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Vascular and Immunobiology of the Circulatory Sphingosine 1-Phosphate Gradient

机译:循环鞘氨酸1-磷酸血管梯度的血管和免疫学

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摘要

Vertebrates are endowed with a closed circulatory system, the evolution of which required novel structural and regulatory changes. Furthermore, immune cell trafficking paradigms adapted to the barriers imposed by the closed circulatory system. How did such changes occur mechanistically? We propose that spatial compartmentalization of the lipid mediator sphingosine 1-phosphate (S1P) may be one such mechanism. In vertebrates, S1P is spatially compartmentalized in the blood and lymphatic circulation, thus comprising a sharp S1P gradient across the endothelial barrier. Circulatory S1P has critical roles in maturation and homeostasis of the vascular system as well as in immune cell trafficking. Physiological functions of S1P are tightly linked to shear stress, the key biophysical stimulus from blood flow. Thus, circulatory S1P confinement could be a primordial strategy of vertebrates in the development of a closed circulatory system. This review discusses the cellular and molecular basis of the S1P gradients and aims to interpret its physiological significance as a key feature of the closed circulatory system.
机译:脊椎动物赋予封闭的循环系统,其演进需要新颖的结构和监管变化。此外,免疫细胞运输范式适用于闭合循环系统施加的屏障。这种变化如何机械地发生?我们提出了脂质介质鞘氨醇1-磷酸(S1P)的空间分区化可以是一种这样的机制。在脊椎动物中,S1P在血液和淋巴循环中在空间上划分,因此包括穿过内皮屏障的尖锐S1P梯度。循环S1P在血管系统的成熟和稳态以及免疫细胞贩运中具有重要作用。 S1P的生理功能与剪切应力紧密相关,血流的关键生物物理刺激。因此,循环S1P限制可能是脊椎动物在封闭循环系统开发中的原始策略。本综述讨论了S1P梯度的细胞和分子基础,并旨在将其生理意义解释为封闭循环系统的关键特征。

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