Repository logo
 
Thumbnail Image
Publication

A novel semi-solid pill for stress-free voluntary oral drug administration in experimental rodents

2019-06-02Other Open access
http://hdl.handle.net/10400.26/32296
Use this identifier to reference this record.
Name:Description:Size:Format: 
Abstract PB 37.pdf46.55 KBAdobe PDF Download

Authors

Martins, B.
Nunes, S.
Palavra, F.
Preguiça, I.
Alves, A.
Nóbrega, C.
Fernandes, R.
Silva, S.

Advisor(s)

Abstract(s)

During compound screening and drug development, long-term oral drug administration to experimental rodents is often required. Oral gavage, a straightforward drug dosing technique, is not suitable for extended treatments considering the recurrent traumatic complications (gastroesophageal injury) and physiological distress (corticosterone levels alterations) that frequently bias experimental design outcomes. These reasons create a challenge for preclinical drug assays and stress-free/metabolic-inert alternatives of oral drug administration are warranted. Herein, it is presented an innovative semi-solid pill optimized to overcome aforementioned drawbacks. After a brief training period, C57BL/6 mice submitted to a chronic oral administration protocol (50 days) displayed a high index of voluntary acceptance of emptyand drug- (e.g. sitagliptin) incorporated vehicle in both healthy and CNS-diseased states. This protocol operates in a pair-housed animal housing fashion, allowing animal socialization throughout entire protocol. At the end of experiments, a normal neurobehavioral phenotype (anxiolytic, memory, locomotion parameters) was recorded. Moreover, this new methodology proved to be safe, preserving serum metabolic (glucose, triglycerides, total cholesterol), hepatic (albumin, total proteins) and renal (urea, creatinine, uric acid) parameters along with normal ileum contractility. Remarkably, coherent sitagliptin ( 10 mg/ml) plasma levels were detected, along with a robust decrease ( 80%) on the activity of its target (dipeptidyl peptidase- 4), unequivocally proving in vivo drug efficacy. Overall, this innovative approach may enclose a breakthrough advance for translational studies in scientific and pharmaceutical fields, providing a reproducible, efficient, metabolic inert and stress-free alternative for voluntary oral drug administration, with expected improvement on the data feasibility.

Description

Keywords

pre-clinical voluntary oral drug administration

URI

http://hdl.handle.net/10400.26/32296

Citation

A novel semi-solid pill for stress-free voluntary oral drug administration in experimental rodents

Research Projects

Organizational Units

Journal Issue

Publisher

SAGE Publishing Ltd

DOI

DOI: 10.1177/0023677219839199

Collections

IPC-ESTeSC - Comunicações em conferências e congressos

CC License

cclicense-by-nc-sa

Altmetrics