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K 和 TRP 通道在心血管生理学中的功能相互作用:衰老和慢性疾病的现代观点。

Functional Interaction among K and TRP Channels for Cardiovascular Physiology: Modern Perspectives on Aging and Chronic Disease.

机构信息

Department of Basic Sciences, 11041 Campus Street, Risley Hall, Loma Linda University, Loma Linda, CA 92350, USA.

出版信息

Int J Mol Sci. 2019 Mar 19;20(6):1380. doi: 10.3390/ijms20061380.

Abstract

Effective delivery of oxygen and essential nutrients to vital organs and tissues throughout the body requires adequate blood flow supplied through resistance vessels. The intimate relationship between intracellular calcium ([Ca]) and regulation of membrane potential (V) is indispensable for maintaining blood flow regulation. In particular, Ca-activated K⁺ (K) channels were ascertained as transducers of elevated [Ca] signals into hyperpolarization of V as a pathway for decreasing vascular resistance, thereby enhancing blood flow. Recent evidence also supports the reverse role for K channels, in which they facilitate Ca influx into the cell interior through open non-selective cation (e.g., transient receptor potential; TRP) channels in accord with robust electrical (hyperpolarization) and concentration (~20,000-fold) transmembrane gradients for Ca. Such an arrangement supports a feed-forward activation of V hyperpolarization while potentially boosting production of nitric oxide. Furthermore, in vascular types expressing TRP channels but deficient in functional K channels (e.g., collecting lymphatic endothelium), there are profound alterations such as downstream depolarizing ionic fluxes and the absence of dynamic hyperpolarizing events. Altogether, this review is a refined set of evidence-based perspectives focused on the role of the endothelial K and TRP channels throughout multiple experimental animal models and vascular types. We discuss the diverse interactions among K and TRP channels to integrate Ca, oxidative, and electrical signaling in the context of cardiovascular physiology and pathology. Building from a foundation of cellular biophysical data throughout a wide and diverse compilation of significant discoveries, a translational narrative is provided for readers toward the treatment and prevention of chronic, age-related cardiovascular disease.

摘要

有效向全身重要器官和组织输送氧气和必需营养物质需要通过阻力血管提供足够的血流。细胞内钙([Ca])和膜电位(V)调节之间的密切关系对于维持血流调节是必不可少的。特别是,Ca 激活的 K⁺(K)通道被确定为将升高的[Ca]信号转换为 V 超极化的传感器,作为降低血管阻力从而增加血流量的途径。最近的证据也支持 K 通道的反向作用,其中它们通过开放非选择性阳离子(例如,瞬时受体电位;TRP)通道促进 Ca 流入细胞内部,与强大的电(超极化)和浓度(~20,000 倍)跨膜 Ca 梯度相协调。这种安排支持 V 超极化的前馈激活,同时可能增加一氧化氮的产生。此外,在表达 TRP 通道但缺乏功能性 K 通道的血管类型(例如,收集淋巴管内皮)中,存在深远的改变,例如下游去极化离子通量和缺乏动态超极化事件。总的来说,这篇综述是一组经过精心整理的循证观点,重点关注内皮 K 和 TRP 通道在多种实验动物模型和血管类型中的作用。我们讨论了 K 和 TRP 通道之间的多种相互作用,以整合 Ca、氧化和电信号在心血管生理学和病理学中的作用。从广泛而多样化的重要发现中细胞生物物理数据的基础出发,为读者提供了一个转化叙述,以治疗和预防慢性、与年龄相关的心血管疾病。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bbb3/6471369/954574da9556/ijms-20-01380-g001.jpg

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