4.7 Article

Basal and LPS-stimulated inflammatory markers and the course of anxiety symptoms

期刊

BRAIN BEHAVIOR AND IMMUNITY
卷 98, 期 -, 页码 378-387

出版社

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.bbi.2021.09.001

关键词

Anxiety severity; Anxiety severity Anxiety disorder; Epidemiology; Inflammation; Longitudinal

资金

  1. Geestkracht program of the Netherlands Organisation for Health Research and Development (ZonMw) [10-000-1002]
  2. Amsterdam University Medical Centers (location VUmc)
  3. GGZ inGeest
  4. Leiden University Medical Center
  5. Leiden University
  6. GGZ Rivierduinen
  7. University Medical Center Groningen
  8. University of Groningen
  9. Lentis
  10. GGZ Friesland
  11. GGZ Drenthe
  12. Rob Giel Onderzoekscentrum

向作者/读者索取更多资源

The study found that high levels of inflammatory markers were significantly associated with anxiety symptoms, particularly with physical arousal and agoraphobia, which persisted over a nine-year period, albeit with small effect sizes, and partly driven by co-morbid depression.
A cross-sectional relationship between low-grade inflammation -characterized by increased blood levels of Creactive protein (CRP) and pro-inflammatory cytokines- and anxiety has been reported, but the potential longitudinal relationship has been less well studied. We aimed to examine whether basal and lipopolysaccharide (LPS-)induced levels of inflammatory markers are associated with anxiety symptom severity over the course of nine years. We tested the association between basal and LPS-induced inflammatory markers with anxiety symptoms (measured with the Beck's Anxiety Inventory; BAI, Fear Questionnaire; FQ and Penn's State Worry Questionnaire; PSWQ) at 5 assessment waves over a period up nine years. We used multivariate-adjusted mixed models in up to 2867 participants of the Netherlands Study of Depression and Anxiety (NESDA). At baseline, 43.6% of the participants had a current anxiety disorder, of which social phobia (18.5%) was most prevalent. Our results demonstrated that baseline inflammatory markers were significantly associated with several outcomes of anxiety at baseline over nine subsequent years. BAI subscale of somatic (arousal) symptoms of anxiety, and FQ subscale of agoraphobia demonstrated the strongest effects with standardized betacoefficients of up to 0.14. The associations were attenuated by 25%-30% after adjusting for the presence of (comorbid) major depressive disorder (MDD), but remained statistically significant. In conclusion, we found that participants with high levels of inflammatory markers have on average high levels of anxiety consisting of physical arousal and agoraphobia, which tended to persist over a period of nine years, albeit with small effect sizes. These associations were partly driven by co-morbid depression.

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