Pharmacokinetics and pharmacodynamics of insulin lispro protamine suspension compared with insulin glargine and insulin detemir in type 2 diabetes

Marcus Hompesch; Scott M Ocheltree; Eshetu T Wondmagegnehu; Linda A Morrow; Alexa P Kollmeier; Barbara N Campaigne; Scott J Jacober

doi:10.1185/03007990903223739

Pharmacokinetics and pharmacodynamics of insulin lispro protamine suspension compared with insulin glargine and insulin detemir in type 2 diabetes

Curr Med Res Opin. 2009 Nov;25(11):2679-87. doi: 10.1185/03007990903223739.

Authors

Marcus Hompesch¹, Scott M Ocheltree, Eshetu T Wondmagegnehu, Linda A Morrow, Alexa P Kollmeier, Barbara N Campaigne, Scott J Jacober

Affiliation

¹ Profil Institute for Clinical Research, Inc., San Diego, CA, USA.

PMID: 19761358
DOI: 10.1185/03007990903223739

Abstract

Objective: The primary aim was to evaluate duration of action of a single 0.8 U/kg dose of insulin lispro protamine suspension (ILPS) in type 2 diabetes (T2DM) patients; secondarily to compare onset and duration of action of ILPS, glargine (G), and detemir (D) (0.8 U/kg) and evaluate pharmacokinetic (PK) and pharmacodynamic (PD) dose responses of ILPS.

Research design and methods: In a single-center, double-blind, five-arm crossover study, 34 patients were randomized to a treatment sequence which included a single subcutaneous 0.8 U/kg dose of G and D and three doses of ILPS (0.4 U/kg, 0.8 U/kg, and 1.2 U/kg) and were studied using 24-hour euglycemic glucose clamps.

Primary outcome measure: Duration of action was determined as the time to the last measurable glucose infusion rate (tR(last)) during glucose clamps.

Results: The duration of insulin action (tR(last)) for ILPS at 0.8 U/kg was >23 hours and was similar to G (p = 0.114) and D (p = 0.570). Post-hoc analysis demonstrated the probability of achieving 24 hours of glucose-lowering activity after a 0.8 U/kg dose: 48% (ILPS), 43% (G), and 26% (D). G(tot) and R(max) were significantly greater for ILPS versus G or D. The median ILPS time-dependent values demonstrated a significantly earlier maximum PD response (tR(max) and early 50% tR(max)) versus either G or D. ILPS demonstrated dose-dependent increases in PK and PD measures across the dose range.

Conclusions: Following a single 0.8 U/kg dose in T2DM patients, ILPS, G, and D demonstrated similar durations of glucose-lowering activity and ILPS demonstrated significantly greater glucose-lowering activity (R(max) and G(tot)) and earlier maximum PD response. These results potentially support once-daily dosing of ILPS in T2DM.

Limitations: The observed number of 24-hour censored observations was higher than expected and the wash-out period for basal insulin treated patients may have been too short to definitively rule out a carry-over effect; however, such an effect, if present, would potentially only affect onset of action and not the primary outcome measure.

Publication types

Randomized Controlled Trial
Research Support, Non-U.S. Gov't

MeSH terms

Adult
Aged
Cross-Over Studies
Diabetes Mellitus, Type 2 / drug therapy
Diabetes Mellitus, Type 2 / metabolism*
Dose-Response Relationship, Drug
Double-Blind Method
Female
Humans
Hypoglycemic Agents / pharmacokinetics
Hypoglycemic Agents / therapeutic use
Insulin / adverse effects
Insulin / analogs & derivatives*
Insulin / pharmacokinetics
Insulin / therapeutic use
Insulin Detemir
Insulin Glargine
Insulin Lispro
Insulin, Long-Acting
Male
Middle Aged
Protamines / adverse effects
Protamines / pharmacokinetics
Protamines / therapeutic use
Suspensions

Substances

Hypoglycemic Agents
Insulin
Insulin Lispro
Insulin, Long-Acting
Protamines
Suspensions
Insulin Glargine
Insulin Detemir