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数量性状基因座分析将 Gabra3 鉴定为调控小鼠行为绝望的调节因子。

Quantitative trait locus analysis identifies Gabra3 as a regulator of behavioral despair in mice.

机构信息

Department of Neuroscience, Scripps Florida, Jupiter, FL 33458, USA.

出版信息

Mamm Genome. 2010 Jun;21(5-6):247-57. doi: 10.1007/s00335-010-9266-6. Epub 2010 May 29.

Abstract

The Tail Suspension Test (TST), which measures behavioral despair, is widely used as an animal model of human depressive disorders and antidepressant efficacy. In order to identify novel genes involved in the regulation of TST performance, we crossed an inbred strain exhibiting low immobility in the TST (RIIIS/J) with two high-immobility strains (C57BL/6J and NZB/BlNJ) to create two distinct F2 hybrid populations. All F2 offspring (n = 655) were genotyped at high density with a panel of SNP markers. Whole-genome interval mapping of the F2 populations identified statistically significant quantitative trait loci (QTLs) on mouse chromosomes (MMU) 4, 6, and X. Microarray analysis of hippocampal gene expression in the three parental strains was used to identify potential candidate genes within the MMUX QTLs identified in the NZB/BlNJ x RIIIS/J cross. Expression of Gabra3, which encodes the GABA(A) receptor alpha3 subunit, was robust in the hippocampus of B6 and RIIIS mice but absent from NZB hippocampal tissue. To verify the role of Gabra3 in regulating TST behavior in vivo, mice were treated with SB-205384, a positive modulator of the alpha3 subunit. SB-205384 significantly reduced TST immobility in B6 mice without affecting general activity, but it had no effect on behavior in NZB mice. This work suggests that GABRA3 regulates a behavioral endophenotype of depression and establishes this gene as a viable new target for the study and treatment of human depression.

摘要

悬尾试验(TST)是一种衡量行为绝望的方法,被广泛用作人类抑郁症和抗抑郁疗效的动物模型。为了鉴定参与 TST 表现调节的新基因,我们将在 TST 中表现出低不动性的近交系(RIIIS/J)与两个高不动性系(C57BL/6J 和 NZB/BlNJ)杂交,创建了两个不同的 F2 杂交群体。所有 F2 后代(n=655)均用 SNP 标记的高密度面板进行基因分型。F2 群体的全基因组区间作图确定了在 MMU 4、6 和 X 染色体上存在统计学上显著的数量性状基因座(QTL)。对三个亲本系的海马基因表达的微阵列分析用于鉴定在 NZB/BlNJ x RIIIS/J 杂交中鉴定出的 MMUX QTL 内的潜在候选基因。编码 GABA(A)受体α3 亚基的 Gabra3 在 B6 和 RIIIS 小鼠的海马体中表达丰富,但在 NZB 海马组织中不存在。为了验证 Gabra3 在体内调节 TST 行为的作用,用 SB-205384 处理小鼠,这是一种 alpha3 亚基的正调节剂。SB-205384 显著降低了 B6 小鼠的 TST 不动性,而不影响一般活动,但对 NZB 小鼠的行为没有影响。这项工作表明 GABRA3 调节抑郁症的行为表型,并将该基因确立为研究和治疗人类抑郁症的可行新靶标。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f998/2890984/70589e42b371/335_2010_9266_Fig1_HTML.jpg

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