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ZP4207(Dasiglucagon) Administered to T1D Patients to Assess the PK and PD Compared to Marketed Glucagon

Primary Purpose

Diabetes Mellitus Type 1

Status
Completed
Phase
Phase 2
Locations
Germany
Study Type
Interventional
Intervention
ZP4207(dasiglucagon) glucagon analogue
Glucagon (Native glucagon)
Sponsored by
Zealand Pharma
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional treatment trial for Diabetes Mellitus Type 1

Eligibility Criteria

18 Years - 64 Years (Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

To be included in the trial, patients have to fulfil all of the following criteria:

  1. Signed and dated informed consent obtained before any trial-related activities. (Trial-related activities are any procedures that would not have been performed during normal management of the patient).
  2. Male and female patients with T1DM for at least 1 year, as defined by the American Diabetes Association1.
  3. Age between 18 and 64 years, both inclusive.
  4. HbA1c < 8.5%.
  5. C-peptide negative defined as below the lower limit of quantification.
  6. Stable insulin regimen via an insulin infusion pump for at least 1 month prior to screening.
  7. Weight between 60 kg and 90 kg, both inclusive.
  8. Patients in good health according to age (medical history, physical examination, vital signs, 12-lead ECGs, lab assessments), as judged by the Investigator.-

Exclusion Criteria:

Patients meeting any of the following criteria during screening evaluations will be excluded from trial participation:

  1. Unable to provide informed consent (e.g., impaired cognition or judgement).
  2. Patients with mental incapacity or language barriers which preclude adequate understanding or cooperation, who are unwilling to participate in the trial, or who in the opinion of the Investigator should not participate in the trial.
  3. Receipt of any medicinal product in clinical development within 3 months prior screening.
  4. Previous exposure to ZP4207(dasiglucagon) or previously randomized to this trial.
  5. Known or suspected allergy to trial product(s) or related products.
  6. History of adverse reaction to glucagon (including allergy) besides nausea and vomiting.
  7. History of multiple and/or severe allergies to drugs or foods or a history of severe anaphylactic reaction.
  8. New onset clinically significant illness within 4 weeks prior to screening, as judged by the Investigator.
  9. History of liver disease that is expected to interfere with the anti-hypoglycemia action of glucagon (e.g., liver failure or cirrhosis). Other liver disease (i.e., active hepatitis, steatosis, active biliary disease, any tumor of the liver, hemochromatosis, glycogen storage disease) may exclude the patient if it causes significant compromise to liver function or may do so in an unpredictable fashion.
  10. Any history or presence of clinically relevant cardiovascular, pulmonary, respiratory, gastrointestinal, renal, metabolic, endocrinological (with the exception of conditions associated with diabetes mellitus), haematological, dermatological, neurological, osteomuscular, articular, psychiatric, systemic, ocular, gynaecologic (if female), or infectious disease, or signs of acute illness as judged by the Investigator.
  11. Clinically significant abnormal haematology, biochemistry or urinalysis screening tests, as judged by the Investigator. In particular, elevated liver enzymes (AST or ALT > 2 times the upper limit of normal, or bilirubin >1.5 the upper limit of normal) or impaired renal function (elevated serum creatinine values above the upper limit of normal).
  12. Hypertension with systolic blood pressure >140 mmHg or diastolic blood pressure >90 mmHg (excluding white-coat hypertension; therefore, if a repeated measurement shows values within the range, the patient can be included in the trial); a heart rate at rest outside the range of 50-90 beats per minute.
  13. Clinically significant abnormal standard 12-lead electrocardiogram (ECG) after 5 minutes resting in supine position at screening, as judged by the Investigator.
  14. Proliferative retinopathy or maculopathy and/or severe neuropathy, in particular autonomic neuropathy, as judged by the Investigator.
  15. Inadequate venous access as determined by trial nurse or physician at time of screening
  16. Any factors that, in the judgment of the Principal Investigator, would interfere with trial endpoints or the safe completion of the trial procedures.
  17. Severe hypoglycaemic events within one year prior to screening, as judged by the Investigator.
  18. Increased risk of thrombosis, e.g. patients with a history of deep leg vein thrombosis or family history of deep leg vein thrombosis, as judged by the Investigator.
  19. Significant history of alcoholism or drug abuse as judged by the Investigator or consuming more than 24 g alcohol per day for men, or more than 12 g alcohol per day for women.
  20. A positive result in the alcohol and/or urine drug screen at the screening visit.
  21. Habitual smoking, i.e., daily smoking or more than 7 cigarettes/week within the last 3 months prior to screening. Patients have to accept refraining from smoking while at the clinical site.
  22. History of cystic fibrosis, pancreatitis, pancreatic tumor, or any other pancreatic disease besides T1DM
  23. History of pheochromocytoma.
  24. History of adrenal disease or tumor.
  25. Positive to the screening test for Hepatitis Bs antigen or Hepatitis C antibodies and/or a positive result to the test for HIV-1/2 antibodies or HIV-1 antigen.
  26. The use of any non-prescribed systemic or topical medication, except routine vitamins and occasional use of acetylsalicylic acid and paracetamol within 2 weeks prior to randomization (and if female with the exception of hormonal contraception or menopausal hormone replacement therapy).
  27. Donation of blood or plasma in the past month, or in excess of 500 mL within 12 weeks prior to screening.
  28. Male who is sexually active and not surgically sterilized who or whose partner(s) is not using highly effective contraceptive methods (highly effective contraceptive measures include surgical sterilisation, hormonal intrauterine devices [coil], oral hormonal contraceptives, each in combination with spermicide-coated condoms), or who is not willing to refrain from sexual intercourse from the first dosing until the end of the trial (Visit 6).
  29. Females of childbearing potential who are pregnant (positive urine human chorionic gonadotropin [HCG]), breast-feeding or intend to become pregnant or are not using highly effective contraceptive methods (highly effective contraceptive methods are considered those with a failure rate less than 1% undesired pregnancies per year including surgical sterilisation, hormonal intrauterine devices (coil), oral hormonal contraceptives, sexual abstinence or a surgically sterilised partner). Females who are postmenopausal can participate in the study without using adequate contraceptive methods. Postmenopausal is defined as women aged < 52 years and being amenorrheic for more than one year with serum FSH level > 40 IU/L or aged >= 52 years and being amenorrheic for less than one year and with serum FSH level > 40 IU/L or aged >= 52 years being amenorrheic for more than one year.

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Sites / Locations

  • Profil Institut für Stoffwechselforschung GmbH

Arms of the Study

Arm 1

Arm 2

Arm Type

Experimental

Active Comparator

Arm Label

ZP4207(dasiglucagon)

Glucagon (Native glucagon)

Arm Description

Intervention: ZP4207(dasiglucagon) glucagon analogue (4 mg/mL) planned doses: 0.03, 0.08, 0.2 and 0.6 mg at euglycemic and hypoglycemic conditions.

Intervention: Glucagon (Native glucagon) 1 mg/mL as active comparator planned doses: 0.03, 0.08 and 0.2 mg at euglycemic conditions.

Outcomes

Primary Outcome Measures

PK endpoint for ZP4207(dasiglucagon) and baseline adjusted glucagon: AUC 0-240 min
Area under the curve from 0-240 min
PK endpoint for ZP4207(dasiglucagon) and baseline adjusted glucagon: Cmax
max. concentration
PK endpoint for ZP4207(dasiglucagon) and baseline adjusted glucagon: tmax
Time to peak plasma concentration
PD endpoint: Plasma glucose profiles above baseline: AUE 0-240 min
Area under the effect curve from 0-240 min
PD endpoint: Plasma glucose profiles above baseline: CEmax
Max concentration effect
PD endpoint: Plasma glucose profiles above baseline: tmax
Time to peak plasma glucose concentration

Secondary Outcome Measures

PK endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: MRT
Mean residence time
PK endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: Vz/f,
Volume of distribution
PK endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: λz
Terminal elimination rate constant
PK endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: t½,
Terminal plasma elimination half-life
PK endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: CL/f
Total body clearance
PK endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: AUC 0-30min
Area under the curve from 0-30 min
PK endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: AUC 0-inf
Area under the curve from 0-inf
Insulin concentrations before and after dosing with ZP4207(dasiglucagon) or glucagon:
Insulin concentrations
PD endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: AUE 0-30min
Area under the effect curve from 0-30 min
PD endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: CE 30min
Concentration effect at 30 min
PD endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: t50%CE, early
Time to half concentration effect
PD endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: t10%CE, late
Time to 90% decrease from CEmax
PD endpoints: Percentage of patients achieving a plasma glucose increase of ≥20 mg/dL within 30 minutes after treatment
PD endpoints: Time to plasma glucose increase of ≥20 mg/dL
PD endpoints: Percentage of patients achieving a plasma glucose concentration ≥70 mg/dL within 30 minutes after treatment (insulin-induced hypoglycemia)
PD endpoints: Time to plasma glucose concentration of ≥70 mg/dL (insulin-induced hypoglycemia)
Safety endpoints: Number of participants with adverse events
Includes events from the first trial related activity after the patient has signed the informed consent until Follow up visit.
Safety endpoints: Local tolerability of injection site
Findings in local tolerability by means of the following assessments: spontaneous pain pain on palpation itching redness oedema induration/infiltration other these assessments will be reported on a scale of 0 (none), 1 (mild), 2 (moderate) and 3 (severe)
Safety endpoints: Laboratory safety parameters
Haematology, biochemistry and urinalysis: Changes or findings from baseline (normal ranges) in clinical safety laboratory parameters during the study duration (from Screening, at treatment visits and at Follow up visit).
Safety endpoints: Physical examination
Physical examination: Changes or findings from baseline (normal ranges) in physical examination during the study duration (at Screening and Follow up visit). An examination of the following body systems will be performed: Head, ears, eyes, nose, throat (HEENT), incl thyroid gland Heart, lung, chest Abdomen Skin and mucosae Musculoskeletal system Nervous system Lymph node Other findings
Safety endpoints: Vital signs
Diastolic and systolic blood pressure (mmHg) are measured after at least 5 min rest in a supine position. At the screening visit blood pressure is measured in both arms. The blood pressure from the arm with the higher systolic value is transcribed into the CRF and this arm is used for all subsequent measurements of the patient's blood pressure in this trial. Pulse (beats per min) measured after at least 5 min rest in a supine position. Body temperature, tympanic (in Celsius). Respiratory frequency (RF/min). Changes or findings from baseline (normal ranges) in vital signs during the study duration (at Screening, at each treatment visit and at Follow up).
Safety endpoints: ECGs
A standard 12-lead electrocardiogram (ECG) will be performed. ECG parameters (Heart rate, PQ, QRS, QT, QTcB) and any abnormality will be recorded and described in the CRF including the Investigator's assessment of clinical significance ('abnormal, not clinically significant' or 'abnormal, clinically significant'). Clinically significant findings at the screening visit should be recorded as concomitant illness. At subsequent visits, any clinically significant deterioration of a pre-existing condition as well as any new clinically significant findings will be recorded as AEs. Changes or findings from baseline (normal ranges) (Screening visit and at Follow up) in ECGs during the study duration.
Safety endpoints: Antidrug antibodies incidences
Antidrug antibodies analyses will be performed. Changes or findings from baseline (normal ranges) in Antidrug antibodies incidences during the study duration (before first dosing, at last treatment visit and at Follow up).

Full Information

First Posted
September 8, 2016
Last Updated
April 20, 2017
Sponsor
Zealand Pharma
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1. Study Identification

Unique Protocol Identification Number
NCT02916251
Brief Title
ZP4207(Dasiglucagon) Administered to T1D Patients to Assess the PK and PD Compared to Marketed Glucagon
Official Title
Randomised, Sequential, Cross-over Trial Assessing PK and PD Responses After Micro-doses of ZP4207 Administered s.c. to Patients With T1D Under eu- and Hypoglycemic Conditions and With Reference to Freshly Reconstituted Lyophilized Glucagon
Study Type
Interventional

2. Study Status

Record Verification Date
April 2017
Overall Recruitment Status
Completed
Study Start Date
December 1, 2016 (Actual)
Primary Completion Date
April 5, 2017 (Actual)
Study Completion Date
April 5, 2017 (Actual)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Sponsor
Name of the Sponsor
Zealand Pharma

4. Oversight

Data Monitoring Committee
No

5. Study Description

Brief Summary
The trial is a single-centre, randomised, sequential, cross-over trial assessing pharmacokinetic and pharmacodynamic responses after micro-doses of ZP4207 (dasiglucagon*) administered subcutaneously to patients with type 1 diabetes mellitus under euglycaemic and hypoglycaemic conditions and compared to marketed glucagon. *dasiglucagon is the proposed International Nonproprietary Name (pINN) for ZP4207
Detailed Description
Seventeen (17) adult patients with T1DM treated with continuous subcutaneous insulin infusion (insulin pumps, CSII) will be randomized and take part at four dosing visits. The dosing visits are separated by 3-7 days. For the three lowest dose levels (0.03 mg, 0.08 mg, and 0.2 mg) the patients will receive two doses of ZP4207(dasiglucagon) (the first at euglycaemic and the second at hypoglycaemic conditions) and one dose of glucagon at euglycaemic conditions at visit 2-4. The first two dose administrations (Day 1, visit 2-4) will be separated by at least five hours. The third dose, which is ZP4207(dasiglucagon) during hypoglycemia, will for all dosing visits be administered the next morning after a standardized carbohydrate-rich meal in the evening before. The patients will stay at the clinical site over night between Day 1 and Day 2. The dose of 0.6 mg will only be administered for ZP4207(dasiglucagon). The order of the micro-dose levels as well as the order of the treatment, ZP4207(dasiglucagon) vs. glucagon, will be randomized. For all patients the 0.6 mg dose of ZP4207(dasiglucagon) will be administered at visit 5. For each dose level there will be 2 sets of PK/PD profiles for ZP4207(dasiglucagon), one initiated during euglycaemia and another during hypoglycaemia. Each patient enrolled will therefore provide a total of 11 PK/PD profiles covering four different dose levels; 8 profiles from ZP4207(dasiglucagon) and 3 profiles from glucagon

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Diabetes Mellitus Type 1

7. Study Design

Primary Purpose
Treatment
Study Phase
Phase 2
Interventional Study Model
Crossover Assignment
Masking
ParticipantInvestigator
Allocation
Randomized
Enrollment
38 (Actual)

8. Arms, Groups, and Interventions

Arm Title
ZP4207(dasiglucagon)
Arm Type
Experimental
Arm Description
Intervention: ZP4207(dasiglucagon) glucagon analogue (4 mg/mL) planned doses: 0.03, 0.08, 0.2 and 0.6 mg at euglycemic and hypoglycemic conditions.
Arm Title
Glucagon (Native glucagon)
Arm Type
Active Comparator
Arm Description
Intervention: Glucagon (Native glucagon) 1 mg/mL as active comparator planned doses: 0.03, 0.08 and 0.2 mg at euglycemic conditions.
Intervention Type
Drug
Intervention Name(s)
ZP4207(dasiglucagon) glucagon analogue
Other Intervention Name(s)
dasiglucagon
Intervention Description
Cross-over design with single s.c. administration in euglycemic and hypoglycemic T1D
Intervention Type
Drug
Intervention Name(s)
Glucagon (Native glucagon)
Other Intervention Name(s)
Lilly Glucagon
Intervention Description
Cross-over design with single s.c. administration in euglycemic T1D
Primary Outcome Measure Information:
Title
PK endpoint for ZP4207(dasiglucagon) and baseline adjusted glucagon: AUC 0-240 min
Description
Area under the curve from 0-240 min
Time Frame
AUC 0-240 min during all treatment periods (V2-V5)
Title
PK endpoint for ZP4207(dasiglucagon) and baseline adjusted glucagon: Cmax
Description
max. concentration
Time Frame
Pre-dose, 5, 15, 30, 60, 90, 150 and 240 minutes post dosing. Peak of plasma concentration during all treatment periods (V2-V 5)
Title
PK endpoint for ZP4207(dasiglucagon) and baseline adjusted glucagon: tmax
Description
Time to peak plasma concentration
Time Frame
Pre-dose, 5, 15, 30, 60, 90, 150 and 240 minutes post dosing. Time to peak plasma concentration during all treatment periods (V2-V5)
Title
PD endpoint: Plasma glucose profiles above baseline: AUE 0-240 min
Description
Area under the effect curve from 0-240 min
Time Frame
Pre-dose, 10, 30, 50, 70, 90, 150, 240 minutes post dosing. AUE 0-240 min during all treatment periods (V2-V5)
Title
PD endpoint: Plasma glucose profiles above baseline: CEmax
Description
Max concentration effect
Time Frame
Pre-dose, 10, 30, 50, 70, 90, 150, 240 minutes post dosing. Peak of plasma glucose concentration during all treatment periods (V2-V5)
Title
PD endpoint: Plasma glucose profiles above baseline: tmax
Description
Time to peak plasma glucose concentration
Time Frame
Pre-dose, 10, 30, 50, 70, 90, 150, 240 minutes post dosing Time to plasma glucose concentration during all treatment periods (V2-V5)
Secondary Outcome Measure Information:
Title
PK endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: MRT
Description
Mean residence time
Time Frame
Pre-dose, 5, 15, 30, 60, 90, 150 and 240 minutes post dosing. Mean residence time for ZP4207(dasiglucagon) and baseline adjusted glucagon during all treatment periods (V2-V5)
Title
PK endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: Vz/f,
Description
Volume of distribution
Time Frame
Pre-dose, 5, 15, 30, 60, 90, 150 and 240 minutes post dosing. Volume of distribution of plasma ZP4207(dasiglucagon) or glucagon during all treatment periods (V2-V5)
Title
PK endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: λz
Description
Terminal elimination rate constant
Time Frame
Pre-dose, 5, 15, 30, 60, 90, 150 and 240 minutes post dosing. Terminal elimination rate constant of ZP4207(dasiglucagon) and baseline adjusted glucagon during all treatment periods (V2-V5)
Title
PK endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: t½,
Description
Terminal plasma elimination half-life
Time Frame
Pre-dose, 5, 15, 30, 60, 90, 150 and 240 minutes post dosing. Terminal plasma elimination half-life of ZP4207(dasiglucagon) or glucagon during all treatment periods (V2-V5)
Title
PK endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: CL/f
Description
Total body clearance
Time Frame
Pre-dose, 5, 15, 30, 60, 90, 150 and 240 minutes post dosing. Total body clearance of plasma ZP4207(dasiglucagon) or glucagon during all treatment periods (V2-V5)
Title
PK endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: AUC 0-30min
Description
Area under the curve from 0-30 min
Time Frame
AUC 0-30 min during all treatment periods (V2-V 5)
Title
PK endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: AUC 0-inf
Description
Area under the curve from 0-inf
Time Frame
Pre-dose, 5, 15, 30, 60, 90, 150 and 240 minutes post dosing. AUC 0-inf during all treatment periods (V2-V 5)
Title
Insulin concentrations before and after dosing with ZP4207(dasiglucagon) or glucagon:
Description
Insulin concentrations
Time Frame
Pre-dose, 5, 15, 30, 60, 90, 150 and 240 minutes post dosing. Insulin concentrations during all treatment periods (V2-V 5)
Title
PD endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: AUE 0-30min
Description
Area under the effect curve from 0-30 min
Time Frame
AUE 0-240 min during all treatment periods (V2-V5)
Title
PD endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: CE 30min
Description
Concentration effect at 30 min
Time Frame
Concentration effect at 30 min during all treatment periods (V2-V5)
Title
PD endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: t50%CE, early
Description
Time to half concentration effect
Time Frame
Pre-dose, 10, 30, 50, 70, 90, 150, 240 minutes post dosing. Time to half concentration effect (t50%CE, early) during all treatment periods (V2-V5)
Title
PD endpoints for ZP4207(dasiglucagon) and baseline adjusted glucagon: t10%CE, late
Description
Time to 90% decrease from CEmax
Time Frame
Pre-dose, 10, 30, 50, 70, 90, 150, 240 minutes post dosing. Time to 90% decrease from peak concentration effect during all treatment periods (V2-V5)
Title
PD endpoints: Percentage of patients achieving a plasma glucose increase of ≥20 mg/dL within 30 minutes after treatment
Time Frame
During all treatment periods (V2-V5) within 30 min after dosing
Title
PD endpoints: Time to plasma glucose increase of ≥20 mg/dL
Time Frame
Pre-dose, 10, 30, 50, 70, 90, 150, 240 minutes post dosing. During all treatment periods (V2-V5) - time plasma glucose increase of ≥20 mg/dL after dosing
Title
PD endpoints: Percentage of patients achieving a plasma glucose concentration ≥70 mg/dL within 30 minutes after treatment (insulin-induced hypoglycemia)
Time Frame
During all treatment periods (V2-V5) within 30 min after dosing (insulin-induced hypoglycemia)
Title
PD endpoints: Time to plasma glucose concentration of ≥70 mg/dL (insulin-induced hypoglycemia)
Time Frame
Pre-dose, 10, 30, 50, 70, 90, 150, 240 minutes post dosing. During all treatment periods (V2-V5) - time plasma glucose increase of ≥70 mg/dL after dosing (insulin-induced hypoglycemia)
Title
Safety endpoints: Number of participants with adverse events
Description
Includes events from the first trial related activity after the patient has signed the informed consent until Follow up visit.
Time Frame
Through study completion. The total trial duration for a patient will be about 5.5 to 12 weeks.
Title
Safety endpoints: Local tolerability of injection site
Description
Findings in local tolerability by means of the following assessments: spontaneous pain pain on palpation itching redness oedema induration/infiltration other these assessments will be reported on a scale of 0 (none), 1 (mild), 2 (moderate) and 3 (severe)
Time Frame
Local tolerability assessed pre-dose (within 30 min) and at 0.5, 2, and 4 hours post-dose (each treatment visit and at Follow up visit).
Title
Safety endpoints: Laboratory safety parameters
Description
Haematology, biochemistry and urinalysis: Changes or findings from baseline (normal ranges) in clinical safety laboratory parameters during the study duration (from Screening, at treatment visits and at Follow up visit).
Time Frame
Through study completion. The total trial duration for a patient will be about 5.5 to 12 weeks.
Title
Safety endpoints: Physical examination
Description
Physical examination: Changes or findings from baseline (normal ranges) in physical examination during the study duration (at Screening and Follow up visit). An examination of the following body systems will be performed: Head, ears, eyes, nose, throat (HEENT), incl thyroid gland Heart, lung, chest Abdomen Skin and mucosae Musculoskeletal system Nervous system Lymph node Other findings
Time Frame
Through study completion. The total trial duration for a patient will be about 5.5 to 12 weeks.
Title
Safety endpoints: Vital signs
Description
Diastolic and systolic blood pressure (mmHg) are measured after at least 5 min rest in a supine position. At the screening visit blood pressure is measured in both arms. The blood pressure from the arm with the higher systolic value is transcribed into the CRF and this arm is used for all subsequent measurements of the patient's blood pressure in this trial. Pulse (beats per min) measured after at least 5 min rest in a supine position. Body temperature, tympanic (in Celsius). Respiratory frequency (RF/min). Changes or findings from baseline (normal ranges) in vital signs during the study duration (at Screening, at each treatment visit and at Follow up).
Time Frame
Through study completion. The total trial duration for a patient will be about 5.5 to 12 weeks.
Title
Safety endpoints: ECGs
Description
A standard 12-lead electrocardiogram (ECG) will be performed. ECG parameters (Heart rate, PQ, QRS, QT, QTcB) and any abnormality will be recorded and described in the CRF including the Investigator's assessment of clinical significance ('abnormal, not clinically significant' or 'abnormal, clinically significant'). Clinically significant findings at the screening visit should be recorded as concomitant illness. At subsequent visits, any clinically significant deterioration of a pre-existing condition as well as any new clinically significant findings will be recorded as AEs. Changes or findings from baseline (normal ranges) (Screening visit and at Follow up) in ECGs during the study duration.
Time Frame
Through study completion. The total trial duration for a patient will be about 5.5 to 12 weeks.
Title
Safety endpoints: Antidrug antibodies incidences
Description
Antidrug antibodies analyses will be performed. Changes or findings from baseline (normal ranges) in Antidrug antibodies incidences during the study duration (before first dosing, at last treatment visit and at Follow up).
Time Frame
Through study completion. The total trial duration for a patient will be about 5.5 to 12 weeks.

10. Eligibility

Sex
All
Minimum Age & Unit of Time
18 Years
Maximum Age & Unit of Time
64 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria: To be included in the trial, patients have to fulfil all of the following criteria: Signed and dated informed consent obtained before any trial-related activities. (Trial-related activities are any procedures that would not have been performed during normal management of the patient). Male and female patients with T1DM for at least 1 year, as defined by the American Diabetes Association1. Age between 18 and 64 years, both inclusive. HbA1c < 8.5%. C-peptide negative defined as below the lower limit of quantification. Stable insulin regimen via an insulin infusion pump for at least 1 month prior to screening. Weight between 60 kg and 90 kg, both inclusive. Patients in good health according to age (medical history, physical examination, vital signs, 12-lead ECGs, lab assessments), as judged by the Investigator.- Exclusion Criteria: Patients meeting any of the following criteria during screening evaluations will be excluded from trial participation: Unable to provide informed consent (e.g., impaired cognition or judgement). Patients with mental incapacity or language barriers which preclude adequate understanding or cooperation, who are unwilling to participate in the trial, or who in the opinion of the Investigator should not participate in the trial. Receipt of any medicinal product in clinical development within 3 months prior screening. Previous exposure to ZP4207(dasiglucagon) or previously randomized to this trial. Known or suspected allergy to trial product(s) or related products. History of adverse reaction to glucagon (including allergy) besides nausea and vomiting. History of multiple and/or severe allergies to drugs or foods or a history of severe anaphylactic reaction. New onset clinically significant illness within 4 weeks prior to screening, as judged by the Investigator. History of liver disease that is expected to interfere with the anti-hypoglycemia action of glucagon (e.g., liver failure or cirrhosis). Other liver disease (i.e., active hepatitis, steatosis, active biliary disease, any tumor of the liver, hemochromatosis, glycogen storage disease) may exclude the patient if it causes significant compromise to liver function or may do so in an unpredictable fashion. Any history or presence of clinically relevant cardiovascular, pulmonary, respiratory, gastrointestinal, renal, metabolic, endocrinological (with the exception of conditions associated with diabetes mellitus), haematological, dermatological, neurological, osteomuscular, articular, psychiatric, systemic, ocular, gynaecologic (if female), or infectious disease, or signs of acute illness as judged by the Investigator. Clinically significant abnormal haematology, biochemistry or urinalysis screening tests, as judged by the Investigator. In particular, elevated liver enzymes (AST or ALT > 2 times the upper limit of normal, or bilirubin >1.5 the upper limit of normal) or impaired renal function (elevated serum creatinine values above the upper limit of normal). Hypertension with systolic blood pressure >140 mmHg or diastolic blood pressure >90 mmHg (excluding white-coat hypertension; therefore, if a repeated measurement shows values within the range, the patient can be included in the trial); a heart rate at rest outside the range of 50-90 beats per minute. Clinically significant abnormal standard 12-lead electrocardiogram (ECG) after 5 minutes resting in supine position at screening, as judged by the Investigator. Proliferative retinopathy or maculopathy and/or severe neuropathy, in particular autonomic neuropathy, as judged by the Investigator. Inadequate venous access as determined by trial nurse or physician at time of screening Any factors that, in the judgment of the Principal Investigator, would interfere with trial endpoints or the safe completion of the trial procedures. Severe hypoglycaemic events within one year prior to screening, as judged by the Investigator. Increased risk of thrombosis, e.g. patients with a history of deep leg vein thrombosis or family history of deep leg vein thrombosis, as judged by the Investigator. Significant history of alcoholism or drug abuse as judged by the Investigator or consuming more than 24 g alcohol per day for men, or more than 12 g alcohol per day for women. A positive result in the alcohol and/or urine drug screen at the screening visit. Habitual smoking, i.e., daily smoking or more than 7 cigarettes/week within the last 3 months prior to screening. Patients have to accept refraining from smoking while at the clinical site. History of cystic fibrosis, pancreatitis, pancreatic tumor, or any other pancreatic disease besides T1DM History of pheochromocytoma. History of adrenal disease or tumor. Positive to the screening test for Hepatitis Bs antigen or Hepatitis C antibodies and/or a positive result to the test for HIV-1/2 antibodies or HIV-1 antigen. The use of any non-prescribed systemic or topical medication, except routine vitamins and occasional use of acetylsalicylic acid and paracetamol within 2 weeks prior to randomization (and if female with the exception of hormonal contraception or menopausal hormone replacement therapy). Donation of blood or plasma in the past month, or in excess of 500 mL within 12 weeks prior to screening. Male who is sexually active and not surgically sterilized who or whose partner(s) is not using highly effective contraceptive methods (highly effective contraceptive measures include surgical sterilisation, hormonal intrauterine devices [coil], oral hormonal contraceptives, each in combination with spermicide-coated condoms), or who is not willing to refrain from sexual intercourse from the first dosing until the end of the trial (Visit 6). Females of childbearing potential who are pregnant (positive urine human chorionic gonadotropin [HCG]), breast-feeding or intend to become pregnant or are not using highly effective contraceptive methods (highly effective contraceptive methods are considered those with a failure rate less than 1% undesired pregnancies per year including surgical sterilisation, hormonal intrauterine devices (coil), oral hormonal contraceptives, sexual abstinence or a surgically sterilised partner). Females who are postmenopausal can participate in the study without using adequate contraceptive methods. Postmenopausal is defined as women aged < 52 years and being amenorrheic for more than one year with serum FSH level > 40 IU/L or aged >= 52 years and being amenorrheic for less than one year and with serum FSH level > 40 IU/L or aged >= 52 years being amenorrheic for more than one year. -
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Hövelmann Ulrike, MD
Organizational Affiliation
Profil Neuss GmbH Neuss, Germany, 41460
Official's Role
Principal Investigator
Facility Information:
Facility Name
Profil Institut für Stoffwechselforschung GmbH
City
Neuss
State/Province
North Rhine-Westphalia
ZIP/Postal Code
41460
Country
Germany

12. IPD Sharing Statement

Plan to Share IPD
Undecided

Learn more about this trial

ZP4207(Dasiglucagon) Administered to T1D Patients to Assess the PK and PD Compared to Marketed Glucagon

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