The undifferentiated carcinoma that became a melanoma: Re-biopsy of a cancer of an unknown primary site: a case report

Cancer of unknown primary site (CUP) accounts for approximately 1 to 5 % of all cancers but has a dismal prognosis of approximately 10 to 20 % 1-year survival and in Australia is the sixth cause of cancer death [1‐4]. Depending on the patient series, up to 40 % of patients with CUP are diagnosed as having metastasis in their lymph nodes, while the remaining patients present with metastasis in their internal organs [5, 6]. In a large series of CUP in various anatomical regions, patients with an affected lymph node showed a wide survival span; patients presenting with affected inguinal lymph nodes had a median survival of 18 months and patients affected intra-abdominally had a median survival of only 4 months [7]. Thus CUP is a very heterogenous entity, where histopathological examination, immunohistochemical profiling, and molecular profiling of the tumor are necessary to improve treatment and survival of patients with these tumors.

The complexity and unusual features of the history of this 62-year-old woman with a fast-growing mass in her left inguinal area, has taught us a lesson that may be important to share with oncologists treating this patient population.

A 62-year-old woman of Norwegian ethnicity, previously healthy, presented in September 2012 with a large fast-growing nodal mass in her left groin; a computed tomography (CT) scan showed a 62 mm tumor infiltrating the subcutis. A clinical examination did not reveal any other pathological glands or any skin lesions. An magnetic resonance imaging (MRI) of her pelvis showed a solitary tumor, and subsequent CT of her thorax and abdomen, mammography, and endoscopy could not reveal or indicate the primary location of the tumor; in addition, the tumor markers we use in our screening were all within normal range: carcinoembryonic antigen (CEA), CA125, CA15-3, CA19-9, neuron-specific enolase (NSE), and chromogranin A (CgA). In November 2012 the tumor was still regarded as operable and surgery was performed. On macroscopic examination, the tumor was a 57 mm solid tumor. Histopathological examination revealed a tumor composed of malignant epithelioid cells, which on immunohistochemical examination stained positive for cytokeratin (CK) AE1/AE3 (diffuse), CK7 (focally), CD10, vimentin, and epithelial membrane antigen (EMA; scattered tumor cells). S100 was positive in scattered cells with dendritic features and possibly in a few scattered tumor cells. Nearly 100 % of the tumor cells were positive for Ki67/MIB1. The cells were negative for BerEP4, CK20, CK5/6, p63, thyroid transcription factor 1 (TTF1), synaptophysin, chromogranin, estrogen and progesterone receptors, human melanoma black 45 (HMB45), melan A, leukocyte common antigen (LCA), desmin, myogenin, smooth muscle actin (SMA), and CD30 (Fig. 1). We screened for actionable targets and molecular genetic analysis was negative for KRAS and synovial sarcoma marker, translocation t(X;18), but revealed BRAF V600E mutation. In the final pathology report, the tumor was classified as a metastasis from an undifferentiated carcinoma.

Our patient had postoperative complications with infection and lymphatic leakage, subsequent CT scanning and positron emission tomography (PET)-CT showed masses to be growing deeper in her pelvis, which could not be removed (Fig. 2).

We decided to give paclitaxel with carboplatin (AUC5) every 3 weeks, which is a standard treatment for CUP and after four courses the masses went into complete remission. Consolidation radiotherapy was performed April to May 2013, 2×(25 to 50) Gy. Our patient was in very good general condition during all the treatment period: World Health Organization (WHO) performance status (PS) grade 0. The remission lasted for 18 months to July 2014, when multiple, fast-growing subcutaneous nodules evolved within and near the surgical wound and radiation field and distally on her left thigh. Moreover, multiple small metastases were seen in both her lungs. One subcutaneous nodule was extirpated for histopathological analysis, which revealed a tumor with a cellular morphology and cellular growth pattern similar to the tumor resected 18 months earlier. The tumor cells were, as previously, negative for BerEP4, CK20, CK5/6, P63, HMB45 and melan A, but surprisingly CK AE1/AE3 was now negative and S100 strongly positive in all tumor cells (Fig. 3). The tumor cells were closely studied, both initially when the first report was made and on reevaluation, and conspicuous pigment was not detected.

The BRAF V600E mutation persisted, strongly indicating that the tumor was of the same origin but probably another clone, or a transformation from the primary tumor after chemoradiation with an unusual or aberrant expression profile for a melanoma.

Due to the previous good results with chemotherapy, one course of paclitaxel and carboplatin was tried. However, the nodules grew more aggressively, and chemotherapy was discontinued in favor of a BRAF inhibitor, dabrafenib, that showed a brief response of 2 months, and subsequently vemurafenib was administered resulting in progressive disease. Combined treatment with a mitogen-activated protein kinase (MEK) inhibitor was not introduced in Norway at that time point. In the meantime, ipilimumab was approved for use in melanomas in Norway and in December 2014 she was offered this treatment. After four cycles of ipilimumab there was a complete response in her skin and her lungs, with no reported side effects (Fig. 4).

Today, 4 years and 4 months after primary diagnosis of aggressive CUP and 2 years and 6 months after metastatic melanoma was diagnosed in the re-biopsy, she is radiologically and clinically cancer-free (Fig. 5).

Currently, with the advent of targeted treatment and immunotherapy, identifying molecular subtypes may be of benefit for several cancer types. Immunotherapy, by ipilimumab, a fourth-line treatment, induced a complete and durable response after recurrence and progression on chemoradiotherapy and two BRAF inhibitors. Moreover this patient had clinical benefit with paclitaxel-carboplatin on what was perceived as an undifferentiated carcinoma, which became resistant when transformed to a S100-positive melanoma.

In conclusion, molecular screening in the primary biopsy and re-biopsy of the recurrence may be of clinical value in CUP, where evaluations with a broad spectrum of immunohistochemical and molecular analyses are necessary.