SREB2/GPR85, a schizophrenia risk factor, negatively regulates hippocampal adult neurogenesis and neurogenesis-dependent learning and memory

被引:44
作者
Chen, Qian [1 ]
Kogan, Jeffrey H. [1 ]
Gross, Adam K. [1 ]
Zhou, Yuan [2 ]
Walton, Noah M. [1 ]
Shin, Rick [1 ]
Heusner, Carrie L. [1 ]
Miyake, Shinichi [1 ]
Tajinda, Katsunori [1 ]
Tamura, Kouichi [1 ]
Matsumoto, Mitsuyuki [1 ]
机构
[1] Astellas Res Inst Amer LLC, CNS, Skokie, IL 60077 USA
[2] Northwestern Univ, Master Biotechnol Program, Evanston, IL USA
关键词
bromodeoxyuridine; cognition; dentate gyrus; mutant mouse; psychiatric disease; DENTATE GYRUS; ENVIRONMENTAL ENRICHMENT; DOUBLECORTIN EXPRESSION; PATTERN SEPARATION; SREB2; GPR85; BRAIN; PROTEIN; NEURONS; PROLIFERATION; INTEGRATION;
D O I
10.1111/j.1460-9568.2012.08180.x
中图分类号
Q189 [神经科学];
学科分类号
071006 ;
摘要
SREB2/GPR85, a member of the super-conserved receptor expressed in brain (SREB) family, is the most conserved G-protein-coupled receptor in vertebrate evolution. Previous human and mouse genetic studies have indicated a possible link between SREB2 and schizophrenia. SREB2 is robustly expressed in the hippocampal formation, especially in the dentate gyrus, a structure with an established involvement in psychiatric disorders and cognition. However, the function of SREB2 in the hippocampus remains elusive. Here we show that SREB2 regulates hippocampal adult neurogenesis, which impacts on cognitive function. Bromodeoxyuridine incorporation and immunohistochemistry were conducted in SREB2 transgenic (Tg, over-expression) and knockout (KO, null-mutant) mice to quantitatively assay adult neurogenesis and newborn neuron dendritic morphology. Cognitive responses associated with adult neurogenesis alteration were evaluated in SREB2 mutant mice. In SREB2 Tg mice, both new cell proliferation and new neuron survival were decreased in the dentate gyrus, whereas an enhancement of new neuron survival occurred in SREB2 KO mouse dentate gyrus. Doublecortin staining revealed dendritic morphology deficits of newly generated neurons in SREB2 Tg mice. In a spatial pattern separation task, SREB2 Tg mice displayed a decreased ability to discriminate spatial relationships, whereas SREB2 KO mice had enhanced abilities in this task. Additionally, SREB2 Tg and KO mice had reciprocal phenotypes in a Y-maze working memory task. Our results indicate that SREB2 is a negative regulator of adult neurogenesis and consequential cognitive functions. Inhibition of SREB2 function may be a novel approach to enhance hippocampal adult neurogenesis and cognitive abilities to ameliorate core symptoms of psychiatric patients.
引用
收藏
页码:2597 / 2608
页数:12
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