Radiologic Evaluation of Incidentally Discovered Adrenal Masses

JONATHON M. WILLATT; ISAAC R. FRANCIS

JONATHON M. WILLATT, MBChB, AND ISAAC R. FRANCIS, MD

Am Fam Physician. 2010;81(11):1361-1366

Author disclosure: Nothing to disclose.

The increasing use of cross-sectional imaging has led to an increase in the incidental discovery of adrenal masses (adrenal incidentalomas). Although most of these lesions are benign, they often present a diagnostic dilemma. Before creating a management plan, the physician should determine if the lesion is benign or malignant and if the lesion is functioning or nonfunctioning. Incidentally discovered adrenal masses usually are benign adenomas; however, myelolipomas, cysts, hemorrhage, pheochromocytomas, metastases, and adrenocortical carcinomas are also possible. Unenhanced computed tomography and chemical shift magnetic resonance imaging can characterize most adenomas because the lesions have high lipid content. Contrast-enhanced computed tomography can further characterize the adenomas because of the washout characteristics with iodinated intravenous contrast media. Fluorodeoxyglucose–positron emission tomography can be helpful in characterizing some lesions, and biopsy is rarely required. This article summarizes the American College of Radiology Appropriateness Criteria for the use of imaging modalities and biopsy to characterize incidentally discovered adrenal masses.

The increasing use of computed tomography (CT) and magnetic resonance imaging (MRI) has led to a rise in the incidental discovery of adrenal masses (adrenal incidentalomas). Approximately 3 to 4 percent of CT and MRI studies of the abdomen reveal an adrenal incidentaloma.^1,2 The most common incidentally discovered adrenal masses are adenomas, which are benign lesions. The prevalence of adenomas rises from 0.2 percent in persons in their twenties to 7 percent in those older than 70 years.^3,4 Other adrenal masses that may be encountered incidentally include myelolipomas, cysts, hemorrhage, pheochromocytomas, metastases, and adrenocortical carcinomas.

Evaluation

Cysts, myelolipomas, and adrenal hemorrhage are benign and often can be characterized on the initial imaging study; however, other lesions cannot be easily characterized without the use of more dedicated, specific imaging techniques. A lesion measuring at least 1 cm is normally considered large enough for further imaging investigation.⁵ There are no data for determining the accuracy of imaging for masses measuring less than 1 cm. Based on anecdotal evidence, most physicians and radiologists believe that masses measuring less than 1 cm do not require further imaging workup. Density measurements with CT may be unreliable at this size. However, patients with small lesions may need hormonal evaluation to determine if they have adrenal hyperfunction.⁶

The purpose of further imaging and clinical workup is to answer two questions: Is the lesion benign or malignant? Is the lesion functioning or nonfunctioning? Examples of hyperfunctioning lesions include pheochromocytoma, and nodules that secrete cortisol (Cushing syndrome) or aldosterone (Conn syndrome).

Patients with an incidentally discovered adrenal mass are typically asymptomatic, but the mass may later prove to be functional. Although the initial evaluation should always include a thorough history, physical examination, and biochemical evaluation when indicated, this article focuses on radiologic studies based on the American College of Radiology Appropriateness Criteria for initiating further imaging (Table 1).⁷

Clinical condition: Incidentally discovered adrenal mass
Radiologic procedure	Rating	Comments	RRL
Variant 1: No history of malignancy; mass 1–4 cm in diameter. Initial evaluation.
CT abdomen without contrast	8	Presumes that a noncontrast CT has not already been performed or if there are suspicious imaging features	Med
CT abdomen without and with contrast	8	Indicated if noncontrast CT is not diagnostic AND if there are concerning imaging features of malignancy	Med
MRI abdomen without contrast	8	May be helpful when nonenhanced CT is equivocal or if there are suspicious imaging features	None
Biopsy adrenal gland	6	A biopsy should only be performed if the lesion is enlarging and if pheochromocytoma is excluded; CT or US guidance could be used	NS
MIBG	2	Only for suspicion of pheochromocytoma	High
MRI abdomen with contrast	2	—	None
MRI abdomen without and with contrast	2	—	None
Iodocholesterol scan	1	This agent may be used to detect functionally active adenomas	High
FDG-PET whole body	1	—	High
X-ray abdomen	1	—	Med
US adrenal gland	1	—	None
Variant 2: No history of malignancy; mass 1–4 cm in diameter. Follow-up evaluation in 12 months.
CT abdomen without contrast	8	—	Med
MRI abdomen without contrast	8	—	None
CT abdomen without and with contrast	1	—	Med
MRI abdomen without and with contrast	1	—	None
Variant 3: No history of malignancy; mass > 4 cm in diameter. (If not typical for adenoma, myelolipoma, hemorrhage, or simple cyst, consider resection.)
CT abdomen with contrast	8	As part of preoperative staging	Med
MRI abdomen with contrast	8	As part of preoperative staging	None
FDG-PET whole body	5	As part of preoperative staging	High
MIBG	2	Only for suspicion of pheochromocytoma	High
CT abdomen without and with contrast	2	—	Med
MRI abdomen without and with contrast	2	—	None
CT abdomen without contrast	1	—	Med
MRI abdomen with contrast	1	—	None
Iodocholesterol scan	1	This agent may be used to detect functionally active adenomas	High
Biopsy adrenal gland	1	—	NS
X-ray abdomen	1	—	Med
US adrenal gland	1	—	None
Variant 4: History of malignancy; mass < 4 cm in diameter. Initial evaluation.
CT abdomen without contrast	8	If there is no prior imaging and assuming that a noncontrast CT has not already been performed	Med
CT abdomen without and with contrast	8	Indicated if noncontrast CT is indeterminate (density > 10 HU) or lesion does not lose signal on out-of-phase images	Med
MRI abdomen without contrast	8	If there is no prior imaging and no prior chemical shift MRI and if washout on dedicated adrenal CT is not diagnostic of adenoma	None
Biopsy adrenal gland	8	A biopsy should only be performed if imaging characteristics cannot characterize mass as benign and if pheochromocytoma is excluded; CT or US guidance could be used	NS
FDG-PET whole body	8	If CT and MRI features are not diagnostic of benign lesion and there is no prior imaging	High
MIBG	2	Only for suspicion of pheochromocytoma	High
Iodocholesterol scan	1	This agent may be used to detect functionally active adenomas	High
X-ray abdomen	1	—	Med
US adrenal gland	1	—	None
MRI abdomen with contrast	1	—	None
MRI abdomen without and with contrast	1	—	None
Variant 5: History of malignancy; mass > 4 cm in diameter.
Biopsy adrenal gland	8	—	NS
FDG-PET whole body	8	—	High
CT abdomen with contrast	1	—	Med
MIBG	1	—	High
MRI abdomen with contrast	1	—	None
Iodocholesterol scan	1	—	High
X-ray abdomen	1	—	Med
US adrenal gland	1	—	None

Is the Mass Benign or Malignant?

The prevalence of primary adrenocortical carcinoma is about 0.06 percent in the general population. A study of 342 patients showed only a 1.2 percent rate of adrenocortical carcinoma in those with adrenal incidentalomas.¹ All of the malignant lesions were greater than 5 cm. In general, the larger the mass, the greater the likelihood of malignancy. Approximately 90 percent of adrenocortical carcinomas are larger than 4 cm when first discovered.⁸

In the absence of a history of malignancy, the discovery of a metastatic lesion in the adrenal gland is rare, occurring in 0.3 percent of patients with incidentalomas.^1,9 In persons with known malignancy, the incidence is higher at 25 to 36 percent.^10–12 Bronchogenic carcinoma, renal cell carcinoma, and melanoma represent the most common primary malignancies with adrenal metastases.

A CT or MRI can usually determine whether an adrenal incidentaloma is benign by detecting lipid in the mass (Table 2). Adenomas usually contain lipid (lipid-rich adenomas); however, most lipid-poor lesions are also adenomas.^1,13 Only a small proportion of lipid-poor lesions are malignant nonadenomas. Unenhanced CT cannot reliably distinguish between lipid-poor adenomas and nonadenomas; however, contrast-enhanced CT with washout calculations has been shown to help make this distinction with high specificity.^14–17 Adenomas (both lipid-rich and lipid-poor) demonstrate rapid washout of the intravenously injected, iodinated contrast media, as opposed to malignant masses.^14–17

Type of incidentaloma*	Findings
Type of incidentaloma*	Size	Attenuation on unenhanced CT	Rapidity of washout of contrast media on enhanced CT	Appearance on MRI (out-of-phase image)	Growth rate
Lipid-rich adrenal adenoma	< 3 cm	≤ 10 HU	Rapid washout	Signal loss	Size usually stable
Lipid-poor adrenal adenoma	< 3 cm	> 10 HU	Rapid washout	No signal loss	Size usually stable
Adrenocortical carcinoma	Usually > 5 cm	> 10 HU	No rapid washout	No signal loss	Usually significant growth
Pheochromocytoma	Variable size	> 10 HU	No rapid washout	No signal loss	Slow growth
Metastasis	Variable size	> 10 HU	No rapid washout	No signal loss	Usually significant growth

Imaging to Determine Malignancy

Most incidentally detected adrenal masses greater than 1 cm are characterized as benign, lipid-rich adenomas using the unenhanced phase of adrenal protocol CT (Figure 1). For masses that do not fit into this category, further contrast-enhanced and delayed-phase CT with washout calculations can be performed as part of the same examination. For patients who are unable to undergo a contrast-enhanced CT because of renal insufficiency or allergy to iodinated contrast media, chemical shift MRI can be performed. CT and MRI demonstrate similar accuracy in the diagnosis of adrenal masses.^18,19 Cost and availability determine which is used as the primary modality in individual centers.

Fluorodeoxyglucose–positron emission tomography (FDG-PET) can be used for lesions that cannot be categorized by CT or MRI. If the lesion still cannot be characterized, biopsy or surgical removal may be indicated.

The tracer m-iodobenzylguanidine (MIBG) localizes to adrenergic nerve endings, and studies using MIBG are useful in patients with suspected pheochromocytoma.

CT

The Hounsfield unit scale is a semiquantitative method of measuring radiography attenuation. Organs and tissues demonstrate variable attenuation depending on their density. Fat- and lipid-containing lesions have lower densities than the spleen, normal adrenal gland, or parenchyma of the liver. If an adrenal mass measures 10 HU or less on unenhanced CT, it is probably a lipid-rich adenoma.¹⁴ The mean Hounsfield unit for adrenal carcinoma, metastasis, and pheochromocytoma is significantly higher.²⁰ A threshold value of 10 HU has a 71 percent sensitivity and 98 percent specificity for identifying adenomas and is generally accepted as a cutoff for diagnosis of lipid-rich adenomas.^21,22

Combined unenhanced and contrast-enhanced CT can be used to identify lipid-poor adenomas (less than 10 HU) using washout calculations.^14–17 This technique raises both the sensitivity and specificity of CT to 96 percent for adrenal adenoma diagnosis.

MRI

Chemical shift MRI uses a technique based on hydrogen and fat protons, which resonate at different frequencies. By using different time parameters during the same MRI examination, it is possible to identify lipid-rich adenomas. These adenomas show signal loss on out-of-phase imaging, as opposed to imaging when the protons are in phase (Figure 2). In contrast, nonadenomas do not show signal loss on out-of-phase imaging.^23,24 Recent studies have shown that 60 to 89 percent of lesions measuring between 10 and 30 HU on unenhanced CT can be characterized using chemical shift MRI.^23,25

FDG-PET

Evaluation using FDG-PET has a high sensitivity for detecting malignancy ²⁶; however, adenomas can also occasionally take up the radiotracer, decreasing the test's specificity. Therefore, FDG-PET is used to determine the need for biopsy in masses that cannot be characterized on CT or MRI.

ADRENAL BIOPSY TO DETECT MALIGNANCY

The role of adrenal biopsy has evolved. Biopsy is not performed to diagnose adrenal adenoma, but mostly to confirm or rule out malignancy in the few cases in which CT or MRI results are equivocal. However, before adrenal biopsy is performed, pheochromocytoma should be excluded with biochemical tests, especially in an incidentally detected mass, because hemorrhage and hypertensive crisis have been reported as complications of pheochromocytomas biopsy.^27,28

Is the Lesion Functioning or Nonfunctioning?

Subclinical hyperfunctioning adrenal nodules are well recognized; pheochromocytomas, aldosteronomas, and cortisol-secreting nodules are the most common.^13,29 Although the literature yields variable results, the incidence of subclinical hyperfunctioning adrenal lesions is between 0.4 and 15 percent. In one study, 19 of 33 adrenal pheochromocytomas were detected incidentally, and only 10 of the 19 patients were hypertensive.³⁰ Although a functioning mass is often suggested by the history and physical examination findings, the absence of these findings does not exclude a hormonally active lesion. Studies have shown detectable secretion of aldosterone, cortisol, or catecholamines in 5 to 23 percent of patients with adrenal incidentalomas.^31–34 Table 3 outlines the biochemical workup to help determine if the lesion is functioning.⁵

Possible cause	Incidentalomas with this diagnosis (%)	Clinical signs	Laboratory tests
Cushing syndrome	5	Hypertension, moon-shaped face, striae, proximal muscle weakness, truncal obesity, thin skin, easy bruising	Overnight dexamethasone suppression test, serum and 24-hour urinary cortisol levels, serum corticotropin level
Pheochromocytoma	3 to 10	Hypertension, headache, diaphoresis, palpitations	24-hour urinary fractionated metanephrine and catecholamines levels
Primary aldosteronism	Less than 1	Hypertension, hypokalemia, hypernatremia	Morning plasma aldosterone concentration and renin activity, aldosterone suppression test

Follow-up and Treatment

Patients with incidentally discovered adrenal masses measuring greater than 4 cm who do not have a history of malignancy usually undergo surgery if the lesions cannot be characterized as cysts or myelolipomas, because of the higher risk of adrenocortical carcinoma in masses of this size.⁶ For lesions measuring 1 to 4 cm that are characterized as adenomas, follow-up unenhanced CT at 12 months can be performed to ensure that there has not been significant growth. Tumors that have grown should be further investigated, and adrenal biopsy or resection should be considered, although even growing adrenal lesions are usually not malignant.¹³ If the size of the mass is stable, no further imaging is required, although serial biochemical evaluation may be needed.³⁵

The National Institutes of Health and the American Association of Clinical Endocrinologists recommend that if autonomous function is not present on the initial study, hormonal evaluation should be repeated annually for at least four years.^5,6,13,35,36 Benign lesions that demonstrate autonomous function are managed either medically or surgically depending on the clinical circumstances.^37,38 Adrenal cysts and myelolipomas usually do not need follow-up; however, surgical evaluation may be needed if the mass is large enough to cause symptoms.

Herrera MF, Grant CS, van Heerden JA, Sheedy PF, Ilstrup DM. Incidentally discovered adrenal tumors: an institutional perspective. Surgery. 1991;110(6):1014-1021.

Bovio S, Cataldi A, Reimondo G, et al. Prevalence of adrenal incidentaloma in a contemporary computerized tomography series. J Endocrinol Invest. 2006;29(4):298-302.

Kloos RT, Gross MD, Francis IR, Korobkin M, Shapiro B. Incidentally discovered adrenal masses. Endocr Rev. 1995;16(4):460-484.

Young WF. Management approaches to adrenal incidentalomas. A view from Rochester, Minnesota. Endocrinol Metab Clin North Am. 2000;29(1):159-185.

Young WF. Clinical practice. The incidentally discovered adrenal mass. N Engl J Med. 2007;356(6):601-610.

Grumbach MM, Biller BM, Braunstein GD, et al. Management of the clinically inapparent adrenal mass (“incidentaloma”). Ann Intern Med. 2003;138(5):424-429.

Francis IR, Casalino DD, Arellano RS, et al.; Expert Panel on Urologic Imaging American College of Radiology Appropriateness Criteria: incidentally discovered adrenal mass. http://www.acr.org/SecondaryMainMenuCategories/quality_safety/app_criteria/pdf/ExpertPanelonUrologicImaging/IncidentallyDiscoveredAdrenalMassDoc7.aspx. Accessed March 7, 2010.

Angeli A, Osella G, Alì A, Terzolo M. Adrenal incidentaloma: an overview of clinical and epidemiological data from the National Italian Study Group. Horm Res. 1997;47(4–6):279-283.

Gajraj H, Young AE. Adrenal incidentaloma. Br J Surg. 1993;80(4):422-426.

Bernardino ME, Walther MM, Phillips VM, et al. CT-guided adrenal biopsy: accuracy, safety, and indications. AJR Am J Roentgenol. 1985;144(1):67-69.

Francis IR, Smid A, Gross MD, Shapiro B, Naylor B, Glazer GM. Adrenal masses in oncologic patients: functional and morphologic evaluation. Radiology. 1988;166(2):353-356.

Oliver TW, Bernardino ME, Miller JI, Mansour K, Greene D, Davis WA. Isolated adrenal masses in nonsmall-cell bronchogenic carcinoma. Radiology. 1984;153(1):217-218.

Song JH, Chaudhry FS, Mayo-Smith WW. The incidental adrenal mass on CT: prevalence of adrenal disease in 1,049 consecutive adrenal masses in patients with no known malignancy. AJR Am J Roentgenol. 2008;190(5):1163-1168.

Hamrahian AH, Ioachimescu AG, Remer EM, et al. Clinical utility of non-contrast computed tomography attenuation value (Hounsfield units) to differentiate adrenal adenomas/hyperplasias from nonadenomas: Cleveland Clinic experience. J Clin Endocrinol Metab. 2005;90(2):871-877.

Caoili EM, Korobkin M, Francis IR, Cohan RH, Dunnick NR. Delayed enhanced CT of lipid-poor adrenal adenomas. AJR Am J Roentgenol. 2000;175(5):1411-1415.

Caoili EM, Korobkin M, Francis IR, et al. Adrenal masses: characterization with combined unenhanced and delayed enhanced CT. Radiology. 2002;222(3):629-633.

Korobkin M, Brodeur FJ, Francis IR, Quint LE, Dunnick NR, Londy F. CT time-attenuation washout curves of adrenal adenomas and nonadenomas. AJR Am J Roentgenol. 1998;170(3):747-752.

Rescinito G, Zandrino F, Cittadini G, Santacroce E, Giasotto V, Neumaier CE. Characterization of adrenal adenomas and metastases: correlation between unenhanced computed tomography and chemical shift magnetic resonance imaging. Acta Radiol. 2006;47(1):71-76.

Yoh T, Hosono M, Komeya Y, et al. Quantitative evaluation of norcholesterol scintigraphy, CT attenuation value, and chemical-shift MR imaging for characterizing adrenal adenomas. Ann Nucl Med. 2008;22(6):513-519.

Korobkin M, Giordano TJ, Brodeur FJ, et al. Adrenal adenomas: relationship between histologic lipid and CT and MR findings. Radiology. 1996;200(3):743-747.

Boland GW, Lee MJ, Gazelle GS, Halpern EF, McNicholas MM, Mueller PR. Characterization of adrenal masses using unenhanced CT: an analysis of the CT literature. AJR Am J Roentgenol. 1998;171(1):201-204.

van Erkel AR, van Gils AP, Lequin M, Kruitwagen C, Bloem JL, Falke TH. CT and MR distinction of adenomas and nonadenomas of the adrenal gland. J Comput Assist Tomogr. 1994;18(3):432-438.

Israel GM, Korobkin M, Wang C, Hecht EN, Krinsky GA. Comparison of unenhanced CT and chemical shift MRI in evaluating lipid-rich adrenal adenomas. AJR Am J Roentgenol. 2004;183(1):215-219.

Mayo-Smith WW, Lee MJ, McNicholas MM, Hahn PF, Boland GW, Saini S. Characterization of adrenal masses (< 5 cm) by use of chemical shift MR imaging: observer performance versus quantitative measures. AJR Am J Roentgenol. 1995;165(1):91-95.

Haider MA, Ghai S, Jhaveri K, Lockwood G. Chemical shift MR imaging of hyperattenuating (>10 HU) adrenal masses: does it still have a role?. Radiology. 2004;231(3):711-716.

Burt M, Heelan RT, Coit D, et al. Prospective evaluation of unilateral adrenal masses in patients with operable non-small-cell lung cancer. Impact of magnetic resonance imaging. J Thorac Cardiovasc Surg. 1994;107(2):584-588.

Casola G, Nicolet V, vanSonnenberg E, et al. Unsuspected pheochromocytoma: risk of blood-pressure alterations during percutaneous adrenal biopsy. Radiology. 1986;159(3):733-735.

McCorkell SJ, Niles NL. Fine-needle aspiration of catecholamine-producing adrenal masses: a possibly fatal mistake. AJR Am J Roentgenol. 1985;145(1):113-114.

Mantero F, Terzolo M, Arnaldi G, et al. A survey on adrenal incidentaloma in Italy. Study Group on Adrenal Tumors of the Italian Society of Endocrinology. J Clin Endocrinol Metab. 2000;85(2):637-644.

Motta-Ramirez GA, Remer EM, Herts BR, Gill IS, Hamrahian AH. Comparison of CT findings in symptomatic and incidentally discovered pheochromocytomas. AJR Am J Roentgenol. 2005;185(3):684-688.

Bülow B, Ahrén B Swedish Research Council Study Group of Endocrine Abdominal Tumours. Adrenal incidentaloma—experience of a standardized diagnostic programme in the Swedish prospective study. J Intern Med. 2002;252(3):239-246.

Caplan RH, Strutt PJ, Wickus GG. Subclinical hormone secretion by incidentally discovered adrenal masses. Arch Surg. 1994;129(3):291-296.

Reincke M, Nieke J, Krestin GP, Saeger W, Allolio B, Winkelmann W. Preclinical Cushing's syndrome in adrenal “incidentalomas”: comparison with adrenal Cushing's syndrome. J Clin Endocrinol Metab. 1992;75(3):826-832.

Bernini GP, Vivaldi MS, Argenio GF, Moretti A, Sgrò M, Salvetti A. Frequency of pheochromocytoma in adrenal incidentalomas and utility of the glucagon test for the diagnosis. J Endocrinol Invest. 1997;20(2):65-71.

NIH state-of-the-science statement on management of the clinically inapparent adrenal mass (“incidentaloma”).. NIH Consens State Sci Statements. 2002;19(2):1-25.

Zeiger MA, Thompson GB, Duh QY, et al. American Association of Clinical Endocrinologists and American Association of Endocrine Surgeons medical guidelines for the management of adrenal incidentalomas: executive summary of recommendations. Endocr Pract. 2009;15(5):450-453.

Funder JW, Carey RM, Fardella C, et al. Case detection, diagnosis, and treatment of patients with primary aldosteronism: an endocrine society clinical practice guideline. J Clin Endocrinol Metab. 2008;93(9):3266-3281.

Lau JH, Drake W, Matson M. The current role of venous sampling in the localization of endocrine disease. Cardiovasc Intervent Radiol. 2007;30(4):555-570.