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下丘脑神经降压素系统的遗传分析。

Genetic analysis of the hypothalamic neurotensin system.

作者信息

Garlow Steven J, Boone Ericka, Kinkead Becky, Nemeroff Charles B

机构信息

Department of Psychiatry and Behavioral Sciences, Emory University School of Medicine, Atlanta, GA 30329, USA.

出版信息

Neuropsychopharmacology. 2006 Mar;31(3):535-43. doi: 10.1038/sj.npp.1300870.

Abstract

This study used B x D recombinant inbred mice to detect and localize genes that control the hypothalamic neurotensin (NT) system. Abundance of transcripts that encode NT and NT receptors 1, 2, and 3 (NTR1, NTR2, and NTR3) in total hypothalamic RNA was the quantitative trait measured. Analysis of transcript abundance data revealed associations with quantitative trait loci (QTL) for NT transcript abundance (NTta) on chromosome 1, 3, 6, 7, 8, and 9; for NTR1ta on chromosome 3, 8, 12, and X; for NTR2ta on chromosome 2, 4, 9, 10, 12, 13, and 17; for NTR3ta on chromosome 1, 7, 11, and 12. NTta QTL on chromosomes 3, 7, and 8 coincide with QTL previously identified that impact NT peptide content and NTR2ta QTL on chromosome 2 and 12 coincide with genes previously associated with NTR2 receptor abundance. The NTta, NTR1ta, and NTR3ta QTL were not linked to their respective structural genes, but there is a highly significant (p<0.001) association for NTR2ta on chromosome 12 that includes the Ntsr2 structural gene. There are areas of potential shared genetic regulation between NTta and NTR3ta on chromosome 1 and 7 and for all three receptors on proximal chromosome 12. The NTta QTL on chromosome 9 includes the dopamine D2 receptor (Drd2) gene and QTL involved in responses to dopaminergic agents (Hts), antipsychotics (Hpic1) and cocaine (Cocrb8), and ethanol (Etohc3). These results further strengthen the hypothesis that the NT system is involved in mediating the actions of antipsychotic agents and drugs of abuse.

摘要

本研究使用B×D重组近交系小鼠来检测和定位控制下丘脑神经降压素(NT)系统的基因。所测量的数量性状是下丘脑总RNA中编码NT及NT受体1、2和3(NTR1、NTR2和NTR3)的转录本丰度。对转录本丰度数据的分析揭示了与1、3、6、7、8和9号染色体上NT转录本丰度(NTta)数量性状位点(QTL)的关联;与3、8、12和X染色体上NTR1ta的关联;与2、4、9、10、12、13和17号染色体上NTR2ta的关联;与1、7、11和12号染色体上NTR3ta的关联。3、7和8号染色体上的NTta QTL与先前确定的影响NT肽含量的QTL一致,2和12号染色体上的NTR2ta QTL与先前与NTR2受体丰度相关的基因一致。NTta、NTR1ta和NTR3ta QTL与其各自的结构基因不连锁,但12号染色体上的NTR2ta存在高度显著(p<0.001)的关联,其中包括Ntsr2结构基因。1和7号染色体上NTta与NTR3ta之间以及12号染色体近端的所有三种受体之间存在潜在的共享遗传调控区域。9号染色体上的NTta QTL包括多巴胺D2受体(Drd2)基因以及参与对多巴胺能药物(Hts)、抗精神病药物(Hpic1)、可卡因(Cocrb8)和乙醇(Etohc3)反应的QTL。这些结果进一步强化了NT系统参与介导抗精神病药物和滥用药物作用的假说。

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