CASE REPORT
Delayed presentation of a virilising, pure testosterone-secreting adrenocortical carcinoma with coexistent composite myelolipoma and a venous thrombus extending to the heart
Rakesh M Sharma,1 Sanjay Sinha,2 Hari B Kishan,3 Michelle De Padua4
1Department of Urological Oncology, Basavatarakam Indo- American Cancer Institute and Research Centre, Hyderabad, Telangana, India 2Department of Urology, Apollo Hospitals, Hyderabad, Telangana, India 3Department of Medicine, Apollo Hospitals, Hyderabad, Telangana, India 4Department of Pathology, Apollo Hospitals, Hyderabad, Andhra Pradesh, India
Correspondence to
Dr Sanjay Sinha, drsanjaysinha@hotmail.com
Accepted 20 December 2017
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To cite: Sharma RM, Sinha S, Kishan HB, et al. BMJ Case Rep Published Online First: [please include Day Month Year]. doi: 10.1136/bcr-2017- 223117
SUMMARY
A 40-year-old normotensive woman presented with abnormal facial hair for 4 years and amenorrhoea for 13 years. Hormonal, biochemical and haematological evaluation showed isolated elevation of serum testosterone and free testosterone. Her follicle- stimulating hormone and luteinising hormone were in the premenopausal range. Until recently she had reconciled to early ‘menopause’ and visited beauty clinics but never sought medical evaluation. Imaging revealed an enhancing left adrenal mass with fat densities and venous thrombus extending through the inferior vena cava to a 7 cm mass in the right atrium. She underwent left kidney-preserving surgery utilising hypothermic cardiopulmonary bypass with early clamping of the pulmonary artery without circulatory arrest. Histology showed adrenocortical carcinoma with composite incidental myelolipoma and neoplastic thrombus. At 2 months, testosterone has normalised and she is doing well. Isolated testosterone-secreting adrenocortical carcinoma with massive venous thrombus is rare as is coincidental composite macroscopic myelolipoma.
BACKGROUND
Hirsutism is a common problem affecting about 10% of women.1 Polycystic ovarian disease is the the most common cause responsible for close to three-fourths with tumours accounting for only 0.3% of 2601 pooled patients in a recently published guideline.1
However, many women consult a beautician rather than a physician.
Our 40-year-old patient had obvious facial hair growth for 4 years for which she was advised laser therapy by a cosmetic clinic. She also had what she regarded as ‘early menopause’ at 27 years that was never evaluated but in retrospect had biochemical features consistent with secondary amenorrhoea due to a testosterone-secreting tumour.
Other unusual aspects of this patient were the extent of the venous thrombus despite a functioning adrenal tumour, the pure testosterone-secreting nature of the adrenocortical carcinoma and the coincidental composite macroscopic myelolipoma. Each of these three have been unusual enough to constitute individual case reports on their own merit.
Notwithstanding the late presentation she was managed surgically successfully and given the docu- mented indolent course may carry an unusually good prognosis.
CASE PRESENTATION
A 40-year-old woman noticed abnormal facial hair growth for the last 4years. She had sought treat- ment to remove the hair from a cosmetic clinic and was advised laser treatment for facial hair but was not advised a medical consultation. She consulted a physician 3 weeks ago when a functioning left adrenal mass was identified and she was referred for management. On presentation, she had no complaint other than the obvious facial hair. She had no recent weight gain, muscle weakness, cramps, headache, sweating, tremors, visual disturbances, irritability or anxiety. She had height 160cm, weight 56kg, blood pressure 110/74mm Hg and pulse 80/min. Physical examination was unremarkable except for the facial hair growth involving primarily the upper lip, chin and lower part of both cheeks (figure 1). She had a modified Ferriman Gallwey hirsutism score (modified Ferriman Gallwey (mFG) score) of 9 (upper lip 3, chin 3, lower abdomen 2, lower back 1). There was no acne, skin stria, baldness, oedema or abnormality of bodily habitus. Abdominal and genital examination was normal. There was no clitoromegaly.
She has two children but had amenorrhoea for the last 13 years that was never evaluated.
INVESTIGATIONS
On biochemical evaluation she was noted to have elevation of serum testosterone 5.6 ng/mL (<0.8 ng/ mL) and free testosterone 18 pg/mL (<4 pg/mL) but normal dehydroepiandrosterone (DHEA) 1.0 µg/mL (<3.6 µg/mL). Serum and urinary cortisol, adrenocorticotrophic hormone, urinary metanephrines, 17-ketosteroids, thyroid-stimu- lating hormone, prolactin, glucose, creatinine, bilirubin, liver enzymes and serum electrolytes were all within normal range. The follicle-stimu- lating hormone (FSH) (7.4 mIU/mL), luteinising hormone (LH) (2.3 mIU/mL) and estradiol (82 pg/ mL) were consistent with secondary amenorrhoea due to a testosterone-secreting tumour.
BMJ
Reminder of important clinical lesson
A triphasic 500-slice CT scan of the abdomen showed a left adrenal mass 3.9 cm size with two distinct hypodense areas with density of -50, consistent with fat (figure 2 CT plain). Arte- rial phase showed patchy enhancement with washout in venous phase leaving a heterogeneous isointense to a hypointense lesion replacing the entire left adrenal gland (figure 3 intra- venous contrast CT). There was a long thrombus extending through the left renal vein into the inferior vena cava and right atrium. The left kidney was functioning normally with collateral circulation via the engorged left gonadal vein (figure 4).
2D Echocardiography showed a 7 cm right atrial mass with a normal ejection fraction.
DIFFERENTIAL DIAGNOSIS
The clinical practice guideline on hirsutism and androgen excess notes five important causes of hirsutism.1 These are polycystic ovarian disease, idiopathic hyperandrogenism, idiopathic hirsutism, non-classic congenital adrenal hyperplasia and andro- gen-secreting tumours. Concomitant secondary amenorrhoea for 13 years is only consistent with the latter two and the hormonal profile excluded all but the last cause.
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Myelolipoma was a possibility going exclusively by imaging in view of the fat densities seen within the mass. However, other clinical, biochemical and imaging features were not consistent with myelolipoma. Myelolipomas are almost always metaboli- cally inactive and do not produce a venous thombus.2
TREATMENT
Surgery was performed in the supine position with transoesoph- ageal echocardiography monitoring (video 1). After placing a cannula into the inferior vena cava through the right femoral vein the abdomen was explored by a midline laparotomy. There was no evidence of metastasis. The entire bowel was mobilised to expose the inferior vena cava, aorta and their branches in the retroperitoneum (figure 5). Renal vessels were dissected and
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taped on both sides as was the infrarenal inferior vena cava. On the left side, a tape was placed between the renal vein-gonadal vein segment (the collateral maintaining kidney viability) and the distal renal vein-adrenal vein segment. The left adrenal was dissected completely, left adrenal vein ligated and specimen removed. Limited mobilisation of the liver was performed in preparation for opening the inferior vena cava. At this stage, the heart was approached by midline sternotomy.
The standard cardiopulmonary bypass procedure was performed with hypothermia 24℃ and reduced flow of 1.7L/ min but no circulatory arrest. Additional pulmonary artery clamping was performed to avoid embolisation of the thrombus.
The renal vessels and infrarenal vena cava were clamped, the inferior vena cava was opened by a midline incision and the thrombus was extracted. There was no vascular wall invasion and the entire long thrombus up to the tricuspid valve could be extracted intact from the abdominal end (figure 6). A sepa- rate incision was given on the renal vein with removal of the previously placed ligature over the adrenal stump. All remaining thrombus was removed. The inferior vena cava and right atrium
HEAD END
Left renal vein with thrombus
Supra-renal inferior vena cava with thrombus
Normal infra-renal inferior vena cava
Right renal vein
FOOT END
INCHES
CENTIMETERS
were flushed to ensure that there was no residual thrombus and the vena cava and left renal vein was closed using 5-0 prolene sutures and the clamps over the vessels released (figure 7).
Standard closure was performed. Cell-saver suction was used to minimise blood loss. One unit of packed red blood cells was used during the surgery. There was satisfactory urine output through the procedure and the patient was extubated 3 hours after surgery.
OUTCOME AND FOLLOW-UP
Her subsequent recovery was uneventful and she was discharged on the sixth postoperative day. Follow-up 2D echocardiography and chest X-ray were satisfactory at discharge. She is doing well at 1 month. Her serum testosterone level is now normal (0.4 ng/ mL).
Histopathology showed a 4.3x4.0x2.8 cm well-encapsulated adrenocortical carcinoma with sheets of neoplastic round cells having mildly pleomorphic nuclei and abundant eosinophilic cytoplasm (figure 8). There were no mitotic figures nor capsular invasion or cellular pleomorphism. Tumour cells displayed a compact cytoplasm and some areas of necrosis consistent with a
Anterior Venotomy on IVC sutured with prolene 5-0 suture
Venotomy on the Lt Renal vein at the Lt Adrenal Vein entry point sutured with prolene 5-0
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Reminder of important clinical lesson
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Weiss score of 3. On immunohistochemistry, tumour cells were positive for inhibin and melan-A (figure 9). Focal mild positivity for AE1/AE3 was seen. Chromogranin and calretenin were nega- tive. The vena cava thrombus measured 18.5 cm, intact, and was composed of similar neoplastic tissue mandating a diagnosis of carcinoma, although low grade (figure 10). The mass also showed foci of adipose tissue with lipomatous and myeloid cells consistent with incidental composite myelolipoma.
DISCUSSION
There are several unusual features about this patient that merit discussion.
This woman noticed prominent pigmented facial hair growth for 4 years but sought help from a beauty clinic rather than a physician. She was advised laser hair removal but no evaluation for a cause for her hirsutism. A reassuringly rapid diagnosis was made once she visited a physician despite residing in a small town. Clinical practice guidelines on hirsutism recommend
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hormonal evaluation for women who present with hirsutism and discuss a scoring system for abnormal hair growth (mFG score ≥8 abnormal).1 However, the guideline emphasises strong ethnic variations, recognises that normal body hair does not exclude an androgen excess syndrome and that the severity of hirsutism does not predict the severity of androgen excess.1 Insufficient suppression of serum DHEA and cortisol by oral dexamethasone has been shown to have a very high accuracy in identifying women with hirsutism due to an adrenal tumour.3 However, these hormones were not elevated in our patient who had exclusive elevation of serum testosterone.
The patient had reconciled herself to what she thought was early ‘menopause’ at the age of 27 years. Given that her serum FSH, LH, prolactin and estradiol were in the normal premeno- pausal range, her ‘menopause’ 13 years ago was in fact secondary amenorrhoea due to the testosterone-secreting tumour. Unfor- tunately she never sought medical attention for this. The algo- rithm for diagnosis of secondary amenorrhoea in the clinical practice guidelines would presumably have led to diagnosis.4 Clinical guidelines specifically mention the critical importance of excluding an androgen-secreting tumour in a setting of viril- isation despite its rarity in view of the profound implications of the diagnosis.1
Clinical practice guidelines are targeted at clinicians but their core message needs to be communicated to beauty clinic profes- sionals since they are often the first point of contact for women with virilisation. This patient faced no delay in diagnosis once she presented to her physician.
This patient had a coincidental myelolipoma that was seen clearly on imaging. Macroscopic fat in an adrenal mass is consid- ered virtually diagnostic of a myelolipoma and such lesions are traditionally left alone.2 Coincidental myelolipoma with an adrenocortical carcinoma is very rare5 although a small series of coincidental adenoma has been reported.6 When myeloli- poma is noted with other adrenal tumours, it could be a colli- sion tumour with two distinct tumours or a composite tumour where the myeloid and lipomatous elements are seen admixed with the other tumour (carcinoma as in this case). In our patient, given the unusual venous extension and virilisation there was never any risk of inappropriate observation. However, in the hypothetical situation where these two features are lacking, one can envisage inappropriate observation instead of extirpation
especially since the tumour was below the threshold size that would trigger suspicion of cancer.2 Hence, one must exercise caution in patients with adrenal masses and perform a screening hormonal evaluation and serial assessment even if imaging suggests myelolipoma.2
Macroscopic fat within an adrenocortical carcinoma is extraordinarily rare7 although it has been suggested that micro- scopic fat might be seen due to ‘myelolipomatous metaplasia’.” As mentioned, our patient had clear histological evidence of myelolipoma.
The patient had extensive venous involvement. Adrenocor- tical carcinoma has been documented to grow occasionally into the inferior vena cava and rarely into the right atrium. However, most of these are non-functioning tumours that grow unnoticed with only occasional case reports of functioning carcinomas growing extensively through the venous system into the heart.
Testosterone-secreting adrenal tumours usually have coex- istent elevated cortisol and DHEA.3 Pure androgen-secreting adrenal tumours are very rare, mostly reported as case reports and are usually adenomas rather than carcinoma.8 This presen- tation of a pure testosterone-secreting adrenocortical carci- noma with venous extension up to the tricuspid cardiac valve is remarkably unusual.
The patient had an adrenal mass with a Weiss score of 3. Many adrenocortical carcinomas especially those with venous throm- bosis grow and metastasize fast with a low life expectancy.9 The most important determinant of cure is a complete surgical resection.1º National Comprehensive Cancer Network (NCCN) guidelines recommend considering adjuvant mitotane only in patients at a high risk of recurrence, which they define as those with positive margins, ruptured capsule, high-grade disease or large tumours.11 Other contemporary studies have questioned the benefit of adjuvant mitotane.12
Learning points
Cosmetic measures rather than a medical evaluation can lead to delay in the diagnosis of a virilising adrenocortical tumour.
Adrenal tumour is a rare but important cause for secondary amenorrhoea.
A pure testosterone-secreting adrenal tumour can rarely present with venous thrombus up to the right heart.
Coincidental macroscopic myelolipoma along with an adrenocortical carcinoma although very rare should be kept in mind especially when the imaging features are atypical or the mass is functional.
One must consider hormonal evaluation in patients with myelolipomas who are otherwise candidates for observation.
Adjuvant therapy for this patient was discussed at a multidis- ciplinary board meeting. The possibility of recurrence was juxta- posed against the demonstrated indolent course of disease in this patient, the lack of good quality evidence regarding adjuvant mitotane after complete surgical resection and drug toxicity with need for lifelong corticosteroid replacement. The board also took into account the need to import Mitotane at an extraordi- narily high cost to the patient (about 1500$ per month). Other forms of adjuvant therapies such as radiotherapy to the tumour bed and alternative systemic therapies were deemed inappro- priate. After a discussion of these issues, a decision was taken to observe the patient.
Contributors RMS and SS: planning, concept, design, case material collection, analysis, reporting, interpretation, revision, final approval, accountable for integrity and overall responsibility. HBK: planning, case material collection, interpretation, revision, final approval, accountable for integrity and overall responsibility. MDP: case material collection, interpretation, revision, final approval, accountable for integrity and overall responsibility.
Competing interests None declared.
Patient consent Obtained.
Provenance and peer review Not commissioned; externally peer reviewed.
C BMJ Publishing Group Ltd (unless otherwise stated in the text of the article) 2018. All rights reserved. No commercial use is permitted unless otherwise expressly granted.
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2 Kutikov A, Crispen PL, Uzzo RG. In: Pathophysiology, evaluation, and medical management of adrenal disorders. Wein AJ, ed. Campbell-Walsh Urology. 11th edn. Philadelphia: Elsevier, 2015:1528-76.
3 Derksen J, Nagesser SK, Meinders AE, et al. Identification of virilizing adrenal tumors in hirsute women. N Engl J Med 1994;331:968-73.
4 Klein DA, Poth MA. Amenorrhea: an approach to diagnosis and management. Am Fam Physician 2013;87:781-8.
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6 Al-Brahim N, Asa S. Myelolipoma with adrenocortical adenoma: an unusual combination that can resemble carcinoma. Endocr Pathol 2007;18:103-5.
7 Egbert N, Elsayes KM, Azar S, et al. Computed tomography of adrenocortical carcinoma containing macroscopic fat. Cancer Imaging 2010;10:198-200.
8 Tong A, Jiang J, Wang F, et al. Pure androgen-producing adrenal tumor: clinical features and pathogenesis. Endocr Pract 2017;23:399-407.
9 Laan DV, Thiels CA, Glasgow A, et al. Adrenocortical carcinoma with inferior vena cava tumor thrombus. Surgery 2017;161:240-8.
10 Libé R. Adrenocortical carcinoma (ACC): diagnosis, prognosis, and treatment. Front Cell Dev Biol 2015;3:45.
11 Kulke MH, Shah MH, Benson AB, et al. Neuroendocrine tumors (NCCN Guidelines) Ver 3.2017. www.NCCN.org (accessed 5 Dec 2017).
12 Postlewait LM, Ethun CG, Tran TB, et al. Outcomes of Adjuvant Mitotane after Resection of Adrenocortical Carcinoma: A 13-Institution Study by the US Adrenocortical Carcinoma Group. J Am Coll Surg 2016;222:480-90.
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