When patients with type 2 diabetes find their oral medications alone can no longer control their blood sugar, insulin therapy is added and injection frequency (having daily injections) is among the main factors that can contribute to failures in treatment adherence (others include worry about weight gain and having hypoglycaemic episodes or ‘hypos’).
Insulin efsitora alfa (efsitora) is a new basal insulin designed for once-weekly administration. Clinical data to date on safety and efficacy have been limited to small phase 1 or phase 2 trials. In this new phase 3 study, the efficacy of once-weekly efsitora was compared to daily injections of insulin degludec (a standard insulin) in adult patients that had not yet begun insulin therapy (on multiple oral diabetes medications but still were not at their glycaemic goals).
The authors conducted a 52-week study in which participants were randomly assigned in a 1:1 ratio to receive efsitora or degludec. The primary end point was the change in the glycated haemoglobin (HbA1c – a measure of blood sugar control) level from baseline to week 52; they hypothesised that efsitora would be noninferior to degludec (non-inferiority margin, 0.4%). Secondary and safety end points included the change in the glycated haemoglobin level in subgroups of participants using and not using the relatively new glucagon-like peptide-1 (GLP-1) receptor agonist antidiabetic medications, the percentage of time that the glucose level was in the target range of 70 to 180 mg per decilitre in weeks 48 through 52, and hypoglycaemic episodes.
A total of 928 participants were randomly assigned to efsitora (466) or degludec (462). The mean glycated hemoglobin level decreased from 8.21% at baseline to 6.97% (absolute change 1.26%) at week 52 with efsitora and from 8.24% to 7.05% (absolute change -1.17%) with degludec; a treatment difference of 0.09% that demonstrated non-inferior reduction of Hb1Ac between efsitora and degludec.
Efsitora was also noninferior to degludec with respect to the change in the glycated haemoglobin level in participants using and not using GLP-1 receptor agonists. The percentage of time that the glucose level was within the target range was 64.3% with efsitora and 61.2% with degludec (estimated treatment difference, 3.1 percentage points; statistically significant). The rate of combined clinically significant or severe hypoglycaemia was 0.58 events per participant-year of exposure with efsitora and 0.45 events per participant-year of exposure with degludec, but this finding was not statistically significant. No severe hypoglycaemia was reported with efsitora; six episodes were reported with degludec. The incidence of adverse events was similar in the two groups.
The authors say: “In adults with type 2 diabetes who had not previously received insulin, once-weekly efsitora was noninferior to once-daily degludec in controlling high blood sugar by reducing glycated haemoglobin levels.”
They add: “A once-weekly insulin has the potential to simplify dose administration and diminish barriers to starting insulin therapy by means of a reduction in injection burden as compared with a once-daily insulin. A recent study evaluating preferences for a once-weekly basal insulin in adults with type 2 diabetes indicated that both patients and providers would prefer once-weekly basal insulin over current basal insulin preparations.”
On GLP-1 agonists, they add: “Given treatment guidelines and recommendations to incorporate GLP-1 receptor agonists earlier in treatment, along with their growing use worldwide, it is relevant to show that efsitora can be effectively and safely added to such therapy. Here, efsitora showed noninferiority to degludec with respect to the change in the glycated haemoglobin level among participants using and not using GLP-1 receptor agonists, without substantial treatment differences in hypoglycaemia between subgroups.”
Journal
New England Journal of Medicine
Article Title
Insulin Efsitora versus Degludec in Type 2 Diabetes without Previous Insulin
Article Publication Date
10-Sep-2024
COI Statement
See article for Dr Wysham's and authors' full disclosures