abstract
Cancer cell lines are good in vitro models to study molecular mechanisms
underlying chemoresistance and cancer recurrence. Recent works have
demonstrated that most of the available ovarian cancer cell lines are
most unlikely high grade serous (HGSOC), the major type of epithelial
ovarian cancer. We aimed at establishing well characterized HGSOC cell
lines, which can be used as optimal models for ovarian cancer research.
We successfully established seven cell lines from HGSOC and provided the
major genomic alterations and the transcriptomic landscapes of them.
They exhibited different gene expression patterns in the key pathways
involved in cancer resistance. Each cell line harbored a unique TP53
mutation as their corresponding tumors and expresses cytokeratins
8/18/19 and EpCAM. Two matched lines were established from the same
patient, one at diagnosis and being sensitive to carboplatin and the
other during chemotherapy and being resistant. Two cell lines presented
respective BRCA1 and BRCA2 mutations. To conclude, we have established
seven cell lines and well characterized them at genomic and
transcriptomic levels. They are optimal models to investigate the
molecular mechanisms underlying the progression, chemo resistance and
recurrence of HGSOC.
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