Distinct roles of Bdnf I and Bdnf IV transcript variant expression in hippocampal neurons

IF 2.4 3区 医学 Q3 NEUROSCIENCES
Hippocampus Pub Date : 2024-02-16 DOI:10.1002/hipo.23600
Svitlana V. Bach, Allison J. Bauman, Darya Hosein, Jennifer J. Tuscher, Lara Ianov, Kelsey M. Greathouse, Benjamin W. Henderson, Jeremy H. Herskowitz, Keri Martinowich, Jeremy J. Day
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Abstract

Brain-derived neurotrophic factor (Bdnf) plays a critical role in brain development, dendritic growth, synaptic plasticity, as well as learning and memory. The rodent Bdnf gene contains nine 5′ non-coding exons (IIXa), which are spliced to a common 3′ coding exon (IX). Transcription of individual Bdnf variants, which all encode the same BDNF protein, is initiated at unique promoters upstream of each non-coding exon, enabling precise spatiotemporal and activity-dependent regulation of Bdnf expression. Although prior evidence suggests that Bdnf transcripts containing exon I (Bdnf I) or exon IV (Bdnf IV) are uniquely regulated by neuronal activity, the functional significance of different Bdnf transcript variants remains unclear. To investigate functional roles of activity-dependent Bdnf I and IV transcripts, we used a CRISPR activation system in which catalytically dead Cas9 fused to a transcriptional activator (VPR) is targeted to individual Bdnf promoters with single guide RNAs, resulting in transcript-specific Bdnf upregulation. Bdnf I upregulation is associated with gene expression changes linked to dendritic growth, while Bdnf IV upregulation is associated with genes that regulate protein catabolism. Upregulation of Bdnf I, but not Bdnf IV, increased mushroom spine density, volume, length, and head diameter, and also produced more complex dendritic arbors in cultured rat hippocampal neurons. In contrast, upregulation of Bdnf IV, but not Bdnf I, in the rat hippocampus attenuated contextual fear expression. Our data suggest that while Bdnf I and IV are both activity-dependent, BDNF produced from these promoters may serve unique cellular, synaptic, and behavioral functions.

Abstract Image

海马神经元中 Bdnf I 和 Bdnf IV 转录本变异表达的不同作用
脑源性神经营养因子(Bdnf)在大脑发育、树突生长、突触可塑性以及学习和记忆中起着至关重要的作用。啮齿类动物的 Bdnf 基因包含九个 5' 非编码外显子(I-IXa),这些外显子拼接成一个共同的 3' 编码外显子(IX)。各个 Bdnf 变体都编码相同的 BDNF 蛋白,其转录由每个非编码外显子上游的独特启动子启动,从而实现了对 Bdnf 表达的精确时空调控和活动依赖性调控。尽管已有证据表明,含有外显子 I(Bdnf I)或外显子 IV(Bdnf IV)的 Bdnf 转录本受神经元活动的独特调控,但不同 Bdnf 转录本变体的功能意义仍不清楚。为了研究活动依赖性 Bdnf I 和 IV 转录本的功能作用,我们使用了一种 CRISPR 激活系统,在该系统中,催化死亡的 Cas9 与转录激活剂(VPR)融合,用单导 RNA 靶向单个 Bdnf 启动子,从而导致转录本特异性的 Bdnf 上调。Bdnf I 的上调与树突生长相关的基因表达变化有关,而 Bdnf IV 的上调则与调节蛋白质分解的基因有关。在培养的大鼠海马神经元中,上调 Bdnf I(而非 Bdnf IV)会增加蘑菇棘的密度、体积、长度和头部直径,并产生更复杂的树突轴。与此相反,在大鼠海马中上调 Bdnf IV 而非 Bdnf I 可减轻情境恐惧的表达。我们的数据表明,虽然 Bdnf I 和 IV 都是活动依赖性的,但这些启动子产生的 BDNF 可能具有独特的细胞、突触和行为功能。
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来源期刊
Hippocampus
Hippocampus 医学-神经科学
CiteScore
5.80
自引率
5.70%
发文量
79
审稿时长
3-8 weeks
期刊介绍: Hippocampus provides a forum for the exchange of current information between investigators interested in the neurobiology of the hippocampal formation and related structures. While the relationships of submitted papers to the hippocampal formation will be evaluated liberally, the substance of appropriate papers should deal with the hippocampal formation per se or with the interaction between the hippocampal formation and other brain regions. The scope of Hippocampus is wide: single and multidisciplinary experimental studies from all fields of basic science, theoretical papers, papers dealing with hippocampal preparations as models for understanding the central nervous system, and clinical studies will be considered for publication. The Editor especially encourages the submission of papers that contribute to a functional understanding of the hippocampal formation.
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