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Functional and Internalizing Disorders Co-Aggregate with Cardiometabolic and Immune-Related Diseases Within Families: A Population-Based Cohort Study

Background: Functional disorders share familial risk with internalizing disorders and are comorbid with cardiometabolic and immune-related diseases. We investigated whether functional and internalizing disorders co-aggregate with these diseases in families, to gain insight into the aetiology of functional and internalizing disorders.  
Methods: We included 166,774 subjects (aged 3-94), from the population-based  Lifelines Cohort Study, a Dutch general population cohort. We defined cases for three functional disorders (myalgic encephalomyelitis/chronic fatigue syndrome; ME/CFS, fibromyalgia, and irritable bowel syndrome; IBS), two internalizing disorders (major depressive disorder; MDD and generalized anxiety disorder; GAD), cardiometabolic diseases (obesity, metabolic associated steatotic liver disease, type 2 diabetes, hypertension and cardiovascular disease) and immune-related diseases (composite measures of auto-immune disease and atopy). We used logistic regression to model the prevalence of these disorders in the general population and in participants with affected relatives. Using these prevalence estimates we assessed familial co-aggregation with 1) recurrence risk ratios (λR), and 2) familial correlations (rf).  
Results: All functional and internalizing disorders co-aggregated with immune-related diseases (λR range 1.06-1.24). ME/CFS, FM and MDD co-aggregated with most cardiometabolic diseases (λR range 1.00-1.23). MDD, fibromyalgia, and ME/CFS showed similar familial correlation patterns with both disease groups (rf range 0.12-0.44), while patterns of IBS and GAD were more variable.
Conclusion: Internalizing and functional disorders share familial risk with immune-related and cardiometabolic diseases. This suggests that risk factors relevant to immune-related and cardiometabolic diseases may also be relevant for FDs. Future studies should investigate such risk factors to identify novel treatment targets. 

Keywords: fibromyalgia, myalgic encephalomyelitis/chronic fatigue syndrome, irritable bowel syndrome, aetiology, familial co-aggregation, cardiometabolic, atopy, autoimmune

Year of publication

2025

Journal

BMC medicine

Author(s)

Steen, O.D.
Bos, M.
van Ockenburg, S.L.
Zhou, Y.
Nolte, I.M.
Snieder, H.
et. al.

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