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发光激活核苷酸环化酶调控 cAMP 的时空合成。

Luminescence-activated nucleotide cyclase regulates spatial and temporal cAMP synthesis.

机构信息

Department of Pharmacology and Chemical Biology, Pittsburgh, Pennsylvania 15261; Molecular Pharmacology Training Program, University of Pittsburgh, Pittsburgh, Pennsylvania 15261.

Department of Pharmacology and Chemical Biology, Pittsburgh, Pennsylvania 15261.

出版信息

J Biol Chem. 2019 Jan 25;294(4):1095-1103. doi: 10.1074/jbc.AC118.004905. Epub 2018 Dec 17.

Abstract

cAMP is a ubiquitous second messenger that regulates cellular proliferation, differentiation, attachment, migration, and several other processes. It has become increasingly evident that tight regulation of cAMP accumulation and localization confers divergent yet specific signaling to downstream pathways. Currently, few tools are available that have sufficient spatial and temporal resolution to study location-biased cAMP signaling. Here, we introduce a new fusion protein consisting of a light-activated adenylyl cyclase (bPAC) and luciferase (nLuc). This construct allows dual activation of cAMP production through temporally precise photostimulation or chronic chemical stimulation that can be fine-tuned to mimic physiological levels and duration of cAMP synthesis to trigger downstream events. By targeting this construct to different compartments, we show that cAMP produced in the cytosol and nucleus stimulates proliferation in thyroid cells. The bPAC-nLuc fusion construct adds a new reagent to the available toolkit to study cAMP-regulated processes in living cells.

摘要

cAMP 是一种普遍存在的第二信使,调节细胞增殖、分化、附着、迁移和其他几个过程。越来越明显的是,cAMP 积累和定位的严格调节赋予了下游途径不同但特定的信号。目前,很少有工具具有足够的空间和时间分辨率来研究位置偏向的 cAMP 信号。在这里,我们引入了一种新的融合蛋白,由光激活的腺苷酸环化酶(bPAC)和荧光素酶(nLuc)组成。这种构建体允许通过时间上精确的光刺激或慢性化学刺激来双重激活 cAMP 的产生,这种刺激可以进行微调,以模拟 cAMP 合成的生理水平和持续时间,从而触发下游事件。通过将这种构建体靶向不同的隔室,我们表明细胞质和核中产生的 cAMP 刺激甲状腺细胞的增殖。bPAC-nLuc 融合构建体为研究活细胞中 cAMP 调节的过程增加了一种新的试剂。

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