Investigation of safety, tolerability, pharmacokinetics, and pharmacodynamics of single and multiple doses of a long‐acting α‐MSH analog in healthy overweight and obese subjects

MC4-NN2-0453 is a novel, long-acting, selective, melanocortin-4-receptor agonist developed for treatment of obesity. This first-human-dose, randomized, double-blind, placebo-controlled trial investigated the safety, tolerability, pharmacokinetics, and pharmacodynamics of single and multiple doses of MC4-NN2-0453 in overweight to obese but otherwise healthy subjects. The trial included a single-dose part of ascending subcutaneous 0.03–1.50 mg/kg doses in overweight to obese but otherwise healthy men, and a multiple-dose part of ascending subcutaneous 0.75–3.0 mg/day doses in obese but otherwise healthy men/women. The single-dose part included 7 cohorts of 8 subjects, randomized 6:2 to active drug/placebo; the multiple-dose part included 4 cohorts of 20 subjects, randomized 16:4 to active drug/placebo. MC4-NN2-0453 was well tolerated and raised no safety concerns except for nonserious skin-related adverse events, this along with lack of weight loss effect led to premature termination of the trial. Headache, sexual–arousal disturbance, and penile erection were also reported. Single-dose pharmacokinetics showed dose-linearity and dose-proportionality. Maximum plasma concentration was observed after 50–100 hours, which then declined with a of approximately 250 hours. Plasma concentration reached steady state after 4 weeks for 0.75 and 1.5 mg/day multiple-dose cohorts, and the was similar to single dose. There were no significant pharmacodynamic effects, including effect on body weight.

This was a randomized, double-blind, placebo-controlled, two-part trial (a sequential s.c. SD ascending part and a semi-sequential s.c. MD ascending part) conducted to investigate the safety, tolerability, PK, and PD of MC4-NN2-0453 in overweight or obese but otherwise healthy male and female subjects.

The MD part consisted of four dose cohorts. In each cohort, 20 subjects were to be randomized 16:4 to receive active drug (0.75, 1.5, 3.0, and 5.0 mg/day) or placebo. Approximately 30 days after the start of each MD cohort, an internal trial safety group evaluated the cumulative safety, tolerability, and PK before agreeing upon the next dose level. All subjects attended an information visit, a screening visit (Days −28 to −2), two extended in-house treatment visits (Days −1 to 5 and Days 69 to 74), nine ambulatory treatment visits (Days 8, 15, 22, 29, 36, 43, 50, 57, and 64), five ambulatory safety visits (Days 77, 84, 91, 98, and 105), an ambulatory follow-up visit (Day 112), and an ambulatory visit for sampling anti-MC4-NN2-0453 antibodies (Day 210). All dose administrations except for those on Days 1 and 4 were done by the subjects themselves after instruction. The drug was to be administered once daily after an overnight fast on Days 1–70.

For the SD part, blood was drawn for PK analysis just before dosing (0 hour) and at time points 2, 6, 12, 18, 24, 32, 40, 48, 56, 64, 72, 80, 88, 96, 104, 112, 120, 128, 144, 168, 216, 264, 312, 360, 408, and 504 hours after dosing (Days 1–22). For the MD part, blood was drawn for PK analysis just before dosing on Days 1, 2, 3, 4, 5, 8, 15, 22, 29, 36, 43, 50, 57, 64, and 70 (trough samples), and at time points 2, 6, 12, and 18 hours post-dosing at Days 1 and 4. Following the last dose (Day 70) for cohort 1, blood was drawn at 2, 6, 12, 18, 24, 32, 40, 48, 72, 96, 168, 336, 504, 672, 840, and 1,008 hours (42 days later) post-final-dose. For cohort 2, the last pre-dose sample was drawn on Day 50 (n = 12) or Day 36 (n = 2), 22 or 15 (n = 1 per day) and for cohort 3, the last pre-dose sample was drawn at Day 15 (n = 14) or Day 8 (n = 2). Dosing was terminated within days hereafter for cohort 2 and cohort 3 subjects. Blood was thereafter drawn at 168, 336, 504, 672, 840, and 1,008 hours post-last-dose. The blood samples were collected by venipuncture or cannulation in EDTA tubes and frozen at −20°C after centrifugation at 4°C.

The primary objective of the trial was safety and tolerability of ascending SD and MD of MC4-NN2-0453 assessed by AEs including sexual disturbance (examination for priapism by an urologist) and hypoglycemic episodes, clinical laboratory tests (anti-MC4-NN2-0453 antibodies for the MD part), Holter monitoring (for the SD part), 12-lead ECG, physical examination, vital signs including blood pressure (BP) monitoring, pulse and temperature, injection-site assessment, and determination of SD and MD maximum tolerated dose (MTD). Mental health was assessed using the PHQ-9 (patient health questionnaires): PoMS (The Profile of Mood States Questionnaire) and C-SSRS (The Columbia Suicidality Severity Rating Scale Questionnaire) questionnaires. The trial was put on hold because of unexpected skin-related AEs, and all subjects were called in for a dermatologic assessment by a dermatologist. All subjects were offered biopsy and standard care by the dermatologist. Twenty-two (22) of the 27 subjects with clinically atypical nevi underwent biopsies including a histology evaluation. The dermatological report showed seven subjects diagnosed with mild histologic atypia. Three (3) of the 27 subjects did not consent to the biopsy, and 2 subjects did not attend the dermatologic assessment visit. Given the dermatological findings, the sponsor decided to terminate the trial prematurely. All subjects in the MD-part were transferred to Visit 13 (ambulatory safety visit) and were followed as per the protocol for the next 10 weeks, and as described earlier all drug-exposed subjects were invited for an extra dermatological follow-up visit 1 year later.

The PD evaluation for the SD part included change in body weight and lipid profile, and the PD evaluation for the MD part included change in body weight, lipid profile, waist and hip circumference, waist–hip ratio, subjective self-reported appetite variables [appetite, taste, hunger, thirst, nausea, cravings, palatability, and fullness using visual analog scale (VAS) scores], caloric intake, and homeostatic model for insulin resistance (HOMA IR).

All dose cohorts in the SD part completed the trial, whereas only cohort 1 (0.75 mg/day) in the MD part completed the trial. Because of unexpected incidents of nonserious skin-related AEs, cohorts 2 (1.5 mg/day) and 3 (3.0 mg/day) were prematurely terminated after approximately 49 and 14 days of treatment, respectively; cohort 4 (5.0 mg/day) was not initiated. The results for all initiated cohorts are presented, including the 1-year dermatological follow-up results for subjects who were on active treatment. In the SD part, 53 of 57 randomized subjects completed the trial. Four subjects in the SD part discontinued the trial due to withdrawal of consent for reasons unrelated to safety. The demographic features and baseline characteristics of the trial subjects are shown in Table 2 for the SD part. The mean age of the SD trial population was 34.9 ± 9.4 years, and mean BMI was 31.7 ± 3.2 kg/m 2 . 2a Baseline Characteristics: Single Dose (Part 1): All Randomized Subjects Placebo (n =14) 0.03 mg/kg (n = 6) 0.06 mg/kg (n = 6) 0.15 mg/kg (n = 6) 0.30 mg/kg (n = 6) 0.60 mg/kg (n = 7) 1.00 mg/kg (n = 6) 1.50 mg/kg (n = 6) Age (years) 32.9 (6.7) 37.3 (11.2) 32.3 (12.3) 39.3 (11.3) 35.2 (11.8) 37.6 (4.5) 35.0 (7.1) 31.8 (13.6) Race, n (%) White 12 (86) 6 (100) 5 (83) 5 (83) 4 (67) 2 (29) 4 (67) 5 (83) Black or African American 2 (14) 0 1 (17) 1 (17) 2 (33) 4 (57) 2 (33) 0 Asian 0 0 0 0 0 0 0 0 Other 0 0 0 0 0 1 (14) 0 1 (17) Body weight (kg) 105.0 (17.3) 96.6 (13.7) 93.2 (8.9) 95.1 (13.1) 89.4 (10.6) 97.0 (8.8) 101.5 (15.1) 97.8 (12.3) BMI (kg/m 2 ) 32.1 (3.1) 32.2 (4.8) 30.8 (2.5) 31.0 (3.4) 30.4 (2.0) 32.3 (2.1) 33.0 (4.2) 31.2 (3.5) Data are mean (standard deviation) unless otherwise specified. BMI, body mass index. Sixty randomized subjects were assigned to one of the three cohorts in the MD part. While the MD part was ongoing, two subjects withdrew consent (not safety-related), one subject was lost to follow-up, and one subject was withdrawn due to nonadherence to scheduled visits. The demographic features and baseline characteristics of the trial subjects are shown in Table 3 . In the MD part, there were 21 males and 39 females. The mean age of the MD part population was 40.1 ± 11.2 years, and mean BMI was 34.4 ± 2.3 kg/m 2 across treatment cohorts. 2b Baseline Characteristics: Multiple Dose (Part 2): All Randomized Subjects Placebo 0.75 mg/day 1.5 mg/day 3.0 mg/day Age (years) 35.4 (11.1) 43.8 (11.9) 38.6 (8.2) 41.4 (12.6) Sex, M:F [n (%)] 5:7 (42:58) 4:12 (25:75) 8:8 (50:50) 4:12 (25:75) Race, n (%) White 10 (83) 13 (81) 8 (50) 14 (88) Black or African American 2 (17) 3 (19) 6 (38) 2 (13) Asian 0 0 1 (6) 0 Other 0 0 1 (6) 0 BMI (kg/m 2 ) 34.5 (2.3) 34.9 (2.4) 34.5 (2.2) 33.8 (2.3) Data are mean (standard deviation) unless otherwise specified. M, male; F, female, BMI, body mass index. Safety No serious AEs, deaths, or discontinuations due to AEs were reported. In the SD part, 41 (71.9%) subjects reported a total of 94 treatment-emergent adverse events (TEAEs); headache (21.1%) followed by increase in frequency and duration of penile erection (14%), and decreased appetite (12%) were the most common TEAEs. All AEs were mild to moderate in severity. In the MD part, 54 (90%) subjects reported a total of 264 TEAEs; melanocytic nevus (45%), skin hyperpigmentation (33.3%), headache (30%), and sexual disturbance (increase in frequency and duration of penile erection or sexual arousals) (27%) were the most common TEAEs. All but three subjects in the MD part recovered; one subject experienced AEs of seborrheic dermatitis and blepharospasm; one subject experienced sciatica and depression; and one subject reported hypothyroidism. All the AEs reported by these three subjects were assessed to be unlikely related to the trial drug. Skin-related AEs In the SD part, clinically atypical melanocytic nevus was reported by one subject (16.7%) in the 1.0 mg/kg cohort and by one subject in the 1.5 mg/kg dose cohort, both revealed mild histological atypia after biopsy. Two subjects (28.6%) in the 0.60 mg/kg dose cohort and one subject (16.7%) in the 1.5 mg/kg dose cohort reported skin hyperpigmentation on sun-exposed areas. None receiving placebo reported either melanocytic nevus or skin hyperpigmentation. No increase in these events with increasing doses was observed. All skin-related AEs were mild in severity. All subjects recovered except for one subject in the 1.5 mg/kg active treatment cohort who reported with typical melanocytic nevus and who was recovering; the subject withdrew from follow-up. In the MD part, clinically atypical melanocytic nevus including the palmar and the plantar location was reported for 6 (37.5%), 12 (75%), and 9 (56.3%) subjects on active treatment in the 0.75, 1.5, and 3.0 mg/day dose cohorts, respectively. All these subjects with clinically atypical nevus were called for a dermatological evaluation during which biopsy performed revealed mild histological atypia for five subjects. There were no reports of

Seven males on active treatment and one male on placebo in the SD part experienced an increase in frequency as well as duration of penile erection. During the MD trial, six males (all on active treatment) were noted to have increased frequency as well as duration of penile erection, and seven females (one on placebo) had disturbance in sexual arousal; however, tolerance to this effect was seen with repeated dosing. None of these events were dependent on exposure, and there was no priapism reported.

Three subjects in the MD part tested positive for low-titer, non-neutralizing, non-cross-reacting antibodies. No injection-site reactions were reported. There were no clinically relevant psychological changes as assessed by PHQ-9 questionnaires. MTD was not established for the SD part. However, the maximum feasible dose reached in the SD part was 1.5 mg/kg. All the doses were nontolerable in the MD part because of the onset of skin-related AEs in all dose cohorts, leading to premature termination of the trial.

Mean plasma concentration–time profiles for MC4-NN2-0453 at steady state following MDs of MC4-NN2-0453 are presented in Figure 2 b. The mean exposure to MC4-NN2-0453 increased with increasing dose after multiple dosing with 0.75, 1.5, and 3.0 mg/day. The plasma PK parameters at steady state are presented in Table 5 . The mean C max and AUC 0–24h on days 1 and 4 increased approximately dose-proportionally after multiple dosing of 0.75, 1.5, and 3.0 mg/day. However, the dose proportionality could not be determined, as only one dose cohort was finalized. Steady state was achieved after Day 29 for the 0.75 and 1.5 mg/day cohorts. From data available for all three cohorts, the mean t max on days 1 and 4 ranged between 19.9 and 23.9 hours. Similar to the SD part, (232–253 hours) was fairly long and consistent across dose cohorts. Accumulation was 25 times in the 0.75 mg/day cohort. AUC 0–∞ was 275,000 h × ng/mL for the 0.75 mg/day dose cohort; AUC 0–∞ was not estimated for the 1.5 or 3.0 mg/day dose cohorts as the trial was prematurely terminated. 3b Multiple Dose (Part 2): Pharmacokinetic Parameters for MC4-NN2-0453 0.75 mg/day 1.5 mg/day 3.0 mg/day Day 1 (n = 16) Day 4 (n = 16) Day 70 (n = 14) Day 1 (n = 16) Day 4 (n = 16) Day 70 (n = 16) Day 1 (n = 16) Day 4 (n = 16) Day 70 (n = 15) C max (ng/mL) 49.7 (12.4) 199 (41.7) 723 (155) 99.4 (21.9) 387 (63.4) NA 229 (47.4) 947 (184) NA t max (hour) 23.6 (1.5) 19.9 (5.2) 24.9 (15.4) 23.9 (0.0) 22.1 (3.6) NA 23.9 (0.0) 21.3 (4.3) NA t ½ (hour) NA NA 232 (31.0) NA NA 234 (40.4) NA NA 253 (31.5) AUC 0–24h (h ng/mL) 698 a (168) 4,320 a (862) 16,500 a (3,580) 1,140 a (397) 8,330 a (1,420) NA 3,320 a (954) 20,800 a (4,170) NA Data are mean (standard deviation). NA, not applicable. Cohort 2 (1.5 mg/day) terminated around Visit 9 and were transferred to Visit 13 within 1 week. Cohort 3 (3.0 mg/day) terminated around Visit 4 and were transferred to Visit 13 within 1 week. a Steady state has not been reached.

This was the first human-dose trial of the long-acting MC4R agonist MC4-NN2-0453, developed for weight loss and weight maintenance in overweight to obese individuals. There were no serious or severe AEs reported in this trial. The trial was prematurely terminated because of unexpected incidences of nonserious skin-related AEs in the three highest dose cohorts in the SD part and in all dose cohorts in the MD part. Though, these skin related AEs of mild severity were well tolerated (these AEs showed recovery) and did not lead to any discontinuations, no possible weight loss benefits were seen at doses where these nonserious skin related AEs started appearing and thus leading to trial termination. All the skin-related AEs were considered likely to be related to the trial drug (all events except one occurred in active treatment groups). Other common AEs reported were headache, sexual disturbance, nausea, and injection-site hemorrhage observed with both MC4-NN2-0453 and placebo. MC1 receptors are located in the skin on human melanocytes mediating the melanogenic and proliferative effects of melanotropic peptides. 20 , 21 The skin hyperpigmentation was therefore unexpected given the low affinity of MC4-NN2-0453 for MC1 receptors and high affinity for the MC4R (MC4:MC1R selectivity 1,000:1). 13 Melanocortin analogs such as melanotan-I and -II are potent, nonselective melanocortin agonists. They have been tested as skin-tanning agents in clinical trials with the therapeutic potential to prevent skin cancer (and intolerance to sun exposure), 22 – 25 suggesting that regulated use of these agents at clinical doses could be safe. Unlicensed use of these nonselective α-MSH analogs has resulted in skin hyperpigmentation and darkening of existing nevus. 26 , 27 This could be explained by their action through MC1R in the skin by increased signaling and proliferation of well-differentiated melanocytes. 21 Skin hyperpigmentation occurring in the SD part could possibly be due to the constant and very high exposure to MC4-NN2-0453; exposure levels of 2.3–3.1 µM were observed, which is close to the K i value of 2.7 µM of MC4-NN2-0453 on the MC1R. 13 Even in the presence of albumin binding, this may be enough to stimulate the melanocytes. In the MD part as well, steady-state exposure levels were 0.34 and 0.67 µM with doses of 0.75 and 1.5 mg/day, respectively; C trough reached with the 3.0 mg dose was 1.05 µM. It is known that exposure to α-MSH analogs leads to up-regulation of MC1 receptors in the skin and in congenital nevi expression of MC1 receptors are increased 28 ; this, along with exposure to UV radiation (which indirectly stimulates α-MSH secretion), leads to increased expression of MC1 receptors. 29 , 30 Furthermore, a synergistic effect on tanning of melanotan-I and UV-B light was reported by Dorr et al. 25 Although MC4-NN2-0453 is an analog with very high receptor specificity for the MC4R versus the MC1R, the high-exposure level and the eventual increase in MC1R expression could explain the increase in number and pigmentation of nevi both in sun-exposed and acral area as well as the hyperpigmentation induced by MC4-NN2-0435 in this trial. Acral nevi have been shown to be associated with ethnicity, pigmentation, age, and cutaneous melanoma risk factors and are not uncommon phenomena. 31 Change in penile erection observed during the trial was reported more frequently in the active treatment group than in the placebo group. The changes can be explained by the role of melanocortin in erectile function. Human trials with melanotan-II and its derivative PT141 have demonstrated erectogenic activity in males with erectile dysfunction 32 , 33 and arousal in females with sexual behavior disorders, 34 indicating a potential for the treatment of sexual dysfunction. In contrast, a clinical trial conducted with the MC4R agonist MK-0493 failed to demonstrate the same effect 35 ; it also failed to demonstrate effect on body weight and energy intake, 36 which perhaps indicates that exposure was too low to affect penile erection and body weight. In the current trial, MC4-NN2-0453 exhibited a neutral effect on BP despite being an MC4R agonist. This is in contrast to the MC4R agonist LY2112688, which significantly ( P < .001) increased both SBP and DBP. 37 The melanocortin system through MC4R regulates BP by modulating central sympathetic flow. 37 The lack of effect on BP in the current trial could have been due to the limited capacity of MC4-NN2-0453 to cross the blood–brain barrier. Though, there was an initial effect on penile erection, indicating some availability to the central nervous system, as penile erection is thought to be centrally mediated, 33 apparently the central exposure may not have been high enough to mediate an effect on body weight. In the SD part, the PK of MC4-NN2-0453 was dose-proportional and linear, but dose proportionality was statistically significant only for AUC 0–24h . AUC 0–24h , however, most likely r

Gitte Konradsen, Ole Eskerod, Birgit S. Hansen, and Birgitte S. Wulff are employees of Novo Nordisk A/S.