Self-emulsifying drug delivery systems (SEDDS) disrupt the gut microbiota and trigger an intestinal inflammatory response in rats

Santhni Subramaniam; Aurelia Elz; Anthony Wignall; Srinivas Kamath; Amin Ariaee; Alexander Hunter; Tahlia Newblack; Hannah R Wardill; Clive A Prestidge; Paul Joyce

doi:10.1016/j.ijpharm.2023.123614

Self-emulsifying drug delivery systems (SEDDS) disrupt the gut microbiota and trigger an intestinal inflammatory response in rats

Int J Pharm. 2023 Dec 15:648:123614. doi: 10.1016/j.ijpharm.2023.123614. Epub 2023 Nov 17.

Affiliations

¹ Centre for Pharmaceutical Innovation (CPI), UniSA Clinical & Health Sciences, University of South Australia, South Australia, Australia.
² Supportive Oncology Research Group, Precision Cancer Medicine (Theme), South Australian Health and Medical Research Institute (SAHMRI), University of Adelaide, South Australia, Australia.
³ Centre for Pharmaceutical Innovation (CPI), UniSA Clinical & Health Sciences, University of South Australia, South Australia, Australia. Electronic address: paul.joyce@unisa.edu.au.

PMID: 37979632
DOI: 10.1016/j.ijpharm.2023.123614

Abstract

Self-emulsifying drug delivery systems (i.e. SEDDS, SMEDDS and SNEDDS) are widely employed as solubility and bioavailability enhancing formulation strategies for poorly water-soluble drugs. Despite the capacity for SEDDS to effectively facilitate oral drug absorption, tolerability concerns exist due to the capacity for high concentrations of surfactants (typically present within SEDDS) to induce gastrointestinal toxicity and mucosal irritation. With new knowledge surrounding the role of the gut microbiota in modulating intestinal inflammation and mucosal injury, there is a clear need to determine the impact of SEDDS on the gut microbiota. The current study is the first of its kind to demonstrate the detrimental impact of SEDDS on the gut microbiota of Sprague-Dawley rats, following daily oral administration (100 mg/kg) for 21 days. SEDDS comprising a lipid phase (i.e. Type I, II and III formulations according to the Lipid Formulation Classification Scheme) induced significant changes to the composition and diversity of the gut microbiota, evidenced through a reduction in operational taxonomic units (OTUs) and alpha diversity (Shannon's index), along with statistically significant shifts in beta diversity (according to PERMANOVA of multi-dimensional Bray-Curtis plots). Key signatures of gut microbiota dysbiosis correlated with the increased expression of pro-inflammatory cytokines within the jejunum, while mucosal injury was characterised by significant reductions in plasma citrulline levels, a validated biomarker of enterocyte mass and mucosal barrier integrity. These findings have potential clinical ramifications for chronically administered drugs that are formulated with SEDDS and stresses the need for further studies that investigate dose-dependent effects of SEDDS on the gastrointestinal microenvironment in a clinical setting.

Keywords: Dysbiosis; Emulsifiers; Gut microbiome; LBDDS; Lipid-based drug delivery systems; Lipid-based formulations; Oral drug delivery; SMEDDS; SNEDDS; Self-microemulsifying drug delivery systems; Self-nanoemulsifying drug delivery systems.

MeSH terms

Administration, Oral
Animals
Biological Availability
Chemistry, Pharmaceutical / methods
Drug Delivery Systems / methods
Emulsions
Gastrointestinal Microbiome*
Lipids
Pharmaceutical Preparations
Rats
Rats, Sprague-Dawley
Solubility

Substances

Pharmaceutical Preparations
Lipids
Emulsions