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A Transgenic Rat for Specifically Inhibiting Adult Neurogenesis

机译:专门抑制成年神经发生的转基因大鼠。

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摘要

The growth of research on adult neurogenesis and the development of new models and tools have greatly advanced our understanding of the function of newborn neurons in recent years. However, there are still significant limitations in the ability to identify the functions of adult neurogenesis in available models. Here we report a transgenic rat (TK rat) that expresses herpes simplex virus thymidine kinase in GFAP+ cells. Upon treating TK rats with the antiviral drug valganciclovir, granule cell neurogenesis can be completely inhibited in adulthood, in both the hippocampus and olfactory bulb. Interestingly, neurogenesis in the glomerular and external plexiform layers of the olfactory bulb was only partially inhibited, suggesting that some adult-born neurons in these regions derive from a distinct precursor population that does not express GFAP. Within the hippocampus, blockade of neurogenesis was rapid and nearly complete within 1 week of starting treatment. Preliminary behavioral analyses indicate that general anxiety levels and patterns of exploration are generally unaffected in neurogenesis-deficient rats. However, neurogenesis-deficient TK rats showed reduced sucrose preference, suggesting deficits in reward-related behaviors. We expect that TK rats will facilitate structural, physiological, and behavioral studies that complement those possible in existing models, broadly enhancing understanding of the function of adult neurogenesis.
机译:近年来,关于成人神经发生的研究的增长以及新模型和工具的发展极大地增进了我们对新生神经元功能的认识。但是,在可用模型中鉴定成人神经发生功能的能力上仍然存在明显的局限性。在这里,我们报告了在GFAP +细胞中表达单纯疱疹病毒胸苷激酶的转基因大鼠(TK大鼠)。用抗病毒药缬更昔洛韦治疗TK大鼠后,成年期在海马和嗅球中均可完全抑制颗粒细胞神经发生。有趣的是,嗅球的肾小球和外部丛状层中的神经发生仅被部分抑制,这表明在这些区域中一些成年出生的神经元来自不表达GFAP的独特前体群体。在海马内,神经发生的阻断作用很快,并且在开始治疗后的1周内几乎完全消失。初步的行为分析表明,在神经发生缺陷的大鼠中,一般的焦虑水平和探索方式通常不受影响。然而,神经发生缺陷的TK大鼠显示出降低的蔗糖偏爱,表明奖励相关行为的缺陷。我们希望TK大鼠将促进结构,生理和行为研究,以补充现有模型中可能存在的那些,从而广泛增强对成年神经发生功能的理解。

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