The colon targeting efficacies of mesalazine medications and their impacts on the gut microbiome

Laura E McCoubrey; Nidhi Seegobin; Nannapat Sangfuang; Frédéric Moens; Hans Duyvejonck; Eline Declerck; Arno Dierick; Massimo Marzorati; Abdul W Basit

doi:10.1016/j.jconrel.2024.04.016

The colon targeting efficacies of mesalazine medications and their impacts on the gut microbiome

J Control Release. 2024 Apr 11:369:630-641. doi: 10.1016/j.jconrel.2024.04.016. Online ahead of print.

Authors

Laura E McCoubrey¹, Nidhi Seegobin¹, Nannapat Sangfuang¹, Frédéric Moens², Hans Duyvejonck², Eline Declerck², Arno Dierick², Massimo Marzorati³, Abdul W Basit⁴

Affiliations

¹ UCL School of Pharmacy, 29-39 Brunswick Square, London WC1N 1AX, UK.
² ProDigest BV, Technologiepark-Zwijnaarde 82, 9052 Ghent, Belgium.
³ ProDigest BV, Technologiepark-Zwijnaarde 82, 9052 Ghent, Belgium; CMET (University of Ghent), Coupure Links 653, 9000 Ghent, Belgium.
⁴ UCL School of Pharmacy, 29-39 Brunswick Square, London WC1N 1AX, UK. Electronic address: a.basit@ucl.ac.uk.

PMID: 38599548
DOI: 10.1016/j.jconrel.2024.04.016

Abstract

Successful treatment of ulcerative colitis (UC) is highly dependent on several parameters, including dosing regimen and the ability to deliver drugs to the disease site. In this study two strategies for delivering mesalazine (5-aminosalicylic acid, 5-ASA) to the colon were compared in an advanced in vitro model of the human gastrointestinal (GI) tract, the SHIME® system. Herein, a prodrug strategy employing bacteria-mediated drug release (sulfasalazine, Azulfidine®) was evaluated alongside a formulation strategy that utilised pH and bacteria-mediated release (5-ASA, Octasa® 1600 mg). SHIME® experiments were performed simulating both the GI physiology and colonic microbiota under healthy and inflammatory bowel disease (IBD) conditions, to study the impact of the disease state and ileal pH variability on colonic 5-ASA delivery. In addition, the effects of the products on the colonic microbiome were investigated by monitoring bacterial growth and metabolites. Results demonstrated that both the prodrug and formulation approaches resulted in a similar percentage of 5-ASA recovery under healthy conditions. On the contrary, during experiments simulating the GI physiology and microbiome of IBD patients (the target population) the formulation strategy resulted in a higher proportion of 5-ASA delivery to the colonic region as compared to the prodrug approach (P < 0.0001). Interestingly, the two products had distinct effects on the synthesis of key bacterial metabolites, such as lactate and short chain fatty acids, which varied according to disease state and ileal pH variability. Further, both 5-ASA and sulfasalazine significantly reduced the growth of the faecal microbiota sourced from six healthy humans. The findings support that the approach selected for colonic drug delivery could significantly influence the effectiveness of UC treatment, and highlight that drugs licensed for UC may differentially impact the growth and functioning of the colonic microbiota.

Keywords: Asacol 1600; Colonic drug delivery; Gastro resistant enteric film coatings; Mesalamine; Microbiome; Phloral and opticore technologies; Targeting the large intestine.