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缺氧选择性地诱导新生牛肺动脉中膜平滑肌细胞特定亚群的增殖。

Hypoxia selectively induces proliferation in a specific subpopulation of smooth muscle cells in the bovine neonatal pulmonary arterial media.

作者信息

Wohrley J D, Frid M G, Moiseeva E P, Orton E C, Belknap J K, Stenmark K R

机构信息

Developmental Lung Biology Laboratory, University of Colorado Health Sciences Center, Denver 80262, USA.

出版信息

J Clin Invest. 1995 Jul;96(1):273-81. doi: 10.1172/JCI118031.

Abstract

Medial thickening of the pulmonary arterial wall, secondary to smooth muscle cell (SMC) hyperplasia, is commonly observed in neonatal hypoxic pulmonary hypertension. Because recent studies have demonstrated the existence of multiple phenotypically distinct SMC populations within the arterial media, we hypothesized that these SMC subpopulations would differ in their proliferative responses to hypoxic pulmonary hypertension and thus contribute in selective ways to the vascular remodeling process. Expression of meta-vinculin, a muscle-specific cytoskeletal protein, has been shown to reliably distinguish two unique SMC subpopulations within the bovine pulmonary arterial media. Therefore, to assess the proliferative responses of phenotypically distinct SMC subpopulations in the setting of neonatal pulmonary hypertension, we performed double immunofluorescence staining on pulmonary artery cryosections from control and hypertensive calves with antibodies against meta-vinculin and the proliferation-associated nuclear antigen, Ki-67. We found that, although neonatal pulmonary hypertension caused significant increases in overall cell replication, proliferation occurred almost exclusively in one, the meta-vinculin-negative SMC population, but not the other SMC population expressing meta-vinculin. We also examined fetal pulmonary arteries, where proliferative rates were high and meta-vinculin expression again reliably distinguished two SMC subpopulations. In contrast to the hypertensive neonate, we found in the fetus that the relative proliferative rates of both SMC subpopulations were equal, thus suggesting the existence of different mechanisms controlling proliferation and expression of cytoskeletal proteins in the fetus and neonate. We conclude that phenotypically distinct SMC populations in the bovine arterial media exhibit specific and selective proliferative responses to neonatal pulmonary hypertension. Distinct SMC subpopulations may, thus, contribute in unique ways to vascular homeostasis under both normal and pathologic conditions.

摘要

肺动脉壁的内侧增厚继发于平滑肌细胞(SMC)增生,这在新生儿缺氧性肺动脉高压中很常见。由于最近的研究表明动脉中膜内存在多个表型不同的SMC群体,我们推测这些SMC亚群对缺氧性肺动脉高压的增殖反应会有所不同,从而以选择性方式促进血管重塑过程。已证明肌特异性细胞骨架蛋白间α-辅肌动蛋白的表达能够可靠地区分牛肺动脉中膜内两个独特的SMC亚群。因此,为了评估新生儿肺动脉高压情况下表型不同的SMC亚群的增殖反应,我们用抗间α-辅肌动蛋白和增殖相关核抗原Ki-67的抗体对对照和高血压犊牛的肺动脉冰冻切片进行了双重免疫荧光染色。我们发现,虽然新生儿肺动脉高压导致总体细胞复制显著增加,但增殖几乎只发生在一个间α-辅肌动蛋白阴性的SMC群体中,而表达间α-辅肌动蛋白的另一个SMC群体则没有增殖。我们还检查了胎儿肺动脉,其增殖率很高,间α-辅肌动蛋白表达再次可靠地区分了两个SMC亚群。与高血压新生儿不同,我们在胎儿中发现两个SMC亚群的相对增殖率相等,这表明胎儿和新生儿中控制增殖和细胞骨架蛋白表达的机制不同。我们得出结论,牛动脉中膜内表型不同的SMC群体对新生儿肺动脉高压表现出特定和选择性的增殖反应。因此,不同的SMC亚群可能在正常和病理条件下以独特方式促进血管稳态。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/031f/185198/54ad6987ae1c/jcinvest00013-0293-a.jpg

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