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CCAAT 盒转录因子 NF-Y 复合物介导秀丽隐杆线虫中 IL1 神经元的特化。

The CCAAT-box transcription factor, NF-Y complex, mediates the specification of the IL1 neurons in C. elegans.

机构信息

Department of Brain Sciences, DGIST, Daegu 42988, Korea.

Department of Life and Nanopharmaceutical Sciences, Kyung Hee University, Seoul 02447, Korea.

出版信息

BMB Rep. 2023 Mar;56(2):153-159. doi: 10.5483/BMBRep.2022-0146.

Abstract

Neuronal differentiation is highly coordinated through a cascade of gene expression, mediated via interactions between transacting transcription factors and cis-regulatory elements of their target genes. However, the mechanisms of transcriptional regulation that determine neuronal cell-fate are not fully understood. Here, we show that the nuclear transcription factor Y (NF-Y) subunit, NFYA-1, is necessary and sufficient to express the flp-3 neuropeptide gene in the IL1 neurons of C. elegans. flp-3 expression is decreased in dorsal and lateral, but not ventral IL1s of nfya-1 mutants. The expression of another terminally differentiated gene, eat-4 vesicular glutamate transporter, is abolished, whereas the unc-8 DEG/ENaC gene and pan-neuronal genes are expressed normally in IL1s of nfya-1 mutants. nfya-1 is expressed in and acts in IL1s to regulate flp-3 and eat-4 expression. Ectopic expression of NFYA-1 drives the expression of flp-3 gene in other cell-types. Promoter analysis of IL1-expressed genes results in the identification of several cisregulatory motifs which are necessary for IL1 expression, including a putative CCAAT-box located in the flp-3 promoter that NFYA-1 directly interacts with. NFYA-1 and NFYA-2, together with NFYB-1 and NFYC-1, exhibit partly or fully redundant roles in the regulation of flp-3 or unc-8 expression, respectively. Taken together, our data indicate that the NF-Y complex regulates neuronal subtype-specification via regulating a set of terminal-differentiation genes. [BMB Reports 2023; 56(3): 153-159].

摘要

神经元分化是通过基因表达的级联反应高度协调的,这种级联反应是通过反式作用转录因子与其靶基因的顺式调控元件之间的相互作用介导的。然而,决定神经元细胞命运的转录调控机制尚不完全清楚。在这里,我们表明核转录因子 Y (NF-Y) 亚基 NFYA-1,对于在秀丽隐杆线虫的 IL1 神经元中表达 flp-3 神经肽基因是必需和充分的。在 nfya-1 突变体中,flp-3 的表达在背部和侧面减少,但在腹部不减少。另一个终末分化基因 eat-4 囊泡谷氨酸转运体的表达被废除,而 unc-8 DEG/ENaC 基因和全神经元基因在 nfya-1 突变体的 IL1 中正常表达。nfya-1 在 IL1 中表达并起作用,以调节 flp-3 和 eat-4 的表达。NFYA-1 的异位表达驱动 flp-3 基因在其他细胞类型中的表达。对 IL1 表达基因的启动子分析导致鉴定出几个顺式调控元件,这些元件对于 IL1 表达是必需的,包括位于 flp-3 启动子中的一个推定的 CCAAT 盒,NFYA-1 可以直接与之相互作用。NFYA-1 和 NFYA-2 与 NFYB-1 和 NFYC-1 一起,在调节 flp-3 或 unc-8 的表达方面分别表现出部分或完全冗余的作用。总之,我们的数据表明 NF-Y 复合物通过调节一组终末分化基因来调节神经元亚型特异性。[BMB 报告 2023;56(3): 153-159]。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8497/10068339/eba9d4aeeb18/bmb-56-3-153-f1.jpg

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