Mixed Meal Test in Type 1 Diabetes on Insulin Pump Therapy: Optimization of Artificial Pancreas

Type 1 Diabetes Mellitus Clinical Trial

Official title:

Meal Glucose Regulation in Type 1 Diabetes on Insulin Pump Therapy: Towards a Better Understanding of the Glucose-Insulin System.

Clinical Trial Details — Status: Active, not recruiting

Administrative data

• NCT number: NCT02003274
• Other study ID #: Verona Artificial Pancreas
• Status: Active, not recruiting
• Phase: N/A
• First received: December 3, 2013
• Last updated: June 29, 2017
• Start date: October 2013
• Est. completion date: October 31, 2017

Study information

• Verified date: March 2017
• Source: Azienda Ospedaliera Universitaria Integrata Verona
• Contact: n/a
• Is FDA regulated: No
• Study type: Interventional

Clinical Trial Summary

BACKGROUND. Optimal glucose control can prevent/relent tissue damage in patients with type 1 diabetes mellitus (T1DM). Ongoing efforts aim at developing closed loop control (CLC) algorithms linking subcutaneous continuous glucose monitoring (CGM) and insulin delivery (CSII). Substantial improvement towards an effective artificial pancreas system is still needed, especially in the regulation of post-meal glucose. Application of metabolic control analysis (MCA) can unveil and quantify distortions in the system properties of the glucose-insulin (pump) system (GIS), by measuring the coefficients of control (CCs) of glucose. Our approach rely on previous experience with our previous pilot protocol (NCT01800734).

AIM. We will outline and compare features of GIS in T1DM patients and in healthy controls during differently sized breakfast meals and during 24-hour periods. The reproducibility of our approach will also be assessed.

METHODOLOGY. Three protocols will be carried out. All T1DM patients will be on CGM/CSII therapy. In all three protocols, study 1 will be an euglycemic insulin clamp in T1DM patients and a frequently sampled intravenous glucose tolerance test (IVGTT) in healthy controls.

• Protocol 1: 10 T1DM patients on CGM/CSII and 10 control subjects will ingest a mixed meal of different size (320 and 640 kcal) on two separate occasions.

• Protocol 2: 5 T1DM patients will ingest two repeat 320 kcal meals, whereas other 5 T1DM patients will ingest two 640 kcal meals on two separate occasions.

• Protocol 3: 10 T1DM patients and 10 controls will be monitored for 24 hours, during which they will ingest 3 mixed meals.

Substrate (including CGM)/hormone responses will be measured in all studies. Comprehensive single meal and 24-hour models of GIS will be built, MCA will be applied and the CCs of glucose assessed, thereby allowing to outline and to compare the CCs of glucose between patients and controls.

EXPECTED RESULTS. Our data will be of use in devising novel clinical strategies in T1DM, including, but not limited to, development and refinement of CLC algorithms along the path towards an effective artificial pancreas system.

Description:

BACKGROUND: Ideally, optimal treatment of T1DM should achieve near-normal glucose with no hypoglycemias and preserved quality of life. In the clinical arena, even the currently available most complex strategy, i.e. glucose sensor augmented insulin pump therapy, in which patients wear both a pump for subcutaneous insulin delivery (CSII) and a subcutaneous glucose sensor for continuous glucose monitoring (CGM), does not fully meet the patients' needs. Artificial pancreas (AP) or integrated closed loop control (CLC) algorithms -which take into account CGM readings and the effects of previous insulin infusions to continuously compute the amount of insulin dose to be administered- aim to minimize, in real time, glucose variability and prevent extreme glucose excursions. A number of research groups have been brilliantly working for years to develop a wearable AP to partially, or totally, free the patient (and/or the caregiver) from the burden of the open loop control. However, a perfect glucose control is still lacking, especially in post-meal glycemic excursions. Further insights might be gained by studies of the substrate/hormone responses to meals in T1DM patients on sensor augmented CSII, possibly compared with the gold standard of normal physiology, with special regard to the relative role played by a number of factors of the glucose-insulin pump system in controlling glucose levels.

Metabolic control analysis (MCA) is a theoretical framework which aims at quantitatively describing metabolic systems and at gauging distribution of control. MCA quantifies the role of each component of a system (e.g.: absorption rate of the fast insulin analogue, carbohydrate absorption through the gut, etc.) in controlling a variable of interest, most notably fluxes or concentrations, of the system itself, by computing the scaled coefficient of controls (CCs). CCs typically range from -1 to +1, and the greater their absolute value, the stronger is the control. Application of MCA to T1DM patients on CGM/CSII could quantify the individual role played by each components of the system, and may help in understanding and potentially overcome the hindrances to achieve stable and tight glucose control and to further develop CLC algorithms for optimal management of the disease.

AIM: To investigate characteristics and determinants of the glucose-insulin pump system in patients with T1DM with CGM with particular emphasis on the system level (i.e. glucose CCs). We will perform single mixed meal tolerance tests as well as 24-hour studies in T1DM patients and in healthy controls. We will apply mathematical modelling tools developed by us and will create virtual patients and virtual controls from this database to gain further insights into the alterations of the glucose-insulin pump system in patients.

SPECIFIC AIMS:

• AIM 1: To outline and compare the features of the glucose-insulin system in T1DM patients and in healthy controls during breakfast meals of different sizes

• AIM 2: To test the reproducibility of model assessed glucose-insulin pump system in T1DM patients

• AIM 3: To outline and compare the features of the glucose-insulin system in T1DM patients and in healthy controls during 24-hour periods

HYPOTHESIS: We hypothesize that in T1DM patients on CGM and CSII:

1. there are distortions in the distribution of plasma glucose control, as assessed by MCA, when compared to healthy individuals;

2. the distribution of control is different between plasma glucose and glucose derived from presently used CGM, which is the putative signal to be used in CLC algorithms of a wearable AP;

3. both the above mentioned putative alterations need be taken into account to develop effective and safe CLC algorithms.

METHODS: This research is articulated in three distinct protocols. All subjects will be on an isocaloric, maze and cane sugar free diet for one week before study. All T1DM patients will be on CGM/CSII and will be recruited from the patient population attending our Outpatient Insulin Pump Therapy Clinic. Each patient will continue to use his/her own pump device, insulin analogue and glucose sensor. All studies will start at 07:00 AM after an overnight fast (≥ 10 hours). All blood samples will be collected in refrigerated tubes and promptly spun at 1500 g; plasma will be separated and stored at -80° C. According to the planned use of plasma, tubes for blood samples will contain ethylenediaminetetraacetic acid (EDTA) for anticoagulation±antiglicolytic agent±serine protease and DPP4 inhibitors.

-PROTOCOL 1: Investigation of the glucose-insulin system during two mixed meal tests in T1DM patients and in healthy controls.

10 T1DM patients and 10 healthy age gender and BMI matched control subjects will be recruited. Patients will be on their usual insulin pump therapy, and the rate of the basal insulinization will be kept constant from 02:00 AM until the end of studies. All subjects will be studied on 3 separate occasions at 1-2 weeks intervals. In patients, study 1 will be a standard 120 min euglycemic insulin clamp. Timed blood samples will be collected to measure insulin levels at 10'-30' intervals. Plasma glucose will be measured at bedside by a YSI Glucose Analyzer; subcutaneous glucose will be monitored by CGM. In controls, study 1 will be a frequently sampled IVGTT of 240 min of duration. Timed blood samples (n=27) for glucose, C-peptide and insulin will be collected. Studies 2 and 3 will be identical in both patients and controls. They will be performed in randomized order and will last 360'. After a 60 min baseline period, at time 0' subjects will ingest either a 320 kcal (study 2) or a 640 kcal (study 3) meal. Meal composition (%Kcal: 53.3% carbohydrate, 28.2% lipid, 18.5% protein) will be Indian corn polenta plus parmesan cheese. Patients will program their pump to inject at time 0' a meal insulin bolus dose, calculated as usual. Blood samples (n=20) will be collected at timed intervals to measure plasma glucose, 13C/12C-glucose ratio, insulin, glucagon and C-peptide (the latter one only in control subjects). At a lower time frequency, triglycerides, non-esterified fatty acids (NEFA), active glucagon-like peptide-1 (GLP1) and total gastric inhibitory peptide (GIP) will also be measured. Subcutaneous glucose will be monitored by CGM only in patients. Data derived from IVGTT in controls will take the role played by the insulin clamp data in T1DM patients. Past experiments and also unpublished observations in our laboratory have shown that similar values of insulin sensitivity are obtained with IVGTT and insulin clamps in healthy people. The other difference is that, instead of the insulin pump, a beta cell secretion minimal model will be used, as previously described. The availability of 12C/13C-glucose ratio determinations will enrich further this picture, allowing to compute the contribution of meal carbohydrate to total plasma glucose and, by difference, the contribution of endogenous (primarily liver) production to total glucose. This data enrichment will result into further model development at step 3 (in both controls and patients) and will allow to split total insulin action into its two components, the one acting on endogenous glucose production and the one acting on glucose utilization. The former will be relevant to interpret the glucagon and, possibly, also the active GLP1 data.

With this strategy, it is possible to compute all relevant CCs of G(t), for both plasma and CGM values. Phenotypic results are layered in three levels of ascending complexity:

1. Model-free measurements: meal substrate and hormone levels, with particular regard to glucagon and active GLP1 for their action on liver glucose production and to total GIP, as a regulator of fat cell metabolism;

2. Model-derived estimates of single traits of the glucose/insulin system: they include, but are not limited to, glucose-sensitivity (SG), insulin sensitivity (SI), carbohydrate transit time to reach systemic circulation, mean transit time of insulin to reach systemic circulation from the subcutaneous depot (only patients);

3. Model-derived assessment of system properties of the glucose-insulin system (controls) and of the glucose-insulin pump system (T1DM) patients: they include all the glucose (also CGM glucose in patients) coefficients of control.

PROTOCOL 2: Reproducibility of the assessment of the glucose-insulin system during a single mixed meal test in T1DM patients.

10 T1DM patients on insulin pump therapy and subcutaneous continuous glucose monitoring (CGM) will be recruited. The study protocol is identical to protocol 1 with the following exceptions: 1. in 5 T1DM patients study 2 and study 3 will be two repeated 320 kcal meals; 2. in 5 T1DM patients study 2 and study 3 will be two repeated 640 kcal meals. The phenotypic results will be layered as in protocol 1 for reproducibility analysis.

-PROTOCOL 3: The glucose-insulin system during a 24-hour period in T1DM patients and in controls.

10 T1DM patients and 10 healthy age gender and BMI matched control subjects will be recruited. All subjects will be studied on 2 separate occasions at 1-2 weeks intervals. Both in patients and in controls, study 1 will be identical to protocol 1 (i.e. an insulin clamp and an IVGTT, respectively). In study 2 all subjects will be admitted to the Clinical Research Center (CRC) on the morning of the study (07:00 AM) and will stay there for its entire duration (24 hours). Subjects will be allowed to move freely within the CRC, but they will not be engaged in any physical exercise. Patients will continue their usual insulin therapy, including meal insulin dose calculation and injection, throughout the study. At 08:00 AM, 13:00 and 19:00 subjects will ingest three mixed meals (200 kcal/m-2 of Body Surface Area (BSA), 400 kcal/m-2 BSA and 400 kcal/m-2 BSA, respectively; diet composition: 54% carbohydrate, 28% lipid, 18% protein). In 6 patients and in 6 controls, the 13:00 meal will be Indian corn polenta plus seasoned Italian DOP parmesan cheese. In the other 6 patients and 6 controls, the 19:00 meal will be Indian corn polenta plus seasoned Italian DOP parmesan cheese. Timed blood samples (n=62) will be collected. Plasma glucose, insulin, glucagon and C-peptide (the latter one only in control subjects) will be measured at all time points. At a lower time frequency, triglycerides, non-esterified fatty acids (NEFA), amino acids, active GLP1 and total GIP will also be measured. In those subjects ingesting the polenta meal at 13:00, the 13C/12C-glucose ratio will be measured from 12:00 until 24:00. In those subjects ingesting the polenta meal at 19:00, the 13C/12C-glucose ratio will be measured from 18:00 until 07:00 the morning after. Subcutaneous glucose will be monitored by CGM only in patients. The polenta meal will be used only in one meal per day to avoid loss of interpretability of 13C/12C-glucose ratio data, owing to ongoing glucose carbon recirculation/recycling through glycogen/gluconeogenesis. The behaviour of the glucose/insulin system at breakfast time is already explored in Protocol 1. Results will be layered and analyzed as described in Protocol 1.

EXPECTATIONS: The combined analysis of insulin clamp and mixed meal test (MMT) data will allow to build a comprehensive model of the glucose insulin system during a MMT in each subject, which will thereby work as an in silico virtual patient, according to a well established methodology developed in our laboratory. The collection of virtual patients with type 1 diabetes undergoing a MMT will form the in silico biobank derived from this study. Virtual patients will be used to carry out MCA to compute CCs. Furthermore, the incretin hormone, glucagon and substrate response to a mixed meal will be quantified, allowing the putative identification of further modifiers of the glucose-insulin system. This database will be instrumental in devising a control algorithm able to guarantee a normal glucose regulation during a mixed meal in patients with type 1 diabetes with CGM on insulin pump therapy.

Recruitment information / eligibility

• Status: Active, not recruiting
• Enrollment: 20
• Est. completion date: October 31, 2017
• Est. primary completion date: October 2016
• Accepts healthy volunteers: Accepts Healthy Volunteers
• Gender: All
• Age group: 18 Years to 65 Years

Eligibility

Inclusion Criteria:

• patient must be aged between 18 (inclusive) and 65 years old;

• patient must have been diagnosed with type 1 diabetes(positive islet cell antibodies;

• use of an insulin pump to treat his/her diabetes for at least 1 year;

• actively using a carbohydrate/insulin ratio for insulin bolus adjustments in order to keep blood glucose in a predefined range;

• patient HbA1c is between 6,0% and 9,0% (standardized with DCCT);

• patient must be willing to avoid consumption of acetaminophen containing products during the study involving DexCom (one CGM system which will be employed in this study) use;

• patient must demonstrate proper mental status and cognition for the study;

• patient has signed informed consent from prior to study entry.

Exclusion Criteria:

• diabetic ketoacidosis within the 6 months prior to enrollment;

• severe hypoglycemia resulting in seizure or loss of consciousness in the 12 months prior to enrollment;

• pregnancy and breast feeding;

• uncontrolled microvascular (diabetic)complications (other than diabetic non-proliferative retinopathy)such as history of laser coagulation, proliferative diabetic retinopathy, known diabetic nephropathy (other than microalbuminuria with normal creatinine) or neuropathy requiring treatment;

• uncontrolled arterial hypertension (diastolic blood pressure >90 mmHg and/or systolic blood pressure >160 mmHg);

• conditions which may increase the risk of hypoglycemia such as uncontrolled coronary artery disease during the previous year (e.g. history of myocardial infarction, acute coronary syndrome, therapeutic coronary intervention, coronary bypass or stenting procedure, stable or unstable angina, episode of chest pain of cardiac etiology with documented EKG changes, or positive stress test or catheterization with coronary blockages >50%), congestive heart failure, history of cerebrovascular event, seizure disorder, syncope, adrenal insufficiency, neurologic disease or atrial fibrillation;

• drugs affecting glucose metabolism (oral steroids, thiazide diuretic, beta-blockers,beta-agonist, nicotinic acid, immunosuppressant agents, antiretroviral drugs and antipsychotics);

• impaired hepatic function measured as alanine aminotransferase or aspartate aminotransferase > three times the upper reference limit;

• impaired renal function measured as creatinine >1.2 times above the upper limit of normal; anticoagulant therapy other than aspirin;

• known current or recent alcohol or drug abuse;

• psychiatric disorders that would interfere with study tasks (e.g. inpatient psychiatric treatment within 6 months prior to enrollment);

• mental incapacity, unwillingness or language barriers precluding adequate understanding or cooperation.

Related Conditions & MeSH terms

• Diabetes Mellitus
• Diabetes Mellitus, Type 1
• Type 1 Diabetes Mellitus

Intervention

Other:
• Clamp-Mixed Meal
Standard clinical parameters will be assessed in all patients. Metabolic tests: A. Euglycemic insulin clamp. A standard euglycemic insulin clamp will be carried out in type 1 diabetic patients to assess insulin sensitivity, as previously described (1). B. Mixed meal test. All participants will ingest a standardized mixed meal and will be monitored for 300 minutes thereafter. Right before meal ingestion, a s.c. fast insulin analogue bolus will be administered by the pump This test will determine the time courses of: 1. plasma glucose, 2. 13C/12C glucose ratio (hence, meal-derived and endogenous glucose), 3. insulin, 4. free fatty acids, 5. aminoacids, 6. glucagon, 7. incretin hormones 8. glucose control coefficients (CCs) during a mixed meal.
• IVGTT-Mixed Meal Arm
Standard clinical parameters will be assessed in all subjects. Metabolic tests: A. IVGTT. A frequently sampled intravenous glucose tolerance test (IVGTT) in healthy controls will be carried out in study 1 and study 3 to assess insulin sensitivity. B. Mixed meal test. All participants will ingest a standardized mixed meal and will be monitored for 300 minutes thereafter. This test will determine the time courses of: 1. plasma glucose, 2.13C/12C glucose ratio (hence, meal-derived and endogenous glucose), 3. insulin, 4. free fatty acids, 5. aminoacids, 6. glucagon, 7. incretin hormones 8. glucose control coefficients (CCs) during a mixed meal.

Locations

Country	Name	City	State
Italy	Clinical Research Center-University Hospital of Verona	c/o Policlinico G.B. Rossi - Piazzale L.A. Scuro, 10	Verona
Italy	Division of Endocrinology and Metabolic Diseases - University Hospital of Verona	Piazzale Stefani 1-Pad. 22	Verona

Sponsors (3)

Lead Sponsor	Collaborator
Azienda Ospedaliera Universitaria Integrata Verona	European Foundation for the Study of Diabetes, Universita di Verona

Country where clinical trial is conducted

Italy, 

References & Publications (6)

Bergman RN, Phillips LS, Cobelli C. Physiologic evaluation of factors controlling glucose tolerance in man: measurement of insulin sensitivity and beta-cell glucose sensitivity from the response to intravenous glucose. J Clin Invest. 1981 Dec;68(6):1456-67. — View Citation

Bonetti S, Trombetta M, Boselli ML, Turrini F, Malerba G, Trabetti E, Pignatti PF, Bonora E, Bonadonna RC. Variants of GCKR affect both ß-cell and kidney function in patients with newly diagnosed type 2 diabetes: the Verona newly diagnosed type 2 diabetes study 2. Diabetes Care. 2011 May;34(5):1205-10. doi: 10.2337/dc10-2218. Epub 2011 Mar 16. — View Citation

Cobelli C, Toffolo GM, Dalla Man C, Campioni M, Denti P, Caumo A, Butler P, Rizza R. Assessment of beta-cell function in humans, simultaneously with insulin sensitivity and hepatic extraction, from intravenous and oral glucose tests. Am J Physiol Endocrinol Metab. 2007 Jul;293(1):E1-E15. Epub 2007 Mar 6. Review. — View Citation

Fell DA. Metabolic control analysis: a survey of its theoretical and experimental development. Biochem J. 1992 Sep 1;286 ( Pt 2):313-30. Review. — View Citation

Marchetti L, Reali F, Dauriz M, Brangani C, Boselli L, Ceradini G, Bonora E, Bonadonna RC, Priami C. A Novel Insulin/Glucose Model after a Mixed-Meal Test in Patients with Type 1 Diabetes on Insulin Pump Therapy. Sci Rep. 2016 Nov 8;6:36029. doi: 10.1038/srep36029. — View Citation

Trombetta M, Boselli L, Cretti A, Calì A, Vettore M, Caruso B, Dorizzi R, Avogaro A, Muggeo M, Bonora E, Bonadonna RC. Type 2 diabetes mellitus: a disease of the governance of the glucose-insulin system: an experimental metabolic control analysis study. Nutr Metab Cardiovasc Dis. 2013 Jan;23(1):23-30. doi: 10.1016/j.numecd.2011.05.006. Epub 2011 Sep 19. — View Citation

Outcome

Type	Measure	Description	Time frame	Safety issue
Primary	1. Composite plasma glucose and hormone responses to a mixed meal; 2. Glucose control coefficients	Timed curves of composite plasma glucose, meal-derived glucose, endogenous glucose, insulin, glucagon and incretin hormone concentrations in response to a mixed meal.; Composite glucose control coefficients (CCs) of each component of the glucose-insulin system at each time point of the mixed meal.	24 months
Secondary	Composite plasma free fatty and amino acid responses to a mixed meal	Composite timed curves of plasma free fatty and amino acid concentrations to a mixed meal.	24 months