The development of insulins has long been central to improvements in the management of diabetes mellitus. The first insulin preparations varied significantly in potency. Also, contamination of insulin solutions was common. Thus, considerable attention was devoted to the development of higher-quality formulations. Intermediate-and long-acting insulins were designed to establish stable background levels of insulin. Improved purification methods and recombinant production techniques virtually eliminated insulin dystrophy and allergy. With the strategy of intensive insulin therapy, a nearly physiologic model of insulin replacement has been introduced.
Nevertheless, poor glycemic control still occurs in many patients.1,2 This outcome is due in part to the essential limitation of using subcutaneous injections to deliver insulin systemically. However, it has also been attributed to insulin formulations that remain suboptimal. The introduction of rapid-and long-acting insulin analogues with action profiles resembling physiologic conditions more closely than conventional insulins yielded hope for substantial improvement in glycemic control.
In this issue of CMAJ, Singh and colleagues3 report on the differences in glycemic control and risk of hypoglycemia between insulin analogues and conventional insulins in adults and children with type 1 diabetes, in adults with type 2 diabetes and in pregnant women with type 1 or gestational diabetes. Regrettably, their results again confirm that conclusions cannot be drawn about the long-term effects of insulin analogues on the risk of diabetes-related complications and death. Despite their efforts to include studies of at least 4 weeks' duration, only short-term trials were available. Singh and colleagues indicate that differences in hemoglobin A1c, risk of hypoglycemia and quality of life were at best minor and of clinically debatable relevance. Their findings are consistent with those of other systematic reviews and meta-analyses of insulin analogues.4–6
Singh and colleagues reported only on insulins that are marketed in Canada. A Cochrane review of rapid-acting insulin analogues published in 2006 looked at a third analogue, insulin glulisine.4 This rapid-acting analogue was shown to be no better than regular insulin in terms of glycemic control or reduced risk of hypoglycemia in patients with type 1 diabetes. Since then, another study that met the Cochrane criteria4 compared insulin glulisine and regular insulin in type 2 diabetes; it also showed no difference in effectiveness between the 2 insulins.7
Despite the evidence, myths abound regarding the benefits of insulin analogues and require correction. First, compared with regular insulin, insulin analogues produce only minor additional reductions in hemoglobin A1c. For all such comparisons, whether of long-acting or rapid-acting insulin analogues in type 1 or type 2 diabetes, the observed difference in hemoglobin A1c is well below 0.4%. This level is commonly accepted in studies as a margin of inferiority. Even if one assumed that reductions in hemoglobin A1c with insulin analogues would result in similar clinical benefits as those observed in the Diabetes Control and Complications Trial,8 about 650 patients with type 1 diabetes would have to be treated with rapid-acting insulin analogues for 1 year to prevent the development of retinopathy in 1 patient.4
Second, severe episodes of hypoglycemia are rare. Even if nocturnal hypoglycemia occurs slightly less frequently with insulin analogues than with conventional insulins, the overall difference in hypoglycemia is small. A cross-sectional study in Germany involving 35 723 patients (5891 with type 1 diabetes and 29 693 with type 2 diabetes), 59% of whom used insulin analogues, showed that treatment with insulin analogues was not associated with a decreased rate of severe hypoglycemia.9
Third, advantages in terms of quality of life reported with rapid-acting insulin analogues were driven mostly by changes in convenience, flexibility and adherence to treatment. Most of the studies had an open-label design. Patients were advised to inject regular insulin on average 30 minutes before meal time, whereas insulin analogues were injected immediately before meals. One may hypothesize that the difference in injection times is a major underlying reason for improved satisfaction with insulin analogues. The rationale for different injection times in intensified insulin therapy has never been proven in controlled studies. In daily life, most patients seem to use short injection–meal intervals or none at all.10 In addition, a double-blind trial comparing rapid-acting insulin analogues with regular insulin did not show an improvement in any quality-of-life measures with insulin analogues.11
The minor benefits seen with insulin analogues appear to be limited mainly to open-label study designs. A switch to a new insulin preparation, which may be strongly encouraged by physicians, consumer groups and industry, generally brings about an increase in patient motivation and compliance with other important aspects of diabetes care. Based on the available evidence in the report by Singh and colleagues and other systematic reviews, older conventional insulins remain effective. Therefore, the extensive promotion of insulin analogues is not justified. Insulin analogues should be reserved for use in selected patients, such as those with nocturnal hypoglycemia.
Structured programs for self-management training of patients with type 1 and type 2 diabetes have shown a more pronounced, clinically relevant and sustained improvement in glycemic control and reduction in risk of severe hypoglycemia12–15 compared with the relative benefit observed to date with insulin analogues. Until well-designed long-term studies consistently demonstrate the benefits of insulin analogues, money should be spent on structured educational programs to improve outcomes for patients with diabetes.
@@ See related research paper by Singh and colleagues, page 385
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The improved glycemic control, reduced risk of hypoglycemia and improved quality of life achieved with insulin analogues versus conventional insulins are at best minor and of clinically debatable relevance.
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Insulin analogues should be reserved for use in selected patients, such as those with nocturnal hypoglycemia.
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Efforts should be focused on offering structured educational programs to help patients manage their diabetes and improve glycemic control.
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Footnotes
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Contributors: All of the authors were involved in the preparation of this manuscript and approved the final version submitted for publication.
Competing interests: The authors are part of a research group that has performed several studies of rapid-and long-acting insulin analogues with the companies Sanofi-Aventis, Eli Lilly and Novo Nordisk. They were involved in the preparation of a report on the effects of rapid-and long-acting insulin analogues for the German Institute for Quality and Efficiency in Health Care.