Prescription Opioids induce Gut Dysbiosis and Exacerbate Colitis in a Murine Model of Inflammatory Bowel Disease

Author:

Sharma Umakant1,Olson Rohini Khatri2,Erhart Federico Nicolas1,Zhang Li1,Meng Jingjing1,Segura Bradley2,Banerjee Santanu1ORCID,Sharma Madhulika1,Saluja Ashok Kumar1,Ramakrishnan Sundaram1,Abreu Maria T3,Roy Sabita1

Affiliation:

1. Department of Surgery, Miller School of Medicine, University of Miami, Miami, FL, USA

2. Department of Surgery, University of Minnesota, Minneapolis, MN, USA

3. Division of Gastroenterology, Miller School of Medicine, University of Miami, Miami, FL, USA

Abstract

Abstract Background and Aims Opioids are the most prescribed analgesics for pain in inflammatory bowel diseases [IBD]; however, the consequences of opioid use on IBD severity are not well defined. This is the first study investigating consequences of hydromorphone in both dextran sodium sulphate [DSS]-induced colitis and spontaneous colitis (IL-10 knockout [IL-10-/-]) mouse models of IBD. Methods To determine the consequences of opioids on IBD pathogenesis, wild-type [WT] mice were treated with clinically relevant doses of hydromorphone and colitis was induced via 3% DSS in drinking water for 5 days. In parallel we also determined the consequences of opioids in a spontaneous colitis model. Results Hydromorphone and DSS independently induced barrier dysfunction, bacterial translocation, disruption of tight junction organisation and increased intestinal and systemic inflammation, which were exacerbated in mice receiving hydromorphone in combination with DSS. Hydromorphone + DSS-treated mice exhibited significant microbial dysbiosis. Predictive metagenomic analysis of the gut microbiota revealed high abundance in the bacterial communities associated with virulence, antibiotic resistance, toxin production, and inflammatory properties. Hydromorphone modulates tight junction organisation in a myosin light chain kinase [MLCK]-dependent manner. Treatment with MLCK inhibitor ML-7 ameliorates the detrimental effects of hydromorphone on DSS-induced colitis and thus decreases severity of IBD. Similarly, we demonstrated that hydromorphone treatment in IL-10-/- mice resulted in accelerated clinical manifestations of colitis compared with control mice. Conclusions Opioids used for pain management in IBD accelerate IBD progression by dysregulation of the gut microbiota, leading to expansion of pathogenic bacteria, translocation of bacteria, immune deregulation and sustained inflammation.

Funder

National Institute on Drug Abuse

National Institutes of Health

General Surgery Resident Research

Miami-Center for AIDS Research

Publisher

Oxford University Press (OUP)

Subject

Gastroenterology,General Medicine

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