Abstract:Background:: A plateau has been reached for conventional therapies in ovarian cancer as there is no definitive increase in overall survival. It is necessary to distinguish molecular subtypes based on multi-omics integration to take more targeted strategies to improve prognosis and increase therapeutic efficacy.
Methods:: A total of 202 patients with mRNA, miRNA, DNA methylation, somatic mutation, and Reverse Phase Protein Array (RPPA) data were assembled into one multi-omics dataset and then developed a model … Show more
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