Research Article

Effectiveness of progressive dose-escalation of exenatide (exendin-4) in reducing dose-limiting side effects in subjects with type 2 diabetes

  1. Mark S. Fineman,
  2. Larry Z. Shen,
  3. Kristin Taylor,
  4. Dennis D. Kim,
  5. Alain D. Baron*

Article first published online: 28 JUL 2004

DOI: 10.1002/dmrr.499

Issue

Diabetes/Metabolism Research and Reviews

Diabetes/Metabolism Research and Reviews

Volume 20, Issue 5, pages 411–417, September/October 2004

Additional Information

How to Cite

Fineman, M. S., Shen, L. Z., Taylor, K., Kim, D. D. and Baron, A. D. (2004), Effectiveness of progressive dose-escalation of exenatide (exendin-4) in reducing dose-limiting side effects in subjects with type 2 diabetes. Diabetes/Metabolism Research and Reviews, 20: 411–417. doi: 10.1002/dmrr.499

Author Information

  1. Amylin Pharmaceuticals, Inc., San Diego, CA, USA

*Amylin Pharmaceuticals, Inc., 9360 Towne Centre Dr., Suite 110, San Diego, CA 92121 USA.

Publication History

  1. Issue published online: 26 AUG 2004
  2. Article first published online: 28 JUL 2004
  3. Manuscript Accepted: 14 MAY 2004
  4. Manuscript Revised: 13 MAY 2004
  5. Manuscript Received: 22 JAN 2004

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Keywords:

  • exenatide;
  • exendin-4;
  • type 2 diabetes;
  • incretin mimetic;
  • dose-escalation;
  • mitigation of side effects;
  • reduction of adverse events

Abstract

Background

Exenatide (exendin-4) exhibits dose-dependent glucoregulatory activity, but causes dose-limiting nausea and vomiting. This study was designed to formally assess the possibility of inducing tolerance to the side effects of nausea and vomiting at therapeutic doses of exenatide, using a dose-escalation methodology.

Methods

In this two-arm, triple-blind, multicenter study, 123 subjects with type 2 diabetes were enrolled and randomized; 99 (80.5%) of them completed the study. Subjects in the exenatide-primed arm received subcutaneous exenatide, starting at 0.02 µg/kg three times a day (TID) and increasing in 0.02 µg/kg per dose increments every 3 days for 35 days. Subjects in the exenatide-naive arm received placebo TID for 35 days. At the end of this 35-day regimen, subjects in both arms received the same highest dose of exenatide (0.24 µg/kg TID) for 3 days. Thus, the exenatide-naive arm received exenatide for the first time on Day 35.

Results

The exenatide-primed arm had a lower proportion of subjects experiencing nausea and vomiting in response to exposure to the highest dose of exenatide (27 vs 56% in the exenatide-naive arm; p = 0.0018). Kaplan–Meier estimates of cumulative incidence were 0.28 in the exenatide-primed arm, compared with 0.68 in the exenatide-naive arm (p ≤ 0.001). As predicted by the study design, fewer subjects in the exenatide-primed arm reported severe nausea (29%) and vomiting (10%) than those in the exenatide-naive arm (48 and 31%, respectively). In the exenatide-primed arm, fasting serum glucose progressively declined over the first 35 days of dosing, but was unchanged in the exenatide-naive arm (placebo phase) during the same interval.

Conclusion

Gradual dose-escalation of exenatide successfully reduced the proportion of subjects experiencing dose-limiting nausea and vomiting, with no loss of glucoregulatory activity, thus demonstrating the value of gradual dose-escalation in mitigating the gastrointestinal side effects of exenatide. Copyright © 2004 John Wiley & Sons, Ltd.

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