生长因子、细胞因子和细胞外基质蛋白对人血管平滑肌细胞中纤连蛋白产生的影响。

The effect of growth factors, cytokines, and extracellular matrix proteins on fibronectin production in human vascular smooth muscle cells.

作者信息

Kaiura T L, Itoh H, Kubaska S M, McCaffrey T A, Liu B, Kent K C

机构信息

Department of Surgery, Division of Vascular Surgery, New York Hospital/Cornell University Medical Center, NY 10021, USA.

出版信息

J Vasc Surg. 2000 Mar;31(3):577-84.

PMID:10709072

Abstract

PURPOSE

Although 60% to 80% of the mature intimal hyperplastic plaque is composed of extracellular matrix (ECM) proteins, little is known about the factors that stimulate smooth muscle cells (SMCs) to produce these proteins. A major component of the ECM protein is fibronectin. Thus we studied fibronectin production and its response to various growth factors, cytokines, and other ECM proteins that are released at the time of vascular injury.

METHODS

Quiescent cultured human SMCs were stimulated for varying intervals with increasing concentrations of agonist. Fibronectin in the cell medium was assayed by immunoblotting with a fibronectin-specific antibody.

RESULTS

After 72 hours of stimulation, transforming growth factor-beta (10 ng/mL) had the most profound effect on fibronectin production (9.6- +/- 2.1-fold; P <.05), followed by epidermal growth factor (100 ng/mL; 5.0- +/- 0.1-fold; P <.05, for both). Surprisingly, the platelet-derived growth factors (AA, AB, and BB) and fibroblast growth factor did not stimulate fibronectin production. Among the matrix proteins studied, only collagen type I (20 microg/mL) stimulated fibronectin production (1.9- +/- 0.1-fold; P <.05), whereas collagen type IV and laminin had no effect. The contractile protein angiotensin II (100 ng/mL) was a weak stimulant of fibronectin (1.6- +/- 0.2-fold; P <.05). Time course studies of fibronectin production up to 72 hours revealed kinetics that varied with each agonist. Transforming growth factor-beta stimulated significant early production of fibronectin, whereas fibronectin production in response to epidermal growth factor and collagen type I was initially modest but increased with time. The effect of angiotensin II did not become evident until 72 hours.

CONCLUSION

Cytokines, growth factors, and matrix proteins have varying quantitative effects on ECM protein production by human vascular SMCs. Knowledge of the factors that influence ECM protein production may allow for the design of specific inhibitors that can prevent intimal hyperplasia.

摘要

目的

尽管60%至80%的成熟内膜增生斑块由细胞外基质（ECM）蛋白组成，但对于刺激平滑肌细胞（SMC）产生这些蛋白的因素却知之甚少。ECM蛋白的一个主要成分是纤连蛋白。因此，我们研究了纤连蛋白的产生及其对血管损伤时释放的各种生长因子、细胞因子和其他ECM蛋白的反应。

方法

用浓度递增的激动剂对静止培养的人SMC进行不同时间间隔的刺激。通过用纤连蛋白特异性抗体进行免疫印迹法测定细胞培养基中的纤连蛋白。

结果

刺激72小时后，转化生长因子-β（10 ng/mL）对纤连蛋白产生的影响最为显著（9.6±2.1倍；P<.05），其次是表皮生长因子（100 ng/mL；5.0±0.1倍；P<.05）。令人惊讶的是，血小板衍生生长因子（AA、AB和BB）和成纤维细胞生长因子并未刺激纤连蛋白的产生。在所研究的基质蛋白中，只有I型胶原（20 μg/mL）刺激了纤连蛋白的产生（1.9±0.1倍；P<.05），而IV型胶原和层粘连蛋白则无作用。收缩蛋白血管紧张素II（100 ng/mL）是纤连蛋白的弱刺激剂（1.6±0.2倍；P<.05）。对长达72小时的纤连蛋白产生进行的时间进程研究显示，每种激动剂的动力学各不相同。转化生长因子-β刺激纤连蛋白显著早期产生，而对表皮生长因子和I型胶原的反应中，纤连蛋白产生最初适度但随时间增加。血管紧张素II的作用直到72小时才变得明显。