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血小板衍生生长因子与成年肺微血管壁重塑:在肺动脉高压中发育的祖代平滑肌细胞中对血小板衍生生长因子受体β和血小板衍生生长因子-BB分子进行成像

PDGF and microvessel wall remodeling in adult lung: imaging PDGF-Rbeta and PDGF-BB molecules in progenitor smooth muscle cells developing in pulmonary hypertension.

作者信息

Jones Rosemary, Capen Diane, Jacobson Margaretha

机构信息

Department of Anesthesia and Critical Care, Harvard Medical School and Massachusetts General Hospital, Boston, Massachusetts 02129, USA.

出版信息

Ultrastruct Pathol. 2006 Jul-Aug;30(4):267-81. doi: 10.1080/01913120600820336.

DOI:10.1080/01913120600820336
PMID:16971352
Abstract

Smooth muscle cells are relatively rare cells in the microvessels of the normal adult lung but develop in high numbers in the clinical pulmonary hypertensions (PHs). Understanding this cellular response has profound implications for determining the pathogenesis of PH, and for the development of therapeutic strategies, yet little is known of the angiogenic molecules responsible. The authors have previously shown that interstitial fibroblasts, and intermediate cells, are the progenitors of smooth muscle cells developing in adult lung microvessels in an in vivo model of experimental PH. The present study evaluates PDGF-Rbeta/PDGF-BB, an important angiogenic signaling pathway, using antibodies linked to protein A-gold (pA-AU) and quantitative high-resolution imaging techniques to detect expression by these cells. Each progenitor cell type in the control lung expressed PDGF-Rbeta and PDGF-BB. In the hypertensive lung, PDGF-Rbeta was highly expressed by fibroblasts developing as perivascular cells, the mean number of pA-AU labeled antigenic sites per cell profile, and their density (microm(-2)), increasing with time: in intermediate cells the mean number of sites per cell profile, although not their density (microm(-2)), also increased with time but less so than in the fibroblasts. In clear contrast to the RTK, constitutive expression levels of PDGF-BB were low in each progenitor cell type and remained restricted in the hypertensive lung.

摘要

平滑肌细胞在正常成年肺微血管中相对少见,但在临床肺动脉高压(PH)中大量出现。了解这种细胞反应对于确定PH的发病机制以及开发治疗策略具有深远意义,但对于负责的血管生成分子却知之甚少。作者先前已经表明,在实验性PH的体内模型中,间质成纤维细胞和中间细胞是成年肺微血管中发育的平滑肌细胞的祖细胞。本研究使用与蛋白A-金(pA-AU)偶联的抗体和定量高分辨率成像技术来检测这些细胞的表达,评估重要的血管生成信号通路PDGF-Rβ/PDGF-BB。对照肺中的每种祖细胞类型均表达PDGF-Rβ和PDGF-BB。在高血压肺中,作为血管周围细胞发育的成纤维细胞高度表达PDGF-Rβ,每个细胞轮廓的pA-AU标记抗原位点的平均数及其密度(μm-2)随时间增加:在中间细胞中,每个细胞轮廓的位点平均数虽然其密度(μm-2)没有增加,但也随时间增加,但比成纤维细胞增加得少。与RTK形成鲜明对比的是,每种祖细胞类型中PDGF-BB的组成型表达水平较低,并且在高血压肺中仍然受到限制。

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