Search CORE

1 research outputs found

Development of Budesonide Microparticles Using Spray-Drying Technology for Pulmonary Administration: Design, Characterization, In Vitro Evaluation, and In Vivo Efficacy Study

Author: A Baxter
A Tronde
AB Schnurch
AH Jansson
AHD Boer
AJ Ribeiro
AK Greenberg
AK Kamada
AM Larsson
Amrita N. Bajaj
BMG Wilson
BS Kang
C Monn
CL Leach
DJ Ball
DO Corrigan
DO Corrigan
E Bondesson
E Bondesson
F Ungaro
FM Spoelstra
GR Pitcairn
GR Pitcairn
GS Zijlstra
H Kaiser
H Larhrib
I Basyigit
I Uings
IJ Smith
IM Smirnov
J Fu
JH Toogood
JR Henry
K Deventer
K Koushik
K Kronkvist
KA Johnson
KB Prinn
KI Brink van den
L Thorsson
LA Sorbera
M Baek
M Cazzola
M Irngartinger
M Jendbro
M Joshi
M Skiba
MA Faouzi
Madhumanjiri M. Gatne
MB Chougule
MJ Myers
ML Landry
ML Sommerville
N Amrutiya
PH Hirst
PN Yadav
Prashant Gurav
Pritam Singh Soni
PWS Heng
R Donnelly
R Gandhi
R Wakode
RN Jashnani
RO Cook
S Edsbacker
S Escotte
S Lewis
SJ Szefler
SK Jain
Sonali R. Naikwade
SP Newman
SP Shah
SR Naikwade
SR Naikwade
SR Naikwade
SR Naikwade
T Cerchiara
T Kouno
T Miyamoto
T Sebti
TF Leung
TP Learoyd
TV Vyve
UB Kompella
V Sanna
W Busse
XM Zeng
Y Fujitani
YC Huang
Z Lee
Z Yu
Publication venue: Springer US
Publication date
Field of study

The purpose of this research was to generate, characterize, and investigate the in vivo efficacy of budesonide (BUD) microparticles prepared by spray-drying technology with a potential application as carriers for pulmonary administration with sustained-release profile and improved respirable fraction. Microspheres and porous particles of chitosan (drug/chitosan, 1:2) were prepared by spray drying using optimized process parameters and were characterized for different physicochemical parameters. Mass median aerodynamic diameter and geometric standard deviation for conventional, microspheres, and porous particles formulations were 2.75, 4.60, and 4.30 µm and 2.56, 1.75, and 2.54, respectively. Pharmacokinetic study was performed in rats by intratracheal administration of either placebo or developed dry powder inhalation (DPI) formulation. Pharmacokinetic parameters were calculated (Ka, Ke, Tmax, Cmax, AUC, and Vd) and these results indicated that developed formulations extended half life compared to conventional formulation with onefold to fourfold improved local and systemic bioavailability. Estimates of relative bioavailability suggested that developed formulations have excellent lung deposition characteristics with extended T1/2 from 9.4 to 14 h compared to conventional formulation. Anti-inflammatory activity of BUD and developed formulations was compared and found to be similar. Cytotoxicity was determined in A549 alveolar epithelial cell line and found to be not toxic. In vivo pulmonary deposition of developed conventional formulation was studied using gamma scintigraphy and results indicated potential in vitro–in vivo correlation in performance of conventional BUD DPI formulation. From the DPI formulation prepared with porous particles, the concentration of BUD increased fourfold in the lungs, indicating pulmonary targeting potential of developed formulations

Crossref

PubMed Central