Population pharmacokinetic-pharmacodynamic modeling of subcutaneous and pulmonary insulin in rats

Mathangi Gopalakrishnan; Sandra Suarez; Anthony J Hickey; Jogarao V S Gobburu

doi:10.1007/s10928-005-0008-4

Population pharmacokinetic-pharmacodynamic modeling of subcutaneous and pulmonary insulin in rats

J Pharmacokinet Pharmacodyn. 2005 Aug;32(3-4):485-500. doi: 10.1007/s10928-005-0008-4.

Authors

Mathangi Gopalakrishnan¹, Sandra Suarez, Anthony J Hickey, Jogarao V S Gobburu

Affiliation

¹ Division of Pharmaceutical evaluation-2, Office of Clinical Pharmacology and Biopharmaceutics, Center for Drug Evaluation and Research, Food and Drug Administration, Rockville, MD 20857, USA.

PMID: 16284921
DOI: 10.1007/s10928-005-0008-4

Abstract

Purpose: To develop a population pharmacokinetic-pharmacodynamic (PKPD) model for insulin in rats.

Methods: Rats were administered insulin either subcutaneously (s.c) (0.26,1.3,2.6 U/kg) or by pulmonary route (spray-instillation (s.i)) (0.26,1.3,2.6,13,26 U/kg). Insulin (0.26,1.3,2.6 U/kg) combined with different combinations of hydroxy methyl amino propionic acid (HMAP: 5,10,16,25 mg/kg) was also administered by spray-instillation. Plasma insulin and glucose concentrations at pre-determined time points were measured. Population pharmacokinetic-pharmacodynamic modeling was performed using NONMEM.

Results: Insulin exhibited dose-disproportional PK across formulations and routes of administration. The kinetic model suggested monoexponential disposition with simultaneous first order (64%-dimeric form of insulin) - zero order (36%-hexameric form of insulin) absorption. Maximum relative bioavailability (relative to s.c - 0.26 U/kg) of spray-instilled insulin was 46%. Addition of HMAP increased the relative bioavailability of insulin administered via spray-instilled route by 40%. The insulin-glucose relationship was characterized using an indirect response model, wherein, insulin stimulation of glucose uptake into muscle cells was assumed. The basal zero order production rate of glucose (k(G, prod)) was estimated as 0.98 mg/dl/min. The SC50 was fixed at 80 mu U/ml based on literature reports and the S(max) was estimated to be 6.

Conclusions: The proposed PKPD model satisfactorily describes insulin disposition and glucose concentrations across range of doses with and without HMAP.

Publication types

Comparative Study

MeSH terms

Adjuvants, Pharmaceutic / administration & dosage
Administration, Inhalation
Alanine / administration & dosage
Alanine / analogs & derivatives
Animals
Biological Availability
Blood Glucose / analysis
Chemistry, Pharmaceutical
Hypoglycemic Agents / administration & dosage
Hypoglycemic Agents / pharmacokinetics*
Hypoglycemic Agents / pharmacology*
Injections, Subcutaneous
Insulin / administration & dosage
Insulin / pharmacokinetics*
Insulin / pharmacology*
Models, Biological*
Rats
Respiratory System / metabolism

Substances

Adjuvants, Pharmaceutic
Blood Glucose
Hypoglycemic Agents
Insulin
Alanine