Hwang In-Hu, Kwon Yong-Kyun, Cho Chong-Kwan, Lee Yeon-Weol, Sung Jung-Suk, Joo Jong-Cheon, Lee Kyung-Bok, Yoo Hwa-Seung, Jang Ik-Soon
* Department of Physiology, Korea University College of Medicine, Seoul 136-705, Republic of Korea.
† East-West Cancer Center, Daejeon University, Daejeon 302-120, Republic of Korea.
Am J Chin Med. 2016;44(5):1081-97. doi: 10.1142/S0192415X16500609. Epub 2016 Jul 19.
Urokinase receptor (uPAR) is enhanced in many human cancer cells and is frequently an indicator of poor prognosis. Activation of [Formula: see text]1-integrin requires caveolin-1 and is regulated by uPAR. However, the underlying molecular mechanism responsible for the interaction between uPAR and [Formula: see text]1-integrin remains obscure. We found that modified regular Panax ginseng extract (MRGX) had a negative modulating effect on the uPAR/[Formula: see text]1-integrin interaction, disrupted the uPAR/integrin interaction by modulating caveoline-1, and caused early apoptosis in cancer cells. Additionally, we found that siRNA-mediated caveoline-1 downregulation inhibited uPAR-mediated [Formula: see text]1-integrin signaling, whereas caveoline-1 up-regulation stimulated the signaling, which suppressed p53 expression, thereby indicating negative crosstalk exists between the integrin [Formula: see text]1 and the p53 pathways. Thus, these findings identify a novel mechanism whereby the inhibition of [Formula: see text]1 integrin and the activation of p53 modulate the expression of the anti-apoptotic proteins that are crucially involved in inducing apoptosis in A549 lung cancer cells. Furthermore, MRGX causes changes in the expressions of members of the Bcl-2 family (Bax and Bcl-2) in a pro-apoptotic manner. In addition, MGRX-mediated inhibition of [Formula: see text]1 integrin attenuates ERK phosphorylation (p-ERK), which up-regulates caspase-8 and Bax. Therefore, ERK may affect mitochondria through a negative regulation of caspase-8 and Bax. Taken together, these findings reveal that MRGX is involved in uPAR-[Formula: see text]1-integrin signaling by modulating caveolin-1 signaling to induce early apoptosis in A549 lung-cancer cells and strongly indicate that MRGX might be useful as a herbal medicine and may lead to the development of new herbal medicine that would suppress the growth of lung-cancer cells.
尿激酶受体(uPAR)在许多人类癌细胞中表达增强,且常常是预后不良的一个指标。α1整合素的激活需要小窝蛋白-1,并受uPAR调控。然而,uPAR与α1整合素之间相互作用的潜在分子机制仍不清楚。我们发现,改良的普通人参提取物(MRGX)对uPAR/α1整合素的相互作用具有负调节作用,通过调节小窝蛋白-1破坏uPAR/整合素的相互作用,并导致癌细胞早期凋亡。此外,我们发现,小干扰RNA介导的小窝蛋白-1下调抑制了uPAR介导的α1整合素信号传导,而小窝蛋白-1上调则刺激了该信号传导,进而抑制了p53表达,这表明整合素α1与p53信号通路之间存在负性串扰。因此,这些发现确定了一种新机制,即α1整合素的抑制和p53的激活调节抗凋亡蛋白的表达,这些蛋白在诱导A549肺癌细胞凋亡中起关键作用。此外,MRGX以促凋亡方式引起Bcl-2家族成员(Bax和Bcl-2)表达的变化。另外,MRGX介导的α1整合素抑制减弱了ERK磷酸化(p-ERK),从而上调了半胱天冬酶-8和Bax。因此,ERK可能通过对半胱天冬酶-8和Bax的负调节影响线粒体。综上所述,这些发现揭示MRGX通过调节小窝蛋白-1信号传导参与uPAR-α1整合素信号传导,从而诱导A549肺癌细胞早期凋亡,并有力表明MRGX可能作为一种草药有用,且可能会促成抑制肺癌细胞生长的新草药的开发。
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