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5-羟色胺转运体多态性(SLC6A4 插入/缺失和 rs25531)不会影响 5-HTT 在活体人脑内与[11C]DASB 结合的可用性。

Serotonin transporter polymorphisms (SLC6A4 insertion/deletion and rs25531) do not affect the availability of 5-HTT to [11C] DASB binding in the living human brain.

机构信息

Medical Research Council Clinical Sciences Centre, Hammersmith Hospital, London, UK.

出版信息

Neuroimage. 2010 Aug 1;52(1):50-4. doi: 10.1016/j.neuroimage.2010.04.032. Epub 2010 Apr 18.

DOI:10.1016/j.neuroimage.2010.04.032
PMID:20406689
Abstract

Studies in vitro suggest that the expression of the serotonin transporter (5-HTT) is regulated by polymorphic variation in the promoter region of the 5-HTT gene (5-HTTLPR); however, results from human brain imaging studies examining the relation between 5-HTT genotype and 5-HTT radioligand binding in vivo have been inconsistent. This inconsistency could reflect small participant numbers or the use of sub-optimal radiotracer for measuring the 5-HTT. We used positron emission tomography in conjunction with the selective 5-HTT ligand [(11)C] DASB to examine the availability of the 5-HTT in seven brain regions in 63 healthy European caucasian volunteers who were genotyped for short (S) and long (L) variants (SLC6A4 and rs25531) of the 5-HTTLPR. [(11)C] DASB binding potential was not influenced by the allelic status of participants whether classified on a biallelic or triallelic basis in any of the regions studied. Our PET findings, in a relatively large sample with a near optimal radiotracer, suggest that 5-HTTLPR polymorphic variation does not affect the availability of 5-HTT to [(11)C] DASB binding in adult human brain. The reported impact of 5-HTTLPR polymorphic variation on emotional processing and vulnerability to depression are more likely therefore to be expressed through effects exerted during neurodevelopment.

摘要

体外研究表明,5-羟色胺转运体(5-HTT)的表达受 5-HTT 基因(5-HTTLPR)启动子区域多态性变异的调节;然而,检查 5-HTT 基因型与 5-HTT 放射性配体结合物在体内的关系的人类大脑成像研究结果并不一致。这种不一致可能反映了参与者数量较少或用于测量 5-HTT 的放射性示踪剂不够理想。我们使用正电子发射断层扫描结合选择性 5-HTT 配体 [11C] DASB,检查了 63 名健康欧洲白种人志愿者的 7 个大脑区域中 5-HTT 的可用性,这些志愿者根据 5-HTTLPR 的短(S)和长(L)变体(SLC6A4 和 rs25531)进行了基因分型。无论在任何研究区域中是根据双等位基因还是三等位基因对参与者的等位基因状态进行分类,[11C] DASB 结合潜能均不受其影响。我们的 PET 研究结果在一个相对较大的样本中使用了近乎最佳的放射性示踪剂,表明 5-HTTLPR 多态性变异不会影响 5-HTT 对 [11C] DASB 结合的可用性在成人脑中。因此,5-HTTLPR 多态性变异对情绪处理和易患抑郁症的影响更有可能通过神经发育过程中的作用来表达。

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