Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT01269047 |
| Other study ID # |
2010 -436 |
| Secondary ID |
R01DK077166 |
| Status |
Completed |
| Phase |
Phase 4
|
| First received |
December 29, 2010 |
| Last updated |
March 13, 2018 |
| Start date |
August 2009 |
| Est. completion date |
December 2016 |
Study information
| Verified date |
March 2018 |
| Source |
Albert Einstein College of Medicine, Inc. |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
The main purpose of the study is to determine the effects of 16 weeks of adjunctive
pramlintide or exenatide use on glycemic control in Type 1 Diabetes.
Description:
After signing an informed consent, prior to study enrollment, a screening evaluation will be
performed in the Clinical Research Center (CRC).
The evaluation will consist of: a medical history, a physical examination with vital signs,
Tanner staging, and a waist circumference. The following laboratory tests will be done: CBC,
HbA1c, creatinine,Liver function tests, amylase, lipid profile, lipase, urine for pregnancy
test (when appropriate) and microalbumin. A urine pregnancy test will be done at each study
visit in menstruating females. Also an anti-GAD,IA12, and anti-insulin antibody test will be
done, if they were not previously done or if records are not available. Each subject will
have a continuous glucose monitoring sensor (CGMS) inserted and will need to wear it for 3
days (72 hours). A person,trained to insert the subcutaneous sensor, will insert the sensor.
The sensor is inserted subcutaneously with an injector device. This site insertion is very
similar to an insulin pump site insertion. A recorder is attached to the sensor and records
blood glucose data for 72 hours. The subject will need to test their blood glucose at least 4
times a day while wearing the sensor. The subject will be asked to keep a log on diet,
insulin and exercise while wearing the CGMS. At the end of the 3 day sensing period, the
subject will remove the sensor and place the recorder on a charger. The sensor will be
brought back by the subject to Visit #1. A Mixed Meal Tolerance Test will be performed at
this visit (as described below): Preparation for Mixed Meal Tolerance Test (MMTT)
1. The test will be performed in the morning (between 7 and 10 AM)
2. Test will be conducted only if fasting value by capillary blood glucose meter is between
70-200 mg/dl (3.9-11.1mMol). If the blood glucose prior to start of MMTT is greater than
350 mg/dl, then urine ketones will be measured. If a subject's blood glucose is less
than 70 mg/dl before the Mixed Meal Tolerance Test, they will receive 5-10 grams of
dextrose 50% by IV. If a subject develops hyperglycemia after the MMTT (which is
expected), they will receive a supplemental bolus of fast acting insulin based on their
usual insulin sensitivity factor. The subject will be instructed by the study staff on
the amount needed. The subject will administer the bolus by themselves
3. Participants on injections will not withhold taking long acting insulin on the morning
of the test. Participants can take very short acting insulin (e.g. Humalog or Novolog)
up to 2 hours before the test if necessary and then that will be withheld during the
test.
4. Participants on insulin pumps will continue with the normal basal rate. Participants can
take very short acting insulin (e.g. Humalog or NovoLog) up to two hours before the test
if necessary.
5. The participant will be fasting for at least 8 hours and will have had no food or drink
(with the exception of water).
6. Local anesthetics may be used as needed to start the I.V. line. Conducting the Mixed
Meal Tolerance Test (MMTT)
1. Baseline blood samples will be drawn at -30 minutes; -10 minutes and 0 minutes
(immediately before the participant starts drinking the liquid meal) Baseline samples will
include glucose, insulin, C-peptide, amylin, GLP-1, glucagon and active ghrelin.
2. The participant will have a standardized liquid meal: Boost HP 6 ml/kg, with a maximum of
360 ml, to be ingested within 5 minutes.
3. Blood samples will be drawn at times: 15, 30, 60, 90 and 120 minutes for glucose, insulin,
C-peptide, amylin, GLP-1,active ghrelin and glucagon after the start of ingestion of Boost.
4. After the test is completed, the participant will receive their usual morning dose of
short acting insulin analog. The short acting analog will be dosed according to the subject's
usual sensitivity factor and insulin to carbohydrate ratio for breakfast as prescribed by the
investigator. Subjects on insulin pump therapy will receive a short acting analog via the
pump, dosed according to the subject's usual sensitivity factor and insulin to carbohydrate
ratio for breakfast as prescribed by the investigator. Subjects will receive a meal tray once
the premeal insulin is administered. A total of 107.6 ml of blood will be drawn at the
screening visit.
Visit 1 (0 months):
If subjects qualify after screening, they will have the opportunity to enroll in the study.
They will meet with a study coordinator in the CRC to make adjustments to their insulin
dosage (if necessary) to optimize treatment and improve glycemic control. As shown in the
preliminary data section, insulin glargine (Lantus), a long acting analog, may be used when
mixed with short acting insulin analogs so as to decrease the total number of injections.
This may also increase compliance to the medication regimen. Parental supervision for
medication administration will be advised. Hypoglycemic events and adherence to insulin
regimen will be noted. Subjects will have vital signs, waist circumference, HbA1C, Glycomark,
and a urine pregnancy test (as appropriate).Dual-emission X-ray absorptiometry (DEXA) body
scan will be done on this day to estimate total body fat. Patients will also be asked to
bring in food diary kept for 3 days so that it can be analyzed for calories being consumed.
During the entire study period, subjects will be assessed using a home blood glucose monitor
that will electronically transfer data to PI (Glucomon). Data will be reviewed daily for week
1 and 2, and then once a week for week 3 and 4. Starting at week 5, data will be reviewed
once every two weeks for the remainder of the study. Contact will be similar for all
subjects. Subjects will receive their Glucomon at this visit. At this visit, subjects will be
randomized into one of three possible groups.
Randomization: Subjects will be randomized using a random number table. Group 1: Pramlintide
+ Insulin Group 2: Exenatide + Insulin Group 3: Insulin monotherapy
Study Medications:
Exenatide dosing: Exenatide will be started at 1.25 mcg as previously determined by us in an
earlier study. Exenatide injection will be given subcutaneously twice a day (within 30
minutes after the start of the meal) and will be separate from insulin injections. Exenatide
dose will be titrated to 2.5 or 5 mcg (depending on response) to keep 2 hr post-prandial
blood glucose concentrations below 200 mg/dl. Initially, premeal bolus insulin dose will be
reduced by 30%. Basal insulin dose will not be changed. Insulin dose may be increased if
pre-meal blood glucose concentrations are greater than 150 mg/dl or to decrease post-prandial
hyperglycemia.
Pramlintide dosing: Based on our preliminary studies, pramlintide will be started at 15 mcg
and then titrated up to 30-45 mcg and capped at 60 mcg. This will be based on demonstration
of acceptable post-prandial glucose excursions without hypoglycemia. Subjects will receive
pramlintide subcutaneously twice a day (within 30 minutes after the start of the meal) and
will be separate from insulin injections. Initially, premeal bolus insulin dose will be
reduced by 30%.Insulin dose may be increased if pre-meal blood glucose concentrations are
greater than 150 mg/dl or to decrease post-prandial hyperglycemia.
At the outset, we will decrease premeal bolus insulin dose by 30% for both groups, but
insulin may be increased as necessary once the subjects are better able to tolerate the drugs
(personal communications regarding unpublished data with Dr. David Maggs, Amylin
pharmaceuticals, on the management of exenatide and/or pramlintide with insulin).
Insulin monotherapy: Subjects randomized to insulin monotherapy will continue on either
long-acting and short acting insulin analogs or subcutaneous insulin pump therapy. Insulin
dose changes will only be made to optimize therapy.
A total of 5.5 ml of blood will be drawn at the Visit 1.
Visit 2 (1 month):
Subjects will have vital signs, waist circumference, HbA1C, Glycomark, and a urine pregnancy
test (as appropriate).
Adherence to insulin/medication regimen and adverse event reporting will be obtained.
A total of 5.5 ml of blood will be drawn at the Visit 2.
Visit 3 (4 months):
Subjects will undergo a medical history, physical examination, vital signs, waist
circumference, HbA1C, Glycomark,amylase, lipase, Liver function tests, CBC, creatinine,
adiponectin, leptin, C-reactive protein, lipid profile, IL-6, and a urine pregnancy test (as
appropriate) . Adherence to insulin/medication regimen and adverse event reporting will be
obtained. Quality of Life (QOL) questionnaires will be repeated. Additionally, subjects will
come in fasting and undergo a MMTT as described in the Screening visit but if subjects are on
pramlintide/ exenatide (Byetta) they will receive that dose prior to the boost
administration. DEXA scan will be done on this day to estimate total body fat. Patients will
also be asked to bring in food diary kept for 3 days so that it can be analyzed for calories
being consumed. Each subject with have a continuous glucose monitoring sensor (CGMS) inserted
and will need to wear it for 3 days (72 hours). A person, trained to insert the subcutaneous
sensor, will insert the sensor. The subject will receive instruction on completion of
logsheets and how to properly remove the sensor. Pramlintide and exenatide will be stopped
after the subject removes the sensor which is again 3 days from its insertion. Each family
would be given a prepaid envelope to mail back the sensor recorder and the remaining study
medication. A total of 104.6 ml of blood will be drawn at the Visit 3. Control subjects
during the MMTT will receive pramlintide or exenatide as a one time dose without insulin.
Visit 4 (6-7 months):
This will be a post-study visit. Subjects will undergo a medical history, physical
examination, vital signs, waist circumference. This visit will be similar to visit 3 for
testing and lab work and pregnancy test (as appropriate). Except that the subject will not
have DEXA scan and a Continuos Glucose Monitoring Sensor. If the subject received pramlintide
previously as study drug in visit 3 they will receive exenatide as a one time dose with the
MMTT. QOL questionnaires will be repeated. Adherence to insulin regimen and adverse event
reporting will be obtained. Subjects will return their Glucomon and all the blood glucose log
books at this visit. A total of 104.6 ml of blood will be drawn at the Visit 4.
During the entire study period, subjects will be assessed using data collected from a study
issued home blood glucose monitor. The subject's blood glucose data will be electronically
transmitted to the PI ensuring data security and patient privacy. Data will be reviewed daily
for weeks 1 and 2, and then once a week for weeks 3 and 4. Starting at week 5,data will be
reviewed once every two weeks for the remainder of the study.
Other known NCT identifiers
