Carvacrol encapsulated nanocarrier/nanoemulsion abrogates angiogenesis by downregulating COX-2, VEGF and CD31 in vitro and in vivo in a lung adenocarcinoma model

被引:33
作者
Khan, Imran [1 ,3 ]
Bhardwaj, Monika [2 ,3 ]
Shukla, Shruti [4 ]
Lee, Hoomin [1 ]
Oh, Mi-Hwa [5 ]
Bajpai, Vivek K. [4 ]
Huh, Yun Suk [1 ]
Kang, Sun Chul [3 ]
机构
[1] Inha Univ, BSRC, Dept Biol Engn, 100 Inha Ro, Incheon 22212, South Korea
[2] Daegu Gyeongbuk Inst Sci & Technol, Lab Biochem & Cellular Engn, Daegu 42988, South Korea
[3] Daegu Univ, Dept Biotechnol, Gyongsan 38453, Gyeongbuk, South Korea
[4] Dongguk Univ Seoul, Dept Energy & Mat Engn, 30 Pildong Ro 1 Gil, Seoul 04620, South Korea
[5] Natl Inst Anim Sci, Anim Prod Res & Dev Div, Jeonju 54875, South Korea
基金
新加坡国家研究基金会;
关键词
Carvacrol encapsulated nanoemulsion; Angiogenesis; A549; In vivo; In silico; NF-KAPPA-B; NANOEMULSION; ACTIVATION; EXPRESSION; DELIVERY; THERAPY; DOCKING; TISSUE; CELLS; ERK;
D O I
10.1016/j.colsurfb.2019.06.016
中图分类号
Q6 [生物物理学];
学科分类号
071011 ;
摘要
Nanoemulsion-based synthesis has been introduced to enhance the bioavailability of natural compounds at target sites for their various biomedical applications. In this study, we synthesized carvacrol nanoemulsion (CN) an oil-in-water (O/W) as a nano-emulsion vehicle system by using ultrasonication emulsification for anti-angiogenesis therapy formulated by combining MCT, lecithin, and polysorbate 80 at the O/W interface called carvacrol encapsulated nanoemulsion (CEN). The diameter of CEN determined by TEM analysis was 105.32 nm. The hydrodynamic droplet size was 101.0 nm with a -39.38-mV zeta potential. The stability of the synthesized CEN was approved till 100 days without any change in diameter size distribution and encapsulation efficiency. We evaluated the role of CEN on angiogenesis in lung adenocarcinoma A549 cells both in vitro and in vivo and observed that it reduced the growth and MMP levels of A549 cells in a dose-dependent manner. Exposure to CEN decreased the activation of MAPK p38 as well as ERK. Moreover, we found that CEN reduced the expression of VEGF and CD31 in A549 cells both in vitro and in vivo. Our in-silico study also indicated the binding of carvacrol to COX-2 and VEGF at the active and allosteric sites of CD31 with low binding energy. Overall, CEN induced anti-angiogenic effects in A549 cells in vitro, in silico, and in vivo, thereby establishing its potential as targeted drug delivery vehicle against angiogenesis.
引用
收藏
页码:612 / 622
页数:11
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