在人肺微血管内皮细胞中,JNK激活需要TNF-α对Rho激酶的激活。
Activation of Rho kinase by TNF-alpha is required for JNK activation in human pulmonary microvascular endothelial cells.
作者信息
Mong Phyllus Y, Petrulio Christian, Kaufman Howard L, Wang Qin
机构信息
Tumor Immunology Laboratory, Division of Surgical Oncology, Department of Surgery, Columbia University, New York, NY 10032, USA.
出版信息
J Immunol. 2008 Jan 1;180(1):550-8. doi: 10.4049/jimmunol.180.1.550.
TNF-alpha induces complex signaling events in endothelial cells (ECs), leading to inflammatory gene transcription and junctional permeability increases. This study examined the activation of RhoA and Rho kinase induced by TNF-alpha in primary human pulmonary microvascular ECs and its role in regulating EC responses to TNF-alpha. TNF-alpha induced a time-dependent activation of RhoA and Rho kinase in these ECs. TNF-alpha also induced activation of JNK that peaked at 15 min and lasted for at least 3 h. Inhibition of Rho kinase using a specific pharmacological inhibitor, Y27632, prevented TNF-alpha-induced early and late JNK activation. Inhibition of RhoA protein expression using small-interfering RNA, however, did not prevent TNF-alpha-induced Rho kinase activation or JNK activation. Studies using MAPK kinase 4 (MKK4) small-interfering RNA showed that MKK4 was not required for TNF-alpha-induced early JNK activation and that Rho kinase modulated early JNK activation through MKK4-independent mechanisms. Rho kinase, however, modulated TNF-alpha-induced late JNK activation mainly through MKK4-dependent mechanisms. Activation of Rho kinase was required for JNK-dependent IL-6 secretion induced by TNF-alpha. Moreover, inhibition of Rho kinase prevented TNF-alpha-induced cytoskeletal changes and permeability increases. Inhibition of JNK activation, however, did not prevent TNF-alpha-induced cytoskeletal changes, suggesting that Rho kinase did not modulate cytoskeletal changes through JNK activation. Therefore, Rho kinase plays important roles in EC responses to TNF-alpha by regulating permeability increases and JNK-dependent IL-6 production during pulmonary inflammation.
肿瘤坏死因子-α(TNF-α)在内皮细胞(ECs)中诱导复杂的信号转导事件,导致炎症基因转录和连接通透性增加。本研究检测了TNF-α在原代人肺微血管内皮细胞中诱导的RhoA和Rho激酶的激活及其在调节内皮细胞对TNF-α反应中的作用。TNF-α在这些内皮细胞中诱导RhoA和Rho激酶的时间依赖性激活。TNF-α还诱导JNK激活,在15分钟时达到峰值并持续至少3小时。使用特异性药理抑制剂Y27632抑制Rho激酶,可阻止TNF-α诱导的早期和晚期JNK激活。然而,使用小干扰RNA抑制RhoA蛋白表达并不能阻止TNF-α诱导的Rho激酶激活或JNK激活。使用丝裂原活化蛋白激酶激酶4(MKK4)小干扰RNA的研究表明,TNF-α诱导的早期JNK激活不需要MKK4,并且Rho激酶通过不依赖MKK4的机制调节早期JNK激活。然而,Rho激酶主要通过依赖MKK4的机制调节TNF-α诱导的晚期JNK激活。TNF-α诱导的JNK依赖性白细胞介素-6分泌需要Rho激酶的激活。此外,抑制Rho激酶可阻止TNF-α诱导的细胞骨架变化和通透性增加。然而,抑制JNK激活并不能阻止TNF-α诱导的细胞骨架变化,这表明Rho激酶不是通过JNK激活来调节细胞骨架变化的。因此,在肺部炎症过程中,Rho激酶通过调节通透性增加和JNK依赖性白细胞介素-6的产生,在内皮细胞对TNF-α的反应中发挥重要作用。
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