Efficacy and Safety of IDegAsp Versus BIAsp 30, Both Twice Daily, in Elderly Patients with Type 2 Diabetes: Post Hoc Analysis of Two Phase 3 Randomized Controlled BOOST Trials

The trial designs for BOOST INTENSIFY PREMIX I (global population) and BOOST INTENSIFY ALL (pan-Asian population) have been described previously [31, 32] and are similar (Fig. 1). Both trials were phase 3a, randomized, parallel, open-label, multicenter trials with an intent-to-treat design and a duration of 26 weeks.

In BOOST INTENSIFY PREMIX I, eligible patients had been treated previously with either premixed or self-mixed insulin (once or twice daily) ± oral antidiabetic drugs (metformin, sulfonylureas, glinides, alpha-glucosidase inhibitors, dipeptidyl peptidase-4 inhibitors, and pioglitazone) for ≥ 3 months. In BOOST INTENSIFY ALL, patients who had been receiving once- or twice-daily basal insulin, a premixed insulin, or a self-mixed insulin ± metformin were eligible. Inclusion criteria for the two trials were otherwise similar; patients were eligible for inclusion if they were ≥ 18 years of age (≥ 20 for BOOST INTENSIFY ALL participants in Japan and Taiwan), with glycated hemoglobin (HbA_1c) 7.0–10.0% (53–86 mmol/mol) and body mass index (BMI) < 40 kg/m² (BOOST INTENSIFY PREMIX I) or < 35 kg/m² (BOOST INTENSIFY ALL). In both trials, patients were excluded if they had a history of recurrent severe hypoglycemia or hypoglycemic unawareness. The Japanese subgroup was drawn from the overall population. For this post hoc analysis, all patients who were aged 65 years or over were included.

The protocols, protocol amendments, consent forms, and subject information sheets of the original BOOST INTENSIFY PREMIX I and BOOST INTENSIFY ALL trials were reviewed and approved by health authorities according to local regulations and by the local independent ethics committees prior to trial initiation [31, 32]. The trials were performed in accordance with the Declaration of Helsinki and good clinical practice [36, 37]. In summary, 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 or comparable ethical standards. Informed consent was obtained from all individual participants included in the study.

The current analyses present pooled data from both trials for the elderly subpopulation. The primary endpoint in both trials was change from baseline in HbA_1c after 26 weeks of treatment. A linear regression model (analysis of covariance) was used to analyze the change in HbA_1c from baseline to end of treatment with trial, treatment, sex, geographic region, and antidiabetic treatment at screening as grouping factors and age and baseline response as covariates. For individual trial groups, trial is not included as a fixed effect. Missing data were accounted for using the last observation carried forward method. Fasting plasma glucose (FPG) and insulin dose (log transformed) were analyzed using the same model.

The number of treatment-emergent confirmed hypoglycemic events was analyzed with a negative binomial regression model, using a log-link function adjusted for trial, treatment, sex, geographic region, and antidiabetic treatment at screening as fixed effects, age as covariate, and the logarithm of the exposure time as offset.

All patients receiving at least one dose of trial product were included in the safety analysis set. Safety was assessed using overall confirmed hypoglycemia and nocturnal hypoglycemia, based on the Novo Nordisk classification for hypoglycemia (plasma glucose 56 mg/dL [< 3.1 mmol/L]). Adverse events were coded using the most recent version of Medical Dictionary for Regulatory Activities (MedDRA) coding (version 13.0 for BOOST INTENSIFY PREMIX I and version 13.1 for BOOST INTENSIFY ALL).

The combined analysis comprised 271 patients (representing 31.2% of the total population from the two trials), of whom 146 were treated with IDegAsp twice daily and 125 were treated with BIAsp 30 twice daily. Japanese patients comprised the largest subgroup (N = 72, 26.6% of the analyzed cohort). Baseline characteristics for the subpopulation of patients aged ≥ 65 years from each trial and from the pooled data are shown in Table 1. The mean age at baseline, BMI, duration of diabetes, HbA_1c (%; mmol/mol), and FPG were similar for both treatment arms in the pooled data. BMI at baseline was lower in the pan-Asian population compared with the global population. Duration of diabetes was longer in the pan-Asian population compared with the global population.

There were no statistically significant differences in HbA_1c in the combined analysis between treatment with IDegAsp or BIAsp 30 (estimated treatment different [ETD, IDegAsp–BIAsp 30]: −0.02% [− 0.19; 0.15]_{95% CI}, p  = 0.8455). A significant reduction in FPG was observed with IDegAsp versus BIAsp 30 (ETD [IDegAsp–BIAsp 30]: − 1.41 mmol/L [− 1.85; − 0.96]_{95% CI}, p  < 0.0001). Similar results were observed in Japanese patients, with an ETD (IDegAsp–BIAsp 30) of − 0.01% [− 0.31; 0.29]_{95% CI}, p  = 0.9521 for HbA_1c and − 1.86 mmol/L [− 2.75; − 0.97]_{95% CI}, p  < 0.0001 for FPG (Table 2).

Overall confirmed and nocturnal hypoglycemic events by classification are shown, by trial population and for the combined analysis, in Table 3. The estimated rate ratios for overall confirmed and nocturnal confirmed hypoglycemia for the combined analysis are shown in Fig. 2. In the combined analysis, there were fewer overall confirmed hypoglycemic events with IDegAsp (1041.18 events/100 patient-years of exposure [PYE]) compared with BIAsp 30 (1134.40 events/100 PYE), estimated rate ratio (ERR): 0.92 [0.67; 1.26]_{95% CI}, p  = 0.5980. There were fewer nocturnal hypoglycemic events in patients treated with IDegAsp compared with patients treated with BIAsp 30, ERR (IDegAsp/BIAsp 30): 0.67 [0.39; 1.18]_{95% CI}, p  = 0.1676. In the Japanese patient population, there was a 12% lower rate of overall confirmed hypoglycemia with IDegAsp compared with BIAsp 30, ERR: 0.88 [0.47; 1.66]_{95% CI}; p = 0.7026. There was also a 42% lower rate of nocturnal hypoglycemia with IDegAsp compared with BIAsp 30, which was not significant, ERR: 0.58 [0.22; 1.51]_{95% CI}, p  = 0.2643, in the Japanese subpopulation.

Mean insulin dose at the end of the trial was significantly lower for patients treated with IDegAsp than for patients treated with BIAsp 30, with an estimated treatment ratio (ETR) of 0.79 [0.73; 0.87]_{95% CI}, p  < 0.0001. Results were similar and also significant in Japanese patients, with an ETR of 0.78 [0.65; 0.95]_{95% CI}, p  = 0.0121 (Table 2).

Overall, 271 patients were included in the safety analysis set, 146 of whom were in the IDegAsp treatment arm and 125 were in the BIAsp 30 treatment arm. A slightly higher percentage of patients reported one or more AE with IDegAsp versus BIAsp 30 (70.5% vs. 60.8%, respectively). There were more withdrawals among patients treated with BIAsp 30 (19.0%) than with IDegAsp (14.4%), but the majority of the withdrawals were not a result of AEs (Table 4). The majority of the AEs were considered unlikely to be related to trial production in BOOST INTENSIFY PREMIX I (71% with IDegAsp and 57% with BIAsp 30) and BOOST INTENSIFY ALL (69% with IDegAsp and 58% with BIAsp 30).