Anastomosing hemangioma: report of two renal cases and analysis of the literature

In 2009, Montgomery and Epstein described 6 peculiar vascular lesions, 4 in the kidney or perirenal tissue and 2 in the testis, anatomical sites which rarely harbor angiomatous tumors, with histologic features mimicking angiosarcoma and evidence of benign behavior [1]. Because they consisted of capillary-size vessels with prominent anastomosing pattern, the term “anastomosing hemangioma (AH) of the genitourinary tract” was proposed. Since then, more than 50 renal cases, more frequently encountered in the context of end-stage renal disease (ESRD), including bilateral and multifocal lesions and approximately a similar number of extra-renal cases involving various internal organs, bone and soft tissue have been reported, mostly as individual cases or in small series [2‐21].

Most lesions are accidental findings, frequently discovered during imaging studies for other tumors in the same, or other organs. All lesions are characterized histologically by anastomosing sinusoidal-like spaces, lined by a single file of CD31/CD34+ and D2-40- endothelial cells, some with hobnail morphology, supported by pericytes, accompanied by mild chronic inflammatory cells, without plasma cells and frequently associated with features of extra-medullary hematopoiesis [1‐21]. They are also negative for the presence of human herpes virus 8 (HHV8). Occasionally, periodic acid–Schiff, diastase-resistant-positive (PAS-D+) hyaline globules, a secondary cavernous component, or increased number of mast cells have been reported [1, 14, 18].

In the present study, two renal cases of AH will be reported in association with a comparative analysis of literature data including renal and extra-renal lesions.

Well differentiated angiosarcoma is probably the most important lesion that must be successfully discriminated against anastomosing hemangioma, a task more demanding in limited biopsy material [1]. It is the irregular architectural pattern and the focally infiltrative features, including fat entrapment and intravascular extension of anastomosing hemangioma that may raise the possibility of an aggressive lesion. However, the lack of significant endothelial nuclear atypia and pleomorphism, lack or rarity of mitosis, low proliferative index, absence of necrosis or broadly infiltrative pattern, as well as the regular pericytic accompanying layer and the absence of multilayering endothelial formations are important features for correct diagnosis. Extramedullary hematopoiesis, a frequent finding in anastomosing hemangioma is an additional clue [1, 21].

There are, also, histologic features of anastomosing hemangioma shared by other vascular tumors, which, therefore, may be included in the differential diagnosis. Hyaline globules, PAS-D-positive structures, believed to be secondary lysosomes, observed in 37% of renal AHs and 27% of non-renal AHs, may be encountered in other types of benign vascular tumors, Kaposi sarcoma and angiosarcoma [22]. However, in contrast to Kaposi sarcoma, all anastomosing hemangiomas are negative for HHV-8 and lack increased number of plasma cells and the characteristic slit-like pattern [1‐21]. Hobnailing of endothelial cells is, also, a feature of retiform hemangioendothelioma, a locally aggressive, but low grade vascular lesion and papillary intralymphatic angioendothelioma, known also as Dabska tumor, a rarely metastasizing neoplasm [22]. However, the first is characterized by a monomorphic arborizing vascular pattern and involves usually the skin and the subcutaneous tissue and the second shows characteristic intraluminal papillary tufts and positivity for the lymphatic endothelial marker D2-40, features not reported in anastomosing hemangioma [1‐21]. The characteristic anastomosing pattern, reminiscent of spleen vasculature must be distinguished from splenosis in deep seated lesions. However, the lack of organized lymphoid tissue and negativity for CD8 assist easily in the discrimination of these two possibilities. Also, since renal lesions can be adipocyte-rich and entrap renal parenchyma, vascular-rich lesions of the kidney, including angiomyolipoma and renal cell carcinoma may be included in the differential diagnosis, a task easily accomplished with the use of immunohistochemical markers including HMB45, Melan-A, cytokeratins and CD10.

It must be added that, while anastomosing hemangioma is emerging as a frequent type of renal vascular lesion, different types of angiomatous lesions including common capillary and cavernous hemangioma, papillary intravascular endothelial hyperplasia, arteriovenous malformations and angiosarcoma may, also, be observed in the kidney [2, 4, 7, 14, 22].

Although kidney is the single organ, harboring more than half of all anastomosing hemangiomas reported so far, recent literature shows that this type of vascular lesion is increasingly observed in various parenchymal organs, with soft tissue and bone cases representing the most frequent extra-renal site of involvement [1, 17‐21]. Although the number of the cases published is still relatively small for drawing definite conclusions, our review of the literature suggests that both renal and non-renal tumors show similar general epidemiological, clinical, macroscopic and histologic characteristics, (Fig. 3). Minor differences, like the younger average age in renal compared to non-renal cases may be explained by the frequent discovery of the lesion in surveys of end stage disease kidneys. Also, the more frequent association of renal cases with extramedullary hematopoiesis probably has to do with the frequent report of AH lesions in ESRD, since this association vanishes if we exclude ESRD-associated lesion. The more frequent presence of extramedullary hematopoiesis in ESRD-associated AH as compared with the rest of renal or exrarenal AHs may be due to pathogenetic factors of the preexisting renal disease, independent of AH development.

Anastomosing hemangioma pathogenesis remains unknown. Possible genetic alterations have not been studied. It is uncertain whether it is a clonal lesion, a true neoplasm, or a polyclonal, hyperplastic, deregulated vascular tissue. Also, the possible pathogenic role of ESRD, the more frequent associated clinical condition, remains obscure. It is highly improbable the occurrence of multifocal lesions exclusively in this context to be accidental. It is possible that additional pathogenetic factors contribute to the development of ESRD-associated AH. Whether, alternatively, a common factor between non-ESRD-associated and ESRD-associated cases, exaggerated in the last group contributes to the pathogenesis of anastomosing hemangioma remains to be studied.

Literature analysis provides strong evidence of the benign behavior of AH. This suggests that less aggressive treatment may be preferable. However, the minimalistic strategy (diagnostic biopsy and no treatment) should be weighed against the potential of significant tissue damage because of the growing lesion in the course of time [20, 21]. More informative imaging analysis may contribute to better decisions.

In conclusion, anastomosing hemangioma seems to be a distinctive type of vascular tumor with similar clinical, biologic and histologic characteristics in renal and non-renal involvement sites. Growing knowledge and better understanding of its pathology may contribute to more accurate diagnosis and optimal treatment choices.