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Test Code ACC Adrenal Mass Panel, 24 Hour, Urine


Shipping Instructions


Ship specimens frozen.



Necessary Information


The following information is required. Testing cannot proceed without this information (NA or Not Applicable are not acceptable responses).

-Age at diagnosis (Years, not offered for pediatric patients)

-Gender (Male, Female)

-Mode of discovery (incidental, cancer staging, other)

-Tumor diameter (mm)

-Unenhanced computerized tomography (CT) (Hounsfield units)

-Hormonal excess (Yes = Present, No=Absent)

-Collection duration in hours and 24-hour volume in milliliters

 

If information is not provided within 5 days of specimen receipt at MCL, testing may be delayed or canceled.

 

If not ordering electronically, Adrenal Mass Panel Patient Information is required.



Specimen Required


Supplies: Sarstedt Aliquot Tube, 5 mL (T914)

Container/Tube: Plastic urine tube

Specimen Volume: 4 mL

Collection Instructions:

1. Collect urine for a full 24 hours (required) and record the total volume.

2. Do not add preservatives. Specimens containing preservatives will be canceled.

3. Entire 24 hour collection must be mixed well prior to aliquoting into a 5 mL plastic tube.

Additional Information: See Urine Preservatives-Collection and Transportation for 24-Hour Urine Specimens for multiple collections.


Forms

Adrenal Mass Panel Patient Information is required if not ordering electronically.

Useful For

Aiding in assessing malignancy in adrenal masses

 

May aid in improving diagnostic and prognostic prediction and dissect disease mechanisms for the following applications:

-Diagnostic assessment and follow up of adrenal cortical carcinoma

-Differential diagnostic assessment of adrenal tumors

-Additional assessment related to Cushing syndrome, mild autonomous cortisol secretion, primary aldosteronism, inborn errors of steroidogenesis, polycystic ovary syndrome

 

This test is not useful for establishing eligibility for a specific treatment as results must be interpreted in conjunction with the clinical status of the patient.

Testing Algorithm

Testing begins with a clinical risk assessment based on clinical data before integration with biochemical steroid data to assess the probability of a malignant adrenal cortical carcinoma (ACC) or other malignancy (sarcoma, lymphoma, other) as well as the probability of a benign mass (adenoma, myelolipoma, cyst, other).

 

Clinical data includes age at diagnosis, gender, mode of discovery and hormonal status along with tumor diameter and an unenhanced computerized tomography (CT) scan density measurement of the tumor (in Hounsfield units).

 

Steroids and their metabolites are extracted, analyzed, quantitated, and reported. Each reported analyte also includes a Z-score. An integrated risk assessment based on clinical data in combination with biochemical steroid data is reported to assess the probability of a malignant ACC or other malignancy as well as the probability of a benign mass.

 

For more information see Adrenal Mass Panel Clinical Data Definition of Malignancy Predictors.

Method Name

Liquid Chromatography Tandem Mass Spectrometry, High-Resolution Accurate Mass (LC-MS/MS HRAM)

Reporting Name

Adrenal Mass Panel, 24 Hr, U

Specimen Type

Urine

Specimen Minimum Volume

2 mL

Specimen Stability Information

Specimen Type Temperature Time Special Container
Urine Frozen (preferred) 90 days
  Refrigerated  14 days

Reject Due To

Gross hemolysis OK
Gross icterus OK

Clinical Information

Approximately 80 million computerized tomography (CT) scans are performed in the United States every year. Adrenal tumors are found incidentally in about 5% of patients undergoing abdominal CT. Most of these tumors will be benign, but a small fraction are adrenal cortical carcinomas (ACC), a cancer with high mortality and frequent recurrence. Even for localized disease, the 5-year survival rates do not exceed 65%, while distant spread is associated with a greater than 90% mortality rate. Early diagnosis of a malignant adrenal mass is therefore imperative to assure timely and appropriate therapy.

 

Unfortunately, CT imaging alone is very limited in its ability to distinguish benign from malignant adrenal tumors since only very small and hypodense lesions can be easily dismissed as benign. The sizeable group of patients with larger or denser tumors ends up with an arduous workup that frequently includes additional imaging studies, hormonal testing, and biopsy. However, even the latter has both a high diagnostic false-positive and false-negative rate, and ultimately the tumor is often resected, sometimes unnecessarily. On the other hand, the delays due to the diagnostic work might compromise optimal care for those tumors that prove malignant.

 

In addition, patients who are believed to probably not have adrenal cancer after their workup, and those who opt out of surgery, often still require long-term follow up with regular re-imaging and repeated hormone testing, with resultant radiation exposure and high healthcare costs.

 

This adrenal mass panel is a noninvasive and more accurate test to diagnose malignant adrenal tumors, via urinary steroid profiling. It differentiates ACC, a rare and lethal tumor, from benign adrenocortical adenomas (ACA), including those that overproduce corticosteroids, or mineral steroids, or sex steroids, or those that are hormonally inactive. The test utilizes both clinical and laboratory data. The clinical parameters are age at diagnosis and sex of the patient, the size of the tumor by CT scanning and its CT density in Hounsfield units, whether it was detected incidentally or not, and whether there is evidence of hormone overproduction. All of this data are readily available for almost all patients with an adrenal mass and are used by an algorithm to calculate the pretest probability of having ACC. The steroid profile testing is then performed, and the results are added into the risk calculation algorithm to generate an integrated probability. The final result will provide the referring physicians a highly accurate probability for ACC and will thereby facilitate the optimal choice of further investigation, if any, based on an informed discussion between doctor and patient. In addition, it allows, albeit with lesser accuracy, the detection of malignant adrenal tumors that are not ACCs.

 

Finally, standalone steroid profiles can be performed for the purpose of offering the diagnosis of complex assessment of steroidal disorders, disease monitoring of patients with ACC, and for novel investigations, such as biopharma studies.

 

Understanding the Adrenal Glands:

The human body has 2 adrenal glands, one above each kidney. Adrenal glands influence many processes and functions of the body, mainly through production of 3 types of steroid hormones:

-Mineralocorticoids (eg, aldosterone, which helps control blood pressure)

-Glucocorticoids (eg, cortisol, which is important for metabolism, immune response, and stress)

-Sex steroids (eg, DHEAS, a precursor of testosterone and estradiol)

 

These steroids are all synthesized from cholesterol via enzymes in the adrenal glands. In benign ACA, near-normal levels of precursor and bioactive steroids are produced. By contrast, ACC frequently shows abnormal patterns of steroid production. By measuring 25 different steroid metabolites, even subtle abnormalities can be detected. This is the basis for the assessment capability of profiling 25 steroids. In addition, catecholamines-the "flight or fight hormones"-are also synthesized in a different portion of the adrenal glands. This portion is not examined in the ACC panel.

 

Epidemiology of Adrenal Tumors:

Adrenal masses are found in 1% to 5% of the adult population. The prevalence increases with age, to around 10% in 70-year-old patients.

 

Although the majority of these tumors are benign, around 30% of adrenal tumors (>4cm) are malignant (half are represented by ACC), and the survival rate for these patients is very poor unless detected early.

Reference Values

Note: Due to the wide range of urine steroid metabolite concentrations seen in healthy individuals and their skewed distribution, the reference values are based on the back calculated ± 3SD of log transformed data.

 

Males 18-49 years:

Androsterone: 182-29,212 mcg/24 h

Etiocholanolone: 133-23,272 mcg/24 h

Dehydroepiandrosterone: <5-81,554 mcg/24 h

16a-OH-Dehydroepiandrosterone: 13-29,945 mcg/24 h

5-Pregnenetriol: 23-7,328 mcg/24 h

5-Pregnenediol: 13-2,823 mcg/24 h

Tetrahydro-11-Corticosterone: 8-1,961 mcg/24 h

Tetrahydro-11-Deoxycorticosterone: <5-316 mcg/24 h

Pregnanediol: 12-3,812 mcg/24 h

17a-OH-Pregnanolone: 15-2,466 mcg/24 h

Pregnanetriol: 66-9,409 mcg/24 h

Pregnanetriolone: <5-550 mcg/24 h

Tetrahydrodeoxycortisol: 7-1520 mcg/24 h

Cortisol: <5-903 mcg/24 h

6B-OH-Cortisol: 13-2,303 mcg/24 h

Tetrahydrocortisol: 152-22,723 mcg/24 h

5a-Tetrahydrocortisol: 157-24,059 mcg/24 h

B-Cortol: 30-5,115 mcg/24 h

11B-OH-Androsterone: 108-11,987 mcg/24 h

11B-OH-Etiocholanolone: 22-8,312 mcg/24 h

Cortisone: 12-842 mcg/24 h

Tetrahydrocortisone: 271-44,355 mcg/24 h

a-Cortolone: 140-14,885 mcg/24 h

B-Cortolone: 72-9,740 mcg/24 h

11-Oxoetiocholanolone: 70-8,446 mcg/24 h

 

Males ≥50 years:

Androsterone: 118-25,389 mcg/24 h

Etiocholanolone: 127-15,640 mcg/24 h

Dehydroepiandrosterone: 7-4,260 mcg/24 h

16a-OH-Dehydroepiandrosterone: 11-6,183 mcg/24 h

5-Pregnenetriol: 24-2,162 mcg/24 h

5-Pregnenediol: 17-1,296 mcg/24 h

Tetrahydro-11-Corticosterone: 16-1,674 mcg/24 h

Tetrahydro-11-Deoxycorticosterone: <5-297 mcg/24 h

Pregnanediol: 23-1,846 mcg/24 h

17a-OH-Pregnanolone: 18-1,747 mcg/24 h

Pregnanetriol: 115-5,432 mcg/24 h

Pregnanetriolone: 5-221 mcg/24 h

Tetrahydrodeoxycortisol: 12-1,277 mcg/24 h

Cortisol: 12-597 mcg/24 h

6B-OH-Cortisol: 22-2,406 mcg/24 h

Tetrahydrocortisol: 331-19,009 mcg/24 h

5a-Tetrahydrocortisol: 155-35,266 mcg/24 h

B-Cortol: 56-3,541 mcg/24 h

11B-OH-Androsterone: 142-13,135 mcg/24 h

11B-OH-Etiocholanolone: 69-6,805 mcg/24 h

Cortisone: 24-732 mcg/24 h

Tetrahydrocortisone: 454-34,576 mcg/24 h

a-Cortolone: 211-17,591 mcg/24 h

B-Cortolone: 114-8,434 mcg/24 h

11-Oxoetiocholanolone: 155-7,174 mcg/24 h

 

Females 18-49 years:

Androsterone: 90-29,625 mcg/24 h

Etiocholanolone: 127-24,568 mcg/24 h

Dehydroepiandrosterone: <5-12,317 mcg/24 h

16a-OH-Dehydroepiandrosterone: 5-31,248 mcg/24 h

5-Pregnenetriol: 17-4,166 mcg/24 h

5-Pregnenediol: 6-2,900 mcg/24 h

Tetrahydro-11-Corticosterone: 13-1,548 mcg/24 h

Tetrahydro-11-Deoxycorticosterone: <5-833 mcg/24 h

Pregnanediol: 8-44,760 mcg/24 h

17a-OH-Pregnanolone: 7-3,208 mcg/24 h

Pregnanetriol: 50-9,768 mcg/24 h

Pregnanetriolone: <5-139 mcg/24 h

Tetrahydrodeoxycortisol: 7-1,047 mcg/24 h

Cortisol: 11-642 mcg/24 h

6B-OH-Cortisol: 22-2,061 mcg/24 h

Tetrahydrocortisol: 185-16,515 mcg/24 h

5a-Tetrahydrocortisol: 45-22,591 mcg/24 h

B-Cortol: 28-4260 mcg/24 h

11B-OH-Androsterone: 59-12,462 mcg/24 h

11B-OH-Etiocholanolone: 32-6,354 mcg/24 h

Cortisone: 19-749 mcg/24 h

Tetrahydrocortisone: 262-32,461 mcg/24 h

a-Cortolone: 207-13,931 mcg/24 h

B-Cortolone: 63-7,489 mcg/24 h

11-Oxoetiocholanolone: 63-7,449 mcg/24 h

 

Females ≥50 years:

Androsterone: 32-10,134 mcg/24 h

Etiocholanolone: 52-10,946 mcg/24 h

Dehydroepiandrosterone: <5-10,046 mcg/24 h

16a-OH-Dehydroepiandrosterone: <5-9,982 mcg/24 h

5-Pregnenetriol: 10-1,901 mcg/24 h

5-Pregnenediol: <5-2,732 mcg/24 h

Tetrahydro-11-Corticosterone: 14-1,229 mcg/24 h

Tetrahydro-11-Deoxycorticosterone: <5-123 mcg/24 h

Pregnanediol: 8-2,138 mcg/24 h

17a-OH-Pregnanolone: <5-571 mcg/24 h

Pregnanetriol: 26-3,444 mcg/24 h

Pregnanetriolone: <5-348 mcg/24 h

Tetrahydrodeoxycortisol: 8-801 mcg/24 h

Cortisol: 9-336 mcg/24 h

6B-OH-Cortisol: 25-1,365 mcg/24 h

Tetrahydrocortisol: 237-14,050 mcg/24 h

5a-Tetrahydrocortisol: 92-12,604 mcg/24 h

B-Cortol: 29-3289 mcg/24 h

11B-OH-Androsterone: 86-9,280 mcg/24 h

11B-OH-Etiocholanolone: 40-7,002 mcg/24 h

Cortisone: 15-555 mcg/24 h

Tetrahydrocortisone: 359-24,320 mcg/24 h

a-Cortolone: 125-17,472 mcg/24 h

B-Cortolone: 82-5,784 mcg/24 h

11-Oxoetiocholanolone: 78-6,571 mcg/24 h

 

Reference values have not been established for patients who are younger than 18 years of age.

Interpretation

Test provides clinical risk values based on clinical data alone as well as integrated risk values based on clinical data in combination with biochemical steroid data. Reported risk values correspond to the probability of a malignant adrenal cortical carcinoma or other malignancy (eg, sarcoma, lymphoma) as well as the probability of a benign mass (eg, adenoma, myelolipoma, cyst).

 

Test results provide the referring physician with probabilities for a variety of outcomes, thereby aiding the interpretation of clinical status and optimal paths for further investigation, if any, based on an informed discussion between provider and patient. Test results should always be interpreted in conjunction with all other clinical findings as they cannot be interpreted as absolute evidence for the presence or absence of malignant disease.

 

For more information see Adrenal Mass Panel Clinical Data Definition of Malignancy Predictors.

Cautions

Test not offered for pediatric patients. Risk assessments are based on adult populations.

 

Test results cannot be interpreted as absolute evidence for the presence or absence of malignant disease. This test should not form the sole basis for a diagnosis or treatment decision as results must be interpreted within the clinical context of the patient and should always be used in conjunction with clinical findings.

 

This test may be difficult to interpret in pregnant women and in patients with severe impairment of liver or kidney function.

 

Risk assignments for other malignancy may not be as accurate as risk assignment for adrenal cortical carcinoma or adrenal cortical adenoma.

Method Description

Steroids and their metabolites are extracted and analyzed with internal standard for detection by liquid chromatography-tandem mass spectrometry, high-resolution accurate mass.(Unpublished Mayo method)

 

Clinical predictors and steroid data are algorithmically integrated to give a likelihood of adrenal cortical carcinoma, other malignancy, or benign mass.

Day(s) Performed

Monday

Report Available

7 to 18 days

Specimen Retention Time

14 months

Performing Laboratory

Mayo Clinic Laboratories in Rochester

Test Classification

This test was developed and its performance characteristics determined by Mayo Clinic in a manner consistent with CLIA requirements. It has not been cleared or approved by the US Food and Drug Administration.

CPT Code Information

0015M

LOINC Code Information

Test ID Test Order Name Order LOINC Value
ACC Adrenal Mass Panel, 24 Hr, U 95556-7

 

Result ID Test Result Name Result LOINC Value
607276 ACC - Clinical Risk 95787-8
607277 Other Malignancy - Clinical Risk 95788-6
607278 Benign Mass - Clinical Risk 95789-4
607279 ACC - Integrated Risk 95790-2
607280 Other Malignancy - Integrated Risk 95791-0
607281 Benign Mass - Integrated Risk 95792-8
607282 Interpretation 73884-9
607333 Comment 77202-0
AC1AG Age at Diagnosis 63932-8
AC2GD Gender 76691-5
AC3MD Mode of Discovery 95557-5
AC4TZ Tumor Diameter (mm) 21889-1
AC5HX Unenhanced CT (Hounsfield Units) 95558-3
AC6HM Hormonal Excess 95559-1
TM66 Collection Duration (h) 13362-9
VL66 Volume (mL) 3167-4
607283 Androsterone 6705-8
607284 Androsterone Z-score 95560-9
607285 Etiocholanolone 2268-1
607286 Etiocholanolone Z-score 95561-7
607287 Dehydroepiandrosterone 13612-7
607288 Dehydroepiandrosterone Z-score 95562-5
607289 16a-OH-Dehydroepiandrosterone 95563-3
607290 16a-OH-DHEA Z-score 95564-1
607291 5-Pregnenetriol 95565-8
607292 5-Pregnenetriol Z-score 95566-6
607293 5-Pregnenediol 95567-4
607294 5-Pregnenediol Z-score 95568-2
607295 Tetrahydro-11-Corticosterone 95569-0
607296 TH-11-Corticosterone Z-score 95570-8
607297 Tetrahydro-11-Deoxycorticosterone 95571-6
607298 TH-11-Deoxycorticosterone Z-score 95572-4
607299 Pregnanediol 2834-0
607300 Pregnanediol Z-score 95573-2
607301 17a-OH-Pregnanolone 95574-0
607302 17a-OH-Pregnanolone Z-score 95575-7
607303 Pregnanetriol 2836-5
607304 Pregnanetriol Z-score 95576-5
607305 Pregnanetriolone 50643-6
607306 Pregnanetriolone Z-score 95577-3
607307 Tetrahydrodeoxycortisol 2996-7
607308 Tetrahydrodeoxycortisol Z-score 95578-1
607309 Cortisol 14158-0
607310 Cortisol Z-score 95579-9
607311 6B-OH-Cortisol 13611-9
607312 6B-OH-Cortisol Z-score 95580-7
607313 Tetrahydrocortisol 2995-9
607314 Tetrahydrocortisol Z-score 95581-5
607315 5a-Tetrahydrocortisol 21044-3
607316 5a-Tetrahydrocortisol Z-score 95582-3
607317 B-Cortol 53634-2
607318 B-Cortol Z-score 95583-1
607319 11B-OH-Androsterone 6701-7
607320 11B-OH-Androsterone Z-score 95584-9
607321 11B-OH-Etiocholanolone 6700-9
607322 11B-OH-Etiocholanolone Z-score 95585-6
607323 Cortisone 14044-2
607324 Cortisone Z-score 95586-4
607325 Tetrahydrocortisone 16116-6
607326 Tetrahydrocortisone Z-score 95587-2
607327 a-Cortolone 55906-2
607328 a-Cortolone Z-score 95588-0
607329 B-Cortolone 95589-8
607330 B-Cortolone Z-score 95590-6
607331 11-Oxoetiocholanolone 6703-3
607332 11-Oxoetiocholanolone Z-score 95591-4

Urine Preservative Collection Options

Note: The application of temperature controls must occur within 4 hours of completion of the collection.

 

Ambient (no additive)

No

Refrigerate (no additive)

OK

Frozen (no additive)

OK

50% Acetic Acid

No

Boric Acid

No

Diazolidinyl Urea

No

6M Hydrochloric Acid

No

6M Nitric Acid

No

Sodium Carbonate

No

Thymol

No

Toluene

No