Ovarian carcinoma or adenocarcinoma

Ovarian cancer is the second most common (endometrial is number one) genital tract malignancy (1% to 2% lifetime risk) and the most deadly (overall 5-year survival of 45%). Familial predisposition accounts for 5% to 10% of women who develop ovarian cancer and is typically associated with BRCA1 and BRCA2 gene mutations. Ovarian cancer is more prevalent with increasing age, usually occurring in postmenopausal women. Most cancers are of the epithelial type, the most common of these being serous cystadenocarcinoma (greater than 50%); the cell type comprising this tumor is very similar to that found in the fallopian tubes. Endometrioid adenocarcinoma (15% to 20% of epithelial ovarian cancers) and clear cell tumors of the ovary (6% of epithelial tumors) are associated with pelvic endometriosis and tend to occur in younger women. Mucinous adenocarcinoma (5% to 10% of epithelial tumors) is a mucin-producing tumor and resembles the intestinal or endocervical cell types. Other rarer cell types include carcinosarcoma (epithelial and mesenchymal mixed tumor), transitional cell, squamous cell carcinoma, and Brenner tumors (see related sections elsewhere in the book).

Pattern recognition and Doppler features of an ovarian mass are the most accurate method of differentiating a malignant from a benign tumor when performed by an experienced practitioner. In general, unilocular clear cysts with smooth borders, no nodularity, and absent internal blood flow are characteristic features of a benign mass. Papillary projections with abundant blood flow, large and irregular solid components, thick septations, and irregular walls are signs of malignancy. These features are characteristic of all epithelial ovarian tumors; hence, it is not possible to distinguish the exact tissue diagnosis sonographically. Once the tumor is advanced, ascites and peritoneal seeding are common and easily visualized sonographically.