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Relato de Caso

Angiosarcoma of the lung

Angiossarcoma pulmonar

Mónica Grafino1, Paula Alves1, Margarida Mendes de Almeida2, Patrícia Garrido1, Direndra Hasmucrai1, Encarnação Teixeira1, Renato Sotto-Mayor1

DOI: http://dx.doi.org/10.1590/S1806-37562016000000193

ABSTRACT

Angiosarcoma is a rare malignant vascular tumor. Pulmonary involvement is usually attributable to metastasis from other primary sites, primary pulmonary angiosarcoma therefore being quite uncommon. We report a case of angiosarcoma with pulmonary involvement, probably primary to the lung, which had gone untreated for more than two years. We describe this rare neoplasm and its growth, as well as the extensive local invasion and hematogenous metastasis at presentation. We also discuss its poor prognosis.

Keywords: Hemangiosarcoma; Lung neoplasms; Sarcoma.

RESUMO

O angiosarcoma é um tumor vascular maligno. O envolvimento pulmonar é geralmente atribuído à metástase de outros sítios primários, sendo o angiossarcoma pulmonar primário extremamente raro. Relatamos um caso de angiossarcoma com envolvimento pulmonar, provavelmente primário no pulmão com mais de dois anos de evolução. Descrevemos seu crescimento e sua extensa invasão local e hematogênica na apresentação. Documentamos ainda seu mau prognóstico.

Palavras-chave: Hemangiossarcoma; Neoplasias pulmonares; Sarcoma.

INTRODUCTION

Angiosarcoma is a malignant endothelial cell tumor of vascular or lymphatic origin and accounts for approximately 2% of all soft tissue sarcomas.(1) The most common primary sites are the skin and the subcutaneous tissue of the head and neck.(2) Pulmonary involvement is almost always metastatic.(3) Primary pulmonary angiosarcoma is extremely rare, only a few cases having been reported.

CASE REPORT

A 78-year-old female nonsmoker had previously been examined, a CT scan of the chest having shown a left upper lobe pulmonary mass (Figure 1A). At that time, she underwent bronchoscopy with BAL and bronchial biopsy. The BAL fluid and the biopsy sample were both negative for neoplastic tissue. She subsequently dropped out of follow-up. Two years later, she was referred to our hospital with a six-month history of shortness of breath, dry cough, and weight loss. A chest X-ray and a chest CT scan (without contrast) identified a 10 × 7 cm lesion in the left upper lobe without forming cleavage plans with the aorta and the pulmonary artery (Figures 1B and 1C), with a small left pleural effusion and small mediastinal lymph nodes. An 18F-fluorodeoxyglucose positron emission tomography-CT (FDG PET-CT) scan (Figure 1D) showed in-creased metabolic activity in many organs, greatest in the mass in the upper left lobe, the maximum standardized uptake value (SUVmax) of which was 22. Metabolic activity was also increased in the mediastinal lymph nodes (SUVmax = 7), as well as in the right and left suprarenal glands (SUVmax = 16 for both); the aortic lumbar lymph nodes (SUVmax = 11); and the right inguinal lymph node (SUVmax = 10). In addition, there was a mesenteric focus, together with subcutaneous tissue nodes and multiple locations in bone.
 



The bronchoscopic examination revealed a mass occluding the left upper lobe bronchus (Figure 2), and a bronchoscopic biopsy was performed. Before the results of the tissue sample examination had been obtained, she developed right hemi-paresis and a new subcutaneous nodule arose. A CT scan showed multiple brain lesions. She was started on corticoster-oids. However, she showed no clinical improvement and brain radiotherapy was proposed.
 



The histological examination of the biopsy specimen showed a soft-tissue neoplasm with a sheet-like or enclosing cleft arrangement of spindle and epithelioid cells with prominent nucleoli, with some multinucleation; mitotic figures were conspicuous, as were extensive necrosis and hemorrhage (Figure 3A). Immunohistochemical staining of the tumor speci-men revealed that it was strongly positive for CD31 (Figure 3B), factor VIII-related antigen (Figure 3C), and vimentin; weakly positive for the nuclear transcription factor Fli-1 and cytokeratin AE1/AE3; and negative for CD34, desmin, and smooth muscle actin. Therefore, the histology and immunohistochemistry were both consistent with epithelioid angiosar-coma.
 



Two weeks after the histologic diagnosis had been made, the patient died. Her death was attributed to the progression of the disease, the brain metastases in particular.

DISCUSSION

Angiosarcoma in the lung usually represents metastasis from another primary site. Nevertheless, we believe that the case presented here was one of primary pulmonary angiosarcoma. The patient had a two-year evolution of a pulmonary mass that had gone unmonitored and untreated for more than two years. It seems apparent that the previous lesion corre-sponded to the pulmonary angiosarcoma that evolved and disseminated during that time. This case report also documents the behavior of a primary pulmonary angiosarcoma, which is characterized by insidious growth with extensive local inva-sion and hematogenous metastasis.(4)

Early diagnosis of pulmonary angiosarcoma is not common, because of its rarity and the low index of suspicion. Accord-ing to data in the literature, the average age of pulmonary angiosarcoma patients is 55.9 years (range, 23.0-82.0 years) and males are more often affected than are female.(5) Patients usually present nonspecific respiratory symptoms that include hemoptysis, cough, dyspnea, chest pain, and weight loss. On CT scans, primary angiosarcoma can be multifocal or can manifest as solitary lesions. (4,6,7) Imaging with PET can be useful in the diagnosis, staging,(8) and follow-up of patients with angiosarcoma. (9) In the case presented here, the FDG PET-CT scan confirmed its usefulness in identifying the regions and systems involved.

Biopsy and immunohistochemical analysis are essential for the diagnosis of angiosarcoma. The histological features can vary within and among cases. Abnormal, pleomorphic, malignant endothelial cells constitute the hallmark of angiosar-coma. Those cells can be rounded, polygonal, or fusiform, with or without an epithelioid appearance. In well-differentiated areas, abnormal endothelial cells form functioning vascular sinusoidal channels that are continuous with normal vascular channels. In patients with progressively more aggressive disease, the architecture becomes more chaotic, with less clear-ly defined vascular spaces. In poorly differentiated areas, the malignant endothelial cells form continuous monolayers, usually with an epithelioid morphology. An angiosarcoma typically expresses endothelial markers including factor VIII-related antigen, CD34, CD31, and Fli-1. Among those markers, factor VIII-related antigen is the most specific but the least sensitive. Positivity for CD31 is relatively specific and extremely sensitive, being detected in approximately 90% of the cases. In approximately 30% of the cases, angiosarcoma expresses cytokeratin.(10)

Due to the rarity of angiosarcoma, no standardized therapy regimen has been established, especially for primary pul-monary angiosarcoma. Patients with pulmonary angiosarcoma have been treated with radiotherapy,(9,11) surgical resec-tion,(4,9) immunotherapy,(4,6,11) chemotherapy,(4,6,9) or a combination of those.(4,6,9,11) Although none of those treatments have been shown to be effective, there have been reports of effective treatments for the condition,(4,9,11) especially in cases of localized disease. It has been proposed that the most effective treatment is surgery, which should be considered as early as possible for resectable tumors.(5) However, neoplasms are often inoperable at the time of diagnosis. Multimo-dality therapy, such as the combination of radiotherapy and immunotherapy (recombinant interleukin-2)(11) and that of surgery and chemotherapy,(4) has also proven to be effective. Chemotherapy with gemcitabine and docetaxel has been reported to produce a complete radiographic response.(9)

The prognosis of pulmonary angiosarcoma is poor, mortality within the first few months after clinical presentation, as occurred in the case presented here, approaching 100%.(4-7)

Angiosarcoma is a rare malignant neoplasm, and only a few dozen cases of primary pulmonary angiosarcoma have been reported in the literature. It is a diagnostic challenge for clinicians and pathologists. A high index of suspicion is essential to its early diagnosis and could improve its poor prognosis.

REFERENCES

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8. Treglia G, Cardillo G, Graziano P. A rare case of primary pulmonary epithelioid angiosarcoma detected by (18)F-FDG PET/CT. Clin Nucl Med. 2014;39(5):450-2. http://dx.doi.org/10.1097/RLU.0b013e318292f3b3
9. Wilson R, Glaros S, Brown RK, Michael C, Reisman D. Complete radiographic response of primary pulmonary angiosarcomas following gemcitabine and taxotere. Lung Cancer. 2008;61(1):131-6. http://dx.doi.org/10.1016/j.lungcan.2007.12.006
10. Travis WD, Brambilla E, Muller-Hermelink HK, Harris CC, editors. World Health Organization Classification of Tumours. Pathology and Genetics of Tumours of the Lung, Pleura, Thymus and Heart. IARC Press: Lyon; 2004
Kojima K, Okamoto I, Ushijima S, Yoshinaga T, Kitaoka M, Suga M, et al. Successful treatment of primary pulmonary angiosarcoma. Chest. 2003;124(6):2397-2400. http://dx.doi.org/10.1378/chest.124.6.2397

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