CLOCK is suggested to associate with comorbid alcohol use and depressive disorders

doi:10.1186/1740-3391-8-1

Journal of Circadian Rhythms

Volume 8

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Sjöholm LK
Kovanen L
Saarikoski ST
Schalling M
Lavebratt C
Partonen T

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Kovanen L
Saarikoski ST
Schalling M
Lavebratt C
Partonen T
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Research

CLOCK is suggested to associate with comorbid alcohol use and depressive disorders

Louise K Sjöholm¹ , Leena Kovanen²^,3 , Sirkku T Saarikoski³ , Martin Schalling¹ , Catharina Lavebratt¹ and Timo Partonen²

¹Department of Molecular Medicine and Surgery, Karolinska Institutet, Neurogenetics Unit CMM L8:00 Karolinska University Hospital, 171 76 Stockholm, Sweden

²Department of Mental Health and Substance Abuse Services, National Institute for Health and Welfare, PO Box 30, 00271 Helsinki, Finland

³Department of Alcohol, Drugs and Addiction, National Institute for Health and Welfare, PO Box 30, 00271 Helsinki, Finland

author email corresponding author email

Journal of Circadian Rhythms 2010, 8:1doi:10.1186/1740-3391-8-1


Published:	21 January 2010

Abstract

Background

Depression and alcohol abuse or dependence (AUD) co-occur in the general population more frequently than expected by chance. Alcohol use influences the circadian rhythms generated by the central pacemaker in the suprachiasmatic nucleus, and circadian rhythm alterations in turn are common in depressive disorders as well as among persons addicted to alcohol.

Methods

32 SNPs in 19 circadian clockwork related genes were analyzed using DNA from 76 individuals with comorbid depression and AUD, 446 individuals with AUD and 517 healthy controls with no psychiatric diagnosis. The individuals participated in a nationwide health examination study, representative of the general population aged 30 and over in Finland.

Results

The CLOCK haplotype TTGC formed by SNPs rs3805151, rs2412648, rs11240 and rs2412646, was associated with increased risk for comorbidity (OR = 1.65, 95% CI = 1.14-2.28, P = 0.0077). The SNPs of importance for this suggestive association were rs2412646 and rs11240 indicating location of the functional variation in the block downstream rs2412648. There was no indication for association between CLOCK and AUD.

Conclusion

Our findings suggest an association between the CLOCK gene and the comorbid condition of alcohol use and depressive disorders. Together with previous reports it indicates that the CLOCK variations we found here may be a vulnerability factor to depression given the exposure to alcohol in individuals having AUD.