[No authors listed]
Objective: Orexins (hypocretins) are neuropeptides expressed in hypothalamic neurons and have regulatory roles in feeding/drinking behaviours, endocrine functions and sleep/wakefulness state. Major depressive disorder (MDD) is a major mood disorder and neurotransmitter dysfunction in hypothalamic neurons may have roles in its formation. Hence, we conducted experiments to determine whether orexin receptor 1 and 2 (, ) genes were associated with MDD development. Methods: Seventy-five MDD patients and 87 healthy controls were enrolled for the study. Genotyping was carried out with real-time polymerase chain reaction (RT-PCR). Hamilton Rating-Scale for Depression (HRSD) and Beck Depression Inventory (BDI) were utilized to evaluate depressive symptom severity. Results: A significant relation was found in genotype frequencies of rs10914456 and rs2271933 variants between MDD patients and controls (pâ=â.009, pâ=â.006). Rs10914456âCC genotype increased MDD risk 3.57 times more than carrying other genotypes (pâ=â.008, OR =3.57;95% CI: 1.39-9.14). However, no association was observed in rs2653349 genotypes for MDD development (pâ>â.05). Although statistically not significant, HRSD scores were diminished in MDD subjects carrying rs10914456âCC variants when compared with CT and TT variants (pâ=â.069). Conclusion. This study suggests that, rs10914456 and rs2271933 can be associated with MDD development. Hence, rs10914456 variants may affect depressive symptom severity.
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