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This article provides an overview of ovarian cancer, including the different types, pathology, and clinical features. It highlights the importance of early detection and emphasizes the need for further research.
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Ovarian cancer Dr. T Allameh Associated professor of Ob & Gyn of IUMS
Ovarian cancer • Epithelial 90% • Germ cell tumors (20-25% of all benign and malignant ovarian neoplasms, only 3% of these are malignant ) • Sex cord stromal tumor 5-8%
Epithelial cancers are the most common ovarian malignancies • Usually asymptomatic until they have metastatized patients have advanced disease at diagnosis in more than 2/3 of cases • It has the highest fatality –to case ration of all the gynecologic malignancies
Epithelial ovarian cancer • APPROXIMATELY 90% OF OVARIAN CANCERS ARE DERIVED FROM TISSUES THAT COME FROM THE COELOMIC EPITHELIUM OR MESOTHELIUM
pathology of invasive cancer • 75% of epithelial cancers are of the serous histologic type • Mucinous 20% • Endometriosis 2% • Clear cell 1%, • Brenner 1% • Undifferentiated 1% • Occur more often in ages of 50-70
Border line tumors • Are lesions that tend to remain confined to the ovary for long periods • Occur predominantly in premenopausal women ( 30-50 y ) • Good prognosis
Borderline tumors • Epithelial proliferation with papillary formation and pseudostratification • Nuclear atypia and increased mytotic activity • Absence of true stromal invasion ( without tissue distraction ) • 20-25% of borderline malignant tumors spread beyond the ovary
Serous tumors • Develop by invagination of the surface ovarian epithelium • Psammoma bodies (focal of foreign material )
Borderline serous tumors • 10% of all ovarian serous tumors • 50% occur before the age of 40 y • 10% have extra ovarian implans (invasive and non invasive) • The invasive implants resemble well differentiated serous carcinoma
Malignant serous carcinoma • Stromal invasion is present • Well differentiated ( papillary and grandular structures predominant ) • Moderately differentiated • Poorly differentiated (solid sheets of cells , nuclear pleomorfism and highly mitotic activity ) • Calcified psammoma bodies in 80%
Mucinous tumors • Have loculi lined with mucin secreting epithelial • 8-10% of epithelial of ovarian tumors • May reach enormous size
Bordeline mucinous tumors • Often a diagnosis difficult to make • Well differentiated mucinous epithelium may be seen adjacent to a poorly differentiated focus
Malignant mucinous carcinoma • 8-10% are bilateral • 95-98% are intraovarian • Most ovarian mucinous carcinomas contain intestinal type cells • Can not be distinguished from metastasis carcinoma of the GI (basis of histology alone ) • Primary ovarian neoplasm rarely metastasized to the mucosa of the bowel ( commonly involved the serous )
Pseudomyxoma peritoneal The neoplastic epithelium secrets large amount of gelatinous mucinous material , most commonly secondary to : a well differentiated appendiceal carcinoma an ovarian mucinous carcinoma A mucocell of the appendix
Endometriod tumors • 6-8% of epithelia tumors • Similar to those seen in uterine cavity • A malignant potential of endometriosis is very low
Borderline endometriod tumors • Wide morphologic spectrum • Resemble an endometrial polyp or complex endometrial hyperplasia • Some have a prominent fibromatus component (adenophibroma)
Malignant endometrial carcinoma • Are characterized by adenomatos pattern with all the potential variations of epithelial found in the uterus • Greatest opportunity to multifocal disease • Entometriod tumors of the ovary are often associated with similar lesions in the endometrium
Mutifocal disease • Metastatic from the uterus to the ovaries have a 30-40% five year survival • Synchronous multifocal disease have a 75-80% five year survival
Clear cell carcinoma • The tumors are made up of clear cells and hobnail cells • The tall clear cells have abundant clear or vacuolated cytoplasm ,hyperchromatic irregular nuclear and nucleoli of various size • Is the histlogically identical to that seen in the uterus or vagina of the young patient who has been exposed to DES in uterus
Brennr tumors Borderline • the epithelium dose not invade the stroma • Resemble low grade papillary transitional cell carcinoma of the urinary bladder
Malignant brenner tumors • The tumor infiltrates the tissue with associated destruction
Transitional cell tumors • Resemble transitional cell carcinoma of the urinary bladder • An appointment finding is that those ovarian carcinomas that contain more than 50% of transitional cell carcinoma are more sensitive to chemotherapy and have a more favorable prognosis • Differ from malignant Brenner tumor in that they are more frequently diagnosed in advanced stage ( poorer survival rate )
Small cell carcinoma • Mainly in young women who may have symptoms of hypercalcemia • Immunohystochemichal stains are helpful to differentiate this tumor from a lymphoma , leukemia
Clinical features • Peak incidence of invasive epithelial ovarian cancer is at 56-60 y • Fewer than 1% occur before 21 y • 30% of ovarian neoplasms in post menopausal women are malignant • 7% of ovarian epithelial tumors in premenopausal patients are malignant
Borderline tumors • Average age 46 y • The chance that a primary epithelial tumor will be of borderline or invasive malignancy before 40 y is 1/ 10 , after that age it rises 1/3
Etiology • Low parity • Infertility • Talk use • Galactose consumption • Early menarche • Late menopause Repetitive disruption and repair of the surface epithelium may lead to mutation
Prevention • 1 child RR 0.3- 0.4 • OC for 5 or more years RR 0.5 • (50% reduction in ovarian cancer ) • 2 children and OC for 5 or more years RR 0.3 ( 70% reduction in ovarian cancer ) • Fenertidine ( 4hydroxyretinoic acid ) . A vitamin A derivative
Screening • BME • Ultrasound : TVS : > 95% sensitivity for the detection of early stage of ovarian cancer ( 10-15 laparatomy for each ovarian cancer ) Trans abdominal + CA 125>30 u/ml (4 laparatomy for each ovarian cancer ) Transvaginal color flow • CA- 125 ( 50% in stage I , 60% in stage II )
Genetic risks of epithelial ovarian cancer • The life time risk of ovarian carcinoma for women in the USA is about 1.4% • Most epithelial ovarian cancer is sporadic • Familial or hereditary patterns in 5-10%
Hereditary ovarian cancer • BRCA 1 mutations (chromosome 17 ) 28- 44 % life time risk • BRCA2 mutations (chromosome 13 ) 27 % life time risk • The mutations are inherited in an autosomal dominant fashion • Full pedigree analysis( maternal and paternal ) • The risk of breast cancer in BRCA1 or BRCA2 mutation is 56-87% .
Hereditary ovarian cancers in general occur in women approximately 10 years younger than those with nonhereditary tumors
Pedigree analysis • In familis with 2first degree relatives (mother ,sister, or daughter ) with premenopausal epithelial ovarian cancer , the risk that a female first degree relative has an affected gene could be 35-40% . • In familis with a single degree relative and single second degree relative (grandmother ,aunt , first cousin , or grandaughter ,) with epithelial ovarian cancers the risk that a woman has an affected gene increase 2-10 fold higher than others.
3- In families with a single post menopausal first degree relative with epithelial ovarian carcinoma a woman may not have an increased risk . • if the ovarian cancers occurs in a premenopausal relative , could be significant and a full pedigree analysis should be undertaken .
4-women with a primary history of breast cancer have twice the expected incidence of ovarian cancer
Linch 2 syndrome • Multiple adenocarcinoma : familial colon cancer (lynch 1) high rate of ovarian endometrial and breast cancers other malignancies of GI and GU • The mutations are MSH2 , MLH 1, PMS 1 and PMS 2 • RR 3 for ovarian cancers
Management of women at high risk for ovarian cancers • Genetic counseling • TVS every 6 months • OC in young women who have completed their families may undergo prophylactic BSO (peritoneal carcinomas occasionally can occur ) • in women also have a strong family history of breast cancer , annual mammographic screening should be performed beginning at age 30 • Women with a HNPCC syndrome should undergo periodic screening mammography , colonoscopy , and endometrial biopsy
Symptoms • Most have no symptoms for long periods of time • Symptoms are vague and non specific • (Irregular menses urinary frequency or constipation, lower abdominal distention, pressure or pain ) • In advance stage : ascites,abdominal distention , bloating ,constipation , nausea , anorexia or early satiety
Signs • Pelvic mass • Upper abdominal mass • Ascites
Diagnosis • CA 125 levels have been shown to be useful in distinguishing malignant from benign pelvic masses • For a postmenopausal patients with an adnexal mass and CA125 > 95u/ml there is a 96% PPV for malignancy • For premenopausal patients the specificity of the test is low
If a cystic mass is > 8cm • Solid • Fixed • Irregular
Pattern of spread • Transcoelomic • Lymphatic • Hematogenous
Treatment Complete surgical staging • Peritoneal washing • TAH- BSO • Pelvic lymphnod Dysection • Paraaortic sampling • Omentectomy Chemotherapy • Taxol • carbopelatin