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ZEB家族因子ZAG-1和NK-2同源结构域因子CEH-28对秀丽隐杆线虫神经元分化的调控

Regulation of C. elegans neuronal differentiation by the ZEB-family factor ZAG-1 and the NK-2 homeodomain factor CEH-28.

作者信息

Ramakrishnan Kalpana, Okkema Peter G

机构信息

Department of Biological Sciences, University of Illinois at Chicago, Chicago, Illinois, United States of America.

出版信息

PLoS One. 2014 Dec 4;9(12):e113893. doi: 10.1371/journal.pone.0113893. eCollection 2014.

Abstract

The C. elegans pharyngeal neuron M4 is a multi-functional cell that acts as a cholinergic motor neuron to stimulate peristaltic pharyngeal muscle contraction and as a neuroendocrine cell secreting neuropeptides and growth factors to affect other cells both inside and outside the pharynx. The conserved transcription factors ZAG-1 and CEH-28 are co-expressed in M4 through most of development, and here we examine how these factors contribute to M4 differentiation. We find ZAG-1 functions upstream of CEH-28 in a branched pathway to activate expression of different sets of M4 differentiation markers. CEH-28 activates expression of the growth factor genes dbl-1 and egl-17, and the neuropeptide genes flp-5 and flp-2, while ZAG-1 activates expression of the serotonin receptor ser-7, as well as expression of ceh-28 and its downstream targets. Other markers of M4 differentiation are expressed normally in both zag-1 and ceh-28 mutants, including the neuropeptide gene flp-21 and the acetylcholine biosynthetic gene unc-17. Unlike ceh-28 mutants, zag-1 mutants completely lack peristaltic muscle contractions resulting from broader defects in M4 differentiation. Despite these defects, neither ZAG-1 nor CEH-28 are terminal selectors of the M4 phenotype, and we suggest they function in a hierarchy to regulate different aspects of M4 differentiation.

摘要

秀丽隐杆线虫的咽神经元M4是一种多功能细胞,它作为胆碱能运动神经元刺激咽蠕动肌肉收缩,同时作为神经内分泌细胞分泌神经肽和生长因子,以影响咽内外的其他细胞。保守的转录因子ZAG-1和CEH-28在M4发育的大部分时间里共同表达,在这里我们研究这些因子如何促进M4分化。我们发现ZAG-1在一条分支途径中位于CEH-28的上游,以激活不同组M4分化标记物的表达。CEH-28激活生长因子基因dbl-1和egl-17以及神经肽基因flp-5和flp-2的表达,而ZAG-1激活5-羟色胺受体ser-7的表达以及ceh-28及其下游靶点的表达。M4分化的其他标记物在zag-1和ceh-28突变体中均正常表达,包括神经肽基因flp-21和乙酰胆碱生物合成基因unc-17。与ceh-28突变体不同,zag-1突变体由于M4分化中更广泛的缺陷而完全缺乏蠕动肌肉收缩。尽管存在这些缺陷,但ZAG-1和CEH-28都不是M4表型的终末选择因子,我们认为它们在一个层次结构中发挥作用,以调节M4分化的不同方面。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cb0e/4256384/44e5a6856c70/pone.0113893.g001.jpg

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