care Research Network/Clinical
Research Network (SPCRN/CRN). In addition potential participants may contact the study team
independently (self-referral) in response to media/press and internet coverage. Those invited
via letter will be requested to either return the reply slip, or call/Short Message Service
(SMS)/email the study team to register their interest.
Parent and child age-appropriate Screening Information will be provided and written consent
and assent will be completed. Consent/assent will only occur after a minimum of 24 hours has
elapsed from study information provision.
Screening will take place in clinically appropriate locations. Screening requires a small
non-fasting blood sample (3.5 mls). Participants will be offered topical anaesthesia prior to
the blood sample being taken.
This sample will be tested for four islet-related antibodies. Two or more antibodies will
infer a positive test, while one or less will conclude a negative test. It is anticipated
that approximately 5% of the screened population will present with a positive results and
thus a 40% risk of diabetes over 5 years and thus are eligible to be invited into Stage 1 of
the study. It is expected that 95% of people screened will test negative and their
participation will conclude (except for remote data linkage relating to diabetes diagnosis
for 10 years post study participation). The antibody tests are posted to the study's partner
laboratory in Bristol, United Kingdom (UK) with results being available within an 8 week
timeframe.
Antibody positive participants/families will receive a result consultation and an invitation
to the intervention stage of the study. Age-appropriate information sheets will be provided
for children/adolescents in addition to parents/guardian information.
If child/adolescent and parent/guardian assent/consent to participant in the RCT phase the
following visits will take place:
Stage 1 Month 0 (M0) visit - lasting approximately 2.5 to 3 hours:
Measure participant height, weight and waist circumference. Urine pregnancy test for all
menstruating female participants. Topical anaesthesia will be offered and applied if
participant agreeable. (Following assessment of anaesthesia) a cannula will be inserted for
blood sampling.
Safety blood samples to measure fasting glucose levels, full blood count, liver function,
urea and electrolytes. Samples sent to local National Health Service (NHS) hospital
accredited laboratories.
Research blood samples: Antibodies, Immunology, deoxyribonucleic acid (DNA -with consent and
Vitamin B12.
Mixed Meal Tolerance Testing (MMTT) baseline samples (Insulin, C-peptide and Glucose)
followed by Ensure Plus (or equivalent) drink at 6ml per kg dose (maximum 360ml) with 4
further blood tests being obtained at 30 minute intervals (via the in situ cannula) for 2
hours; Time points: 0, 30, 60, 90, 120 minutes.
Randomisation will occur following eligibility criteria and safety sample results review by
PI. If the participant is not eligible the participant and parent will be informed of the
rationale for non-eligibility and the participant' s family doctor will be informed of any
clinically significant findings (with consent.) Participants will be provided with study
medication (Metformin or placebo) and given instructions on dose and administration after
randomisation has taken place at M0 visit.
If eligible, more than one sibling can be screened and, if seropositive, recruited. To avoid
treatment contamination, immediate family members will be allocated to the same treatment
group, with the first family member tested being the one who is randomly allocated.
The required study medication dose is calculated using the participant's weight using a
dosing algorithm using 2.5kg increments to the nearest 0.5mls.
On commencement of treatment metformin can cause gastric intolerance, therefore to minimise
side effects for the first two weeks participants will be requested to take once daily
10mg/kg - half the target dose. Medication is administered/ taken orally.
Month 0 + 2 weeks:
Research nurse will contact the parent/participant to review tolerability and if tolerated
increase to twice daily dosing of 10mg/kg and will assess adverse event profile. New written
dosing instructions will be provided. If the participant is not tolerating dose they will be
withdrawn from the study.
Month 1 Visit - lasting approximately 2.5 to 3 hours:
Procedures are the same as M0 without an antibody blood sample. Study medication is increased
to the target dose of 20mg/kg, twice daily. Participants are provided with new written dosing
instructions.
Month 1 + 1 week:
Research nurse will phone the parent/participant to review tolerability of up-titrated dose
and assess adverse event profile. If the dose is not tolerated they their dose will be
reduced to the previous tolerated dose of 10mg/kg, twice a day which will continue for the
remainder of the trial. Where down-titration occurs new written dosing instructions will be
provided.
Month 4, 8, 12, 18, (Late Stage 2: 24, 30, 36) - lasting approximately 2.5 to 3 hours:
Procedures are the same as M0 with antibody sample. Clinical significant results will
reported as per local laboratory ranges and protocol.
Months 1, 2 & 3 and every 3 months or as required the research nurse will contact
parent/participant to assess adverse event profile.
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