Radiation-induced angiosarcoma masquerading as recurrent carcinoma cervix - A diagnostic challenge

Case history

A 56 year old female was diagnosed with focally keratinising grade 3 squamous cell carcinoma for which she had undergone hysterectomy elsewhere and was referred to our institute for radiotherapy. She underwent external beam radiotherapy of the pelvis (Telecobalt, total 3771 cGy in 25 fractions) and intravaginal brachytherapy (30 Gy). After a latency period of 6 years the patient presented with a lower abdominal wall nodule in the midline.

Imaging

CT pelvis showed a nodular heterogeneously enhancing soft tissue lesion in the lower anterior abdominal wall in the midline, 3 cm superior to the pubic symphysis. No recurrent lesion was seen in the vault.

Cytology

PAP smear from vaginal vault showed no malignant cells. FNA of abdominal wall nodule was reported as Positive for malignancy with a differential diagnosis of -

Recurrent squamous cell carcinoma with abdominal wall metastasis.

Post radiation sarcoma.

Histopathological examination

A wide local excision of the abdominal wall nodule was done and sent for histopathological examination.

Gross findings

Skin with an underlying grey tan tumour with ill defined borders measuring 4x3.5x1.8 cms.

Microscopy

Sections showed highly pleomorphic spindle shaped cells arranged in sheets and nodules infiltrating into the subcutaneous tissue. Areas of necrosis, haemorrhage and dilated vascular spaces were also seen. Overlying skin showed features of seborrheic keratosis. Differential diagnosis on the basis of morphology alone included -

Metastatic squamous cell carcinoma.

Endometrial stromal sarcoma.

Malignant melanoma.

Post radiation sarcomas viz angiosarcoma.

Immunohistochemistry (IHC)

The tumour cells showed strong CD34, CD31 immunoreactivity, strong Cyclin D1 nuclear staining, weak D2-40 and CD10 cytoplasmic staining. Ki67 proliferative index was 30%. The tumour cells were negative for panCK, EMA, ER, PR, p16, p40, p63, HMB45 and S100 which excluded the diagnosis of metastatic squamous cell carcinoma, endometrial stromal sarcoma and malignant melanoma. Following IHC a diagnosis of post-radiation angiosarcoma was given.

Radiation-induced angiosarcoma

Radiotherapy is an independent risk factor for the development of angiosarcoma.^[3] The median interval between irradiation and diagnosis of angiosarcoma was 6 years in one study.^[4] Although the association between radiotherapy and subsequent angiosarcoma is best described for breast cancer therapy, it is not exclusive to breast lesions and can occur in patients with cancers of cervix, uterus, ovary, melanoma, Hodgkin’s lymphoma.^[2], ^[4] There have been around 22 cases of post radiation angiosarcoma reported following irradiation for the treatment of carcinoma cervix. The most common sites of involvement of angiosarcoma following irradiation for carcinoma cervix include abdominal wall, gluteal region, vaginal vault, small intestine and rarely the mesentery and serosa of appendix.^[5], ^[6] The histological spectrum of angiosarcoma varies from well to poorly differentiated lesions with vascular channels.^[4] The poorly differentiated angiosarcomas pose a challenge in diagnosis because the vascular channels are difficult to identify. Therefore immunohistochemistry becomes an important adjunctive procedure in identifying these lesions.^[1] Angiosarcomas typically express endothelial markers including von Willebrand factor, CD34, CD31, Ulex europaeus agglutinin 1, and vascular endothelial growth factor (VEGF).^[3] Laminin and type IV collagen can also be used to accentuate the vascular channel formation.^[1] D2-40 immunostaining is seen in a subset of post radiation angiosarcomas.^[7] Also MYC over expression was found to be a hallmark of secondary angiosarcoma.^[7] In our case neoplastic cells expressed endothelial cell markers like CD34, CD31 and D2-40 with over expression of Cyclin D1 which is an unusual finding previously reported in one case of uterine angiosarcoma.^[8]