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体内测定收集淋巴管对白蛋白的通透性:淋巴管在交换中的作用。

In vivo determination of collecting lymphatic vessel permeability to albumin: a role for lymphatics in exchange.

机构信息

Department of Medical Pharmacology & Physiology, University of Missouri School of Medicine, Columbia, MO 65212, USA.

出版信息

J Physiol. 2010 Jan 1;588(Pt 1):243-54. doi: 10.1113/jphysiol.2009.179622. Epub 2009 Nov 16.

Abstract

While it is well established that the lymphatic vasculature is central to fluid and solute homeostasis, how it accomplishes this task is not well defined. To clarify the basic mechanisms underlying basal fluid and solute homeostasis, we assessed permeability to rat serum albumin (P(RSA)(s)) in mesenteric collecting lymphatic vessels and venules of juvenile male rats. Using the quantitative microfluorometric technique originally developed for blood capillaries, we tested the hypothesis that as a consequence of venules and collecting lymphatics sharing a common embryological origin, their P(RSA)(s) would not differ significantly. Supporting our hypothesis, the median collecting lymphatic P(RSA)(s) (3.5 +/- 1.0 x 10(7) cm s(-1), N = 22) did not differ significantly from the median venular P(RSA)(s) (4.0 +/- 1.0 x 10(7) cm s(-1), N = 8, P = 0.61). For collecting lymphatics the diffusive permeability (P(d) = 2.5 x 10(7) cm s(-1)) was obtained from the relationship of apparent P(RSA)(s) and pressure. While the measured P(RSA)(s), P(d) and estimated hydraulic conductivity of collecting lymphatics and venules were similar, the contribution of convective coupling differs as a result of the higher hydrostatic pressure experienced by venules relative to collecting lymphatics in vivo. In summary, the data demonstrate the capacity for collecting lymphatics to act as exchange vessels, able to extravasate solute and filter fluid. As a consequence these data provide experimental support for the theory that prenodal lymphatic vessels concentrate intraluminal protein.

摘要

虽然淋巴管系统对液体和溶质的稳态至关重要,但它如何完成这一任务还没有明确界定。为了阐明基础液体和溶质稳态的基本机制,我们评估了幼年雄性大鼠肠系膜收集淋巴管和小静脉对大鼠血清白蛋白的通透性(P(RSA)(s))。我们使用最初为血液毛细血管开发的定量微荧光技术,测试了以下假设:由于小静脉和收集淋巴管具有共同的胚胎起源,它们的 P(RSA)(s) 不会有显著差异。支持我们的假设,收集淋巴管的中位数 P(RSA)(s)(3.5 +/- 1.0 x 10(7) cm s(-1),N = 22)与小静脉的中位数 P(RSA)(s)(4.0 +/- 1.0 x 10(7) cm s(-1),N = 8,P = 0.61)没有显著差异。对于收集淋巴管,扩散通透性(P(d) = 2.5 x 10(7) cm s(-1))是从表观 P(RSA)(s) 和压力的关系中获得的。虽然测量的 P(RSA)(s)、P(d)和估计的收集淋巴管和小静脉的水力传导率相似,但由于小静脉在体内比收集淋巴管承受更高的静水压力,对流耦合的贡献不同。总之,这些数据表明收集淋巴管有能力作为交换血管,能够渗出溶质和过滤液体。因此,这些数据为理论提供了实验支持,即前淋巴结淋巴管浓缩管腔内的蛋白质。

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