研究目的
To compare two types of ovarian cancer orthotopic xenograft (OCOX) mouse models, i.e. cellular orthotopic injection (COI) and surgical orthotopic implantation (SOI), regarding xenograft formation rate, in vivo imaging, tumor growth and metastasis, and tumor microenvironment.
研究成果
SOI is a feasible and reliable technique to establish OCOX mouse models that mimic the clinical process of ovarian cancer growth and metastasis more accurately than COI, despite being more technically challenging.
研究不足
The study acknowledges that SOI is more technically difficult and time-consuming than COI, which may limit its applicability in some research settings.
1:Experimental Design and Method Selection:
The study compared COI and SOI methods for establishing OCOX mouse models using ovarian cancer cell lines ES2 and SKOV3. Tumor formation and progression were monitored by bioluminescent in vivo imaging. Cell proliferation and migration abilities were detected by EdU and scratch assays, respectively. Expression of various markers in tumor samples was detected by immunohistochemistry.
2:Tumor formation and progression were monitored by bioluminescent in vivo imaging. Cell proliferation and migration abilities were detected by EdU and scratch assays, respectively. Expression of various markers in tumor samples was detected by immunohistochemistry.
Sample Selection and Data Sources:
2. Sample Selection and Data Sources: Female Balb/c-nu/nu mice were used, and tumor cells were implanted either by COI or SOI methods. Tumor growth and metastasis were monitored using in vivo imaging.
3:List of Experimental Equipment and Materials:
In vivo imaging system (IVIS, Xenogen Corp./Caliper Life Science), D-Luciferin potassium salt (Perkin-Elmer), isoflurane for anesthesia, and various antibodies for immunohistochemistry.
4:Experimental Procedures and Operational Workflow:
Mice were randomized into four groups based on cell line and implantation method. Tumor growth was monitored weekly by BLI. At the endpoint, mice were euthanized, and tumors and metastases were analyzed.
5:Data Analysis Methods:
Data were analyzed using Student's t-test for differences between groups. Immunohistochemistry results were quantified using Image-Pro Plus software.
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