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心肌前毛细血管小动脉和后毛细血管小静脉的壁结构在体外进行了重新检查和重建,以便研究屏障功能。

Wall structures of myocardial precapillary arterioles and postcapillary venules reexamined and reconstructed in vitro for studies on barrier functions.

机构信息

Department of Physiology, University of Munich, Germany.

出版信息

Am J Physiol Heart Circ Physiol. 2012 Jan 1;302(1):H51-68. doi: 10.1152/ajpheart.00358.2011. Epub 2011 Oct 7.

DOI:10.1152/ajpheart.00358.2011
PMID:21984546
Abstract

The barrier functions of myocardial precapillary arteriolar and postcapillary venular walls (PCA or PCV, respectively) are of considerable scientific and clinical interest (regulation of blood flow and recruitment of immune defense). Using enzyme histochemistry combined with confocal microscopy, we reexamined the cell architecture of human PCA and PVC and reconstructed appropriate in vitro models for studies of their barrier functions. Contrary to current opinion, the PCA endothelial tube is encompassed not by smooth muscle cells but rather by a concentric layer of pericytes cocooned in a thick, microparticle-containing extracellular matrix (ECM) that contributes substantially to the tightness of the arteriolar wall. This core tube extends upstream into the larger arterioles, there additionally enwrapped by smooth muscle. PCV consist of an inner layer of large, contractile endothelial cells encompassed by a fragile, wide-meshed pericyte network with a weakly developed ECM. Pure pericyte and endothelial cell preparations were isolated from PCA and PCV and grown in sandwich cultures. These in vitro models of the PCA and PCV walls exhibited typical histological and functional features. In both plasma-like (PLM) and serum-containing (SCM) media, the PCA model (including ECM) maintained its low hydraulic conductivity (L(P) = 3.24 ± 0.52·10(-8)cm·s(-1)·cmH(2)O(-1)) and a high selectivity index for transmural passage of albumin (SI(Alb) = 0.95 ± 0.02). In contrast, L(P) and SI(Alb) in the PCV model (almost no ECM) were 2.55 ± 0.32·10(-7)cm·s(-1)·cmH(2)O(-1) and 0.88 ± 0.03, respectively, in PLM, and 1.39 ± 0.10·10(-6)cm·s(-1)·cmH(2)O(-1) and 0.49 ± 0.04 in SCM. With the use of these models, systematic, detailed studies on the regulation of microvascular barrier properties now appear to be feasible.

摘要

心肌毛细血管前小动脉和后小静脉壁(分别为 PCA 或 PCV)的屏障功能具有重要的科学和临床意义(调节血流和招募免疫防御)。我们使用酶组织化学结合共聚焦显微镜,重新检查了人类 PCA 和 PVC 的细胞结构,并重建了适当的体外模型,以研究它们的屏障功能。与当前的观点相反,PCA 内皮管不是由平滑肌细胞包围,而是由被包裹在富含微粒的细胞外基质(ECM)中的同心层周细胞包围,该 ECM 对小动脉壁的紧密性有很大贡献。这个核心管延伸到上游较大的小动脉,在那里还有平滑肌包裹。PCV 由内层大的、可收缩的内皮细胞组成,被脆弱的、网孔宽大的周细胞网络包围,周细胞网络的 ECM 发育不良。从 PCA 和 PCV 中分离出纯周细胞和内皮细胞,并在三明治培养物中培养。这些 PCA 和 PCV 壁的体外模型表现出典型的组织学和功能特征。在血浆样(PLM)和含血清(SCM)培养基中,PCA 模型(包括 ECM)保持低水力传导率(L(P) = 3.24 ± 0.52·10(-8)cm·s(-1)·cmH(2)O(-1))和白蛋白跨壁通透性的高选择性指数(SI(Alb) = 0.95 ± 0.02)。相比之下,PCV 模型中的 L(P)和 SI(Alb)(几乎没有 ECM)分别为 2.55 ± 0.32·10(-7)cm·s(-1)·cmH(2)O(-1)和 0.88 ± 0.03 在 PLM 中,以及 1.39 ± 0.10·10(-6)cm·s(-1)·cmH(2)O(-1)和 0.49 ± 0.04 在 SCM 中。使用这些模型,对微血管屏障特性的调节进行系统、详细的研究现在似乎是可行的。

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