Shared Genetic Loci Between Schizophrenia and White Blood Cell Counts Suggest Genetically Determined Systemic Immune Abnormalities

Author:

Steen Nils Eiel12ORCID,Rahman Zillur12,Szabo Attila13,Hindley Guy F L14ORCID,Parker Nadine12,Cheng Weiqiu12ORCID,Lin Aihua1,O’Connell Kevin S12,Sheikh Mashhood A56,Shadrin Alexey12,Bahrami Shahram12,Karthikeyan Sandeep12,Hoseth Eva Z17,Dale Anders M8910,Aukrust Pål5611,Smeland Olav B12ORCID,Ueland Thor5612,Frei Oleksandr113,Djurovic Srdjan1415,Andreassen Ole A123

Affiliation:

1. NORMENT Centre, Institute of Clinical Medicine, University of Oslo , Oslo , Norway

2. Division of Mental Health and Addiction, Oslo University Hospital , Oslo , Norway

3. K.G. Jebsen Centre for Neurodevelopmental Disorders, Institute of Clinical Medicine, University of Oslo , Oslo , Norway

4. Institute of Psychiatry, Psychology and Neuroscience, King’s College London , London , UK

5. Research Institute of Internal Medicine, Oslo University Hospital , Rikshospitalet, Oslo , Norway

6. Faculty of Medicine, University of Oslo , Oslo , Norway

7. Division of Mental Health, Helse Møre Romsdal HF , Kristiansund , Norway

8. Department of Radiology, University of California, San Diego , La Jolla, CA , USA

9. Department of Cognitive Sciences, University of California, San Diego , La Jolla, CA , USA

10. Department of Neurosciences, University of California, San Diego , La Jolla, CA , USA

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

12. K.G. Jebsen—Thrombosis Research and Expertise Center (TREC), University of Tromsø , Tromsø , Norway

13. Center for Bioinformatics, Department of Informatics, University of Oslo , Oslo , Norway

14. NORMENT Centre, Department of Clinical Science, University of Bergen , Bergen , Norway

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

Abstract

Abstract Background Immune mechanisms are indicated in schizophrenia (SCZ). Recent genome-wide association studies (GWAS) have identified genetic variants associated with SCZ and immune-related phenotypes. Here, we use cutting edge statistical tools to identify shared genetic variants between SCZ and white blood cell (WBC) counts and further understand the role of the immune system in SCZ. Study Design GWAS results from SCZ (patients, n = 53 386; controls, n = 77 258) and WBC counts (n = 56 3085) were analyzed. We applied linkage disequilibrium score regression, the conditional false discovery rate method and the bivariate causal mixture model for analyses of genetic associations and overlap, and 2 sample Mendelian randomization to estimate causal effects. Study Results The polygenicity for SCZ was 7.5 times higher than for WBC count and constituted 32%–59% of WBC count genetic loci. While there was a significant but weak positive genetic correlation between SCZ and lymphocytes (rg = 0.05), the conditional false discovery rate method identified 383 shared genetic loci (53% concordant effect directions), with shared variants encompassing all investigated WBC subtypes: lymphocytes, n = 215 (56% concordant); neutrophils, n = 158 (49% concordant); monocytes, n = 146 (47% concordant); eosinophils, n = 135 (56% concordant); and basophils, n = 64 (53% concordant). A few causal effects were suggested, but consensus was lacking across different Mendelian randomization methods. Functional analyses indicated cellular functioning and regulation of translation as overlapping mechanisms. Conclusions Our results suggest that genetic factors involved in WBC counts are associated with the risk of SCZ, indicating a role of immune mechanisms in subgroups of SCZ with potential for stratification of patients for immune targeted treatment.

Funder

American National Institutes of Health

Research Council of Norway

US Norway Collaboration

European Union’s Horizon

Publisher

Oxford University Press (OUP)

Subject

Psychiatry and Mental health

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