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. 2025 Aug:350:116557.
doi: 10.1016/j.psychres.2025.116557. Epub 2025 May 20.

Pro-inflammatory processes and metabolic syndrome: combined risk of resistance to treatment in patients with schizophrenia from the FACE-SZ cohort

Kaori Saitoh  1 Mohamed Lajnef  2 Wahid Boukouaci  2 Myrtille Andre  3 Christelle Andrieu  4 Bruno Aouizerate  5 Caroline Barau  6 Jihène Bouassida  2 Delphine Capdevielle  3 Isabelle Chereau  7 Julie Clauss-Kobayashi  8 Nathalie Coulon  9 Jean-Michel Dorey  10 Caroline Dubertret  11 Eric Fakra  12 Guillaume Fond  4 Tudi Goze  13 Philippe Le Corvoisier  6 Sylvain Leignier  9 Pierre-Michel Llorca  7 Jasmina Mallet  11 David Misdrahi  14 Nicolas Oriol  12 Baptiste Pignon  15 Romain Rey  10 Paul Roux  16 Franck Schürhoff  15 Benoit Schorr  8 Mathieu Urbach  16 Etienne Very  13 Ching-Lien Wu  2 FACE-SZ (FondaMental Academic Centers of Expertise for Schizophrenia) collaboratorsMarion Leboyer  15 Ophélia Godin  2 Ryad Tamouza  15
Affiliations

Pro-inflammatory processes and metabolic syndrome: combined risk of resistance to treatment in patients with schizophrenia from the FACE-SZ cohort

Kaori Saitoh et al. Psychiatry Res. 2025 Aug.

Abstract

Schizophrenia (SZ) is characterized by a variable clinical expression and course peppered/hampered by severe complications. In particular, resistance to treatment (overall-TRS, treatment resistant SZ including UTRS, ultra-TRS) and metabolic syndrome (MetS) are highly prevalent, and both demonstrated to be underpinned, at least partly, by pro-inflammatory processes. Given that such processes also underlie SZ per se, we hypothesized that potential inter-twinning between SZ- and MetS-related inflammatory processes may exert a combined effect on the risk of having overall-TRS/UTRS. A total of 419 outpatients with SZ underwent clinical assessments and blood sample collection. Using the values of circulating levels of eleven cytokines, we built a ratio between pro- and anti-inflammatory components respectively corresponding to the immunoinflammatory response system (IRS) and the compensatory immunoregulatory reflex system (CIRS) which overall reflect the underlying inflammatory status. Such ratios allowed to categorize the patients according to Inflammation and MetS on four categories as follow: Inflammation(+)MetS(+), Inflammation(+)MetS(-), Inflammation(-)MetS(+) and Inflammation(-)MetS(-). Multivariate logistic regression analysis showed that the combination of inflammation and MetS modulate the risk of having the overall-TRS [Inflammation(+)MetS(-): OR=2.28, 95 %CI [1.04-5.00], p = 0.039 and Inflammation(+)MetS(+): OR=4.59, 95 % CI [1.76-11.97], p = 0.002 overall in comparison to Inflammation(-)MetS(-)]. Moreover, we observed that individuals with UTRS are those associated with both inflammation and/or MetS. Our results demonstrated the potential combined effect of MetS and inflammation towards resistance to treatment. Given that overall-TRS/UTRS are unpredictable while both inflammation and MetS can be early detected and managed, our findings shed new light on the possibility to better prevent treatment resistance in SZ.

Keywords: Cytokine; Inflammation; Metabolic syndrome; Resistance to treatment; Schizophrenia.

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Conflict of interest statement

Declaration of competing interest The authors declare no competing interests.

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