Delivery Capacity and Anticancer Ability of the Berberine-Loaded Gold Nanoparticles to Promote the Apoptosis Effect in Breast Cancer.
Chen-Feng ChiuRu-Huei FuShan-Hui HsuYang-Hao Alex YuChiao-Wen LinThomas Chang-Yao TsaoKai-Bo ChangChun-An YehCheng-Ming TangSheng-Chu HuangHuey-Shan HungPublished in: Cancers (2021)
Gold nanoparticles (AuNPs) were fabricated with biocompatible collagen (Col) and then conjugated with berberine (BB), denoted as Au-Col-BB, to investigate the endocytic mechanisms in Her-2 breast cancer cell line and in bovine aortic endothelial cells (BAEC). Owing to the superior biocompatibility, tunable physicochemical properties, and potential functionalization with biomolecules, AuNPs have been well studied as carriers of biomolecules for diseases and cancer therapeutics. Composites of AuNPs with biopolymer, such as fibronectin or Col, have been revealed to increase cell proliferation, migration, and differentiation. BB is a natural compound with impressive health benefits, such as lowering blood sugar and reducing weight. In addition, BB can inhibit cell proliferation by modulating cell cycle progress and autophagy, and induce cell apoptosis in vivo and in vitro. In the current research, BB was conjugated on the Col-AuNP composite ("Au-Col"). The UV-Visible spectroscopy and infrared spectroscopy confirmed the conjugation of BB on Au-Col. The particle size of the Au-Col-BB conjugate was about 227 nm, determined by dynamic light scattering. Furthermore, Au-Col-BB was less cytotoxic to BAEC vs. Her-2 cell line in terms of MTT assay and cell cycle behavior. Au-Col-BB, compared to Au-Col, showed greater cell uptake capacity and potential cellular transportation by BAEC and Her-2 using the fluorescence-conjugated Au-Col-BB. In addition, the clathrin-mediated endocytosis and cell autophagy seemed to be the favorite endocytic mechanism for the internalization of Au-Col-BB by BAEC and Her-2. Au-Col-BB significantly inhibited cell migration in Her-2, but not in BAEC. Moreover, apoptotic cascade proteins, such as Bax and p21, were expressed in Her-2 after the treatment of Au-Col-BB. The tumor suppression was examined in a model of xenograft mice treated with Au-Col-BB nanovehicles. Results demonstrated that the tumor weight was remarkably reduced by the treatment of Au-Col-BB. Altogether, the promising findings of Au-Col-BB nanocarrier on Her-2 breast cancer cell line suggest that Au-Col-BB may be a good candidate of anticancer drug for the treatment of human breast cancer.
Keyphrases
- growth factor
- sensitive detection
- reduced graphene oxide
- recombinant human
- cell cycle
- cell proliferation
- gold nanoparticles
- endothelial cells
- oxidative stress
- healthcare
- mental health
- emergency department
- signaling pathway
- cell death
- squamous cell carcinoma
- public health
- heart failure
- single cell
- mass spectrometry
- high resolution
- visible light
- type diabetes
- high throughput
- physical activity
- social media
- cell migration
- metabolic syndrome
- coronary artery
- aortic valve
- risk assessment
- left ventricular
- pulmonary artery
- body weight
- human health
- drug release
- weight loss
- cell therapy
- drug induced
- health promotion
- replacement therapy