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具有串联感觉 PAS 结构域的细胞周期激酶整合细胞命运线索。

A cell cycle kinase with tandem sensory PAS domains integrates cell fate cues.

机构信息

Department of Developmental Biology, Stanford University School of Medicine, Stanford, California 94305, USA.

Department of Biochemistry, Stanford University School of Medicine, Stanford, California 94305, USA.

出版信息

Nat Commun. 2016 Apr 27;7:11454. doi: 10.1038/ncomms11454.

Abstract

All cells must integrate sensory information to coordinate developmental events in space and time. The bacterium Caulobacter crescentus uses two-component phospho-signalling to regulate spatially distinct cell cycle events through the master regulator CtrA. Here, we report that CckA, the histidine kinase upstream of CtrA, employs a tandem-PAS domain sensor to integrate two distinct spatiotemporal signals. Using CckA reconstituted on liposomes, we show that one PAS domain modulates kinase activity in a CckA density-dependent manner, mimicking the stimulation of CckA kinase activity that occurs on its transition from diffuse to densely packed at the cell poles. The second PAS domain interacts with the asymmetrically partitioned second messenger cyclic-di-GMP, inhibiting kinase activity while stimulating phosphatase activity, consistent with the selective inactivation of CtrA in the incipient stalked cell compartment. The integration of these spatially and temporally regulated signalling events within a single signalling receptor enables robust orchestration of cell-type-specific gene regulation.

摘要

所有细胞都必须整合感觉信息,以协调空间和时间上的发育事件。弯曲杆菌(Caulobacter crescentus)利用双组分磷酸信号来调节空间上不同的细胞周期事件,其通过主调控因子 CtrA 实现这一功能。在这里,我们报告称,CtrA 的上游组氨酸激酶 CckA 采用串联 PAS 结构域传感器来整合两个不同的时空信号。我们使用在脂质体上重组的 CckA 进行实验,结果表明一个 PAS 结构域以 CckA 密度依赖的方式调节激酶活性,模拟了 CckA 激酶活性在从弥散状态过渡到细胞两极密集状态时所发生的刺激。第二个 PAS 结构域与不对称分配的第二信使环二鸟苷酸(cyclic-di-GMP)相互作用,抑制激酶活性,同时刺激磷酸酶活性,这与 CtrA 在初始柄细胞区室中的选择性失活一致。这些时空调节的信号事件在单个信号受体中的整合,使得细胞类型特异性基因调控能够得到稳健的协调。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3e9b/4853435/33096bca89ad/ncomms11454-f1.jpg

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