期刊
JOURNAL OF AFFECTIVE DISORDERS
卷 225, 期 -, 页码 422-428出版社
ELSEVIER
DOI: 10.1016/j.jad.2017.08.066
关键词
FKBP5; Systematic review; Gene-environment interaction; Meta-analysis; Risk alleles
资金
- National Institute of Mental Health [R01MH082802, R21MH081099, 1R01MH101890, R01MH100616, 1R01MH107183-01]
- American Foundation for Suicide Prevention [SRG-1-042-14]
- NATIONAL INSTITUTE OF MENTAL HEALTH [R01MH107183, R01MH101890, R01MH082802, R21MH081099, R01MH100616] Funding Source: NIH RePORTER
Background: Gene-environment interaction contributes to the risks of psychiatric disorders. Interactions between FKBP5 gene variants and early-life stress may enhance the risk not only for mood disorder, but also for a number of other behavioral phenotypes. The aim of the present study was to review and conduct a meta-analysis on the results from published studies examining interaction between FKBP5 gene variants and early-life stress and their associations with stress-related disorders such as major depression and PTSD. Methods: A literature search was conducted using PsychINFO and PubMed databases until May 2017. A total of 14 studies with a pooled total of 15109 participants met the inclusion criteria, the results of which were combined and a meta-analysis was performed using the differences in correlations as the effect measure. Based on literature, rs1360780, rs3800373, and rs9470080 SNPs were selected within the FKBP5 gene and systematic review was conducted. Results: Based on the Comprehensive Meta-Analysis software, no publication bias was detected. Sensitivity analysis and credibility of meta-analysis results also indicated that the analyses were stable. The meta-analysis showed that individuals who carry T allele of rs1360780, C-allele of rs3800373 or T-allele of rs9470080 exposed to early-life trauma had higher risks for depression or PTSD. Limitations: The effects of ethnicity, age, sex, and different stress measures were not examined due to limited sample size. Conclusions: These results provide strong evidence of interactions between FKBP5 genotypes and early-life stress, which could pose a significant risk factor for stress-associated disorders such as major depression and PTSD.
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