Mano Sharmy Saimon, Kanehira Koki, Taniguchi Akiyoshi
Cell-Materials Interaction Group, Biomaterials Unit, Nano-Life Field, International Center for Materials Nanoarchitectonics (MANA), National Institute for Materials Science, 1-1, Namiki, Tsukuba, Ibaraki 305-0044, Japan.
Int J Mol Sci. 2013 Jun 26;14(7):13154-70. doi: 10.3390/ijms140713154.
The innate immune response is the earliest cellular response to infectious agents and mediates the interactions between microbes and cells. Toll-like receptors (TLRs) play an important role in these interactions. We have already shown that TLRs are involved with the uptake of titanium dioxide nanoparticles (TiO2 NPs) and promote inflammatory responses. In this paper, we compared role of cellular uptake and inflammatory response via TLR 4 to lipopolysaccharide (LPS) and TiO2 NPs. In the case of LPS, LPS binds to LPS binding protein (LBP) and CD 14, and then this complex binds to TLR 4. In the case of TiO2 NPs, the necessity of LBP and CD 14 to induce the inflammatory response and for uptake by cells was investigated using over-expression, antibody blocking, and siRNA knockdown experiments. Our results suggested that for cellular uptake of TiO2 NPs, TLR 4 did not form a complex with LBP and CD 14. In the TiO2 NP-mediated inflammatory response, TLR 4 acted as the signaling receptor without protein complex of LPS, LBP and CD 14. The results suggested that character of TiO2 NPs might be similar to the complex of LPS, LBP and CD 14. These results are important for development of safer nanomaterials.
先天性免疫反应是对感染因子最早的细胞反应,并介导微生物与细胞之间的相互作用。Toll样受体(TLR)在这些相互作用中起重要作用。我们已经表明,TLR参与二氧化钛纳米颗粒(TiO2 NPs)的摄取并促进炎症反应。在本文中,我们比较了通过TLR 4对脂多糖(LPS)和TiO2 NPs的细胞摄取和炎症反应的作用。对于LPS,LPS与LPS结合蛋白(LBP)和CD 14结合,然后该复合物与TLR 4结合。对于TiO2 NPs,使用过表达、抗体阻断和siRNA敲低实验研究了LBP和CD 14对诱导炎症反应和细胞摄取的必要性。我们的结果表明,对于TiO2 NPs的细胞摄取,TLR 4未与LBP和CD 14形成复合物。在TiO2 NP介导的炎症反应中,TLR 4作为信号受体,不存在LPS、LBP和CD 14的蛋白复合物。结果表明,TiO2 NPs的特性可能与LPS、LBP和CD 14的复合物相似。这些结果对于开发更安全的纳米材料很重要。
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