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高度可塑性感觉运动神经回路中微小RNA和信使RNA季节性动态的网络分析

Network analysis of microRNA and mRNA seasonal dynamics in a highly plastic sensorimotor neural circuit.

作者信息

Larson Tracy A, Lent Karin L, Bammler Theo K, MacDonald James W, Wood William E, Caras Melissa L, Thatra Nivretta M, Budzillo Agata, Perkel David J, Brenowitz Eliot A

机构信息

Department of Biology, University of Washington, Seattle, WA, 98195, USA.

Present Address: Basic Sciences Division, Fred Hutchinson Cancer Research Center, 1100 Fairview Ave N, Seattle, WA, 98109, USA.

出版信息

BMC Genomics. 2015 Nov 6;16:905. doi: 10.1186/s12864-015-2175-z.

Abstract

BACKGROUND

Adult neurogenesis and the incorporation of adult-born neurons into functional circuits requires precise spatiotemporal coordination across molecular networks regulating a wide array of processes, including cell proliferation, apoptosis, neurotrophin signaling, and electrical activity. MicroRNAs (miRs) - short, non-coding RNA sequences that alter gene expression by post-transcriptional inhibition or degradation of mRNA sequences - may be involved in the global coordination of such diverse biological processes. To test the hypothesis that miRs related to adult neurogenesis and related cellular processes are functionally regulated in the nuclei of the avian song control circuit, we used microarray analyses to quantify changes in expression of miRs and predicted target mRNAs in the telencephalic nuclei HVC, the robust nucleus of arcopallium (RA), and the basal ganglia homologue Area X in breeding and nonbreeding Gambel's white-crowned sparrows (Zonotrichia leucophrys gambelli).

RESULTS

We identified 46 different miRs that were differentially expressed across seasons in the song nuclei. miR-132 and miR-210 showed the highest differential expression in HVC and Area X, respectively. Analyzing predicted mRNA targets of miR-132 identified 33 candidate target genes that regulate processes including cell cycle control, calcium signaling, and neuregulin signaling in HVC. Likewise, miR-210 was predicted to target 14 mRNAs differentially expressed across seasons that regulate serotonin, GABA, and dopamine receptor signaling and inflammation.

CONCLUSIONS

Our results identify potential miR-mRNA regulatory networks related to adult neurogenesis and provide opportunities to discover novel genetic control of the diverse biological processes and factors related to the functional incorporation of new neurons to the adult brain.

摘要

背景

成体神经发生以及新生神经元整合到功能回路中,需要跨越调控一系列广泛过程的分子网络进行精确的时空协调,这些过程包括细胞增殖、凋亡、神经营养因子信号传导和电活动。微小RNA(miR)——通过对mRNA序列进行转录后抑制或降解来改变基因表达的短非编码RNA序列——可能参与了这些不同生物过程的整体协调。为了验证与成体神经发生及相关细胞过程相关的miR在鸟类鸣叫控制回路的细胞核中受到功能调控这一假设,我们使用微阵列分析来量化繁殖期和非繁殖期的甘贝尔白冠雀(Zonotrichia leucophrys gambelli)端脑核团HVC、弓状皮质粗核(RA)和基底神经节同源区域X中miR及其预测靶mRNA的表达变化。

结果

我们鉴定出46种在鸣叫核团中随季节差异表达的不同miR。miR - 132和miR - 210分别在HVC和区域X中表现出最高的差异表达。对miR - 132的预测mRNA靶标进行分析,确定了33个候选靶基因,这些基因调控HVC中的细胞周期控制、钙信号传导和神经调节蛋白信号传导等过程。同样,miR - 210被预测靶向14种在不同季节差异表达的mRNA,这些mRNA调控血清素、GABA和多巴胺受体信号传导以及炎症。

结论

我们的结果确定了与成体神经发生相关的潜在miR - mRNA调控网络,并为发现与新神经元功能性整合到成体大脑相关的各种生物过程和因子的新型遗传控制提供了机会。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/26be/4636775/e40688562ac0/12864_2015_2175_Fig1_HTML.jpg

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