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Medication
Female hormones or clomiphene may be prescribed. These help shrink or destroy some tumors. Oral contraceptives are often used as the first step in treatment.
LAPAROSCOPY
Ovarian cyst and benign tumors can also be resected by this technique
Staging The Federation Internationale de Gynecologie et d'Obstetrique (FIGO) and the American Joint Committee on Cancer (AJCC) have designated staging.
y tumours involving 1 or both ovaries with distant metastasis. Parenchymal liver metastasis equals stage IV.
Management
Treatment Options
The treatment of ovarian cancers based on the stage of the disease which is a reflection of the extent or spread of the cancer to other parts of the body. It also depends on histologic cell type, and the patient's age and overall condition. There are basically three forms of treatment of ovarian cancer:
surgery Chemotherapy radiation treatment, treatment,
GENERAL GUIDELINES:
Standard treatment is surgery (staging and optimal debulking) followed by adjuvant chemotherapy in most cases. Even if optimal surgery is not possible, removing as much tumor as possible will provide significant palliation of symptoms. Borderline lesions may be treated with conservative surgery
GENERAL GUIDELINES:
Germ cell tumors are treated with surgery and multimultiagent chemotherapy in most cases Advanced epithelial ovarian cancer is very sensitive to chemotherapy with responses in the range of 70-80% to 70firstfirst-line chemotherapy. The majority, however, relapse and ultimately die of chemotherapy-resistant disease. chemotherapySecondSecond-line chemotherapy to date is disappointing in all forms of epithelial ovarian cancer with virtually no chance of successful second-line treatment following secondfailure of initial regime.
SURGERY
Stage I
Generally a total abdominal hysterectomy, removal of both ovaries and fallopian tubes, omentectomy, biopsy of lymph nodes and other tissues in the pelvis and abdomen,is done. Young women whose disease is confined to one ovary are often treated by a unilateral salpingosalpingo-oophorectomy without a hysterectomy and removal of the opposite ovary being performed Depending on the pathologist's interpretation of the tissue removed, there may be no further treatment if the cancer is low grade, or if the tumor is high grade the patient may receive combination chemotherapy.
Stage II
Treatment is almost always hysterectomy and bilateral salpingosalpingo-oophorectomy as well as debulking of as much of the tumor as possible and sampling of lymph nodes and other tissues in the pelvis and abdomen that are suspected of harboring cancer. After the surgical procedure, treatment may be one of the following: 1) combination chemotherapy with or without radiation therapy or 2) combination chemotherapy.
Stage III
Treatment is the same as for Stage II ovarian cancer. Following the surgical procedure, the patient may either receive combination chemotherapy possibly followed by additional surgery to find and remove any remaining cancer.
Stage IV
CYTOREDUCTIVE SURGERY/DEBULKING:
surgery to remove as much of the tumor as possible. Most researchers consider residual disease of <1 cm to be optimal debulking surgery. followed by combination chemotherapy
Trial of 146 patients with stage III and IV ovarian cancer treated with cisplatin at Rosewell park Cancer Institute:
SIZE OF RESIDUAL DISEASE
SURVIVAL
5 YEARS 8 YEARS
CHEMOTHERAPY
Prolongs remission and survival Also used for palliative treatment in advanced n recurrent disease Administered in all cases beyond stage Ia Earlier single agents were used, nowadays combination therapy is favoured
CHEMOTHERAPY
No chemotherapeutic agent kills all cancer cells in one treatment ,Tf treatment needs to be repeated several times All agents used should be active against that particular tumor should have different modes of action to avoid drug resistance n should have differenr mechanisms of toxicity.
CHEMOTHERAPY
This allows each of them to be used as nearv to the full dose as possible. Drugs are given at 3 weeks intervals Intraperitoneal chemotherapy is also done
The initial treatment of ovarian cancer is called firstfirstline therapy. If the cancer continues to grow with first-line therapy or firstreturns after first-line therapy, additional treatment, firstcalled second-line therapy, may be administered. secondtherapy, If the tumor continues to grow after second-line secondtherapy, the next therapy is called third-line therapy, thirdtherapy, and so on.
FirstFirst-Line Chemotherapy
FirstFirst-line chemotherapy for ovarian cancer typically consists of two drugs given together. The combination =paclitaxel + platinum drug either carboplatin or cisplatin. Select women may benefit from administration of chemotherapy directly into the abdomen called intraperitoneal therapy in addition to conventional intravenous administration.
SecondSecond-Line Chemotherapy
The choice of drugs for second-line therapy depends secondlargely on which drugs were administered for first-line firsttherapy and how long it has been since the first-line firsttherapy was stopped. chemotherapy drugs) for the treatment of ovarian cancer that has returned: GEMZAR (gemcitabine HCl for injection) plus another chemotherapy, carboplatin, is indicated ,6 months after their first-line therapy; first-
SecondSecond-Line Chemotherapy
Hycamtin (topotecan HCl for injection) is indicated as a single agent (one drug) for the treatment of ovarian cancer upon failure of first-line therapy; firstand Doxil (doxorubicin HCl liposome injection) is approved for use to treat women whose cancer has returned following first-line therapy. first-
Topotecan is recommended as an option for second-line second(or subsequent) treatment only for those women with platinum-refractory or platinum-resistant platinumplatinumadvanced ovarian cancer, or those who are allergic to platinum-based compounds, for whom PLDH and platinumsinglesingle-agent paclitaxel are considered inappropriate.
CP
CISPLATIN PACLITAXEL CARBOPLATIN PACITAXEL CISPLATIN CYCLOPHOSPHAMIDE CYCLOPHOSPHAMIDE DOXORUBICIN CISPLATIN BLEOMYCIN ETOPOSIDE CISPLATIN
75 mg/sq.m 135135-175mg/sq.m AUC=5 135135-175mg/sq.m 75mg/sq.m 750mg/sq.m 600mg/sq.m 50mg/sq.m 75mg/sq.m 10mg/sq.m x 3 days 20mg/sq.m x 5days 100mg/sq.m
CT
DC
CAP
BEP
VBC
BEP
SIDE EFFECTS
While chemotherapy drugs kill cancer cells, they also damage some normal cells, causing side effects. These side effects will depend on the type of drugs given, the amount taken, and how long treatment lasts. Temporary side effects might include the following: nausea and vomiting loss of appetite hair loss hand and foot rashes kidney or nerve damage mouth sores
an increased chance of infection (from a shortage of white blood cells) bleeding or bruising after minor cuts (from a shortage of platelets) tiredness (from low red blood cell counts)
RADIOTHERAPY:
Now, has a very small role since platinum based protocols and paclitaxel have improved the median survival.
-However it can be used as a palliative treatment for metastatic bone or brain lesions or of localized recurrence to alleviate the pain.
Also used in recurrent germ cell tumors especially dysgerminomas which is very radiosensitive. Radioactive isotopes of gold-Au198 and phosphorus-P32 goldphosphorushave been used intraperitoneally along with external radiotherapy. However there s no improvement in survival rate. High incidence of bowel complications have been noted.
SecondSecond-Look Surgery
The use of second-look surgery can help diagnose and secondmanage ovarian cancer. evidence of enhanced survival after this procedure is lacking. It is defined as re-exploration n patients with advanced restage III and stage IV ovarian cancer after a standard course of chemotherapy have no clinical, biochemical, ro radiologic evidence of disease
Patients who develop recurrent cancer despite surgery and primary chemotherapy, and will be given salvage chemotherapy, chemotherapy, may be placed into one of three groups (A-C): (A-
GROUP A
are patients resistant to primary therapy and have shown tumor growth during treatment. This persisting tumor is considered to be refractory i.e. have absolute platinumplatinum-resistance. Secondary non-cross resistant nonchemotherapies or biological therapies should be considered.
GROUP B
are patients who respond well to initial chemotherapy, but develop recurrent cancer within months after the end of primary care. This group with relatively platinum resistant tumor has an intermediate prognosis.
GROUP C
are patients who showed a good response to primary chemotherapy, and did not develop recurrent cancer for more than 6 months after the end of primary treatment. This group with platinum-sensitive tumor shows the best platinumresponses to re-treatment with a platinum-containing replatinumregimen.
prognosis
Overall 5-year survival in ovarian epithelial carcinoma is low 5because of the preponderance of late-stage disease at diagnosis. lateStage I and II: 80-100% 80Stage III: 15-20% 15Stage IV: 5%
Patients under 50 in all stages have considerably better 5-year 5survival than older patients (40% compared to 15%) Dysgerminomas treated by surgery and radiation have an excellent cure rate in both early and late-stage disease lateEndodermal sinus tumour has poor prognosis.
prevention
Diet: a high-fat diet may play a role in the highaetiology of ovarian cancer. Oral contraceptives appear to reduce the risk of ovarian cancer for up to 10 years following cessation of use. This protective effect appears to apply to patients with BRCA mutations as well. Patients who have used fertility drugs should be counselled as to their possible increase in risk of ovarian cancer.