Metastatic mesenteric dedifferentiated leiomyosarcoma: a case report and a review of literature

Leiomyosarcoma (LMS) represents between 10 and 20 % of all newly diagnosed soft tissue sarcomas [1]. It is classified based on anatomical site of origin, a factor that is important for outcome and prognosis [2]. Abdominal LMS is highly aggressive with an overall 5 year survival rate between 20 and 30 % [3]. Although histologically similar, the different anatomic variants of abdominal LMS have varying clinical behaviour and differ in prognosis [4]. Surgical resection is the cornerstone of curative treatment for localized disease if adequate margins are obtained [1, 5]. However, this is often not possible due to anatomical restrictions and large tumor size at diagnosis. Moreover, LMS tends to metastasize, most commonly to the lungs and liver. Unfortunately, there are no clear guidelines regarding the role of oncological treatment; neither in the primary nor metastatic setting [5]. In fact, almost all patients with metastatic disease are considered incurable and, thus, offered only palliative treatment.

Here, we present a patient with an abdominal LMS, specifically a mesenteric LMS. This is a rare malignancy, with only a few cases reported in the literature [6‐9]. The LMS was surgically resected with an R0 margin and no adjuvant oncological therapy was given. Unfortunately, the patient developed metastatic disease both to the liver and lungs. Histological evaluation of metastases revealed a highly malignant, pleomorphic sarcoma that resembled her primary tumor, but was not morphologically identical. It was categorized as dedifferentiated LMS [3, 10]. An aggressive multimodal therapeutic strategy was chosen, including staggered intensive chemotherapy tailored to the histological-subtype of the metastasis [11]. Presently, she is in complete clinical remission about 36 months following diagnosis of metastatic disease and without any demonstrable long-term side effects from chemotherapy.

Our patient is a 40 year old woman who had no significant medical history except for an appendectomy when she was 20 years-old. She presented with a two-month history of left sided abdominal pain accompanied by abdominal discomfort and distention. Additionally, she suffered from nausea and vomiting without any changes in stool pattern.

On physical examination, a large palpable mass was detected in the left quadrant. This mass was very tender upon palpation, but there were no signs of peritonitis. Blood tests revealed increased acute phase proteins and reduced haemoglobin but were otherwise unremarkable. Computerized tomography (CT) of the abdomen revealed an intraperitoneal tumor in the left quadrant measuring 8 × 7 cm axially and 7 cm craniocaudally (Fig. 1a). The tumor was closely related to the descending colon and small intestine and revealed heterogenous contrast enhancement with necrotic areas (Fig. 1b). There was no pelvic or retroperitoneal adenopathy, though some ascites was seen in the pelvis minor. A sarcoma was suspected and the patient was referred to the Section for Sarcoma at The Norwegian Radium Hospital.

About two weeks later, the patient was operated via a midline laparotomy. The tumor, which was partly adherent to the sigmoid mesocolon, was removed en bloc together with 15 cm of small intestine and colon. An antiperistaltic side-to-side-anastomosis was established at the splenic flexure as well as a small intestinal anastomosis about 120 cm proximal to the ileocaecal valve. No intraperitoneal metastases were seen, but tumor perforation to the peritoneal cavity and resulting bloody ascites was documented perioperatively. Despite this high risk for tumor relapse, no adjuvant therapy was given to the patient in line with guidelines regarding adjuvant therapy for abdominal LMS [5].

Histopathological investigations revealed that the resected tumor measured 11 × 9 × 7 cm, was well circumscribed and without infiltration of the small or large intestine. However, the tumor diffusely invaded the serosal surface. More than 50 % of the tumor showed necrosis macroscopically. Histologically, the tumor consisted of pleomorphic, spindle cells with eosinophilic cytoplasm and focally cigar shaped nuclei resembling a high grade, pleomorphic leiomyosarcoma. Up to 14 mitoses per 10 high power fields (1734 mm²) were found (French malignancy grade 3) (Fig. 2a, b). No invasion of blood vessels was seen. Immunohistochemical examination showed distinct, focal positivity for caldesmon, SMA and desmin, supporting the diagnosis of LMS (Fig. 2 c–e).

About three months after the operation, the patient experienced intermittent abdominal pain. No local tumor recurrence was seen on the CT of the abdomen, but multiple contrast enhancing lesions, typical for metastases, were seen in the liver, the largest measuring close to 3 cm (Fig. 3a). Chest CT revealed multiple round, well-circumscribed lesions in both lungs consistent with metastases (Fig. 3b). Biopsy of a liver lesion confirmed metastatic disease and showed only large, pleomorphic cells (Fig. 3a insert) consistent with a highly malignant pleomorphic sarcoma. After multidisciplinary assessment, we decided to treat the patient with 6 cycles of doxorubicin (50 mg/m², for the first treatment and 75 mg/m² for the other cycles) and ifosfamide (5 g/m²) with granulocyte colony-stimulating factor (G-CSF) given at 3 weeks interval. The patient showed a radiological response, exhibiting partial remission with a reduction in size and number of liver and lung metastases (Fig. 4). No new metastases were seen. Moreover, her side effects of treatment were surprisingly modest. Hence, to further enhance the chemotherapeutic effect, we added 5 cycles of weekly doxorubicin monotherapy (20 mg) and 6 cycles with gemcitabine 675 mg/m² days 1 and 8 with docetaxel 75 mg/m² on day 8 and G-CSF on day 9 (every three weeks). This induced a further reduction in the number and size of metastases in the liver and lungs. Due to side effects with water retention and muscle pain we switched to 3 cycles of high dose ifosfamide 12 g/m². Subsequent radiological assessment confirmed an almost complete radiological response to this intense schedule of chemotherapies (Fig. 4).

After a multidisciplinary discussion, we considered the remaining visible lesions in the lungs and liver to be resectable. Therefore, the patient underwent combined left hepatectomy in combination with radiofrequency ablation of metastatic foci in the right liver lobe, followed by a thoracoscopic wedge resection of metastasis in the right lung. The rationale of removing metastases was to decrease tumor burden, as this has been shown to prolong disease-free survival and probably also overall survival, similar to what is seen in patients who undergo resection of metastases limited to the lungs [12]. This combination of surgery and/or radiofrequency ablation of residual lesions was performed to improve chances of long-term clinical remission, as there was no evidence of tumor outside the liver and lungs. An immediate postoperative MRI of the abdomen showed three residual lesions in the liver which were not visible on the perioperative ultrasound and suspicious subcutaneous lesions near the midline laparotomy scar. A repeat laparotomy was then performed in which the abdominal scar was removed in combination with ultrasound/MRI-image fusion guided re-ablation of the liver. Histological evaluation of the aforementioned lesions revealed only fibrotic changes with no viable tumor cells. Postoperatively, the patient received 2 cycles of weekly doxorubicin 20 mg due to a strong desire from the patient. Post operative CT of the abdomen and thorax revealed only postoperative changes in the liver and lungs. A complete outline and scheduling of the various chemotherapies are displayed in Fig. 5.

Five months after surgery for metastatic disease, the patient developed abdominal pain and constipation. CT of the abdomen and thorax revealed only postoperative changes. Moreover, upper and lower endoscopy was unremarkable. A contrast study showed no pathology, only stenosis of the small intestine, which was dilatated, and the patient showed symptomatic relief after laxative therapy. The patient is presently in clinical remission, 36  months following diagnosis of metastatic disease.

To our knowledge, this is the first report of a patient with metastatic mesenteric LMS who developed complete clinical and radiological remission without any demonstrable long-term side effects from chemotherapy, after receiving multimodal therapy including an unconventional histological-subtype-tailored chemotherapy comprising 3–4 regimens, surgical resection and radiofrequency ablation of metastatic foci. Given the rarity of mesenteric leiomyosarcoma and lack of guidelines regarding oncological therapy, we suggest that multimodal therapy including aggressive histological-subtype tailored chemotherapy can result in complete remission under the guidance of a multidisciplinary team.