par Köhler-Forsberg, Ole;Rietschel, Marcella;McGuffin, Peter;Aitchison, Katherine;Uher, Rudolf;Mors, Ole;Buttenschøn, Henriette Nørmølle;Tansey, Katherine K.E.;Maier, Wolfgang;Hauser, Joanna Wiktoria;Dernovsek, Mojca Zvezdana;Henigsberg, Neven;Souery, Daniel ;Farmer, Anne
Référence Brain, behavior, and immunity, 62, page (344-350)
Publication Publié, 2017-05
Référence Brain, behavior, and immunity, 62, page (344-350)
Publication Publié, 2017-05
Article révisé par les pairs
Résumé : | Introduction Population-based studies have associated inflammation, particularly higher C-reactive protein (CRP), with depressive severity, but clinical trials in major depressive disorder were rather non-specific without examining the role of gender. We aimed to investigate the association between CRP and overall depression severity including specific depressive symptoms and to examine potential gender differences. Methods We included 231 individuals with major depressive disorder from the Genome-Based Therapeutics Drugs for Depression (GENDEP) study. At baseline, we assessed high-sensitivity CRP levels and psychopathology with the Montgomery Aasberg Depression Rating Scale (MADRS). We performed linear regression analyses to investigate the association between baseline CRP levels with overall MADRS severity and specific symptoms at baseline and adjusted for age, gender, anti-inflammatory and psychotropic drug treatment, body mass index, smoking, inflammatory diseases, and recruitment center. Results Higher CRP levels were significantly associated with greater overall MADRS symptom severity (p = 0.02), which was significant among women (p = 0.02) but not among men (p = 0.68). Among women, higher CRP was associated with increased severity on observed mood, cognitive symptoms, interest-activity, and suicidality, but we found no significant associations among men. Interaction analyses showed no significant gender differences on the overall MADRS score or specific symptoms. Discussion Our results support the sickness syndrome theory suggesting that chronic low-grade inflammation may be associated with a subtype of depression. The potential gender differences in psychopathology may be explained by biological and/or psychosocial factors, e.g. differential modulation of immune responses by sex hormones. Clinical studies should investigate symptom-specific and/or gender-specific treatment guided by peripheral inflammatory markers. |