研究目的
To develop zinc oxide nanocarriers with ginsenoside by green synthesis for improving water dispersibility, stability, and therapeutic effect as effective anticancer agents.
研究成果
Rh2HAZnO induces apoptosis and DNA damage in lung, colon, and breast cancer cells through activation of the caspase-9 pathway and effects on Caspase-9/p38 MAPK markers for anticancer activity.
研究不足
The study is limited to in vitro experiments; further in vivo experimental analysis is required to confirm the potential antitumor agent against various cancer cells.
1:Experimental Design and Method Selection:
Zinc oxide (ZnO) nanocomposites functionalized by hyaluronic acid (HA) were prepared by a co-precipitation method and further functionalized with ginsenoside Rh
2:Sample Selection and Data Sources:
Human cancer cell lines (A549, MCF-7, and HT29) and normal human keratinocytes (HaCaTs) were used.
3:List of Experimental Equipment and Materials:
Included SEM, FE-TEM, XRD, zeta potential and hydrodynamic particle size of nanocomposites, and FTIR spectroscopy.
4:Experimental Procedures and Operational Workflow:
Included MTT assay, ROS generation measurement, apoptosis detection, qRT-PCR, and Western blotting.
5:Data Analysis Methods:
Statistical significance was evaluated by one-way ANOVA and Student’s t-test.
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SEM
Characterization of nanoparticles
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FE-TEM
Characterization of nanoparticles
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XRD
Characterization of nanoparticles
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FTIR spectroscopy
Characterization of nanoparticles
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MTT assay
Evaluation of toxicity in cancer cells
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ROS staining
Measurement of intracellular reactive oxygen species
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Hoechst staining
Detection of apoptotic cells
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qRT-PCR
Analysis of gene expression
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Western blotting
Analysis of protein expression
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