A Clinical Study to Evaluate the Safety, Tolerability, PK, PD, and Efficacy of KBP-089 in Patients With T2DM

Sponsor

KeyBioscience AG (Industry)

Overall Status

Terminated

CT.gov ID

NCT03907202

Collaborator

Eli Lilly and Company (Industry), Nordic Bioscience A/S (Industry), Profil Institut für Stoffwechselforschung GmbH (Industry)

Enrollment

Location

Arms

19.5

Actual Duration (Months)

1.3

Patients Per Site Per Month

Study Details

Study Description

Brief Summary

KeyBioscience is developing KBP-089, a dual activator of both the amylin and calcitonin receptors, for the treatment of type II diabetes mellitus, using a subcutaneous injectable mode of administration.

This is a double-blind, placebo-controlled, randomised, multiple-ascending dose phase I trial to evaluate the safety, tolerability, pharmacokinetics, pharmacodynamics, and efficacy of KBP-089 in patients with type 2 diabetes, who are on stable therapy with metformin.

Subjects will receive daily subcutaneous injections in the abdomen over a period of 28 days. The planned maximum doses of KBP-089 to be investigated in the trial are 20 µg in cohort 1, 60 µg in cohort 2, and 150 µg in cohort 3. For cohort 1, the dose is planned to be escalated every 7 ±1 days, and for cohort 2 and cohort 3, every 3 days. Doses may be modified according to individual tolerability, but the dose regimen will not exceed 28 days.

The IMP is administered by daily subcutaneous injections taken in the morning before breakfast.

The trial is performed in Germany and at least 36 patients will be enrolled in the trial. The trial will be randomised 1:1:1 between maximum doses of KBP-089 of 20 µg, 60 µg, 150 µg and placebo. Within each of the three cohorts, 12 patients will be randomised 3:1 to KBP-089 and placebo.

Condition or Disease	Intervention/Treatment	Phase
Type II Diabetes Mellitus	Drug: Daily injection of KBP/placebo for up to 28 days	Phase 1

Study Design

Study Type:

Interventional

Actual Enrollment :

25 participants

Allocation:

Randomized

Intervention Model:

Parallel Assignment

Intervention Model Description:

Randomised, patient-blind, investigator-blind, placebo-controlled, multiple ascending dose study. There will be 3 cohorts in which patients are randomised to receive either treatment with KBP-089 or placebo.Randomised, patient-blind, investigator-blind, placebo-controlled, multiple ascending dose study. There will be 3 cohorts in which patients are randomised to receive either treatment with KBP-089 or placebo.

Masking:

Triple (Participant, Care Provider, Investigator)

Masking Description:

To preserve the blinding of the study for KBP-089 and placebo, all study site personnel, except pharmacy staff who prepare and dispense study medication, and the Sponsor's medical monitor who interacts with site personnel will be blinded to treatment allocation. Blinding of KBP-089 and placebo will be maintained throughout the conduct of the trial until after the completion of the trial and final data review. Treatment assignment will be kept strictly confidential and accessible only to authorised persons until after the time of unblinding. Codes with treatment assignment will, however, be readily available to the blinded personnel in case of an emergency.

Primary Purpose:

Treatment

Official Title:

A Double-blind, Placebo-controlled, Randomised, Multiple-ascending Dose Study to Evaluate the Safety, Tolerability, Pharmacokinetics, Pharmacodynamics, and Efficacy of KBP-089 in Patients With Type II Diabetes

Actual Study Start Date :

Apr 17, 2018

Actual Primary Completion Date :

Dec 3, 2019

Actual Study Completion Date :

Dec 3, 2019

Arms and Interventions

Arm	Intervention/Treatment
Active Comparator: KBP-089 Three cohorts: Cohort 1: starting dose 5 µg, maximum dose 20 µg, uptitration step 7 days, dose increment 5 µg Cohort 2: starting dose 7.5 µg, maximum dose 60 µg, uptitration step 3 days, dose increment 7.5 µg Cohort 3: starting dose 5 µg, maximum dose 120 µg, uptitration step 3 days, dose increment 5, 10, 15 and 20 µg	Drug: Daily injection of KBP/placebo for up to 28 days Daily sub-cutaneous injection of KBP-089/Placebo into a lifted skin fold of the abdominal wall.The injection will be administered in the morning before breakfast.
Placebo Comparator: Placebo For all the cohorts, sentinel dosing for the first two patients will be performed 1:1 in a blinded manner.	Drug: Daily injection of KBP/placebo for up to 28 days Daily sub-cutaneous injection of KBP-089/Placebo into a lifted skin fold of the abdominal wall.The injection will be administered in the morning before breakfast.

Arm

Intervention/Treatment

Active Comparator: KBP-089

Three cohorts: Cohort 1: starting dose 5 µg, maximum dose 20 µg, uptitration step 7 days, dose increment 5 µg Cohort 2: starting dose 7.5 µg, maximum dose 60 µg, uptitration step 3 days, dose increment 7.5 µg Cohort 3: starting dose 5 µg, maximum dose 120 µg, uptitration step 3 days, dose increment 5, 10, 15 and 20 µg

Drug: Daily injection of KBP/placebo for up to 28 days

Daily sub-cutaneous injection of KBP-089/Placebo into a lifted skin fold of the abdominal wall.The injection will be administered in the morning before breakfast.

Placebo Comparator: Placebo

For all the cohorts, sentinel dosing for the first two patients will be performed 1:1 in a blinded manner.

Drug: Daily injection of KBP/placebo for up to 28 days

Daily sub-cutaneous injection of KBP-089/Placebo into a lifted skin fold of the abdominal wall.The injection will be administered in the morning before breakfast.

Outcome Measures

Primary Outcome Measures

Treatment Emergent Adverse Events (TEAEs). [Day -1 to day 28]
All TEAEs will be coded using MedDRA and summarized by treatment and dose.
Vital sign - Blood Pressure. [Day -1 to day 28]
Diastolic and systolic blood pressure (mmHg) are measured after at least 5 min rest in a supine position. Vital signs will be summarised by descriptive statistics by treatment, dose and timepoint.
Vital sign - Pulse (beats per min). [Day -1 to day 28]
measured after at least 5 min rest in a supine position. Vital signs will be summarised by descriptive statistics by treatment, dose and timepoint.
Vital sign - Body Temperature. [Day -1 to day 28]
Body temperature, tympanic (in Celcius). Vital signs will be summarised by descriptive statistics by treatment, dose and timepoint.
Vital sign - Respiratory frequency. [Day -1 to day 28]
Respiratory frequency measured as breaths per min. Vital signs will be summarised by descriptive statistics by treatment, dose and timepoint.
Electrocardiogram (ECG) - PQ interval. [Day -1 to day 28]
PQ interval (in msec) 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').
Electrocardiogram (ECG) - QRS complex. [Day -1 to day 28]
QRS interval (in msec) 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').
Electrocardiogram (ECG) - QT interval. [Day -1 to day 28]
QT interval (in msec) 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').
Safety laboratory parameter - lipids. [Day -1 to day 28]
Standard Lipid assessments will be summarized by treatment (including dose) using descriptive statistics (number, mean, standard deviation, minimum, median and maximum). (Lipid parameters measured: Total cholesterol, High-density lipoprotein (HDL) cholesterol, Low-density lipoprotein (LDL) cholesterol, Triglycerides).
Safety laboratory parameter - haematology. [Day -1 to day 28]
Standard Biochemistry assessments will be summarized by treatment (including dose) using descriptive statistics (number, mean, standard deviation, minimum, median and maximum). (Haematology parameters measured: Haematocrit, Haemoglobin, Erythrocytes, Mean corpuscular volume (MCV), Mean corpuscular haemoglobin (MCH), Mean corpuscular haemoglobin concentration (MCHC), Thrombocytes (platelets), Leucocytes, Neutrophile granulocytes (total count and relative), Lymphocytes (total count and relative), Monocytes (total count and relative), Eosinophile granulocytes (total count and relative), Basophile granulocytes (total count and relative))
Safety laboratory parameter - coagulation. [Day -1 to day 28]
Standard coagulation assessments will be summarized by treatment (including dose) using descriptive statistics (number, mean, standard deviation, minimum, median and maximum). (coagulation parameters measured: International normalised ratio (INR), Activated partial thromboplastin time (APTT)
Safety laboratory parameter - urinalysis. [Day -1 to day 28]
Standard Biochemistry assessments will be summarized by treatment (including dose) using descriptive statistics (number, mean, standard deviation, minimum, median and maximum). (Urinalysis parameters measured: Protein, Glucose, Erythrocytes, Leucocytes, pH, Ketones)

Secondary Outcome Measures

Pharmacokinetic Evaluation - KBP-089 Area Under Curve. [Day -1 to day 28]
PK parameter (AUC 0-24) will be derived by non-compartmental analysis of the plasma concentration data for KBP-089
Pharmacokinetic Evaluation - KBP-089 Cmax. [Day -1 to day 28]
PK parameter (Cmax) will be derived by non-compartmental analysis of the plasma concentration data for KBP-089
Gastric emptying - Paracetamol Cmax. [Day -1 to day 28]
Gastric emptying is measured using paracetamol Cmax at baseline (Day -1), Day 1, and Day 28 for Cohorts 1 and 2 only
Gastric emptying - Paracetamol Tmax. [Day -1 to day 28]
Gastric emptying is measured using paracetamol Tmax at baseline (Day -1), Day 1, and Day 28 for Cohorts 1 and 2 only
Gastric emptying - Paracetamol Area Under Curve (AUC). [Day -1 to day 28]
Gastric emptying is measured using paracetamol AUC at baseline (Day -1), Day 1, and Day 28 for Cohorts 1 and 2 only
Fasting and postprandial glucose concentration. [Day -1 to day 28]
Fasting and postprandial glucose following OGTT at baseline (Days -1) and Day 28
Fasting and postprandial insulin concentration. [Day -1 to day 28]
Insulin following OGTT at baseline (Days -1) and Day 28
Fasting and postprandial C-peptide concentration. [Day -1 to day 28]
Fasting and postprandial C-peptide following OGTT at baseline (Days -1) and Day 28
Fasting and postprandial glucagon concentration. [Day -1 to day 28]
Fasting and postprandial glucagon following OGTT at baseline (Days -1) and Day 28
Body weight. [Day -1 to day 28]
Body weight at Day -1 (baseline) and Day 28 (in kg)
N-(1-deoxy)-fructosyl-haemoglobin (HbA1c). [Day -1 to day 28]
HbA1c at Day -1 (baseline) and Day 28 (in mmol/mol)
Fridericia's corrected QT interval (QTcF). [Day 1 to day 27]
Fridericia's corrected QT interval (QTcF) at Day 1 and Day 27 (in msec)

Eligibility Criteria

Criteria

Ages Eligible for Study:

18 Years to 64 Years

Sexes Eligible for Study:

All

Accepts Healthy Volunteers:

Inclusion 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 or female patient with T2DM.
Age between 18 and 64 years, both inclusive.
Body Mass Index (BMI) >= 25.0 kg/m^2.
HbA1c >= 7 and <=9.5%.
Stable therapy with metformin ± treatment with a second oral anti-diabetes drug (OAD) belonging to the class of dipeptidyl-peptidase 4 (DPP-4) inhibitors or sulfonylureas for at least 2 months prior to inclusion into the trial or not treated with glucose-lowering medications. Patients who are receiving stable treatment with a second OAD will be asked to discontinue the DPP-4 inhibitor or a sulfonylurea for at least 14 days prior the Initial Inpatient Dosing Visit.
Considered generally healthy (apart from T2DM) upon completion of medical history, physical examination, vital signs, ECG and analysis of laboratory safety variables, as judged by the Investigator.

Exclusion Criteria:

Known or suspected hypersensitivity or allergy to paracetamol or related products.
Prior treatment with a dual amylin and calcitonin receptor agonist (DACRA) or salmon calcitonin.
Receipt of any medicinal product in clinical development within 30 days or 5 half-lives of the medicinal product (whichever is longer) before randomisation in this trial.
History of multiple and/or severe allergies to drugs or foods or a history of severe anaphylactic reaction.
Any history or presence of clinically relevant cardiovascular, pulmonary, respiratory, gastrointestinal, hepatic, 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.
Medically unable or unwilling to discontinue current anti-diabetic therapy with DPP-4 inhibitor or sulfonylurea for at least 14 days prior to admission to the research facility (Day -2) and remain off medication until the follow-up visit. Patients taking metformin therapy at entry will continue their metformin at the usual individual dose throughout the trial.
Have had a significant change in weight, defined as a gain or loss of at least 5% body weight in the 3 months prior to screening.
A positive result in the alcohol and/or urine drug screen at the screening visit.
Positive to the screening test for Hepatitis Bs antigen (HBsAg) or Hepatitis C antibodies and/or a positive result to the test for human immunodeficiency virus (HIV)-1/2 antibodies or HIV-1 antigen.
Have had a blood transfusion or severe blood loss within the past 6 months or have known hemoglobinopathy, hemolytic anemia, sickle cell anemia, or have a hemoglobin value <11 g/dL (males) or <10 g/dL (females), or any other condition known to interfere with HbA1c methodology.
Blood donation or blood loss of more than 500 mL within the last 3 months or any blood donation within the last month prior to screening.
Females of childbearing potential.
Males with pregnant partners.