Elevated Systemic Levels of Markers Reflecting Intestinal Barrier Dysfunction and Inflammasome Activation Are Correlated in Severe Mental Illness

Author:

Jensen Søren B1,Sheikh Mashhood A1,Akkouh Ibrahim A23,Szabo Attila234,O’Connell Kevin S2,Lekva Tove1,Engh John A25,Agartz Ingrid4678,Elvsåshagen Torbjørn2,Ormerod Monica B E G28,Weibell Melissa A910,Johnsen Erik111213,Kroken Rune A111213,Melle Ingrid28,Drange Ole K141516,Nærland Terje417,Vaaler Arne E1415,Westlye Lars T2418,Aukrust Pål11920,Djurovic Srdjan23418,Eiel Steen Nils28,Andreassen Ole A248,Ueland Thor12021

Affiliation:

1. Research Institute of Internal Medicine, Oslo University Hospital , Oslo , Norway

2. Division of Mental Health and Addiction, Norwegian Centre for Mental Disorders Research, NORMENT, Oslo University Hospital , Oslo , Norway

3. Department of Medical Genetics, Oslo University Hospital , Oslo , Norway

4. K.G. Jebsen Center for Neurodevelopmental disorders, Institute of Clinical Medicine, University of Oslo , Oslo , Norway

5. Division of Mental health and Addiction, Vestfold Hospital Trust , Tønsberg , Norway

6. Department of Clinical Neuroscience, Centre for Psychiatry Research, Karolinska Institutet and Stockholm Health Care Services, Stockholm County Council , Stockholm , Sweden

7. Department of Psychiatric Research, Diakonhjemmet Hospital , Oslo , Norway

8. Norwegian Centre for Mental Disorders Research, NORMENT, Institute of Clinical Medicine, University of Oslo , Oslo , Norway

9. Division of Psychiatry, Network for Clinical Psychosis Research, Stavanger University Hospital , Stavanger , Norway

10. Network for Medical Sciences, Faculty of Health, University of Stavanger , Stavanger , Norway

11. Division of Psychiatry, Haukeland University Hospital , Bergen , Norway

12. Department of Clinical Medicine, University of Bergen , Bergen , Norway

13. NORMENT Center of Excellence, University of Bergen and Haukeland University Hospital , Bergen , Norway

14. Department of Mental Health, Norwegian University of Science and Technology , Trondheim , Norway

15. Department of Østmarka, Division of Mental Health, St. Olavs University Hospital , Trondheim , Norway

16. Department of Psychiatry, Sørlandet Hospital , Kristiansand , Norway

17. Department of Rare Disorders, Division of Child and Adolescent medicine, Oslo University Hospital , Oslo , Norway

18. Department of Psychology, University of Oslo , Oslo , Norway

19. Section of Clinical Immunology and Infectious Diseases, Oslo University Hospital Rikshospitalet , Oslo , Norway

20. Institute of Clinical Medicine, University of Oslo , Oslo , Norway

21. K.G. Jebsen Thrombosis Research and Expertise Center, University of Tromsø , Tromsø , Norway

Abstract

Abstract Background and Hypothesis Gut microbiota alterations have been reported in severe mental illness (SMI) but fewer studies have probed for signs of gut barrier disruption and inflammation. We hypothesized that gut leakage of microbial products due to intestinal inflammation could contribute to systemic inflammasome activation in SMI. Study Design We measured plasma levels of the chemokine CCL25 and soluble mucosal vascular addressin cell adhesion molecule-1 (sMAdCAM-1) as markers of T cell homing, adhesion and inflammation in the gut, lipopolysaccharide binding protein (LBP) and intestinal fatty acid binding protein (I-FABP) as markers of bacterial translocation and gut barrier dysfunction, in a large SMI cohort (n = 567) including schizophrenia (SCZ, n = 389) and affective disorder (AFF, n = 178), relative to healthy controls (HC, n = 418). We assessed associations with plasma IL-18 and IL-18BPa and leukocyte mRNA expression of NLRP3 and NLRC4 as markers of inflammasome activation. Study Results Our main findings were: (1) higher levels of sMAdCAM-1 (P = .002), I-FABP (P = 7.6E−11), CCL25 (P = 9.6E−05) and LBP (P = 2.6E−04) in SMI compared to HC in age, sex, BMI, CRP and freezer storage time adjusted analysis; (2) the highest levels of sMAdCAM-1 and CCL25 (both P = 2.6E−04) were observed in SCZ and I-FABP (P = 2.5E−10) and LBP (3) in AFF; and (3), I-FABP correlated with IL-18BPa levels and LBP correlated with NLRC4. Conclusions Our findings support that intestinal barrier inflammation and dysfunction in SMI could contribute to systemic inflammation through inflammasome activation.

Funder

South East Norway Health Authority

Publisher

Oxford University Press (OUP)

Subject

Psychiatry and Mental health

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