ACR Appropriateness Criteria®
Clinical Condition: Staging and Follow-up of Ovarian Cancer
Variant 1: Pretreatment staging ovarian cancer.
Radiologic Procedure |
Rating |
Comments |
RRL* |
CT abdomen and pelvis |
9 |
|
High |
CA–125 |
9 |
|
None |
MRI abdomen and pelvis |
5 |
Evidence shows equivalent staging accuracy compared to CT. Problem solving modality for patients who cannot have contrast enhanced CT. See comments regarding contrast in text under "Anticipated Expectations." |
None |
US pelvis transvaginal |
5 |
Evidence shows equivalent staging accuracy compared to CT and MRI, but scan time and coverage may limit efficiency. |
None |
CT chest |
4 |
For abnormal chest x-ray including pleural effusions, supraclavicular adenopathy |
Med |
X-ray colon barium enema |
3 |
|
Med |
X-ray intravenous urography |
2 |
|
Low |
Rating Scale: 1=Least appropriate, 9=Most appropriate |
*Relative Radiation Level |
Note: Abbreviations used in the tables are listed at the end of the "Major Recommendations" field.
Variant 2: Rule out recurrent ovarian cancer.
Radiologic Procedure |
Rating |
Comments |
RRL* |
CT abdomen and pelvis |
9 |
|
High |
CA–125 |
9 |
|
None |
CT chest abdomen and pelvis |
9 |
Indicated if abnormal chest x-ray, known extensive abdominal disease, or markedly elevated CA–125, or preoperatively for debulking to insure disease is limited to the abdomen. |
High |
FDG-PET/CT abdomen and pelvis |
7 |
If available, can substitute for CT. |
High |
MRI abdomen and pelvis |
5 |
Problem solving modality. Appropriate for patients who cannot have contrast-enhanced CT. See comments regarding contrast in text under "Anticipated Expectations." |
None |
US pelvis transvaginal |
4 |
May be used as problem solving tool for disease in the pelvis. |
None |
FDG-PET abdomen and pelvis |
4 |
Limited due to difficulties in spatial localization, especially in the abdomen. |
High |
X-ray colon barium enema |
3 |
|
Med |
X-ray intravenous urography |
2 |
|
Low |
Rating Scale: 1=Least appropriate, 9=Most appropriate |
*Relative Radiation Level |
Note: Abbreviations used in the tables are listed at the end of the "Major Recommendations" field.
Summary of Literature Review
Ovarian cancer is the fifth most common cause of cancer death in women in the United States behind lung, breast, colorectal, and pancreatic cancers, accounting for more than 3% of all cancers in women and causing more deaths than any other gynecologic malignancy. Many common benign conditions of the ovaries have an acute presentation, while ovarian cancer is a silent killer, often presenting late with advanced stage III–IV disease after the disease has spread widely. The roles of diagnostic imaging have been ovarian mass characterization, determination of preoperative disease extent, and prediction of tumor resectability. Surgical staging is both diagnostic and therapeutic, and an experienced gynecologic surgeon is critical in optimum debulking of this tumor. However, up to 40% of patients may be understaged at laparotomy.
Transvaginal ultrasound (US) has a role in ovarian cancer screening and characterization of ovarian masses as benign or malignant. It can be used to determine the site of origin of a pelvic mass and to characterize the lesion. A combination of morphology and Doppler waveform analysis may provide the most accurate risk assessment for an adnexal lesion by US.
The proper choice of treatment for ovarian cancer depends on accurate staging. Computed tomography (CT) and magnetic resonance imaging (MRI) have been used to determine the resectability of tumors, the candidacy of patients for effective cytoreductive surgery, the need for preoperative chemotherapy if debulking is suboptimal, and the need for referral to a gynecologic oncologist. Limited disease means stage I or II. Regional disease means stage II, involving one or both ovaries with pelvic extension. Advanced disease means stages III and IV.
Cytoreductive surgery is the standard treatment for ovarian cancer. However, in patients with advanced disease, medical co-morbidities, or stage IV disease, using initial adjuvant chemotherapy and/or radiation therapy followed by cytoreduction results in optimal tailored patient management, decreased morbidity and mortality, and improved survival. Standard radiographic techniques such as chest radiograph, barium enema, and excretory urography have been replaced in many countries, including the United States, by cross sectional imaging, especially CT, for ovarian cancer staging. CT is the imaging modality of choice in the preoperative evaluation of ovarian cancer and has been validated as an accurate method to predict successful surgical cytoreduction. CT has been useful for detecting local tumor involvement of the pelvic ureter and uterine serosa, as well as metastases to the peritoneum, omentum, mesentery, liver, spleen, and lymph nodes. CT has a reported accuracy for ovarian cancer staging of up to 94%. Current high-resolution multidetector CT scanners can detect peritoneal implants as small as 5 mm (specificity 100%, accuracy 80% for all sites except diaphragm and pelvis) and improves the false negative rate (which is up to 50% for helical CT) when using multiplanar reconstruction for optimal depiction of disease. The most important limitation of CT in staging ovarian cancer is its inability to reliably detect bowel surface, mesenteric, or peritoneal tumor implants smaller than 5 mm, especially in the absence of ascites.
MRI is an excellent problem-solving technique by virtue of its ability to define common conditions such as fibroids, dermoid cysts, endometriomas, and other benign lesions. Two studies found no statistical difference between CT and MRI in defining disease extent. A multivariate analysis showed that the accuracy of MRI with gadolinium enhancement in diagnosing ovarian malignancy was 93%. Gadolinium enhancement improved diagnostic confidence and tissue characterization. However, the role of MRI has been limited because the use of intraluminal gastrointestinal contrast agents with MRI is not routine as it is with CT, MRI generally costs more than CT, and there are fewer experienced radiologists to interpret MRI. Thus, CT is currently the recommended modality to stage ovarian cancer. MRI is recommended for patients with a contraindication to the use of iodinated contrast agents (allergy, renal insufficiency), patients who are pregnant, and those for whom CT findings are inconclusive.
For predicting the nonresectability of ovarian cancer, cross sectional imaging (CT or MRI) plays a critically important role in finding significant lesions (greater than 2 cm) at the root of the mesentery, gastrosplenic ligament, omentum of the lesser sac, porta hepatic, intersegmental fissure of the liver, diaphragm, liver dome, lymphadenopathy at or above the celiac axis, presacral extraperitoneal disease, and pelvic sidewall invasion. Unresectable disease can be managed by needle or laparoscopic biopsy, chemotherapy, and possibly a later attempt at optimal debulking, resulting in improved survival by virtue of optimal response to chemotherapy.
The use of fluorodeoxyglucose positron emission tomography (FDG-PET) imaging in the primary diagnosis and tissue characterization of ovarian cancer is unsupported to date. Specificity has been reported as low as 54% and moderate sensitivity as high as 86%. Also, false negative results have been reported with borderline tumors, early carcinomas, and adenocarcinomas. False positive results have been reported with dermoid cysts, hydrosalpinges, and endometriosis.
However, FDG-PET, especially when combined with CT, is a valuable tool for diagnosing advanced disease and detecting recurrent tumor. The use of FDG-PET combined with serum tumor marker CA-125 has had a reported sensitivity as high as 98%, and PET alone has a sensitivity of 85%. Second look laparotomy is no longer routinely performed. The noninvasive diagnosis of recurrence obviates the need for unnecessary surgery.
Because optimal debulking after chemotherapy improves survival in patients with recurrence, this information is critical to patient management. MRI and CT are roughly equivalent for identifying lesions larger than 2 cm. CT is 58% sensitive and 100% specific in predicting unsuccessful debulking. The reported accuracy of MRI for detecting lesions larger than 2 cm is comparable to that of CT at 93% to 95%. CT remains the preferred imaging method for detecting recurrence for the same reasons as those that are discussed above for primary staging.
The preoperative evaluation of patients with suspected ovarian carcinoma usually includes a serum CA-125 determination. Only about 50% of all patients with ovarian cancer have a true positive result. Thus, this test alone is inadequate when used in isolation as a screening tool. However, with stage II or greater ovarian cancer, the true positive rate is as high as 80%. There is a very high correlation between CA-125 levels and the clinical course of the patient after surgery. False positive results have been reported with endometriosis, benign ovarian cysts, pregnancy, and pelvic inflammatory disease. Pancreatic cancer and cirrhosis have caused elevated CA-125 levels. CA-125 levels can also predict tumor recurrence among patients who are clinically tumor free.
Anticipated Exceptions
Nephrogenic systemic fibrosis (NSF, also known as nephrogenic fibrosing dermopathy) was first identified in 1997 and has recently generated substantial concern among radiologists, referring doctors and lay people. Until the last few years, gadolinium-based MR contrast agents were widely believed to be almost universally well tolerated, extremely safe and non-nephrotoxic, even when used in patients with impaired renal function. All available experience suggests that these agents remain generally very safe, but recently some patients with renal failure who have been exposed to gadolinium contrast agents (the percentage is unclear) have developed NSF, a syndrome that can be fatal. Further studies are necessary to determine what the exact relationships are between gadolinium-containing contrast agents, their specific components and stoichiometry, patient renal function and NSF. Current theory links the development of NSF to the administration of relatively high doses (e.g., >0.2 mM/kg) and to agents in which the gadolinium is least strongly chelated. The FDA has recently issued a "black box" warning concerning these contrast agents (http://www.fda.gov/cder/drug/InfoSheets/HCP/gcca_200705HCP.pdf).
This warning recommends that, until further information is available, gadolinium contrast agents should not be administered to patients with either acute or significant chronic kidney disease (estimated GFR <30 mL/min/1.73m2), recent liver or kidney transplant or hepato-renal syndrome, unless a risk-benefit assessment suggests that the benefit of administration in the particular patient clearly outweighs the potential risk(s).
Abbreviations
- CA, cancer antigen
- CT, computed tomography
- FDG-PET, fluorodeoxyglucose positron emission tomography
- Med, medium
- MRI, magnetic resonance imaging
- US, ultrasound