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Neuropeptide Y: a promising candidate in affective disorders

Published online by Cambridge University Press:  24 June 2014

Katharina Domschke
Katharina Domschke
Affiliation:
Department of Psychiatry, University of Wuerzburg, Fuechsleinstrasse 15, D-97080 Wuerzburg, Germany
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Abstract

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Type
Editorial
Information
Acta Neuropsychiatrica , Volume 24 , Issue 2 , April 2012 , pp. 65 - 66
Copyright
Copyright © Cambridge University Press 2012

There is an increasing support for a crucial role of neuropeptides in the pathogenesis of affective disorders transcending the monoaminergic neurotransmitter systems traditionally suspected to constitute the major neurobiological pathomechanism of depression and anxiety. Particular evidence has accumulated for neuropeptide Y (NPY), one of the most abundant peptides in the human brain, to influence the pathogenesis of depression: NPY has been found to be decreased in rodent models of depression and in the cerebrospinal fluid of depressed patients. In turn, NPY administration seems to counteract depression-like behaviour in animals, and antidepressant treatment increases NPY and NPY receptor expression (Reference Wu, Feder and Wegener1). Accordingly, the human gene coding for NPY on chromosome 7p15.1 has attracted much attention in the investigation of the molecular genetic basis of affective disorders.

In this issue of Acta Neuropsychiatrica, Koefoed et al. (Reference Koefoed, Woldbye and Hansen2) report on a case–control-based association study of the NPY Leu7Pro (T20C, formerly T1128C; rs16139) polymorphism in a large Danish sample of 593 patients and 2912 controls. Authors discerned association of the Pro7 allele with depression, while no association was observed in a sample of patients with schizophrenia (n = 503) as a psychiatric disease control group. Authors additionally explored potential functional effects of the Pro7 substitution in vitro and reported evidence for Pro7 to confer reduced levels of NPY in cell cultures without affecting mRNA levels.

This study provides an additional major piece in the molecular genetic puzzle of affective disorders, strengthening the role of neuropeptides, particularly NPY in the picture. While the observed decrease in NPY levels conferred by the presently associated Pro7 allele is consistent with animal models suggesting a deficit in NPY to increase the risk of depression-related behaviour, the present results are in contrast to previous studies reporting association of the Leu7 allele with depression (Reference Heilig, Zachrisson and Thorsell3,Reference Sjöholm, Melas, Forsell and Lavebratt4). This flip-flop phenomenon of allelic association potentially due to multilocus effects and variation in interlocus correlations is a well-known occurrence in molecular genetic research in complex disorders (Reference Lin, Vance, Pericak-Vance and Martin5), not necessarily diminishing the generally confirmatory nature of the finding.

The present study by Koefoed et al. (Reference Koefoed, Woldbye and Hansen2) did not discern association with anxiety-related traits within the examined sample of patients with depression. However, there is an accumulating evidence from rodent and human studies for NPY to be involved as well as in the pathogenesis of anxiety, partly in interaction with environmental stressors (e.g. panic disorder, generalised anxiety disorder and anxious depression) (Reference Wu, Feder and Wegener1,Reference Amstadter, Koenen and Ruggiero6Reference Domschke, Hohoff and Jacob8), suggesting a potential common molecular genetic trunk for affective and anxiety disorders to be mediated, at least in part, by NPY.

Therefore, the NPY system seems to hold great promise for the investigation of the molecular genetic underpinnings of affective and anxiety disorders and thereby to have high potential for the development of innovative therapeutic mechanisms in these disorders (Reference Crespi9). Furthermore, pharmacogenetic studies of NPY gene variation in affective disorders (Reference Domschke, Dannlowski and Hohoff7) might contribute to a genotype-based personalised medicine with an individually tailored antidepressive pharmacotherapy according to genotype thus reducing the patients' suffering and lowering healthcare costs at the same time.

References

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