A Randomized Trial Investigating the Pharmacokinetics, Pharmacodynamics, and Safety of Subcutaneous Semaglutide Once-Weekly in Healthy Male Japanese and Caucasian Subjects

This was a clinical pharmacology, single-center, parallel-group, randomized, double-blind, placebo-controlled trial with two doses of semaglutide (0.5 mg and 1.0 mg) administered subcutaneously to healthy male Caucasian and Japanese subjects.

Healthy male subjects, age 20–55 years, with good glycemic control [HbA_1c 6.0% (42 mmol/mol) or less]; body mass index (BMI) in the range of 20–25 kg/m² with body weight of at least 54 kg; and with both parents either Japanese (for Japanese subjects) or Caucasian (for Caucasian subjects) were eligible for inclusion. Exclusion criteria included the presence or history of endocrine disorders and the existence of a first-degree relative with T2D, and were otherwise standard criteria for clinical pharmacology studies in healthy subjects.

Subjects were randomized within each ethnic group (Japanese and Caucasian) to receive either semaglutide 0.5 mg, semaglutide 1.0 mg, placebo 0.5 mg, or placebo 1.0 mg in an 8:8:3:3 ratio. Subjects were assigned to the lowest available randomization number on a subject-specific prepacked trial product (Clinical Supplies Coordination, Novo Nordisk A/S). Randomization to either active treatment or placebo was double-blinded, but assignment across doses was not blinded, because of differences in treatment volume.

Subjects received once-weekly subcutaneously administered semaglutide or volume-matched placebo for 13 weeks, with 5 weeks’ follow-up (Fig. 1). Doses were administered subcutaneously by the investigator at the clinic, using a prefilled PDS290 pen-injector. Semaglutide steady state was reached using the same dose-escalation regimen as in the phase 3 semaglutide program: subjects assigned to 0.5 mg treatment received 0.25 mg for 4 weeks, then 0.5 mg for 9 weeks. Those in the semaglutide 1.0 mg arm received 0.25 mg for 4 weeks, followed by 0.5 mg for 4 weeks and 1.0 mg for 5 weeks.

Prior to initiation, the trial protocol and any amendments, the consent form, and the subject information sheet were reviewed and approved according to local regulations by appropriate health authorities, and by an institutional review board (IRB). The IRB for this study was Medical Co. LTA Hakata Clinic IRB, Japan. The trial was conducted in accordance with the Declaration of Helsinki [34] and the International Conference on Harmonization Good Clinical Practice guidelines [35]. Informed consent was obtained before any trial-related activities were initiated.

The primary endpoint of the trial was area under the plasma semaglutide concentration–time curve during a dosing interval (0–168 h) at steady state (AUC_{0–168h,sema,SS}). Secondary pharmacokinetic endpoints for semaglutide at steady state after the last dose of semaglutide, 0.5 mg or 1.0 mg, included maximum plasma concentration (C_max,sema,SS), time to C_max,sema,SS (t_max,sema,SS), total apparent clearance (CL/F_sema,SS), terminal elimination half-life (t_1/2,sema,SS), and apparent volume of distribution (V_z/F_sema,SS). Secondary pharmacokinetic endpoints after the first dose of semaglutide (0.25 mg) were AUC_{0–168h,sema,SD}, C_max,sema,SD, and t_max,sema,SD. Other secondary pharmacokinetic endpoints included trough plasma concentration, 168 h after each dose of semaglutide 0.25 mg, 0.5 mg, and 1.0 mg (C_trough,sema). The dose-corrected accumulation ratio (R_acc,DC,sema) was calculated on the basis of AUC_{0–168h,sema,SD} after the first dose and AUC_{0–168h,sema,SS} after the last dose.

The pharmacodynamic endpoints were change from baseline to end of treatment—defined as 1 week after the last dose—in body weight, fasting plasma glucose (FPG), and other fasting glucose metabolism parameters (insulin, C-peptide, glucagon, and pro-insulin). Safety endpoints included incidence of adverse events, number of hypoglycemic episodes, incidence of anti-semaglutide antibodies at follow-up, and change in vital signs, electrocardiogram (ECG) readings, physical examination, and laboratory tests (hematology, biochemistry, calcitonin, and urinalysis).

Blood samples for pharmacokinetic assessment of semaglutide were taken before the first dose (0 h), for 1 week following a single 0.25 mg dose (6, 12, 18, 24, 30, 36, 42, 48, 60, 72, 84, 96, 120, 144, 168 h), then weekly prior to the next dose (trough values), and for 5 weeks following the final dose (0 h then 6, 12, 18, 24, 30, 36, 42, 48, 60, 72, 84, 96, 120, 144, 168, 336, 504, 672 and 840 h).

Bioanalysis of blood samples was performed at a specialized laboratory (Celerion Switzerland AG; Fehraltorf, Switzerland), which used a validated liquid chromatography–mass spectrometry (LC–MS/MS) assay [22]. This assay measured the total semaglutide concentration and had a lower limit of quantification (LLOQ) of 0.7 nmol/L [22].

Body weight was measured at baseline (before first dosing) and at 8 and 12 weeks after first dosing and 1 week following the final dose. Subjects were weighed without shoes and wearing light clothing. Blood samples for assessment of glucose metabolism parameters (glucose, insulin, C-peptide, glucagon, and pro-insulin) were collected during fasting state: at baseline (before first dosing), 1 week after the fourth dose of 0.5 mg, and 1 week following the final dose. These parameters were analyzed using standardized procedures at a central laboratory (ICON Laboratory Services Inc., Dublin, Ireland) while Celerion Switzerland AG was responsible for the analysis of semaglutide and anti-semaglutide antibodies. Local laboratory facilities (Medical Co. LTA, Sumida Hospital; LSI Medscience Cooporation, and SRL Inc. [all Tokyo, Japan]) provided additional analyses including biochemistry, hematology, urinalysis, and other laboratory assessments.

Safety assessments included monitoring of adverse events/serious adverse event and vital signs, ECG, physical examination, hypoglycemic episodes, and laboratory testing (including presence of anti-semaglutide antibodies or hypersensitivity). All adverse events were coded using the Medical Dictionary for Regulatory Activities (MedDRA), version 17.1. Hypoglycemia was monitored at the trial site during the in-house visits by glucose measurement. Hypoglycemia was classified as severe according to ADA guidelines [36] or blood glucose-confirmed symptomatic hypoglycemia by a plasma glucose value of less than 56 mg/dL (3.1 mmol/L) with symptoms indicative of hypoglycemia.

Sample size was not based on a formal statistical power calculation. A total of 44 subjects (22 Japanese and 22 Caucasian) were planned to be randomized to semaglutide 1.0 mg (n = 8), semaglutide 0.5 mg (n = 8), placebo 0.5 mg (n = 3), or placebo 1.0 mg (n = 3). In the analysis, the two placebo groups were pooled assuming no correlation between endpoints and placebo volume. A withdrawal rate of 15.0% was anticipated, which allowed for at least six steady-state pharmacokinetics profiles per dose and race group to be available for evaluation. All subjects who were randomized and exposed to at least one dose of trial product contributed to the pharmacokinetics, pharmacodynamics, and safety analyses.

The pharmacokinetic primary endpoint, AUC_{0–168h,sema,SS}, was derived from the concentration–time curve during a dosing interval (0–168 h) at steady state using the linear trapezoidal method on the observed concentrations at actual time points. The AUC_{0–168h,sema,SS} and other steady-state pharmacokinetic endpoints (C_max,sema,SS and R_acc,DC,sema) were analyzed separately by linear normal models based on log-transformed values with race (Japanese or Caucasian), dose group (0.5 mg or 1.0 mg), and race-by-dose group interaction as fixed factors. Estimated race differences (Japanese/Caucasian) by dose group and estimated dose-group differences (1.0 mg/0.5 mg) by race were transformed back to the original scale and presented as ratios with two-sided 95% confidence intervals (CI). A p value for the test of race-by-dose group interaction was also calculated. The race ratio for the pharmacokinetic endpoints (AUC_{0–168h,sema,SD} and C_max,sema,SD) after the first dose (0.25 mg) was estimated by linear normal models on log-transformed values.

For each pharmacodynamic assessment, treatment contrasts (semaglutide 0.5 mg and 1.0 mg versus placebo) at the end of treatment were estimated using a mixed model for repeated measurements using all post-baseline measurements up to the end of treatment. The model included visit, dose group, race, and race-by-dose interaction as fixed factors and baseline value as covariate. Furthermore, interaction terms of visit-by-dose group, visit-by-race, visit-by-race-by-dose group, and visit-by-baseline value were included. Fasting insulin, C-peptide, glucagon, and pro-insulin were logarithmically transformed.

Safety endpoints were summarized descriptively. We used SAS version 9.3 for all analyses.

In total, 44 subjects (Japanese, n = 22; Caucasian, n = 22) were randomized and exposed to the trial product between May and October 2014, from 108 subjects initially screened for eligibility. Three Caucasian subjects withdrew from the trial for personal reasons: one in the semaglutide 0.5 mg group (day 50) and two in the semaglutide 1.0 mg group (days 29 and 36). Baseline characteristics and demographics are shown in Table 1. Caucasian subjects were on average taller and weighed more than their Japanese counterparts (73.0 versus 63.6 kg, respectively). There were no other marked differences in baseline characteristics between dose groups, and BMI levels were comparable between the populations. In line with the criteria for healthy volunteers, glycemic parameters were within the normal range. Baseline insulin, pro-insulin, C-peptide, and glucagon levels were also similar between race groups.

Plasma levels of semaglutide were detectable in all semaglutide-treated subjects, and below the assay LLOQ in all subjects receiving placebo. The full plasma concentration–time profile of semaglutide, from first dose until follow-up, is shown in Fig. 2. Mean semaglutide concentration profile was comparable between race groups throughout the trial period at both dose levels. Semaglutide concentrations increased from day 28, reflecting the dose-escalation step from 0.25 to 0.5 mg in all groups. Similarly, mean semaglutide concentrations increased from day 56 in the 1.0 mg groups, following the final dose-escalation step from 0.5 to 1.0 mg. Pharmacokinetic samples were taken more frequently for 0–168 h following the first dose (day 0) and 0–840 h after the last dose (day 84), as indicated by the graph peaks (Fig. 2).

The mean semaglutide concentration profile during the dosing interval at steady state, from day 84, was similar in Japanese and Caucasian subjects within each dose group (Fig. 3). The exposure of semaglutide at steady state (AUC_{0–168h,sema,SS}) was comparable between Japanese and Caucasian subjects in both dose groups (Table 2), with similar estimated race ratios for semaglutide 0.5 and 1.0 mg doses (Table 3). There was a dose-dependent increase for AUC_{0–168h,sema,SS} in both populations, which is in accordance with dose proportionality (Table 2), as shown by estimated treatment ratios (semaglutide 1.0 mg/semaglutide 0.5 mg) that were close to 2 for both populations (Table 3). There was no statistically significant race-by-dose group interaction.

The C_max,sema,SS of semaglutide at steady state was also similar between Japanese and Caucasian subjects (Table 2), with estimated race ratios close to 1 and estimated treatment ratios close to 2 (Table 3). Other pharmacokinetic endpoints at steady state (t_max,sema,SS, CL/F_sema,SS) were comparable between the populations in both dose groups (Table 2). The elimination of semaglutide during follow-up, following the final dose, is shown in Supplementary Fig. S1. Although the V_z/F_sema,SS of semaglutide was similar between the populations and doses, the half-life of semaglutide (t_1/2,sema,SS) appeared to be slightly lower in the 0.5 mg Japanese group versus the other dose groups (Table 2).

The exposure (AUC_{0–168h,sema,SD}) and C_max,sema,SD after a single dose (0.25 mg) of semaglutide was slightly higher in Japanese versus Caucasian subjects, as shown by estimated race ratios above 1 (Supplementary Table S1; Supplementary Fig. S2) and the t_max,sema,SD was earlier for Japanese subjects than for Caucasian subjects.

Trough plasma concentrations (C_trough,sema concentration 1 week after the fourth dose of all dose levels) were similar between race groups and across doses, and trough levels were greater with the higher 1.0 mg dose upon dose escalation (Fig. 2). The dose-corrected accumulation ratio (R_{acc, DC,sema}) was slightly lower in Japanese subjects than in Caucasian subjects (Table 3) but was comparable among dose groups (0.5 and 1.0 mg).

Mean body weight was decreased by 1.4 and 5.0 kg with semaglutide 0.5 and 1.0 mg, respectively, compared with an increase of 1.1 kg with placebo in Japanese subjects [estimated treatment difference versus placebo − 2.4 kg (p ≤ 0.05) and − 6.1 kg (p ≤ 0.05)]. In Caucasian subjects, mean body weight was reduced by 3.6 kg with semaglutide 0.5 mg and 7.5 kg with semaglutide 1.0 mg, versus an increase of 0.7 kg with placebo [estimated treatment difference − 4.3 kg (p ≤ 0.05) and − 8.3 kg (p ≤ 0.05)] (Supplementary Table S2).

No clinically significant changes in the different parameters of glucose metabolism from baseline to end of treatment were observed. There was a slight reduction in FPG in Japanese subjects receiving semaglutide 0.5 and 1.0 mg, compared with placebo and in Caucasian subjects receiving semaglutide 1.0 mg (Supplementary Table S2).

Overall, 32 subjects were exposed to semaglutide and 12 subjects to placebo across both populations. No deaths, serious adverse events, or adverse events leading to withdrawal were reported. The proportions of Japanese subjects reporting adverse events were 75.0% and 62.5% with semaglutide 0.5 and 1.0 mg, respectively, compared with 16.7% of subjects receiving placebo. In the Caucasian population, 50.0%, 62.5%, and 33.3% of subjects reported adverse events with semaglutide 0.5, 1.0 mg, and placebo, respectively (Supplementary Table S3). The number of events was higher in the semaglutide 1.0 mg group, compared with the 0.5 mg group (driven by three subjects having multiple events), with no apparent difference between the race groups. All adverse events were mild to moderate in severity; none were severe. Gastrointestinal adverse events were the most frequently reported events, and more common with semaglutide than placebo. A higher proportion of Japanese subjects reported gastrointestinal adverse events than Caucasian subjects: 62.5%, 37.5%, and 16.7% of Japanese subjects receiving semaglutide 0.5, 1.0 mg and placebo, respectively, versus 25.0%, 25.0% and 0.0% of Caucasian subjects, respectively (Supplementary Table S3). No hypoglycemic events were reported during the trial.

There was an elevation in pulse rate from baseline to end of treatment in subjects receiving semaglutide, with no apparent difference across the races and doses. Pulse rate increased by 8.5 beats per minute (bpm) and 10.4 bpm in Japanese subjects receiving semaglutide 0.5 and 1.0 mg, respectively, versus a decrease of 0.5 bpm with placebo. In Caucasian subjects, pulse rate increased by 14.6, 10.5, and 2.8 bpm with semaglutide 0.5, 1.0 mg, and placebo, respectively.

There were no clinically significant abnormalities in ECG readings or physical examinations. No noticeable trends were found in the biochemistry parameters, including amylase, lipase and calcitonin, in any of the treatment or race groups. No subjects developed anti-semaglutide antibodies as a consequence of semaglutide treatment.

Below is the link to the electronic supplementary material.

Sponsorship for this study, article processing charges, and the open access fee were funded by Novo Nordisk, A/S.

We also thank Gurudutt Nayak (Novo Nordisk A/S, Denmark) for his review and input to the manuscript, and Nicole Antonio, PhD (AXON Communications, UK) for medical writing and editorial assistance. Support for this assistance was funded by Novo Nordisk.

All of the named authors meet the International Committee of Medical Journal Editors (ICMJE) criteria for authorship for this manuscript, take responsibility for the integrity of the work as a whole, and have given final approval for the version to be published. All authors had full access to all of the data in this study and take full responsibility for the integrity of the data and accuracy of the data analysis.

We thank all the participants, investigators, and trial-site staff from Medical Co. LTA, Sumida Hospital in Tokyo, Japan who were involved in the conduct of the trial.

Shin Irie’s institution has received funding to conduct clinical trials from Novo Nordisk, Eli Lilly and Company, Teijin Pharma, Daiichi Sankyo Company, Takeda Pharmaceutical Company Limited, Sanofi K.K., Nippon Boehringer Ingelheim Co., and AstraZeneca. Ippei Ikushima’s institution has also received funding to conduct clinical trials from Novo Nordisk, Eli Lilly and Company, Teijin Pharma, Daiichi Sankyo Company, Takeda Pharmaceutical Company Limited, Sanofi K.K., Nippon Boehringer Ingelheim Co., and AstraZeneca. Lene Jensen is an employee and shareholder of Novo Nordisk A/S. Anne Flint is an employee and shareholder of Novo Nordisk A/S. Jeppe Zacho is an employee and shareholder of Novo Nordisk A/S. Tomoyuki Nishida is an employee of Novo Nordisk Pharma Ltd. and shareholder of Novo Nordisk A/S.

Prior to initiation, the trial protocol and any amendments, the consent form, and the subject information sheet were reviewed and approved according to local regulations by appropriate health authorities, and by an institutional review board (IRB). The IRB for this study was Medical Co. LTA Hakata Clinic IRB, Japan.

All procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and/or national research committee and with the 1964 Declaration of Helsinki and its later amendments and the International Conference on Harmonization Good Clinical Practice guidelines. Informed consent was obtained from all individual participants included in the study.

The datasets generated and/or analyzed during the current study are not publicly available as this was a phase I study, but are available from the corresponding author on reasonable request.

This article is distributed under the terms of the Creative Commons Attribution-NonCommercial 4.0 International License (http://creativecommons.org/licenses/by-nc/4.0/↗), which permits any noncommercial use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made.

The datasets generated and/or analyzed during the current study are not publicly available as this was a phase I study, but are available from the corresponding author on reasonable request.