Levodopa-carbidopa Intestinal Gel High Concentration Formulation is Clinically Bioequivalent to Commercial Formulation

Overview

Journal Pharmacol Res Perspect

Date 2019 Apr 13

PMID 30977301

Citations 3

Authors

Matthew Rosebraugh

Hari V Kalluri

Wei Liu

Charles Locke

Dilraj Sidhu

Jian-Hwa Han

Janet Benesh

Affiliations

Soon will be listed here.

Abstract

A new levodopa-carbidopa intestinal gel (LCIG) system featuring a higher levodopa/carbidopa (LD/CD) concentration and viscosity, LCIG-HV, is being developed to reduce the intrajejunal volume of LD/CD that is administered as compared to the current commercial formulation, LCIG-LV. This study characterizes the LCIG-HV formulation and compares it to the LCIG-LV formulation via dissolution testing and a clinical pharmacokinetic bioequivalence study. In vitro release profiles of LD/CD were determined using a USP Dissolution Apparatus 2 with 500 mL of phosphate buffer (pH 4.5) operating at 25 RPM. A single dose, open-label study was conducted according to a two-period, randomized, crossover design in 28 healthy subjects. The point estimate (PE) of the levodopa C geometric mean for the LCIG-HV formulation was 4% higher than that of the LCIG-LV formulation. PEs of levodopa AUC and AUC geometric means were comparable for both formulations. PEs of carbidopa C , AUC and AUC geometric means for the LCIG-HV formulation were 3%-5% higher than those of the LCIG-LV formulation. For both formulations, the median T for levodopa was 1.0 and 3.0 hours for carbidopa. The levodopa half-life harmonic mean was 1.6 hour for both formulations. The carbidopa half-life harmonic mean was 1.9 and 2.0 hour, respectively, for the LCIG-HV and LCIG-LV formulations. C , AUC and AUC of LD/CD carbidopa were comparable for both formulations. The current study demonstrates that the LCIG-LV and LCIG-HV formulations are clinically bioequivalent for LD/CD according to FDA guidance. However, the dissolution method was over discriminatory of formulation differences.

Citing Articles

Pharmaceutical and pharmacokinetic evaluation of a newly formulated multiparticulate matrix of levodopa and carbidopa.

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PMID: 36778908 PMC: 9909728. DOI: 10.5599/admet.1474.

Effects of Levodopa-Carbidopa Intestinal Gel Compared with Optimized Medical Treatment on Nonmotor Symptoms in Advanced Parkinson's Disease: INSIGHTS Study.

Chung S, Calopa M, Ceravolo M, Tambasco N, Antonini A, Chaudhuri K Parkinsons Dis. 2022; 2022:1216975.

PMID: 36388237 PMC: 9652073. DOI: 10.1155/2022/1216975.

Levodopa-carbidopa intestinal gel high concentration formulation is clinically bioequivalent to commercial formulation.

Rosebraugh M, Kalluri H, Liu W, Locke C, Sidhu D, Han J Pharmacol Res Perspect. 2019; 7(2):e00473.

PMID: 30977301 PMC: 6452870. DOI: 10.1002/prp2.473.

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