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正常和肿瘤血管网络的结构适应性。

Structural adaptation of normal and tumour vascular networks.

机构信息

Department of Physiology, University of Arizona, Tucson, AZ 85724, USA.

出版信息

Basic Clin Pharmacol Toxicol. 2012 Jan;110(1):63-9. doi: 10.1111/j.1742-7843.2011.00815.x. Epub 2011 Nov 9.

Abstract

Vascular networks are dynamic structures, adapting to changing conditions by structural remodelling of vessel diameters and by growth of new vessels and regression of existing vessels. The vast number of blood vessels in the circulatory system, more than 10⁹, implies that vessels' arrangement and structure are not under individual genetic control but emerge as a result of generic responses of each segment to the various stimuli that it experiences. To obtain insight into the types of response that are needed, a network-oriented approach has been used, in which theoretical models are used to simulate structural adaptation in vascular networks, and the results are compared with experimental observations. With regard to the structural control of vessel diameters, this approach shows that responses to both haemodynamic and metabolic stimuli are needed for the formation of functionally adequate and efficient network structures. Furthermore, information transfer in both upstream and downstream directions is essential for balancing flows between long and short flow pathways. Otherwise, functional shunting occurs, that is, short pathways become enlarged and flow bypasses longer pathways. Information transfer in the upstream direction is achieved by conducted responses communicated along vessel walls. Simulations of structural adaptation in tumour microvascular networks indicate that impaired vascular communication, resulting in functional shunting, may be an important factor causing the dysfunctional microcirculation and local hypoxia typically observed in tumours. Anti-angiogenic treatment of tumours may restore vascular communication and thereby improve or normalize flow distribution in tumour vasculature.

摘要

血管网络是动态结构,通过血管直径的结构重塑以及新血管的生长和现有血管的退化来适应不断变化的条件。循环系统中大量的血管(超过 10^9)意味着血管的排列和结构不受个体遗传控制,而是作为每个节段对其经历的各种刺激的通用反应而出现的。为了深入了解所需的反应类型,采用了面向网络的方法,其中使用理论模型来模拟血管网络的结构适应,并且将结果与实验观察进行比较。关于血管直径的结构控制,该方法表明,需要对血液动力学和代谢刺激做出反应,才能形成功能上适当和有效的网络结构。此外,上下游的信息传递对于平衡长路径和短路径之间的流量是必不可少的。否则,会发生功能分流,即短路径扩大,而流量绕过较长的路径。上游方向的信息传递是通过沿着血管壁传递的传导反应来实现的。肿瘤微血管网络结构适应性的模拟表明,血管通讯受损导致功能分流,可能是导致肿瘤中通常观察到的功能失调微循环和局部缺氧的重要因素。肿瘤的抗血管生成治疗可能恢复血管通讯,从而改善或使肿瘤血管中的血流分布正常化。

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