Diagnosis and Evaluation of Adrenal Mass: Difference between revisions
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*** Clinically overt disease | *** Clinically overt disease | ||
== Differential | == Differential Diagnoses == | ||
*'''<span style="color:#ff0000">Differential diagnosis of incidental adrenal mass ( | *'''<span style="color:#ff0000">Differential diagnosis of incidental adrenal mass (10)</span>''' | ||
** '''<span style="color:#ff0000">Malignant ( | ** '''<span style="color:#ff0000">Malignant (3):</span>''' | ||
**# '''<span style="color:#ff0000">Adrenal cortical carcinoma</span>''' | **# '''<span style="color:#ff0000">Adrenal cortical carcinoma</span>''' | ||
**# '''<span style="color:#ff0000">Metastasis</span>''' | **# '''<span style="color:#ff0000">Metastasis</span>''' | ||
**#'''<span style="color:#ff0000">Sarcoma</span>''' | |||
** '''<span style="color:#ff0000">Benign (7):</span>''' | ** '''<span style="color:#ff0000">Benign (7):</span>''' | ||
**# '''<span style="color:#ff0000">Pheochromocytoma</span>''' | **# '''<span style="color:#ff0000">Pheochromocytoma</span>''' | ||
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* See 2011 CUA Incidental Adrenal Mass Guideline [https://test.urologyschool.com/index.php/CUA:_Adrenal_Mass_(2011) Notes] | * See 2011 CUA Incidental Adrenal Mass Guideline [https://test.urologyschool.com/index.php/CUA:_Adrenal_Mass_(2011) Notes] | ||
* '''<span style="color:#ff0000">Hypercortisolism''' | * '''<span style="color:#ff0000">Hypercortisolism''' | ||
** '''Assessed by overnight low-dose (1 mg) dexamethasone suppression test''' (sensitivity: 85-90 specificity: 95-99) | ** '''<span style="color:#ff0000">Assessed by overnight low-dose (1 mg) dexamethasone suppression test</span>''' (sensitivity: 85-90 specificity: 95-99) | ||
*** Consideration can be given to using the 24-hour urine free cortisol (sensitivity: 80-98, specificity: 45-98) for screening, with the low dose 1 mg dexamethasone suppression test used to differentiate Cushing’s from subclinical Cushing’s syndrome if the cortisol level on the 24-hour test is elevated. | *** Consideration can be given to using the 24-hour urine free cortisol (sensitivity: 80-98, specificity: 45-98) for screening, with the low dose 1 mg dexamethasone suppression test used to differentiate Cushing’s from subclinical Cushing’s syndrome if the cortisol level on the 24-hour test is elevated. | ||
*** Further [https://www.ncbi.nlm.nih.gov/pubmed/31069279 details on hypercortisolism testing] | *** Further [https://www.ncbi.nlm.nih.gov/pubmed/31069279 details on hypercortisolism testing] | ||
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** '''<span style="color:#ff0000">Routine testing of incidentalomas for sex hormones is not currently recommended''' | ** '''<span style="color:#ff0000">Routine testing of incidentalomas for sex hormones is not currently recommended''' | ||
*** '''Hypersecretion of adrenal sex steroids by adrenal masses, especially incidentalomas, is exceedingly rare and typically present with concomitant clinical symptoms (i.e., feminization or virilization)''' | *** '''Hypersecretion of adrenal sex steroids by adrenal masses, especially incidentalomas, is exceedingly rare and typically present with concomitant clinical symptoms (i.e., feminization or virilization)''' | ||
**'''Assessed with (2):''' | |||
**#'''Serum DHEA-S''' | |||
**#'''24-hour urine 17-ketosteroids''' | |||
* '''<span style="color:#ff0000">Confirmatory hormonal testing for all positive screening tests is recommended to limit false positive results and unnecessary surgery''' | * '''<span style="color:#ff0000">Confirmatory hormonal testing for all positive screening tests is recommended to limit false positive results and unnecessary surgery''' | ||
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* '''Should be pursued if diagnosis remains equivocal and the result of biopsy will influence management.''' | * '''Should be pursued if diagnosis remains equivocal and the result of biopsy will influence management.''' | ||
** '''Most useful in patients with primary malignancies that have potentially recurred in the adrenal gland and whose management will be affected by the biopsy results.''' | ** '''Most useful in patients with primary malignancies that have potentially recurred in the adrenal gland and whose management will be affected by the biopsy results.''' | ||
* '''ALWAYS exclude possibility of pheochromocytoma before biopsy''' '''to avoid potentially life-threatening hemorrhage and hypertensive crisis''' | * '''<span style="color:#ff0000">ALWAYS exclude possibility of pheochromocytoma before biopsy''' '''to avoid potentially life-threatening hemorrhage and hypertensive crisis''' | ||
== Management == | == Management == |
Latest revision as of 09:57, 17 March 2024
- Includes 2011 CUA Incidental Adrenal Mass Guidelines
- See 2011 CUA Incidental Adrenal Mass Guideline Notes
Background[edit | edit source]
- Definition of incidental adrenal mass: adrenal lesion >1cm discovered on radiologic examination done for reasons other than to investigate for primary adrenal disease
- Exclusions to definition include:
- Known malignancy or high suspicion of malignant processes [since adrenal mass has high likelihood of being a metastatic deposit]
- Clinically overt disease
- Exclusions to definition include:
Differential Diagnoses[edit | edit source]
- Differential diagnosis of incidental adrenal mass (10)
- Malignant (3):
- Adrenal cortical carcinoma
- Metastasis
- Sarcoma
- Benign (7):
- Pheochromocytoma
- Adenoma (functional vs. non-functional)
- Oncocytoma
- Cyst
- Myelolipoma
- Ganglioneuroma
- Abscess
- Malignant (3):
- ≈20% of incidental adrenal masses are found to be potential surgical lesions
- See Campbell's 11th edition Table 65-15 for Characteristics of Incidental Adrenal Masses as Described in a Systematic Review of Published Series of Adrenal Incidentalomas
Diagnosis and Evaluation[edit | edit source]
- 2011 CUA: ALL incidental adrenal masses (excluding myelolipomas, hemorrhages, and cysts) initially require a comprehensive workup, including thorough clinical, radiologic and hormonal evaluations to distinguish benign from malignant processes, as well as non-functioning from hyperfunctioning tumours.§
UrologySchool.com Summary[edit | edit source]
- History and Physical Exam
- Labs (3)§
- Low-dose dexamethasone suppression test or 24-hour urinary cortisol to rule out hypercortisolism AND
- 24-hour urinary metanephrines and/or catecholamines to rule out pheochromocytoma +/-
- Aldosterone-renin ratio in patients with hypertension to rule out hyperaldosteronism
- Imaging (1)
- Unenhanced CT
- If attenuation ≥ 10HU, obtain contrast enhanced CT with adrenal washout
- Unenhanced CT
History and Physical Exam[edit | edit source]
- Most patients are asymptomatic
- Screen for signs and symptoms related to disorders of
- Adrenal hyperfunction
- Hypercortisolism (9)
- Central obesity
- Moon facies
- Buffalo hump
- Facial plethora
- Menstrual disturbances
- Hirsuitism
- Proximal muscle weakness
- Easy bruisability
- Abdominal striae
- Systemic manifestations include dyslipidemia, insulin resistance, and hypertension
- Hyperaldosteronism: hypertension
- Hypertension classified as
- Elevated blood pressure: SBP 120-129 mm Hg; DBP < 80 mm Hg
- Stage 1 hypertension: SBP 130 - 139 mm Hg; DBP 80 - 89 mm Hg
- Stage 2 hypertension: SBP ≥140 mm Hg; DBP ≥ 90 mm Hg
- Hypertension classified as
- Pheochromocytoma (3):
- Headache
- Episodic sudden perspiration
- Tachycardia
- Adrenal sex steroid hypersecretion
- Hypercortisolism (9)
- Adrenal malignancy
- Adrenal hyperfunction
Labs[edit | edit source]
- See 2011 CUA Incidental Adrenal Mass Guideline Notes
- Hypercortisolism
- Assessed by overnight low-dose (1 mg) dexamethasone suppression test (sensitivity: 85-90 specificity: 95-99)
- Consideration can be given to using the 24-hour urine free cortisol (sensitivity: 80-98, specificity: 45-98) for screening, with the low dose 1 mg dexamethasone suppression test used to differentiate Cushing’s from subclinical Cushing’s syndrome if the cortisol level on the 24-hour test is elevated.
- Further details on hypercortisolism testing
- Assessed by overnight low-dose (1 mg) dexamethasone suppression test (sensitivity: 85-90 specificity: 95-99)
- Pheochromocytoma
- Assessed by 24-hour urine metanephrines and catecholamines
- Fractionated plasma metanephrines is a newer test that may be more sensitive, but less specific. As such, its use should be reserved for confirmatory testing as opposed to primary screening.
- Plasma metanephrine testing may not be widely available outside select centers, therefore 24-hour urinary metanephrines is suggested for initial screening.
- Fractionated plasma metanephrines is a newer test that may be more sensitive, but less specific. As such, its use should be reserved for confirmatory testing as opposed to primary screening.
- Assessed by 24-hour urine metanephrines and catecholamines
- Hyperaldosteronism
- Assessed in hypertensive patients by upright plasma aldosterone concentration to plasma renin ratio (ARR).
- Pre-testing considerations
- Mineralocorticoid receptor blockers (e.g. spironolactone) and some diuretics, particularly potassium sparing diuretics (e.g. amiloride, triamterene) and potassium wasting diuretics (e.g. furosemide, HCTZ, indapamide), should be discontinued at least 4 weeks prior to the ARR
- If ARR results are not diagnostic and hypertension can be controlled with relatively noninterfering antihypertensives, withdrawal of other potentially interfering medications (angiotensin-converting enzyme inhibitors, angiotensin receptor blockers, renin inhibitors, dihydropyridine calcium channel antagonists, β-blockers, central α-2 agonists and non-steroidal anti-inflammatory drugs) for at least 2 weeks prior to a repeat ARR is recommended.
- Patients should be informed to liberalize salt intake leading up to the test to ensure accurate results
- Acute fluctuations in dietary sodium are reported to not affect the diagnostic accuracy of the ARR
- Pre-testing considerations
- Normokalemia occurs in up to 50% of patients with hyperaldosteronism.
- Traditionally, hyperadlosteronism has been clinically associated with hypertension and hypokalemia
- Assessed in hypertensive patients by upright plasma aldosterone concentration to plasma renin ratio (ARR).
- Adrenal Sex Steroid Hypersecretion
- Routine testing of incidentalomas for sex hormones is not currently recommended
- Hypersecretion of adrenal sex steroids by adrenal masses, especially incidentalomas, is exceedingly rare and typically present with concomitant clinical symptoms (i.e., feminization or virilization)
- Assessed with (2):
- Serum DHEA-S
- 24-hour urine 17-ketosteroids
- Routine testing of incidentalomas for sex hormones is not currently recommended
- Confirmatory hormonal testing for all positive screening tests is recommended to limit false positive results and unnecessary surgery
Imaging[edit | edit source]
CT[edit | edit source]
- Unenhanced CT scan is the first test
- Myelolipoma, cysts and hemorrhages have distinct features on imaging
- Most easily interpreted test for intracellular lipid
- Adenomas typically contain a greater proportion of intracellular fat in comparison to malignant incidentalomas.
- If attenuation of a region of interest over a mass on unenhanced CT
- <10 HU, diagnostic for an adrenal adenoma (corresponds to high intracytoplasmic lipid content)
- This cutoff has ≈70% sensitivity and 98% specificity for the diagnosis of adrenal adenomas
- ≈30% of adrenal adenomas exhibit an attenuation >10 HU on unenhanced CT owing to their lower lipid content
- These “atypical adenomas” or "lipid-poor adenomas" are indistinguishable from non-adenomas on non-contrast CT density measurements alone
- ≈30% of adrenal adenomas exhibit an attenuation >10 HU on unenhanced CT owing to their lower lipid content
- This cutoff has ≈70% sensitivity and 98% specificity for the diagnosis of adrenal adenomas
- >10 HU, obtain contrast enhanced CT with washout
- Contrast enhanced CT with washout has excellent sensitivity and specificity in differentiating between adenomas and non-adenomatous incidentalomas
- The diagnostic information from a single-phase enhanced CT scan for adrenal lesions is quite limited, as there is considerable overlap in post-contrast attenuation of adenomas and non-adenomas
- Phases of adrenal CT study (3):
- Non-contrast 5-mm images through the adrenal
- Enhanced (1-minute post-bolus imaging)
- 15-minute washout imaging
- Delayed (washout) imaging indicative of adrenal adenoma
- Absolute percent washout > 60% ([Enhanced − delayed]/[Enhanced − unenhanced] × 100%)
- Relative percent washout (RPW) > 40% ([Enhanced − delayed]/ [Enhanced] × 100%)
- Lipid-poor adenomas possess identical properties to lipid-rich adenomas regarding their rapid loss (washout) of enhancement after CT contrast
- RCC metastases and HCC mets may exhibit washout characteristics similar to those of lipid-poor adenomas
- Contrast enhanced CT with washout has excellent sensitivity and specificity in differentiating between adenomas and non-adenomatous incidentalomas
- <10 HU, diagnostic for an adrenal adenoma (corresponds to high intracytoplasmic lipid content)
- Characteristics of pheochromocytoma and malignant processes include (5):
- Size (>3 cm)
- Heterogenous texture
- Increased vascularity
- Attenuation of >10 HU on unenhanced CT
- Decreased contrast washout at 10 to 15 minutes
MRI[edit | edit source]
- Similar to CT scan, chemical-shift MRI uses the lipid-rich property of most adenomas to differentiate benign from malignant
- CT with washout is considered the gold standard and is better than chemical shift MRI for identifying adenomas
Ultrasound[edit | edit source]
- Suboptimal imaging modality for detecting and characterizing adrenal lesions
Functional imaging[edit | edit source]
- The role of functional imaging for the diagnosis of pheochromocytoma is limited, given that most pheochromocytomas can be accurately diagnosed with cross-sectional imaging and metabolic evaluation for catecholamines and their metabolites.
PET[edit | edit source]
- 2-[18F] FDG-PET scan can be useful in detecting metastasis in patients with a history of malignancy, as metabolically-active lesions typically have increased uptake of FDG versus benign lesions.
Adrenal biopsy[edit | edit source]
- Currently NOT recommended for the routine workup of adrenal incidentaloma
- Limited role in contemporary era:
- Modern imaging in the context of clinical characteristics affords superb diagnostic capabilities
- Histologically, adenomas cannot be reliably differentiated from adrenal carcinomas
- Risks of biopsy
- Limited role in contemporary era:
- Should be pursued if diagnosis remains equivocal and the result of biopsy will influence management.
- Most useful in patients with primary malignancies that have potentially recurred in the adrenal gland and whose management will be affected by the biopsy results.
- ALWAYS exclude possibility of pheochromocytoma before biopsy to avoid potentially life-threatening hemorrhage and hypertensive crisis
Management[edit | edit source]
- Options (2):
- Adrenalectomy
- Observation
Adrenalectomy[edit | edit source]
- Indications (11):
- Size ≥ 4 cm (with exception of myelolipoma)
- Most adrenocortical carcinomas are >4cm in size
- Masses >6 cm should be considered malignant until proved otherwise.
- Although management of masses between 4-6 cm is controversial, in otherwise healthy individuals, masses >4 cm should be resected
- Radiologically benign masses >4 cm may be followed in patients who are not prime candidates for surgery
- The incidence of benign adrenal adenomas increases with age
- Adrenal lesions in younger patients, even those < 4 cm, must be managed with greater caution than similar lesions in an older patient.
- Lesions >4 cm in older patients with significant comorbidities may be better served with observation than resection
- Most adrenocortical carcinomas are >4cm in size
- Size increases > 1 cm on follow-up imaging
- Current recommendation is to resect masses that grow >1 cm; however, incidence of malignancy among these patients is low
- Adrenal hyperfunction
- Some patients with primary aldosteronism may be managed medically, especially if they are poor surgical candidates
- Clinically silent adrenal hyperfunction is an area of debate.
- Due to the potentially life-threatening complications, it is accepted that any lesions exhibiting silent pheochromocytoma, an adrenal incidentaloma with hormonal and radiologic signs of pheochromocytoma but without clinical symptoms, should be surgically removed after adequate adrenergic blockade
- Surgery may be elected for younger patients with subclinical Cushing syndrome or those with new onset, medically resistant or deteriorating disease attributable to cortisol excess. The remainder should be admitted to follow-up and recommended for surgery if they develop clinical signs of Cushing’s syndrome.
- Mass with imaging findings that are suggestive of malignancy (e.g., lipid poor, heterogeneous, irregular borders, infiltrates surrounding structures), regardless of size
- Extremely large and/or symptomatic cyst or myelolipoma
- Isolated adrenal metastasis (multidisciplinary decision making required)
- During renal surgery for renal cell carcinoma if:
- Adrenal abnormal or not visualized because of large renal tumor size on imaging
- Vein thrombus to level of adrenal vein
- Failed neurosurgical treatment of Cushing disease, necessitating bilateral adrenalectomy
- Select patients with ectopic adrenocorticotropic hormone (ACTH) syndrome, requiring bilateral adrenalectomy
- ACTH-independent macronodular adrenal hyperplasia (AIMAH)
- Primary pigmented nodular adrenocortical disease (PPNAD)
- *First 4 consistent with CUA Incidental Adrenal Mass Guidelines
- Size ≥ 4 cm (with exception of myelolipoma)
Observation[edit | edit source]
- Follow-up protocol
- Myelolipomas, hemorrhages, cysts do not necessarily require further evaluation
- Non-functioning adenomas, typically < 4 cm, and masses not deemed resectable at initial diagnosis should undergo clinical, hormonal, and radiological surveillance.
- No consensus on the proper methodology for follow-up.
- Surveillance proposed in 2011 CUA Guidelines:
- Annual clinical and hormonal testing for up to 4 years
- There is no agreement on the best mechanism and frequency for hormonal follow-up. However, it should include the same screening tests used at primary evaluation
- Radiographic assessments (depends on lesion characteristics +/- size)
- Benign appearing masses
- <1 cm, consider no further follow-up or enrolment in a clinical trial
- 1-2cm, first follow-up scan at 12 months if clinical picture warrants
- 2-4cm, first follow-up scan at 12 months
- Radiologically suspicious lesions not initially removed
- Any size, first follow-up scan should be at 3-6 months
- Further imaging follow-up should be directed by clinical judgment. Consider 1-3 assessments with the first 2 years of diagnosis.
- Benign appearing masses
- Tumours that remain stable on imaging and annual hormonal evaluation may be considered for discharge from follow-up after 4 years
- Annual clinical and hormonal testing for up to 4 years
- Surveillance proposed in 2011 CUA Guidelines:
Questions[edit | edit source]
- What are the absolute and relative percent washout on CT suggestive of adrenal adenoma?
- What is the initial imaging of choice for adrenal adenomas? What is the gold standard imaging for adrenal adenomas?
Answers[edit | edit source]
- What are the absolute and relative percent washout on CT suggestive of adrenal adenoma?
- What is the initial imaging of choice for adrenal adenomas? What is the gold standard imaging for adrenal adenomas?
References[edit | edit source]
- Wein AJ, Kavoussi LR, Partin AW, Peters CA (eds): CAMPBELL-WALSH UROLOGY, ed 11. Philadelphia, Elsevier, 2015, chap 65
- Kapoor, Anil, Topher Morris, and Ryan Rebello. "Guidelines for the management of the incidentally discovered adrenal mass." Canadian Urological Association Journal 5.4 (2011): 241.