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脑内皮细胞 TRPA1 通道启动神经血管耦联。

Brain endothelial cell TRPA1 channels initiate neurovascular coupling.

机构信息

Department of Pharmacology, Center for Molecular and Cellular Signaling in the Cardiovascular System, University of Nevada, Reno School of Medicine, Reno, United States.

Department of Pharmacology, College of Medicine, University of Vermont, Burlington, United States.

出版信息

Elife. 2021 Feb 26;10:e63040. doi: 10.7554/eLife.63040.

Abstract

Cerebral blood flow is dynamically regulated by neurovascular coupling to meet the dynamic metabolic demands of the brain. We hypothesized that TRPA1 channels in capillary endothelial cells are stimulated by neuronal activity and instigate a propagating retrograde signal that dilates upstream parenchymal arterioles to initiate functional hyperemia. We find that activation of TRPA1 in capillary beds and post-arteriole transitional segments with mural cell coverage initiates retrograde signals that dilate upstream arterioles. These signals exhibit a unique mode of biphasic propagation. Slow, short-range intercellular Ca signals in the capillary network are converted to rapid electrical signals in transitional segments that propagate to and dilate upstream arterioles. We further demonstrate that TRPA1 is necessary for functional hyperemia and neurovascular coupling within the somatosensory cortex of mice in vivo. These data establish endothelial cell TRPA1 channels as neuronal activity sensors that initiate microvascular vasodilatory responses to redirect blood to regions of metabolic demand.

摘要

脑血流通过神经血管耦合进行动态调节,以满足大脑的动态代谢需求。我们假设毛细血管内皮细胞中的 TRPA1 通道受到神经元活动的刺激,并引发一种传播的逆行信号,使上游实质小动脉扩张,从而启动功能性充血。我们发现,毛细血管床和具有壁细胞覆盖的后动脉段中 TRPA1 的激活会引发逆行信号,使上游小动脉扩张。这些信号表现出独特的双相传播模式。毛细血管网络中的缓慢、短距离细胞间 Ca 信号转化为过渡段中的快速电信号,这些信号传播并扩张上游小动脉。我们进一步证明,TRPA1 对于体内小鼠体感皮层中的功能性充血和神经血管耦合是必需的。这些数据确立了内皮细胞 TRPA1 通道作为神经元活动传感器,启动微血管舒张反应,将血液重新引导到代谢需求区域。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bdd7/7935492/6a97a3526f1c/elife-63040-fig1.jpg

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