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心房利钠肽和脑利钠肽对集合淋巴管渗透性和收缩反应的影响。

Permeability and contractile responses of collecting lymphatic vessels elicited by atrial and brain natriuretic peptides.

机构信息

V. H. Huxley: Department of Medical Pharmacology and Physiology, University of Missouri School of Medicine, 1 Hospital Dr., MA415, Columbia, MO 65212, USA.

出版信息

J Physiol. 2013 Oct 15;591(20):5071-81. doi: 10.1113/jphysiol.2013.260042. Epub 2013 Jul 29.

Abstract

Atrial and brain natriuretic peptides (ANP and BNP, respectively) are cardiac hormones released into the bloodstream in response to hypervolaemia or fluid shifts to the central circulation. The actions of both peptides include natriuresis and diuresis, a decrease in systemic blood pressure, and inhibition of the renin-angiotensin-aldosterone system. Further, ANP and BNP elicit increases in blood microvessel permeability sufficient to cause protein and fluid extravasation into the interstitium to reduce the vascular volume. Given the importance of the lymphatic vasculature in maintaining fluid balance, we tested the hypothesis that ANP or BNP (100 nM) would likewise elevate lymphatic permeability (Ps) to serum albumin. Using a microfluorometric technique adapted to in vivo lymphatic vessels, we determined that rat mesenteric collecting lymphatic Ps to rat serum albumin increased by 2.0 ± 0.4-fold (P = 0.01, n = 7) and 2.7 ± 0.8-fold (P = 0.07, n = 7) with ANP and BNP, respectively. In addition to measuring Ps responses, we observed changes in spontaneous contraction amplitude and frequency from the albumin flux tracings in vivo. Notably, ANP abolished spontaneous contraction amplitude (P = 0.005) and frequency (P = 0.006), while BNP augmented both parameters by ∼2-fold (P < 0.01 each). These effects of ANP and BNP on contractile function were examined further by using an in vitro assay. In aggregate, these data support the theory that an increase in collecting lymphatic permeability opposes the absorptive function of the lymphatic capillaries, and aids in the retention of protein and fluid in the interstitial space to counteract volume expansion.

摘要

心房利钠肽和脑利钠肽(分别为 ANP 和 BNP)是心脏激素,在血容量增加或液体转移到中心循环时释放到血液中。这两种肽的作用包括利钠和利尿、降低全身血压以及抑制肾素-血管紧张素-醛固酮系统。此外,ANP 和 BNP 引起的血液微血管通透性增加足以导致蛋白质和液体渗出到间质中,以减少血管容量。鉴于淋巴血管系统在维持液体平衡方面的重要性,我们测试了以下假设:ANP 或 BNP(100 nM)同样会增加淋巴对白蛋白的通透性(Ps)。我们使用适应于体内淋巴管的微荧光技术,确定大鼠肠系膜收集淋巴管对大鼠血清白蛋白的 Ps 分别增加了 2.0±0.4 倍(P=0.01,n=7)和 2.7±0.8 倍(P=0.07,n=7)。除了测量 Ps 反应外,我们还观察到白蛋白通量追踪记录中自发收缩幅度和频率的变化。值得注意的是,ANP 完全消除了自发收缩幅度(P=0.005)和频率(P=0.006),而 BNP 则将这两个参数分别增加了约 2 倍(P<0.01)。通过使用体外测定法进一步检查了 ANP 和 BNP 对收缩功能的这些影响。总的来说,这些数据支持这样一种理论,即收集淋巴管通透性的增加与淋巴毛细血管的吸收功能相反,并有助于保留间质空间中的蛋白质和液体,以抵消体积扩张。

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