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候选Agtr2影响的基因和通路,是通过对Agtr2(-/y)小鼠发育中的大脑进行表达谱分析确定的。

Candidate Agtr2 influenced genes and pathways identified by expression profiling in the developing brain of Agtr2(-/y) mice.

作者信息

Pawlowski Traci L, Heringer-Walther Silvia, Cheng Chun-Huai, Archie John G, Chen Chin-Fu, Walther Thomas, Srivastava Anand K

机构信息

J. C. Self Research Institute of Human Genetics, Greenwood Genetic Center, SC, USA

出版信息

Genomics. 2009 Sep;94(3):188-95. doi: 10.1016/j.ygeno.2009.05.011. Epub 2009 Jun 6.

Abstract

Intellectual disability (ID) is a common developmental disability observed in 1 to 3% of the human population. A possible role for the Angiotensin II type 2 receptor (AGTR2) in brain function, affecting learning, memory, and behavior, has been suggested in humans and rodents. Mice lacking the Agtr2 gene (Agtr2(-/y)) showed significant impairment in their spatial memory and exhibited abnormal dendritic spine morphology. To identify Agtr2 influenced genes and pathways, we performed whole genome microarray analysis on RNA isolated from brains of Agtr2(-/y) and control male mice at embryonic day 15 (E15) and postnatal day one (P1). The gene expression profiles of the Agtr2(-/y) brain samples were significantly different when compared to profiles of the age-matched control brains. We identified 62 differently expressed genes (p< or =0.005) at E15 and in P1 brains of the Agtr2(-/y) mice. We verified the differential expression of several of these genes in brain samples using quantitative RT-PCR. Differentially expressed genes encode molecules involved in multiple cellular processes including microtubule functions associated with dendritic spine morphology. This study provides insight into Agtr2 influenced candidate genes and suggests that expression dysregulation of these genes may modulate Agtr2 actions in the brain that influences learning and memory.

摘要

智力残疾(ID)是一种常见的发育障碍,在1%至3%的人群中可见。在人类和啮齿动物中,已有人提出血管紧张素II 2型受体(AGTR2)在影响学习、记忆和行为的脑功能中可能发挥作用。缺乏Agtr2基因的小鼠(Agtr2(-/y))在空间记忆方面表现出显著损伤,并呈现出异常的树突棘形态。为了鉴定受Agtr2影响的基因和通路,我们对从胚胎第15天(E15)和出生后第1天(P1)的Agtr2(-/y)雄性小鼠和对照雄性小鼠大脑中分离的RNA进行了全基因组微阵列分析。与年龄匹配的对照大脑的基因表达谱相比,Agtr2(-/y)大脑样本的基因表达谱有显著差异。我们在Agtr2(-/y)小鼠的E15和P1大脑中鉴定出62个差异表达基因(p≤0.005)。我们使用定量RT-PCR验证了这些基因中的几个在大脑样本中的差异表达。差异表达基因编码参与多种细胞过程的分子,包括与树突棘形态相关的微管功能。本研究深入了解了受Agtr2影响的候选基因,并表明这些基因的表达失调可能调节Agtr2在大脑中影响学习和记忆的作用。

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