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Nerve growth factor (NGF) prevents the shift in ocular dominance distribution of visual cortical neurons in monocularly deprived rats

机译:神经生长因子(NGF)防止单眼剥夺大鼠视皮质神经元的眼优势分布发生变化

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摘要

The hypothesis that NGF could play a role in the plasticity of the developing mammalian visual cortex was tested in monocularly deprived (MD) rats. In particular, we have asked whether an exogenous supply of NGF could prevent the changes in ocular dominance distribution induced by monocular deprivation. Hooded rats were monocularly deprived for 1 month, starting at postnatal day 14 (P14), immediately before eye opening, by means of eyelid suture. In eight rats, only monocular deprivation was performed; in eight rats, monocular deprivation was combined with intraventricular injections of beta-NGF, and in three rats, with intraventricular injections of cytochrome C. Injections (2 microliters) were given every other day for a period of 1 month. Single neuron activity was recorded in the primary visual cortex of MD rats, MD rats treated with NGF, and MD rats treated with cytochrome C at the end of the deprivation period, and in normal rats of the same age. We found that monocular deprivation caused a striking change in the ocular dominance distribution of untreated MD rats, reducing binocular cells by a factor of two and increasing by a factor of eight the number of cells dominated by the nondeprived eye. In MD NGF-treated rats, the ocular dominance distribution was indistinguishable from the normal. Cytochrome C treatment was completely ineffective in preventing the ocular dominance shift induced by monocular deprivation. To test whether NGF affected cortical physiology or interfered with transmission of visual information, we evaluated in NGF-treated rats the spontaneous discharge and the orientation selectivity. We found these functional properties to be in the normal range. We conclude that NGF is effective in preventing the effects of monocular deprivation in the rat visual cortex and suggest that NGF is a crucial factor in the competitive processes leading to the stabilization of functional geniculocortical connections during the critical period.
机译:在单眼剥夺(MD)大鼠中测试了NGF可能在发育中的哺乳动物视皮层可塑性中起作用的假说。特别是,我们已经问过,NGF的外源供应是否可以阻止由单眼剥夺引起的眼优势分布的变化。从出生后的第14天(P14)开始,立即用眼睑缝合剥夺有头戴的大鼠1个月。在八只大鼠中,仅进行了单眼剥夺。在八只大鼠中,单眼剥夺与脑室内注射β-NGF结合,在三只大鼠中,脑室注射细胞色素C。每隔一天注射一次(2微升),持续1个月。在剥夺期结束时,在MD大鼠,NGF处理过的MD大鼠和细胞色素C处理过的MD大鼠以及同龄正常大鼠的初级视皮层中记录了单个神经元的活性。我们发现单眼剥夺导致未经治疗的MD大鼠的眼优势分布发生显着变化,使双眼细胞减少2倍,而无剥夺性眼占优势的细胞数量增加8倍。在用MD NGF治疗的大鼠中,眼的优势分布与正常人没有区别。细胞色素C治疗在预防由单眼剥夺引起的眼优势转移方面完全无效。为了测试NGF是否会影响皮层生理或干扰视觉信息的传递,我们在NGF治疗的大鼠中评估了自发放电和方向选择性。我们发现这些功能特性在正常范围内。我们得出的结论是,NGF可有效预防大鼠视皮层单眼剥夺的影响,并表明NGF是竞争过程中的关键因素,在关键时期可导致功能性基因核连接稳定。

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