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缺乏G蛋白γ3的小鼠体型消瘦且会癫痫发作。

Mice with deficiency of G protein gamma3 are lean and have seizures.

作者信息

Schwindinger William F, Giger Kathryn E, Betz Kelly S, Stauffer Anna M, Sunderlin Elaine M, Sim-Selley Laura J, Selley Dana E, Bronson Sarah K, Robishaw Janet D

机构信息

Geisinger Clinic, Weis Center for Research, 100 North Academy Ave., Danville, PA 17822, USA.

出版信息

Mol Cell Biol. 2004 Sep;24(17):7758-68. doi: 10.1128/MCB.24.17.7758-7768.2004.

Abstract

Emerging evidence suggests that the gamma subunit composition of an individual G protein contributes to the specificity of the hundreds of known receptor signaling pathways. Among the twelve gamma subtypes, gamma3 is abundantly and widely expressed in the brain. To identify specific functions and associations for gamma3, a gene-targeting approach was used to produce mice lacking the Gng3 gene (Gng3-/-). Confirming the efficacy and specificity of gene targeting, Gng3-/- mice show no detectable expression of the Gng3 gene, but expression of the divergently transcribed Bscl2 gene is not affected. Suggesting unique roles for gamma3 in the brain, Gng3-/- mice display increased susceptibility to seizures, reduced body weights, and decreased adiposity compared to their wild-type littermates. Predicting possible associations for gamma3, these phenotypic changes are associated with significant reductions in beta2 and alphai3 subunit levels in certain regions of the brain. The finding that the Gng3-/- mice and the previously reported Gng7-/- mice display distinct phenotypes and different alphabetagamma subunit associations supports the notion that even closely related gamma subtypes, such as gamma3 and gamma7, perform unique functions in the context of the organism.

摘要

新出现的证据表明,单个G蛋白的γ亚基组成有助于数百种已知受体信号通路的特异性。在12种γ亚型中,γ3在大脑中大量且广泛表达。为了确定γ3的特定功能和关联,采用基因靶向方法培育出缺乏Gng3基因(Gng3-/-)的小鼠。Gng3-/-小鼠未检测到Gng3基因的表达,但反向转录的Bscl2基因的表达未受影响,这证实了基因靶向的有效性和特异性。与野生型同窝小鼠相比,Gng3-/-小鼠表现出对癫痫发作的易感性增加、体重减轻和肥胖程度降低,这表明γ3在大脑中具有独特作用。这些表型变化与大脑某些区域中β2和αi3亚基水平的显著降低有关,这预测了γ3可能的关联。Gng3-/-小鼠与先前报道的Gng7-/-小鼠表现出不同的表型和不同的αβγ亚基关联,这一发现支持了这样一种观点,即即使是密切相关的γ亚型,如γ3和γ7,在生物体中也具有独特功能。

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